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一种细胞毒性人杂交瘤单克隆抗体(TrJ6),可识别由HLA-DQ4和-DQ5表达的一个表位。

A cytotoxic human hybridoma monoclonal antibody (TrJ6) defining an epitope expressed by HLA-DQ4 and -DQ5.

作者信息

Ge J, Hannestad K

机构信息

Department of Immunology, University of Tromsø School of Medicine, Norway.

出版信息

Hum Immunol. 1994 Feb;39(2):106-12. doi: 10.1016/0198-8859(94)90108-2.

Abstract

We have generated a cytotoxic human hybridoma monoclonal IgM lambda antibody, designated TrJ6, that is specific for a new epitope shared by HLA-DQ4 and -DQ5. TrJ6 strongly killed all ten DQ4-bearing cells and weakly killed all four DQ5-bearing cell lines. In contrast, none of the 36 cell lines lacking DQ4 and DQ5 antigens was recognized by TrJ6. This was confirmed by fluorescence cytometry. The specific binding of TrJ6 to a DQ4-bearing line was efficiently blocked by IIB3 (murine anti-DQ8+9+4+5+6 mAb) and TrG6 (human IgG mAb against DQ4+5+6), confirming that TrJ6 is specific for a polymorphic DQ epitope. TrJ6 can be used to distinguish DQ5+ from DQ6+ B-lymphoblastoid cells. DQ4 beta and DQ5 beta chains share one unique residue (Ser-74) and one relatively unique residue (Val-75), which may therefore need to be coexpressed in order for the TrJ6 epitope to be formed. Alternatively, Ser-74 alone contributes critically to the allospecificity of this epitope. In addition, one or more of three residues unique for DQ4 (Leu-56, Glu-70, and Asp-71 on the DQ4 beta chain) could also contribute to the TrJ6 epitope because TrJ6 reacted stronger with DQ4- than with DQ5-bearing cell lines.

摘要

我们制备了一种具有细胞毒性的人杂交瘤单克隆IgM λ抗体,命名为TrJ6,它对HLA-DQ4和-DQ5共有的一个新表位具有特异性。TrJ6能强烈杀伤所有10种携带DQ4的细胞,并微弱杀伤所有4种携带DQ5的细胞系。相比之下,36种缺乏DQ4和DQ5抗原的细胞系均未被TrJ6识别。这一点通过荧光细胞术得到了证实。TrJ6与携带DQ4的细胞系的特异性结合能被IIB3(鼠抗-DQ8+9+4+5+6单克隆抗体)和TrG6(抗DQ4+5+6的人IgG单克隆抗体)有效阻断,这证实了TrJ6对多态性DQ表位具有特异性。TrJ6可用于区分DQ5+和DQ6+ B淋巴母细胞。DQ4 β链和DQ5 β链共有一个独特残基(Ser-74)和一个相对独特的残基(Val-75),因此可能需要共表达才能形成TrJ6表位。或者,仅Ser-74对该表位的同种特异性起关键作用。此外,DQ4特有的三个残基(DQ4 β链上的Leu-56、Glu-70和Asp-71)中的一个或多个也可能对TrJ6表位有贡献,因为TrJ6与携带DQ4的细胞系的反应比与携带DQ5的细胞系更强。

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