THE LEPTIN FACTOR

[Guest guest]

Did you know? The retina of the eye is a microcosm of the brain. It contains

many of the cell types and neurotransmitters found in the brain.

 

Chapter 15

THE LEPTIN FACTOR

Obesity is a symptom . . . not a diagnosis!

_http://www.chronicneurotoxins.com/learnmore/obesityresearch.cfm_

(http://www.chronicneurotoxins.com/learnmore/obesityresearch.cfm)

 

By Ritchie Shoemaker, M.D.

 

Crack open your morning newspaper, these days, and the odds are high that you

’ll soon find yourself reading an alarming health story about “the growing

obesity epidemic in America.â€

 

Unfortunately, most of those breathless, page-one stories are all too

accurate. Take a look around; the proof is there. The “American Waddler†is

all

too commonly sighted in public places and doctor’s offices. If you missed

seeing the Waddler on the streets, you will see him on the Evening News,

rippling

past the camera, arms swinging wide over the layers of belly-rolls and

thunder thighs. You don’t need a Ph.D. in human physiology to understand that

Americans (and especially American children) are getting fatter with each

passing

year.

 

How bad is the U.S. “obesity problem†today, and why is it becoming

increasingly worse?

 

This bad: According to the latest data from the number-crunchers at the U.S.

Centers for Disease Control and Prevention (CDC) in Atlanta, fully one-third

of America’s 280 million citizens are currently classified as medically

overweight.

 

Even more ominous, say public health officials, is the fact that “clinical

obesity†– a chronic disease with a variety of potentially life-threatening

consequences – is now affecting more than 56 million Americans (about 20

percent of us), day in and day out. Just 10 years ago, the numbers were

significantly lower.

 

Here’s the bad news for Americans in the first decade of the new millennium:

Although the CDC opinion released for public consumption is often wrong

about medical issues and frequently distorts scientific research-findings for

the

sake of its own narrow political agenda, the agency is dead-on correct about

the threat from the spreading obesity problem. What the CDC hasn’t figured

out yet, however, forms the heart and soul of this chapter – the startling

fact that obesity is actually a chronic illness, either genetically based in

abnormal leptin and insulin physiology or acquired in ways related to the

immune

responses that are part of other chronic, “biotoxin-associatedâ€

environmental illnesses of our day (such as Sick Building Syndrome). Indeed,

the biggest

news in weight-loss treatment right now is the recent discovery – based on

research from the seemingly unrelated field of chronic biotoxin illnesses such

as “Post-Lyme Disease Syndrome†– that there is a close link between our

increasingly chemically polluted environment and a new family of

biotoxin-linked ailments that often trigger both obesity and diabetes.

 

So far, only a few isolated researchers (and they’re not in Atlanta!) have

grasped the relationship between the fact that as our environment continues to

change rapidly under the influence of the 70,000 industrial and agricultural

chemicals pumped into air, soils, rivers, estuaries and oceans each year,

Americans are getting fatter and fatter. Nor have the “Medical Mandarinsâ€

at

the CDC (or their counterparts in the largest and most prestigious university

medical research departments) yet understood that obesity is an illness of

over-storage of fat that has almost nothing to do with “overeating†alone .

.. .

and everything to do with physiological resistance to metabolic hormones

such as insulin and leptin. While we can’t alter the genetic predisposition

to

leptin and insulin problems, we can control that resistance with new

medications and the No-Amylose Diet. The role of other “new†obesity

related

hormones, including gherlin and neuropeptide Y, shows promise for additional

interventions to defeat obesity in the future. But treatment of the obesity

epidemic

linked to hormone resistances is here now. (More on the exciting recent

breakthroughs in leptin and insulin resistance and its links to inflammation

from

the hidden “environmental diseases†in a minute.)

 

Make no mistake: America’s “fat epidemic†is rapidly spiraling out of

control, and the negative impact on grownups and kids alike can be observed

from

the rocky coastline of Maine to the towering redwoods of California. Example:

According to the latest health statistics, more than 300,000 Americans are

now dying each year from diseases (such as diabetes, hypertension, sleep apnea,

colon cancer and breast cancer) that have been linked directly to obesity.

If heart disease is added to the toll (and many physicians believe it should

be), there can be no doubt that obesity now ranks as our nation’s biggest

health threat. Even if the extra fat doesn’t kill right away, the multiple

impairments caused by obesity make life miserable, from the unnecessary pain

from

arthritic weight bearing joints, reduced ability to walk up a flight of stairs

or even put on a pair of shoes. The derogatory attitudes about obesity in

our society add to the misery, as many overweight people are regarded as

self-indulgent gluttons. Being overweight is a sign of personal slothfulness in

the

eyes of many who view obesity as a “preventable illness.†And who would

list “obesity†on a job application as an important self-accomplishment

that

would help convince a personnel manager to offer employment?

 

These obesity-associated health problems cause untold anguish for the

victims and their families, of course. But the carnage produced by obesity also

hits America hard in her pocketbook, while adding more than $900 million per

year to the cost of health care in this country. Alarmed by the surge in

fat-related costs, no less a figure than the U.S. Surgeon General recently

warned

the nation that if the current trend continues, “Obesity may soon cause as

much

preventable disease as cigarette smoking.†For those on the front lines of

obesity treatment and research, his words need to be changed to reflect the

real issue: obesity has a series of understandable mechanisms and it can be

treated before it causes disease by understanding those mechanisms.

