Strategic Issues The Business of Obesity: Trends in Developing and Commercializing Therapeutics for the Worldwide Marketplace Evelyn B. Kelly, PhD
Obesity is the most prevalent, fatal chronic disease of the twenty-first
century and is increasing at rates only seen with infectious diseases.
Obesity causes 300,000 premature deaths each year and accounts for
$93 billion in medical expenses annually.
The issue of obesity transcends health emerging as a global problem
that will remain with us for years to come.
The Food and Drug Administration (FDA) must balance the new
status of a health crisis and “obesity as disease” with the troubled
well-publicized fiascos such as Phen-fen and OTC products like
Despite advances in scientific understanding, diagnosis, and drug
development, substantial unmet needs must be translated into
Sales for the two approved drugs- Meridia and Xenical- have been
disappointing. Forming partnerships between innovators and big
pharma offers risk sharing and will achieve greater revenue faster and
ultimately provide more value for an emerging pharma or biotech
Regulating, developing, and financing drugs for the obesity market
were among topics discussed at the “World Obesity Congress and
Expo,” a conference sponsored by Global Business Research, Ltd.&
Business Access LC (Nevada City, CA). It was held July 12-13 at the
Washington Hilton, Washington, DC. The article provides selected
This article was written by Evelyn B. Kelly, Ph.D., a medical writer in
Ocala, Florida. She can be reached at [email protected].
The anatomy of an epidemic
Obesity is a side effect of the success of genes for survival in an
atmosphere of plenty. Over the last decade alone, obesity has increased 70%,
occurring in all population subsets- young, old, rich, poor, black, and white.
Two-thirds of all Americans are overweight or obese. And it is not just in the
US. In the past 20 years, obesity has increased at alarming rates. About 900
million adults worldwide are overweight, including about 5% of the world’s
Obesity is defined as “an abnormal increase in fat in the subcutaneous
connective tissue” and quantified by Body Mass Index (BMI), calculated by
weight in kilograms divided by height in meters squared. See Table 1: Obesity and Body Mass Index. An obese person has a BMI of 30 to 40,
while those in category of 40 or above are morbidly obese. Obesity results
from insufficient caloric expenditure caused by lack of movement or
exercise and/or excessive caloric intake. Calorie intake rose from 1774
kilocalories per day in the two-year period of 1989 –1991 to 2002 kcal/day
in 1994 to 1996. Technology has enabled food costs to decline as the costs
of being inactive have also declined. One in four persons do not exercise at
Obesity is responsible for about 400,000 deaths per year and is related
to a host of adverse health consequences:
Type 2 diabetes (majority of cases are obesity related) Heart disease Stroke Hyperlipidemia Hypertension Several types of cancer Gallbladder disease Sleep apnea Mood disorders Eating disorders Gout Osteoarthritis Perhaps other conditions such as Alzheimers disease, back pain.
Eric Finkelstein, RTI International (Research Triangle, NC), presented
the adverse financial consequences of obesity in the US. Medical costs are
over $90 billion per year. About 9% of aggregate medical spending goes to
treating obesity-related disease; these costs now rival those created by
smoking. Each taxpayer pays about $180 per year on obesity-related medical
costs for public sector health plans, which accounts for about half of obesity-
attributable dollars paid by Medicare and Medicaid. Employers and
employees also subsidize the costs of obesity for those with private
insurance. In addition, absenteeism due to illness rises with BMI Finkelstein
has developed an “Obesity Cost Calculator” that employers can use to
quantify the costs of obesity to their firm. Finkelstein sees the best argument
for interventions may rest in these financial arguments relating to
Obesity is both a personal and societal issue. Thus, genetics may load
the gun, but environment pulls the trigger. According to Gerard Musante,
Ph.D., founder of Structure House (Durham, NC), for success interventions
must be multifaceted. The interplay of advertising, parental influences,
environmental influences, psychological factors, social factors, and
physiological factors affect obesity. A direct link exists between urban
sprawl and health: where people walk less, weigh more, and suffer from
elevated blood pressure. Physical education is no longer a mainstay in
schools; Illinois the only state to require daily physical fitness education.
