Net loss
per share is computed using the weighted average number of shares of common
stock outstanding. Common equivalent shares from stock options and warrants are
excluded as their effect is anti-dilutive.
Income
taxes are accounted for under the asset and liability method. Deferred tax
assets and liabilities are recognized for future tax consequences attributable
to differences between the financial statement carrying amounts of existing
assets and liabilities and their respective tax bases and operating loss and tax
credit carryforwards. Deferred tax assets and liabilities are measured using
enacted tax rates expected to apply to taxable income in the years in which
those temporary differences are expected to be recovered or settled. The effect
on deferred tax assets and liabilities of a change in tax rate is recognized in
operations in the period that includes the enactment date. Deferred tax assets
are reduced to estimated amounts expected to be realized by the use of a
valuation allowance.
ASC 740,
Income Taxes, clarifies
the accounting for uncertainty in income taxes by prescribing a two-step method
of first evaluating whether a tax position has met a more likely than not
recognition threshold and second, measuring that tax position to determine the
amount of benefit to be recognized in the financial statements. ASC 740 provides
guidance on the presentation of such positions within a classified statement of
financial position as well as on derecognition, interest and penalties,
accounting in interim periods, disclosure, and transition. ASC 740 was adopted
by the Company effective January 1, 2007. The Company recognized
a $252,827 increase in the liability for unrecognized tax benefits that are
related to research and development credits, which was accounted for as a
reduction to the January 1, 2007 balance of the deferred tax asset and
related valuation allowance. The entire amount of this unrecognized tax benefit,
if recognized, would result in an increase to the deferred tax asset valuation
allowance, and would not have an impact on the effective tax rate.
The
Company files its income tax returns in the U.S. federal jurisdiction and in
Florida. With few exceptions, the Company is no longer subject to federal or
state income tax examinations by tax authorities for years before
2003.
|
4.
|
Fair
Value of Financial Instruments
|
ASC 820,
Fair Value Measurements and
Disclosures, defines fair value,
provides guidance for measuring fair value and requires certain disclosures.
This standard discusses valuation techniques, such as the market approach
(comparable market prices), the income approach (present value of future income
or cash flow), and the cost approach (cost to replace the service capacity of an
asset or replacement cost). The standard utilizes a fair value hierarchy that
prioritizes the inputs to valuation techniques used to measure fair value into
three broad levels. The following is a brief description of those three
levels:
Level 1. Observable inputs
such as quoted prices in active markets;
Level 2. Inputs, other than
the quoted prices in active markets, that are observable either directly or
indirectly; and
Level 3. Unobservable inputs
in which there is little or no market data, which require the reporting entity
to develop its own assumptions.
The
Company does not have any assets or liabilities measured at fair value on a
recurring basis at September 30, 2009. The Company did not have any fair value
adjustments for assets and liabilities measured at fair value on a nonrecurring
basis during the nine months ended September 30, 2009.
|
5.
|
Stock
Options Expense During the 3rd Quarter,
2009
|
During
the 3rd quarter, no stock options were issued and there were 2,340,000 options
forfeited due to employee layoffs, employee separations and Board member
departures. On August 13, 2009, the compensation committee approved the
acceleration of the vesting of certain outstanding option awards, the
vesting of which was tied to our share price reaching certain levels in the
future. Option awards previously made to Mr. David Hirsch,
our President and Chief Executive Officer, Dr. Jeffrey Hillman, our Chief
Science Officer and certain other Company employees were impacted by
the accelerated vesting of these options (433,333 shares for Mr. Hirsch, 500,000
shares for Dr. Hillman, 563,333 for other Company employees). Following
the acceleration of vesting by the compensation committee, Mr. Hirsch's grant of
options to acquire 500,000 shares of our common stock at $0.49
per share is now fully vested and exercisable (including
the 433,333 shares impacted by the acceleration of vesting), Dr. Hillman's
grant of options to acquire 700,000 shares of our common stock at $0.85 per
share is now fully vested and exercisable (including the 500,000 shares
impacted by the acceleration of vesting). All other terms of the prior
option awards, including the share amounts covered by the options and
exercise prices remained the same.
From
January, 1, 2009 to the date of this filing, 1,736,665 stock options previously
granted have vested and 2,340,000 have been forfeited. Stock option
compensation expense of $250,690 was recorded and is a non-cash
expense. This amount is included in research and development and
selling, general and administrative expenses in the accompanying statement
of operations.
|
6.
|
Common
Stock Issued During the 3rd Quarter,
2009
|
In
September, the Company issued 500,000 shares of restricted common stock to
Media4Equity LLC (“M4E”) pursuant to an agreement whereby Media4Equity will
provide consulting services to us with respect to national media exposure of
placements of print and radio features. The agreement was made
effective on September 3, 2009 and also requires us to pay a monthly fee to M4E
of $10,000 during the three year term of the agreement, subject to certain
termination rights. The shares of common stock have a fair market
value of $115,000 based on a price of $0.23 per share. This amount is
included in selling, general and administrative expenses in the accompanying
statement of operations.
In July, we entered into a short term
note payable for $70,023 with an interest rate of 5.75% to finance our directors
and officers liability insurance. This note matures on May 24, 2010.
In
August, we repaid a short term note in full to an accredited investor in the
amount of $100,000 plus outstanding accrued and unpaid interest
thereon. The note was issued on April 15, 2009 and had a maturity
date of April 15, 2011 with an interest rate of 15% per
annum.
|
8.
|
Outstanding
Warrants and Stock Options
|
As of the
date of this filing there are approximately 7,127,778 warrants outstanding and
there are approximately 2,330,000 stock options have been granted that have not
been forfeited. The total number of outstanding warrants and
unexercised stock options is 9,457,778. If all warrants and stock
options were exercised, the total number of outstanding shares would be
approximately 100,324,676. This share amount exceeded the number of
shares of common stock authorized in our Articles of Incorporation as of
September 30, 2009. We held a shareholder meeting on October 28, 2009
and our shareholders voted to amend our Articles of Incorporation to increase
our authorized shares of common stock to 300,000,000.
|
9.
|
Entry
into a Material Definitive
Agreement
|
On June
29, 2009, the Company entered into and consummated a private placement of equity
and debt financing pursuant to a Securities Purchase Agreement (the “Securities
Purchase Agreement”) with an accredited investor. Pursuant to the
terms of the Securities Purchase Agreement the Company issued 50,000,000 shares
of its Common Stock to the Koski Family Limited Partnership (“KFLP”) and
warrants to the KFLP to acquire 1,000,000 shares of Company common stock at an
exercise price of $0.10 per share in exchange for $4,000,000, the payment of
which consisted of the following: $1,500,000 in cash at closing and $2,500,000
pursuant to a non-interest bearing promissory note providing for five
consecutive monthly installment payments of $500,000 commencing July 31,
2009. The promissory note was recorded as a stock subscription
receivable and shown as a reduction to shareholders’ equity. KFLP
also provided a secured loan of $1,000,000 to the
Company. The loan is secured by substantially all of the Company’s
assets (excluding receivables) and bears interest at the rate of Prime plus 4.0%
which is payable quarterly. The principal of the loan is due in five
years. The warrants expire in five years and are immediately
exercisable.
As a
result of the transaction the board of directors believes there was a change of
control of the Company with the KFLP acquiring a controlling interest of
approximately 56.6 % of our outstanding voting common stock. Two
Koski family members, Robert C. Koski and Christine L. Koski were appointed to
our Board of Directors. In addition, following the transaction, the
KFLP also has the ability to consent to the selection and appointment of two
outside directors.
The KFLP was also granted registration
rights in connection with any offerings by the Company of its
shares. Such registration rights require the Company to include a
certain amount of the KFLP shares in a Company offering determined based upon
15% of the shares to be publicly offered.
In connection with, and as a condition
to the Securities Purchase Agreement, the purchasers, including George Hawes our
largest shareholder prior to this transaction, under that certain securities
purchase agreement dated June 12, 2008, (the “Hawes Agreement”) entered into
waiver and release agreements with us. In addition, such individuals
waived and relinquished any special rights they possessed pursuant to agreements
with the Company, including, but not limited to, (i) rights of first refusal
(ii) antidilution regarding future equity sales and (iii) covenants regarding
secured lending. In connection with such waivers and releases,
warrants to acquire 3,220,000 shares of our common stock at an exercise price of
$1.30 per share that were previously issued under the Hawes Agreement were
subject to the right of exchange for new replacement warrants to acquire the
same number of shares under the same terms except for a change in the exercise
price from $1.30 to $0.75.
In
addition to the above, as a further condition to the consummation of the
transaction contemplated by the Securities Purchase Agreement the Company was
required to obtain satisfactory arrangements with three main creditors for
reductions in the amounts payable by the Company to such
creditors. As of June 29, 2009 the agreed upon reductions in accounts
payable with such creditors amounted to $707,674 in aggregate and the reductions
were conditioned upon prompt payment of the remaining balances owed to such
creditors after taking into account the reductions agreed to by such
creditors. Further reductions to amounts owed to creditors were
agreed to during the three months ending September 30, 2009 in the amount of
$46,268. The total amount of reductions for the nine months ending
September 30, 2009 was $753,942 which was recorded as a gain on extinguishment
of payables and reported as Other Income.
