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  4.         <h1></h1>

  5. 

  6.         <p>

  7.             <strong>

  8.                 Cascara, energy, cancer and the FDA's laxative abuse</strong>

  9.         </p>The medical culture and the general culture share some attitudes about the nature of the most common

  10.         ailments--colds, cancer, arthritis, constipation, heart problems, etc., and they often agree about which things

  11.         can be treated at home, and which require special medical care. These background ideas are important because

  12.         they influence the actions of insurance companies, legislators, and regulatory agencies. They also influence the

  13.         judgments people make about their own health, and, too often, the way physicians treat their patients.The

  14.         prevalence of chronic constipation in North America has been estimated to be 27%, and in a ten year study, the

  15.         occurrence of new cases was about 16%.--the prevalence increases with aging. In some studies, women are 3 times

  16.         as likely as men to suffer from constipation. A recent Canadian article commented that "While chronic

  17.         constipation (CC) has a high prevalence in primary care, there are no existing treatment recommendations to

  18.         guide health care professionals." Almost everyone in the US is familiar with the idea of "laxative abuse," of

  19.         using laxatives when they aren"t absolutely necessary, and with the idea that chronic laxative use will create a

  20.         dependency, the way an addictive drug does. Contemporary doctors are likely to prescribe stool softeners for

  21.         constipated old people, rather than "stimulant laxatives," probably because "softener" doesn"t have the

  22.         pejorative connotation that "stimulant drug" has--not because there is a scientific basis for the choice.Many

  23.         doctors advise constipated patients to drink more water and exercise. While there is some physiological basis

  24.         for recommending exercise, the advice to drink more water is simply unphysiological. A study in Latin America

  25.         found no evidence of benefit from either of those recommendations, and recommended the use of fiber in the diet.

  26.         The right kind of fiber can benefit a variety of bowel problems. However, some types of fiber can exacerbate the

  27.         problem, and some types (such as oat bran) have been found to increase bowel cancer in animal studies.Despite

  28.         the greater prevalence of constipation in women and older people, even specialists in gastroenterology are very

  29.         unlikely to consider the role of hypothyroidism or other endocrine problems in chronic constipation.Because of

  30.         the cultural clich"s about constipation--that it"s caused by not eating enough fiber or drinking enough water,

  31.         for example--and the belief that it"s not very important, there is seldom an effort made to understand the

  32.         actual condition of the intestine, and the causes of the problem. Aging and stress increase some of the

  33.         inflammatory mediators, tending to reduce the barrier function of the bowel, letting larger amounts of bacterial

  34.         toxins enter the bloodstream, interfering with energy metabolism, creating inflammatory vicious circles of

  35.         increasing leakiness and inflammation. Often people visualize something like a sausage casing when they think of

  36.         the intestine, but when the intestine is becoming inflamed its wall may swell to become an inch thick. As it

  37.         thickens, the channel narrows to a few millimeters in diameter, and may even close in some regions. In the

  38.         swollen, edematous, inflamed condition the contractile mechanism of the smooth muscle is impaired. The failure

  39.         of contraction is caused by the same structural changes that increase permeability. (Garcia, et al., 1996;

  40.         Skarsgard, et al., 2000; Plaku and von der Weid, 2006; Uray, et al., 2006; Miller and Sims, 1986; Schouten, et

  41.         al., 2008; Gosling, et al., 2000.)Obviously, in the very swollen, structurally deformed intestine, with almost

  42.         no lumen, neither a stimulant nor a simple fibrous bulk could restore functioning, because even with stimulation

  43.         the smooth muscle is unable to contract, and the closed channel won"t admit bulk. Even gas is sometimes unable

  44.         to pass through the inflamed intestine. Mechanical thinking about the intestine fails when inflammation is

  45.         involved; now that inflammation is known to play an important role in Alzheimer"s disease and heart disease, it

  46.         will be more acceptable to consider its role in constipation.The contractile ability of smooth muscle, that"s

  47.         impaired by swelling and inflammation, can be restored by antiinflammatory agents, for example aspirin (or other

