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用非肥胖糖尿病(NOD)小鼠的脾细胞转移自身免疫性糖尿病

Transfer of autoimmune diabetes mellitus with splenocytes from nonobese diabetic (NOD) mice.

作者信息

Wicker L S, Miller B J, Mullen Y

出版信息

Diabetes. 1986 Aug;35(8):855-60. doi: 10.2337/diab.35.8.855.

Abstract

The nonobese diabetic (NOD) mouse, a model of human type I diabetes, develops insulitis beginning at 4-6 wk of age. By 30 wk of age, 72% of females and 39% of males develop spontaneous diabetes, apparently because of an overwhelming autoimmune response to the insulin-producing beta-cells within the islets. To identify the immune mechanism responsible for destruction of beta-cells in the NOD mouse, we developed an adoptive transfer protocol that induces diabetes in NOD mice at an age when spontaneous diabetes is rarely observed. Splenocytes from overtly diabetic NOD mice were unable to transfer diabetes to very young (less than or equal to 6 wk) irradiated NOD mice but effectively transferred diabetes to irradiated NOD mice greater than 6 wk of age. In such transfers, overt diabetes was induced within 12-22 days in greater than 95% (79/82) of the recipients. Thus, transfer of splenocytes to young mice induces them to become diabetic at a higher frequency and at a younger age than their untreated littermates. Equally successful transfers with as few as 5 X 10(6) spleen cells have been performed in male and female NOD mice, even though males display a lower spontaneous incidence of diabetes than females. Splenocytes obtained from diabetic mice maintained on insulin for up to 2 mo also transferred diabetes. Because NOD mice display increasing levels of insulitis with age, spleen cells obtained from nondiabetic NOD mice of different ages were tested for their ability to transfer diabetes.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

非肥胖型糖尿病(NOD)小鼠是人类I型糖尿病的一种模型,在4至6周龄时开始发生胰岛炎。到30周龄时,72%的雌性和39%的雄性会自发患上糖尿病,这显然是由于对胰岛内产生胰岛素的β细胞产生了压倒性的自身免疫反应。为了确定NOD小鼠中导致β细胞破坏的免疫机制,我们开发了一种过继转移方案,该方案能在很少观察到自发糖尿病的年龄诱导NOD小鼠患上糖尿病。明显患有糖尿病的NOD小鼠的脾细胞无法将糖尿病转移给非常年幼(小于或等于6周)且经过辐射的NOD小鼠,但能有效地将糖尿病转移给6周龄以上经过辐射的NOD小鼠。在这种转移中,超过95%(79/82)的受体在12至22天内出现明显的糖尿病。因此,将脾细胞转移给幼鼠会使其比未处理的同窝幼崽更频繁、更年幼地患上糖尿病。即使雄性NOD小鼠的自发糖尿病发病率低于雌性,在雄性和雌性NOD小鼠中,用低至5×10⁶个脾细胞进行的转移同样成功。从维持胰岛素治疗长达2个月的糖尿病小鼠中获得的脾细胞也能转移糖尿病。由于NOD小鼠的胰岛炎水平会随着年龄增长而升高,因此对不同年龄的非糖尿病NOD小鼠的脾细胞转移糖尿病的能力进行了测试。(摘要截断于250字)

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