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Dive into the research topics where Michael A. Adams is active.

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Featured researches published by Michael A. Adams.


The Journal of Urology | 2000

EFFECTS OF AN ENVIRONMENTAL ANTI-ANDROGEN ON ERECTILE FUNCTION IN AN ANIMAL PENILE ERECTION MODEL

Susan E. Brien; Jeremy P.W. Heaton; William J. Racz; Michael A. Adams

PURPOSEnErectile function is testosterone dependent. For example, interference with either the levels or receptor binding of this steroid hormone may induce erectile dysfunction. Several environmental contaminants can interfere with the actions of endogenous hormones and have been termed endocrine disrupters. p,p-DDE, a prominent and persistent metabolite of the insecticide DDT, has been shown to be an androgen receptor antagonist. The objective was to determine whether endocrine disrupters, as exemplified by p,p-DDE, are factors in the etiology of erectile dysfunction.nnnMATERIALS AND METHODSnUsing the established rat model of apomorphine-induced (80 microg./kg, s.c.) erections we assessed the dose-response effects of p,p-DDE in comparison to the known androgen receptor antagonist flutamide in acute (0.5 to 12 hours) and short-term (up to 8 weeks) experiments in both intact (Study 1) and castrated (Study 2) rats. As a follow up (Study 3), castrated rats treated with p,p-DDE were given increasing doses of testosterone (0.48 to 2.4 mg./kg., i.p.), eight weeks after p,p-DDE administration, to assess reversibility of p,p-DDE effect.nnnRESULTSnA single dose of flutamide (50 mg./kg., i.p.) was found to significantly decrease apomorphine-induced erections to less than 50% over 12 hours following flutamide administration with recovery of erectile response within 48 hours. In comparison, a single dose of p,p-DDE (500 mg./kg., i.p.) decreased apomorphine-induced erections for at least two weeks (1.15+/-0.3 versus 2.5+/-1.1). Castration significantly decreased apomorphine-induced erections to approximately 0.5 erections/30 minutes. Flutamide (50 mg./kg.; i.p.) or p,p-DDE (50 mg./kg.; i.p.) did not further suppress the apomorphine erections in castrated rats. Testosterone supplementation (480 microg./kg; s.c.) in vehicle treated castrated rats recovered erectile response to pre-castrated levels, whereas p,p-DDE treated castrated rats required 4 times the dose of testosterone (2 mg./kg.; s.c.) given to vehicle treated rats to recover erections.nnnCONCLUSIONSnThe endocrine disrupter p,p-DDE can markedly interfere with erectile function and demonstrates persistence after a single dose. This supports our novel concept that environmental hormones may cause erectile dysfunction.


Archive | 2001

Formulations and methods of using nitric oxide mimetics against a malignant cell phenotype

Michael A. Adams; Charles H. Graham; Jeremy P. W. Heaton; Lynne-Marie Postovit


Archive | 2001

Methods and compositions for improving sleep

C. Bruce Ackman; Michael A. Adams; Jeremy P. W. Heaton; Jordan D. Ratz


Archive | 1997

Combination therapy for treatment of erectile dysfunction

Michael A. Adams; Jeremy P. W. Heaton; Donald H. Maurice


Archive | 2002

Methods for remodeling neuronal and cardiovascular pathways

Michael A. Adams; Jeremy P. W. Heaton


Archive | 1998

Microdose therapy of vascular conditions by no donors

Michael A. Adams; Jeremy P. W. Heaton; James D. Banting


Archive | 2003

Method for ameliorating male erectile dysfunction

Ragab El-Rashidy; Jeremy P. W. Heaton; Alvaro Morales; Michael A. Adams


Archive | 2005

Use of nitric oxide mimetics in cancer treatment

Michael A. Adams; Charles H. Graham; Jeremy P. W. Heaton; Lynne-Marie Postovit


Archive | 1995

Sublinguale Dosierungsformen enthaltend Apomorphinzur Verwendung bei der Behandlung von erektiler D ysfunktion

Ragab El-Rashidy; Jeremy P. W. Heaton; Alvaro Morales; Michael A. Adams


Archive | 2001

Formulations et methodes d'utilisation d'agents mimetiques de l'oxyde nitrique contre un phenotype cellulaire malin

Michael A. Adams; Charles H. Graham; Jeremy P. W. Heaton; Lynne-Marie Postovit

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Alvaro Morales

University of North Carolina at Chapel Hill

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Susan E. Brien

Kingston General Hospital

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William J. Racz

Kingston General Hospital

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