  48.         inhibitor of prostaglandin synthesis) or antihistamines. This applies to the muscles of lymphatic vessels (Wu,

  49.         et al., 2005, 2006; Gosling, 2000), that must function to reduce edema, as well as to the bowel muscles that

  50.         cause peristalsis. If someone thinks of constipation as the result of a lack of neuromuscular stimulation, then

  51.         it might seem reasonable to design a drug that intensifies the contractions produced by one of the natural

  52.         transmitter substances, such as serotonin, histamine, or acetylcholine. That"s apparently what Novartis did,

  53.         with tegaserod, a drug that increases the bowel"s sensitivity to serotonin. That drug, called Zelnorm, was

  54.         approved by the FDA in 2002, after a couple of years of publications praising it. At the time of its approval,

  55.         there was already evidence that people using it were more likely to have abdominal surgery, especially for

  56.         gallbladder disease, and there was doubt about its effectiveness.Strangely, the drug was approved to be used for

  57.         only 4 to 6 weeks, taking two tablets daily without interruption. When patients benefitted from the first

  58.         treatment, they might be eligible for an additional 4 to 6 weeks, but then it would be necessary for them to

  59.         find another way to deal with their constipation.Zelnorm side effects: abdominal pain, chest pain, flushing,

  60.         facial edema, hypertension, hypotension, angina pectoris, syncope, arrythmia, anxiety, vertigo, ovarian cyst,

  61.         miscarriage, menorrhagia, cholecystitis, appendicitis, bilirubinemia, gastroenteritis, increased creatine

  62.         phosphokinase. back pain, cramps, <strong>breast cancer, attempted suicide, </strong>impaired concentration,

  63.         increased appetite, sleep disorder, depression, anxiety, asthma, increased sweating, renal pain, polyuria.

  64.         (Later, it was found to cause heart attacks and intestinal ischemia/necrosis.) Why would the FDA approve a drug,

  65.         without evidence that it was more effective than harmless things that were already widely available?Zelnorm

  66.         Prices ~ In the US, Novartis estimates that Zelnorm tablets will sell for somewhere in the range of $3 to $4

  67.         each. The drug is expected to generate $1 billion in annual sales for Novartis.During the years just before the

  68.         new drug was approved, there were several publications reporting that emodin, the main active factor in cascara,

  69.         a traditional laxative, had some remarkable antiviral and anticancer activities. Other studies were reporting

  70.         that it protected against some known mutagens and carcinogens. Less than 3 months before approving Zelnorm, the

  71.         FDA announced its Final rule [Federal Register: May 9, 2002 (Volume 67, Number 90)] "Certain Additional

  72.         Over-the-Counter Drug Category II and III Active Ingredients." "the stimulant laxative ingredients aloe

  73.         (including aloe extract and aloe flower extract) and cascara sagrada (including casanthranol, cascara

  74.         fluidextract aromatic, cascara sagrada bark, cascara sagrada extract, and cascara sagrada fluidextract),"

  75.         determining that they "are not generally recognized as safe and effective or are misbranded. This final rule is

  76.         part of FDA's ongoing OTC drug product review. This rule is effective November 5, 2002."Historically, the FDA

  77.         has ruled against traditional generic drug products when the drug industry is ready to market a synthetic

  78.         substitute product.In 2007, the FDA withdrew its approval for Zelnorm, but allowed it to be licensed as an

  79.         "Investigational New Drug." <em>"On April 2, 2008, after more than eight months of availability, the company has

  80.             re-assessed the program and has made a decision to close it. Novartis is in the process of communicating

  81.             this decision to physicians participating in the program. Patients who had access to Zelnorm via this

  82.             program are instructed to discuss alternative treatment options with their physicians.</em>"Cascara and aloe

  83.         are not among the treatment options approved by the FDA, so cascara isn"t widely available (though anyone can

  84.         grow aloe plants easily). However, there is considerable interest in the drug industry in the possibility of

  85.         developing products based on emodin, or aloe-emodin, as anticancer or antiviral drugs. Even if it were proved to

