白细胞介素-1受体基因敲除小鼠小肠上皮细胞更新增加。
Increased small bowel epithelial turnover in interleukin-1 receptor knockout mice.
作者信息
Wolf S E, Debroy M A, Ikeda H, Jeschke M, Matin S, Rajaraman S, Ko T C, Englander E W, Norman J G, Thompson J C
机构信息
Department of Surgery, The University of Texas Medical Branch and The Shriners Hospitals for Children, Galveston, Texas, USA.
出版信息
Ann Surg. 2000 Jul;232(1):42-5. doi: 10.1097/00000658-200007000-00006.
OBJECTIVE
To determine whether interleukin-1 (IL-1) affects the cellular homeostasis of small bowel mucosa, the authors studied apoptosis and proliferation in small bowel epithelium in two groups of C57 mice: an IL-1 receptor knockout group, and a control wild-type group.
SUMMARY BACKGROUND DATA
Gut mucosal integrity is maintained by a balance of cell proliferation and cell death. Recent reports suggest that IL-1, a proinflammatory cytokine, increases cell death by apoptosis in some epithelial cells.
METHODS
Twenty-four male C57BL6 IL-1 receptor (type I) knockout mice were killed, and small bowel was removed for study. Twenty-four wild-type mice (C57-BL6) served as controls. Body weights, bowel length, and mucosal morphology were examined for phenotypic differences. Apoptosis was quantified by terminal deoxyuridine nick-end labeling (TUNEL) immunohistochemical staining and cellular proliferation by proliferation cell nuclear antigen staining. Whole mucosal protein was analyzed for nuclear factor-kappaB expression. Groups were analyzed by t test.
RESULTS
The absence of IL-1 type I receptor in knockout mice was verified by reverse transcriptase-polymerase chain reaction. IL-1 receptor null mice were larger than wild-type controls, with a longer small bowel; however, the index of small bowel length to total body weight did not differ between groups. The percentage of apoptotic cells was higher in IL-1 receptor null mice than in wild-type mice; the proliferation index also increased. Mucosal height and other measures of mucosal morphology were not different. Genotypic absence of IL-1 receptors was associated with decreased expression of nuclear factor-kappaB in whole mucosal protein extracts.
CONCLUSIONS
Both apoptosis and proliferation increased in gut epithelial cells of mice without IL-1 receptors, suggesting increased cell turnover with no change in net balance. This model represents an opportunity to examine potential mechanisms of gut epithelial turnover in vivo, under both normal conditions and in conditions of mucosal proliferation and atrophy.
目的
为了确定白细胞介素 -1(IL-1)是否影响小肠黏膜的细胞稳态,作者研究了两组C57小鼠小肠上皮细胞的凋亡和增殖情况:一组为IL-1受体敲除组,另一组为对照野生型组。
摘要背景数据
肠道黏膜完整性通过细胞增殖和细胞死亡的平衡来维持。最近的报告表明,促炎细胞因子IL-1可通过诱导某些上皮细胞凋亡来增加细胞死亡。
方法
处死24只雄性C57BL6 IL-1受体(I型)敲除小鼠,并取出小肠进行研究。24只野生型小鼠(C57-BL6)作为对照。检查体重、肠长度和黏膜形态以寻找表型差异。通过末端脱氧尿苷酸缺口末端标记(TUNEL)免疫组化染色定量凋亡,通过增殖细胞核抗原染色定量细胞增殖。分析全黏膜蛋白中核因子 -κB的表达。采用t检验对各组进行分析。
结果
通过逆转录聚合酶链反应验证了敲除小鼠中I型IL-1受体的缺失。IL-1受体缺失小鼠比野生型对照更大,小肠更长;然而,两组之间小肠长度与总体重的比值并无差异。IL-1受体缺失小鼠的凋亡细胞百分比高于野生型小鼠;增殖指数也增加。黏膜高度和其他黏膜形态指标并无差异。IL-1受体的基因缺失与全黏膜蛋白提取物中核因子 -κB表达降低相关。
结论
在没有IL-1受体的小鼠肠道上皮细胞中,凋亡和增殖均增加,提示细胞更新增加但净平衡无变化。该模型为研究正常条件下以及黏膜增殖和萎缩条件下体内肠道上皮更新的潜在机制提供了契机。
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