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对正常人类受试者进行体内重组人干扰素-γ治疗后,吞噬细胞FcγRI表达增加,且Fcγ受体介导的吞噬作用得到改善。

Increased phagocyte Fc gammaRI expression and improved Fc gamma-receptor-mediated phagocytosis after in vivo recombinant human interferon-gamma treatment of normal human subjects.

作者信息

Schiff D E, Rae J, Martin T R, Davis B H, Curnutte J T

机构信息

Department of Molecular and Experimental Medicine, The Scripps Research Institute, La Jolla, CA 92037, USA.

出版信息

Blood. 1997 Oct 15;90(8):3187-94.

PMID:9376602
Abstract

Recombinant human interferon-gamma (rhIFN-gamma) decreases the frequency of serious infections in patients with chronic granulomatous disease (CGD) through an unknown mechanism. To test the hypothesis that it exerts a beneficial effect by enhancing clearance of microbes from the bloodstream and tissues, normal human subjects were treated in vivo with rhIFN-gamma. Phagocyte opsonic receptor expression, serum opsonin levels, and phagocytosis of bacteria were then measured. A 4.7-fold increase in neutrophil expression of the high-affinity Fc gamma-receptor (Fc gammaRI) was observed that peaked 48 hours after the initiation of rhIFN-gamma treatment (P < .05). Monocyte expression of Fc gammaRI, Fc gammaRII, Fc gammaRIII, CD11a, CD11b, CD18, and HLA-DR also significantly increased with peak expression at 48 hours. Phagocytosis by neutrophils of killed Staphylococcus aureus opsonized with heat-inactivated pooled human serum significantly improved after rhIFN-gamma treatment (P < .05) and correlated with Fc gammaRI expression by neutrophils (r = .8, P < .001). This increase in ingestion could be inhibited by anti-Fc gammaRI monoclonal antibodies. Levels of the serum opsonin lipopolysaccharide-binding protein also significantly increased after in vivo rhIFN-gamma (P < .05). These results suggest that the protective effect of rhIFN-gamma in patients with CGD may involve improved microbial clearance. Moreover, improved phagocyte trafficking may occur secondary to increased expression of monocyte beta2-integrins. Because these IFN-gamma-related improvements in host defense were seen in normal hosts, rhIFN-gamma may have broader applications in the treatment of various disorders of immunity in addition to its demonstrated efficacy in CGD.

摘要

重组人干扰素-γ(rhIFN-γ)可降低慢性肉芽肿病(CGD)患者严重感染的发生率,但其机制尚不清楚。为了验证其通过增强从血液和组织中清除微生物而发挥有益作用的假说,对正常人体进行了rhIFN-γ体内治疗。然后测量吞噬细胞调理素受体表达、血清调理素水平和细菌吞噬作用。观察到高亲和力Fcγ受体(FcγRI)的中性粒细胞表达增加了4.7倍,在rhIFN-γ治疗开始后48小时达到峰值(P<0.05)。FcγRI、FcγRII、FcγRIII、CD11a、CD11b、CD18和HLA-DR的单核细胞表达也显著增加,在48小时达到峰值表达。用热灭活的混合人血清调理的死金黄色葡萄球菌经rhIFN-γ治疗后,中性粒细胞的吞噬作用显著改善(P<0.05),并与中性粒细胞的FcγRI表达相关(r = 0.8,P<0.001)。这种摄取增加可被抗FcγRI单克隆抗体抑制。体内给予rhIFN-γ后,血清调理素脂多糖结合蛋白水平也显著增加(P<0.05)。这些结果表明,rhIFN-γ对CGD患者的保护作用可能涉及改善微生物清除。此外,单核细胞β2整合素表达增加可能继发吞噬细胞运输改善。由于在正常宿主中观察到了这些与IFN-γ相关的宿主防御改善,除了其在CGD中已证实的疗效外,rhIFN-γ在治疗各种免疫紊乱方面可能有更广泛的应用。

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