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                      Dr. Barry Sears 
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                    		|  |  |  OMEGA 3 BENEFITSSilent Killer: The Link between 
                Obesity and Type 2 Diabetes
 CBN.com  
                 Obesity is one of the biggest generators of silent inflammation. 
                Since nearly two-thirds of Americans are now overweight, this 
                means that the epidemic of silent inflammation is also out of 
                control. By the same token, our diabetes epidemic has grown by 
                33 percent in the last decade. It should come as no surprise that 
                all three epidemics have worsened in recent years. All three are 
                intricately connected with a condition known as insulin resistance. Insulin resistance occurs when your cells become less responsive 
                to the actions of insulin, forcing your pancreas to continuously 
                produce more insulin to drive glucose into cells. This excess 
                insulin (produced as that response to insulin resistance) also 
                increases the storage of body fat. So the real question behind 
                our current obesity epidemic is what actually causes insulin resistance? 
               No one knows for sure, but there is a growing opinion that the 
                molecular cause of insulin resistance may originate in the endothelial 
                cells. Endothelial cells form a very thin barrier that separates 
                the bloodstream from your organs. If this barrier is not working 
                very well, you have a condition called endothelial dysfunction, 
                which means among other things that insulin can no longer easily 
                pass from the bloodstream through the endothelial barrier to interact 
                with its receptors on the cell surface. It’s only when insulin 
                interacts with these receptors that the cell can take up glucose 
                from the bloodstream. Any difficulty insulin has in getting to 
                its receptors will keep blood glucose levels elevated. The body 
                responds by pumping out still more insulin, now creating a condition 
                known as hyperinsulinemia. Obesity from a Different ViewWhat if the epidemic rise in obesity in the last twenty years 
                was not primarily due to the usual suspects (fast food, TV, junk 
                food), but fueled by increased silent inflammation, which increases 
                insulin resistance? This means that unless you reduce the underlying 
                silent inflammation, any other approach to reduce obesity may 
                be doomed to failure. This also means that simply restricting 
                calories will not be enough to turn back our current obesity epidemic.
 I believe that obesity starts with excess arachidonic acid (AA). 
                (Click 
                here to read more about Arachidonic Acid.) You can increase 
                arachidonic acid in the bloodstream either directly by eating 
                too much of it (it’s particularly high in fatty red meats 
                and egg yolks) or indirectly by consuming too many high glycemic-load 
                carbohydrates, which increase insulin production, which in turn 
                promotes increased AA production. Either way, the body goes to 
                great lengths to take any excess AA out of the circulation and 
                store it away in your fat depots in an effort to keep inflammation 
                under control.  Here is where the trouble starts, because fat cells aren’t 
                simply inert balls of lard sitting on our stomach, thighs, and 
                hips. These cells are very active glands that can secrete out 
                large amount of inflammation mediators if they’re given 
                the right stimulus. As your fat cells become filled with more 
                AA, it causes an overproduction of pro-inflammatory eicosanoids 
                in the adipose (fatty) tissue.  Eicosanoids play an integral role in your health. Just ask 
                the Nobel Prize committee, which awarded the 1982 prize in medicine 
                for the discovery of eicosanoids. They are also the most powerful 
                hormones, since they affect the synthesis of virtually every other 
                hormone in your body. In a sense, you can think of eicosanoids 
                as “super-hormones” capable of bringing great health 
                benefits (“good” eicosanoids), or great harm (“bad” 
                eicosanoids), depending on which one a cell produces. Now you can probably guess what happens. These “bad” 
                eicosanoids induce the formation of new inflammatory mediators 
                that spew forth from fat cells into the surrounding circulation--and 
                generate systemic silent inflammation. Now before you start cursing all your fat, I want to emphasize 
                that all fat is not created equal. Some types of fat are far more 
                harmful than others. It depends on their metabolic activity. Subcutaneous 
                fat--the fat that collects on your hips, thighs, and buttocks 
                and makes you look like a pear--isn’t that harmful. It may 
                not look too good, but at least it won’t kill you, because 
                your body is in no rush to mobilize the AA out of these fat cells. 
                That’s why this type of fat is considered metabolically 
                inactive. It is primarily a storage depot.  On the other hand, visceral fat can be a killer. This kind of 
                fat collects around the abdominal organs, such as the liver, kidneys, 
                and gallbladder and makes you look like an apple.  How do I spot visceral fat? You may think that the easiest way to see if you have visceral 
                fat is to look at yourself in a mirror. But this may be deceptive, 
                because visceral fat is often found with in close contact with 
                subcutaneous fat in the abdominal region. The real indication 
                of the amount of your abdominal fat that is actually visceral 
                fat is measured by either your TG/HDL ratio or your fasting insulin 
                levels.
 Visceral fat is very metabolically active and causes the constant 
                release of stored AA into the bloodstream. This is the last place 
                you want excess AA, since it’s then taken up by every one 
                of your sixty trillion cells, making each one more likely to generate 
                more pro-inflammatory eicosanoids, and therefore more silent inflammation 
                throughout the body.  Visceral fat is even more insidious because it also continually 
                releases other inflammatory mediators in addition to stored AA. 
