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Hormone
DHEA (Dehydroepiandrosterone)
Nutrition
nutrition
definition
DHEA (Dehydroepiandrosterone):
» chemistry:
First identified in 1934, Dehydroepiandrosterone (DHEA) is a steroid hormone secreted by the adrenal gland. Even though its function has only recently begun to be understood, there is more DHEA produced than any other adrenal steroid, with circulating levels of DHEA and its sulfate-containing ester DHEA-S up to 20 times higher than those of any other adrenal steroid.
» chemical name: Dehydroepiandrosterone; Dehydroepiandrosterone-sulfate.
» metabolism:
DHEA levels peak early in life and begin declining in early adulthood. By the age of seventy, a typical individuals DHEA levels are only 20% as high as they had been as a young adult. This age-related decline does not occur with any of the other adrenal steroids. Nevertheless, no conclusive evidence has emerged as to whether these lower DHEA levels associated with age represent a true deficiency.
After being secreted by the adrenal glands, it circulates in the bloodstream as DHEA-Sulfate (DHEAS).
DHEA is structurally similar to other steroid hormones (such as estrogen. progesterone. and testosterone) and can be converted into other hormones, including estrogen and testosterone. As much as half of testosterone in men and about three-quarters of estrogen in women (and close to 100% after menopause) are derived from DHEA.
(Labrie F, Belanger A, Simard J, et al. Ann NY Acad Sci 1995;774:16-28.)
DHEA may be capable of indirectly raising the levels of progesterone. Although DHEA is not converted directly into progesterone, it may, through a feedback mechanism, indirectly increase the production of progesterone. Both DHEA and progesterone are produced from the same precursor hormone, pregnenolone. If DHEA levels are adequate, then pregnenolone will be converted primarily to progesterone, rather than to DHEA.
One of the breakdown products of DHEA, a compound called 5-androstene-3B, 178-diol, is known to bind strongly to estrogen receptors. Therefore, DHEA. like estrogen, might inhibit bone resorption.
Androgens, a class of hormones which includes DHEA and testosterone, stimulate bone formation and calcium absorption. DHEA might. therefore. augment the bone-building effect of progesterone. DHEA appears to be the only hormone which appears capable of both inhibiting bone resorption and stimulating bone formation.
» function:
Dehydroepiandrosterone (DHEA; prasterone) is a major adrenal hormone with no well accepted function.
For many years researchers, uncertain as to the specific functions of DHEA, assumed that it was merely a buffer hormone a reservoir upon which the adrenals could draw in order to produce other hormones. More recently researchers have discovered that cells contain specific DHEA receptor sites.
Aging in humans is accompanied by a progressive decline in the secretion of the adrenal androgens dehydroepiandrosterone (DHEA) and DHEA sulfate (DS), paralleling that of the GH-insulin-like growth factor-I (GH-IGF-I) axis. Although the functional relationship of the decline of the GH-IGF-I system and catabolism is recognized, the biological role of DHEA in human aging remains undefined.
Studies on animals and humans have suggested that DHEA-S has antiatherogenic effects. It has been hypothesized that insulin may have an atherogenic role and it has been reported recently that, surprisingly, DHEA-S levels decreased in normal men and women during the hyperinsulinemic-euglycemic technique.
» Chinese:
Tonifies Kidney Yang.
» requirements:
RDA: DHEA is not considered an essential nutrient.
No RDA has been established.
» lab:
Blood: Serum levels of DHEA and DHEA-S are measured by some laboratories. DHEA-S is a byproduct of DHEA which is easier to measure and which provides a rough estimate of DHEA levels.
Although serum measurements of DHEA and DHEA-S are available through most laboratories, it is not clear how closely one should rely on these measurements; nor is it clear whether DHEA or DHEA-S is the more reliable test. The normal range for DHEA-S as listed by some laboratories as 350-4,300 ng/ml for women and 800-5,600 ng/ml for men. Many, older individuals have values near or below the lower limit of normal. However, you may not want to use an age-adjusted reference range (as published by some labs), since it seems that the age-related decline in serum DHEA-S is undesirable.
When DHEA therapy appears to be clinically indicated, some experienced physicians consider treating a woman whose DHEA-S level is below 600 ng/ml and a man whose level is below 1200 ng/ ml. Ultimately, there are as yet no data on what constitutes an optimum serum level.
(Gaby AR. Alt Med Rev. 1996:1(2);67)
Saliva: Other tests commonly, such as the Adrenal Stress Index, used by physicians to evaluate DHEA levels involve sampling saliva at set intervals in a 24 hour period to determine the timing and relative amount of cortisol and DHEA.
These measurements may provide some estimate of DHEA status. but they cannot predict with certainty who will benefit from treatment or what the dosage should be.
Jonathan V. Wright. M.D., a leading authority in nutritional medicine, has observed that absence of hair on the lower third of the legs is suggestive of DHEA deficiency.
(Gaby AR. Holistic Medicine. Spring, 1993:19-24.)
» food sources:
Animal proteins are the richest dietary sources of DHEA.
» deficiency:
Aging: Overall, studies that have been conducted in humans show that DHEA treatment at dosages that restore serum levels may achieve normalization in some aging physiological systems and thereby indicate that DHEA deficiency may expedite the development of some diseases that are common in the elderly.
(Araneo B, et al. Ann N Y Acad Sci 1995;774:232-248; Morales AJ, et al. J Clin Endocrinol Metab 1994;78:1360-1367; Watson RR, et al. Drugs Aging 1996 Oct;9(4):274-91; Kalimi M, Regelson W. 1990.;361-385; Yen SS, et al, O. Ann N Y Acad Sci 1995;774:128-142.
Depressed levels of DHEA have been reported in women with asthma, compared with matched controls.
(Weinstein, RE, et al. J Allerg Clin Immol 1996;97:1-8.)
» mode of action:
Stimulation and supplementation of adrenal hormone levels.
» therapeutics:
Acquired Immunodeficiency Syndrome (AIDS):
Interest in DHEA accelerated with the publication of Jacobsen et als epidemiological data published in the Journal of Infectious Diseases in 1991 showing the decreased levels of serum DHEA was a predictor for progression to AIDS in asymptomatic HIV infected men. DHEA levels are reduced in people infected with HIV and these levels decline even more as the disease progresses to full-blown AIDS. (Merril CR, et al. In: Kalimi M, Regelson W. 1990; 101-105.) DHEA has been reported to inhibit the replication of HIV, the virus believed to cause AIDS. In addition, this hormone has been shown to enhance the immune response to viral infections.
As mentioned above, a study of 105 HIV-positive men with marginally low helper T-cell counts, found that those with serum DHEA levels below normal were 2.34 times as likely to progress to AIDS as were those with normal DHEA levels. (Jacobsen, M, et al. J Infectious Dis 164:864-868, 1991) These studies provide evidence that a deficiency of DHEA occurs in individuals with HIV infection and that this deficiency may be one of the factors contributing to immune system failure. Another study showed that both DHEA levels and CD4 counts were independent predictors of disease progression in HIV infected men. (Mulder, 1992 #132) While a correlational study of CD4 counts and serum cortisol and DHEA-Sulfate showed a positive relationship between immune status as measured by CD4 count and DHEA, supporting an hypothesis that DHEA deficiency may worsen immune status in HIV infected patients.
(Wisniewski TL, et al. Am J Med Sci 305:79-83, 1993.)
The effects of oral administration of DHEA in 13 HIV+ patients with baseline CD4 counts of 250-600 cells/mm3 was evaluated in phase I study. (Dyner TS, et al. J AIDS 6:459-465, 1993) Five patients treated with the highest of three doses (750 mg/day) had CD4+ cell increases at 8 weeks from a mean of 373/(l pre-treatment to 463/(l after 8 weeks. In another open label, uncontrolled study in 12 HIV+ patients, DHEA therapy (75 mg/day) increased CD4 and CD8 cell counts in the majority of patients.
(Hasheev D, et al. Intl AIDS Conference Abstract no PB0322, 1994.)
A subsequent study (Dyner et al, 1993) evaluated escalating oral doses of DHEA (750 mg/day up to 2,250 mg/day) for 16 weeks in 31 HIV+ patients with baseline CD4 counts between 250 and 600 cells/ul. Dose proportionality was not evidenced by serum DHEA nor by DHEA-Sulfate. No sustained increases in CD4 counts nor decreases in serum p24 antigen or beta-2-microglobiulin levels were observed. However, serum neopterin levels decreased transiently by 23-40% at 8 weeks. Suzuki et al (1995) have suggested that low levels of DHEA may cause immunological deficits via deficient IL-2 production in lymphocytes. Abnormal levels of DHEA were associated with low levels of serum IL-2.
Direct murine lymphocyte exposure to DHEA at low concentrations (10-10 - 10-7 M) enhanced secretion of IL-2 following immunological challenge.
(Daynes R, et al. Eur J Immunol 20:793-802, 1990.)
DHEA is a modest selective inhibitor of HIV-1 replication in human lymphocytes and macrophages. The antiviral mechanism does not appear to be mediated through reverse transcriptase inhibition since DHEA did not inhibit HIV-1 RT enzymatic activity when tested up to 100 uM. Acute infection of normal human lymphocytes was also inhibited by DHEA at 10-100uM. (Schinazi RF, et al. Intr AIDS Conf Abstract # MCP 55, 1994) In another in vitro experiment, 50% inhibition of macrophage HIV p24 expression occurred at concentrations of 3-30 mcg/ml.
(Jacobsen M, et al. J Infectious Dis 164:864-868, 1991.)
In a small open-label trial with 20 HIV+ people, DHEA as monotherapy at fairly high doses of 600 mg twice a day was shown to reduce viral load by 0.6 log unit in HIV patients with baseline CD4 counts of 50-300.