On October 28, 2009 at our annual
shareholder meeting our proposal to amend the Company’s articles of
incorporation to increase the authorized shares of common stock from 100,000,000
to 300,000,000 was approved by shareholders and the amendment to our articles of
incorporation was filed with the Florida Department of State. In
addition, at our annual meeting our shareholders also approved a second
amendment to our Amended and Restated 2002 Stock Option and Incentive Plan to
increase the shares available for grant thereunder from 5,000,000 to
12,500,000. The Company reviewed for subsequent events through
November 13, 2009.
ITEM 2. MANAGEMENT’S DISCUSSION AND ANALYSIS
OF FINANCIAL CONDITION AND RESULTS OF OPERATIONS
The
following information should be read in conjunction with the Financial
Statements, including the notes thereto, included elsewhere in this Form 10-Q.
This discussion contains certain forward-looking statements that involve risks
and uncertainties. Our actual results and the timing of certain events could
differ materially from those discussed in these forward-looking statements as a
result of certain factors, including, but not limited to, those set forth herein
and elsewhere in this Form 10-Q.
Overview
We are a
multi-faceted biopharmaceutical company focused on the discovery,
development and commercialization of a variety of products and
technologies. We are currently transitioning from a company
with a historic focus on research and development to a company with increased
focus on immediate and long term commercialization.
We
generate revenue through the sale of our consumer healthcare
products. We are optimistic about the ongoing level of interest
we are experiencing with our lead branded consumer healthcare products at this
time. As our Probiora3 and EvoraPlus manufacturing, marketing and selling
initiatives progress, we expect to continue to experience a higher level of
overall expenses associated with such efforts as well as with the continued
development of our technologies. We expect the current increases in our
expenses to continue into the near future as we fully implement the
initiatives we have underway.
Our goal
is to achieve positive operational cash flow as quickly as possible by
allocating most of our resources on the commercialization or monetization of
technologies that can provide revenues in the near term. This
initially means that our first priority will be to focus the bulk of our
resources on the Consumer Healthcare Division. We will also seek
opportunities in Biomarker Discovery that either provide up-front money or
fee-for-service arrangements. Concurrently, we expect to seek
additional capital to accelerate the development of our
technologies. While we are pursuing these priorities, we expect to
simultaneously make incremental progress in Antibiotics, Biomarker Discovery and
Biologics until they reach an inflexion point and can be
monetized. The pace of any incremental progress we may achieve,
however, will be based on the amount of our limited available capital resources
we are able to allocate to each individual technology. If we are able
to obtain sufficient additional capital, the pace of progress would be expected
to increase. Once we begin to monetize our current technologies, we will
also be able to commit greater capital to further research and development
alternative technologies that are in alignment with our vision and strategic
goals.
Financial
Strategy
Since our
inception, we have funded a significant portion of our operations from the
public and private sales of our securities. Furthermore, we have not earned
significant revenue from operations during the last two years. Until
recently most of our revenue has been from sponsored research agreements and
various governmental grants. We will require additional capital to fund our
business operations and we continue to seek additional capital to effectuate our
business plans. The further development, testing and
commercialization of our technologies, individually and in the aggregate, are
expected to be costly to undertake and complete and will require additional
capital over and above what we currently have available to us. Our current
available capital limits our ability to fully develop our technologies. We
expect to allocate our limited capital resources to the development of our
technologies while we continue to explore additional capital raising
opportunities. There can be no assurances that such additional capital will be
available to us or on favorable terms or at all. The time periods for the
expected continued development of our technologies have been extended from those
previously indicated by us from time to time due primarily to our insufficient
capital position. The time periods for expected developments could
also change in the future depending on the progress of our ability to negotiate
a partnering arrangement, as well as our efforts to raise additional
capital.
Although
we have started to earn revenue from the sales of our Consumer Healthcare
products and technologies, revenue to date has been modest. Our
objective is that the revenue from Consumer Healthcare products will be able to
fully and sufficiently support the continued operations of the Consumer
Healthcare Products Division. We anticipate additional purchase
orders and/or revenue from the sale of EvoraPlusTM, our
oral probiotic for adults, during the remainder of the current calendar year and
we are optimistic about the prospects for Teddy’s PrideTM, our
oral probiotic for the companion pet market. We also anticipate that,
we will have opportunities to partner with or license some of our technologies
to larger global companies. We hope to be able to negotiate upfront
payments in connection with these potential partnerships and/or
licenses.
Operational
Strategy
We have a
number of products and platforms. These products and platforms are structured
and viewed by us as four distinct Divisions:
(1)
Consumer Healthcare, which consists of ProBiora3TM, the
EvoraPlusTM,
Teddy’s PrideTM and
EvoraKidsTM as well
as the LPT3-04TM weight
loss agent;
(2)
Biomarker Discovery (formerly referred to by us as “Diagnostics”), which
consists of the PIVIATTM and
PCMATTM
platforms;
(3)
Antibiotics, which consists of our lead antibiotic, MU 1140, and the DPOLTTM
lantibiotic synthesis platform; and
(4)
Biologics (formerly referred to by us as “Replacement Therapy”), which consists
of our SMaRTTM
Bacterial Replacement Therapy technology.
Because
we have limited capital and human resources, we cannot pursue commercialization
and further development of each and every technology that we own
simultaneously. As such, we have decided to pursue a strategic course
that focuses the majority of our resources towards those technologies that
present the best opportunity to generate revenue for the Company in the
short-term. The allocation of resources is determined by us on a
case-by-case basis and is subject to periodic review. Currently, we
are rolling out products in our Consumer Healthcare Division and most of our
resources are being deployed in support of that endeavor. However, we
expect to continue to commit our remaining available resources to our other
three divisions. As the Consumer Healthcare Division matures and
begins to generate meaningful revenue and is able to become self-sustaining, we
anticipate being able to allocate greater resources to the other
divisions. We believe that each of our products and platform
technologies addresses potentially large market opportunities.
Consumer
Healthcare - Operational Highlights
We
believe we are making progress in our Consumer Healthcare
Division. Set forth below are some of the highlights of our
progress.
Large Retailers - The
Drugstore & Big Box Retail Channels:
We are in
discussions with several large drugstore and big box retailers regarding our
Consumer Healthcare products. The process for product adoption by
large retailers typically has five essential phases; (1) the incorporation of a
product into a retailer's "planagram", (2) the assignment of a "vendor ID" to
the vendor and the establishment of connectivity, typically using electronic
data interchange, (3) the transmission and receipt of an initial order, (4) the
fulfillment and delivery of the initial order, and (5) the subsequent re-order
by the retailer to replenish inventory. In early November 2009, we
received written confirmation that EvoraPlusTM would
be included in the planagram of one of the nation's largest drugstore
chains. In connection with our efforts with this drugstore chain, we
have established a vendor ID. We currently anticipate we will receive
an initial order from this potential customer sometime in the first quarter of
2010 and that the order would be fulfilled and delivered shortly
thereafter. However, this retailer can, at its sole discretion,
change its planagram at any time. Therefore, there can be no
assurances that we will in fact receive the anticipated initial
order. Also, should we receive, fulfill and deliver an initial order
from this prospective customer, there can no assurances that we will receive
subsequent re-orders. We expect to be coming to decision points with other
prospective retail customers in the coming weeks and we are optimistic about our
prospects.
Grocery Store
Channel:
We are in
discussions with several grocery store chains including some of the largest
grocery chains in the United States. During the last several weeks we
received orders from several large regional grocery store chains. We
are optimistic about the potential opportunities for of our products in this
channel, there can be no assurances, however, that our products will be
successfully received by the marketplace through this channel.
Private Label
Channel:
Our first
private label customer, Garden of Life, formally launched its first private
label product containing ProBiora3 from Oragenics. Garden of Life has
since placed subsequent orders for their private label product using ProBiora3
and they have placed initial orders for a similar private label product for the
pet market. It is also anticipated that they will begin rolling out a
children's product in early 2010.
Trade
Show:
In
mid-November, we exhibited our products at the Supply-Side West trade show,
which is one of the largest raw material / ingredient shows in the
world. We experienced a substantial amount of interest from a number
of company representatives in attendance at the show and we are optimistic about
the potential for future business arising from such initial
interest.
Media
Exposure:
In July,
a segment on EvoraPlus appeared on Fox News throughout the United
States. This segment was followed by a subsequent segment that aired
on November 4, 2009 on Fox News. We believe this media coverage was
beneficial for us in our efforts to gain market traction and acceptance of our
consumer healthcare products.
International
Interest:
We have
experienced an increase in interest and demand for our consumer products
internationally. To address such interests, we have retained a
Director of International Sales and Marketing with substantial international
marketing experience and we remain optimistic about potential future
developments from this channel.
Technology
Descriptions and Objectives
Consumer
Healthcare
The
specific goal for our Consumer Healthcare division is to rapidly and effectively
commercialize ProBiora3TM and
LPT3-04TM.