Given the current trends, only a concerted effort on many fronts will curb
FDA Approval and Oversight Trends
Lester M. Crawford, D.V.M., Ph.D., Deputy Commissioner of FDA and
chair of the FDA Obesity Working Group (OWG), reported that in March
2004 recommendations were made to the Agency to combat epidemic. They
Improve food labeling Urge restaurants to voluntarily provide calorie and nutrition
Follow through with plans for the development of obesity
therapeutics. According to Crawford, the report notes that ideally
individuals will avoid becoming overweight or obese through diet
and exercise, but it also recognizes that extremely obese individuals
are likely to need medical intervention to reduce weight and mitigate
The OWG also urged the FDA to convene an advisory committee to address
challenges, as well as gaps in knowledge of existing therapies, to continue
discussion with pharmaceutical and medical device sponsors about new
obesity medical products, and to revise and reissue for comment the 1996
draft guidance for the Clinical Evaluation of Weight-Control Drugs.
Mark Mansour, Morgan, Lewis, & Bockius LLP explained how the
1996 draft that sets forth the Agency’s recommendation for the design and
conduct of Phase I through III clinical studies to demonstrate the
effectiveness and safety of weight loss medications. Effective criteria
A mean weight loss in the drug treated group that is 5% greater than
the mean weight loss in the placebo group following one year of
The proportion of patients that lose at least 5% of their baseline
weight must be greater in the drug vs. the placebo group. Under the
1996 criteria sibutramine (Meridia®) was approved in 1997 and
orlistat (Xenical®) was approved in 1997. Dexfenfluramine was
approved in 1996 and withdrawn in 1997 for safety reasons. In April
2004 the FDA ruled that ephedra-containing supplement may no
longer be sold in the US. Reasons: The totality of the data showed
little benefit from products with ephedra other than modest short-term
weight loss while raising blood pressure and otherwise stressing the
circulatory system. See Table 2: Current Approved Drugs. In April
2004 FDA sent warning letter to 16 dietary supplement distributors
making false and misleading claims over the Internet. In December
2003, the Federal Trade Commission (FTC) announced a “Red Flag”
education campaign to assist media outlets in screening out false
Who should pay for treatment?
According to Dwight “Pete” Fullerton, Ph.D., R.Ph., Strategic
Pharmacy Innovations (Seattle, WA), FDA approval may only be the first
step to broad acceptance for reimbursement. In order to maximize
information, more persuasive information about drugs designed specifically
for obesity is needed. FDA and some manufactures are “gun shy” from past
controversies like Phen-fen. The role of obesity in costly chronic diseases is
far from precise and quantifiable, and the culpability of genetics vs. behavior
will further cloud the issue of who should be financially responsible.
Fullerton recommended the following approaches to making a compelling
Build a convincing case that health outcomes will cause other
medical costs to go down; just showing a link is not enough.
Use Academy of Managed Care Pharmacy (AMCP) dossiers to
Utilize health-outcomes modeling when long term studies have
Go beyond safety and efficacy and show short term cost
savings, impact on emergency room visits, and need for
Use a model that includes indirect costs such as productivity,
To convince managed care of reimbursement needs, drug developers must
build their cases based on economic modeling predicated on solid data, as
well as aggressive patient support with disease management programs. In
other words, managed care demands, “Show us the value.”
Better marketing for the science-based obesity market involves
putting the customer first, according to Greg Kitzmiller, Indiana University
School of Business. Focusing on the customer is more than the job of the
people in public relations; it is the job of everyone in a company to
understand the customer. This is not just a set of buzzwords like TQM but a
true cultural change. To build the customer-focused concept, management
must focus on identifying and satisfying consumer needs to ensure the
organization’s long-term profitability objectives. The whole firm from the
telephone operator to salesperson to shipping dockworker must think
“customer.” He emphasized that companies working in this area must
understand seven common myths about obesity. See Table 3: Common Myths About Obesity Obesity as Disease
Morgan Downey, J.D., Executive Director, American Obesity
Association, (AOA) spoke on the future of obesity and public policy. The
AOA mission is to have obesity, the most prevalent, fatal chronic disease of
the twenty-first century, recognized and regarded as a major disease
epidemic in the United States and abroad. The association advocates
research, health insurance reimbursement, prevention programs, education,
consumer protection, and an end to discrimination.
Downey emphasized the present Washington public health paradigm
is that obesity is a behavior and that diet and exercise will solve all
problems. However, the new paradigm that obesity is a disease is confirmed
by the definition of obesity and the definition of disease. A disease is
defined as “an interruption, cessation or disorder of bodily functions,
systems, or organs.” Likewise like a disease, obesity has identifiable signs
and symptoms: excess accumulation of adipose tissue, endocrine organ
effects, increased glucose, elevated cholesterol and triglycerides, decreased
HDL, pain, breathlessness, and effect on fertility.
