Saturday, January 31, 2009

Adrenal Cortex's Aldosterone

No, aldosterone is not a new dietary supplement to pump you up the size of Arnold. It’s a hormone made up by your adrenal glands to help you hold onto sodium and rid off potassium whenever needed (1).

How is aldosterone released?
  • Particularly it begins with the electrolyte-fluctuation-sensitive kidneys (1). They stimulate aldosterone production by secreting renin, a proteolytic enzyme (1). The secretion happens whenever there is decreased perfusion pressure that’s sensed by receptors in the kidneys’ juxtaglomerular apparatuses (“kidney brains” that tell the kidneys’ functional units, its nephrons, what to do) (1). The renin hydrolyzes angiosteninogen, a free-wheeling protein coming from the liver, to angiotensin I (1). Another enzyme, appropriately named angiotensin-converging enzyme (ACE), converts angiotensin I to angiotensin II. Angiotensin II interacts with adrenal cortical cell receptors and voila! aldosterone is released (1).
  • Decreased atrial natriuretic peptide will stimulate release. This hormone from atrial cells ends up occurring if blood pressure elevates and, as opposed to aldosterone, causes excretion of sodium (1).
  • Other possibilities for release are increased potassium concentration, increased ACTH, or decreased sodium (1).

Aldosterone and hypertension

High aldosterone levels are also a good indicator for transient ischemia attack and stroke (2-4). ACE inhibitors are a leading therapy (and subject to numerous new research papers) for intervening in the renin-angiotensin-aldosterone system along with angiotensin II type 1 receptor antagonists (2-4). The research on these are proving they are useful for those with hypertenstion and helping to prevent cardiac arrhythmias and sudden cardiac death (2-4).

Vitamin D appears to have association with aldosterone and hypertension. Just a few days ago a French study reported what many have suspected--that as the seasons change and the days become warmer, blood pressure begins to lower (5). And according to ScienceDaily, the study may be explained due to vitamin D deficiency (6).

The data is supported by the Framingham Heart Study and Nurses Health Study, which found vitamin D deficiency increased risk of hypertension, heart attack and stroke (6). A 1989 study that showed that long-term vitamin D supplementation lowered blood pressure in patients with essential hypertension (7).

References

1. Gropper SS, Smith JL, Groff JL. Advanced Nutrition and Human Metabolism, 5th ed. Belmont, CA: Thomson Wadsworth, 2009, p 553.

2. Ishiguro K, Hayashi K, Sasamura H, Sakamaki Y, Itoh H. "Pulse" treatment with high-dose angiotensin blocker reverses renal arteriolar hypertrophy and regresses hypertension. Hypertension 2009;53:83-9.2.

3. Makkar KM, Sanoski CA, Spinler SA. Role of Angiotensin-Converting Enzyme Inhibitors, Angiotensin II Receptor Blockers, and Aldosterone Antagonists in the Prevention of Atrial and Ventricular Arrhythmias. Pharmacotherapy 2009;29:31-48.3.

4. Qian C, Schoemaker RG, van Gilst WH, Roks AJ. The role of the renin-angiotensin-aldosterone system in cardiovascular progenitor cell function. Clin Sci (Lond) 2009;116:301-14.4. Vyssoulis GP, Karpanou EA, Tzamou VE et al. Aldosterone levels and stroke incidence in essential hypertensive patients. Int J Cardiol 2009.

5. Alperovitch A, Lacombe JM, Hanon O et al. Relationship between blood pressure and outdoor temperature in a large sample of elderly individuals: the Three-City study. Arch Intern Med 2009;169:75-80.

6. ScienceDaily. Blood Pressure Varies by the Season. 20 Jan 2009. Available at: http://www.sciencedaily.com/releases/2009/01/090116091523.htm

7. Lind L, Wengle B, Wide L, Ljunghall S. Reduction of blood pressure during long-term treatment with active vitamin D (alphacalcidol) is dependent on plasma renin activity and calcium status. A double-blind, placebo-controlled study. Am J Hypertens 1989;2:20-5.