  86.         be safe and effective for use as a laxative, its potential use as an alternative to extremely profitable cancer

  87.         and virus treatments would make it a serious threat to the drug industry.Although the standard medical journals

  88.         have only recently begun writing about it as a cancer treatment, emodin and related chemicals have been of

  89.         interest as a non-toxic way to treat cancer, allergies, and viral and bacterial diseases for a long time. In

  90.         1900, Moses Gomberg demonstrated the synthesis of a stable free radical (triphenylmethyl), but for years many

  91.         chemists believed free radicals couldn"t exist. A student of Gomberg"s, William F. Koch, came to believe that

  92.         cellular respiration involved free radicals, and experimented with the metabolic effects of many organic

  93.         molecules, quinones of several kinds, that can form free radicals, looking for the most useful ones. For more

  94.         than 50 years the U.S. Government and the main medical instititutions actively fought the idea that a free

  95.         radical or quinone could serve as a biological catalyst to correct a wide variety of health problems. A free

  96.         radical has an unpaired electron. In 1944 Yevgeniy Zavoisky devised a way to measure the behavior of unpaired

  97.         electrons in crystals, but it was many years before it was recognized that they are essential to cellular

  98.         respiration. Alex Comfort demonstrated them in living tissue in 1959. By the time coenzyme Q<sub>10</sub>,

  99.         ubiquinone, was officially discovered, Koch had moved to Brazil to continue his work with the biological effects

  100.         of the quinones, including the anthraquinone compound of brazilwood, which is used as a dye. He also used a

  101.         naphthoquine, lapachon Although vitamin K was identified as a quinone (naphthoquinone) not long after coQ<sub

  102.         >10</sub> was found to be a ubiquitous component of the mitochondrial respiratory system, it wasn"t immediately

  103.         recognized as another participant in that system, interacting with coQ<sub>10</sub>.Although Koch was unable to

  104.         publish in any English language medical journal after 1914, his work was widely known. In the 1930s, Albert

  105.         Szent-Gyorgyi, following Koch"s ideas about electrons in cells, interacting with free radicals, began working on

  106.         the links between electronic energy and cellular movement. Since free (or relatively free) electrons absorb

  107.         light, Szent-Gyorgyi worked with many colorful substances. When he came to the US in 1947, and wanted to expand

  108.         his research, a team of professors from Harvard investigated, and told the government funding agency that his

  109.         work didn"t deserve support. For the rest of his life, he worked on related ideas, expanding ideas that Koch had

  110.         first developed.Emodin and the anthraquinones (and naphthoquinones, such as lapachone) weren"t the reagents that

  111.         Koch considered the most powerful, but emodin can produce to some degree all of the effects that he believed

  112.         could be achieved by correcting the cellular respiratory apparatus<strong>: </strong>Antiinflammatory,

  113.         antifibrotic (Wang, et al., 2007) antiviral, antidepressant, heart protective, antioxidant, memory enhancing,

  114.         anticancer, anxiolytic and possibly antipsychotic.Working backward from these effects, we get a better

  115.         perspective on the "laxative" function of emodin and cascara. Koch and Szent-Gyorgyi believed that cellular

  116.         movement and secretion were electronically regulated. In one of his demonstrations, Szent-Gyorgyi showed that

  117.         muscles could be caused to contract when they were exposed to two substances which, when combined, partially

  118.         exchange an electron, causing an intense color reaction, but without causing an ordinary chemical

  119.         (oxidation-reduction) reaction. This kind of reaction is called a Donor-Acceptor reaction, and it is closely

  120.         related to the phenomenon of semiconduction. The reacting molecules have to be exactly "tuned" to each other,

  121.         allowing an electron to resonate between the molecules.In a muscle, any D-A matched pair of molecules would

  122.         cause a contraction, but the same molecules, combined in pairs that weren"t exactly tuned to each other, failed

  123.         to cause contraction. Szent-Gyorgyi believed that biological signal substances operated in a similar way, by

  124.         adjusting the electronic balance of cellular proteins. An effective laxative (besides preventing inflammation)