(Salvata, et al. XI International Conference on AIDS Abstract We.B.3385, 1996.)
DHEA is frequently prescribed to, and self prescribed by, many HIV+ patients in the U.S. Caution may be appropriate given that high serum DHEA levels have also been implicated in the pathogenesis of Kaposis sarcoma in HIV/AIDS. DHEA levels were significantly higher, as were testosterone and androstenedione in 34 HIV+ patients with KS vs. 35 HIV+ controls without KS. (Christieff N, Gharakhanian C, Thobie N, et al. J Clin Pathology 48:513-518, 1995)
(Special thanks to Leanna Standish, N.D., Ph.D. and the Bastyr University AIDS Research Center for these excerpts from HIV/AIDS: Naturopathic Medical Principles and Practice, 1997)
Adrenal insufficiency:
DHEA in appropriate replacement doses appears to have remedial effects with respect to its ability to induce an anabolic growth factor, increase muscle strength and lean body mass, activate immune function, and enhance quality of life in aging men and women, with no significant adverse effects.
(Yen SS, et al. Ann NY Acad Sci 1995;774:128-142.)
However, supplemental DHEA can antagonize the effects of cortisol. Therefore, it is important to measure both DHEA and cortisol levels before administering DHEA therapy.
Allergic Disorders:
Eight patients with severe attacks of hereditary angioedema were treated with 37 or 74mg per day of DHEA-S (equivalent to 25 or 50mg. respectively, of DHEA) every 1-3 days for 3-29 months. DHEA-S treatment resulted in a dramatic clinical improvement in all eight patients.
(Koo E, et al. Klin Wochenschr 1983;61:715-717.)
Practitioners have reported positive results in treating a variety of allergies and sensitivites with DHEA and observed that treatment sometimes reduces the severity of food or chemical allergies. Alan Gaby, M.D. reported several patients with multiple chemical sensitivities who responded to physiologic doses of DHEA (5-IS mg/day for women, 10-30 mg/day for men), but added that it is difficult to predict which patients will improve.
(Gaby AR. Alt Med Rev. 1996:1(2);64.)
Asthmatics commonly have subnormal serum levels of DHEA-S. Corticosteroid-induced adrenal suppression might contribute to a DHEA deficiency. However, low levels of DHEA-S were also found in 21% of asthmatics who were not taking steroids. DHEA deficiency may also result from long-term administration of inhaled corticosteroids. In a study of 36 post-menopausal asthmatic women, those who were receiving at least 1 mg per day of beclomethasone dipropionate had nearly a 50% reduction in serum DHEA levels, compared with women who were not receiving the drug. Apparently, inhaled corticosteroids are absorbed in amounts sufficient to cause some degree of adrenal suppression.
(Dunn, PJ, et al. NZ Med J 1984:97:805-808; Smith, BJ, et al. Aust AZ J Med 1994:24:396-401.)
Alzheimers disease:
There was much initial discussion of the potential benefits of DHEA in treating Alzheimers disease, but recent studies do not support the original suggestion that low serum DHEA levels are associated with Alzheimer's disease and other forms of cognitive dysfunction in the elderly.
(Merril CR, et al. 1990;101-105.)
Autoimmune diseases
Studies in animals suggest that DHEA may have a beneficial effect on autoimmune processes. The initial interest was sparked by a study involving New Zealand Black mice, a strain which spontaneously develops an autoimmune syndrome resembling SLE. Administering DHEA to these animals prevented the kidney failure and the hemolytic anemia associated with this syndrome.
(Regelson W, et al. Ann NY Acad Sci 1988:521:260-273.)
See also specific conditions in this section.
Enhancing immune response to viral and bacterial infections:
DHEA exerts a number of different effects on the immune system. Some of these effects appear to result from the anti-glucocorticoid actions of DHEA. Several studies using mice found that DHEA antagonized the suppressive effects of dexamethasone on lymphocyte proliferation, prevented glucocorticoid-induced thymic involution, preserved immune competence in burned mice, and protected against acute lethal infections with coxsackie virus B4 and herpes simplex type 2 encephalitis in mice. Overall, DHEA appeared to act by preventing the suppression of immune competence caused by the viral infections.
(Blauer KL, et al. Endocr 1991:129:3174-3179; May M, et al. Life Sci 1990:46:1627-1631; Araneo BA, et al. Arch Surg 1993:128:318-325; Aranen B, Daynes R. Endocr 1995:136:393-401; Loria RM. et al. J Med Viral 1988:26:301-314.)
DHEA has also been shown to influence immune function in humans. In a double-blind study, administration of 50 mg/day of DHEA to postmenopausal women (mean age. 56.1 years) produced a two-fold increase in natural killer cell activity and a 6% decrease in the proportion of helper T cells. While the increase in natural killer cell activity might be expected to enhance immune surveillance against cancer and viral infections, the decline in helper T cells could have adverse consequences. Nevertheless, DHEA is known to mediate T cell responses. However, the decline in helper T cells merely could be a reflection of enhanced T cell function.
(Casson PR, et al. Fertil Steril 1995;63:1027-1031; Regelson W, et al. Ann NY Acad Sci 1994:719;553-563; Gaby AR. Alt Med Rev. 1996:1(2);63.)
Anti-aging/Premature aging:
Elderly patients who suffer from weakness, muscle wasting, tremulousness, fatigue, depression, declining memory, and other signs of aging frequently have serum DHEA-S levels near or below the lower limit of normal. Treatment with DHEA (usually 5-10 mg/day for women and 10-20 mg/day for men) often results in improved mood, energy, memory, appetite, and skin color, sometimes after as little as two weeks. With continued treatment, the benefits may become even more pronounced and muscle wasting may be partially reversed.
(Gaby AR. Alt Med Rev. 1996:1(2);62.)
Aging in humans is accompanied by a progressive decline in the secretion of the adrenal androgens dehydroepiandrosterone (DHEA) and DHEA sulfate (DS), paralleling that of the GH-insulin-like growth factor-I (GH-IGF-I) axis. DHEA levels peak early in life and gradually decline, starting in early adulthood. By the age of sixty, DHEA levels are only 5-15% of what they were at their peak at younger ages. This age-related decline is not known to occur with any of the other adrenal steroids.
(Ebeling P, Koivisto VA. Lancet 1994;343:1479-1481.)
Although the functional relationship of the decline of the GH-IGF-I system and catabolism is recognized, the biological role of DHEA in human aging remains undefined. It has therefore been suggested that some of the manifestations of aging may be caused by DHEA deficiency. However, while several studies have found that even while DHEA may not extend the duration of life, it has demonstrated clear potential for improving the quality of life. Overall, studies that have been conducted in humans show that DHEA treatment at dosages that restore serum levels may achieve normalization in some aging physiological systems and thereby indicate that DHEA deficiency may expedite the development of some diseases that are common in the elderly. In a recent randomized, double-blind, placebo-controlled trial involving men and women 60 to 79 years of age, Baulieu et al found that DHEA replacement therapy could normalize some of the effects of aging. After receiving 50 mg/day of DHEA for 1 year DHEAS levels of the subjects increased to, or exceeded, levels typical of young adults after 6 months of administration and decreased after 12 months, except in men over 70. Testesterone levels increased in women after 6 months and decreased after 12 months, but were unaffected in men. DHEA also demonstrated a positive effect on bone mineral density in women and on libido in women over 70. In addition, DHEA induced positive effects on skin hydration, pigmentation, sebum production, and epidermal thickness. Thus, DHEA in appropriate replacement doses appears to have remedial effects with respect to its ability to induce an anabolic growth factor, increase muscle strength and lean body mass, activate immune function, and enhance quality of life in aging men and women, with no significant adverse effects.
(Araneo B, et al. Ann NY Acad Sci 1995;774:232-248; Morales AJ, et al. J Clin Endocrinol Metab 1994;78:1360-1367; Watson RR, et al. Drugs Aging 1996 Oct;9(4):274-91; Kalimi M, Regelson W. 1990; 361-385; Yen SS, et al, O. Ann NY Acad Sci 1995;774:128-142; Baulieu EE, et al. Proc Natl Acad Sci USA. 2000;97(8):4279-4284..)
Cancer:
DHEA has been found to inhibit or prevent cancers in a variety of animal studies. In a strain of mice that develops spontaneous breast cancer, long-term administration of DHEA prevented the cancer from occurring.
(Schwartz AG. Cancer Res. 1979:39:1129-1132.)
Treatment of mice with DHEA also delayed the appearance of colon tumors resulting from administering the carcinogen 1.2-dimethylhydrazine.
(Nyce JW, et al. Carcinogenesis 1984:5:57-62)
In addition. administering DHEA inhibited the development of liver cancer in rats treated with chemical carcinogens.
(Mayer D, et al. 1990, 361-385.)
Other studies indicate that there is an association between DHEA levels and human breast cancer. In one study by Arguelles et al, urinary excretion of DHEA was below normal in a group of premenopausal women with breast cancer. Zumoff and other researchers confirmed that DHEA levels are low in premenopausal breast cancer patients, but found that some postmenopausal women with breast cancer had elevated DHEA levels. In another study, women with DHEA levels in the highest tertile were 60% less likely to develop breast cancer than were women in the lowest tertile.
(Arguelles, AB, et al Lancet 1973:1:165-168; Zumoff, B, et al. Canc Res 1981;41:3360-3363; Helzlsouer KJ, et al. Cancer Res 1992:52:1-4.)
It appeared that the low levels in the premenopausal patients were due primarily to decreased production, while the elevated levels in the postmenopausal patients were due to delayed breakdown. Whatever the reason for the changes. these studies suggest a possible role for DHEA in the prevention or treatment of at least some cases breast cancer.