Sunday, January 25, 2009

Exercise lowers inflammation associated with heart disease

A study published in 2005 evaluated levels of C-reactive protein in sedentary men and women when placed on an exercise training program for five months. The patients significantly reduced the C-reactive proteins in the blood. 

High levels of C-reactive protein in the blood indicates inflammation associated with heart disease, stroke and hypertension. 

The patients who exercised also produced marked changes in body weight, glucose, LDL cholesterol, HDL cholesterol, triglycerides, and blood pressure. 

What does this mean? That despite all my efforts to avoid exercise by living an otherwise healthy lifestyle, I gotta head to the gym. Or else.  

Reference

Lakka TA, Lakka HM, Rankinen T, Leon AS, Rao DC, Skinner JS, Wilmore JH, Bouchard C. Effect of exercise training on plasma levels of C-reactive protein healthy adults: the HERITAGE Family Study. European Heart Journal, 26, 2018–2025, 2005 doi:10.1093/eurheartj/ehi394

What? Another possible risk factor for heart disease?

More research is needed to determine if hyperhomocysteinemia may be a risk factor to heart disease, but if it is, then that's just another reason to eat less meat (1). Eating meat increases levels of homocysteine in the blood (1). Leafy greens and a variety of fruits in the diet supplies folic acid and B vitamins, which help break homocysteine down (1). Vitamin B12 (almost exclusive to meat) helps as well so choosing to give up meat entirely is not advisable (1).

Reference
Web MD. Homocysteine: Heart disease risk. Available at: http://www.webmd.com/heart-disease/guide/homocysteine-risk

Fats and Heart Disease

Just because fats don't have a direct affect on heart disease, it doesn't mean they shouldn't be worried about. Saturated fats and trans fats increase LDL cholesterol in the blood (1) creating a greater situation of LDL oxidation, which contributes to inflammation that is the cause of heart disease. A diet with a high ratio of omega-6 to omega-3 oils creates a proinflammatory state (2), which also enhances risk. 

Through knowledge of fats and how they affect the body in different ratios, it is possible change course of health. Additional omega-3 fatty acids and lesser amounts of saturated fats, trans fats, and omega-6 fatty acids could largely benefit through reduction of LDL cholesterol in the blood, reduction of triglycerides and less inflammation.

References

1. http://www.mayoclinic.com/health/fat/NU00262
2. http://www.medscape.com/viewarticle/555736

Cause of Heart Disease: Inflammation? Yes, but don't forget cholesterol's role

The medical establishment in the U.S. has been professing benefits of controlling cholesterol since 1985, because of research linking cholesterol to atherosclerosis and coronary artery disease (1). Short sighted, however, is the regard to these diseases as based completely on excess cholesterol as often assumed (2-3). 

New research has proved that an assay of C-reactive proteins in the blood can predict coronary artery events (2). The higher C-reactive proteins are in the blood, the higher risk of an event and less likelihood of survival from the event (2). The C-reactive proteins, which increase during inflammation, suggest heart disease itself is an inflammatory condition (2). 

If inflammation is the cause of heart disease, then inflammation should be the target of therapy, but it's important to not forget the link between cholesterol and heart disease. The atherogenic nature of LDL cholesterol in the arteries (now considered an independent factor to heart disease) leads to oxidation of LDL, which produces low-grade inflammation (2-3)! LDL is still partly to blame. Further, these findings bring oxidative stress in as a factor. 

There are also many other causes of low-grade inflammation associated with coronary artery disease such as smoking, high blood pressure and hyperglycemia (2). These also produce oxidation of LDL. In fact, those with insulin resistance due to hyperglycemia also show an increased amount of oxidized LDL (4). 

My opinion on heart disease is formed by all the different sides. Moving a patient from a pro-inflammatory state to a healthy state requires medical treatment and diet designed to take in all factors. These should include levels of C-reactive proteins, LDL cholesterol, oxidation of LDL cholesterol and other causes of inflammation.   