  125.         causes not only coordinated contraction of the smooth muscles of the intestine, but also adjusts secretions and

  126.         absorption, so that an appropriate amount of fluid stays in the intestine, and the cells of the intestine don"t

  127.         become water-logged.In the presence of bacterial endotoxin, respiratory energy production fails in the cells

  128.         lining the intestine. Nitric oxide is probably the main mediator of this effect.The shift from respiration to

  129.         glycolysis, from producing carbon dioxide to producing lactic acid, involves a global change in cell functions,

  130.         away from specialized differentiated functioning, toward defensive and inflammatory processes.This global change

  131.         involves a change in the physical properties of the cytoplasm, causing a tendency to swell, and to admit

  132.         dissolved substances that normally wouldn"t enter the cells.The interface between the cells lining the intestine

  133.         and the bacteria-rich environment involves processes similar to those in cells at other interfacial situations

  134.         throughout the body--kidney, bladder, secretory membranes of glands, capillary cells, etc. The failure of the

  135.         intestinal barrier is especially dangerous, because of the generalized toxic consequences, but the principles of

  136.         maintaining and restoring it are general, and they have to do with the nature of life. Some leakage from the

  137.         lumen of the intestine or the lumen of a blood vessel can occur between cells, but it is often claimed that the

  138.         "paracellular" route accounts for all leakage. (Anthraquinones may inhibit paracellular leakage [Karbach &amp;

  139.         Wanitschke, 1984].) When a cell is inflamed or overstimulated or fatigued, its cytoplasmic contents leak out. In

  140.         that state, its barrier function is weakened, and external material can leak in. This was demonstrated long ago

  141.         by Nasonov, but the "membrane" doctrine is incompatible with the facts, so the paracellular route is claimed to

  142.         explain leakage. Since the cells that form the barrier begin to form regulatory substances such as nitric oxide

  143.         when they are exposed to endotoxin, it is clear that major metabolic and energetic changes coincide in the cell

  144.         with the observed leakiness. Permeability varies with the nature of the substance, its oil and water solubility,

  145.         and the direction of its movement, arguing clearly that it isn"t a matter of mere holes between cells.Besides

  146.         endotoxin, estrogen, vibrational injury, radiation, aging, cold, and hypoosmolarity, increase NO synthesis and

  147.         release, and increase cellular permeabilities throughout the body. Estrogen excess (relative to progesterone and

  148.         androgens), as in pregnancy, stress, and aging, reduces intestinal motility, probably by increasing nitric oxide

  149.         production. The anthraquinones inhibit the formation of nitric oxide, which is constantly being promoted by

  150.         endotoxin.Cells regulate their water content holistically, and, to a great extent, autonomously, by adjusting

  151.         their structural proteins and their metabolism, but in the process they communicate with surrounding cells and

  152.         with the organism as a whole, and consequently they will receive various materials needed to improve their

  153.         stability, by adjusting their energy production, sensitivity, and structural composition.When these intrinsic

  154.         corrective processes are inadequate, as in hypothyroidism, with increased estrogen and serotonin, extrinsic

  155.         factors, including special foods and drugs, can reinforce the adaptive mechanisms. These "adaptogens" can

  156.         sometimes restore the system to perfect functioning, other times they can merely prevent further injury.

  157.         Sometimes the adaptogens are exactly like those the body normally has, but that are needed in larger amounts

  158.         during stress. Coenzyme Q<sub>10</sub>, vitamin K, short-chain fatty acids, ketoacids, niacinamide, and glycine

  159.         are examples of this sort--they are always present, but increased amounts can improve resistance to stress.

  160.         Another kind of adaptogen resembles the body"s intrinsic defensive substances, but isn"t produced in significant

  161.         quantities in our bodies. This type includes caffeine and the anthraquinones (such as emodin) and aspirin and

  162.         other protective substances from plants. These overlap in functions with some of our intrinsic regulatory

  163.         substances, and can also complement each other"s effects.Emodin inhibits the formation of nitric oxide,

  164.         increases mitochondrial respiration, inhibits angiogenesis and invasiveness, inhibits fatty acid synthase

  165.         (Zhang, et al., 2002), inhibits HER-2 neu and tyrosine phosphorylases (Zhang, et al., 1995, 1999), and promotes

  166.         cellular differentiation in cancer cells (Zhang, et al., 1995). The anthraquinones, like other antiinflammatory

  167.         substances, reduce leakage from blood vessels, but they also reduce the absorption of water from the intestine.