 

Disturbing facts about the epidemic, its cost and its consequences? You bet.

Even more disturbing, though, is the clear failure of all “medically accepted

†attempts to defeat the epidemic with lifestyle changes. Our National Fat

Attack has been taking place during an era dedicated to “physical fitnessâ€

..

.. . during an era in which most of us are bombarded daily with powerful

propaganda about the vital importance of “eating right and getting plenty of

exercise,†if we wish to enjoy healthy, vigorous lives and stay slim. For

reasons

you have already read and more to come, the “eat less and exercise moreâ€

idea is worse than worthless for the vast majority of overweight people. When

the “American Waddler†finally gets up the gumption to go out in the cold

and

rain four times a week to walk before the sun comes up, and he cuts back on

everything enjoyable at the dinner table, he still doesn’t lose much weight

and

he certainly never keeps it off. Now add worsened self-esteem from his

failed weight loss attempt to his ongoing weight problem. Why did the Waddler

fail? Could it be that the reason for his obesity has nothing to do with

trivial

amounts of exercise or elimination of foods unrelated to weight gain from his

diet… and a great deal to do with his daily consumption of fat-generating

food?

 

The experts have a ready answer for the Waddler’s failed weight loss

attempt: he is the reason for the failure, not the “eat less, exercise

more†model.

Just try to find an obesity expert who doesn’t explain the failure of the “

eat less and exercise more†strategy by blaming the patient. “Well, Mr.

Jones joined the fitness club, but only went there three times last year. And

he

never stopped having the French fries and the triple cheeseburgers.†But Mr.

Jones did his exercise and he ate the low fat, low cholesterol meals, with

salads, pasta and whole wheat as he was instructed. He did what he was told,

but he still failed.

 

The wrong entity is being blamed! In medicine, the failure of an accepted

idea to explain what we observe usually means the idea is tossed out, like

garbage bound for the landfill. In other words, we learn more in medicine by

observing what intervention didn’t work, and adjusting our model to

accommodate

the treatment failures, than we do by only observing what did work. If the

model doesn’t explain what actually happens, then the model, like “eat less

and

exercise more,†is wrong.

 

In spite of our continuing obsession with “avoiding dietary fat†and

jogging or walking at least 30 minutes each day,†the remarkable fact

remains:

Americans are fatter now than ever before in their history. Somehow, our model

of

treatment of obesity that is based on devotion to the ideas from the Greek

goddess of health, Hygeia – the patron saint of the “hygienic†approach

to

health, which insists that the key to curing illnesses is to “clean up†our

bad lifestyle-habits, such as overeating and lack of exercise – hasn’t

succeeded in overcoming our national predilection for getting fat and staying

fat.

 

The obvious question becomes, “Does that mean that the treatment for obesity

has little to do with lifestyle?†Other questions follow immediately, once

we realize that Hygeia doesn’t have our answers:

 

Why do most people who become overweight tend to remain overweight . . .

even if they do manage to shrug off a few pounds now and then, before promptly

gaining them back again? And why are some people able to eat all they want,

meal after meal, while remaining wonderfully, infuriatingly slender? Even more

challenging is the question: “Why do many people gain weight that they never

lose, while eating less than their slender counterparts?†Finally, “What

can

we do that will work to control the chronic disease of obesity?

 

As a veteran family physician who’s helped thousands of obese patients lose

weight (and keep it off) during the past 25 years, I’ve spent many hours

studying the latest research from around the world . . . while also conducting

countless patient-interviews and medical examinations aimed at solving the

mystery of why so many people tend to remain fat in spite of their frequent and

courageous efforts at dieting and exercising. Obesity, like any chronic

disease, needs a proper diagnosis. We don’t blame the patient for having

hypertension, we find out what is wrong, look for acquired blood pressure

problems (we

can cure those), and if we find the problem is one of unknown cause (“

essential hypertension†is the medical term), possibly genetic (Did your

parents

have hypertension, Mr. Jones?), we treat it, without complaining that the

patient isn’t doing something to prevent his illness. Sure, we will try

modifying

diet, exercise, salt consumption, stress, and other lifestyle factors, but

when the Hygeia approach predictably doesn’t work, we use medications.

Treatment

of obesity should be no different.

 

Imagine my surprise years ago, when my treatment of obese patients – along

with my continuing inquiries on the causes of the disease- demonstrated a

remarkable fact: the mechanisms that underlay obesity shared many of the same

physiologic principles involved in chronic, biotoxin-associated illnesses. It

was crystal clear that a proper diagnosis of obesity involved looking at

interactions of genetics and hormones like leptin and insulin, as well as the

chemical messengers called cytokines (more on inflammation and cytokines coming

up) that help white blood cells monitor and manage our internal immune

defenses. The same disturbances in cytokines and leptin, many with a genetic

basis,

which were operating in Sick Building Syndrome, were the active players in

obesity, too! Here was the new information, based on rock-solid science, needed

to challenge the “conventional wisdom†on obesity that has ruled American

medical opinion for the past several decades. Imagine the mixture of

exhilaration and wonderment I felt, when I analyzed the latest data on human

biochemistry from obesity literature and seemingly unrelated fields of

neurotoxicology

and cytokine physiology, and began to realize: We’ve been wrong about fat

from the very beginning!