ProBiora3TM
(Probiotics). ProBiora3TM
contains three naturally occurring, live microorganisms that help maintain
dental and oral health when administered to the host in adequate amounts. The
use of yogurt containing live
Lactobacillus cultures is an example of a probiotic
application. We will market ProBiora3TM under
self-proclaimed GRAS (“Generally Recognized As Safe”) status, which will
expedite our marketing efforts because it relieves us of the need for extensive
regulatory oversight. Two sets of subjects completed our ProBiora3TM human
study in 2006, and we believe the results confirmed that the product is safe for
human use and demonstrated a substantial effect of ProBiora3TM in
reducing the levels of specific bacteria in the mouths of young, healthy adult
subjects.
We have
developed a bifurcated strategy whereby we have established a separate brand for
the active ingredient, ProBiora3TM, and we
have developed the three house brand names below. Our house
brands contain different ratios, or blends, of the three natural strains
contained in ProBiora3TM and
potentially different delivery mechanisms such that each product will be
tailored to the needs of specific markets. The products currently in production
or the product pipeline are:
a product with equal weight of all
three strains that is optimally designed for the general consumer
market.
a product that has a mixture
which focuses primarily on promoting breath freshening and tooth whitening in
companion pets.
a product that has a greater
concentration of the Probiora3 strain designed to promote dental health, which
is more of an issue for children.
Other
house products with different formulations and delivery systems are also
planned. EvoraPlusTM was the
first product to market. EvoraPlusTM is a
probiotic mint packaged in a 60 unit box with four 15 dose blister packs. The
intended usage is to take one mint twice a day after brushing. As such, one box
is designed to include a one-month’s supply of EvoraPlus TM. We
have completely outsourced the manufacturing and fulfillment
processes. Our manufacturer is a large, Good Manufacturing Practices
certified manufacturer with the ability to scale production to meet our expected
needs. We recently announced the launch of Teddy’s PrideTM. Teddy's
PrideTM, our
product for the companion pet market, comes in a powder form and is contained in
a small pale that holds a 60-day supply and is administered by sprinkling a
specific dose on the pet's food once per day.
Marketing
Progress. We believe we are starting to gain acceptance with
our first product, EvoraPlusTM and we
are starting to see traction with Teddy's PrideTM, our
product for the companion pet market. Although our progress has been
somewhat slower than anticipated for a variety of reasons, we remain optimistic
about the future prospects for these products.
Our
initial efforts to drive sales of our house products through the production of a
one-minute television spot have been delayed. Initial testing of our
spot ad was not satisfactory. However, we expect to re-format our
spot ad with a new version that we anticipate will be more successful in
generating demand for our products. However, our ability to purchase
adequate media time may be limited due to a lack of available capital
resources.
We
believe we have made significant progress in our efforts to generate interest in
the sale or licensing of ProBiora3TM as an
active ingredient. We continue to engage in meaningful discussions
with several large, global consumer products companies who are interested in
incorporating the technology into products already in the stream of
commerce. Many of these products are well known and used by millions
of people on a daily basis.
Despite
our efforts to sell our house products and commercialize ProBiora3TM, there
can be no assurances that we will meet our timeline for commercialization or
that the product will meet the sales projections we have
anticipated.
LPT3-04TM. LPT3-04TM is a
small molecule weight management agent for which we filed a U.S. patent
application on April 5, 2006 to protect our intellectual property rights to the
agent and its analogs. As a natural substance, LPT3-04TM is
orally available, and we believe it has an excellent safety and tolerability
profile. As with ProBiora3TM,
LPT3-04TM would
fall under the self-proclaimed GRAS status and we will be able to market
products containing the technology without the burden of substantial regulatory
oversight in most, if not all, of the markets in which we plan on introducing
products.
Our
strategy for our LPT3-04TM is
similar to that of our oral probiotic in that we plan on developing a bifurcated
strategy where we market the technology as an active ingredient for licensing or
private labeling and we develop a house brand to market to consumers directly
and through mass retail. We plan on developing several products under the house
brand that will vary by formulation and delivery mechanism. We will also develop
a product for the Pet Market since obesity is a problem that is present in the
animal markets as well. Design work for the house brand is in progress and we
anticipate having it completed by year’s end. We may also market directly to
Medical Professionals and Veterinary Offices.
We are
currently in the process of developing an adequate delivery system for
LPT3-04TM. We
anticipate that this process will be complete by the end of 2009. Once this has
been accomplished, we plan on initiating subsequent and more comprehensive human
trials, which, once commenced, should last approximately four to five
months. If the results are satisfactory, we will initiate marketing
efforts immediately thereafter; however there can be no assurances that the
results of our contemplated clinical trials will prove successful.
Biomarker
Discovery
The goal
of our Biomarker Discovery unit is to utilize the PIVIATTM and
PCMATTM
platforms to identify and secure intellectual property rights to gene targets
associated with the natural onset and progression of infections, cancers and
other diseases in humans, animals, and agricultural products. We believe these
platforms provide a number of profitable business models from which to realize
value.
PIVIATTM and
PCMATTM
Proteomics-based In Vivo Induced Antigen
Technology (PIVIATTM) is a
platform technology that enables rapid identification of novel targets for use
in the diagnosis and treatment of human infectious diseases. The method is
faster, more cost effective, and more sensitive than other methods currently in
use to identify such targets. As an example, a recent tuberculosis project has
yielded 44 novel targets for
Mycobacterium tuberculosis that are currently being analyzed for their
use in vaccine and diagnostic strategies.
We are
currently in discussions with various collaborators to look at specific
diagnostic markers and to develop vaccines utilizing our PIVIATTM gene
targets.
Proteomics-based
Change Mediated Antigen Technology (PCMATTM) is a
platform technology that was derived from and greatly extends the potential
applicability of PIVIATTM. This
technology rapidly identifies proteins (and their genes) that are expressed when
a cell undergoes any sort of change. PCMAT TM has
been used to identify proteins of plants that are expressed when it becomes
infected. Such genes are excellent targets for manipulation to increase the
resistance of the plant to infection. It has also been used to identify novel
proteins of human bowel cells that are expressed when the cell undergoes
transformation to a cancerous cell. Such proteins are excellent targets for new
diagnostics and therapeutic strategies. PCMATTM has the
potential to study an extraordinary range of medical and agricultural
applications.
The first
major commercial effort that we have undertaken utilizing the PCMATTM
platform has been to extract genetic targets from tissue samples containing
colorectal cancer. Colorectal cancer affects millions of people worldwide. The
current “Gold Standard” in the detection of colorectal cancer is the use of a
colonoscopy. Due to the invasive nature and cost of colonoscopies, patient
compliance is low. As such, many cases of bowel cancer go undetected until the
cancer has reached an advanced stage. Using the PCMATTM
diagnostic platform, we have discovered what we believe to be unique genetic
markers that appear during the earliest stages of colorectal cancer. As
announced last summer, we entered into a Collaboration Agreement with a major,
global diagnostics company regarding our gene targets for various stages of
colorectal cancer that we discovered using the PCMATTM
platform. Although we are highly optimistic about this Collaboration Agreement,
there can be no assurances that this Agreement will result in a diagnostic test
that will be marketed to appropriate health care professionals, nor can there be
any assurance that upon further examination, the diagnostic company will elect
to use these markers. We anticipate that the diagnostics company will
finish validation by the end of the fourth quarter, 2009, at which point they
will likely make a decision on whether to include our targets into a diagnostic
test. If they choose to do so, our agreement provides for the payment
of milestone fees upon the filing of a 510K application with the
FDA.
We have
identified a number of diseases that hold the greatest promise for future
revenues from a diagnostic test using gene targets. We plan on utilizing our
platforms to discover gene targets for these diseases. We anticipate that we
will begin this process by the end of the fourth quarter, 2009.
Antibiotics
The
cornerstone of our Antibiotics Division is the DPOLTTM
(Differentially Protected Orthogonal Lantionine Technology) Synthetic Chemistry
Platform, which affords us the ability to synthesize a unique class of
antibiotics known as lantibiotics.
DPOLTTM (Differentially
Protected Orthogonal Lantionine Technology). DPOLTTM is a
novel organic chemistry synthesis platform that will enable large scale, cost
effective production of clinical grade MU1140 and 50 other known lantibiotics.
Over the past 80 years, efforts to devise methods to investigate the usefulness
of this class of antibiotics have met with uniform failure. DPOLTTM is
anticipated to lead to 6-10 new antibiotics with novel mechanisms of action.
This represents a substantial potential pipeline of antibiotics to replace ones
that are currently failing due to the development of bacterial
resistance.
As
mentioned earlier, we announced the successful synthesis of an antibiotic using
our proprietary DPOLTTM
technology. The molecule belongs to a class of antibiotics called Lantibiotics
that were first discovered over 80 years ago. Although there are now over 50
different Lantibiotics known, this is the first report of a cost-effective
method for making one in sufficient amounts and with sufficient purity to enable
comprehensive testing and commercial viability.