  168.         Reduced water absorption can be seen in a slight shrinkage of cells in certain circumsstances, and is probably

  169.         related to their promotion of cellular differentiation. All of these are basic antistress mechanisms, suggesting

  170.         that emodin and the antiinflammatory anthraquinones are providing something central to the life process

  171.         itself.Zelnorm was said to "act like serotonin." Serotonin slows metabolism, reduces oxygen consumption, and

  172.         increases free radicals such as superoxide and nitric oxide<strong>;</strong> the production of reactive oxygen

  173.         species is probably an essential part of its normal function. Emodin has an opposing effect, increasing the

  174.         metabolic rate. It increases mitochondrial oxygen consumption and ATP synthesis, while decreasing oxidative

  175.         damage (Du and Ko, 2005, 2006; Huang, et al., 1995).The Zelnorm episode was just an isolated case of a drug

  176.         company"s exploiting cultural beliefs, with the FDA providing a defensive framework, but the contrast between

  177.         tegaserod and emodin hints at a deeper and more deadly problem. W.F. Koch"s approach to immunity emphasized the

  178.         role of energy in maintaining the coherence of the organism, in which toxins were oxidized and made nontoxic.

  179.         There was no emphasis on destruction either of bacteria or of cancer cells, but only of the toxic factors that

  180.         interfered with respiration. He demonstrated that the udders of healthy cows could contain more bacteria than

  181.         those with mastitis, but the bacterial toxins were absent after the cows were treated with his catalyst. He

  182.         identified the "activated carbonyl group" as the essential feature of antibiotics, the same group that makes

  183.         coenzyme Q<sub>10</sub> function in the respiratory system. Koch"s understanding of the oxidative apparatus of

  184.         life, as a matter of electron balances, involved the idea that molecules with a low ionization potential, making

  185.         them good electron donors, amines specifically, interfered with respiration, while quinones, with a high

  186.         affinity for electrons, making them electron acceptors, activated respiration. The toxic effects of tryptophan

  187.         derivatives, indoles, and other amines related to the behavior of their electrons. (Serotonin wasn"t known at

  188.         the time Koch was doing his basic research.) Koch believed that similar electronic functions were responsible

  189.         for the effects of viruses.Both chemical and physical interactions of substances cause electrons to shift in

  190.         each substance, according to its composition. The shift of electrons accounts for the ability of adsorbed

  191.         molecules or ions to form multiple layers on a surface, and changes in the electrons of a complex biological

  192.         molecule affect the shape and function not only of that molecule, but of the molecules associated with it.

  193.         Interactions of the large molecules of cells, and their adsorbed substances, tend toward stable arrangements, or

  194.         phases. The type of energy production, and the nature of the regulatory molecules that are present, influence

  195.         the stability of the various states of an organism"s cells. (For more information on cooperative adsorption, see

  196.         <a href="http://www.gilbertling.org" target="_blank">www.gilbertling.org</a>.)Koch and Szent-Gyorgyi were

  197.         applying to biology and medicine concepts that were simultaneously being developed in metallurgy,

  198.         electrochemistry, colloid and surface science, and electronics. They were in the scientific mainstream, and it

  199.         was the medical-pharmaceutical industry that moved away from this kind of exploration of the interactions of

  200.         substances, electrons, and organisms.For Koch, antibiotics and anticancer agents weren"t necessarily distinct

  201.         from each other, and would be expected to have other beneficial effects as well.But an entirely different view

  202.         of the immune system was taking over the medical culture just as Koch began his research. Mechnikov"s

  203.         morphogenic view, in which the essential function of "the immune system" was to maintain the integrity of the

