J IMMUNOL：1型糖尿病治疗新靶标

2017-06-06 MedSci MedSci原创

1型糖尿病患者受损的β细胞无法完成将葡萄糖运送至细胞的任务，使葡萄糖积聚在血液之中，如果不及时注射胰岛素，便会损伤神经、血管和体内器官。B淋巴细胞通过作为优先支持自身反应性致病性T细胞扩增的APC亚型在1型糖尿病（T1D）发展中起关键作用。因为其致病重要性的结果，B淋巴细胞靶向治疗已经作为潜在的T1D干预措施，并且具有广泛的前景。遗憾的是，迄今所测试的B淋巴细胞导向的T1D干预措施未能阻止β细胞死

1型糖尿病多发生在儿童和青少年，也可发生于各种年龄。起病比较急剧，体内胰岛素绝对不足，容易发生酮症酸中毒，必须用胰岛素治疗才能获得满意疗效，否则将危及生命。近日，国际杂志Science translational medcine上在线发表一项关于采用PARP和MEK抑制剂合理联合疗法可以降低RAS突变型癌症的治疗负担的研究。

1型糖尿病患者受损的β细胞无法完成将葡萄糖运送至细胞的任务，使葡萄糖积聚在血液之中，如果不及时注射胰岛素，便会损伤神经、血管和体内器官。B淋巴细胞通过作为优先支持自身反应性致病性T细胞扩增的APC亚型在1型糖尿病（T1D）发展中起关键作用。因为其致病重要性的结果，B淋巴细胞靶向治疗已经作为潜在的T1D干预措施，并且具有广泛的前景。遗憾的是，迄今所测试的B淋巴细胞导向的T1D干预措施未能阻止β细胞死亡。

在本研究中，研究人员使用了基因操纵手段来筛选潜在的能阻止B细胞启动糖尿病诱导程序的代谢靶标。他们证明对非肥胖型糖尿病（non-obese diabetic，NOD）老鼠使用特定的通路（AID/RAD51）抑制后，大大降低了糖尿病的发展。

研究表明，初始的CRISPR / Cas9介导的遗传修饰方法已经将AID / RAD51轴识别作为为潜在的临床转化药理学方法的目标，可以通过将B淋巴细胞转化为抑制疾病的CD73 +调节状态来阻断T1D发展。

原始出处：

Ratiu JJ, Racine JJ, Hasham MG. et.al. Genetic and Small Molecule Disruption of the AID/RAD51 Axis Similarly Protects Nonobese Diabetic Mice from Type 1 Diabetes through Expansion of Regulatory B Lymphocytes. May 2017.

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2018-05-10 zhanglin3079

#糖尿病治疗#

28 0
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2017-06-07 柳叶一刀

#靶标#

30 0
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2017-06-06 清风拂面

谢谢分享，学习了

61 0
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2017-06-06 ylzr123

认真学习，把间接经验应用到临床实践中去，然后再总结出新思路。给点赞啦

55 0
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2017-06-06 赵淘淘

很不错，值得学习，谢谢分享了

51 0
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2017-06-06 飛歌

已经到分子水平了，以后怎么看病吧

64 0
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2017-06-06 邓启付

1型糖尿病严重危害儿童及青少年身体健康。

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