This
initial antibiotic is very closely related to our lead antibiotic, MU 1140,
which has the potential to treat a wide variety of infections, including those
caused by MRSA and other drug resistant Gram positive bacteria. Domestically,
hospital borne infections alone have been on the rise, with an estimated
two-million patients contracting dangerous infection annually leading to
one-hundred-thousand deaths. Preliminary studies indicate that MU 1140 may be
the first new antibiotic in 35 years for the treatment of tuberculosis. In
addition to MU 1140, this technology will allow us to synthesize all 50 of the
known lantibiotics and to conveniently modify their structures in order to
improve their usefulness as antibiotics for the treatment of infectious
diseases. In effect, DPOLTTM will
provide a much needed pipeline of antibiotics at a time when drug resistant
bacteria are on the rise.
As a
first step in further development, the Company has retained a leading contract
manufacturer to refine and scale-up GMP production of the synthetic MU 1140
analog to achieve sufficient quantities for it to be fully tested for regulatory
approval. It is estimated that the regulatory process will take a minimum of
three years before this drug could become available. Other lantibiotics will
follow as they are developed and tested.
Last
fall, we announced that we were successful in using the DPOLTTM
platform to synthetically produce an analog of the MU 1140
molecule. We are now in the process of having the synthetic version
of MU 1140 scaled to production by Almac Sciences, one of Europe’s largest and
most reputable peptide manufacturers. This endeavor is more than half way
complete and we anticipate the process of scaling MU 1140 should take an
additional four to five months to complete. This, in turn, should
provide us with enough synthetic MU 1140 to conduct preclinical
testing. Once preclinical testing is complete, we will seek
partnership and/or licensing opportunities with major pharmaceutical companies
with the intent to fund subsequent phase I, II & III FDA clinical
trials.
Biologics
Our
Biologics Division is centered on SMaRTTM
Replacement Therapy, our product for dental caries (tooth decay).
SMaRTTM Replacement
Therapy. SMaRTTM
Replacement Therapy™ is a professional/Rx product intended for the prevention of
dental caries (tooth decay). Dental caries remain a major health problem
afflicting a majority of the population in the United States and worldwide.
Lactic acid production by the oral bacterium Streptococcus mutans has long
been known to be integral to the pathogenic process for dental caries. Oragenics
Inc.’s replacement therapy technology replaces the indigenous, acid-producing
S. mutans with a
SMaRTTM
effector strain, which has been genetically modified so as not to produce the
acid associated with caries formation.
The
wild-type S mutans
originally used for construction of the SMaRT strain was isolated from a
human subject and was carefully selected based on its ability to produce the
antibiotic, MU1140. MU1140 has been shown to kill all other strains of S. mutans that it has been
tested against. The SMaRTTM
effector strain was generated by transforming this wild-type parent strain with
recombinant DNA that introduced a large deletion mutation in the gene for
lactate dehydrogenase (LDH) eliminating the strain’s ability to produce lactic
acid.
Our
SMaRTTM
effector strain for the replacement therapy of dental caries has the following
advantages over existing decay-prevention technologies: (1) a single treatment
regimen involving application of SMaRTTM cells
onto patients’ tooth surfaces using a cotton tipped swab for five minutes has
the potential to provide lifelong protection against most tooth decay; (2) the
possibility of deleterious side-effects are negligible since the effector strain
is essentially identical to the microorganism which is found universally on the
teeth of humans; (3) minimal patient education and compliance is
required.
SMaRTTM
Replacement Therapy offers the potential for lifelong protection against dental
caries following a single, painless application of a genetically modified
bacterial strain to the surfaces of the teeth. This technology is currently
approved for FDA phase 1b clinical trials. At present, our plans are to initiate
phase 1b trials once adequate financing has been achieved. We
anticipate the cost of conducting phase 1b to be under $1M. We also
anticipate that phase 1b trials will take less than six months to
complete. Once phase 1b trials have been completed and safety has
been established, we plan on seeking partnerships and/or licensing arrangements
with major pharmaceutical companies. It would be our intent to use
these partnerships and/or licensing arrangements to fund subsequent clinical
trials, which we anticipate will be costly and may take several years to
complete.
Global
Expansion
Although
we are domiciled in the United States, we believe there are opportunities and
advantages in utlilizing foreign talent and markets for a variety of our
products and technologies. While we have established a subsidiary in
Mexico and embarked upon other global strategic iniitiatives, we are currently
reviewing and evaluating our global strategic plans given our limited
capital resources and the costs associated with such efforts and the expected
benefits.
Critical
Accounting Estimates
Our
discussion and analysis of our financial condition and results of operations are
based upon our financial statements, which have been prepared in accordance with
accounting principles generally accepted in the United States of America. The
preparation of financial statements in accordance with accounting principles
generally accepted in the United States of America requires us to make estimates
and assumptions that affect reported amounts and related disclosures. We
consider an accounting estimate to be critical if it requires assumptions to be
made that were uncertain at the time the estimate was made; and changes in the
estimate or different estimates that could have been made could have a material
impact on our results of operations or financial condition. Our financial
statements do not include any significant estimates other than stock based
compensation that would have a material impact on our results of operations or
financial condition.
New
Accounting Pronouncements
In
October 2009, the FASB issued ASU No. 2009-13, “Revenue Recognition (ASC
Topic 605) — Multiple-Deliverable Revenue Arrangements.” ASU
No. 2009-13 addresses the accounting for multiple-deliverable arrangements
to enable vendors to account for products or services (deliverables) separately
rather than as a combined unit. This guidance establishes a selling price
hierarchy for determining the selling price of a deliverable, which is based on:
(a) vendor-specific objective evidence; (b) third-party evidence; or
(c) estimates. This guidance also eliminates the residual method of
allocation and requires that arrangement consideration be allocated at the
inception of the arrangement to all deliverables using the relative selling
price method. In addition, this guidance significantly expands required
disclosures related to a vendor’s multiple-deliverable revenue arrangements. ASU
No. 2009-13 is effective prospectively for revenue arrangements entered
into or materially modified in fiscal years beginning on or after June 15,
2010 and early adoption is permitted. A company may elect, but will not be
required, to adopt the amendments in ASU No. 2009-13 retrospectively for
all prior periods. Management is currently evaluating the requirements of ASU
No. 2009-13 and has not yet determined the impact on the Company’s
financial statements.
In August
2009, the FASB issued ASU 2009-05, “Fair Value Measurements and Disclosures (ASC
Topic 820) — Measuring Liabilities at Fair Value” (“Update 2009-05”).
Update 2009-05 provides clarification regarding valuation techniques when a
quoted price in an active market for an identical liability is not available in
addition to treatment of the existence of restrictions that prevent the transfer
of a liability. Update 2009-05 also clarifies that both a quoted price in an
active market for an identical liability at the measurement date and the quoted
price for an identical liability when traded as an asset in an active market
(when no adjustments to the quoted price of the asset are required) are
Level 1 fair value measurements. This standard is effective for the first
reporting period, including interim periods, beginning after issuance. Adoption
of Update 2009-05 did not have a material effect on Company’s financial
statements.
Three
Months Ended September 30, 2009 and 2008
We had
$199,675 in revenues in the three months ended September 30, 2009 compared with
$100,000 of revenues in the same period in 2008. The revenue was generated from
$ 85,372 of EvoraPlus product sales and $114,303 of grant revenue recorded
during the quarter. In the quarter, deferred grant revenue was
recorded in the amount of $110,267. This amount represents the NSF
SBIR Phase II grant for the small peptide antibiotic synthesis program using our
proprietary DPOLTtm in the
amount of $86,374 and the University of Florida grant to identify
disease-specific proteins expressed during citrus greening using our proprietary
PCMAT in the amount of $23,893.
Cost of
sales of $65,461 were recorded in the three months ended September 30, 2009
compared with no cost of sales in the same period in 2008. These
costs include the production and manufacture of our Consumer Healthcare products
totaling $33,627. Cost of sales also includes shipping and processing
expenses of $21,200. This amount includes one-time costs to relocate
inventory from our order fulfillment center in New York to a new fulfillment
center in California, costs to enhance our order processing services and higher
shipping expenses due to an increase in our manufacturing vendor supply
chain. Cost of sales also includes scrap expense of $10,634 which
represents the replacement of inventory in July with our new improved EvoraPlus
product.
Our third
quarter operating expenses consist of Research and Development (R&D)
expenses and Selling, General and Administrative (SG&A)
expenses. Our operating expenses increased by 27.1% to $1,593,353 in
the three months ended September 30, 2009 from $1,253,200 in the same period in
2008. R&D expenses decreased 15.1% to $427,541 in the three
months ended September 30, 2009 from $503,685 in the same period in
2008. Even though total R&D expenses declined, stock options
expense increased by $93,887 as a result of the acceleration of vesting of
options. Compared to the same period in 2008, R&D expenses
reflect reductions in salaries and fringe costs as a result of the decrease in
staff by $54,950, reduced consulting fees by $51,967, lower royalty expenses by
$32,108, lower supplies of $26,536 and reductions in legal patent expenses of
$17,428. S,G&A expenses increased 55.5% to $1,165,812 in the
three months ended September 30, 2009 from $749,515 in the same period in 2008.