                Two of the worst are the pro-inflammatory cytokines, tumor necrosis 
                factor (TNF), and interleukin-6 (IL-6). TNF is implicated in creating 
                even more insulin resistance, whereas IL-6 triggers the liver 
                to synthesize C-reactive protein (CRP), which can stimulate your 
                white blood cells to begin to mount an inflammatory response to 
                a potential infection (even though there isn’t one). About 
                a third of the CRP circulating in your blood came directly from 
                visceral fat cells. These pro-inflammatory cytokines are produced 
                in your visceral fat as a response the increased pro-inflammatory 
                eicosanoid production caused by increased AA levels.  This means the fatter you are (really, the more visceral fat 
                you have), the more silent inflammation you generate. This is 
                the smoking gun that links obesity with increased rates of heart 
                disease, cancer, or Alzheimer’s. Anything that increases 
                silent inflammation is going to be bad for your future.  Can you be fat and healthy?Surprisingly, the answer is yes--but with a few caveats. You can 
                be overweight and in a state of wellness if you keep your levels 
                of silent inflammation under control. Since obesity generates 
                inflammation, you may have to take more fish oil than the average 
                person to reverse the silent inflammation induced by it. While 
                losing weight is slow and hard, reducing silent inflammation using 
                Ultra Refined high-dose fish oil is rapid. How much Ultra Refined 
                high-dose fish oil do you need? This depends on your diet. If 
                you are following the Zone Diet, you might only need to take 5 
                grams of EPA and DHA per day. If you follow the typical American 
                (very high glycemic-load) diet, you’ll need to increase 
                your dosage of Ultra Refined high-dose fish oil to a higher level.
 Remember, all the medical complications of obesity come from 
                the inflammation it generates. Ultra Refined high-dose fish oil 
                is an immediate antidote to that inflammation.  Keep in mind being fat and healthy can be a dangerous game to 
                play. It’s a little like lighting a cigarette with a stick 
                of dynamite. You can do it, but you have to be very careful. The 
                day you stop taking adequate levels of Ultra Refined high-dose 
                fish oil is the day your silent inflammation will return, accelerating 
                you toward chronic disease and faster aging. As long as you keep 
                your Silent inflammation Profile under control, the likelihood 
                of maintaining your wellness is pretty good in spite of your weight. 
               The one-two punch of silent inflammation and increased hyperinsulinemia 
                caused by insulin resistance if left unchecked can lead to one 
                of the most costly of chronic diseases: diabetes. The Diabetes ConnectionDiabetes used to be a very rare disease, but times have changed. 
                Over the last twenty years, it has become an epidemic. Okay, let 
                me clarify this. Type 2 (adult-onset) diabetes has become an epidemic, 
                while type 1 (juvenile) diabetes still remains relatively rare. 
                Type 1 diabetes is caused by a condition in which the pancreas 
                completely shuts down and fails to produce any insulin, causing 
                blood sugar levels to spiral upward out of control. The more common 
                type 2 (90 percent of all diabetics have this version) occurs 
                when the patient develops long-term insulin resistance. As I mentioned 
                above, insulin resistance causes the pancreas to secrete more 
                insulin (hyperinsulinemia) in an effort to reduce blood glucose 
                levels. Eventually the pancreas (really the beta cells in the 
                pancreas) just get tired and stop producing enough excess insulin. 
                This is called beta-cell burnout. The result is that without enough 
                insulin becoming secreted by the pancreas, blood glucose levels 
                begin to raise to dangerous levels. The danger comes from two 
                factors; (a) excess glucose in the blood produces free radicals 
                (oxidative stress), and (b) excess glucose is neurotoxic to the 
                brain. Hyperinsulinemia usually precedes the development of type 
                2 diabetes by about eight years, but they both come from increased 
                insulin resistance. Starting to see the connection?
 Obviously, not everyone who is has insulin resistance becomes 
                a type 2 diabetic. However, enough do--there are an estimated 
                16 million Americans afflicted with type 2 diabetes. This devastating 
                disease puts a person at a 2 to 4 times greater risk of dying 
                from heart disease and also increases the likelihood of kidney 
                failure, blindness, impotence, and amputation. Because of these 
                expensive complications, type 2 diabetes is the most expensive 
                of all chronic diseases, costing approximately $132 billion per 
                year. As our obesity epidemic increases, so will the epidemic 
                of type 2 diabetes. That’s very bad news for the health 
                care industry.   The good news is that taking Ultra Refined high-dose fish oil 
                to reduce silent inflammation (the molecular cause of insulin 
                resistance) and following the Zone Diet will help reduce hyperinsulinemia 
                (the consequence of insulin resistance) and begin to reverse type 
                2 diabetes in just six weeks. 
 Excerpted from The Anti-Inflammation Zone - Reversing The 
                Silent Epidemic That's Destroying Our Health. Copyright 2005 
                by Barry Sears, Ph.D. Used by permission. 
 *These statements have not been evaluated by the Food and 
                Drug Administration. This product is not intended to diagnose, 
                treat, cure, or prevent any disease. As with any natural product, 
                individual results will vary.   For more information about Dr. Barry Sears, his incredible fish 
                oil supplements, or the popular Zone Diet, please visit www.zoneliving.com. If you purchase any Zone Labs, Inc. products, part of the 
                proceeds support CBN ministries.  Dr. Barry Sears is a leader in the field of 
                dietary control of hormonal response. A former research scientist 
                at the Boston University School of Medicine and the Massachusetts 
                Institute of Technology, Dr. Sears has dedicated his efforts over 
                the past 25 years to the study of lipids and their inflammatory 
                role in the development of chronic disease. He holds 13 U.S. Patents 
                in the areas of intravenous drug delivery systems and hormonal 
                regulation for the treatment of cardiovascular disease.  
 
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