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在衰老和胰岛损伤后,小鼠胰岛中的前体细胞在体内产生新的β细胞。

Precursor cells in mouse islets generate new beta-cells in vivo during aging and after islet injury.

机构信息

State University of New York-Downstate Medical Center, Department of Cell Biology, 450 Clarkson Avenue, Brooklyn, New York 11203, USA.

出版信息

Endocrinology. 2010 Feb;151(2):520-8. doi: 10.1210/en.2009-0992. Epub 2010 Jan 7.

Abstract

Whereas it is believed that the pancreatic duct contains endocrine precursors, the presence of insulin progenitor cells residing in islets remain controversial. We tested whether pancreatic islets of adult mice contain precursor beta-cells that initiate insulin synthesis during aging and after islet injury. We used bigenic mice in which the activation of an inducible form of Cre recombinase by a one-time pulse of tamoxifen results in the permanent expression of a floxed human placental alkaline phosphatase (PLAP) gene in 30% of pancreatic beta-cells. If islets contain PLAP(-) precursor cells that differentiate into beta-cells (PLAP(-)IN(+)), a decrease in the percentage of PLAP(+)IN(+) cells per total number of IN(+) cells would occur. Conversely, if islets contain PLAP(+)IN(-) precursors that initiate synthesis of insulin, the percentage of PLAP(+)IN(+) cells would increase. Confocal microscope analysis revealed that the percentage of PLAP(+)IN(+) cells in islets increased from 30 to 45% at 6 months and to 60% at 12 months. The augmentation in the level of PLAP in islets with time was confirmed by real-time PCR. Our studies also demonstrate that the percentage of PLAP(+)IN(+) cells in islets increased after islet injury and identified putative precursors in islets. We postulate that PLAP(+)IN(-) precursors differentiate into insulin-positive cells that participate in a slow renewal of the beta-cell mass during aging and replenish beta-cells eliminated by injury.

摘要

虽然人们相信胰腺导管中含有内分泌前体细胞,但胰岛中是否存在胰岛素祖细胞仍存在争议。我们检测了成年小鼠的胰岛中是否存在前体细胞β细胞,这些细胞在衰老和胰岛损伤后会启动胰岛素的合成。我们使用双基因小鼠,其中单次给予他莫昔芬后激活诱导型 Cre 重组酶,会导致 30%的胰岛β细胞中永久性表达 floxed 人胎盘碱性磷酸酶(PLAP)基因。如果胰岛中含有分化为β细胞的 PLAP(-)前体细胞(PLAP(-)IN(+)),那么 IN(+)细胞总数中 PLAP(+)IN(+)细胞的比例会下降。相反,如果胰岛中含有启动胰岛素合成的 PLAP(+)IN(-)前体细胞,那么 PLAP(+)IN(+)细胞的比例会增加。共聚焦显微镜分析显示,PLAP(+)IN(+)细胞在胰岛中的比例从 6 个月时的 30%增加到 12 个月时的 45%,再增加到 60%。随着时间的推移,PLAP 在胰岛中的水平增加,这一事实通过实时 PCR 得到了证实。我们的研究还表明,胰岛损伤后胰岛中 PLAP(+)IN(+)细胞的比例增加,并鉴定出了胰岛中的潜在前体细胞。我们推测,PLAP(+)IN(-)前体细胞分化为胰岛素阳性细胞,参与衰老过程中β细胞质量的缓慢更新,并补充因损伤而丧失的β细胞。

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