ENDOMETRIOSIS & DIOXINS
Information for physicians, nurses, and other healthcare professionals
The Environmental Protection Agency (EPA) stated in its Draft Dioxin Reassessment (1994) that the “general population’s current body burdens and exposures of dioxin are already at levels which affect our health.” One of the health effects EPA specifically identified was “a higher probability of experiencing endometriosis and the reduced ability to withstand an immunological challenge.”1
Incidence Is Rising Dramatically.
Doctors have puzzled over why incidence of endometriosis, which was considered relatively rare even in the early 1980s, has been skyrocketing. Affecting at least 7.5 million women and girls in the United States and Canada, it afflicts millions more worldwide. Endometriosis is a disease of the endocrine and immune systems in which tissue similar to the endometrial tissue of the uterus occurs abnormally in other areas of the abdomen.2 Infertility afflicts 30% to 40% of women with endometriosis and is very common with progression of the disease.3
Advances in diagnosis and reporting do not explain the current epidemic rates of endometriosis. Greater awareness fails to explain documented increased rates of hysterectomies due to endometriosis, most notably in teenage girls. According to data from the U.S. National Center for Health Statistics, and analysis by Dr. Gary Berger (Medical Director, Chapel Hill Fertility Center), hysterectomies for endometriosis increased 250% for young women between the ages of 15-24 and 186% between the ages of 25-34 during 1965 to 1984.
Earlier age of onset, increasing severity
Results of a 1998 study by the Endometriosis Association, presented at the VI World Congress on Endometriosis, provided startling data about the disease.5 Mary Lou Ballweg, Association President, and Bob Fichtner, statistician, analyzed data on 4000 North American women with diagnosed endometriosis. On average it took 9.28 years for women to receive a correct diagnosis of endometriosis. The study also revealed that the earlier the onset of symptoms, the greater the length of time before diagnosis, and the wider the variety of symptoms young women experienced. Those with symptoms as teenagers were more likely to suffer disability from the disease—a significant fact, considering that 66% reported having initial symptoms before age twenty. The data suggest that more girls may be experiencing more severe symptoms at younger ages.
There is growing concern that hormonally active chemicals, such as dioxins and other chemicals that mimic hormones or cause other dysfunctions in the endocrine and immune systems, are accelerating the onset of puberty. According to a recent study in the Journal of Pediatrics, girls in the United States are reaching puberty earlier than ever. Nearly half of African American girls and 15% of Caucasian girls are beginning to develop sexually at the age of eight. Development of breasts and pubic hair were two of the characteristics occurring at significantly younger ages than previously.6 The authors of the study called for more investigation into whether hormonally active chemicals (which are more prevalent in communities of color7) are responsible for these findings.
Greater range of symptoms
A far more complex and sophisticated understanding of the disease has developed in recent years, including the recognition of a range of symptoms associated with endometriosis (see chart).
Symptomatology of Endometriosis
% of total
Dysmenorrhea and/or pain throughout cycle ____95
Fatigue, exhaustion, low energy ______________87
Diarrhea, painful bowel movements,
or other intestinal upsets w/menses __________83
Abdominal bloating _______________________84
Heavy or irregular periods _________________65
Dyspareunia (painful sexual intercourse) _______64
Nausea, stomach upset at time of menses ______64
Dizziness, headaches w/menses or pain ________63
Low resistance to infections ________________43
Infertility ______________________________41
Low-grade fever _________________________32
No symptoms __________________________ 1
What Are Dioxins?
According to the EPA, dioxins are the most potent synthetic carcinogens yet tested.8 Dioxins are a class of chemicals with similar properties; these include the parent compound—2,3,7,8-tetrachlorodibenzo-p-dioxin (TCDD)—and certain types of chlorinated dibenzodioxins, dibenzofurans, and polychlorinated biphenyls (PCBs). Whereas PCBs are man-made (and act like dioxin in the body and bioaccumulate), dioxins are an accidental byproduct of a multitude of industrial processes in which chlorine is present, such as municipal and medical waste incineration, chemical and plastics manufacturing, pesticide and herbicide production, and pulp/paper bleaching.9
Major sources of exposure
Once created, dioxins concentrate dramatically in the food chain. Dioxins contaminate beef, fish, poultry, and dairy products. Animals consume pesticide- and herbicide-laden food, and humans consume animals and fish, our primary exposure to dioxin.1 Dioxins are measured in fish at levels up to a million times greater than those found in the surrounding water. The remainder of human exposure occurs from contaminated air, water, and bleached paper products.
Menstrual hygiene products and exposure?
According to the U.S. Food and Drug Administration (USFDA), tampons and sanitary pads made of rayon or bleached cotton contain low levels of dioxins.10 The USFDA allays concern about chemicals in these products by asserting that levels at parts per trillion are so low that risk is minimal.10 EPA tests, however, assert that dioxin levels once thought acceptably low, adversely affect the reproductive and immune systems.8,11
Tampon safety legislation, introduced in Congress in January 2003 (H.R. 373, Carolyn B. Maloney, 14th District, New York) would direct the National Institutes of Health (NIH) to research health risks to women—including endometriosis and cancers of the breast, ovaries, and cervix—from the presence of dioxin, synthetic fibers, and other additives in feminine products.12,13 Until research addresses the risks, health experts recommend unbleached, organic cotton sanitary pads and tampons (without plastic applicators).14
Bioaccumulation in the body
In the process of bioaccumulation, dioxin, even in very low doses, builds up in the body over time, as it concentrates in fatty tissues. Dioxin also biomagnifies through the food chain as higher organisms consume plants and small animals.2 According to the EPA, the half-life of TCDD in the body (the time to rid the body of half of the amount of bioaccumulated dioxin) is about seven years, while the half-life of PCBs is variable.2 ,15,16
In general, our body burden of dioxins increases as we get older. The time of exposure to TCDD during our lives may also affect our body burden of dioxin as adults. A recent study (Seveso, Italy) showed that girls younger than age 10, who were exposed to dioxin, retained higher levels of dioxin later as adults, as compared to women not exposed until teen or adult years.17
“19It is possible for a woman to “excrete half of her accumulated amount of dioxin during lactation.”
