NEW TREATMENTS FOR AIDS AND AIDS-RELATED INFECTIONS
艾滋病和艾滋病相关感染的新疗法
基本信息
- 批准号:3546952
- 负责人:
- 金额:$ 119.43万
- 依托单位:
- 依托单位国家:美国
- 项目类别:
- 财政年份:1987
- 资助国家:美国
- 起止时间:1987-09-30 至 1992-08-31
- 项目状态:已结题
- 来源:
- 关键词:
项目摘要
The objective of this proposal is to establish an AIDS Clinical
Study Group (CSG) to unify and maximize the effectiveness of the
future AIDS clinical research carried out at The New York
Hospital-Cornell Medical Center. The emphasis in this
application is on new and improved treatments for AIDS and
AIDS-related opportunistic infections (OI), and our principal focus
will be to determine if immune reconstitution with gamma
interferon (IFN-gamma) can act synergistically with anti-HIV
chemotherapy (azidiothymidine (AZT), ribavirin) to prevent (a)
new OI in AIDS patients or (b) progression to AIDS and OI in
immunodeficient ARC patients. Our studies have demonstrated
that IFN-gamma is a key T4+ cell-derived lymphokine critical for
successful activation of mononuclear phagocytes to exert
enhanced antimicrobial activity. In addition, we have established
that T4+ cells from AIDS patients with OI fail to secrete antigen-
induced IFN-gamma, a state which renders them vulnerable to and
unable to control opportunistic pathogens. In parallel, we have
also demonstrated, however, that the AIDS peripheral blood
monocyte, monocyte-derived macrophage, and tissue (alveolar)
macrophages is fully responsive to activation by exogenous IFN-
gamma in vitro, and in a recent in vivo trial, showed that AIDS
monocytes respond to intravenous recombinant (Tau) IFN-gamma
with clear evidence of activation and enhanced antimicrobial
capacity. In an on-going prospective study of patients at high risk
for AIDS conducted in our well-established Immune Deficiency
Research Unit (IDRU), we have also reported that the capacity to
secrete antigen-stimulated IFN-gamma is an accurate predictor
of the risk of progressing to AIDS and developing an OI.
We now propose to extend our work using several specific aims:
(1) Continue and expand our IDRU longitudinal study of at-risk
patients. (2) Determine in two trials, if combination
immunotherapy (IFN-gamma) plus antiviral therapy (AZT) is
superior to AZT alone in the treatment of AIDS patients with a
prior OI in (a) decreasing the occurrence of new OI and (b)
permitting a reduction in AZT dose to diminish toxicity while
preserving clinical efficacy. (3) Determine if rIFN-gamma plus
ribavirin is superior to ribavirin alone in preventing the
progression of ARC to AIDS. And (4) Determine the efficacy of
new treatments for OI: (a) spiramycin in cryptosporidiosis, (b)
Fansidar prophylaxis in reactivated toxoplasmosis, and (c)
fluconazole in cryptococcosis. The morbidity and mortality of
AIDS-related OI clearly rationale the need for new experimental
approaches.
这项提议的目的是建立一个艾滋病诊所
项目成果
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HENRY W. MURRAY其他文献
HENRY W. MURRAY的其他文献
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{{ truncateString('HENRY W. MURRAY', 18)}}的其他基金
NEW TREATMENTS FOR AIDS AND AIDS-RELATED INFECTIONS
艾滋病和艾滋病相关感染的新疗法
- 批准号:
3546955 - 财政年份:1987
- 资助金额:
$ 119.43万 - 项目类别:
NEW TREATMENTS FOR AIDS AND AIDS-RELATED INFECTIONS
艾滋病和艾滋病相关感染的新疗法
- 批准号:
3546957 - 财政年份:1987
- 资助金额:
$ 119.43万 - 项目类别:
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