Nevertheless, the fact that DHEA is converted in part to estrogen and testosterone and that some postmenopausal women with breast cancer have elevated levels of DHEA provide significant grounds for caution and further study.
Cardiovascular disease:
The results of several studies raise the possibility that, in individuals with low DHEA levels, supplementing with DHEA may help prevent heart disease. In one study, plasma levels of DHEA-S were measured in 242 men, aged 50-79 years. DHEA-S levels were significantly lower in men with a history of heart disease than in those with no history of heart disease. Among men with healthy hearts, those who had low levels of DHEA were 3.3 times more likely to die of heart disease during the next 12 years than were those with normal DHEA levels. Furthermore, administering DHEA has also been shown to lower serum LDL-cholesterol. Similar findings have been reported by others, although another epidemiologic investigation found only a modest protective effect of DHEA.
(Barrett-Connor B, et al. N EngI J Med 1986.315:1519-1524; Regelson W, Loria S, Kalimi M. Ann NY Acad Sci 1988:521:260-273; Newcomer LM, et al. Am J Epidemiol 1994:140:870-875; Mitchell LE. et al. Circulation 1994:89:89-93.)
In women, no inverse association was found between DHEA-S levels and cardiovascular disease. In fact, cardiovascular death rates were highest in women in the upper tertile of DHEA-S levels and lowest in women in the middle tertile (a U-shaped distribution). (Barrett-Connor B, Khaw K-T. N Engl J Med 1987:317:711.)
Chronic Fatigue Syndrome (CFS):
Some patients with chronic fatigue syndrome (CFS) have also improved clinically with DHEA therapy. However, since cortisol deficiency appears to be the primary problem in some patients with CFS and, since DHEA can antagonize the effects of cortisol, DHEA therapy might actually cause some patients with CFS to worsen. It is important, therefore, to measure both DHEA and cortisol levels before treating CES patients with DHEA.
(Gaby AR. Alt Med Rev. 1996:1(2);64.)
Depression:
DHEA and DHEA-S levels are lower in depressed patients, and depression in six depressed patients significantly improved with DHEA supplements of 30-90 mg per day for four weeks. Nevertheless, DHEA is probably only indicated for a minority of people with depression.
(Wolkowitz OM, et al. Ann NY Acad Sci 1995;774:337-339; Gaby AR. Nutr Healing Jun 1997:8.)
Diabetes mellitus:
One study found low DHEA-S levels during chronic insulin administration therapy. Other research found that both T-lymphocyte insulin binding and degradation increased with DHEA supplementation and associations between dehydroepiandrosterone, enhanced tissue insulin sensitivity and lowered serum triglycerides, particularly in regard to postmenopausal women.
(Loviselli A, et al. Minerva Endocrinol 1994;19:113-119; Casson PR, et al. Fertil Steril 1995;63:1027-1031.)
When an inbred strain of mice, predisposed to develop diabetes, was given 0.4% DHEA in their diet, the diabetes was rapidly reversed and the beta-cells were preserved. In a study of other animals without this genetic disorder, DHEA reduced the severity of diabetes resulting from administering a diabetes-inducing chemical called streptozotocin.
(Coleman DL, et al. Diabetes 1982:31:830-833.)
However, one study found that very large doses of DHEA (1,600 mg/day for 28 days) caused mild abnormalities of glucose metabolism.
(Mortola JF, Yen SS. J Clin Endocrinol Metab 1990;71:696-704.)
Hypercholesterolemia:
Studies on animals and humans have suggested that DHEA-S has antiatherogenic effects. It has been hypothesized that insulin may have an atherogenic role and it has been reported recently that, surprisingly, DHEA-S levels decreased in normal men and women during the hyperinsulinemic-euglycemic technique.
(Loviselli A, et al. Minerva Endocrinol 1994;19:113-119.)
Menopause and Osteoporosis:
Low doses of DHEA (usually 5-10 mg/day) may be especially appropriate for postmenopausal women whose serum DHEA-S levels are near or below the lower limit of normal. In some cases, DHEA relieves symptoms such as hot flashes that are usually attributed to estrogen deficiency. A combination of DHEA and identical-to-natural progesterone (usually given as a topical cream may be more effective against hot flashes than either treatment alone.
(Gaby AR. Alt Med Rev. 1996:1(2);66.)
It has been shown that menopause is associated with a reduction in DHEA levels. DHEA is manufactured by the adrenal glands. In the adrenals, DHEA is a source of estrogen and testosterone and may be capable of raising the levels of progesterone. DHEA is also one of the four major hormones produced by the ovaries; the others being estrogen. progesterone. and testosterone. At the time of menopause, the amount of DHEA manufactured by the ovaries declines. And, even though the ovaries are not the major source of DHEA, serum DHEA levels decline by more than 60% after menopause. After menopause, when ovarian production of DHEA slows down. the adrenal glands may not be not capable of taking over, and a marked deficiency of DHEA results. It is quite possible that giving DHEA to postmenopausal women with adrenal insufficiency would prevent the accelerated bone loss that these women experience. In one study. the average plasma level of DHEA (ng/100 ml) was 542 in premenopausal women, 197 in post-menopausal women, and only 126 in women whose ovaries had been surgically removed.
(Monroe SE, Menon KMJ. Clin Obstet Gynecol 1977:20:113-122.)
Recent research has also found that hormone replacement therapy using 2mg/day of oral micronized estradiol reduced the mean blood levels of DHEA-S by 23% and of testosterone by 42%.
(Casson PR, et al. Obstet Gynecol 1997.90:995-998.)
The decline in DHEA levels appears to be a factor in age-related bone loss. In one important study, bone mineral density was measured at the lumbar spine, hip, and radius in 105 women, aged 45-69. Fifty women had normal measurements, whereas 55 had low bone density. The average serum DHEA-S level was 60% lower in the women with low bone density than in those with normal bones. Women with low DHEA values were 40 times more likely to have osteoporosis than were women with normal DHEA levels. In contrast, there was no relationship between estrogen levels and bone density. (Szathmari M, et al. Osteoporsis Int 1994:4:84-88.) In a group of 29 post-menopausal women. there was a significant positive correlation between bone mineral content of the distal radius and ulna and age-adjusted serum DHEA levels. (Brody, S, et al. Maturitas 1987:9:25-32) A study of Belgian women found significant correlations were found between bone mineral content and DHEA levels (measured as DHEA-S.), even after correcting for the effects of age. These studies support the proposed role of DHEA in maintaining bone mass.
There are several mechanisms by which DHEA might prevent osteoporosis:
The partial conversion of DHEA to estrogen and testosterone would be expected to provide additional protection against bone loss. DHEA is converted into both estrogen and testosterone, both of which play a role in prevention of bone loss. In a study of postmenopausal women, administering DHEA increased serum levels of both testosterone and estrogens (estradiol and estrone).
Although DHEA is not converted directly into progesterone, it may, through a feedback mechanism, indirectly increase the production of progesterone. Both DHEA and progesterone are produced from the same precursor hormone, pregnenolone. If DHEA levels are adequate, then pregnenolone will be converted primarily to progesterone, rather than to DHEA.
One of the breakdown products of DHEA, a compound called 5-androstene-3B, 178-diol, is known to bind strongly to estrogen receptors. Therefore, DHEA. like estrogen, might inhibit bone resorption.
Androgens, a class of hormones which includes DHEA and testosterone, stimulate bone formation and calcium absorption. DHEA might, therefore. augment the bone-building effect of progesterone.
DHEA appears to be the only hormone which appears capable of both inhibiting bone resorption and stimulating bone formation.
(Casson PR, et al. Fertil Steril 1995;63:1027-1031; Labrie F, et al. Ann NY Acad Sci 1995;774:16-28; Buster JE et al. Am J Obstet Gynecol 1992;166:1163-1168; Mortola JF, Yen SS. J Clin Endocrinol Metab 1990;71:696-704; Weinstein RE, et al. J Allerg Clin Immol 1996;97:1-8; Yen SS, et al. Ann NY Acad Sci 1995;774:128-142.)
Multiple sclerosis: Administration of relatively large doses of DHEA has also been reported to increase stamina and improve the sense of wellbeing in patients with multiple sclerosis.
(Calabrese VP, et al. 1990. pp. 95-100.)
During the past several years a number of practitioners have been prescribing DHEA for patients with a variety of autoimmune diseases. Pre-treatment plasma levels of DHEA or DHEA-S are usually below normal in patients receiving prednisone or related drugs, because these medications cause adrenal suppression. However, DHEA-S levels are also frequently low in patients with autoimmune disease who are not receiving corticosteroids. The conditions for which various practitioners have found DHEA to be an effective component of treatment includerheumatoid arthritis, infl;ammatory bowel disease, ulcerative colitis, and lupus.
(Gaby AR. Alt Med Rev. 1996:1(2);63.)
Obesity:
Animal studies suggest that DHEA may be effective in treating obesity. In one by Yen et al, DHEA prevented the development of obesity without any toxic effects and did not suppress appetite, indicating that its effect was to speed up the metabolism. In another study, Cleary et al found that administering DHEA (0.6% of the diet) decreased body weight and body fat in both lean and obese Zucker rats. The decrease in body fat was primarily due to a decrease in the number of fat cells in lean rats and to decreases in both the number and size of fat cells in obese rats.
(Yen SS, et al. Ann N Y Acad Sci 1995;774:128-142; Cleary, MP, et al. J Nutr 1984:114:1242-1251.)
