首页> 美国卫生研究院文献>The Journal of Experimental Medicine >The immunosuppressant 15-deoxyspergualin correction of 15- deoxyspergualin reveals commonality between preT and preB cell differentiation
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The immunosuppressant 15-deoxyspergualin correction of 15- deoxyspergualin reveals commonality between preT and preB cell differentiation

机译:免疫抑制剂15-脱氧精瓜林15-脱氧精林的校正显示了preT和preB细胞分化之间的共性

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摘要

15 [correction of 1,5] deoxyspergualin (DSG) is a potent immunosuppressant whose mechanism of action is still somewhat of a mystery. We have studied the generation of lymphocytes in mice treated with this drug. The differentiation of T cells in the thymus was blocked at an important early control point: the CD4-8- --> CD4+8+ transition, known to depend on the expression of a preTCR complex that includes the variable TCR-beta, but not TCR-alpha, chain. In clear contrast, a later control point, the CD4+8+ --> CD4+8- or CD4-8+ transition, dependent on the display of a conventional alpha:beta TCR complex, appeared unaffected, as did activation of mature T cells both in vitro and in vivo. Interestingly, preB cell differentiation in the bone marrow was blocked at a precisely equivalent point: the A-C --> C' transition, controlled by expression of a pre-receptor complex containing the Ig heavy, but not light, chain. Mature B cells seemed unperturbed. These findings have theoretical implications, suggesting common signaling pathways in early lymphocytes that are distinct from those employed by more mature cells, and are also of practical interest, to be considered in the design of DSG treatment protocols.
机译:15 [1,5的校正]脱氧精胰岛素(DSG)是一种有效的免疫抑制剂,其作用机理仍是一个谜。我们已经研究了用这种药物治疗的小鼠中淋巴细胞的产生。胸腺中T细胞的分化在一个重要的早期控制点被阻止:CD4-8-> CD4 + 8 +过渡,已知依赖于包含可变TCR-beta的preTCR复合物的表达,但是不是TCR-alpha链。与之形成鲜明对比的是,依赖于常规α:βTCR复合物的显示,后来的控制点CD4 + 8 +-> CD4 + 8-或CD4-8 +过渡似乎不受影响,而成熟T的活化也没有受到影响。体外和体内细胞。有趣的是,骨髓中的preB细胞分化在一个精确的等价点被阻止:A-C-> C'过渡,由包含Ig重链但不轻链的前受体复合物的表达控制。成熟的B细胞似乎没有受到干扰。这些发现具有理论意义,表明早期淋巴细胞中的常见信号传导途径与成熟细胞所采用的信号途径不同,并且在设计DSG治疗方案时也具有实际意义。

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