首页> 外文期刊>Proceedings of the National Academy of Sciences of the United States of America >Lsh, an SNF2/helicase family member, is required for proliferation of mature T Lymphocytes
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Lsh, an SNF2/helicase family member, is required for proliferation of mature T Lymphocytes

机译:SNF2 /解旋酶家族成员Lsh是成熟T淋巴细胞增殖所必需的

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Lsh (Hells) is closely related to SNF2/helicase family members that remodel chromatin and thus regulate gene transcription. In the adult mouse Lsh is expressed primarily in lymphoid tissue, showing the highest level in thymocytes. Lsh gene expression can be induced in thymic pro-T cells by pre-T cell receptor crosslinking and in mature T cells by T cell receptor crosslinking together with costimulation via CD28. The time course of Lsh gene and protein expression correlated closely with the onset of S phase of the cell cycle. To explore the function of LSh during lymphoid development or activation, we deleted the Lsh gene by homologous recombination in ES cells. Fetal liver cells from Lsh~-/- were used as a source of hematopoietic precursors to reconstitute lymphoid development in Rag2~-/- mice. Lsh~-/- (compared to LSh+/+ or ±) chimeras showed a modest reduction in thymocyte numbers due to a partial arrest at the transition from the CD4-CD8- stage to the CD4~+CD8~+ stage of T cell development. Mature peripheral lymphocytes were reduced in num- ber to ≈60/100 for T cells and 40/100 for B cells; however. V(D)J recom- bination of the immune receptor genes was normal. Although poly- clonal activation of Lsh - / - T cells induced normal levels of cytokines, cell proliferation was severely suppressed and cells underwent apo- ptosis. Several genes involved in the regulation of apoptosis were expressed normally with the exception of BcI-2 that was actually elevated. These findings demonstrate that Lsh is not obligatory for normal lymphoid development but is essential for normal prolifera- tion of peripheral T lymphocytes.
机译:Lsh(Hells)与SNF2 / helasease家族成员密切相关,后者可以重塑染色质并从而调节基因转录。在成年小鼠中,Lsh主要在淋巴样组织中表达,在胸腺细胞中显示最高水平。 Lsh基因表达可以在胸腺pro-T细胞中通过前T细胞受体交联来诱导,在成熟T细胞中通过T细胞受体交联以及通过CD28的共刺激来诱导。 Lsh基因和蛋白质表达的时间过程与细胞周期S期的发生密切相关。为了探索LSh在淋巴发育或激活过程中的功能,我们通过在ES细胞中进行同源重组删除了Lsh基因。来自Lsh1-/-的胎儿肝细胞被用作造血前体的来源,以重构Rag2 2-/-小鼠的淋巴样发育。 Lsh〜-/-(与LSh + / +或±相比)嵌合体显示出胸腺细胞数量的适度减少,这是由于T细胞发育从CD4-CD8-阶段过渡到CD4〜+ CD8〜+阶段而部分停滞。成熟的外周血淋巴细胞减少到T细胞约60/100,B细胞约40/100。然而。免疫受体基因的V(D)J重组正常。尽管Lsh-/-T细胞的多克隆激活诱导正常水平的细胞因子,但细胞增殖被严重抑制,细胞经历了凋亡。除了实际升高的BcI-2外,正常表达几种参与细胞凋亡调控的基因。这些发现表明,Lsh不是正常淋巴发育所必需的,而是对外周T淋巴细胞正常增殖必不可少的。

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