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人类FcεRIγ亚基与新型细胞表面多肽的关联。

Association of the human Fc epsilon RI gamma subunit with novel cell surface polypeptides.

作者信息

Schöneich J T, Wilkinson V L, Kado-Fong H, Presky D H, Kochan J P

机构信息

Department of Molecular/Cellular Biology and Biological Chemistry, Hoffmann-La Roche, Inc., Nutley, NJ 07110.

出版信息

J Immunol. 1992 Apr 1;148(7):2181-5.

PMID:1532003
Abstract

It has recently been demonstrated that the gamma-subunits of the high affinity Fc epsilon RI are required for the cell surface expression of not only the Fc epsilon RI alpha-subunit, but also for the low affinity Fc gamma RIIIA alpha (CD16). In addition, formation of heterodimeric complexes of the gamma-subunit with the zeta- and eta-chains of the TCR have also been reported. The exact role of the gamma-subunit in the function of these receptors is not known. To gain additional insight into the association of the gamma-subunit with these and other cell surface polypeptides, we have generated a mAb, 4D8, directed against the human Fc epsilon RI gamma-subunit. Using this antibody we have been able to demonstrate that Fc epsilon RI alpha and Fc gamma RIIIA alpha are associated with Fc epsilon RI gamma at the cell surface. Furthermore, we have identified the expression of Fc epsilon RI gamma in HL60 and U937 cells, which are negative for the TCR, Fc epsilon RI, and Fc gamma RIII. Analysis of these cells reveals the presence of novel Fc epsilon RI gamma-associated polypeptides. These results suggest that Fc epsilon RI gamma plays a common functional role in a number of different receptor complexes. The availability of the anti-gamma antibody 4D8 will help to define this role, and allow the characterization of cell surface polypeptides that are associated with the Fc epsilon RI gamma-subunit.

摘要

最近有研究表明,高亲和力FcεRI的γ亚基不仅是FcεRIα亚基细胞表面表达所必需的,也是低亲和力FcγRIIIAα(CD16)细胞表面表达所必需的。此外,也有报道称γ亚基与TCR的ζ链和η链形成异二聚体复合物。γ亚基在这些受体功能中的具体作用尚不清楚。为了进一步深入了解γ亚基与这些及其他细胞表面多肽的关联,我们制备了一种针对人FcεRIγ亚基的单克隆抗体4D8。利用该抗体,我们能够证明FcεRIα和FcγRIIIAα在细胞表面与FcεRIγ相关联。此外,我们还鉴定出HL60和U937细胞中FcεRIγ的表达,这两种细胞对TCR、FcεRI和FcγRIII呈阴性。对这些细胞的分析揭示了新型FcεRIγ相关多肽的存在。这些结果表明,FcεRIγ在许多不同的受体复合物中发挥着共同的功能作用。抗γ抗体4D8的可用性将有助于确定这一作用,并有助于鉴定与FcεRIγ亚基相关的细胞表面多肽。

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