Rheumatoid Arthritis:
DHEA levels have also been found to be low in women with rheumatoid arthritis, a condition frequently associated with osteoporosis. In a study of 49 postmenopausal women with rheumatoid arthritis, DHEA levels (measured as DHEA-S ) were significantly lower than in healthy controls. DHEA levels were reduced to a greater extent in women taking corticosteroids for their arthritis than in those who were not. This is not surprising since corticosteroids are known to be an important cause of osteoporosis. However, DHEA levels were also significantly reduced in arthritic women who were not receiving corticosteroids. In this group of 49 women, DHEA levels correlated significantly with bone mineral density of the neck of the femur (a bone in the hip) and the spine. The serum level of DHEA was able to predict bone mineral density, even after corticosteroid therapy was taken into account.
(Gaby AR. Holistic Medicine. Spring, 1993:22.)
Systemic Lupus Erythematosus (SLE): Several lines of investigation lead to the consideration of DHEA as a candidate for hormonal therapy in systemic lupus erythematosus, including DHEA deficiency in patients with SLE, the effects of sex steroids on SLE, the immunomodulatory effects of DHEA, and the results of DHEA in animal models of SLE. DHEA has been shown to increase the production of interleukin-2, a component of the immune system which is consistently decreased in individuals with SLE.
In one study of ten female patients, with mild to moderate SLE and various disease manifestations, using 200 mg/day of DHEA orally, all indices for overall SLE activity including the SLEDAI (SLE Disease Activity Index) score and physicians overall assessment were improved, and corticosteroid requirements were decreased. Another series of uncontrolled observations in 50 patients suggested that DHEA has overall benefits for lupus activity, alleviating specific lupus symptoms as well the systemic manifestations of lupus, with incremental benefits over 3 to 12 months of treatment. DHEA appeared to decrease the number of lupus flares and to have a steroid sparing effect. A more recent study of 23 women with mild to moderate SLE found statistically significant improvements were found in all lupus outcomes over 6 months, with an optimum serum DHEAS of 1000 microg/dl, but that the clinical response to DHEA was not clearly dose dependent and that serum levels of DHEA and DHEAS correlated only weakly with lupus outcomes.
(Van Vollenhoven RF, et al. Arthritis Rheum 1994;37:1305-1310; Van Vollenhoven RF, McGuire, JL. Ann Med Interne Paris 1996;147(4):290-296; Derksen RH. Semin Arthritis Rheum 1998 Jun;27(6):335-347; Barry NN, McGuire JL, van Vollenhoven RF. J Rheumatol 1998 Dec;25(12):2352-2356.)
» dosage:
Maintenance dose: Usually not necessary. Optimal levels of intake have not been established. Individuals who have not based diagnosed as having a hormonal deficiency pattern, preferably via lab tests, should usually not take DHEA as a supplement.
Therapeutic dose: There is no consensus among practitioners who prescribe DHEA as to an optimal dose; some practitioners are routinely prescribing 50 mg per day for healthy men and 100 mg per day for healthy women, while others typically prescribe 2-30 mg per day. Much larger doses are being often given to patients with cancer, AIDS, and other serious conditions. Even when using lab testing to evaluate appropriateness of and response to DHEA, there are as yet no data on what constitutes an optimum serum level. Consequently. the judicious practice would be to err on the side of caution by using low doses of DHEA and observe discrimination in the use of supraphysiologic doses.
One useful set of guidelines was provided by Alan Gaby, M.D., in Alternative Medicine Review, where he wrote that he usually prescribes 5-15 mg per day for women and 10-30 mg per day for men. Many patients have obvious improvements with these doses. With some patients who have not improved I have prescribed larger doses, but in most cases, the larger doses were not helpful either. The one exception has been patients with lupus or other autoimmune diseases, who sometimes needed as much as 100 mg per day or more to obtain benefit. (Gaby AR. Alt Med Rev. 1996:1(2);60-69.)
Beyond those who prescribe DHEA, its supplementation is a controversial issue. Opinions vary widely as to the benefits and risks of using hormones, such as DHEA, as nutritional supplements. Any such usage should be monitored by a physician and is best undertaken after initially testing DHEA levels.
» forms:
DHEA has usually been available as DHEA or in the DHEA-S forms.
A synthetic form of DHEA is available as a supplement in tablet, capsule, liquid, and sublingual forms. The source material of either soy or wild yams is converted to DHEA in a laboratory.
While some products have claimed to contain natural DHEA precursors from wild yam, no studies have ever confirmed that the body can convert any compounds in wild yam to DHEA or other steroid hormones .
One recommended form of DHEA is in capsule form, in a base of hvdroxymethvlcellulose.
(Gaby AR. Alt Med Rev. 1996:1(2);67.)
3-Acetyl-7-Oxo DHEA (also known as 7-Keto DHEA) is a recently introduced an analog of DHEA which cannot be metabolized to active androgenic or estrogenic hormones but retains and enhances the immunologic, memory-enhancing and thermogenic effects of DHEA.
(Weeks C, et al. FASEB Jrnl, Abstracts Part II, 4428 (1998); Davidson MH, et al. FASEB Jrnl, Abstracts Part II, 4429; 1998.)
» mechanism: Stimulation and supplementation of adrenal hormone levels.
» side effects:
DHEA appears to be quite safe. Dosages as high as 1,600 mg per day have been given for periods of 28 days without any serious side effects, although mild abnormalities of blood sugar metabolism occurred in some cases. Minor side effects, such as acne or a slight increase in hair growth on the arms and legs, may occasionally occur when DHEA is taken.
In one study of Lupus, utilizing 200 mg per day of DHEA orally for 3-6 months treatment, the only frequently noted side effect being mild acneiform dermatitis.
(Van Vollenhoven RF, et al. Arthritis Rheum 1994;37:1305-1310.)
» toxicity:
For a steroid hormone, DHEA appears to be relatively safe. But, as with any hormonal supplementation, caution should be exercised in the use of DHEA as a supplement or therapeutic agent and use without the involvement of a nutritionally-trained healthcare professional is inadvisable. This is especially true when there is no data available on the effects of long-term administration of DHEA.
Excessive levels of DHEA may be of particular concern to women due to their risk of inducing a variety of hormonal imbalances, including the potential effect of raising testosterone levels and possibly triggering male secondary sex characteristics at supplemental doses. One study found that a woman taking 100 mg of DHEA per day for one year started to develop facial hair, presumably as a consequence of. Some concerns have been raised that DHEA might contribute to liver damage or even liver cancer but no substantial confirmation of these harmful effects has been demonstrated.
(Casson PR, et al. Fertil Steril 1995;63:1027-1031.)
In one study, the addition of 0.6% DHEA to the diet of rats reduced body weight and enhanced the development of chemically-induced pre-neoplastic pancreatic lesions. (Tagliaferro, AR, et al. Adv Exp Med Biol 1992:322:119-129.). Although that dose of DHEA is extremely large (the equivalent human dose would be approximately 2.000 mg/day, this report indicates that DHEA is by no means innocuous and therefore it should be used with caution.
(Gaby AR. Alt Med Rev. 1996:1(2);67.)
The new possibilities presented by keto-7 DHEA may significantly reduce or eliminate many of the potential side effects and/or toxicities associated with use of DHEA.
» contraindications:
Some nutritional experts caution against anyone under 40 years of age using supplemental DHEA outside the supervision of an informed physician and primarily in the context of specifically-indicated health conditions.
(Murray M, Pizzorno J, 1998.)
Personal or family history of hormone-related cancer, such as breast or prostate cancer. Given the role of DHEA as a precursor to both estrogen and testosterone, special caution should be exercised by individuals with a family history of hormone-related cancer. Some researchers have expressed concern that while younger women with breast cancer may have low levels of DHEA, postmenopausal women with breast cancer appear to have high levels of DHEA.
(Zumoff B, et al. Canc Res 1981;41:3360-3363.)
Kaposis sarcoma: Caution may be appropriate given that high serum DHEA levels have been implicated in the pathogenesis of Kaposis sarcoma in HIV/AIDS.
(Christieff N, et al. J Clin Pathology 48:513-518, 1995.)
Initial indications are that keto-7 DHEA may significantly reduce or eliminate many of the potential side effects and/or toxicities associated with use of DHEA.
» clinical observations:
Thyroid hormone: Alan Gaby, M.D., has reported that about 10% of patients who are taking thyroid hormone develop symptoms of thvrotoxicosis after starting DHEA therapy. That observation is consistent with a report that DHEA potentiates the action of thyroid hormones.
(McIntosh MK, Berdanier CD. J Nutr Biochem 1992:3;194-199.)
Symptoms of thyroid over-treatment responded to a reduction in the thyroid-hormone dosage. and patients reported that they felt better on DHEA plus lower-dose thyroid hormone than they did on thyroid hormone alone.
(Gaby AR. Alt Med Rev. 1996:1(2);67.)
Recent research has also found that hormone replacement therapy using 2 mg perday of oral micronized estradiol reduced the mean blood levels of DHEA-S by 23% (and of testosterone by 42%).
(Casson PR, et al. Obstet Gynecol 1997.90:995-998.)
» interactions:
nutrient potentially affecting drug toxicity: Corticosteroids including Prednisone
mechanism: The presence of exogenous corticosteroids from use of prednisone or related drugs can confuse the internal hormonal regulatory processes. If the pituitary senses that corticosteroid levels are higher than normal the regulatory feedback loops can send a signal to decrease the production of ACTH (adrenocortical stimulating hormone) and thus reduce the levels of several key hormones. As a consequence of these changes in hormonal balance, the internal stimulation to produce DHEA can often fall, androgen levels can rise, and the cascade of side effects, such as muscle wasting, ensue.
nutritional support: Individuals using corticosteroids for extended periods should consult with their prescribing physician and/or a nutritionally trained healthcare professional about the potential benefits of supplementing with DHEA to prevent muscle wasting without losing the antiinflammatory effect of prednisone. Laboratory tests can determine the degree to which DHEA has been adversely affected and suggest an appropriate level of supplementation, if needed.
