抗原受体交联可诱导正常小鼠而非易患自身免疫病小鼠的腹膜B细胞凋亡。

Antigen-receptor cross-linking induces peritoneal B-cell apoptosis in normal but not autoimmunity-prone mice.

作者信息

Tsubata T, Murakami M, Honjo T

机构信息

Department of Medical Chemistry, Faculty of Medicine, Kyoto University, Japan.

出版信息

Curr Biol. 1994 Jan 1;4(1):8-17. doi: 10.1016/s0960-9822(00)00003-8.

DOI:10.1016/s0960-9822(00)00003-8

PMID:7922322

Abstract

BACKGROUND

Programmed cell death (apoptosis) is an essential process in the development of various tissues and seems to be involved in the elimination of self-reactive immature T and B lymphocytes when they interact with self antigens. Indeed, signaling through the antigen receptor of immature T cells induces their apoptotic cell death. Immature B cells have also been shown to be eliminated when they interact with antigens, although the involvement of apoptosis has yet to be demonstrated. In contrast, little is known about the elimination of mature lymphocytes upon interaction with antigens. We have previously demonstrated that Ly1 B cells in the peritoneal cavity of transgenic mice undergo apoptotic cell death upon interaction with antigens. As Ly1 B cells constitute a B-cell lineage distinct from conventional B cells, it is important to know whether conventional B cells also undergo apoptosis upon antigen-receptor cross-linking.

RESULTS

Our experiments show that, in vivo, strong cross-linking of cell-surface immunoglobulins induced apoptotic death of normal, mature B cells in the peritoneal cavity, regardless of whether they were conventional or Ly1 B cells. The same treatment did not kill, but rather activated, B cells in bcl-2-transgenic, apoptosis-resistant mice. Peritoneal B cells from autoimmune-disease-prone New Zealand mouse strains were also found to be resistant to cell death induced by surface immunoglobulin cross-linking.

CONCLUSION

Self-reactive B cells are eliminated by the binding of antigen at both mature and immature stages. B-cell activation appears to require, in addition to antigen binding, a second signal that induces expression of rescue molecules such as the bcl-2 gene product. Resistance to B-cell apoptosis induced by antigen receptor cross-linking may play a crucial role in the production of autoantibodies and in the pathogenesis of the autoimmune diseases found in the strains of mice used here.

摘要

背景

程序性细胞死亡（凋亡）是各种组织发育过程中的一个重要过程，似乎参与了自身反应性未成熟T和B淋巴细胞与自身抗原相互作用时的清除。实际上，通过未成熟T细胞的抗原受体发出的信号诱导其凋亡性细胞死亡。未成熟B细胞在与抗原相互作用时也已被证明会被清除，尽管凋亡的参与尚未得到证实。相比之下，关于成熟淋巴细胞与抗原相互作用后的清除情况知之甚少。我们之前已经证明，转基因小鼠腹腔中的Ly1 B细胞在与抗原相互作用后会发生凋亡性细胞死亡。由于Ly1 B细胞构成了一个与传统B细胞不同的B细胞谱系，了解传统B细胞在抗原受体交联后是否也会发生凋亡很重要。

结果

我们的实验表明，在体内，细胞表面免疫球蛋白的强烈交联会诱导腹腔中正常成熟B细胞的凋亡性死亡，无论它们是传统B细胞还是Ly1 B细胞。相同的处理不会杀死bcl-2转基因、抗凋亡小鼠中的B细胞，反而会激活它们。还发现来自易患自身免疫性疾病的新西兰小鼠品系的腹腔B细胞对表面免疫球蛋白交联诱导的细胞死亡具有抗性。

结论

自身反应性B细胞在成熟和未成熟阶段都会因抗原结合而被清除。B细胞激活似乎除了抗原结合外，还需要第二个信号来诱导诸如bcl-2基因产物等拯救分子的表达。对抗原受体交联诱导的B细胞凋亡的抗性可能在自身抗体的产生以及此处所用小鼠品系中发现的自身免疫性疾病的发病机制中起关键作用。

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抗原受体交联可诱导正常小鼠而非易患自身免疫病小鼠的腹膜B细胞凋亡。

Antigen-receptor cross-linking induces peritoneal B-cell apoptosis in normal but not autoimmunity-prone mice.

作者信息

机构信息

出版信息

BACKGROUND

RESULTS

CONCLUSION

背景

结果

结论

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