  204.         organism, was submerged by Ehrlich"s approach, which emphasized killing pathogens, and at the same time, the

  205.         genetic theory of cancer was replacing the developmental-environmental theory. Following the early work on the

  206.         carcinogenicity of estrogens, and the estrogenicity of carcinogens such as polycyclic aromatic hydrocarbons from

  207.         soot, a few German and French chemists (e.g., Schmidt and the Pullmans) began calculating the high electron

  208.         densities of highly reactive regions of the anthracene molecule, showing formally why certain molecules are

  209.         carcinogenic. At that time, their work was compatible with a developmental view of cancer. But the fact that the

  210.         polycyclic molecules could interact with the new model of the DNA gene caused the Pullmans" work to be reduced

  211.         to nothing but a minor theory of mutagenesis.Anthraquinones, because of the presence of several oxygen

  212.         molecules, had low electron densities and were stable. The tetracyclines, with related structure, have some

  213.         similar properties, and are antiinflammatory, as well as antibiotic. When a polycyclic bacterial antibiotic,

  214.         adriamycyn (later called doxorubicin), was found to be too toxic to use as an antibiotic, the fact that it was

  215.         toxic to cancer cells caused it to be developed as a cancer drug. It continued to be widely used even after it

  216.         was found to cause heart failure in many of the "cured" patients, because of its "success" in killing cancer

  217.         cells.The fact that many kinds of cancer cells can be killed by emodin makes it slightly interesting as a cancer

  218.         drug, but its simple generic nature has caused the drug industry to look for a more Ehrlichian magic bullet; for

  219.         example, they are still looking for ways to keep doxorubicin from destroying the heart. Emodin isn"t a magic

  220.         bullet (in fact it isn"t a bullet/toxin of any sort), but when combined with all the other adaptogens, it does

  221.         have a place in cancer therapy, as well as in treating many other ailments. None of the basic metaphors of

  222.         mainstream medicine--receptors, lock-and-key, membrane pores and pumps--can account for the laxative,

  223.         anticancer, cell-protective effects of emodin. The new interest in it provides an opportunity to continue to

  224.         investigate the effects of adjusting the electrical state of the cell substance, building on the foundations

  225.         created by William F. Koch, Albert Szent-Gyorgyi, and Gilbert Ling. <span style="white-space: pre-wrap"> </span>

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  273.         Kim SJ, Lee CH, Yoo H, Shin SH, Song ES, Lee SH.Food Chem Toxicol. 1991 Nov;29(11):765-70. <strong>Effect of

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  275.         >

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  277.             macrophages.

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  279.         Apr;23(2):152-71. <strong>Aloe-emodin metabolites protected N-methyl-d-aspartate-treated retinal ganglion cells

  280.             by Cu-Zn superoxide dismutase.</strong> Lin HJ, Lai CC, Lee Chao PD, Fan SS, Tsai Y, Huang SY, Wan L, Tsai

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  283.             constitute of Polygonatum multiflorum, on cycloheximide-induced impairment of memory consolidation in rats.

  284.         </strong>Lu MC, Hsieh MT, Wu CR, Cheng HY, Hsieh CC, Lin YT, Peng WH.Indian J Biochem Biophys. 2009

  285.         Feb;46(1):130-2. <strong>Alterations in plasma nitric oxide during aging in humans.</strong> Maurya PK, Rizvi

  286.         SI. Nitric oxide (NO) is relatively harmless, but along with superoxide radical becomes precursor of many toxic

  287.         species, such as peroxy and hydroxyl radicals, hydrogen peroxide, and peroxynitrite. In the present study, we

  288.         determined plasma NO as a function of human age and correlated NO levels with total antioxidant capacity of the

  289.         plasma. <strong>Results showed significant increase in NO level as a function of human age and plasma NO level

  290.             positively correlated with total antioxidant potential. Increased NO may contribute to the development of

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  294.             Contractile elements in the regulation of macromolecular permeability.

