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转基因小鼠角质形成细胞中白细胞介素-7(IL-7)的过表达导致一种以中间型T细胞受体(TCR)细胞为主的淋巴细胞增生性皮肤病:皮肤T细胞中IL-7反应性存在等级差异的证据。

IL-7 overexpression in transgenic mouse keratinocytes causes a lymphoproliferative skin disease dominated by intermediate TCR cells: evidence for a hierarchy in IL-7 responsiveness among cutaneous T cells.

作者信息

Williams I R, Rawson E A, Manning L, Karaoli T, Rich B E, Kupper T S

机构信息

Harvard Skin Disease Research Center, Division of Dermatology, Brigham and Women's Hospital, Boston, MA 02115, USA.

出版信息

J Immunol. 1997 Sep 15;159(6):3044-56.

PMID:9300730
Abstract

IL-7 is a keratinocyte-derived lymphocyte growth factor critical for the development of gammadelta T cells including murine dendritic epidermal T cells (DETC). We derived transgenic mice that overexpress IL-7 in basal keratinocytes under the control of the human K14 promoter. These K14/IL-7 mice develop dermal and epidermal T cell infiltrates associated with alopecia. This lymphoproliferative skin disease is substantially more severe in mice homozygous for the K14/IL-7 transgene. Conventional DETC expressing a Vgamma5 Vdelta1 TCR are rare or absent among the cutaneous T cells in these mice. The T cells in the skin infiltrates of young K14/IL-7 mice are predominantly gammadelta T cells that express intermediate levels of TCR, are negative for E-cadherin, often lack expression of CD2, and include cells that coexpress NK1.1. T cells expressing intermediate levels of a TCR-alphabeta are also present in transgenic skin, and progressively increase in number as the mice age. Phenotypically similar intermediate gammadelta and alphabeta T cell subsets also constitute the major lymphocyte populations recovered from organ culture of normal mouse skin in the presence of IL-7, suggesting that the T cells that accumulate in the epidermis of K14/IL-7 mice are derived from precursors normally resident in skin. We conclude that intermediate TCR cells, some of which coexpress NK1.1, can be selectively expanded in skin under the influence of IL-7 produced locally. Our results also suggest that features of the epidermal microenvironment besides keratinocyte-derived IL-7 account for the normal predominance of Vgamma5 Vdelta1 DETC in mouse epidermis.

摘要

白细胞介素-7是一种角质形成细胞衍生的淋巴细胞生长因子,对γδT细胞(包括小鼠树突状表皮T细胞,即DETC)的发育至关重要。我们构建了在人K14启动子控制下,在基底角质形成细胞中过表达白细胞介素-7的转基因小鼠。这些K14/IL-7小鼠会出现与脱发相关的真皮和表皮T细胞浸润。这种淋巴细胞增生性皮肤病在K14/IL-7转基因纯合小鼠中更为严重。在这些小鼠的皮肤T细胞中,表达Vγ5Vδ1TCR的传统DETC很少或不存在。年轻K14/IL-7小鼠皮肤浸润中的T细胞主要是γδT细胞,它们表达中等水平的TCR,E-钙黏蛋白呈阴性,通常缺乏CD2表达,并且包括共表达NK1.1的细胞。表达中等水平TCR-αβ的T细胞也存在于转基因皮肤中,并且随着小鼠年龄增长数量逐渐增加。表型相似的中等γδ和αβT细胞亚群也构成了在白细胞介素-7存在下从正常小鼠皮肤器官培养物中回收的主要淋巴细胞群体,这表明在K14/IL-7小鼠表皮中积累的T细胞来源于正常驻留在皮肤中的前体细胞。我们得出结论,一些共表达NK1.1的中等TCR细胞可以在局部产生的白细胞介素-7的影响下在皮肤中选择性扩增。我们的结果还表明,除了角质形成细胞衍生的白细胞介素-7之外,表皮微环境的特征也解释了Vγ5Vδ1DETC在小鼠表皮中正常占主导地位的原因。

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