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几种新型抗P-糖蛋白单克隆抗体的表征与表位图谱分析

Characterization and epitope mapping of several new anti-P-glycoprotein monoclonal antibodies.

作者信息

Shapiro A B, Duthie M, Childs S, Okubo T, Ling V

机构信息

Division of Molecular and Structural Biology, Ontario Cancer Institute/Princess Margaret Hospital, Toronto, Canada.

出版信息

Int J Cancer. 1996 Jul 17;67(2):256-63. doi: 10.1002/(SICI)1097-0215(19960717)67:2<256::AID-IJC17>3.0.CO;2-9.

Abstract

Monoclonal antibodies (MAbs) were raised against partially purified Class I P-glycoprotein from multidrug-resistant Chinese hamster ovary CHRB30 cells. Fifteen stable monoclonal hybridoma cell lines were established, and the secreted antibodies were classified into 8 groups on the basis of banding pattern on immunoblots of P-glycoprotein digested with cyanogen bromide or partially digested with proteases. One representative of each group was tested further for several activities. Six of the 8 recognized human P-glycoprotein in the multidrug-resistant SKVLBI cell line. None of the antibodies recognized P-glycoprotein in unfixed cells, suggesting that all recognize cytoplasmic epitopes or extracellular epitopes not accessible in native P-glycoprotein. All 8 antibodies were able to immunoprecipitate P-glycoprotein from non-denaturing detergent solution. The linear epitopes of the antibodies were mapped to 11-27 amino acids. Two of the antibodies had epitopes in the linker region, 3 in the N-terminal nucleotide binding domain, 2 in the C-terminal nucleotide binding domain and 1 in the predicted cytoplasmic loop between predicted transmembrane helices 8 and 9. These antibodies, with known epitopes, could have uses for P-glycoprotein detection, structure/function studies, purification and quantitation.

摘要

针对来自多药耐药中国仓鼠卵巢CHRB30细胞的部分纯化的I类P - 糖蛋白制备了单克隆抗体(MAb)。建立了15个稳定的单克隆杂交瘤细胞系,并根据用溴化氰消化或用蛋白酶部分消化的P - 糖蛋白免疫印迹上的条带模式将分泌的抗体分为8组。对每组中的一个代表性抗体进一步测试了几种活性。这8种抗体中有6种识别多药耐药SKVLBI细胞系中的人P - 糖蛋白。没有一种抗体能识别未固定细胞中的P - 糖蛋白,这表明所有抗体识别的是细胞质表位或天然P - 糖蛋白中无法接近的细胞外表位。所有8种抗体都能够从非变性去污剂溶液中免疫沉淀P - 糖蛋白。抗体的线性表位定位在11 - 27个氨基酸处。其中两种抗体的表位在连接区,3种在N端核苷酸结合结构域,2种在C端核苷酸结合结构域,1种在预测的跨膜螺旋8和9之间的预测细胞质环中。这些具有已知表位的抗体可用于P - 糖蛋白的检测、结构/功能研究、纯化和定量。

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