References

1. FDA. Available at: http://www.fda.gov/bbs/topics/CONSUMER/CON00052.html
2. AHA. Available at: http://www.americanheart.org/presenter.jhtml?identifier=4648
3. AHA. Atherogenic lipoprotein particles in atherosclerosis. Available at http://circ.ahajournals.org/cgi/content/full/109/23_suppl_1/III-2
4. Scazzocchio B, Varì R, D'Archivio M, Santangelo C, Filesi C, Giovannini C, Masella R. J Lipid Res. 2009 Jan 9. [Epub ahead of print] Links
Oxidized low-density lipoproteins impair adipocyte response to insulin by activating serine/threonine kinases. Available at: http://www.ncbi.nlm.nih.gov/pubmed/19136667?ordinalpos=13&itool=EntrezSystem2.PEntrez.Pubmed.Pubmed_ResultsPanel.Pubmed_DefaultReportPanel.Pubmed_RVDocSum

Goods and Bads of Antipyretic Therapy

Should antipyretic therapy be used at all?

A fever is a natural response to infections, toxins, immunologic diseases or injury in many a warm-blooded animal (1p58). It can help enhance immune system function and filtering out of infection through phagocytosis (1p58). The elevated temperature also can interfere with bacteria's ability to grow and reproduce (1p58). 

"Goods" of Antipyretic Therapies

 A fever should max out at 105 degrees Fahrenheit, but if it reaches 106 degrees then a potential malfunctioning hypothalamus means it's time to go to the emergency medical care (1p58). The fever is to the point that cranial pressure is posing a risk to the brain, the heat may interfere with cardiac function in compromised patients, and the elevated core temperature could hurt a fetus if pregnant (1p58). 

It's time to intervene with antipyretic therapy. Wet cloths, cool blankets, ice baths and cold IVs all help to offset the elevated temperature (1p59). Drugs like aspirin, or acetylsalicylic acid), and acetaminophen work by inhibiting prostaglandin production in the hypothalamus blocking their signals and effectively reducing the body's temperature set point to that of near normal levels (1p59). 

"Bads" of Antipyretic Therapies

Aspirin and acetaminophen all are blockers of cyclooxygenase (COX) activity (1pp40-41). There are two isoforms of COX. COX-1 maintains the the gastric mucosa, regulates perfusion in the kidneys and is involved in platelet aggregation needed for coagulation (1pp40-41). COX-2 mediates inflammation and prostaglandin production. Because the antypyretics are not selective in which COX they inhibit, they damage the gastric mucosa, acetaminophen is toxic to the kidneys, and aspirin diminishes platelet function (1pp40-41). Children should also avoid use of aspirin because of it is associated with Reyes syndrome (1p59).

Reference

1. Nowak TJ, Hanfod AG. Pathophysiology: Concepts and applications for health care professionals, 3rd ed. 2004. New York, McGraw-Hill, pp58-60. 

Don't mix Tylenol and Motrin

I've got a fever right now that's driving my head crazy. After reading my Pathophys chapters I've got a wet cloth on my forehead. But still it's making it very difficult to take the dive into my exam. 

Pain stinks. I'm strongly considering that Tylenol/Motrin combination. But, no... 

While multimodual analgesic combinations such as Tylenol and Motrin do provide significantly more pain relief, the safety of this kind of use has not been completely determined, at least since 2001 (1). But, pending further, research, combinations could be useful such as before surgery (2-3). 

Reference

1. http://www.americantherapeutics.com/pt/re/ajt/abstract.00045391-200111000-00008.htm;jsessionid=J8LWFGlcf03xsySCLsR15pGrc1w1yVLGzL6F7jjh4n2l1rqdQPcc!-1854079795!181195628!8091!-1

2. http://linkinghub.elsevier.com/retrieve/pii/S1366007104000749

3. http://www.anesthesia-analgesia.org/cgi/content/abstract/105/1/228

Don't take Tylenol without protecting your liver

Acetaminophen like Tylenol depletes glutathione and damages the liver (1), but chances are people won't be getting away from using them anytime soon. What can be done is help protect the liver from damage induced through supplementation. 