The increase over the prior period was due to advertising expense of $226,752
which includes the issuance of common stock to Media4Equity with a fair market
value of $115,000. Stock option expense increased by $92,299 as a
result of the acceleration of vesting of certain outstanding options and the
addition of sales staff and associated expenses by $193,582 which was offset by
a decrease in investor and public relation expenses totaling
$111,402.
Other
income of $22,131 increased by $7,048 for the three months ended September 30,
2009. Other income included the gain on extinguishment of payable of
$46,268 due to the reduction in expenses owed to several creditors following the
June 29, 2009 financing transaction. Interest expense for the three
months ended September 30, 2009 totaling $24,412 represents interest expense for
the short term note with an accredited investor that was repaid during the
quarter, and accrued interest expense on the long term note with the Koski
Family Limited Partnership which was part of the June 29, 2009 financing
transaction. Interest income decreased by $14,806 in the three months
ended September 30, 2009 compared to the same period in 2008. This
decrease is primarily due to the Company’s reduced cash position during the
third quarter resulting from use of cash to pay amounts owed following the June
29, 2009 financing transaction with the KFLP.
We
incurred net losses of $1,437,008 and $1,138,117 during the three months ended
September 30, 2009 and 2008, respectively. The increase in our net loss was
principally caused by the increase in sales and marketing expenses, acceleration
of options expense and the issuance of common stock to
Media4Equity.
Nine
Months Ended September 30, 2009 and 2008
We had
$365,842 in revenues in the nine months ended September 30, 2009 compared with
$225,000 in revenues in the same period in 2008. EvoraPlus product
revenues totaled $151,539 and grant revenues were $214,303. Grant
revenue was generated from the National Science Foundation (NSF) Phase II grant
for work utilizing the Company’s proprietary DPOLT TM
technology in the amount of $176,108 and with the University of Florida to
identify disease-specific proteins expressed during citrus greening in the
amount of $38,195.
Cost of
sales of $100,844 were recorded in the nine months ended September 30, 2009
compared with no cost of sales for the same period in 2008. Our cost
of sales represents costs in connection with the production and manufacture of
our Consumer Healthcare products totaling $60,163, shipping and processing costs
of $26,714 and scrap costs in the amount of $13,967.
Our
operating expenses increased by 60.8% to $5,291,500 in the nine months ended
September 30, 2009 from $3,290,848 in the same period in
2008. R&D expenses decreased by 4.6% to $1,407,516 in the nine
months ended September 30, 2009 from $1,474,725 in the same period in
2008. R&D expenses declined due primarily to the reduction in
stock options expense of $179,829. S,G&A expenses increased
113.9% to $3,883,984 in the nine months ended September 30, 2009 from $1,816,123
in the same period in 2008. The increase can be attributed to the
Company’s hiring of a new management and new sales team totaling $522,353 in
salaries and fringe benefits. Consulting fees for investor relations
increased by $578,982 due to the need for several investment firms to assist
with our cash raising activities. Legal fees increased by $568,042 to
support rights offering initiative, the Alternext Paris exchange and services to
expand our global business in Mexico and France. Marketing and
advertising costs increased by $377,867 for our EvoraPlus and Teddy’s Pride
products.
Other
income of $739,920 increased by $698,937 for the nine months ended September 30,
2009. Other income included the gain on extinguishment of payable of
$753,942 due to the reduction in expenses owed to three creditors that was
agreed to in connection with the June 29, 2009 financing transaction plus
additional creditor reductions realized during the 3rd quarter. Gain
on the sale of equipment for the nine months ended September 30, 2009 totaling
$11,274 represents the sale of equipment no longer needed to support on-going
Mutacin research. Interest expense for the nine months ended
September 30, 2009 totaling $25,915 is primarily interest expense for the short
term note with an accredited investor and interest expense for the long term
note with the Koski Family Limited Partnership which was part of the June 29,
2009 financing transaction. Interest income decreased $28,617 in the
nine months ended September 30, 2009 from $29,413 during the same period in
2008. This decrease is primarily due to the Company’s reduced cash position and
cash settlements made following the Koski Family investment.
We
incurred net losses of $4,286,582 and $3,024,865 during the nine months ended
September 30, 2009 and 2008, respectively. The increase in our net loss was
principally caused by the increase in S,G&A expenses.
Liquidity
and Capital Resources
Since our
inception, we have funded our operations through the sale of equity securities
in private placement and our initial public offering, the sale of equity
securities and warrants in private placements, debt financing and
grants. For the first nine months of 2009, we have received $200,000
of restricted funds as part of the $500,000 NSF Phase II grant to advance
development of its small peptide antibiotic synthesis program using our
proprietary DPOLTtm. This
federal grant will support studies focused on the synthesis and testing of our
lead antibiotic, MU 1140. During the 3rd quarter, we have received
$124,570 from the University of Florida under the prime grant with
the Florida Citrus Production Advisory Council.
Our
operating activities used cash of $4,413,596 for the nine months ended September
30, 2009 and $2,331,553 for the nine months ended September 30,
2008. Our working capital deficit was ($10,273) as of September 30,
2009. Cash used by operations in the nine months ended September 30, 2009
resulted primarily from our net loss from operations of $4,286,582.
Our
investing activities provided an increase in cash of $18,926 during the nine
month period ended September 30, 2009 as compared with a net decrease in cash of
$9,158 for the same period ending September 30, 2008.
Our
financing activities for the nine months ended September 30, 2009 provided net
cash increase of $3,953,704. This increase was attributable to the
purchase of $4,000,000, less stock subscription receivable of $1,000,000, of our
common stock by the KFLP; the loan from the KFLP in the amount of
$1,000,000. Additional details of our financing activities are
provided below:
Warrant Exercises – Q1 2008 –
On August 7, 2007, we closed on $1,171,591 in equity based
financing. We issued a total of 4,600,000 shares of restricted common stock and
warrants to acquire 4,600,000 shares of common stock in a private placement to
accredited investors. The shares were sold to accredited investors at $0.25 per
share, except that per AMEX requirements, our former CEO, Dr. Ronald Evens
acquired his shares at $0.44 per share, which was the closing share price on
August 7, 2007. Each warrant to purchase shares of common stock is
exercisable at the price of $0.58 per share. The unexercised warrants expired on
August 8, 2008 (the “August 2007 Warrants”). On January 31, 2008 we
amended the August 2007 Warrants, to reduce the exercise price to $0.44, which
was the fair market value on the date of the amendment for a designated period
of time (from January 28, 2008 to February 29, 2008). In
February 2008, amended Warrants, of 4,536,364 were issued upon exercise at the
amended exercise price resulting in additional working capital proceeds to us of
$1,996,000. The remaining unexercised August 2007 warrants expired unexercised
on August 8, 2008.
Private Placement, June 2008 –
On June 12, 2008, our Securities Purchase Agreement with accredited
investors became binding and we closed on $2,600,000 in equity based financing
with net proceeds of $2,515,000. We issued a total of 5,777,778 shares of
restricted common stock in the private placement. The shares were sold to
accredited investors at $0.45 per share. Each participating investor
also received warrants to purchase shares of common stock at the price of $1.30
per share. One warrant was issued for each share of common stock issued for a
total of 5,777,778 shares that may be acquired upon exercise of the warrants.
The warrants are exercisable and expire May 30, 2013. In connection
with, and as a condition to the June 29, 2009 financing transaction described
below, the purchasers, including George Hawes our largest shareholder prior to
this transaction, under that certain securities purchase agreement dated June
12, 2008, (the “Hawes Agreement”) entered into waiver and release agreements
with us. In addition, such individuals waived and relinquished any
special rights they possessed pursuant to agreements with the Company,
including, but not limited to, (i) rights of first refusal (ii) antidilution
regarding future equity sales and (iii) covenants regarding secured
lending. In connection with such waivers and releases, warrants to
acquire 3,220,000 shares of our common stock at an exercise price of $1.30 per
share that were previously issued under the Hawes Agreement were subject to the
right of exchange for new replacement warrants to acquire the same number of
shares under the same terms except for a change in the exercise price from $1.30
to $0.75. We intend to use the proceeds from the exercise of the
warrants, if any, for working capital and general corporate
purposes.
Line of Credit – On October
20, 2008, the Company obtained from Signature Bank of New York, a revolving line
of credit in the amount of up to $1,000,000, for the purpose of providing
working capital to the Company. We did not draw on this line and on
January 21, 2009, this line of credit was terminated by us.
Short
Term Notes Payable
In March
2009, the Company
entered into a short term note payable for $53,087 with an interest rate of
5.75% to finance product liability insurance. This note matures on
January 10, 2010. At September 30, 2009 the balance due was
$15,926.
On April
15, 2009 we entered into a loan agreement with an accredited investor
for a short term note in the amount of $100,000. On August 21,
2009 we paid the short term note and outstanding accrued interest in
full. The note included an interest rate of 15% per annum
and its maturity date was April 15, 2011. In connection with this
borrowing we also issued warrants to acquire 100,000 shares of our
common stock at an exercise price of $.50 per share and such warrants are
exercisable for five years.
