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The nonimmunoglobulin protion of λ5 mediates cell-autonomous pre-B cell receptor signaling

机译:λ5的非免疫球蛋白介导细胞自主前B细胞受体信号转导

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摘要

The pre-B cell receptor (preBCR), composed of μ immunoglobulin (Ig) and surrogate light chains, signals large 'preB-II' cells to proliferate in the apparent absence of ligands or cooperating cells. We deleted the N-terminal, nonimmunoglobulin (nonlg) protion of λ5, or mutated seven arginine residues in it to serine residues. PreBCRs with such mutant λ5 proteins showed increased cell surface representation and a diminished rate of aggregation and internalization. Tyrosine phosphorylation of preBCR complexes containing mutant λ5 proteins was abolished. These results indicate that the nonlg protion of λ5, and the seven arginine residues in it, are needed for signal transduction, and that signaling could be cell utonomous. We propose two models to explain the apparently constitutive, ligand-independent signal-transducing capacity of the preBCR.
机译:由μ免疫球蛋白(Ig)和替代轻链组成的pre-B细胞受体(preBCR)向大型“ preB-II”细胞发出信号,使其在明显缺乏配体或协作细胞的情况下增殖。我们删除了λ5的N端非免疫球蛋白(nonlg)配基,或将其中的7个精氨酸残基突变为丝氨酸残基。具有此类突变λ5蛋白的PreBCRs显示出增加的细胞表面表达,以及降低的聚集和内化速率。取消了含有突变型λ5蛋白的preBCR复合物的酪氨酸磷酸化作用。这些结果表明,信号转导需要λ5的壬基保护以及其中的7个精氨酸残基,并且信号转导可能是细胞融合的。我们提出了两个模型来解释preBCR的明显组成型,不依赖配体的信号转导能力。

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