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  309.             of antitumor anthracenediones, mitoxantrone and ametantrone, in oxygen radical generation catalyzed by NADH

  310.             dehydrogenase.</strong>

  311.         <strong>Enzymatic and molecular modelling studies.</strong> Tarasiuk J, Mazerski J, Tkaczyk-Gobis K, Borowski E.

  312.         "It was shown that the <strong>distribution of the molecular electrostatic potential (MEP), around the quinone

  313.             system was crucial for this ability.</strong>

  314.         <strong>We have found for non-stimulating anthracenediones that the clouds of positive MEP cover the quinone

  315.             carbon atoms</strong> while for agents effective in stimulating reactive oxygen species formation the clouds

  316.         of negative MEP cover continuously the aromatic core together with the quinone system."Br J Nutr. 2008

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  324.         </strong>Wang CH, Gao ZQ, Ye B, Cai JT, Xie CG, Qian KD, Du Q.Eur J Pharmacol. 1995 Jan 5;272(1):87-95. <strong

  325.         >Inhibition of hind-paw edema and cutaneous vascular plasma extravasation in mice by acetylshikonin.

  326.         </strong>Wang JP, Raung SL, Chang LC, Kuo SC.Yao Xue Xue Bao. 2004 Apr;39(4):254-8. <strong>Inhibitory effects

  327.             of emodin on angiogenesis.

  328.         </strong>Wang XH, Wu SY, Zhen YS.Pharmacology. 1988;36 Suppl 1:98-103. <strong>Influence of rhein on rat colonic

  329.             Na+,K+-ATPase and permeability in vitro.</strong> Wanitschke R, Karbach U.Am J Physiol Gastrointest Liver

  330.         Physiol. 2006 Oct;291(4):G566-74. <strong>Contractile activity of lymphatic vessels is altered in the TNBS model

  331.             of guinea pig ileitis.</strong> Wu TF, Carati CJ, Macnaughton WK, von der Weid PY.Mem Inst Oswaldo Cruz.

  332.         2005 Mar;100 Suppl 1:107-10. <strong>Lymphatic vessel contractile activity and intestinal inflammation.</strong>

  333.         Wu TF, MacNaughton WK, von der Weid PY.Life Sci. 2007 Oct 13;81(17-18):1332-8. <strong>Emodin-mediated

  334.             protection from acute myocardial infarction via inhibition of inflammation and apoptosis in local ischemic

  335.             myocardium.

  336.         </strong>Wu Y, Tu X, Lin G, Xia H, Huang H, Wan J, Cheng Z, Liu M, Chen G, Zhang H, Fu J, Liu Q, Liu DX.Zhonghua

  337.         Gan Zang Bing Za Zhi. 2001 Aug;9(4):235-6. <strong>[Effects of emodin on hepatic fibrosis in rats]

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  341.         <strong>Suppressed transformation and induced differentiation of HER-2/neu-overexpressing breast cancer cells by

  342.             emodin.

  343.         </strong>Zhang L, Chang CJ, Bacus SS, Hung MC.Oncogene. 1996 Feb 1;12(3):571-6. <strong>Sensitization of

  344.             HER-2/neu-overexpressing non-small cell lung cancer cells to chemotherapeutic drugs by tyrosine kinase

  345.             inhibitor emodin.</strong>Zhang L, Hung MC.Clin Cancer Res. 1999 Feb;5(2):343-53. <strong>Tyrosine kinase

  346.             inhibitor emodin suppresses growth of HER-2/neu-overexpressing breast cancer cells in athymic mice and

  347.             sensitizes these cells to the inhibitory effect of paclitaxel.</strong> Zhang L, Lau YK, Xia W, Hortobagyi

  348.         GN, Hung MC.J Surg Res. 2006 Mar;131(1):80-5. Epub 2005 Nov 3.<strong>

  349.             Effects of emodin on Ca2+ signal transduction of smooth muscle cells in multiple organ dysfunction

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  351.         May;215(1):61-9. <strong>Emodin promotes atherosclerotic plaque stability in fat-fed apolipoprotein E-deficient

  352.             mice.</strong> Zhou M, Xu H, Pan L, Wen J, Guo Y, Chen K.

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