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首页> 外文期刊>The journal of immunology >The TCRβ Enhancer Is Dispensable for the Expression of Rearranged TCRβ Genes in Thymic DN2/DN3 Populations but Not at Later Stages
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The TCRβ Enhancer Is Dispensable for the Expression of Rearranged TCRβ Genes in Thymic DN2/DN3 Populations but Not at Later Stages

机译:TCRβ增强子对于胸腺DN2 / DN3群体中重排的TCRβ基因表达是必不可少的,但在后期则不是

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The Eβ enhancer has been shown to be dispensable for germline transcription of nonrearranged TCRβ segments but appears to be required for TCRβ V to DJ rearrangement. Eβ dependency of the subsequent expression of VDJ-rearranged TCRβ genes in thymic subpopulations has so far not been analyzed. We generated transgenic mice, using a Vβ8.2Dβ1Jβ1.3-rearranged TCRβ bacterial artificial chromosome, which lacked Eβ, and monitored transgene expression by flow cytometry using Vβ-specific mAbs and an IRES-eGFP reporter. Transgene expression was found in double negative (DN)2 and DN3 but not at later stages of thymopoesis. There was no toxicity associated with the transgene given that apoptosis in DN3, DN4 was not increased, and the number of DN4 cells generated from DN3 cells in reaggregate thymic organ cultures was not diminished. The transgenic TCRβ gave rise to a pre-TCR, as suggested by its ability to suppress endogenous TCRβ rearrangement, to facilitate β-selection on a TCRβ-deficient background and to inhibit γδ T cell lineage development. The results suggest that the Vβ8.2 promoter is sufficient to drive expression of rearranged TCRβ VDJ genes Eβ independently in DN2/DN3 but not at later stages.
机译:已经证明Eβ增强子对于非重排TCRβ片段的种系转录是可有可无的,但是似乎是TCRβV至DJ重排所必需的。迄今为止,尚未分析胸腺亚群中VDJ重排的TCRβ基因后续表达的Eβ依赖性。我们使用缺少Eβ的Vβ8.2Dβ1Jβ1.3重排的TCRβ细菌人工染色体生成了转基因小鼠,并使用Vβ特异性mAb和IRES-eGFP报告基因通过流式细胞仪监测了转基因的表达。在双阴性(DN)2和DN3中发现了转基因表达,但在胸腺造血术的后期未发现。鉴于DN3,DN4的凋亡没有增加,并且在重聚的胸腺器官培养物中由DN3细胞生成的DN4细胞数量没有减少,因此与转基因没有毒性。正如转基因TCRβ抑制内源性TCRβ重排,在缺乏TCRβ的背景上促进β选择以及抑制γδT细胞谱系发育的能力所暗示的那样,它产生了pre-TCR。结果表明,Vβ8.2启动子足以驱动重排的TCRβVDJ基因Eβ在DN2 / DN3中独立表达,但在随后的阶段却不能。

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