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尽管胰岛生长,但将瘦小鼠的胰岛成功移植到肥胖高血糖小鼠的脾脏内未能治愈后者。

Failure of successful intrasplenic transplantation of islets from lean mice to cure obese-hyperglycaemic mice, despite islet growth.

作者信息

Andersson A, Eriksson U, Petersson B, Reibring L, Swenne I

出版信息

Diabetologia. 1981 Mar;20(3):237-41. doi: 10.1007/BF00252634.

Abstract

Implantation of allogeneic pancreatic islets encapsulated in Millipore diffusion chambers has been reported to normalize the obese-hyperglycaemic syndrome in mice. In the present study, both young and adult ob/ob mice remained hyperglycaemic and gained weight after intrasplenic implantation of 500 isogeneic islets isolated from lean mice. Such islets normalized the elevated blood-glucose of alloxan-diabetic lean mice. Morphometric analysis of the intrasplenically implanted islets showed that the mean islet volume in the ob/ob mice was five times larger than that of the lean, non-diabetic mice. Immunocytochemical staining of the spleens showed an increased proportion of B-cells in the enlarged, intrasplenic islets in the ob/ob mice. Moreover, autoradiographical examination of these islets demonstrated the presence of several labelled cells. These results suggest that the growth of the implanted "lean" islets is due to extrapancreatic factors which stimulate islet cell replication in the obese-hyperglycaemic mouse.

摘要

据报道,将包裹在密理博扩散小室中的同种异体胰岛植入小鼠体内,可使肥胖 - 高血糖综合征恢复正常。在本研究中,无论是幼年还是成年的ob/ob小鼠,在脾脏内植入从瘦小鼠分离的500个同基因胰岛后,血糖仍持续升高且体重增加。而这些胰岛可使四氧嘧啶诱导的糖尿病瘦小鼠升高的血糖恢复正常。对脾脏内植入的胰岛进行形态计量分析显示,ob/ob小鼠胰岛的平均体积是瘦的非糖尿病小鼠的五倍。对脾脏进行免疫细胞化学染色显示,ob/ob小鼠脾脏内增大的胰岛中B细胞比例增加。此外,对这些胰岛的放射自显影检查显示存在多个标记细胞。这些结果表明,植入的“瘦”胰岛的生长是由于胰腺外因素刺激肥胖 - 高血糖小鼠的胰岛细胞复制所致。

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