(Gennari R, Alexander JW. Crit Care Med 1997 Jul;25(7):1207-1214.)
Footnotes
Akwa Y, Baulieu EE. [Neurosteroids: behavioral aspects and physiological implications]. J Soc Biol. 1999;193(3):293-298. (Review) [Article in French]
Araneo BA, et al. Administration of dehydroepiandrosterone to burned nice preserves normal immunologic competence. Arch Surg 1993:128:318-325.
Aranen B, Daynes R. Dehydroepiandrosterone functions as more than an antiglucocorticoid in preserving immunocompetetence after thermal injury. Endocr 1995:136:393-401.
Araneo B, Dowell T, Woods ML, et al. DHEA-S as an effective vaccine adjuvant in elderly humans. Proof-of-principle studies. Ann NY Acad Sci 1995;774:232-248.
Abstract: Mice immunized shortly after oral dosing with DHEA-S demonstrated high serum antibody titers and complete protection from paralysis. These results became the basis for initiating proof-of-principle studies in human volunteers above age 65 using a licensed influenza vaccine and tetanus toxoid in two independent studies. The use of an oral delivery form of DHEA-S before influenza vaccination was associated with a demonstrable increase in the number of individuals with a fourfold increase in HAI titers following vaccination. The overall mean increase in HAI titers was highest in the DHEAS-treated group. The use of DHEA-S in the immunization of elderly subjects against tetanus toxoid, while unable to enhance the responses, was not a detriment to antibody response.
Arguelles AB, Poggi UL, Saborida C, Hoffman C, Chekherdemian M, et al . Endocrine profiles and breast cancer. Lancet 1973:1:165-168.
Barrett-Connor B, Khaw K-T, Yen SSC. A prospective study of dehydroepiandrosterone sulfate. mortality, and cardiovascular disease. N Engl J Med 1986.315:1519-1524.
Barrett-Connor B, Khaw K-T. Absence of an inverse relation of dehvdroepiandrosterone sulfate with cardiovascular mortality in postmenopausal women. N Engl J Med 1987:317:711.
Barry NN, McGuire JL, van Vollenhoven RF. Dehydroepiandrosterone in systemic lupus erythematosus: relationship between dosage, serum levels, and clinical response. J Rheumatol 1998 Dec;25(12):2352-2356.
Abstract: OBJECTIVE: To examine in women with systemic lupus eythematosus (SLE) who participated in a clinical trial the relationship between daily dose of dehydroepiandrosterone (DHEA), serum levels of DHEA and DHEA sulfate (DHEAS), clinical effectiveness, and side effects. METHODS: Twenty-three women with mild to moderate SLE were treated with DHEA for a 6 month period. The starting dose was 50 mg/day, and monthly stepwise increases were allowed. Subjects were assessed monthly by the Systemic Lupus Erythematosus Disease Activity Index, Systemic Lupus Activity Measure (SLAM), Health Assessment Questionnaire, and other outcomes. Serum testosterone, DHEA, and DHEAS levels were obtained and side effects noted monthly. RESULTS: Statistically significant improvements were found in all lupus outcomes over 6 months. Serum DHEA and DHEAS levels correlated with the dose of DHEA. Serum DHEA and DHEAS correlated negatively with SLAM score. A second order regression analysis of serum DHEAS level versus SLAM score suggested that the optimal serum level of DHEAS was 1000 microg/dl. The most common side effect was acne. CONCLUSION: The clinical response to DHEA was not clearly dose dependent. Serum levels of DHEA and DHEAS correlated only weakly with lupus outcomes, but suggested an optimum serum DHEAS of 1000 microg/dl. Monitoring these serum levels appears to have limited clinical utility.
Baulieu EE, Thomas G, Legrain S, Lahlou N, Roger M, Debuire B, Faucounau V, Girard L, Hervy MP, Latour F, Leaud MC, Mokrane A, Pitti-Ferrandi H, Trivalle C, de Lacharriere O, Nouveau S, Rakoto-Arison B, Souberbielle JC, Raison J, Le Bouc Y, Raynaud A, Girerd X, Forette F. Dehydroepiandrosterone (DHEA), DHEA sulfate, and aging: contribution of the DHEAge Study to a sociobiomedical issue. Proc Natl Acad Sci USA. 2000;97(8):4279-4284.
Abstract: The secretion and the blood levels of the adrenal steroid dehydroepiandrosterone (DHEA) and its sulfate ester (DHEAS) decrease profoundly with age, and the question is posed whether administration of the steroid to compensate for the decline counteracts defects associated with aging. The commercial availability of DHEA outside the regular pharmaceutical-medical network in the United States creates a real public health problem that may be resolved only by appropriate long-term clinical trials in elderly men and women. Two hundred and eighty healthy individuals (women and men 60-79 years old) were given DHEA, 50 mg, or placebo, orally, daily for a year in a double-blind, placebo-controlled study. No potentially harmful accumulation of DHEAS and active steroids was recorded. Besides the reestablishment of a "young" concentration of DHEAS, a small increase of testosterone and estradiol was noted, particularly in women, and may be involved in the significantly demonstrated physiological-clinical manifestations here reported. Bone turnover improved selectively in women >70 years old, as assessed by the dual-energy x-ray absorptiometry (DEXA) technique and the decrease of osteoclastic activity. A significant increase in most libido parameters was also found in these older women. Improvement of the skin status was observed, particularly in women, in terms of hydration, epidermal thickness, sebum production, and pigmentation. A number of biological indices confirmed the lack of harmful consequences of this 50 mg/day DHEA administration over one year, also indicating that this kind of replacement therapy normalized some effects of aging, but does not create "supermen/women" (doping).
Baulieu EE. Neuroactive neurosteroids: dehydroepiandrosterone (DHEA) and DHEA sulphate. Acta Paediatr Suppl. 1999 Dec;88(433):78-80.
Baulieu EE. Neurosteroids: a novel function of the brain. Psychoneuroendocrinology. 1998 Nov;23(8):963-987. (Review)
Blauer KL, et al. Dehvdroepiandrosterone antagonizes the suppressive effects of dexamethasone on lymphocyte proliferation. Endocr 1991:129:3174-3179.
Brody S, et al. Adrenal steroids in post-menopausal women: relatiotin to obesity and to bone mineral content. Maturitas 1987:9:25-32.
Buster JE, Casson PR, Straughn AB, Dale D, Umstot ES, Chiamori N, Abraham GE. Postmenopausal steroid replacement with micronized dehydroepiandrosterone: preliminary oral bioavailability and dose proportionality studies. Am J Obstet Gynecol 1992;166:1163-1168.
Abstract: Eight postmenopausal women randomly received either a placebo or 150 or 300 mg of oral micronized dehydroepiandrosterone in a lipid matrix. Serum dehydroepiandrosterone, dehydroepiandrosterone sulfate, testosterone, and estradiol were measured periodically over the 12 hours after each dose. Mean peak steroid concentrations after 150 mg (300 mg) doses were dehydroepiandrosterone 1617 (2639) ng/dl, 7 (11.5)-fold above placebo; dehydroepiandrosterone S 1185 (1688) micrograms/dl, 14 (20)-fold above placebo; and testosterone 183 (311) ng/dl, 4 (7)-fold above placebo. Estradiol concentrations remained less than 20 pg/ml, but androgen concentrations rose by 1 hour and remained elevated through the twelfth hour. Peak androgen concentrations and areas under the curves exhibited proportionality with both doses. A testosterone radioimmunoassay revealed a 300% overestimation for testosterone. Thus after appropriate readjustment maximum testosterone concentrations were observed consistently within physiologic premenopausal ranges after the 150 mg dose. The study concluded that micronized dehydroepiandrosterone may provide a steroidal postmenopausal replacement that is adjunctive to estrogens and worthy of further investigation.
Calabrese VP, Isaacs ER, Regelson W. Dehydroepiandrostemone in multiple sclerosis: positive effects on the fatigue syndrome in a non-randomized study. In Kalimi, M, Regelson, W. The Biological Role of Dehydroepiandrosterone. de Gruyter. New York. 1990. 95-100.
Casson PR, Elkind-Hirsch KE, Buster JE, Hornsby PJ, Carson SA, Snabes MC. Effect of postmenopausal estrogen replacement on circulating androgens. Obstet Gynecol 1997 Dec;90(6):995-998.
Abstract: OBJECTIVE: To determine the effect of estrogen replacement therapy (ERT) on serum androgen levels in postmenopausal women. METHODS: We measured serum dehydroepiandrosterone (DHEA), DHEA-sulfate, testosterone, estradiol (E2), LH, FSH, and sex hormone binding globulin in 8:00 AM fasting serum samples from a previous randomized, blinded, placebo-controlled crossover study in which 28 postmenopausal women (27 naturally menopausal) were given 2 mg/day of oral micronized estradiol. The treatment arms were 12 weeks with a 6-week washout. RESULTS: Estrogen replacement therapy raised mean (+/- standard error of the mean [SEM]) serum E2 from 8.7 +/- 1.0 to 117 +/- 18.7 pg/mL (P < .001 from baseline). Concurrently, mean (+/- SEM) DHEA-sulfate fell from 67.3 +/- 9.6 to 52.1 +/- 6.4 micrograms/dL (P < .001), and mean (+/- SEM) testosterone fell from 16.1 +/- 2.4 to 9.4 +/- 1.4 ng/dL (P = .006). Both FSH and LH declined significantly. Sex hormone binding globulin increased by 160% with ERT (P < .001). CONCLUSION: Menopausal ERT decreases serum androgen levels, decreasing DHEA-sulfate and testosterone by 23% and 42%, respectively. Whereas the decline in testosterone is likely due to decreased LH-driven ovarian stromal steroidogenesis, the declining levels of DHEA-sulfate also may imply a direct adrenal effect of estrogen. Bioavailable testosterone likely is reduced even more profoundly because sex hormone binding globulin is increased 160% by estrogen. Thus, menopausal ERT may induce relative ovarian and adrenal androgen deficiency, creating a rationale for concurrent physiologic androgen replacement.