Silymarin (from milk thistle) may serve as a support while taking acetaminophen. In a rat study, acetaminophen decreased glutathione and glycogen quickly (1). Unlike the control, rats taking silymarin showed no significant increase in lipid peroxidation or disruption of enzyme activities (1). Thus, while the silymarin didn't prevent glutathione depletion in rats, it did protect the liver possibly through antioxidant properties and helped with restoring glycogen (1). 

Human studies have not yet been conducted, but many doctors already recommend silymarin supplements based on its recent research (2). 

Reference

1. Muriel, P; Garciapina, T; Perez Alvarez, V; Mourelle, M. Silymarin protects against paracetamol-induced lipid peroxidation and liver damage. J Appl Toxicol. 1992 Dec; 12(6): 439-42

2. http://health.med.umich.edu/healthcontent.cfm?xyzpdqabc=0&id=6&action=detail&AEProductID=HW_CAM&AEArticleID=hn-1072008&AEArticleType=Cam

What's the most important part of the cell?

The earliest cell is thought to have emerged at least 3.8 billion years ago at a time when the environment was anaerobic in nature (1-2). It is suggested that simple organic molecules formed and gave rise to a self-replicating RNA that found itself within a phospholipid membrane (2).   

The evolution of metabolism began with glycolysis (2), the sequence of reactions would produce life's universal energy source: ATP (1-3). Photosynthesis and oxidative phosphorylation would come later (2). 

While cells may not need certain parts to remain living, all still depend on glycolysis to generate energy (2). The pathway is contained within the cytoplasmic matrix (1-2). Thus, I propose the cytoplasmic matrix is the most important part of the cell. 

References

1. Dennison KJ, Topping J, Caret RL. General, Organic, and Biochemistry. New York: McGraw-Hill, 2007.

2. Cooper, G.M. "The Origin and Evolution of Cells." The Cell: A Molecular Approach. Available at: http://www.ncbi.nlm.nih.gov/books/bv.fcgi?rid=cooper.section.90.

3. Gropper SS, Smith JL, Groff JL. Advanced Nutrition and Human Metabolism, 5th ed. Belmont, CA: Thomson Wadsworth, 2009.

Saturday, January 24, 2009

Trust a biochemist

At the molecular level of life matters may be small and energy gains and losses seemingly insignificant, but a broad understanding of biochemistry leads to profound, larger conclusions of cell biology and the energy of which is ultimately the existence of life. Just as the smallest ingredient such as a dash of salt can change the flavor of a recipe, the cell can be affected by the slightest difference that ultimately means life or death.

Biochemical knowledge, in short, is fundamental for comprehending cells. And because cell biology is fundamental to all biological sciences, lack of biochemistry training severely limits the would-be biologist, medical practitioner, and health practitioner. 

So be sure to ask your doctor, nutritionist and nutrition science writer, "How's your biochemistry?" If they can adequately explain the difference between activation energy and change in free energy (see last post), then they pass the test. If they roll their eyes at you, be cautious.

The reason why hemolytic anemia probably exists

Hemolytic anemia

Within the cytoplasmic matrix of a red blood cell occurs an anaerobic pathway of glucose catabolism known as glycolysis consisting of 10 reactions (1). The enzyme that catalyzes the last reaction is pyruvate kinase (1). The reaction is one of two that produces ATP and also pyruvate, the molecule generally converted to acetyl CoA for entry into aerobic respiration (1). A deficiency of pyruvate kinase results in low ATP levels (2). It is one of the most common defects of a blood cell (2).

A young red blood cell, or reticulocyte, starts out with organelles and then loses them. While retaining their mitochondria they require a lot more oxygen and if it goes through the spleen while in this stage it could mean its failure, since the spleen is deficient in oxygen and glucose (2).

Lack of sufficient energy causes failure of ion pumps leading to a disrupted intracellular electrolyte concentration (2). The performance of the pentose phosphate pathway is diminished (2). The pathway is necessary for anabolism of glutathione, necessary for the cell’s defense against oxidative stress (2). Membrane injury results in distortion, rigidity and dehydration of the cell (2).