Obesity is recognized as a disease by the National Academy of
Sciences, World Health Organization, National Institutes of Health,
International Classification of Diseases #278, Food and Drug
Administration, Federal Trade Commission, Social Security Administration,
and several associations and textbooks. It is not recognized as a disease by
the public, Medicare*, Medicaid, and private insurance. Those who argue
that obesity is not a disease contend that the condition is a personal choice.
Therefore, they reason that because obesity is self-inflicted, it is not a
disease and deserves no sympathy. But Downey countered with the question
of personal responsibility compared to what? Many other conditions, such as
sexually transmitted diseases, lung cancer, or sports injuries, are the result of
personal choices. He rebuts that the claims are not justified and asks just
how effective must a treatment be for consideration. This attitude holds
obesity to a miracle cure standard where with other chronic diseases, such as
Alzheimers and Parkinsons disease, drugs do not cure but may make the
patient better for a short period of time.
According to Jeremy Nobel, MD, MPH, Harvard School of Public
Health, obesity should no longer be viewed as a lack of will power but as a
chronic disease model, where the patient and practitioner must understand
that it requires a lifelong effort. The focus needs to be on making the patient
healthier not merely leaner. Supporting data show that as little as a 10%
makes a difference in health symptoms. Lessons learned from other chronic
disease management initiatives need to be applied to obesity management,
A Market of Unmet Needs
Obesity is garnering much attention in the press and other areas
because it is a major risk factor for serious medical conditions. For example,
over 55 percent of those with hypertension are obese. Carole Gleeson,
Decision Resources, Inc., showed startling epidemiology figures. The total
prevalence of obesity in the three major regions- Japan, Europe, and the
United States- will continue to grow 2 % over the next ten years. In the US
alone the number will expand from 68 million people to 88 million in 2013.
Today, few pharmacological options are available to patients if diet
and exercise fail. While many physicians favor drug treatment of obesity,
some are hesitant because of the insufficient efficacy of currently marketed
drugs. To address unmet needs, Gleeson listed the following essentials:
Safe and effective drug therapies that would result in a 10
percent weight loss; however, patients want and expect 20 %.
Reimbursement for antiobesity therapies. Wider array of drug options
Physician education and skill building Patient awareness/motivation
Certain drivers and constraints will shape the future of the obesity
market. The leading driver is that the prevalence of obesity will continue at a
steady pace, especially as the medical community recognizes obesity as a
disease. There will be a continued demand for new agents that offer long-
term maintenance of weight loss. The down side of the picture is led by the
lack of reimbursement of third-party payors. Doctors, likewise, will be
reticent to treat obesity with a drug until clinically long-term effective drugs
enter the market. A final constraint is that research has only begun to unravel
the etiology and pathophysiology of obesity.
Gleeson emphasizes the high unmet need and increasing prevalence of
obesity point to both challenges and the following opportunities in this
The newest drugs- sibutramine and orlistat- are far from optimal; great
commercial opportunity exists for a drug that improves on current
therapies in efficacy, safety, and cost.
Physicians assail the cost of therapy as a major reason for
noncompliance and stopping treatment; a low-cost alternative would
While acceptance of obesity as a medical condition is increasing, the
behavioral support system of dieticians, behavior therapists, and
exercise physiologists are currently lacking in most facilities.
Establishing comprehensive services and full funding for them will be
Because of the complex nature of obesity, research challenges
abound. Scientists have identified potential useful targets for treating
obesity but identifying the subpopulations that can benefit from these
therapies is a major scientific challenge.
Despite the high prevalent population of obese people in the seven major
markets, the total market for antiobesity agents only reached $520 million in
2002. Gleeson foresees that in 2012, the market will grow 18 % annually to
$1.7 billion, driven by the increase in the obesity population and the
availability of new agents as follows: orlistat, 5%; ATL-962, 15%; other
peripheral acting agents, 3%; sibutramine, 7%; CNTF, 10%; rimonabant,
40%; other centrally-acting agents, 20%.