 

It became increasingly clear that the weight-loss advice from popular diet

books such as Sugar Busters, The Zone and The New Diet Revolution was either

incomplete or was simply wrong. As heretical as this may sound, today’s

ongoing Obesity Epidemic provides incontrovertible evidence for the fact that

even

Dr. Robert Atkins – the legendary “guru†of weight-loss in America since

the

1970s – had failed to incorporate into his work the complex biochemical,

hormonal and genetic factors that actually cause most people to become

overweight and stay overweight!

 

As I studied the research and examined my patients during the 1980s and

1990s, I was gradually discovering that the assumptions of medical science

about

how we store fat and gain weight were deeply flawed. And yet those same

flawed ideas – which failed to pinpoint the biochemistry and genetics of

hormone

resistance as the real source of weight-gain, while blaming it on mere “

lifestyle†factors such as overeating and “couch-napping†– had been

repeated so

often over the years that they’d become accepted as Gospel, all across the

increasingly fat USA! The “thermodynamics†idea about weight, namely,

calories

in equals calories out, wasn’t the right answer (Chapter 5); exercise wasn’t

the answer unless the overweight patient had 12 hours a week for intense

activity (Chapter 11); eliminating all carbohydrates ignored the different

effects of carbohydrates on blood sugar (Chapter 2); and permitting some

starches

was a prescription for failure for insulin resistant patients (Chapter 6).

What really do we have to do to understand treatment of the chronic disease we

call obesity?

 

But let’s back up for a second. In order to understand why the conventional

wisdom about fat is flat-out incorrect, we need to look at how the process of

getting fat actually works...even as we ask ourselves the key question that

will solve the fat-mystery once and for all:

 

Question: What would happen if we looked at obesity as a symptom, rather

than as a diagnosis? In other words: “What’s different about the

biochemical

process of fat manufacture and fat storage in obese patients – when compared

to

fat manufacture and storage in those who aren’t overweight? If we know that

answer, then we know why obesity is a symptom telling us to look at genetic,

environmental, biochemical, and hormonal factors.

 

To answer that question, we need to spend a few moments reviewing our notes

from The History of 20th-Century Fat, 101:Or, Why Low-Carbohydrate Diets

Alone Failed To Keep America Trim.

 

Obesity and Leptin: A Primer

 

When Dr. Robert C. Atkins appeared on the national scene in 1972 with the

publication of his first “Diet Revolution†guide to weight-loss, the public

quickly hailed him as a bold pioneer with a radically different approach to

dieting. The Medical Establishment was horrified, however, by the idea that

eating fat and rich food actually was a good idea. Remember, back then, and

continuing today, the cholesterol argument influenced the weight argument:

“Low

fat and low cholesterol foods are good – that’s all there is to it!â€

Until the

arrival of the famous diet doc, whose books on “no-carbohydrate†eating

would eventually be purchased by millions, most scientific thinking about

weight-loss focused on the importance of measuring (and limiting) the intake of

dietary fat and reducing total calories, along with the need for lots of

vigorous exercise.

 

But the controversial Atkins had a different idea, one that opened the door

for later challenges to the dietary dogma of obesity.

 

According to the dieting revolutionary, the real culprit in weight-gain wasn’

t fat or lack of exercise but carbohydrates – complexes of carbon and water

molecules, found mostly in sugar and starches, which the human body rapidly

stores in fat cells for future use.

 

Imagine the shock waves that must have rippled through the U.S. medical

community, when Dr. Atkins began insisting that the best way to lose weight was

to avoid all carbohydrates . . . and that eating moderate amounts of fat would

not make most people gain weight!

 

Controversial or not, the Atkins approach turned out to be reasonably

effective for millions of people, in the short run. By cutting back on

“carbs,â€

the adherents of the Diet Revolution collectively lost millions of pounds . . .

even if the lost weight was almost invariably re-gained by the dieters

within a matter of a few months. Regardless of these problems with “

weight-maintenance,†however, the Atkins strategy was generally declared to be

a success

and the weight-loss author became a household American name as a result.

 

But now let’s flash-forward 30 years and take a look around.

 

Let’s ask ourselves: What ultimately became of the “eat-no-carbohydratesâ€

approach to dieting that had made Dr. Atkins so famous?

 

Answer: Over the long haul, it simply didn’t work.

 

Why did it fail? Although the biochemical explanation is complex (we’ll

worry about the chemistry a bit later), the fundamental reason for the failure

is

easy to grasp. That reason is based on the fact that although Dr. Atkins did

a great job of focusing national attention on issues of weight-loss, he and

most of his fellow-researchers were using the wrong “model†with which to

understand how human beings get fat.