On August
6, 2009 the Company entered into a short term note payable for $70,023 with an
interest rate of 5.75% to finance directors and officers liability
insurance. This note matures on May 24, 2010. At September
30, 2009 the balance due was $56,019.
Other
Financings
On May 4,
2009 and June 10, 2009, we borrowed $32,556 and $13,100, respectively,
from Dr. Jeffery Hillman, our founder, Chief Science Officer and
director. These borrowings were to be repaid upon demand by Dr. Hillman,
were unsecured and did not bear interest. The proceeds from
these borrowings were used to purchase inventory for our Consumer
Health Care products division. On June 29, 2009 the aggregate amount
of these obligations of $45,656 were repaid by us in full through the issuance
of 456,564 shares of our common stock at a price of $.10 per share, which was
the closing price of our common stock on June 29, 2009.
Grants
On
February 15, 2008, we were awarded a two year NSF SBIR Phase II grant to
advance development of our small peptide antibiotic synthesis program using the
Company’s proprietary DPOLTtm. This
federal grant supports studies focused on the synthesis and testing of our lead
antibiotic, MU 1140. While the grant will total $500,000, to date we have
received $425,000 of these restricted funds during the last two
years.
On
September 1, 2009 we received a grant funding from the University of Florida
under the prime grant with the Florida Citrus Production Advisory
Councilin the amount of $124, 570. The purpose of the University of
Florida grant is to identify disease-specific proteins expressed during citrus
greening using our proprietary PCMAT technology.
Private Placement, June 2009 –
On June 29, 2009, we successfully entered into and consummated a private
placement of equity and debt financing pursuant to a Securities Purchase
Agreement with an accredited investor. Pursuant to the terms of the
Securities Purchase Agreement the Company issued 50,000,000 shares of its Common
Stock to the Koski Family Limited Partnership (“KFLP”) and issued warrants to
the KFLP to acquire 1,000,000 shares of Company common stock at an exercise
price of $0.10 per share in exchange for $4,000,000, the payment of which
consisted of the following: $1,500,000 in cash at closing and $2,500,000
pursuant to a non-interest bearing promissory note providing for five
consecutive monthly installment payments of $500,000 commencing July 31, 2009
and the KFLP provided a secured loan of $1,000,000 to the
Company. The loan is secured by substantially all of the Company’s
assets (excluding receivables) and bears interest at the rate of Prime plus 4.0%
which is payable quarterly. The principal of the loan is due in five
years. The warrants expire in five years and are immediately
exercisable.
Immediately
following the closing of the aforementioned June 29, 2009 financing transaction,
our Chief Executive Officer Mr. Hirsch was awarded a bonus of $100,000 which was
paid in 1,000,000 shares of our common stock at a price per share of
$0.10. In addition, we issued 250,000 shares of our common stock to our
newly appointed Chief Financial Officer for deferred compensation we owed to him
and we issued 343,750 shares of our common stock to another employee for
deferred compensation we owed to him.
As of
September 30, 2009, included in our accounts payable for the period were amounts
that we owed to (i) our Chief Science Officer for compensation incurred that we
were not able to pay and (ii) former independent directors for prior meeting
fees. The deferred aggregate amount owed to our Chief Science Officer
and former directors as of September 30, 2009 was $60,250 and consisted of
$26,250 and $34,000, respectively. The deferred amounts are expected
to be settled by us in future periods. The deferrals of payments to our
officer and former directors did not reduce our expenses, but served to preserve
our limited cash resources at this time to the extent necessary to maintain our
operations.
Our business is based on
commercializing entirely new and unique technologies, and our current business
plan contains a variety of assumptions and expectations that are subject to
uncertainty, including assumptions and expectations about manufacturing
capabilities, clinical testing cost and pricing, continuing technological
improvements, strategic licensing relationships and other relevant matters.
These assumptions take into account recent financings, as well as expected but
currently unidentified additional financings. We have
experienced losses from operations during the last three fiscal years and have
an accumulated deficit of $24,279,117 as of September 30, 2009. The
net loss from operations for the first nine months of 2009 was
$4,286,582. Cash used in operations for the nine months ended
September 30, 2009 was $4,413,596. As of September 30, 2009, our
principal source of liquidity was $724,967 of cash and cash equivalents and
$1,000,000 in stock subscriptions receivable from the KFLP. These
operating results occurred while developing and attempting to commercialize and
manufacture products from entirely new and unique technologies. Our business
plan requires significant spending related to our commercialization efforts,
clinical testing expenditures, as well as conducting basic
research. These factors place a significant strain on our limited
financial resources and adversely affect our ability to continue as a going
concern. Our ultimate success will likely depend on our ability to
continue to raise capital for our operations.
Our
capital requirements for the remainder of 2009 will depend on numerous factors,
including the initial success of our commercialization efforts and of our
research and development, the resources we devote to develop and support our
technologies and the success of pursuing strategic licensing and funded product
development relationships with external partners. Subject to our ability to
generate revenue and cash flow from our Consumer Healthcare products division
and our ability to raise additional capital including through possible joint
ventures and/or partnerships, we expect to need to incur substantial
expenditures to further commercialize or develop each of our technologies
including continued increases in costs related to research, preclinical testing
and clinical studies, as well as significant costs associated with being a
public company. We will require substantial funds to conduct research and
development and preclinical and Phase I clinical testing of our licensed,
patented technologies and to develop sublicensing relationships for the Phase II
and III clinical testing and manufacture and marketing of any products that are
approved for commercial sale. We must generate additional capital resources to
enable us to continue as a going concern. Our plans include seeking financing,
alliances or other partnership agreements with entities interested in our
technologies, or other business transactions that would generate sufficient
resources to assure continuation of our operations and research and development
programs as well as seeking equity financing.
Our
future success depends on our ability to continue to raise capital and
ultimately generate revenue and attain profitability. We cannot be certain that
additional capital, whether through selling additional debt or equity securities
or obtaining a line of credit or other loan, will be available to us or, if
available, will be on terms acceptable to us. If we issue additional securities
to raise funds, these securities may have rights, preferences, or privileges
senior to those of our common stock, and our current stockholders may experience
substantial dilution.
While we
continue to focus on our products and technologies, we may not have sufficient
capital resources to market our products and complete the development of our
technologies. We had a working capital deficit at September 30, 2009
of ($10,273). While we believe our currently available cash and cash
equivalents of $1,724,967 (which includes the stock subscription receivable
from KFLP of $1,000,000) is sufficient to enable us to continue to operate
during the remainder of 2009, we do not have sufficient capital to operate
beyond that time. During this time, if additional capital is not
raised, we would need to significantly adjust our current plan of operations
until we are able to acquire additional funding. In addition, we
expect to continue to explore strategic alternatives that may be available to us
and our technologies.
ITEM
4T. CONTROLS AND PROCEDURES
Evaluation
of Disclosure Controls and Procedures
Management's
evaluation of the effectiveness of the Company's disclosure controls and
procedures as defined in Rules 13a-15(e) and 15d-15(e) of the Exchange Act was
performed under the supervision and with the participation of our senior
management, including our Chief Executive Officer and Chief Financial Officer.
The purpose of disclosure controls and procedures is to ensure that information
required to be disclosed in the reports filed or submitted under the Exchange
Act is recorded, processed, summarized and reported within the time periods
specified in the SEC's rules and forms, and that such information is accumulated
and communicated to management, including our Chief Executive Officer and
Principal Financial Officer, to allow timely decisions regarding required
disclosures.
As
previously disclosed under Item 4T, Controls and Procedures, in
our Quarterly Report on Form 10-Q for the quarter ended June 30, 2009,
management concluded that the Company's internal control over financial
reporting was not effective because of the existence of material weaknesses in
internal control over financial reporting. Based on those material weaknesses,
our Chief Executive Officer and Principal Financial Officer have concluded that,
as of the quarter ended September 30, 2009, disclosure controls and procedures
were not effective. Nevertheless, based on a number of factors, including the
performance of additional procedures by management designed to ensure the
reliability of our financial reporting, management believes that the financial
statements in this Quarterly Report on Form 10-Q fairly present, in all material
respects, our financial position, results of operations, and cash flows for the
periods presented in conformity with GAAP.
For the
period referenced above, the matters involving internal controls and procedures
that our management identified and considered to be material weaknesses were:
(1) lack of a functioning audit committee due to a lack of a majority of
independent members and a lack of outside directors on our board of directors,
resulting in ineffective oversight in the establishment and monitoring of
required internal controls and procedures; (2) inadequate staffing and
supervision that could lead to the untimely identification and resolution of
accounting and disclosure matters and failure to perform timely and effective
reviews, (3) limited documentation of our system of internal control, (4)
insufficient personnel to employ segregation of duties; (5) lack of formal
written policies and procedures for accounting and financial reporting with
respect to the requirements and application of U.S. GAAP and SEC disclosure
requirements and related documentation; (6) deficiencies in our material
technology systems and (7) ineffective controls over period end financial
disclosure and reporting processes. In addition, our corporate governance
activities and processes are not always formally documented or adequately
communicated. Specifically, decisions made by the board to be carried out
by management should be documented and communicated on a timely basis to reduce
the likelihood of any misunderstandings regarding key decisions affecting our
operations and management. These deficiencies and weaknesses were
largely attributable to the significant lack of available financial resources
and corresponding personnel reductions experienced by us during the quarter
ended September 30, 2009.
