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皮内注射重组干扰素-γ对瘤型麻风患者的局部和全身影响。

Local and systemic effects of intradermal recombinant interferon-gamma in patients with lepromatous leprosy.

作者信息

Nathan C F, Kaplan G, Levis W R, Nusrat A, Witmer M D, Sherwin S A, Job C K, Horowitz C R, Steinman R M, Cohn Z A

出版信息

N Engl J Med. 1986 Jul 3;315(1):6-15. doi: 10.1056/NEJM198607033150102.

Abstract

Evidence that interferon-gamma may be a physiologic macrophage-activating factor, and that macrophage activation may be defective in lepromatous leprosy, led us to test the effects of intradermal injection of low doses of recombinant interferon-gamma in six patients with this disease. Interferon-gamma, 1 or 10 micrograms, was administered daily by jet gun for three days into a single cutaneous lesion. A biopsy specimen was taken from the injection site on the sixth study day and compared with specimens obtained previously from a site where no injection had been made or where excipient alone had been injected in the same way as the interferon. Interferon-gamma elicited local effects similar to certain features of delayed-type hypersensitivity reactions or tuberculoid leprosy, including induration, T-cell and monocyte infiltration, keratinocyte proliferation, diminution of epidermal Langerhans cells, and dermal and epidermal cell HLA-DR (Ia) antigen expression. At some of the sites of interferon-gamma injection, there was also an apparent decrease in acid-fast bacilli. Before treatment, monocytes from patients with lepromatous leprosy released 48 percent as much hydrogen peroxide as did monocytes from controls in response to phorbol myristate acetate, and 36 percent as much as those from controls in response to Mycobacterium leprae. When recombinant interferon-gamma was injected, these responses became normal. No toxic effects were observed. These observations suggest that interferon-gamma can mediate certain manifestations of delayed-type hypersensitivity or cell-mediated immunity in vivo, and that recombinant interferon-gamma should be tested for possible therapeutic effects in certain nonviral infectious diseases.

摘要

有证据表明,γ干扰素可能是一种生理性巨噬细胞激活因子,且巨噬细胞激活在瘤型麻风病中可能存在缺陷,这促使我们对6例该疾病患者进行低剂量重组γ干扰素皮内注射效果的测试。将1微克或10微克的γ干扰素通过喷枪每日注射到单个皮肤损害处,持续三天。在研究的第6天从注射部位取活检标本,并与之前从未注射或仅注射赋形剂(注射方式与γ干扰素相同)的部位所取标本进行比较。γ干扰素引发了类似于迟发型超敏反应或结核样型麻风病某些特征的局部效应,包括硬结、T细胞和单核细胞浸润、角质形成细胞增殖、表皮朗格汉斯细胞减少以及真皮和表皮细胞HLA - DR(Ia)抗原表达。在一些γ干扰素注射部位,抗酸杆菌也明显减少。治疗前,瘤型麻风病患者的单核细胞在佛波酯肉豆蔻酸酯刺激下释放的过氧化氢量仅为对照组单核细胞的48%,在麻风杆菌刺激下释放的过氧化氢量为对照组的36%。注射重组γ干扰素后,这些反应恢复正常。未观察到毒性作用。这些观察结果表明,γ干扰素可在体内介导迟发型超敏反应或细胞介导免疫的某些表现,并且重组γ干扰素应在某些非病毒性感染疾病中测试其可能的治疗效果。

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