 

In a sentence: The Atkins model, like most others of his day, was based on

analyzing and controlling the foods that people eat...rather than on

understanding and then controlling (with medications, where appropriate) the

human body

’s response to those foods during the processes of digestion, fat

manufacture and fat storage. Those processes involve hormones, including

insulin and

leptin, genetics, inflammation and also discrete centers that regulate hunger

and satiety in a part of the brain, the hypothalamus. The pivotal role of

rapid rises of blood sugar after eating one common type of complex carbohydrate

starch, amylose, and its effect on insulin-driven fat storage was also

ignored. But all too soon, the lack of precision in defining “fat-causing

carbohydrates†caused motivated patients to abandon the Atkins plan and

others like it,

because the dieters weren’t allowed to eat the fruits and vegetables that

are not only safe for a weight-loss plan, but also essential in order to

maintain a reasonable “quality of life†while losing weight.

 

Dr. Atkins and his colleagues can’t really be blamed for failing to

understand that being overweight or obese is primarily a result of the

patient’s own

unique biochemistry (that is, of the multiple interactions of his or her

fat-regulating hormones) . . . and not a result of overeating or refusal to

exercise. They simply didn’t have the data on hormone interactions that in

those

days “belonged to the future†of obesity-treatment. But that future is now

here, creating a model for understanding new treatments based on molecular

biochemistry, and not on total calories or fat grams. The powerful new model of

obesity, one that includes multiple factors, tells us that managing our weight

successfully is primarily a matter of understanding and then manipulating

hormones – based on their efficiency (or lack thereof) at transporting and

transforming nutrients during the process of digestion and fat storage.

 

Sounds a bit complicated, you say?

 

Not really. All you really need to know in order to take advantage of the

molecular research that has radically changed our understanding of obesity in

recent years is one simple fact: Weight-loss is actually about hormones (such

as insulin and leptin) . . . and specifically about defeating the

“resistanceâ€

to the effect those hormones normally produce. It is hormone mechanisms

gone awry that cause us to become fat, prevent us from losing much fat when we

try, and make us gain weight – even when strictly observing the same “lower

total-calorie diets†being eaten by those without hormone abnormalities!

Obviously, those same hormone defects are also the root-cause of today’s

failure

to achieve maintenance of fat loss, among millions of struggling “yo-yoâ€

dieters.

 

The bottom line: If you’re one of the millions of Americans whose “genetic

inheritance†prevents your fat controlling hormones (and especially leptin)

from working efficiently because of hormonal resistance, the good news is that

medicine can now fix that problem with a new arsenal of medications (such as

“leptin-modifying†drugs) designed to overcome the resistance and help you

eliminate fat safely and eat good food without fear of re-gain.

 

For dieters everywhere, the future of weight-loss and weight-maintenance has

finally arrived! In the wake of the latest obesity research, it’s now

possible to reliably correct the problems of excess leptin due to leptin

resistance, and the problems of excess insulin due to insulin resistance. This

simple

fact is going to completely revolutionize the way we treat obesity in the

future.

 

Earlier in this book, you learned that leptin is a key factor in controlling

your weight because of the way it turns on the brain’s “stop-eating

centerâ€

– also known as the “satiety center.†You may also recall from Chapter 14

that this process occurs in the hypothalamus, the area of the brain that

regulates functions such as hunger, temperature and moods.

 

Now, here’s where the recent research on hunger and hormones gets really

interesting. Remember those exciting photos of genetically fat mice that

didn’t

make leptin? When they were given leptin supplements, they all lost weight.

At first glance, you might expect that a heavyset patient (let’s call him “

Mr. Overweightâ€) who’s suffering from leptin resistance (and thus from a

shortage of leptin effect in the hypothalamus, even though there’s plenty of

leptin moving through his system that normally would do its job) could be coaxed

into losing his excess poundage, simply by giving him periodic doses of leptin,

right?

 

Wrong. Extra leptin just makes Mr. Overweight fatter. Although research

shows that this approach works effectively on mice, our “leptin replacement

strategy†doesn’t translate to Mr. Overweight. Why not? Once again, the

answer

lies in biochemistry . . . in the fact that hormones can only do their work in

human cells by first binding to “receptors†(think of them as cellular “

docking stationsâ€) that must function normally to carry the hormone message

across cell membranes.

 

Key point: If the patient has leptin resistance, leptin doesn’t work

properly to connect with its “docking station†– and the hormone never

initiates

all the later effects (we call them a “cascadeâ€) that result in both

turning

off hypothalamic hunger centers and burning fat directly in fat cells.

 

Surprisingly, the major breakthrough in our understanding of how leptin

resistance helps to make people fat came from a study recently completed by our

research group in Maryland. For several years now, our group has been

investigating and publishing scientific articles on a threatening new family of

chronic “biotoxin-associated†illnesses linked to recent alterations in the

rapidly changing human environment.

 

Interestingly enough, our research group – which includes Environmental

Protection Agency neurotoxicologist Ken Hudnell, Ph.D., along with Dennis

House,

the statistician at the Center for Research on Biotoxin-Associated Illnesses

–

recently discovered a key fact that affects leptin resistance. What we

learned was that the immune responses to toxins released by microbial organisms

such as those involved in chronic ailments like fibromyalgia, Sick Building

Syndrome, and Post-Lyme Disease Syndrome also have a powerful negative impact

on the body’s leptin receptors!