According to Alexander Young, Ph.D., president of Mirabila (San
Diego, CA), a company that contracts business development for venture
capital firms, investment banks, biotechnology companies and
pharmaceutical companies, the huge obesity market is out there as predicted
by the success of current and past weight-loss businesses such as
herbiceuticals, OTC medications, bariatric surgery, liposuction, Phen/fen
clinics, and fitness and weight loss centers. He also emphasized how poorly
understood and complicated mechanisms can lead to unanticipated side
effects. For example, Fenfluramine/Phentermine was launched in 1995 for
an off-label combination therapy and withdrawn in a flurry of doubt in 1997.
Dexfenfluramine was approved in 1996 and withdrawn in 1997.Topamax
was approved in 1997 for epilepsy and had a Phase III trial for obesity
pulled in 2002. Meridia was launched in 1998 and withdrawn by the Italian
Therapeutic Development for Obesity
According to Jose Caro, MD, Lilly Research Laboratories,
(Indianapolis, IN), the FDA’s fast-track drug approval mechanism is being
expanded to obesity and diabetes drugs. Under fast-track, drug makers can
hold meetings with FDA staff to get feedback on their development plans,
submit their new drug applications in sections rather than all at once, and
request their study be judged using surrogate rather than primary endpoints
Today only about 4% of obese people (US) are getting prescription
medicine to treat their condition. If obesity were treated as often as
hypertension, 66% of obese people would receive prescription medication.
Obesity is just as bad as hypertension in causing co-morbidities and social
economic burdens. Lilly Internal Market Research (2003) revealed that 28%
of obese patients are using non-traditional means, such as other
prescriptions, over-the-counter products, surgeries, extreme diet/exercise to
treat their obesity. Fen-Phen peak sales was $650MM worldwide in 1996-
Caro said that a multi-platforms approach must be take to the
treatment of obesity. Effective treatment may need to modify more than one
Brain and the translation system- what kind of food and is it the right
Effector system or energy balance; how can the body make the
Messenger system in the peripheral tissues.
The industry obesity pipeline shows several compounds in development. See Table 4: Selected Compounds in Development. Two products are near
approval and may be on the market soon. Carole Gleeson sees rimonabant
(Acomplia® Sanofi-Aventis) as the most promising agent emerging from the
obesity pipeline in 2006. In a double-blind, placebo-controlled study, 1036
obese patients, who also had dyslipidemia were randomized to receive daily
treatments of 5 mg or 20 mg rimonabant or placebo. Patients were also
placed on a reduced calorie diet for a period of one year. After one year,
patients treated with the highest dose of rimonabant lost an average of 8.6 kg
body weight whereas those receiving placebo only lost 2.3 kg. Nearly 75 %
of those receiving the higher dose lost at least 5% of their body weight
compared to 42% of patients on the lower dose and 28% of those receiving
placebo. The most common side effects were nausea and dizziness, which
occurred more often in patients receiving the highest dose. Participants did
not exhibit increased blood pressure or heart rate when compared to those on
placebo. The weight loss in preliminary trials was similar to that of orlistat
and sibutramine. The drug acts on multiple pathways within the CNS. Its
less expensive oral formulation makes dosing easier and will make it a
strong competitor. Sanofi-Synthelabo (New York, NY) plans to market the
drug as a preventive medication for cardiovascular health.
A second product is Regeneron’s (Tarrytown,NY) Axokine®, a
modified form of a naturally-occurring protein called Ciliary Neurotrophic
Factor (CNTF). In preclinical models of obesity, Axokine signals the satiety
center of the brain to decrease food intake. In a Phase II trial, obese people
lost weight during a twelve-week period. A Phase III pivotal trial began in
2001 with about 2000 patients enrolled. In March 2003 results of the double-
blind, placebo- controlled showed many individuals lost weight, but the
average weight loss was limited by the development of antibodies.
Additional studies were initiated as part as part of the Phase III program
designed to assess the function after short-term dosing periods and to
measure weight change after cessation of short-term treatment. To date,
Axokine has demonstrated a favorable safety and tolerability profile in
Obesity Treatment Methods
Weight is a part of a cycle of nutrients that are taken into the body
with interactions from the nervous system, endocrine system, and energy
storage system and metabolism involving adipocytes, liver, and muscle. Co-
morbidities result from the breakdown of homeostasis of multiple
complicated systems. Three target areas include drugs that affect the central
nervous system (CNS), metabolic modifiers, and those that are thermogenic.
