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组装过程中的后期事件决定了分泌型IgM的聚合物结构和生物学活性。

Late events in assembly determine the polymeric structure and biological activity of secretory IgM.

作者信息

Brewer J W, Corley R B

机构信息

Department of Microbiology, Boston University School of Medicine, MA 02118, U.S.A.

出版信息

Mol Immunol. 1997 Mar;34(4):323-31. doi: 10.1016/s0161-5890(97)00029-1.

Abstract

IgM antibodies can be secreted in at least two functional polymeric forms that can be distinguished according to subunit composition. While IgM hexamers comprise six H2L2 monomeric subunits, pentamers contain an additional polypeptide, the J chain. In the presence of high abundance J chain protein, IgM pentamers are preferentially assembled at the expense of hexamers. To determine the mechanism by which J chain regulates the assembly process, we defined the point at which J chain is added to assembling polymers. We found no evidence for the presence of J chain in small IgM assembly intermediates of IgM, suggesting that it was not stably associated with these complexes. However, J chain was found associated with large polymeric IgM complexes exhibiting sedimentation properties of intracellular pentameric structures. These complexes were frequently not completely covalently assembled; however, complete covalent assembly of J chain-containing pentameric complexes did occur prior to their maturation in the Golgi. These data argue that pentameric structures are the substrate for J chain incorporation into assembling IgM and suggest that the incorporation of J chain is thermodynamically favored over the addition of a sixth monomeric subunit into an assembling polymer. We conclude that late events in IgM polymer assembly, specifically the insertion of J chain, the exclusion of an additional monomeric subunit, and the covalent closure of the pentameric IgM molecule, determine the polymeric structure and, consequently, the biological activity of secreted IgM.

摘要

IgM抗体可以以至少两种功能性多聚体形式分泌,这两种形式可根据亚基组成来区分。IgM六聚体由六个H2L2单体亚基组成,而五聚体则含有一种额外的多肽,即J链。在高丰度J链蛋白存在的情况下,IgM五聚体优先组装,而六聚体的组装则受到抑制。为了确定J链调节组装过程的机制,我们确定了J链添加到组装聚合物中的时间点。我们没有发现IgM小组装中间体中存在J链的证据,这表明它与这些复合物没有稳定结合。然而,发现J链与具有细胞内五聚体结构沉降特性的大的多聚体IgM复合物相关。这些复合物通常没有完全共价组装;然而,含J链的五聚体复合物在高尔基体中成熟之前确实发生了完全共价组装。这些数据表明五聚体结构是J链掺入组装IgM的底物,并表明J链的掺入在热力学上比向组装聚合物中添加第六个单体亚基更有利。我们得出结论,IgM聚合物组装的后期事件,特别是J链的插入、额外单体亚基的排除以及五聚体IgM分子的共价封闭,决定了聚合物结构,进而决定了分泌型IgM的生物学活性。

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