 

As noted in Chapter 14, these biotoxin-linked diseases cause their multiple

persistent symptoms (fatigue, headaches, muscle aches, blurred vision,

short-term memory loss, and many more) because of the way they instantly set

off

alarm bells within the body’s disease-fighting immune system. When the

“alarmâ€

sounds, the system quickly begins to churn out some powerhouse chemicals

(known as “pro-inflammatory cytokinesâ€) designed to help neutralize and

eliminate the toxins. Illness symptoms continue when genetically susceptible

patients can’t stop the cytokine response.

 

So far, so good. But even as the inappropriate release of cytokines is

causing many adverse health effects (Remember your last bout with the flu?

Those

muscle aches, headaches, fatigue, fever and maybe some cognitive changes, too,

were due to an appropriate release of cytokines in response to the virus.

When the virus was successfully repelled, the cytokine response was stopped and

the symptoms cleared up.), our “biochemistry plot†suddenly takes another

astonishing twist. The twist occurs when the continuous bombardment of

inflammatory agents begins damaging the receptor for leptin (it is a cytokine

receptor too) in the hypothalamus – thus preventing the leptin receptors there

from

doing their proper job of allowing the hormone to turn on the satiety

center!

 

You can imagine the reaction among the members of our research group, when

we realized that we were confronting a completely new concept in weight-loss

and weight-maintenance – the notion that much of the resistance to leptin

(and

other hormones such as insulin) was actually due to cytokine-damage

resulting from exposure to environmental toxins!

 

At first we were in shock. But when we stepped back and reflected on our

find, we came to the startling realization that a high percentage of the

patients who were overweight because of insulin/leptin resistance had actually

acquired their resistance as a result of exposure to biotoxins from the

environment. As matter of fact, there is now convincing evidence to show that

about

one-third of all leptin resistance is “environmentally acquired†in this

fashion; the remaining two-thirds is the result of “endogenous†internal

genetic

factors, inherited from birth. A simple, non-invasive bedside test of visual

contrast sensitivity (VCS) can separate patients with environmental sources of

leptin resistance from those who were born with genes guaranteeing excessive

fat storage.

 

Exciting? You better believe it. Based on our studies of thousands of

affected patients, three obesity-related discoveries were now crystal-clear.

 

First: Being overweight or obese is not about food or “overeatingâ€; it’s

about resistance to fat-related hormones, which shuts down the effect of leptin

on the brain’s satiety center, among other effects, so that it fails to tell

the patient: “Stop eating!†For 98 percent of weight-loss patients, this

scenario is a major reason why they can’t lose weight and keep it off.

 

Second: For about two-thirds of these resistance-linked weight-loss patients

(and that’s about 60 million people!) internal genetic flaws related to

insulin resistance and leptin resistance account for the body’s excessive fat

storage and inability burn fat properly.

 

Third: For the remaining one-third, the resistance – and the failure to

activate the satiety center – is “exogenous†. . . meaning that it’s

actually

caused by biotoxins left behind by chronic, environmentally acquired illnesses

such as Sick Building Syndrome and the Post-Lyme Syndrome.

 

The implications of our research seem far-reaching, to say the least. For

one thing, we’re now exploring an entirely new approach to the

pro-inflammatory

cytokine syndrome that underlies not only obesity but also diabetes . . . to

say nothing of cholesterol-linked atherosclerosis caused by similar

cytokine-triggered cell membrane failures. Inflammation is the new buzzword in

heart

disease- and those same effects are felt to be critically important in many

of our “modern diseases.â€

 

For weight-loss patients, of course, these implications are far-reaching, as

well. What we read about fat and weight loss in the best-selling books didn’

t include the causative role of inflammatory effects, controlled by genes, on

fat manufacture and fat storage. No wonder the “eat less and exercise moreâ€

idea didn’t work. As if willpower had anything to do with inflammation or

genetics! We are left with one crucially important fact: If we can defeat the

inflammatory basis of leptin and insulin resistance and control the genetic

basis of those hormone resistances, we can defeat obesity!

 

In order to understand exactly why, let’s review a little bit more of our “

Biochemistry 201†review. (Hang on; we’re almost there.)

 

In recent chapters of this book, you’ve heard me talking repeatedly about

the benefits of my “No-Amylose diet†for the large number of patients who

are

overweight primarily because of insulin resistance. But now I’m going to

expand on that concept . . . by telling you how the same No-Amylose regime will

benefit those heavyset patients who suffer from leptin resistance, as well. We

are going to put the hypothalamus and inflammatory cytokines backstage for a

minute.

 

Let’s start our discussion by remembering that leptin is made from fat

cells, and it is released into the bloodstream after we eat fat. Normally, the

rising leptin will tell the satiety center that we have had enough to eat. In

the case of the leptin resistant patient, however, the effect of fat

consumption isn’t to turn off hunger; in this case, the “turn-off†signal

is simply

ignored. But the key thing to emphasize here is that more leptin is still being

made by fat cells in response to ongoing eating. All that extra leptin

affects weight-gain in two important ways. First, the hormone works to prevent

uptake (storage) of fatty acids in fat cells, keeping them suspended (free) in

the blood. Second, the leptin prevents normal fat cell burning of the fatty

acids it has already collected.

