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人类B细胞CD20受体的分子克隆预测其为一种具有多个跨膜结构域的疏水蛋白。

Molecular cloning of the human B cell CD20 receptor predicts a hydrophobic protein with multiple transmembrane domains.

作者信息

Einfeld D A, Brown J P, Valentine M A, Clark E A, Ledbetter J A

机构信息

ONCOGEN, Seattle, WA 98121.

出版信息

EMBO J. 1988 Mar;7(3):711-7. doi: 10.1002/j.1460-2075.1988.tb02867.x.

Abstract

CD20 is an antigen expressed on normal and malignant human B cells that is thought to function as a receptor during B cell activation. Here we report the isolation of a CD20-specific cDNA clone from a lambda gt11 library using a polyclonal antiserum raised against purified CD20 antigen. Additional cDNA clones were then isolated from a lambda gt10 library. Alignment of the sequences of overlapping lambda clones reveal a single consensus sequence except for a divergence that preceded the first methionine within the open reading frame. Normal B cells and B cell lines contain a prominent 2.6 kb mRNA and a lower level of a 3.3 kb mRNA. An oligonucleotide derived from one of the divergent sequences hybridized to the 3.3 kb mRNA only, indicating that the two mRNA species are derived from an alternative splicing mechanism. The predicted amino acid sequence of CD20 reveals three major hydrophobic regions of approximately 53, 25 and 20 amino acids. CD20 lacks an NH2-terminal signal peptide and contains a highly charged COOH-terminal domain. Although CD20 is immunoprecipitated as a doublet of 33 and 35 kd proteins from B cells, in vitro translation of CD20 cDNA produced a single 33 kd protein that was specifically immunoprecipitated with monoclonal CD20 antibodies. CD20 was strongly phosphorylated on resting B cells after CDw40 stimulation, suggesting that CD20 may be functionally regulated by a protein kinase(s).

摘要

CD20是一种在正常和恶性人B细胞上表达的抗原,被认为在B细胞激活过程中起受体作用。在此,我们报告使用针对纯化的CD20抗原产生的多克隆抗血清,从λgt11文库中分离出一个CD20特异性cDNA克隆。随后从λgt10文库中分离出其他cDNA克隆。重叠λ克隆序列的比对揭示了一个单一的共有序列,但开放阅读框内第一个甲硫氨酸之前存在一处差异。正常B细胞和B细胞系含有一条突出的2.6 kb mRNA以及一条水平较低的3.3 kb mRNA。源自其中一个差异序列的寡核苷酸仅与3.3 kb mRNA杂交,表明这两种mRNA是由可变剪接机制产生的。CD20的预测氨基酸序列显示有三个主要的疏水区域,分别约含53、25和20个氨基酸。CD20缺乏NH2末端信号肽,且含有一个高度带电的COOH末端结构域。尽管从B细胞中免疫沉淀出的CD20是33 kd和35 kd蛋白质的双峰,但CD20 cDNA的体外翻译产生了一个单一的33 kd蛋白质,该蛋白质可被单克隆CD20抗体特异性免疫沉淀。在CDw40刺激后,静息B细胞上的CD20被强烈磷酸化,这表明CD20可能受一种或多种蛋白激酶的功能调控。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/69f1/454379/37ced037aef2/emboj00140-0137-a.jpg

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