Casson PR, Faquin LC, Stentz FB, Straughn AB, Andersen RN, Abraham GE, Buster JE. Replacement of dehydroepiandrosterone enhances T-lymphocyte insulin binding in postmenopausal women. Fertil Steril 1995;63:1027-1031.
Abstract: Oral micronized DHEA (50 mg/d) was administered in 3-week treatments to 11 postmenopausal women in a prospective, placebo-controlled, randomized, blinded, crossover trial with an interarm washout. After dose (23 hour) serum DHEA, DHEAS, T, and cortisol levels were measured, as were fasting lipoproteins, oral glucose tolerance tests (OGTT), T-lymphocyte insulin binding and degradation, and urine collagen cross-links. Morphometric changes were determined by hydrostatic weighing. Dehydroepiandrosterone sulfate, DHEA, T, and free T increased up to two times premenopausal levels with treatment. Fasting triglycerides declined; no change in collagen cross-links or morphometric indexes was noted. Oral glucose tolerance test parameters did not change, but both T-lymphocyte insulin binding and degradation increased with DHEA. Fifty milligrams per day of oral DHEA gives suprahysiologic androgen levels; 25 mg/d may be more appropriate. Dehydroepiandrosterone enhanced tissue insulin sensitivity and lowered serum triglycerides. Rationale is provided for postmenopausal replacement therapy with this androgen.
Christieff N, Gharakhanian C, Thobie N, et al. Differences in androgens of HIV positive patients with and without Kaposis sarcoma. J Clin Pathology 1995;48:513-518.
Cleary MP, Shepherd A, Jenks B. Effect of dehydroepiandrosterone on growth in lean and obese Zucker rats. J Nutr 1984:114:1242-1251.
Coleman DL, Leiter EH, Schwizer RW. Therapeutic effects of dehydroepiandrosterone (DHEA) in diabetic mice. Diabetes 1982:31:830-833.
Davidson MH, Weeks CE, Lardy H, Maki K, Umporowicz D. Safety and Endocrine Effects of 3-Acetyl-7-Oxo DHEA (7-Keto DHEA). FASEB Jrnl, Abstracts Part II, 4429 (1998)
Abstract: The present study examined the effects of 7-keto-DHEA on several endocrine and safety parameters in healthy adult men (18-49 years of age). 7-Keto-DHEA (n=18) or placebo (n=6) were administered for 8 weeks. The 7-keto-DHEA dose was increased weekly to a maximum of 100 mg twice daily during the final 4 weeks of treatment. Levels of the hormones measured did not differ between groups (p>0.10) at baseline or during treatment. End-of-trial levels of dihydrotestosterone, estradiol, cortisol and insulin were not different from baseline values (p>0.10). A small reduction in total testosterone [601 ± 142 (SD) vs. 554 ± 149 ng/dL, p<0.01] and a small, clinically insignificant, increase in free testosterone [27 ± 5 vs. 31 ± 8 pg/mL, p<0.01] were observed among men receiving, 7-keto-DHEA. All hormone levels were within normal limits. This study shows that 7-keto-DHEA is well-tolerated at doses up to 200 mg/d and does not produce clinically important sex hormone changes in healthy men.
Daynes R, Dudley DJ, Araneo BA. Regulation of murine lymphokine production in vivo II. DHEA is a natural enhancer of interleukin 2 synthesis by helper T cells. Eur J Immunol 20:793-802, 1990
Derksen RH. Dehydroepiandrosterone (DHEA) and systemic lupus erythematosus. Semin Arthritis Rheum 1998 Jun;27(6):335-347. (Review)
Abstract: OBJECTIVE: This study was performed to evaluate in vivo and in vitro data on the effects of the adrenal steroid dehydroepiandrosterone (DHEA) with emphasis on its potential use in the treatment of systemic lupus erythematosus (SLE). METHODS: The literature dealing with DHEA was reviewed. RESULTS: Initially, research on DHEA focused on effects of DHEA in relation to obesity. Over the past decade, research stimulated by associations between the physiological decline in DHEA and aging, cardiovascular disease, changes in metabolism, brain function, and immune senescence have generated insight into the many effects that DHEA or its metabolites may have. In SLE a role for sex hormones in both the etiopathogenesis and disease activity is recognized. In SLE, as in aging, low DHEA levels are frequently found, especially with corticosteroid treatment. CONCLUSIONS: Research data in the elderly, on both hormonal and immunologic effects, suggest that DHEA may become an adjunctive treatment for SLE patients.
Dunn PJ, et al. Dehydroepiandrosterone sulphate concentrations in asthmatic patients: pilot study. NZ Med J 1984:97:805-808.
Dyner TS, et al. An open-label dose-escalation trial of oral dehydroepiandrosterone tolerance and pharmacokinetics in patients with HIV disease. J AIDS 1993;6:459-465.
Ebeling P, Koivisto VA. Physiological importance of dehydroepiandrosterone. Lancet 1994;343:1479-1481.
Gaby AR. Dehydroepiandrosterone: Biological Effects and Clinical Significance. Alternative Medicine Review. 1996:1(2);60-69.
Gaby AR. DHEA: The Hormone that Does it All. Holistic Medicine. Spring, 1993: 19-24.
Gaby AR. Preventing and Reversing Osteoporosis. Prima Publishing: Rocklin, CA, 1993.
Gaby AR. Research Review. Nutr Healing Jun 1997: 8.
Gennari R, Alexander JW. Arginine, glutamine, and dehydroepiandrosterone reverse the immunosuppressive effect of prednisone during gut-derived sepsis. Crit Care Med 1997 Jul;25(7):1207-1214.
Abstract: OBJECTIVE: Corticosteroids are used broadly in clinical practice but may profoundly impair resistance to infections. In contrast, arginine and glutamine are safe and effective immunonutrients that can improve resistance to infection in both animals and humans. This study assessed whether arginine and/or glutamine, with or without dehydroepiandrosterone, a natural endogenous steroid, could reverse the susceptibility to infection caused by prednisone in a burned animal model. DESIGN: Prospective, randomized study. SETTING: A laboratory approved by the American Association for the Accreditation of Laboratory Animal Care at the Shriners Burns Institute, Cincinnati Unit. SUBJECTS: Adult female Balb/c mice, weighing 18 to 22 g. INTERVENTIONS: Animals were prefed an arginine- and/or glutamine- or a glycine-supplemented diet for 14 days. Dehydroepiandrosterone (25 mg/kg/day) and/or prednisone (10 mg/kg/day) were given on days -4 to 0 before animals were given a gavage of 10(9) 111indium-oxine-radiolabeled or -unlabeled Escherichia coli and 20% total body surface area burn injury. Survival rate and the extent of translocation of E. coli were determined. MEASUREMENTS AND MAIN RESULTS: Feeding with diets supplemented with arginine, glutamine, and arginine plus glutamine and treatment with dehydroepiandrosterone reversed the susceptibility to infections caused by prednisone and burn injury. The beneficial effects were mediated by enhanced killing of translocated bacteria and/or by an improved gut barrier function. CONCLUSIONS: Dietary supplementation can reverse the susceptibility to infections caused by prednisone. Both arginine and glutamine as well as dehydroepiandrosterone may be useful therapeutic agents for preventing infections in steroid-treated patients.
Hasheeve, D, Salvato, P, Thompson, C. DHEA: a potential treatment for HIV disease. Intl AIDS Conference Abstract no PB0322, 1994.
Helzlsouer, KJ, et al. Relationship of prediagnostic serum levels of dehydroepiandrosterone and dehydroepiandrosterone sulfate to the risk of developing premenopausal breast cancer. Cancer Res 1992:52:14.
Jacobson, MA, Fusaro, RE, Galznarini, M, Lang, W. Decreased serum dehydroepiandrosterone is associated with an increased progression of human immunodeficiency virus infection in men with CD4 cell counts of 200-499. J Infect Dis 1991:164:864-868.
Koo E, Feher KG, Feher T, Fust G. Effect of dehydroepiandrosterone on hereditary angioedema. Klin Wochenschr 1983;61:715-717.
Abstract: Hereditary angioneurotic edema (HAE) is a complement-related clinical disorder with a deficiency of the C1 esterase inhibitor protein. Eight patients with severe attacks of the disease were treated with the adrenal androgen dehydroepiandrosterone sulphate (DS). Steroid therapy for 3-28 months resulted in dramatic improvement in their clinical state and a moderate increase in the serum concentration of C1 inhibitor. There was a significant increase in the serum level of either unconjugated dehydroepiandrosterone (D) or of DS during treatment.
Labrie F, Belanger A, Simard J, et al. DHEA and peripheral androgen and estrogen formation: Intracrinology. Ann NY Acad Sci 1995;774:16-28.
Loria, RM. et al. Protection against acute lethal viral infections with the native steroid dehydroepiandrosterone (DHEA). J Med Viral 1988:26:301-314..
Loviselli A, Pisanu P, Cossu E, et al. Low levels of dehydroepiandrosterone sulfate in adult males with insulin-dependent diabetes mellitus. Minerva Endocrinol 1994;19:113-119.