CNS methods include neurotransmitter targets, serotonic reuptake
inhibitors, cholinergic reuptake inhibitors, hypothalamus targets, anti-
depressants, and anti-epileptics. The neurotransmitters serotonin and
norepinephrine are released when the axon terminal on a presynaptic neuron
is excited. The substances travel across the synapse to act of the target cell to
either inhibit or excite it. For instance, the approved drug sibutramine works
to inhibit the reuptake of these chemicals by neurons serotonergic and
Metabolic modifiers include lipase inhibitors, fatty acid targets,
cortisol-insulin modulation, angiogenesis inhibitors, leptin, and ghrelin.
In the bloodstream cholesterol and fat-soluble vitamins are present.
Triglycerides are converted by gastrointestinal lipase into monoacylglycerol
and fatty acids. The formation of micelle in the intestinal lumen allows 90%
of dietary triglyceride to be absorbed as monoglyacylglycerol and fatty
acids. Cholesterol and fat-soluble vitamins are absorbed with lipids. With
orlistat, approximately 1/3 of dietary triglyceride is excreted unchanged in
stool. Absorption of cholesterol and fat-soluble vitamins is also decreased.
Although the drug did have long-term desired effects of weight loss when
compared to placebo, certain undesirable gastrointestinal side effects, such
as fatty, oily stools, fecal incontinence, and fecal urgency were noted. These
side effects are probably the reason it is not a $3 billion drug.
Following the Money: Wall Street and Venture Capital
Albert L. Rauch, Ph.D., CFA, Vice President, AG Edwards & Sons,
Inc., spoke of “big pharma” strategies for developing obesity therapeutics
that consider revenue projections and risk. Roche Pharmaceuticals sales of
Xenical in 2003 were $108 million in US revenue in 2003; Abbott’s sales of
Meridia were $68 million. Generic phentermine generated $86 million in
2003. Short-term outlook also includes off label us products such as
Welbutrin (Glaxo), an anti-depressant that decreases hunger and various
levothyroxines that increase metabolism.
Rauch presented the following strategic approach:
Establish a “beachhead.” The best immediate possibility is
developing a product focused on treating Type II diabetes via
weight reduction. This product would be used off label. This
sub-set of the obesity population would lead to faster
penetration of a smaller market and expand into a larger obesity
overweight market. At present there are 11 Phase II products, 5
Phase II, and 3 in Phase III in development for diabetes with
potential in obesity. See Table 5: Leading Developers of Drugs for Obesity/diabetes.
Command a frontal assault. Develop products focused solely on
weight loss. This approach involves establishing medical
benefit to gain regulatory approval. The efficacy hurdle may be
difficult to obtain. Likewise, it may be difficult to establish
economic benefit. The legacy of phen-fen, the diet drug that
was pulled from the market because of harmful side effects,
may be difficult to overcome. The large problem of
reimbursement looms and may be difficult to obtain.
T. Scott Johnson, M.D., founding partner of JSB Partners, L.P., an
investment bank specializing in mergers and acquisitions, private financings,
and corporate alliances, focused on how partnering offers advantages for
emerging companies. Partnering can offer advantages both to small
companies and large pharma. Small companies can push to Phase II then
usually find the expenses and risk beyond their reach. For example, in the
development of the product Xenical, Phase III trials involved 4800 patients
followed for two years. Launch and marketing will require a combination of
extensive detailing to primary care physicians, endocrinologists, OB-Gyn,
and DTC advertising, demanding a costly sales force. The risk is staggering;
many products have failed to achieve positive results even in late stages of
clinical trials. Major players are more capable of rapid launch and greater
ultimate revenue. Large pharma also benefits from partnerships. They may
access innovation in a market, made complex due to many targets and
pathways. Partnership with a small company give the advantages of risk
sharing, efficient cost expenditure, and specialists who have worked in the
The potential for this market is huge. However, sales of the two drugs
approved for the treatment of obesity have been disappointing. This makes
the tendency to make deals reflect this current reality rather than the
enormous potential market. Thus, the onus of risk is usually placed on the
innovator. In this spirit, a strong big pharma partner offers risk sharing and
will achieve greater revenue faster and ultimately provide more value for an
emerging pharma or biotech company with an innovative obesity product. It
is worthwhile for a small company to look to big pharma, according to
Bernice Welles, M.D., Venture Partner, MPM Capital, presented
promising emerging technologies and companies and showed how US IPO
markets are at historic lows. Most of those with venture capital are looking
for later state products, with the ideal being phase IIB. Although she
believes obesity represents an opportunity to make profitable investments,
less than 7% of venture capital investment made in 1999-2003 was focused
in the area of metabolic disease. However, the positive side is a recent
upswing in original papers published, drugs in development, and patents.