Management’s
Remediation Initiatives
Although
management has not fully remediated the material weaknesses mentioned above,
management believes progress has been made during the quarter ending September
30, 2009. We engaged
a consulting firm specializing in Sarbanes-Oxley Section 404 compliance to
assist us in the implementation of internal controls for financial reporting and
disclosure and our remediation efforts. During the quarter the
consulting firm completed an initial entity level control evaluation (ELC),
control documentation and gap analysis for financial
close and reporting. Following such evaluation management prepared a
remediation plan to be implemented during the coming
months. Management also expects to review various facets of our
information processing system, such as cash disbursements, sales and billing,
cash receipts and other procedures. We continue to evaluate and address these
weaknesses to ensure adherence to our policies, completeness of reporting,
segregation of incompatible duties and compliance with generally accepted
accounting principles; and we intend to continue to monitor and evaluate these
and other factors affecting our internal controls as our available liquidity
permits. Until such time, our internal controls over financial
reporting may be subject to additional material weaknesses and deficiencies that
we have not yet identified. Management is responsible for and is committed to
achieving and maintaining a strong control environment, high ethical standards,
and financial reporting integrity. This commitment continues to be
communicated to and reinforced with our employees.
In an
effort to remediate the identified material weaknesses and
other deficiencies and enhance our internal controls, we plan to
initiate other measures as sufficient funds become available to
us. For example, we expect to increase our personnel resources and
technical accounting expertise within the accounting function and to create
a position to segregate duties consistent with control objectives. In addition,
we also plan to appoint one or more outside directors to our board of
directors who shall be appointed to an audit committee resulting in a fully
functioning audit committee who will undertake the oversight in the
establishment and monitoring of required internal controls and procedures
such as reviewing and approving estimates and assumptions made by
management as funds become available to us. Management believes that the
appointment of one or more outside directors, who shall be appointed to a
fully functioning audit committee, will remedy the lack of a functioning
independent audit committee and a lack of outside directors on our
Board.
We
anticipate that these initiatives will take time to fully implement following
the period of insufficient financial resources we experienced. While we received
additional funding on June 29, 2009, we still require funding and our existing
capital resources may not be sufficient to address our operational needs or to
fully address the weaknesses we have identified. We cannot guarantee
that any measures we take will remediate the material weaknesses that we have
identified, or that any additional material weaknesses will not arise in the
future. In addition, our size prevents us from being able to employ
sufficient resources to enable us to have adequate segregation of duties within
our internal control system. Management is required to apply its judgment in
evaluating the cost-benefit relationship of possible controls and
procedures.
Because
of its inherent limitations, internal control over financial reporting may not
prevent or detect misstatements. Projections of any evaluation of effectiveness
to future periods are subject to the risk that controls may become inadequate
because of changes in conditions, or that the degree of compliance with the
policies or procedures may deteriorate. All internal control systems, no matter
how well designed, have inherent limitations. Therefore, even those systems
determined to be effective can provide only reasonable assurance with respect to
financial statement preparation and presentation. Because of the inherent
limitations of internal control, there is a risk that material misstatements may
not be prevented or detected on a timely basis by internal control over
financial reporting. However, these inherent limitations are known features of
the financial reporting process. Therefore, it is possible to design into the
process safeguards to reduce, though not eliminate, this risk.
Changes
in Internal Controls Over Financial Reporting
PART
II – OTHER INFORMATION
We are
not a party to any pending legal proceeding that is not in the
ordinary course of business or otherwise material to our financial condition or
business.
In
addition to the other information set forth in this Form 10-Q, you should
carefully consider the factors discussed in Part I, Item 1A, subsection “Risk
Factors” of our Annual Report on Form 10-K for the fiscal year ended
December 31, 2008 which could materially affect our business, financial
condition or future results of operations. The risks described in our Annual
Report on Form 10-K for the fiscal year ended December 31, 2008 are
not the only risks that we face. Additional risks and uncertainties not
currently known to us or that we currently deem to be immaterial may also
materially adversely affect our business, financial condition and future results
of operations. Other than as set forth below, there have been no material
changes from the risk factors previously disclosed in Item 1A, subsection “Risk
Factors” to Part I of our Annual Report on Form 10-K for the fiscal year
ended December 31, 2008.
You
should carefully consider the risks described below before making an investment
decision in our securities. These risk factors are effective as of the date of
this Form 10-Q and shall be deemed to be modified or superseded to the extent
that a statement contained in our future filings modifies or replaces such
statement. All of these risks may impair our business operations. The
forward-looking statements in this Form 10-Q involve risks and uncertainties and
actual results may differ materially from the results we discuss in the
forward-looking statements. If any of the following risks actually occur, our
business, financial condition or results of operations could be materially
adversely affected. In that case, the trading price of our stock could decline,
and you may lose all or part of your investment.
Risks
Related to Our Business
We
have a limited operating history with significant losses and expect to continue
to experience losses for the foreseeable future and our independent auditors
have expressed doubt about our ability to continue as a going
concern.
We have
yet to establish any history of profitable operations. Our
profitability will require the successful commercialization of one or more of
the technologies we either license or own. Since our organization, we have
incurred operating losses and negative cash flow from operating activities as a
result of minimal sales coupled with our significant clinical development,
research and development, general and administrative, sales and marketing and
business development expenses. Furthermore, our cash burn rate and expenses have
recently increased significantly due to our aggressive commercialization,
marketing and international initiatives. We expect to incur losses for at least
the next several quarters as we expand our sales and marketing capabilities,
make use of the sales and marketing capabilities of third parties and continue
our clinical trials and research and development activities. Losses
have totaled approximately:
$4,286,582
for the nine months ended September 30, 2009
$6,021,742
for the year ended December 31, 2008
$2,311,712
for the year ended December 31, 2007
$2,935,719
for the year ended December 31, 2006
These
losses, among other things, have had and will continue to have an adverse effect
on our working capital, total assets and stockholders’ deficit. In light of our
recurring losses, accumulated deficit and cash flow difficulties, the report of
our independent registered public accounting firm on our financial statements
for the year ended December 31, 2008 contains an explanatory paragraph raising
substantial doubt about our ability to continue as a going concern. Our
financial statements do not include any adjustments that may be necessary in the
event we are unable to continue as a going concern.
We have
experienced losses from operations during the last three years and have an
accumulated deficit of $24,279,117 as of September 30, 2009 and $19,992,535 as
of December 31, 2008. We have an operating cash flow deficit of
$4,413,596 for the nine months ended September 30, 2009 and $3,835,190 for the
year ended December 31, 2008 and we sustained operating cash flow deficits of
$1,913,760 and $2,224,538 in 2007 and 2006, respectively. Our
accounts payable and accrued expenses have also increased due to operational
changes instituted in connection with the launch of our consumer
products. At September 30, 2009, December 31, 2008 and December 31,
2007, we had working capital (deficit) of approximately ($10,273), ($500,672)
and $260,534, respectively.
The
Company's principal source of liquidity at September 30, 2009 was $1,724,967
which includes $724,967 in cash and cash equivalents and $1,000,000 in stock
subscriptions receivable. The Company currently has sufficient
capital to operate for the remainder of 2009.
We
continue to require additional financing to operate beyond 2009.
We do not
have sufficient capital to sustain our operations beyond 2009 and we require
additional financing. If we are not able to raise additional capital, among
other things, we could:
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be
forced to reorganize under the protection of the Federal Bankruptcy
Laws;
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need
to scale back or cease our marketing and development
efforts;
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be
forced to cease operations;
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be
unable to pursue further development of our
technologies;
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be
forced to sell off our technologies prior to maximizing their potential
value;
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be
unable to aggressively market our products;
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be
unable to pursue patenting some of our technologies and development of our
technologies and products;
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have
to lay-off personnel;
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be
unable to continue to make public filings; and
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have
our licenses for our SMaRT™ Replacement Therapy technology and MU 1140
technology could be terminated.
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There can
be no assurance that we will be able to raise additional capital and any of
these events would significantly harm our business.
The
Koski Family Limited Partnership (“KFLP”) has a controlling interest in our
outstanding shares of common stock.
The KFLP
own approximately 55% of our outstanding shares of common stock. Our directors,
officers and principal (greater than 5%) security holders, taken as a group,
together with their affiliates, beneficially own, in the aggregate,
approximately 74% of our outstanding shares of $.001 par value common stock.
Certain principal security holders are our directors or executive officers. As a
result of such ownership, these security holders may be able to exert
significant influence, or even control, matters requiring approval by our
security holders, including the election of directors. In addition, certain
provisions of Florida law could have the
effect of making it more difficult or more expensive for a third party to
acquire, or of discouraging a third party from attempting to acquire, control of
us.