Eventually the red blood cell is filtered out by the spleen or liver (2). A hemolytic anemia occurs due to low blood count resulting from the rate of red blood cells lost outnumbering the rate of production of red blood cells by bone marrow (3). Because red blood cells carry oxygen via their hemoglobin, anemia reduces oxygen distributed in the body (3).

How did a defect such as hemolytic anemia such as sickle cell make it into the human gene pool?

You might find it interesting to learn that the latest research into sickle cell and other hemolytic anemias suggest the diseases may have acted as a protective mechanism against malaria. The theory has been tested in mice and humans (4-6). It is suggested that the rapid elimination of infected red blood cells may have increased overall survival to infection (4;6).

References

1. Dennison KJ, Topping J, Caret RL. General, Organic, and Biochemistry. New York: McGraw-Hill, 2007.

2. Frye, R. E. and Deloughery, T. G. Pyruvate Kinase Deficiency. WebMD . 12-31-2008. Ref Type: Online Source

3. National Heart and Lung Institute. Hemolytic Anemia. Diseases and Conditions Index . 2006. Ref Type: Online Source

4. Min-Oo G, Fortin A, Tam MF, Gros P, Stevenson MM. Phenotypic expression of pyruvate kinase deficiency and protection against malaria in a mouse model. Genes Immun 2004;5:168-75.

5. Min-Oo G, Tam M, Stevenson MM, Gros P. Pyruvate kinase deficiency: correlation between enzyme activity, extent of hemolytic anemia and protection against malaria in independent mouse mutants. Blood Cells Mol Dis 2007;39:63-9.

6. Durand PM, Coetzer TL. Pyruvate kinase deficiency protects against malaria in humans. Haematologica 2008;93:939-40.

How does stuff happen anyway?

Activation Energy

A sling shot metaphor can be used to help understand activation energy. In endothermic reactions—like the force used pull the rubber strip of a sling shot—activation energy is the energy invested to raise reactant molecules to an "elevated" intermediate state. In exothermic reactions—like the force of letting go of the rubber—activation energy is also the energy required to release the reactant molecules in exothermic reactions. Enzyme catalysis can reduce the amount of activation energy needed.  

Change in Free Energy

Change in free energy is the amount of energy that occurs at a standard condition in which there is a precise temperature, pressure and concentration of reactants and their products. It is calculated as the difference between free energy of the reactants and the content of the products in that standard condition.

Reference

Gropper SS, Smith JL, Groff JL. Advanced Nutrition and Human Metabolism, 5th ed. Belmont, CA: Thomson Wadsworth, 2009, pp 22-26. 

Animation

http://205.246.6.53/cooper/4e/animations0301.html

Sunday, January 18, 2009

Don't drink and eat french fries


A high-fat diet and alcohol may lead to a harmful combination. A proposal in Am J Clin Nutr in 2006 proposed that cells containing extra fat made them more susceptible to lipid peroxidation. The hypothesis is because of a tie between elevated levels of the detox enzyme GGT and obesity. Elevated levels of GGT may be a compensatory factor. According to the study, obesity in animals and humans can accentuate alcohol-induced liver damage and cell injury.

Reference

http://www.ajcn.org/cgi/reprint/83/6/1351.pdf

Fish oil for joint pain


An effective natural treatment for joint inflammation such as that occurs with rheumatoid arthritis may be high-dose fish oil, according to a study published in 1995 in Arthritis Rheumatology. The study had patients on NSAIDs take up dietary supplementation of fish oil. The patients taking the fish oil showed improvement including a reduction innumber of tender joints after eight weeks. Some patients were able to discontinue NSAIDs without any further flare-ups.

Note: The study used dosages of 130mg of DHA/EPA omega-3 fatty acids from fish oil per kg daily.

Reference

Kremer JM, Lawrence DA, Petrillo GF, Litts LL, Mullaly PM, Rynes RI, Stocker RP, Parhami N, Greenstein NS, Fuchs BR, et al. Effects of high-dose fish oil on rheumatoid arthritis after stopping nonsteroidal antiinflammatory drugs. Clinical and immune correlates. Arthritis Rheum. 1995 Aug;38(8):1107-14.

