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来自自身免疫性“活的食母生”突变小鼠的杂交瘤产生异常免疫球蛋白。

Synthesis of abnormal immunoglobulins by hybridomas from autoimmune "viable motheaten" mutant mice.

作者信息

Schweitzer P A, Taylor S E, Shultz L D

机构信息

Jackson Laboratory, Bar Harbor, Maine 04609.

出版信息

J Cell Biol. 1991 Jul;114(1):35-43. doi: 10.1083/jcb.114.1.35.

Abstract

Secretory defects in abnormal plasma cells, called Mott cells, that appear in lymphoid tissues of spontaneously autoimmune, "viable motheaten" (mev/mev) mice lead to deposition of immunoglobulin in RER-bound vesicles. Such vesicles have been termed Russel bodies. Cells with Russel bodies can also be observed rarely in normal animals, usually as a result of extreme antigenic loads or pathologic states. To understand why these abnormal cells appear commonly in mev/mev mice, we have established a panel of hybridomas that contain Russell bodies. Using immunochemical analysis and immunoelectron microscopy, we have characterized the secretory defects. Although these hybridoma cells synthesize a normal size heavy chain and it associates with light chain, the Russell bodies have many characteristics of inclusion bodies, which commonly appear in cells synthesizing mutant proteins and often are associated with incompletely or abnormally folded proteins. Pulse-chase experiments showed that immunoglobulins synthesized by these hybridomas accumulate rapidly into insoluble complexes and have an intracellular half life approximately 10 time greater than normal immunoglobulins. The defect affected only the immunoglobulin derived from the mev/mev mice and did not affect the secretion of normal immunoglobulin produced by an IgG1-secreting fusion partner. In addition to accumulating intracellular immunoglobulins, many mutant cell lines also secreted immunoglobulin. Endoglycosidase H digestion was used to determine the state of processing of the N-linked carbohydrates on the immunoglobulin molecules. This analysis demonstrated that the N-linked carbohydrates on the secreted immunoglobulin were resistant to endoglycosidase H digestion, indicating that they were processed normally. The insoluble IgM molecules were sensitive to endoglycosidase H, which is consistent with their localization to the RER. We propose several models by which these abnormal immunoglobulin-secreting cells commonly appear in this autoimmune mutant mouse.

摘要

在自发自身免疫性“可行的病毛鼠”(mev/mev)小鼠的淋巴组织中出现的异常浆细胞,即莫特细胞,其分泌缺陷导致免疫球蛋白沉积在与粗面内质网结合的囊泡中。这种囊泡被称为拉塞尔小体。在正常动物中也很少能观察到带有拉塞尔小体的细胞,通常是极端抗原负荷或病理状态的结果。为了理解为什么这些异常细胞在mev/mev小鼠中普遍出现,我们建立了一组含有拉塞尔小体的杂交瘤。通过免疫化学分析和免疫电子显微镜,我们对分泌缺陷进行了表征。尽管这些杂交瘤细胞合成了正常大小的重链并且它与轻链结合,但拉塞尔小体具有包涵体的许多特征,包涵体通常出现在合成突变蛋白的细胞中,并且常常与不完全或异常折叠的蛋白相关。脉冲追踪实验表明,这些杂交瘤合成的免疫球蛋白迅速积累形成不溶性复合物,其细胞内半衰期比正常免疫球蛋白大约长10倍。该缺陷仅影响源自mev/mev小鼠的免疫球蛋白,而不影响由分泌IgG1的融合伙伴产生的正常免疫球蛋白的分泌。除了在细胞内积累免疫球蛋白外,许多突变细胞系也分泌免疫球蛋白。使用内切糖苷酶H消化来确定免疫球蛋白分子上N-连接碳水化合物的加工状态。该分析表明,分泌的免疫球蛋白上的N-连接碳水化合物对内切糖苷酶H消化具有抗性,表明它们加工正常。不溶性IgM分子对内切糖苷酶H敏感,这与其定位于粗面内质网一致。我们提出了几种模型,通过这些模型这些异常分泌免疫球蛋白的细胞在这种自身免疫突变小鼠中普遍出现。

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