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杂合子 Men1 小鼠 5 周龄时胰岛细胞加速增殖和差异表达的全局基因:Men1 是一个杂合不足的抑制剂。

Accelerated proliferation and differential global gene expression in pancreatic islets of five-week-old heterozygous Men1 mice: Men1 is a haploinsufficient suppressor.

机构信息

Department of Medical Sciences, Science for Life Laboratory, Uppsala University, S-751 85 Uppsala, Sweden.

出版信息

Endocrinology. 2012 Jun;153(6):2588-98. doi: 10.1210/en.2011-1924. Epub 2012 Apr 4.

Abstract

Individuals carrying heterozygous (hz) MEN1 (Multiple Endocrine Neoplasia Syndrome Type 1) germ line mutations develop endocrine tumors as a result of somatic loss of the wild-type (wt) allele. However, endocrine cell proliferation has been observed despite wt allele retention, indicating haploinsufficiency. To study downstream molecular effects of the hz haplotype, a germ line Men1 hz mouse model was used to explore differences in global endocrine pancreatic gene expression. Because islet cells of 5-wk-old hz mice express Menin from the retained wt Men1 allele, these were isolated after collagenase digestion of the pancreas, and used for global gene expression array. Wild-type littermates were used for comparison. Array findings were corroborated by quantitative PCR, Western blotting, in situ proximity ligation assay, and immunohistochemistry. The hz islets show increased proliferation: the Ki-67 index was twice as high as in wt islets (3.48 vs. 1.74%; P = 0.024). The microarray results demonstrated that several genes were differentially expressed. Some selected genes were studied on the protein level, e.g. the cytoskeletal regulator myristoylated alanine-rich protein kinase C substrate (Marcks) was significantly less expressed in hz islets, using in situ proximity ligation assay and Western blotting (P < 0.001 and P < 0.01, respectively). Further, gene ontology analysis showed that genes with higher mRNA expression in the hz endocrine pancreas were associated with e.g. chromatin maintenance and apoptosis. Lower mRNA was observed for genes involved in growth factor binding. In conclusion, despite retained Menin expression, proliferation was accelerated, and numerous genes were differentially expressed in the endocrine pancreas of 5-wk-old hz Men1 mice, corroborating the hypothesis that MEN1 is a haploinsufficient suppressor.

摘要

携带杂合性 (hz) MEN1(多发性内分泌肿瘤综合征 1 型)种系突变的个体由于野生型 (wt) 等位基因的体细胞丢失而发展为内分泌肿瘤。然而,尽管保留了 wt 等位基因,仍观察到内分泌细胞增殖,表明单倍不足。为了研究 hz 单倍型的下游分子效应,使用种系 Men1 hz 小鼠模型来研究全球内分泌胰腺基因表达的差异。由于 5 周龄 hz 小鼠的胰岛细胞从保留的 wt Men1 等位基因表达 Menin,因此在胰腺胶原酶消化后将其分离,并用于全基因表达阵列。野生型同窝仔鼠用于比较。通过定量 PCR、Western 印迹、原位邻近连接测定和免疫组织化学证实了阵列结果。hz 胰岛显示出增加的增殖:Ki-67 指数是 wt 胰岛的两倍(3.48% vs. 1.74%;P=0.024)。微阵列结果表明,有几个基因表达存在差异。选择一些基因在蛋白质水平上进行研究,例如,使用原位邻近连接测定和 Western 印迹,hz 胰岛中肌球蛋白酰化富含丙氨酸的蛋白激酶 C 底物(Marcks)的表达明显降低(P<0.001 和 P<0.01)。此外,基因本体分析表明,hz 内分泌胰腺中 mRNA 表达较高的基因与染色质维持和细胞凋亡等有关。生长因子结合相关的基因的 mRNA 表达降低。总之,尽管保留了 Menin 的表达,但在 5 周龄 hz Men1 小鼠的内分泌胰腺中,增殖加速,并且许多基因的表达存在差异,这支持了 MEN1 是一种单倍不足抑制剂的假说。

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