Lupus summary

One in 700 women aged 20 to 65 and 1 in 245 American black women will be affected by systemic lupus erythematosus (lupus), a chronic inflammatory disorder that occurs when the body's own immune system attacks organs and tissues (1-2). Lupus means "wolflike", so named because symptoms of the autoimmune disease include an appearance of a rash over cheeks and the nose (1). Symptoms can also include mouth sores, joint pain, swelling around the lungs and heart, and kidney disease (2). 

Diagnosis and Treatment 

An antinuclear antibody (ANA) test makes it easy to diagnose lupus because almost every lupus patient tests positive (1). Other ways to diagnose are with complete blood count since lupus can commonly cause anemia, erythrocyte sedimintation due to inflammation, kidney and liver assesment, urinalysis that checks for protein and red blood cells in urine, chest X-ray to see inflammation, electrocariogram to identify irregular rhythms or damage in the heart, and a syphilis test because a false-positive result can indicate anti-phospholipid antibodies in the blood (3). Drugs such as NSAIDs, anti-malarial drugs and corticosteroids treat the inflammation itself (4). Other treatments and drugs can also be used for the symptoms (4). New treatments such as stem cell transplants, DHEA and Rituxan may be used in the future (4). 

References
1. Nowak TJ, Hanfod AG. Pathophysiology: Concepts and applications for health care professionals, 3rd ed. 2004. New York, McGraw-Hill. 
2. Mayo Clinic. Lupus: Definition. Available at: http://www.mayoclinic.com/health/lupus/DS00115
3. Mayo Clinic. Lupus: Tests and Diagnosis. Available at: http://www.mayoclinic.com/health/lupus/DS00115/DSECTION=tests%2Dand%2Ddiagnosis
4. Mayo clinic. Lupus: Treatment and Drugs. Available at: http://www.mayoclinic.com/health/lupus/DS00115/DSECTION=treatments%2Dand%2Ddrugs

A possible cause for IBS

The cause of IBS/IBD is considered unknown, but the inflammation is suggested to be due to small intestine bacterial overgrowth (SIBO), according to research published in JAMA in 2004 (1). Normally bacteria reside in the large intestine, but little if any is found in the small intestine (1).

A few years earlier in 2000, California researchers found that in IBS patients SIBO could be discovered using a simple breath test (2). When given treatment of antibiotics almost half of patients showed IBS symptoms were eliminated (2). Other studies did not show the same results (3) so more research is necessary.

Based on this research, nutritionists and doctors have often used antibiotics to treat IBS and then followed up with using probiotics and prebiotics to replenish healthy gut flora.

References

1. University Of Southern California (2004, September 3). Bacteria May Be The Cause Of Irritable Bowel Syndrome. ScienceDaily. Available at: http://www.sciencedaily.com/releases/2004/09/040903093237.htm

2. http://www3.interscience.wiley.com/journal/119001339/abstract?CRETRY=1&SRETRY=0

3. http://www.medscape.com/viewarticle/544511

Saturday, January 17, 2009

Testing for Detox Enzymes

When a high level of a toxin like alcohol or poison is in the body, the cells respond quickly with detoxification enzymes (1p23). One such enzyme is glutamyl transferase (GGT) (1p23) that is largely present in hepatocytes. The enzyme plays a role in transferring amino acids across the cell membrane and the biosynthesis of the antioxidant glutathione (2).

A simple blood test called a gamma-glutamyl transpeptidase (GGTP) can indicate if levels of GGT are greater than normal (2). The test is performed by drawing blood from the elbow orback of the hand (2).

An increase in GGT levels could be caused by alcohol intake, heart failure, cholestatis, cirrhosis, hepatitis, liver ischemia, liver necrosis, liver tumor or a drug/poison toxic to the liver (2). A decrease in levels could be caused by clofibrte or birth control pills (2).