 

One incredibly important result of keeping these free fatty acids in the

bloodstream is the effect on insulin. Free fatty acids in the blood

dramatically

worsen the problem of insulin resistance if it is pre-existing, and make the

resistance appear if it isn’t–by shutting down the efficiency of insulin

receptors on muscle cells, thereby reducing intake of sugar (glucose) by

muscle. Faced with too much glucose, the liver responds by breaking down the

extra

sugar, to piece together and rearrange the sugar fragments into … more fatty

acids! The liver did its job to prevent diabetes in the leptin resistant

patient, only to make him fatter. The extra fatty acids, meanwhile,

simultaneously drive up leptin release. When that happens, an overweight patient

receives

additional signals that it’s “time to stop eating.†Unfortunately,

however,

the leptin resistance – now combined with functional insulin resistance –

prevents the body from turning off the spigot that’s causing the flood of

fatty

acids. The key point: Fat storage, without fat-burn, is activated both by

rising blood sugar and by rising fatty acid levels.

 

Without this normal “feedback control†on appetite, our leptin resistant

Mr. Overweight just keeps on eating. At the same time, the resistance fouls up

the storage system for fatty acids in the bloodstream. And the result? Poor

Mr. O gets hit twice, as a result of his leptin resistance. He eats more, and

his body does a great job of storing as fat the calories he takes in. And

don’

t forget: The fatty acids already in fat cells that normally would be used

for fuel are just sitting there, not being burned to release energy as they

should be when we have stopped eating. Without the energy from direct fat cell

burn of fatty acids, the leptin resistant patient who ate a sandwich (amylose

in the bread) or a biscuit (more amylose) for breakfast will feel sluggish

and tired about two hours later, when the sugar is gone and the fatty acids

aren

’t mobilized to keep him going. So what does Mr. O do? He eats and

“Stores!â€

some more.

 

Okay: We now understand the “double whammy†faced by those who struggle

with leptin resistance. And now the plot thickens even further..when we

remember

that the development of leptin resistance is essentially no different than

the development of insulin resistance: Both disorders are deeply affected by

both genetic inheritance and the cytokines that result from the body’s

response to environmentally acquired toxins – with both impacting the

brain’s

satiety center and the body’s physiological fat-storage mechanism.

 

To understand why this happens, let’s move in closer. When a leptin molecule

goes into position on a receptor, lots of interesting things start to occur.

First of all, the receptor activates a “second messenger,†which promptly

sends a bulletin to certain genes: Get busy and make some new fat-controlling

molecules! But what happens if the receptor balks, due to resistance? In that

ugly situation, the second messenger is never dispatched, and the new

anti-fat molecules don’t get manufactured. In the end, the entire biochemical

cascade of effects – the process that should limit excessive fat-manufacture

for

the struggling Mr. O – gets shut down, and he winds up putting on more flab.

 

Question: Are you beginning to see, now, why “eating fewer carbohydrates and

getting more exercise†simply won’t get the job done – for 98 percent of

those who are significantly overweight? If you do, welcome to the brand-new

Leptin Resistance Era in American dieting!

 

But if our poor Mr. O has no chance to control his weight-gain through sheer

“will power or exercise†what hope is there for him?

 

Enter now the fabulous Greek god Panacea (even as we say “Bye-bye†to

Hygeia!), the inventor of medicines, who’s carrying a very hopeful message

for all

of us: the recognition that, once we properly identify the real culprits in

obesity, hormone resistance, genetics and inflammation, we can use

appropriate drugs to rapidly offset their impact and restore a healthy

biochemistry.

 

The really good news for all of us here is that these drugs will work –

unlike the Atkins approach, which relied on people eating fat each day to

activate their leptin production and thereby turning on the satiety center.

(This

was the real reason why Atkins sold all those books, by the way; his diet kept

people from feeling hungry and miserable most of the time!) But Dr. Atkins’s

technique failed, in the end, because it didn’t factor leptin resistance or

insulin resistance or inflammation into the dietary equation for fat. Nor did

he properly understand the crucial role played by amylose – the key

carbohydrate that triggers a rapid rise in blood sugar and thus triggers both

insulin

and leptin resistance. (Sure, Atkins recommended that people stop eating

carbs – but he failed to see the great importance of amylose as the

carbohydrate

that primarily sets off insulin resistance. Dieters of the world: Avoid

amylose.)

 

Based on the latest discoveries at the molecular level, science now

understands that the truly effective way to keep weight off is to reduce leptin

and

insulin resistance. For many people – those who own genes that cause the

resistance – the solution to being overweight will likely mean taking a

medication

that blocks the overactive leptin response and the overactive insulin

response every day, in order to overcome their flawed internal chemistry.

 

For those of us whose leptin resistance is an environmentally acquired,

inflammatory illness, however (an office worker who’s struggling with

biotoxins

from the “Sick Building†where he or she works each day, for example), the

solution to the weight problem begins with removal of the offending toxins from

the bloodstream.

 

And what about the two percent of overweight patients who don’t have either

endogenous or acquired leptin resistance? For this tiny minority, the old

rules still apply; to lose weight, they will have to eat less and exercise

more!

 

Okay, time for the next Big Question: Does Dr. Shoemaker really have solid,

convincing research data on which to base his recent claim that about

one-third of all leptin-resistance comes from the chronic biotoxin illnesses

that

are now spreading rapidly across America? (I thought you’d never ask.)