We have
pledged substantially all
of our assets as collateral to secure our indebtedness to
the Koski Family Limited Partnership
which may limit our
ability to incur additional indebtedness or to raise additional capital,
and if we fail to meet our payment or other obligations under this debt,
the KFLP could foreclose on, and acquire control of, substantially all of
our assets.
We have
pledged substantially
all our assets as security for borrowings under our promissory note to
the Koski Family Limited Partnership. Since substantially all of our assets are
used to secure this debt obligation, we have a limited amount of collateral
that is available for future secured debt or credit support. As a result, we may
be limited in our ability to incur additional debt or equity financings. In
addition, if we fail to comply
with the terms of our promissory note the KFLP could declare all funds
borrowed thereunder to be immediately due and payable. If we are
unable to repay the amount owed the KFLP
could foreclose on, and acquire control of, substantially all our assets that
serve as collateral.
We cannot provide any assurances that we will be able to generate
sufficient cash from our operations or any financing efforts to repay the
promissory note.
Our business may be adversely
affected by the current economic recession.
The
domestic and international economies are experiencing a significant recession.
This recession has been magnified by the tightening of the credit markets. The
domestic and international markets may remain depressed for an undeterminable
period of time. A prolonged recession could have a material adverse
effect on the Company's revenues, profits and its ability to obtain additional
financing if sales revenue is insufficient to sustain our operations as
needed. In such event, we could be forced to limit our marketing and
development efforts and significantly curtail or suspend our operations,
including laying-off employees, recording asset impairment write-downs and other
measures. We must generate significant revenues to achieve and maintain
profitability.
We
must spend at least $1 million annually on development of our MU 1140™ and
SMaRT™ Replacement Therapy technologies and $100,000 annually as minimum
royalties under our license agreements with the University of Florida Research
Foundation, Inc. We must also comply with certain other conditions of our
licenses. If we do not, our licenses to these and other technologies may be
terminated, and we may have to cease operations.
We hold
our MU 1140™ and SMaRT™ Replacement Therapy technologies under licenses from the
University of Florida Research Foundation, Inc. Under the terms of the licenses,
we must spend at least $1 million per year on development of those technologies
before the first commercial sale of products derived from those technologies. In
addition, we must pay $25,000 per quarter as minimum royalties to the University
of Florida Research Foundation, Inc. under our license agreements. The
University of Florida Research Foundation, Inc. may terminate our licenses in
respect of our MU 1140™ and our SMaRT™ Replacement Therapy technology and
technology if we breach our obligations to timely pay monies to it, submit
development reports to it or commit any other breach of the covenants contained
in the license agreements. There is no assurance that we will be able to comply
with these conditions. If our license is terminated, our investment in
development of our SMaRT™ Replacement Therapy™ and MU 1140™ technologies will
become valueless and we may have to cease operations.
Until
commercial sales of any products developed from these licensed technologies take
place, we will not be earning revenues from the sale of products derived from
them and will, therefore, have to raise the money we must spend on development
of our technologies by other means, such as commercialization and sale of our
consumer products, or the sale of our common stock. There is no assurance we
will achieve a sufficient level of sales to provide such funding or be able to
raise the financing necessary to meet our obligations under our licenses. If we
cannot, we may lose our licenses to these technologies and have to cease
operations.
If
we fail to maintain an effective system of internal controls, we may not be able
to accurately report our financial results or prevent fraud which could subject
us to regulatory sanctions, harm our business and operating results and cause
the trading price of our stock to decline.
Effective
internal controls required under Section 404 of the Sarbanes-Oxley Act of
2002 are necessary for us to provide reliable financial reports and effectively
prevent fraud. If we cannot provide reliable financial reports or prevent fraud,
our business, reputation and operating results could be harmed. We have
discovered, and may in the future discover, areas of our internal controls that
need improvement. For example, “material weaknesses” were identified in
our quarter ended June 30, 2009 which means that there was “a significant
deficiency, or a combination of significant deficiencies, that results in more
than a remote likelihood that a material misstatement of the annual or interim
financial statements will not be prevented or detected.” During this period, we
were under significant operational stress due to a lack of liquidity and much of
our staff was terminated. During this period and until we can
complete our remediation efforts including the re-staffing and training of our
accounting personnel, we have a higher risk of deficiencies in our financial
reporting. We cannot be certain that the measures we have taken or intend to
take will ensure that we maintain adequate controls over our financial processes
and reporting in the future. Any failure to implement required new or improved
controls or difficulties encountered in their implementation could subject us to
regulatory sanctions, harm our business and operating results or cause us to
fail to meet our reporting obligations. Inferior internal controls could also
harm our reputation and cause investors to lose confidence in our reported
financial information, which could have a negative impact on the trading price
of our stock.
Forward-Looking
Statements
This 10-Q
contains forward-looking statements within the meaning of Section 27A of the
Securities Act of 1933, as amended and Section 21E of the Securities Exchange
Act of 1934, as amended. Such forward-looking statements include statements
regarding, among other things, (a) our need for and availability of working
capital, (b) our financing plans, (c) our strategies, (d) our projected sales
and profitability, (e) anticipated trends in our industry. Forward-looking
statements, which involve assumptions and describe our future plans, strategies,
and expectations, are generally identifiable by use of the words “may,” “will,”
“should,” “expect,” “anticipate,” “estimate,” “believe,” “intend,” or “project”
or the negative of these words or other variations on these words or comparable
terminology. This information may involve known and unknown risks,
uncertainties, and other factors that may cause our actual results, performance,
or achievements to be materially different from the future results, performance,
or achievements expressed or implied by any forward-looking statements. These
statements may be found under “Management’s Discussion and Analysis or Plan of
Operation” and “Business,” as well as in this 10-Q generally. Actual events or
results may differ materially from those discussed in forward-looking statements
as a result of various factors, including, without limitation, the risks
outlined under “Risk Factors” and matters described in this 10-Q generally. In
light of these risks and uncertainties, there can be no assurance that the
forward-looking statements contained in this filing will in fact occur. In
addition to the information expressly required to be included in this filing, we
will provide such further material information, if any, as may be necessary to
make the required statements, in light of the circumstances under which they are
made, not misleading.
ITEM 2. UNREGISTERED SALE OF EQUITY
SECURITIES AND USE OF PROCEEDS
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(a)
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We
issued the following restricted securities during the period covered by
this report to the named individual pursuant to exemptions under the
Securities Act of 1933 including
Section 4(2):
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On
September 16, 2009 we issued 500,000 shares of our common stock, par value $.001
per share, to Media4Equity LLC (“M4E”). The restricted shares were
issued to M4E pursuant to the terms of an agreement we entered into with M4E
effective September 3, 2009, whereby M4E will provide national media exposure
consulting services to us relating to the placement of print and radio
features. The shares have a fair market value of $115,000 based on a
price of $0.23 per share. This amount is included in selling, general
and administrative expenses in the accompanying statements of
operations. In addition to the issuance of common stock the agreement
with M4E requires us to make monthly payments to M4E of $10,000 over the three
year term of the agreement, subject to certain termination rights.
On
September 14, 2009 we issued a warrant to Strategic Growth International,
Inc.(“SGI”) to acquire 250,000 shares of our common stock at $0.30 per
share. The warrant was issued in connection with an agreement with
SGI to provide investor relations services to us.
The
warrant is currently exercisable and has a three year term. The
warrant is substantially similar in form to that of the form of the warrant
granted by us to KFLP in connection with our June 29, 2009 financing
transaction.
ITEM
5. OTHER INFORMATION
None.
ITEM
6. EXHIBITS
Incorporated by reference to Exhibits
filed after signature page.
SIGNATURES
In
accordance with the requirements of the Exchange Act, the registrant caused this
report to be signed on its behalf by the undersigned, thereunto duly authorized
on this 13 day of November, 2009.
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ORAGENICS,
INC.
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/s/
David B. Hirsch
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David
B. Hirsch, President and Chief Executive Officer
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EXHIBIT
INDEX
Incorporated
by Reference
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Exhibit
Number
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Exhibit
Description
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Form
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File
No
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Exhibit
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Filing
Date
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Filed
Herewith
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31.1
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Certification
of Principal Executive Officer pursuant to Rule 13a-14 and Rule 15d-14(a),
promulgated under the Securities and Exchange Act of 1934, as
amended.
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X
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31.2
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Certification
of Principal Financial Officer pursuant to Rule 13a-14 and Rule 15d-14(a),
promulgated under the Securities and Exchange Act of 1934, as
amended.
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X
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32.1
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Certification
pursuant to 18 U.S.C. Section 1350, as adopted pursuant to Section 906 of
the Sarbanes-Oxley Act of 2002 (Chief Executive Officer).
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X
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32.2
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Certification
pursuant to 18 U.S.C. Section 1350, as adopted pursuant to Section 906 of
the Sarbanes-Oxley Act of 2002 (Chief Financial Officer).
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