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首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >Fc receptors for IgG (Fc gamma Rs) on human monocytes and macrophages are not infectivity receptors for human immunodeficiency virus type 1 (HIV-1): studies using bispecific antibodies to target HIV-1 to various myeloid cell surface molecules including the Fc gamma R.
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Fc receptors for IgG (Fc gamma Rs) on human monocytes and macrophages are not infectivity receptors for human immunodeficiency virus type 1 (HIV-1): studies using bispecific antibodies to target HIV-1 to various myeloid cell surface molecules including the Fc gamma R.

机译:人类单核细胞和巨噬细胞上IgG的Fc受体(FcγRs)不是人类免疫缺陷病毒1型(HIV-1)的感染性受体:使用双特异性抗体将HIV-1靶向各种髓样细胞表面分子(包括Fcγ)的研究R.

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Fc gamma Rs (Fc gamma RI, Fc gamma RII, and Fc gamma RIII) are highly expressed on human mononuclear phagocytes and function in the clearance of immune complexes and opsonized pathogens. We have examined the role of Fc gamma R in mediating antibody-dependent clearance of HIV-1 by human monocytes and monocyte-derived macrophages by using bispecific antibodies (BsAbs) to independently target the virus to Fc gamma RI, Fc gamma RII, or Fc gamma RIII. Virus production was markedly reduced in monocytes cultured with strain HIV-1IIIB opsonized with BsAbs that target the virus to either Fc gamma RI or Fc gamma RII compared to monocytes cultured with virus in the absence of BsAbs or in the presence of BsAbs that target the virus to non-Fc gamma R surface antigens (CD33 and HLA-A,B,C). These results were confirmed using the monotropic isolate HIV-1JRFL. Interaction of HIV-1JRFL with Fc gamma RI or Fc gamma RII on human monocytes and Fc gamma RI, Fc gamma RII, or Fc gamma RIII on monocyte-derived macrophages resulted in markedly reduced levels of virus production in these cultures. Moreover, HIV-1 infection of monocytes and monocyte-derived macrophages was completely blocked by anti-CD4 monoclonal antibodies, indicating that interaction with CD4 is required for infectivity even under conditions of antibody-mediated binding of HIV-1 to Fc gamma R. Thus, we propose that highly opsonized HIV-1 initiates high-affinity multivalent interactions with Fc gamma R that trigger endocytosis and intracellular degradation of the antibody-virus complex. At lower levels of antibody opsonization, there are two few interactions with Fc gamma R to initiate endocytosis and intracellular degradation of the antibody-virus complex, but there are enough interactions to stabilize the virus at the cell surface, allowing antibody-dependent enhancement of HIV-1 infection through high-affinity CD4 interactions. However, our results suggest that interaction of highly opsonized HIV-1 with Fc gamma Rs through BsAbs may reduce viral infectivity through Fc gamma R-mediated cytotoxic mechanisms and, therefore, that BsAbs offer promise as therapeutic reagents in HIV-1 infections.
机译:FcγRs(FcγRI,FcγRII和FcγRIII)在人单核吞噬细胞上高度表达,并在清除免疫复合物和调理病原体中起作用。我们已经通过使用双特异性抗体(BsAbs)将病毒独立地靶向FcγRI,FcγRII或Fc,研究了FcγR在人单核细胞和单核细胞衍生的巨噬细胞介导的HIV-1抗体依赖性清除中的作用。 γRIII。与在不存在BsAbs或存在针对该病毒的BsAbs的情况下用病毒培养的单核细胞相比,在用BsAb调理过的BsAb毒株培养的单核细胞中,病毒的产生显着减少非FcγR表面抗原(CD33和HLA-A,B,C)。使用单向分离株HIV-1JRFL证实了这些结果。 HIV-1JRFL与人单核细胞上的FcγRI或FcγRII以及在单核细胞衍生的巨噬细胞上的FcγRI,FcγRII或FcγRIII相互作用导致这些培养物中病毒产生的水平显着降低。此外,单核细胞和单核细胞衍生的巨噬细胞的HIV-1感染被抗CD4单克隆抗体完全阻断,这表明即使在抗体介导的HIV-1与FcγR结合的条件下,感染性也需要与CD4相互作用。 ,我们建议高度调理的HIV-1与FcγR引发高亲和力多价相互作用,从而触发抗体-病毒复合物的内吞作用和细胞内降解。在较低的抗体调理作用下,与FcγR的相互作用很少,以引发抗体-病毒复合物的内吞作用和细胞内降解,但是有足够的相互作用可以使病毒稳定在细胞表面,从而使抗体依赖性的HIV增强作用-1通过高亲和力CD4相互作用感染。但是,我们的结果表明,高度调理的HIV-1通过BsAb与FcγR的相互作用可能会通过FcγR介导的细胞毒性机制降低病毒感染性,因此BsAb有望作为HIV-1感染的治疗剂。

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