 

The answer, of course, is a resounding “yes.†Quite recently, Dr. Ken

Hudnell, Dennis House and I presented an academic paper on Sick Building

Syndrome

in which we analyzed 21 SBS patients who were working in five different

buildings crawling with toxic mold. After we documented the numerous symptoms of

chronic, biotoxin-associated illness (see Chapter 14, if you want a review) –

including chronic fatigue, high leptin levels and deficits in the special

neurotoxicology test, VCS – we prescribed a toxin-binding and

toxin-eliminating

medication (cholestyramine, CSM) that would help them shrug off the poisons

and restore their health, while also correcting their VCS deficit.

 

As we expected, the patients improved dramatically within a couple of weeks –

and all experienced an immediate reduction of their leptin resistance, with

resultant weight loss! In other words, as our published and scientifically

verified findings presented at recent meetings of both the 83rd Endocrine

Society (6/01) and the American Diabetes Association (6/02) made clear, these

unhappy folks were actually being made sick and tired and fat by their toxic

environments!

 

In order to test our hypothesis prospectively (this part of the study

provides definitive proof of causation), we stopped the medication briefly in

order

to observe the effect of avoidance of the implicated building. The symptoms,

VCS scores and leptin levels didn’t change. We then watched as the patients

returned to their toxic indoor environments, without CSM to protect them.

Within three days, when we looked at them again, their biotoxin-illness

symptoms

had returned, their VCS scores had plummeted and their leptin resistance was

soaring again. We then re-treated the patients, while they were still being

exposed to the now-confirmed Sick Building, and saw a return to the baseline

treated state, without symptoms, VCS deficits and overproduction of leptin.

 

The fact that we confirmed the leptin-changes within three days didn’t

surprise us, since we knew that the adverse effects on leptin receptors from

cytokine responses to biotoxins occurs almost instantaneously. The rapid shifts

in

leptin were associated with changes in weight as well. Falling leptin,

meaning reduced cytokine effects on leptin receptors, gave weight loss, with no

changes in diet. Rising leptin, again without dietary changes, gave weight

gain. Later, when these patients left their sick buildings behind and then

flushed the biotoxins out of their bodies once and for all with CSM, they all

lost

impressive amounts of weight, without changes in diet. If our data on several

thousand patients with biotoxin illnesses seems like a small number,

remember our studies are only several years old and were performed in a rural

area

of Maryland. How many cases of Sick Building Syndrome are there if 10% of the

workplaces and 15% of the schools in America have toxin-forming fungi as

NIOSH stated several years ago? How many of those patients are part of the

Obesity Epidemic that is currently being blamed on sedentary lifestyle,

self-indulgent eating and dietary excess? We won’t know the answer if we

don’t know to

ask the question.

 

All right, then: We’re almost to the finish line now, in our effort to

understand how controlling the body’s hormone resistance (insulin, leptin)

will

help us to control our weight. But one obvious question remains: What

medications can help us most here, and what’s the basis for their

effectiveness in

shutting down resistance?

 

Panacea, may I have the envelope, please?

 

And the winner is . . . the thiazolidinedione family of medications, which

we can simply call “TZDs,†in order to avoid the horrors of pronunciation.

These medications – they’re commonly used to control diabetes, by the way

–

consist primarily of two key substances, pioglitazone and rosiglitazone, and

they work by turning on a string of valiant, fat cell-based genes (known as “

PPAR gammaâ€) that produce many powerful organic compounds. TZDs block

excessive

inflammatory cytokine production, lower leptin, increase fatty acid uptake

into fat cells and activate direct burning of fatty acids inside fat cells

(Chapter 13). What more could an insulin/leptin resistant patient want? These

compounds work effectively to help offset both leptin and insulin resistance,

in other ways, too, but this time I’ll spare you the complex chemistry. Of

great interest for weight loss is the discovery that all these wonderful

benefits from use of TZDs disappear when the patient begins to add amylose into

his

diet. Even worse, weight gain, some due to fluid retention, also occurs when

TZDs are used in conjunction with a diet that includes amylose. Remember: If

you are considering TZDs, you must use the No-Amylose diet, without fail.

 

In an earlier chapter, you read how we can use TZDs to help lower insulin

resistance, and also control diabetes. Understandably enough, the U.S. Food and

Drug Administration (which regulates the use of medicines in this country)

long ago designated – or “labeled†– TZDs as a diabetes medication.

This

means that our use of the substance for weight-loss will have to be

“off-label,â€

as the doctors say . . . but so what? In fact, physicians prescribe such

off-label usage of medications day in and day out: Such usage is strictly

routine, and perfectly legal and ethical – provided only that the patient is

properly informed of the “off-label†status. We always monitor liver

function

tests in our patients who take TZDs, just like we do with the statin

cholesterol-lowering drugs, but especially because an earlier TZDs,

troglitazone, was

blamed for causing liver disease and was pulled from the market. No one, in my

opinion, should consider using TZDs for targeted gene therapy of leptin

resistance, insulin resistance and weight loss, until he has been evaluated

carefully by a physician, found to have obesity refractory to standard measures

and

been shown to be able to stay on the No-Amylose diet. Then, following

informed consent, the patient can take the drug under strict medical

management.