Abstract: 805 participants were divided into three groups. In all three groups serum concentrations of DHEAS, 17 OH progesterone (17 OHP), delta 4 androstenedione (A4) and cortisol (F) were measured. In 10 patients from group A and in 9 patients from group B the ACTH test (9.25 mg IM Synacthen) was administered and the same hormonal pattern was measured after 60 min. In group C the same hormonal evaluation was performed 5 +/- 2.8 months after commencement of insulin therapy. The study found that DHEA-S serum concentrations were significantly decreased in group A (median 2.9; range 1.1-5.2 mumol/l) with respect to group B (median 5.7; range 3.0-9.5 mumol/l) (p < 0.0012). However, the serum concentrations of 17 OHP (median 3.9 nm/l; range 2.9-6.9 nm/l and A4 (median 5.2 nm/l; range 1.8-10.2 nm/l) were also significantly reduced, while cortisol levels and the 17 OHP/A4 ratio were comparable to group B. After administration of ACTH, the delta increment in cortisol percentage showed a frank increase (55.1%) in group A with respect to group B (33.1%) (p < 0.01). The rise in DHEA-S showed a lower increase in group A (10.2%) with respect to group B (65.5%) even though not statistically significant, while the other hormones showed an overlap between the two groups. In group C the serum concentrations of hormones before insulin therapy did not show any statistical differences with respect to the values in group B. A second evaluation, which was performed during insulin therapy, showed that only the 17 OHP/A4 ratio tended towards higher values with respect to pretherapy values (1.1 and 0.6 respectively; p = 0.07). In conclusion our data confirm low DHEA-S levels during chronic insulin administration therapy. The underlying mechanism could be a general aspecific reduction in the activity of P 450 C 21 SCC enzymes in contrast with the specific inhibition of 17.20-lyase obtained during insulin bolus. Whether the low serum concentrations of DHEA-S can determine an atherogenic effect of insulin needs further investigation, but the hormone could constitute a new parameter for the follow-up of patients affected by diabetes mellitus.
May M. et al. Protection from glucocorticoid induced thymic involution by dehydroepiandrosterone. Life Sci 1990:46:1627-1631.
Mayer D, Weber E, Bannasch P. Modulation of liver carcinogenesis by dehydroepiandrosterone. In Kalimi, M, Regelson, W. The Biological Role of Dehydroepiandrosterone. de Gruyter. New York. 1990. pp. 361-385.
McIntosh MK, Berdanier CD. Influence of dehydroepiandrosterone (DHEA) on the thyroid hormone status of BHE/cdb rats. J Nutr Biochem 1992:3;194-199.
Merril CR, Harrington MG, Sunderland T. Reduced plasma dehydroepiandrosterone concentrations in HIV infection and Alzheimers disease. In Kalimi, M, Regelson, W. The Biological Role of Dehydroepiandrosterone. de Gruyter. New York. 1990. 101-105.
Mitchell LE, et al. Evidence for an association between dehydroepiandrosterone sulfate and nonfatal, premature myocardial infarction in males. Circulation 1994:89:89-93.
Monroe SE, Menon KMJ. Changes in reproductive hormone secretion during the climacteric and postmenopausal periods. Clin Obstet Gynecol 1977:20:113-122.
Morales AJ, Nolan JJ, Nelson JC, Yen SS. Effects of replacement dose of dehydroepiandrosterone in men and women of advancing age. J Clin Endocrinol Metab 1994;78:1360-1367.
Abstract: A randomized placebo-controlled cross-over trial of nightly oral DHEA administration (50 mg) of 6-month duration was conducted to study the effect of a replacement dose of DHEA in 13 men and 17 women, 40-70 years of age. During each treatment period, concentrations of androgens, lipids, apolipoproteins, IGF-I, IGF-binding protein-1 (IGFBP-1), IGFBP-3, insulin sensitivity, percent body fat, libido, and sense of well-being were measured. A subgroup of men (n = 8) and women (n = 5) underwent 24-h sampling at 20-min intervals for GH determinations. DHEA and DS serum levels were restored to those found in young adults within 2 weeks of DHEA replacement and were sustained throughout the 3 months of the study. A 2-fold increase in serum levels of androgens (androstenedione, testosterone, and dihydrotestosterone) was observed in women, with only a small rise in androstenedione in men. There was no change in circulating levels of sex hormone-binding globulin, estrone, or estradiol in either gender. High density lipoprotein levels declined slightly in women, with no other lipid changes noted for either gender. Insulin sensitivity and percent body fat were unaltered. Although mean 24-h GH and IGFBP-3 levels were unchanged, serum IGF-I levels increased significantly, and IGFBP-1 decreased significantly for both genders, suggesting an increased bioavailability of IGF-I to target tissues. This was associated with a remarkable increase in perceived physical and psychological well-being for both men (67%) and women (84%) and no change in libido. In conclusion, restoring DHEA and DS to young adult levels in men and women of advancing age induced an increase in the bioavailability of IGF-I, as reflected by an increase in IGF-I and a decrease in IGFBP-1 levels. These observations together with improvement of physical and psychological well-being in both genders and the absence of side-effects constitute the first demonstration of novel effects of DHEA replacement in age-advanced men and women.
Mortola JF, Yen SS. The effects of oral dehydroepiandrosterone on endocrine-metabolic parameters in postmenopausal women. J Clin Endocrinol Metab 1990;71:696-704.
Abstract: 1600 mg/day (in four divided doses) were administered orally to six postmenopausal women for 28 days in a double blind placebo-controlled cross-over study to discern the pharmacological effects of DHEA in older women with low endogenous DHEA and DHEA sulfate (DS),. Serum concentrations of androgens after the first 400-mg dose of DHEA increased rapidly and reached a maximum at 180-240 min, resulting in increases over baseline of 6-fold for DHEA, 12-fold for DS and androstenedione, 2.5-fold for testosterone, and 15-fold for dihydrotestosterone, but estrone, estradiol, and sex hormone-binding globulin (SHBG) were unchanged. Assessment at weekly intervals revealed a further increase in all androgens which was maximal at 2 weeks and remained markedly elevated, although it declined somewhat by 4 weeks. The increments observed after 2 weeks of DHEA administration reached 15-fold for DHEA, 9-fold for testosterone, and 20-fold for DS, androstenedione, and dihyrotestosterone. Both estrone and estradiol showed a progressive increase to 2-fold the basal value at 4 weeks. Integrated SHBG and thyroid binding globulin levels decreased (P less than 0.05) during DHEA treatment. However, LH, FSH, body weight, and percent body fat, as measured by underwater weighing, were unaltered during the 4-week experiment. A marked decline of 11.3% (P less than 0.05) in serum cholesterol and 20.0% (P less than 0.05) in high density lipoprotein noted within the first week of DHEA administration persisted for the 28-day period and was accompanied by a nonsignificant downward trend in low density lipoprotein, very low density lipoprotein, and triglycerides. Peak insulin levels during the 3-h oral glucose tolerance test were significantly higher (P less than 0.05) after the 28 days of DHEA and were accompanied by a 50% increase in the integrated insulin response (P less than 0.01) without a significant change in fasting glucose insulin or glucose-6-phosphate dehydrogenase values. These data show that oral DHEA is rapidly adsorbed, and a prompt conversion to DS as well as all potent androgens and estrogens occurs with a sustained effect for the 28-day duration of treatment. Thus, in postmenopausal women there appears to be abundant and effective enzymatic systems for the biotransformation of DHEA to C-19 and C-18 sex steroids. Further, pharmacologically imposed DHEA in postmenopausal women induced insulin resistance, altered cholesterol and the high to low density lipoprotein ratio, and decreased circulating SHBG and thyroid binding globulin concentrations. These findings appear to result from the induction of a highly androgenic state and its impact on several endocrine-metabolic parameters in older postmenopausal women.
Murray M, Pizzorno J. The Encyclopedia of Natural Medicine. Revised Second Edition. Prima Publishing: Rocklin, CA, 1998.
Newcomer LM, et al. Dehydroepiandrosterone sulfate and the risk of myocardial infarction in US male physicians: a prospective study. Am J Epidemiol 1994:140:870-875.
Nyce JW, Magee PN, Hard GC, Schwartz AG. Inhibition on 1 .2-dimethythydrazine-induced colon tumorigenesis in Balb/c mice by dehydroepiandrosterone. Carcinogenesis 1984:5:57-62.
Regelson W, Loria S, Kalimi M. Hormonal intervention: buffer hormones or state dependency. The role of dehydroepiandrosterone (DHEA), thyroid hormone, estrogen and hypophysectomy in aging. Ann NY Acad Sci 1988:521:260-273.
Regelson W, et al. Dehydroepiandrosterone (DHEA) - the mother steroid I. Immunologic action. Ann NY Acad Sci 1994:719;553-563.
Salvata, et al. XI International Conference on AIDS Abstract We.B.3385, 1996.
Sandre C, Geniteau-Legendre M, Scherrmann JM, Quero AM, Labarre C. Immunoreactivity of endogenous digitalis-like substances in cord blood sera studied with antidigitoxin monoclonal antibodies. Ther Drug Monit 1995 Feb;17(1):19-24.