Because it is unclear what elevated GGT levels may indicate, physicians will often also include other tests such as one for the enzyme ALP (3). If only GGT is elevated, then the cause may be alcohol abuse, but if GGT and ALP are elevated, then the diagnosis could be liver disease (3). In some people ALP only may be elevated, which could indicate bone disease (3).

References

1. Nowak TJ, Hanfod AG. Pathophysiology: Concepts and applications for health care professionals, 3rd ed. 2004. New York, McGraw-Hill.

2. MedlinePlus. Gamma-glutamyl transpeptidase. Available at: http://www.nlm.nih.gov/medlineplus/ency/article/003458.htm.

3. Lab Tests Online. GGT. Available at: http://www.labtestsonline.org/understanding/analytes/ggt/test.html.

Neurotoxic pesticides and how to avoid them

To find out just how much we are exposed to chemicals, look up the research from National Human Adipose Tissue Survey performed by U.S. Environmental Protection Agency and others (1-3). Unfortunately, according to their research, most of us have organophosphate and carbamate pesticides accumulated in our fat tissue. Included in these are neurotoxins that can affect cognition, mood, and associated with chronic neurological illnesses like Alzheimer's disease (3). The organophosphates, first synthesized for nerve gas research, actually destroys acetylcholinesterase and its effects are irreversible (3). Without it you get an excess of acetylcholine causing problems and the effects worsen if exposure continues (3). More of the enzyme needs to be produced to restore health of the synapses (3). Carbamates bind to acetylcholinesterase and its effects don't last because the bond is reversible via hydrolysis (3). 
References

1. Phillips LJ, Birchard GF. Regional variations in human toxics exposure in the USA: an analysis based on the National Human Adipose Tissue Survey. Arch Environ Contam Toxicol 1991;21:159-68.

2. Phillips LJ. A comparison of human toxics exposure and environmental contamination by census division. Arch Environ Contam Toxicol 1992;22:1-5.

3. Crinnion, WJ. Environmental Medicine, Part 1: The Human Burden of Environmental Toxins and Their Common Health Effects. Available at: http://www.headlice.org/lindane/health/toxicology/enviromed_crinnion.htm.

Friday, January 16, 2009

Your brain on wine, tea and chocolate


Who would've thought? Before my next game of chess, I'll drink a glass of cabernet, a cup of green tea and a bite into a piece of chocolate.


All three foods contain antioxidant flavonoids that support brain health and, according to a study of Oxford and Norwegian researchers, elderly subjects had better test scores in cognitive performance when they consumed these foods. Those that consume all three foods in moderation generated the best test scores.


You don't need much of each. The study revealed that a maximum effect of cognition at an intake of 10g of chocolate, 75-100ml of wine and the same for wine.


Too much of either of these three foods are known to have ill effects.


Reference


Nurk E, Refsum H, Drevon CA, Tell GS, Nygaard HA, Engedal K, Smith AD. Intake of flavonoid-rich wine, tea, and chocolate by elderly men and women is associated with better cognitive test performance. J Nutr. 2009 Jan;139(1):120-7. Epub 2008 Dec 3. Available at: http://www.ncbi.nlm.nih.gov/pubmed/19056649.



Sunday, January 11, 2009

Expanding my tea horizons

You fill up my senses with a hint of orange peel that drives me to sing John Denver songs and your light bitterness warms my complex taste buds like no other tea. Oh, Taragui "Sabor Naranja" maté! Could I ever fall in love with any other tea? 

Doubtful. So it's a good thing I have enough bags to last me six months because you never know when there might be an disaster. That trek to Argentina is a long one.  

But I am interested in mixing up my tea-drinking habit. We've all heard about—what seems like weekly—the studies that come out about green tea's preventive effects on cancer and heart disease. And while maté does have the same antioxidant epicatechins that tea has there are studies that suggest its tannins can cause possible cancers such as esophageal and bladder cancer [1-6]. While I believe more research is necessary to prove these effects and because some of the studies may have been related to other factors like how hot a maté is, I gotta drink it only in moderation. 