Obesity-related partnerships do represent attractive opportunities,
according to Welles. In 1996, Amgen paid Rockefeller University $20MM
to acquire the rights to develop and market leptin-based products. Other
Zymogenetics and Amgen (preclinical) Solvay and BMY for a cannabinoid type I receptor
Peptimmune and Genzyme for a pancreatic lipase
Esperion acquired by Pfizer, Inc. for $1.3 billion for a
Such early stage alliances must weigh value creation versus value loss.
Welles presented three investment examples made by MPM:
Enteromedics (St. Paul, MN). The company originated as a device
incubator for a reversible vagus nerve modulator that shrinks the
stomach, impairs fat absorption, and increased the sensation of satiety.
A current prototype is underdevelopment for obesity with the intent to
displace bariatric surgery. (first funded 2002)
Biovitrium AB (Stockholm, Sweden). Founded in 2001 as a spin-off
of Pharmacia to focus on drugs to treat metabolic diseases, the
company announced in 2002 an agreement with GSK to develop and
commercialize 5-HT2C receptor agonists for obesity and other medical disorders. In 2003 Biovitrium AB announced an agreement with
Amgen to give exclusive rights to develop and commercialize their
11BHSD1 enzyme inhibitors for treatment of metabolic diseases and
Peptimmune (Cambridge, MA). This company has developed
programs in autoimmune disorders and is broadening the focus to
A showcase of future strategies for the treatment of obesity
Development of islet and gut peptide hormones
Christian Weyer, M.D., Director of Clinical Research, Amylin
Pharmaceuticals (San Diego,CA), presented the development of islet and gut
peptide hormones as anti-obesity targets. To date most efforts have focused
on small molecules directed toward CNS targets involved in food intake and
food regulation. However, islet and gut peptide hormones are normally
released in response to meals and are thought to play an important
physiological role in the regulation of food intake and postprandial
metabolism following the meal. Food intake is a complex behavior involving
sensory, cognitive, post-ingestive, and post-absorptive mechanisms.
Building on their experience in the diabetes field, Amylin is with the
metabolic properties common to all three conditions. The hormones include:
PYY3-36 (AC162352 Obesity program). Peptide YY(PYY) is a
naturally occurring 36 amino acid gastrointestinal peptide
hormone expressed/produced in the entero-endocrine cells in
the small and large intestine and secreted in response to meals.
It is cleaved in vivo by the DPP-IV enzyme to PYY[3-36]. In
two clinical studies the drug reduced hunger and food intake in
both lean and obese subjects. The IND for AC162352
(synthetic PYY3-36) was submitted in December 2003 and is
Amylin/Pramlintide (AC137 Obesity Program). This program
uses existing clinical experience with pramlintide, a synthetic
analog of the beta-cell hormone amylin. Amylin, a 37-amino
acid peptide, co-related and co-secreted with insulin from
pancreatic β-cells is deficient in diabetes. The synthetic analog
is specifically engineered to overcome the tendency of human
amylin to aggregate and adhere to surfaces and to form
insoluble particles. The potency is equal or greater than human
amylin. Clinical trials have shown a reduction in ad-libitum
food intake observed in insulin-treating subjects with type 2
diabetes and in obese, non-diabetic subjects, as well as
significant reduction in body weight. Phase II studies are
The genetic relationship to obesity is the target of investigation. See Table 6: Selected Genes and Their Effects.
According to Wei-Wei Zhang, M.D., Ph.D., President and CEO,
GenWay Biotech, Inc., (San Diego, CA) growing evidence indicates that
abnormality of the adiponectin gene and decreased production of
adiponectin that is expressed in adipose tissue might be link obesity with
metabolic and other obesity disorders. Recent pharmacological studies
indicate that fat tissue itself plays a key role as an endocrine organ and
produces various kinds of adipokines with adiponectin as one of them.
Adiponectin has multiple potential therapeutic potentials, as well as a novel
diagnostic marker. GenWay has developed recombinant functional
adiponectin and its monoclonal antibodies.
