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具有条件性淋巴细胞缺陷的Thy-1 tk转基因小鼠。

Thy-1 tk transgenic mice with a conditional lymphocyte deficiency.

作者信息

Dzierzak E, Daly B, Fraser P, Larsson L, Müller A

机构信息

Laboratory of Gene Structure and Expression, National Institute for Medical Research, Mill Hill, London, UK.

出版信息

Int Immunol. 1993 Aug;5(8):975-84. doi: 10.1093/intimm/5.8.975.

Abstract

Thy-1 has been used as a cell surface marker for identification of mature T cells, T lymphoid precursors and the hematopoietic stem cell. The developmental program of these cells during hemato/lymphopoiesis is complex because of heterogeneity of the populations and subsequent migration. To study the differentiation of Thy-1 positive cells at precise periods of in vivo development we have used a strategy based on cell specific toxicity. In the transgenic mouse studies presented here, Thy-1 positive cells are ablated by targeting the expression of the conditional toxin Herpes simplex virus 1 thymidine kinase (tk) with Thy-1 transcriptional control elements. We demonstrate the controlled expression of HSV1 tk in Thy-1 expressing cells of adult transgenic mice and the conditional ablation of > 90% of maturing thymocytes. We describe the distinct subpopulations of cells remaining within individual ablated thymuses and show by phenotypic analyses that Thy-1 tk induced ablation enriches for CD4 low and double negative thymocytes. Furthermore, we demonstrate a differential effect of thymus directed ablation on the maturing peripheral T cell compartment at various times in mouse development. This strategy is successful for production of a conditional T lymphocyte deficiency and could be useful in the study of T lineage development and direct in vivo isolation of enriched T precursor cell populations.

摘要

Thy-1已被用作细胞表面标志物,用于鉴定成熟T细胞、T淋巴细胞前体和造血干细胞。由于这些细胞群体的异质性以及随后的迁移,它们在血液/淋巴细胞生成过程中的发育程序很复杂。为了研究Thy-1阳性细胞在体内发育特定阶段的分化,我们采用了一种基于细胞特异性毒性的策略。在本文介绍的转基因小鼠研究中,通过用Thy-1转录控制元件靶向条件毒素单纯疱疹病毒1胸苷激酶(tk)的表达来消除Thy-1阳性细胞。我们证明了成年转基因小鼠Thy-1表达细胞中HSV1 tk的可控表达以及>90%成熟胸腺细胞的条件性消除。我们描述了各个被切除胸腺中剩余的不同细胞亚群,并通过表型分析表明,Thy-1 tk诱导的切除使CD4低和双阴性胸腺细胞富集。此外,我们证明了胸腺定向切除在小鼠发育的不同时间对成熟外周T细胞区室有不同影响。该策略成功地产生了条件性T淋巴细胞缺陷,可用于研究T谱系发育以及直接在体内分离富集的T前体细胞群体。

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