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携带CDw78表位的MHC II类分子亚群的性质。

The nature of the subset of MHC class II molecules carrying the CDw78 epitopes.

作者信息

Drbal K, Angelisová P, Rasmussen A M, Hilgert I, Funderud S, Horejsí V

机构信息

Institute of Molecular Genetics, Academy of Sciences of the Czech Republic, Prague.

出版信息

Int Immunol. 1999 Apr;11(4):491-8. doi: 10.1093/intimm/11.4.491.

DOI:10.1093/intimm/11.4.491
PMID:10323201
Abstract

A CDw78 mAb FN1 was shown to recognize DP and/or DR molecules under the conditions of Western blotting. DP molecules were specifically retarded on a column of the FN1 immunosorbent; binding of FITC-labeled FN1 to B cell lines was completely blocked by excess of mAb to DR/DP beta chains, partially by several mAb to DP and weakly by some mAb to DR. The binding of two other CDw78 mAb, FN4 and MR11, to the B cell surface was most strongly inhibited by excess of different mAb to DR. Kinetics of stable binding of the CDw78 mAb indicated that their monovalent binding is of low affinity and that the stable binding to the surface is due to bivalent binding to two spatially close MHC class II molecules. FN1-based immunosorbent effectively immunoisolated complexes of MHC class II proteins with several tetraspanin molecules from a mild detergent lysate of a B cell line. It is concluded that FN1 and most likely also the other two CDw78 mAb recognize with low affinity determinants on MHC class II molecules (DP or DR) and preferentially bind in a stable fashion to dimerized or aggregated MHC class II molecules. Such dimers or aggregates may either exist as preformed on the cell surface or may be gradually formed and stabilized by bivalent interaction with mAb. These structures may be related to the previously described 'superdimers' of MHC class II and/or 'MHC-tetraspanin complexes'. CDw78 mAb may be valuable tools targeting such aggregated fraction of MHC class II molecules which can exhibit important signaling and antigen-presenting properties.

摘要

在蛋白质印迹条件下,一种CDw78单克隆抗体FN1被证明可识别DP和/或DR分子。DP分子在FN1免疫吸附柱上被特异性阻滞;异硫氰酸荧光素标记的FN1与B细胞系的结合被过量的抗DR/DPβ链单克隆抗体完全阻断,被几种抗DP单克隆抗体部分阻断,被一些抗DR单克隆抗体微弱阻断。另外两种CDw78单克隆抗体FN4和MR11与B细胞表面的结合被过量的不同抗DR单克隆抗体最强烈地抑制。CDw78单克隆抗体稳定结合的动力学表明,它们的单价结合亲和力低,而与表面的稳定结合是由于与两个空间上接近的MHC II类分子的二价结合。基于FN1的免疫吸附剂有效地从B细胞系的温和去污剂裂解物中免疫分离了MHC II类蛋白与几种四跨膜蛋白分子的复合物。得出的结论是,FN1以及很可能另外两种CDw78单克隆抗体以低亲和力识别MHC II类分子(DP或DR)上的决定簇,并优先以稳定方式结合二聚化或聚集的MHC II类分子。这种二聚体或聚集体可能作为预先形成的结构存在于细胞表面,或者可能通过与单克隆抗体的二价相互作用逐渐形成并稳定。这些结构可能与先前描述的MHC II类“超级二聚体”和/或“MHC-四跨膜蛋白复合物”有关。CDw78单克隆抗体可能是靶向MHC II类分子这种聚集部分的有价值工具,该部分可表现出重要的信号传导和抗原呈递特性。

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