Abstract: The presence of digitoxin-like immunoreactive substances, whose nature is yet unknown, has been demonstrated in the umbilical cord blood. We selected six antidigitoxin monoclonal antibodies (MAb) having different specificity profiles concerning digitoxin analogs and steroid hormones. These antibodies were tested in a digitoxin radioimmunoassay (RIA). With the help of this technique, we measured the concentrations of apparent digitoxin in the cord blood drawn either at birth or in utero from mothers not undergoing any digitalis treatment. In the cord blood of newborns, the concentrations of apparent digitoxin, measured by the two MAbs that have the highest cross-reactions with dehydroepiandrosterone (DHEA) (123A23 and 145A41), were two or three times higher than with the other antibodies. In the fetal cord blood, where the concentration of DHEA is five to seven times lower than that observed at birth, these antibodies revealed a threefold lower concentration of apparent digitoxin than that observed in blood drawn at birth. Furthermore, MAbs that had similar specificities towards digitoxin analogs and steroids showed different measurements of digitoxin-like concentrations. These observations suggest that digitoxin-like immunoreactive compounds detected by the RIA may constitute a group of different molecules, one of which would be the DHEA.
Schwartz AG. Inhibition of spontaneous breast cancer formation in female C3H (A vy/a) mice by long-term treatment with dehydroepiandrosterone. Cancer Res. 1979:39:1129-1132.
Schinazi RF, Eriksson B, Arnold B, Lekas P, McGrath M. Effect of DHEA in lymphocytes and macrophages infected with HIV-1. Intr AIDS Conf Abstract # MCP 55, 1994.
Smith BJ, et al. Does beclomethasone dipropionate suppress dehydroepiandrosterotie sulphate in postmenopausah women? Aust AZ J Med 1994:24:396-401
Standish LJ, Ruhland JF, DiDomenico B, Gmeiner K. HIV/AIDS: Naturopathic Medical Principles and Practice. Bastyr University AIDS Research Center, 1997.
Szathmari M, et al. Dehydroepiandrosterone sulphate and bone mineral density. Osteoporosis Int 1994:4:84-88.
Taelman P, Kaufman JM, Janssens X, Vermeulen A. Persistence of increased bone resorption and possible role of dehydroepiandrosterone as a bone metabolism determinant in osteoporotic women in late post-menopause. Maturitas 1989:11:65-73.
Tagliaferro AR, et al. Enhancement of pancreatic carcinogenesis by dehydroepiandrosterone. Adv Exp Med Biol 1992:322:119-129.
Usiskin KS, Butterworth S, Clore JN, et al. Lack of effect of dehydroepiandrosterone in obese men. Int J Obes 1990;14:457-463.
Abstract: Six obese men were studied at baseline, after 28 days of placebo administration, and again after 28 days of DHEA (1600 mg/day) administration to assess the effects of dehydroepiandrosterone (DHEA) on weight and body fat mass in young obese men. Body fat mass was assessed on each occasion by three separate methods: hydrostatic weighing, impedance plethysmography, and skinfold measurements at four body sites. Waist-to-hip ratios were recorded. In addition, tissue sensitivity to insulin was determined using the modified minimal model technique, and serum lipids were assayed. Serum DHEA-Sulfate levels rose from 7.4 +/- 1.7 mumol/l at baseline to 39.8 +/- 11.9 mumol/l after DHEA administration (P less than 0.05). Although body fat mass was reduced in two of the six men following DHEA administration, for the group as a whole neither total body weight, body fat mass, or waist-to-hip ratio changed significantly during the study. No change in either tissue insulin sensitivity or serum lipids was observed. These observations suggest that, at a daily dose of 13.4-19.7 mg/kg, short-term DHEA administration does not affect the total weight, body fat mass, fat distribution, insulin sensitivity, or lipid status of obese young men.
Van Vollenhoven RF, Engleman EG, McGuire JL. An open study of dehydroepiandrosterone in systemic lupus erythematosus. Arthritis Rheum 1994;37:1305-1310.
Abstract: Ten female patients with mild to moderate SLE and various disease manifestations were given DHEA (200 mg/day orally) for 3-6 months. The patients were given other medications as clinically indicated, and followed with respect to overall disease activity and specific outcome parameters. After 3-6 months of DHEA treatment, indices for overall SLE activity including the SLEDAI (SLE Disease Activity Index) score and physicians overall assessment were improved, and corticosteroid requirements were decreased. Of 3 patients with significant proteinuria, 2 showed marked and 1 modest reductions in protein excretion. DHEA was well tolerated, the only frequently noted side effect being mild acneiform dermatitis. Study concluded that DHEA shows promise as a new therapeutic agent for the treatment of mild to moderate SLE. Further studies of DHEA in the treatment of SLE are warranted.
Van Vollenhoven RF, McGuire JL. Studies of dehydroepiandrosterone (DHEA) as a therapeutic agent in systemic lupus erythematosus. Ann Med Interne (Paris) 1996;147(4):290-6.
Abstract: Several lines of investigation led to the consideration of dehydroepiandrosterone (DHEA) as a candidate for hormonal therapy in systemic lupus erythematosus, including DHEA deficiency in patients with SLE, the effects of sex steroids on SLE, the immunomodulatory effects of DHEA, and the results of DHEA in animal models of SLE. Uncontrolled observations in 50 patients suggested that DHEA has overall benefits for lupus activity, alleviating specific lupus symptoms as well the systemic manifestations of lupus, with incremental benefits over 3 to 12 months of treatment. DHEA, which was very well tolerated and safe, appeared to decrease the number of lupus flares and to have a steroid sparing effect. These results were confirmed in a small placebo-controlled trial, although the results were of borderline statistical significance. Currently, a number of additional trials with DHEA are underway, and it is anticipated that DHEA will find its place as a useful agent in the treatment of SLE.
Watson RR, Huls A, Araghinikuam M, Chung S. Dehydroepiandrosterone and diseases of aging. Drugs Aging 1996 Oct;9(4):274-91.
Abstract: Dehydroepiandrosterone (DHEA; prasterone) is a major adrenal hormone with no well accepted function. In both animals and humans, low DHEA levels occur with the development of a number of the problems of aging: immunosenesence, increased mortality, increased incidence of several cancers, loss of sleep, decreased feelings of well-being, osteoporosis and atherosclerosis. DHEA replacement in aged mice significantly normalized immunosenescence, suggesting that this hormone plays a key role in aging and immune regulation in mice. Similarly, osteoclasts and lymphoid cells were stimulated by DHEA replacement, an effect that may delay osteoporosis. Recent studies do not support the original suggestion that low serum DHEA levels are associated with Alzheimer's disease and other forms of cognitive dysfunction in the elderly. As DHEA modulates energy metabolism, low levels should affect lipogenesis and gluconeogenesis, increasing the risk of diabetes mellitus and heart disease. Most of the effects of DHEA replacement have been extrapolated from epidemiological or animal model studies, and need to be tested in human trials. Studies that have been conducted in humans show essentially no toxicity of DHEA treatment at dosages that restore serum levels, with evidence of normalization in some aging physiological systems. Thus, DHEA deficiency may expedite the development of some diseases that are common in the elderly.
Weeks C, Lardy H, Henwood S. Preclinical Toxicology Evaluation of 3-Acetyl-7-oxo-dehydroepiandrosterone (7-Keto DHEA). FASEB Jrnl, Abstracts Part II, 4428 (1998).
Abstract: The objective of these studies is to evaluate the toxicological profile of 7-Keto DHEA using Salmonella and E. coli/mammalian microsome reverse mutation assays, plus acute oral dose rat and subchronic oral dose monkey studies. For mutagenicity assays, concentrations were 0.1 to 5.0 mg per plate with or without S-9 mix in S. typhimurium. strains TA98, 100, 1535, and 1537 and E. coli WP2uvrA. In the rat study, five groups of rats (five/sex/group) were given 0, 250, 500, 1,000 or 2,000 mg/kg in a single oral dose; animals were sacrificed on day 15 and necropsied. Rhesus monkeys (two/sex) were given oral doses of 250, 500 and 1,000 mg/kg on days 1, 3, 5 respectively and 1,000 mg/kg on days 7 through 11; animals were necropsied on day 12. No increase in the number of revertants per plate in any tester strain ± S-9 was observed. In rats, the single oral no observable adverse effect dose was greater than 2,000 mg/kg. Oral administration of 7-Keto DHEA to monkeys demonstrated no adverse clinical or anatomical pathology results. 7-Keto DHEA is now in clinical trials to further establish safety. (Abstract courtesy of PhytoPharmica, Inc.)
Weinstein RE, Lobocki CA, Gravett S, et al. Decreased adrenal sex steroid in the absence of glucocorticoid suppression in postmenopausal asthmatic women. J Allerg Clin Immol 1996;97:1-8.
Werbach MR. Foundations of Nutritional Medicine. Tarzana, CA: Third Line Press, 1997. (Review).
Wisniewski TL, Hilton CW, Morse EV, Svec F. The relationship of serum DHEA-S and cortisol levels to measures of immune function in human immunodeficiency virus-related illness. Am J Med Sci 1993:305:79-83.
Wolkowitz OM, Reus VI, Roberts E, et al. Antidepressant and cognition-enhancing effects of DHEA in major depression. Ann NY Acad Sci 1995;774:337-339.
Yen SS, Morales AJ, Khorram O. Replacement of DHEA in aging men and women. Potential remedial effects. Ann N Y Acad Sci 1995;774:128-142.
Abstract: DHEA in appropriate replacement doses appears to have remedial effects with respect to its ability to induce an anabolic growth factor, increase muscle strength and lean body mass, activate immune function, and enhance quality of life in aging men and women, with no significant adverse effects. Further studies are needed to confirm and extend our current results, particularly the gender differences.
Yen TT, Allan JA, Pearson DV, Acton JM, Greenberg MM. Prevention of obesity in A vy/a mice by dehydroepiandrosterone. Lipids 1977:12:409-413.
Zumoff B, et al. Abnormal 24-hr mean plasma concentrations of dehydroisoandrosterone and dehydroandrosterone sulfate in women with primary operable breast cancer. Canc Res 1981;41:3360-3363.