Department of Medicine, University of Virginia, Charlottesville, Virginia, USA.
Am J Physiol Gastrointest Liver Physiol. 2012 Jan 1;302(1):G105-15. doi: 10.1152/ajpgi.00194.2011. Epub 2011 Sep 15.
SAMP1/YitFcs mice serve as a model of Crohn's disease, and we have used them to assess gastritis. Gastritis was compared in SAMP1/YitFcs, AKR, and C57BL/6 mice by histology, immunohistochemistry, and flow cytometry. Gastric acid secretion was measured in ligated stomachs, while anti-parietal cell antibodies were assayed by immunofluorescence and enzyme-linked immunosorbent spot assay. SAMP1/YitFcs mice display a corpus-dominant, chronic gastritis with multifocal aggregates of mononuclear cells consisting of T and B lymphocytes. Relatively few aggregates were observed elsewhere in the stomach. The infiltrates in the oxyntic mucosa were associated with the loss of parietal cell mass. AKR mice, the founder strain of the SAMP1/YitFcs, also have gastritis, although they do not develop ileitis. Genetic studies using SAMP1/YitFcs-C57BL/6 congenic mice showed that the genetic regions regulating ileitis had comparable effects on gastritis. The majority of the cells in the aggregates expressed the T cell marker CD3 or the B cell marker B220. Adoptive transfer of SAMP1/YitFcs CD4(+) T helper cells, with or without B cells, into immunodeficient recipients induced a pangastritis and duodenitis. SAMP1/YitFcs and AKR mice manifest hypochlorhydria and anti-parietal cell antibodies. These data suggest that common genetic factors controlling gastroenteric disease in SAMP1/YitFcs mice regulate distinct pathogenic mechanisms causing inflammation in separate sites within the digestive tract.
SAMP1/YitFcs 小鼠可作为克罗恩病模型,我们用其来评估胃炎。我们通过组织学、免疫组化和流式细胞术比较了 SAMP1/YitFcs、AKR 和 C57BL/6 小鼠的胃炎。我们通过结扎胃来测量胃酸分泌,通过免疫荧光和酶联免疫斑点测定来检测抗壁细胞抗体。SAMP1/YitFcs 小鼠表现出以胃体为主的慢性胃炎,伴有单核细胞的多灶性聚集,包括 T 和 B 淋巴细胞。在胃的其他部位观察到的聚集相对较少。胃窦黏膜中的浸润与壁细胞质量的丧失有关。SAMP1/YitFcs 的创始株 AKR 小鼠也有胃炎,但它们不会发生回肠炎。使用 SAMP1/YitFcs-C57BL/6 近交系小鼠的遗传研究表明,调节回肠炎的遗传区域对胃炎具有相当的影响。聚集物中的大多数细胞表达 T 细胞标志物 CD3 或 B 细胞标志物 B220。将 SAMP1/YitFcs CD4(+)辅助性 T 细胞(有或没有 B 细胞)过继转移到免疫缺陷受体中,会引起全胃炎和十二指肠炎。SAMP1/YitFcs 和 AKR 小鼠表现出低胃酸分泌和抗壁细胞抗体。这些数据表明,控制 SAMP1/YitFcs 小鼠胃肠道疾病的共同遗传因素调节了导致消化道不同部位炎症的不同致病机制。