 

Welcome, then, to the Brave New Weight-Loss World of using TZDs to

dramatically reduce leptin resistance and thus help overweight patients attack

the

real culprit behind their flabbiness. By using TZDs in combination with a

No-Amylose diet, we can now achieve results that Dr. Atkins and his fellow

fat-book

authors only dreamed of: We can control body-weight almost at will, and

without starving our patients half to death in the process!

 

This breaking news about the wonders of TZDs will be especially welcome

among the estimated 30 million Americans whose overweight status is due to

chronic, biotoxin-associated illnesses, such as Sick Building Syndrome and some

cases of Chronic Fatigue Syndrome. For these individuals, a few weeks of CSM

therapy will kick off the complex process that underlies effective treatment.

Once the toxins that are causing their leptin resistance are removed and the

hypothalamic pathways that leptin activates are working normally again

(sometimes, this is process quite complex), what we will see is a removal of

the

leptin resistance, which will then allow patients to shed their excess poundage

quickly and painlessly.

 

The enormously hopeful news for overweight patients everywhere is that your

hour of liberation is at hand. Instead of blaming yourselves (or being blamed

by Dan Rather & Co. on national television) for your fat, and instead of

blaming Burger Doodle for serving up too many triple-cheeseburgers, we’re

going

to put the blame where it belongs: on human biochemistry, and on the

insulin/leptin resistance which is the legacy of our biological evolution – as

creatures whose forbears lived for countless millennia (as hunter-gatherers)

under

conditions of “feast or famine. "

 

Make no mistake: The Obesity Epidemic isn’t anyone’s “faultâ€; it is

simply

a product of our history. Until the arrival of mechanized agriculture, only

about a century ago, the human body had never been exposed to a continuous

flood of sugars and fats – a flood that now never stops. For at least 200

centuries, and probably much longer, the human response to such sugars and fats

had been: “Convert this stuff to fat, so that it will carry us through the

next

famine!†Remember: The famines prevented repetitive blood sugar-rises and

blood fatty acid rises; during the long spells without much food, the fat

storage process would slowly unwind, releasing stored energy, allowing

primordial

populations to survive winter and drought.

 

Is it any wonder, given this evolutionary reality, that many contemporary

humans with hormonal resistance, both genetic and acquired, when exposed to an

endless flood of excess nutrients, are turning into chunky, double-chinned

folks who closely resemble our struggling Mr. O? And is it any wonder, given

the explosion of buildings with indoor resident toxin-forming fungi, now

bathing the HVAC with mycotoxins-of-the-day, that thousands and thousands of

patients who work, live or go to school in these buildings are getting fat? Add

in

the many other biotoxin-forming organisms that seemingly are emerging from

the mud each month, and we see the Obesity Epidemic in a whole new perspective:

It isn’t the calories we eat that counts, it is the calories that we store

as fat. Cytokines are necessary for life; excess downstream cytokine effects

cause excess weight that won’t go away by using willpower and pushing away

from the table.

 

Ladies and gentlemen, the Brave New World of Weight-Control has already

begun. Armed with TZD and a new, rapidly growing understanding of molecular

physiology in human beings, we’re going to go far beyond the early

contributions

of Dr. Atkins and his fellow-authors. We’re going to enter – have already

begun to enter – a world in which losing excess weight and keeping it off

will

be about as difficult as having your teeth cleaned by the dental hygienist (we

can’t escape Hygeia altogether).

 

We’re also about to enter a world in which fat people – folks like Mr.

Overweight and the “American Waddler†– will no longer be denigrated as

failures

who couldn’t control their own eating habits. Instead of being made cruel

sport of, they’ll be able to quickly and painlessly solve their

weight-problems

by asking a physician to measure their levels of insulin, leptin and

cytokines, while also testing them with Visual Contrast Sensitivity and seeking

symptoms that could be related to environmentally acquired, biotoxin-induced

leptin and/or insulin resistance. (For more information about these easily

performed tests and the TZD- and cholestyramine-based therapies that will help

overweight patients to lose their excess pounds rapidly and easily, visit

_www.chronicneurotoxins.com_ (http://www.chronicneurotoxins.com) on the

Internet.)

 

In summary, then: The bottom-line message of this chapter – and the message

of LOSE THE WEIGHT YOU HATE – is that the Battle Against Fat has nearly been

won. All that remains now is the process of educating ourselves about the

actual physiology involved . . . and then taking the necessary steps to keep

obesity at bay through the judicious use of effective medications such as TZD,

while also remaining vigilant about over-consumption of those relatively few,

amylose-based foods that also trigger hormonal resistance.

 

Dieters, rejoice: As this new world of molecular-based weight therapy takes

off in earnest, you are going to live much better, healthier lives. You have

nothing to lose but your flab!

 

 

 

 

--

 

500 Market Street Pocomoke City, MD 21851 _info@chronicneurotoxins_

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Privacy Policy | © 2002-2008 ChronicNeurotoxins, Inc.

 

 

Prior to launching a new version of this website in June, 2002, the earlier

version had been online for about a year and a half. Over 3,600 registered

users had taken the preliminary and VCS tests. About half of the test results

were positive for potential chronic, neurotoxin-induced illness. We do not

know exactly how many of those used our treatment protocol with their local

physician, or the outcome for all that did. We do know, however, that many used

the protocol with success, and that many others were successfully treated by

Dr. Shoemaker or another physician.

 

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