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在一种新型转基因小鼠模型中，Stat3将银屑病发展所需的活化角质形成细胞和免疫细胞联系起来。

Stat3 links activated keratinocytes and immunocytes required for development of psoriasis in a novel transgenic mouse model.

作者信息

Sano Shigetoshi, Chan Keith Syson, Carbajal Steve, Clifford John, Peavey Mary, Kiguchi Kaoru, Itami Satoshi, Nickoloff Brian J, DiGiovanni John

机构信息

Department of Carcinogenesis, University of Texas, M. D. Anderson Cancer Center, Science Park - Research Division, 1808 Park Road 1C, PO Box 389, Smithville, Texas 78957, USA.

出版信息

Nat Med. 2005 Jan;11(1):43-9. doi: 10.1038/nm1162. Epub 2004 Dec 12.

DOI:10.1038/nm1162

PMID:15592573

Abstract

Here we report that epidermal keratinocytes in psoriatic lesions are characterized by activated Stat3. Transgenic mice with keratinocytes expressing a constitutively active Stat3 (K5.Stat3C mice) develop a skin phenotype either spontaneously, or in response to wounding, that closely resembles psoriasis. Keratinocytes from K5.Stat3C mice show upregulation of several molecules linked to the pathogenesis of psoriasis. In addition, the development of psoriatic lesions in K5.Stat3C mice requires cooperation between Stat3 activation in keratinocytes and activated T cells. Finally, abrogation of Stat3 function by a decoy oligonucleotide inhibits the onset and reverses established psoriatic lesions in K5.Stat3C mice. Thus, targeting Stat3 may be potentially therapeutic in the treatment of psoriasis.

摘要

我们在此报告，银屑病皮损中的表皮角质形成细胞具有激活的Stat3特征。角质形成细胞表达组成型激活Stat3的转基因小鼠（K5.Stat3C小鼠）会自发地或在受伤后出现与银屑病极为相似的皮肤表型。来自K5.Stat3C小鼠的角质形成细胞显示出与银屑病发病机制相关的几种分子上调。此外，K5.Stat3C小鼠中银屑病皮损的发展需要角质形成细胞中的Stat3激活与活化T细胞之间的协同作用。最后，诱饵寡核苷酸对Stat3功能的废除可抑制K5.Stat3C小鼠银屑病皮损的发生并逆转已形成的皮损。因此，靶向Stat3可能对银屑病治疗具有潜在的治疗作用。

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在一种新型转基因小鼠模型中，Stat3将银屑病发展所需的活化角质形成细胞和免疫细胞联系起来。

Stat3 links activated keratinocytes and immunocytes required for development of psoriasis in a novel transgenic mouse model.

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