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γ2b转基因小鼠作为免疫球蛋白在B细胞发育中作用的模型。

Gamma 2b transgenic mice as a model for the role of immunoglobulins in B cell development.

作者信息

Storb U, Roth P, Kurtz B K

机构信息

Department of Molecular Genetics and Cell Biology, University of Chicago, Ill., USA.

出版信息

Immunol Res. 1994;13(4):291-8. doi: 10.1007/BF02935620.

Abstract

The development of B lymphocytes is tightly linked to the expression of immunoglobulins (Igs). Pro/preB cells which do not correctly rearrange heavy/light chain genes are aborted. Correctly rearranged Ig transgenes are apparently recognized by the developing B cells and can prevent the rearrangement of endogenous Ig genes. Both mu and gamma 2b heavy chain genes cause this feedback inhibition of heavy chain gene rearrangement. Mu transgenes can in addition replace endogenous MU in its preB cell survival/maturation function. However, several different transgenic lines have shown that gamma 2b transgenes do not provide the nurturing functions of mu, except for one unique gamma 2b transgenic line, the C line. In this line mature B cells express gamma 2b only. Presumably, an unknown gene has been activated at the transgene integration site whose product overcomes the need for mu. The function of this gene depends of the presence of the surrogate light chain (sL), and thus must operate in combination with the preB cell receptor or in a downstream signaling/antiapoptosis event requiring the gamma 2b/sL receptor. The analysis of the two types of gamma 2b transgenic mice shows that the signals for preB cell development are highly complex and promises to reveal new insights into the molecular and cellular mechanisms of B cell maturation.

摘要

B淋巴细胞的发育与免疫球蛋白(Igs)的表达紧密相关。未正确重排重链/轻链基因的前B细胞/前体B细胞会凋亡。正确重排的Ig转基因显然能被发育中的B细胞识别,并可阻止内源性Ig基因的重排。μ链和γ2b重链基因均可导致重链基因重排的这种反馈抑制。此外,μ转基因可在其前B细胞存活/成熟功能中替代内源性μ链。然而,几个不同的转基因品系表明,γ2b转基因不能提供μ链的滋养功能,除了一个独特的γ2b转基因品系,即C品系。在这个品系中,成熟B细胞仅表达γ2b。据推测,在转基因整合位点有一个未知基因被激活,其产物克服了对μ链的需求。该基因的功能依赖于替代轻链(sL)的存在,因此必须与前B细胞受体共同发挥作用,或在需要γ2b/sL受体的下游信号传导/抗凋亡事件中发挥作用。对这两种γ2b转基因小鼠的分析表明,前B细胞发育的信号高度复杂,有望揭示B细胞成熟的分子和细胞机制的新见解。

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