So I'm willing to bet there's a few other teas I like. Being January, and to start the year off with a healthy habit, I've decided to join the "Tea of The Month Club" at teavana.com. Their Web site design is beautiful and the stories on each tea are addicting. Anyway, I am interested in achieving that sought-after title, "tea connoisseur". 

Which should I start with? I was thinking at trying one of the blends. But not the Silver Monkey Rare Tea Blend. I'm just not into monkeys picking my tea leaves. Geez, I mean, is this a new way to avoid child labor? And do they at least give those monkeys a decent 401(k) plan and health insurance? 

References

1. Heck CI, de Mejia EG.Yerba Mate Tea (Ilex paraguariensis): a comprehensive review on chemistry, health implications, and technological considerations. J Food Sci. 2007 Nov;72(9):R138-51.

2. Kamangar F, Schantz MM, Abnet CC, Fagundes RB, Dawsey SM. Cancer Epidemiol Biomarkers Prev. High levels of carcinogenic polycyclic aromatic hydrocarbons in mate drinks. 2008 May;17(5):1262-8.

3. Sewram V, De Stefani E, Brennan P, Boffetta P. Maté consumption and the risk of squamous cell esophageal cancer in uruguay. Cancer Epidemiol Biomarkers Prev. 2003 Jun;12(6):508-13. Available at: http://www.ncbi.nlm.nih.gov/pubmed/12814995?dopt=Abstract.

4. De Stefani E, Boffetta P, Deneo-Pellegrini H, Correa P, Ronco AL, Brennan P, Ferro G, Acosta G, Mendilaharsu M. BMC Cancer. 2007 Mar 29;7:57. Links
Non-alcoholic beverages and risk of bladder cancer in Uruguay. Available at: http://www.ncbi.nlm.nih.gov/pubmed/17394632?ordinalpos=1&itool=EntrezSystem2.PEntrez.Pubmed.Pubmed_ResultsPanel.Pubmed_RVDocSum.

5. De Stefani E, Fierro L, Mendilaharsu M, Ronco A, Larrinaga MT, Balbi JC, Alonso S, Deneo-Pellegrini H. Br J Cancer. Meat intake, 'mate' drinking and renal cell cancer in Uruguay: a case-control study. 1998 Nov;78(9):1239-43.

6. Goldenberg D. Maté: a risk factor for oral and oropharyngeal cancer. Oral Oncol. 2002 Oct;38(7):646-9.
 

Thursday, January 1, 2009

New Year's Health Resolutions

If I was a rational human I wouldn't wait until New Year's Day to make a health resolution. But like most humans I know, I'm not very rational. I'm really emotional. My habits largely depend on how I feel.

Every morning before work I hug my pillow for as long as possible because it feels good and procrastinate getting ready for the day. My resolution last year to get up early and jog daily lasted less than a month.

My resolution to make healthy lunches and take them with me to work died much sooner than that. Why go through the trouble when I could easily settle for a cheap, big greasy burrito at mid-day.

After work? Forget exercise. I'm taking kids to dance, cheer and jiu jitsu. No time to make a balanced meal for dinner either. I've got homework. Kids, we're having pasta again. 

The obvious is that what I need is discipline. Easier said. The idea of punishment and reward feels like jail. And no matter how rational it is, rationalization can always take over. No, what I need is some kind of inspiration to eat better and motivation to exercise. 

Maybe if I played a sport. When I used to play sports I was a lot more determined. It's the competitive nature of it all. 

Maybe if I took up a class. Nothing pushes you more than when you are graded for progress. If not a class, then maybe a trainer.

Maybe what I need is a friend. A friend who makes goals with you keeps you in check. And keeping him or her in check helps motivate too.

Whatever my method, my resolution is to bring my health back. I've gone for too long being the all-knowledgeable nutrition writer, but not so much the doer. I get sick often enough, my cardio has suffered tremendously and I have noticed some atrophy and muscle replaced by flab. 

Right now I'm sure I'm just seeing the tip of the glacier of what is my bad health. And it's time to turn this ship around.