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幼年HLA - B27转基因大鼠盲肠炎和结肠炎的免疫病理学特征

Immunopathologic characterization of typhlitis and colitis in juvenile HLA-B27 transgenic rats.

作者信息

Gough A W, Mosley R L, Stubbs C J

机构信息

Department of Pathology and Experimental Toxicology, Parke-Davis Pharmaceutical Research Division, MI 48105, USA.

出版信息

Pathobiology. 1994;62(5-6):221-31. doi: 10.1159/000163914.

Abstract

Adult HLA-B27 transgenic rats carrying high copy numbers of human HLA-B27 and beta 2-microglobulin genes spontaneously develop spondyloarthropathy and enterocolitis comparable to human HLA-B27-associated disease. In this investigation, juvenile HLA-27 transgenic rats were utilized to study incipient immunopathologic events in HLA-B27-associated gastrointestinal inflammation. Flow cytometric analysis of peripheral lymphocytes demonstrated distinctive differences in HLA-B27 protein expression and prompted the division of these transgenic rodents into 2 groups: HLA-B27hi and HLA-B27lo. The HLA-B27hi group, which represented 60% of the rats (aged 8-12 weeks) had inflammation in the colon, anorectal junction and cecum but spared the small intestine. Inflammation coexisted with high levels of surface HLA-B27 expression by hematopoietically derived cells as determined by immunofluorescence staining and flow cytometric analysis of intestinal lymphocytes. Inflammation, which was most intense in the cecum and anorectal junction, was characterized by mixed cellular infiltrate, crypt hyperplasia, transepithelial migration of neutrophils and a reduction in goblet cells. T lymphocytes, particularly CD4+ T cells, predominated over other lymphocytes in the inflammatory infiltrate of the lamina propria. Conversely, no inflammation was evident at any level of the gastrointestinal tract in the HLA-B27lo group (8 weeks of age) which constituted 40% of the juvenile transgenic rats. These animals all expressed low level of HLA-B27 protein. Collectively, these data indicate that HLA-B27 protein expression increases dramatically from 8 to 12 weeks of age and that the level of protein expression and intestinal inflammation are interrelated. These associated gastrointestinal events occur during puberty and thus we speculate that the high level of protein expression may be hormonally mediated.

摘要

携带高拷贝数人类HLA - B27和β2 -微球蛋白基因的成年HLA - B27转基因大鼠会自发发展出与人类HLA - B27相关疾病相似的脊柱关节病和小肠结肠炎。在本研究中,利用幼年HLA - 27转基因大鼠来研究HLA - B27相关胃肠道炎症初期的免疫病理事件。对外周淋巴细胞进行流式细胞术分析显示HLA - B27蛋白表达存在显著差异,并促使将这些转基因啮齿动物分为两组:HLA - B27高表达组(HLA - B27hi)和HLA - B27低表达组(HLA - B27lo)。HLA - B27hi组占大鼠(8 - 12周龄)的60%,其结肠、肛门直肠交界处和盲肠有炎症,但小肠未受累。通过免疫荧光染色和肠道淋巴细胞流式细胞术分析确定,炎症与造血来源细胞表面高水平的HLA - B27表达共存。炎症在盲肠和肛门直肠交界处最为严重,其特征为混合性细胞浸润、隐窝增生、中性粒细胞跨上皮迁移以及杯状细胞减少。在固有层的炎症浸润中,T淋巴细胞,尤其是CD4 + T细胞,比其他淋巴细胞占优势。相反,占幼年转基因大鼠40%的HLA - B27lo组(8周龄)在胃肠道任何水平均未出现明显炎症。这些动物均表达低水平的HLA - B27蛋白。总体而言,这些数据表明HLA - B27蛋白表达在8至12周龄时显著增加,且蛋白表达水平与肠道炎症相互关联。这些相关的胃肠道事件发生在青春期,因此我们推测高水平的蛋白表达可能是由激素介导的。

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