HMGene is a company that directly targeting adipose tissue. The
discovery strategy identifies genes central to adipocyte physiology using
HMGene’s AdiposenseTM platform. This platform has identified and
prioritized 139 putative obesity genes. After validating selected targets, the
company generates therapeutics for human obesity. HM-21, an endogenous
secreted protein, is a key protein that signals a known adipogenic pathway
and is highly expressed in fat tissues. HMGene believes that HM-21 shows
preclinical therapeutic potential and hopes to accomplish IND filing within
two years. HM-12 is also a validated target illustrated by knockout mice that
have a profound reduction in fat. This drug is a target for small-molecule
therapy and NCE generation is currently in progress.
According to Mark Tepper, Ph.D., President & Founder Araios-
CyTRX,(Worchester, MA), RNAi based molecular medicines will treat
obesity and Type II diabetes. The company is developing powerful new
RNAi gene silencing technology to drive the discovery and development of
both traditional small molecules and new RNAi-based therapies. Araios
plans to develop lead candidates through early proof of concept to the clinic.
According to Jeff Leighton, Ph.D., Founder and Director of Drug
Discovery, Adipogenix, (Boston, MA), obesity can be effectively treated
effectively at the fat cell level rather than indirectly by modulating the CNS
mechanisms. Leighton discussed the use of functional human cell-based
assays to screen for small molecules that modulate fat uptake, storage,
breakdown, and burning. AdipoGenix is a biopharmaceutical company
founded by members of the Obesity Research Center at the Boston
Chris Adams, CEO, Compellis Pharmaceuticals, (Boston, MA),
presented a unique therapeutic approach using olfactory perception. Nasal
administration of the calcium channel blocker diltiazem, now marketed for
hypertension, has been shown to decrease food intake and weight gain in
rats. The intranasal route tested against intraperitoneal and oral delivery
showed a significant reduction in weight gain in a dose-dependent manner.
Diltiazem is a proven drug with known toxicity and tolerable side effects.
The drug is now in Phase I study with 50 clinical trial subjects in 8 groups.
* On July 23, after this conference, Medicare deleted the edict that obesity is
not a disease; officials said they would consider paying for treatment but
only if that treatment can be shown to work.
Table 1: Obesity and Body Mass Index BMI=weight (kg)/height(m2) Source: D&MD Table 2: Current Approved Drugs Brand/company Mode of operation
Benzphetamine Didrex/Pharmacia/Upjohn Noradrenergic $2.50
Phendimetrazine Bontril/Mallinckrodt Noradrenergic
Source: D&MD
Table 3: Common Myths About Obesity: Based on interviews of 5000 consumers by the Hartman Group, Belleview, WA Myth Reality
Most think their own weight is average and are
People look to media images to People look at their friends and social networks as the set the standards for weight
cues to decide to lose weight; they keep an eye on their friends; they do not look to their physician for advice
People blame manufacturers or Most see obesity as a very personal issue with personal food retailers for the obesity
Most do not perceive themselves at risk for health
Most use events, like looking in the mirror or at an old
determine their weight People try to lose weight by
Most cite increased physical activity as the preferred
way to lose weight rather than changing eating habits
Most are using the moderation principle as a guide for
dieting: small changes over the long term
Source: Adapted by D&MD Table 4: Selected Compounds in Development Company Phase Mechanism Comments name/generic
MLN-4760 Abbott/Millenium I Carboxypeptidase
Source: D&MD Table 5: Leading Drugs in development for Obesity/Diabetes Compound Company Development Mode of Comments operation Source: D&MD Table 6: Selected Genes and Their Effects
Official Journal of the European Communitiesadapting to technical progress for the 27th time Council Directive 67/548/EEC on theapproximation of laws, regulations and administrative provisions relating to the classification,packaging and labelling of dangerous substances(*)THE COMMISSION OF THE EUROPEAN COMMUNITIES,Having regard to the Treaty establishing the EuropeanThe texts in Annexes I a
II-OP-2 – LA MISSION DE MAITRISE D’OEUVRE DEFINITION DE LA MISSION En bâtiment , pour une construction neuve, la mission confiée au Maître ATTENTION ! d’Oeuvre doit correspondre au moins à la totalité de la mission dite « missionde base » qui couvre l’ensemble de la conception et du contrôle des travaux,de l’esquisse jusqu’à la réception des travaux. contenu de l