Studies have shown that humans and wildlife are exposed to a myriad of dioxin chemicals. How do we determine our total exposure to dioxins? The toxicity of individual dioxin-like chemicals is assessed using a toxic equivalency
Approach. Based on all available studies, chemicals that are dioxin-like are assigned a relative potency factor that expresses their toxicity in relation to that of TCDD. The total toxic TCDD equivalency quotient (TEQ) is the sum of the amount of each chemical present in a biological sample, times its individual TEF.
Thus, the total body burden of dioxins present in our blood is measured as total serum TEQ. It is important to consider the total TEQ of dioxins in assessing the health risk of exposure, rather than TCDD alone. In the general population, TCDD contributes approximately 15% of the body burden of dioxins, while dibenzodioxins, dibenzofurans, and PCBs constitute about 85% of the dioxin body burden.18
Gynecologists and other physicians are already aware of the effects of prenatal exposure to hormones, such as the synthetic estrogen, diethylstilbestrol (DES), and that the prenatal and neonatal stages are critical times of development and sensitivity to toxic chemicals. A multi-generational effect of embryonic exposure to dioxin has now been shown in an animal model of endometriosis.59 It is possible for a woman to “excrete half of her accumulated amount of dioxin during lactation.”19 Dioxins have been found in breast milk worldwide—the highest concentrations in industrialized countries.20
Behavior of dioxins in the body
Dioxins interfere with the cell’s gene processes. Entering a cell, dioxins bind to the aryl hydrocarbon receptor protein, or AhR, which is present in many parts of the body including liver, lungs, lymphocytes, and placenta.21 Once bound to the AhR, dioxins can move freely inside the cell, and when binding to DNA inside the nucleus, they are able to switch genes on and off.21,22 The genes targeted by dioxins influence hormone metabolism and growth factors, and thus affect reproduction, endocrine, and immune functions.
Dioxin Exposure and Endometriosis
A 1992 study analyzed rhesus monkeys exposed for four years to 5 ppt and 25 ppt of TCDD, the most toxic form of dioxin. 23 Association researchers concluded that “the incidence of endometriosis was directly correlated with dioxin exposure and the severity of disease was dependent upon the dose administered.”23 This study demonstrated that “chronic exposure to the chemical toxin dioxin is directly correlated with an increased incidence in the development of endometriosis in rhesus monkeys.”23
In addition to these findings, the dioxin-exposed monkeys showed immune abnormalities and altered GI microflora similar to those observed in women with endometriosis. 61 Dioxins adversely affect production of cytokines known to participate in the regulation of uterine physiology.22,24,25,26,27,28,63 Dioxins “turn on” genes that promote inflammation and disrupt normal growth processes that may lead to the development and progression of endometriosis.51,64 Uterine endometrium and endometriotic lesions express the genes for the AhR, and studies suggest that these tissues are targets for dioxin action. A recent report demonstrates that exposure of endometrium and endometriosis tissues to a combination of 17ß-E2 and TCDD increases the expression of growth factors and receptors involved in allergic inflammation (I-309-CCR8). 62 An excellent review of dioxin’s inflammatory properties ties together many of the steps from exposure (which may be embryonic) to full-blown endometriosis.65 Dioxins also modulate various hormone receptor systems that play a role in uterine function. 23,29,30
Research utilizing a rodent model further supports the 1992 findings, by demonstrating that “administration of TCDD to rats and mice also resulted in the promotion of the growth of endometriotic sites.”31 The rats demonstrated endocrine dysfunction and subtle tissue changes, while the mice responded with growth of endometriotic tissue.31,33
Studies using mice also found that dioxins act as a disruptor of progesterone action, by blocking the ability of progesterone to prevent ectopic human tissue lesions in mice and by altering the expression of progesterone receptors during gestational development.33,59 Further, dioxin can disrupt ovarian synthesis of progesterone and inhibit the steroid regulation of endometrial matrix metalloproteinase (MMP) expression, specifically TGF-B2.33, 34 Progesterone-induced expression of TGF-B2 is also critical to maintain an appropriate endometrial environment for pregnancy.33 Primate studies indicate that TCDD exposure increases spontaneous abortion,36 a uterine event that may be linked to endometriosis.35 Recent work demonstrates that dioxin exposure of human endometrial cells results in reduced expression of progesterone receptor-B and increased MMP expression similiar to endometrial tissues from women with endometriosis.37 Progesterone can prevent or minimize endometriosis whereas MMP expression is critical to the establishment of endometrial lesions. 33 Thus, alterations in the ability of endometrium to respond to progesterone and the aberrent expression of MMPs induced by dioxins could mediate the establishment of endometrial lesions.
In addition, a 2001 study of the monkey colony demonstrated both elevated-serum TCDD and elevated serum triglycerides in the monkeys exposed to dioxin.
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