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HD小鼠:一种在CD4(+) T细胞生成方面存在特定缺陷的新型小鼠突变体。

HD mice: a novel mouse mutant with a specific defect in the generation of CD4(+) T cells.

作者信息

Dave V P, Allman D, Keefe R, Hardy R R, Kappes D J

机构信息

Fox Chase Cancer Center, 7701 Burholme Avenue, Philadelphia, PA 19111, USA.

出版信息

Proc Natl Acad Sci U S A. 1998 Jul 7;95(14):8187-92. doi: 10.1073/pnas.95.14.8187.

Abstract

We have identified a spontaneous mutation in mice, which we term HD for "helper T cell deficient." This mouse is distinguished by the virtual absence of peripheral T cells of the CD4(+)8(-) major histocompatibility complex (MHC) class II-restricted T helper subset due to a specific block in thymic development. The developmental defect is selective for CD4(+)8(-) cells; the maturation of CD4(-)8(+) and gamma delta T cells is normal. The autosomal recessive mutation underlying the HD phenotype is unrelated to MHC class II, since it segregates independently of the MHC class II locus. Moreover, the HD phenotype is not caused by a defect of the CD4 gene. Bone marrow transfer experiments demonstrate that the defect is intrinsic to cells of the hematopoietic lineage, i.e., most likely to developing thymocytes themselves. The frequency of CD4(+)8(low) intermediate cells is markedly increased in HD mice, suggesting that class II-restricted thymocytes are arrested at this stage. This is the first genetic defect of its kind to be described in the mouse and may prove highly informative in understanding the molecular pathways underlying lineage commitment.

摘要

我们在小鼠中鉴定出一种自发突变,我们将其命名为HD,即“辅助性T细胞缺陷”。这种小鼠的特征是,由于胸腺发育存在特定阻滞,几乎没有外周CD4(+)8(-)主要组织相容性复合体(MHC)II类限制性辅助性T细胞亚群。这种发育缺陷对CD4(+)8(-)细胞具有选择性;CD4(-)8(+)和γδT细胞的成熟是正常的。HD表型所基于的常染色体隐性突变与MHC II类无关,因为它与MHC II类基因座独立分离。此外,HD表型并非由CD4基因缺陷引起。骨髓移植实验表明,该缺陷是造血谱系细胞所固有的,即很可能是发育中的胸腺细胞自身所固有的。HD小鼠中CD4(+)8(低)中间细胞的频率显著增加,这表明II类限制性胸腺细胞在此阶段停滞。这是在小鼠中首次描述的此类遗传缺陷,可能对理解谱系定向所涉及的分子途径具有高度的指导意义。

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