首页> 外文期刊>Journal of cellular and molecular medicine. >Kit K641E oncogene up-regulates Sprouty homolog 4 and Trophoblast glycoprotein in interstitial cells of Cajal in a murine model of gastrointestinal stromal tumours
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Kit K641E oncogene up-regulates Sprouty homolog 4 and Trophoblast glycoprotein in interstitial cells of Cajal in a murine model of gastrointestinal stromal tumours

机译:试剂盒K641E癌基因在胃肠道间质瘤小鼠模型中上调Cajal间质细胞中的Sprouty同源物4和滋养层糖蛋白

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Gastrointestinal stromal tumours (GIST) are thought to derive from the interstitial cells of Cajal (ICC) or an ICC precursor. Oncogenic mutations of the receptor tyrosine kinase KIT are present in most GIST. KIT K642E was originally identified in sporadic GIST and later found in the germ line of a familial GIST cohort. A mouse model harbouring a germline Kit K641E mutant was created to model familial GIST. The expression profile was investigated in the gastric antrum of the Kit K641E murine GIST model by microarray, quantitative PCR and immunofluorescence. Gja1/Cx43 , Gpc6 , Gpr133 , Pacrg , Pde3a , Prkar2b , Prkcq/Pkce , Rasd2 , Spry4 and Tpbg/5T4 were found to be up-regulated. The proteins encoded by Gja1/Cx43 , Pde3a , Prkcq/Pkce were localized in Kit-ir ICC in wild-type and Kit K641E animals while Spry4 and Tpbg/5T4 were detected in Kit-ir cells only in Kit K641E , but not in Kit WT/WT animals. Most up-regulated genes in this mouse model belong to the gene expression profile of human GIST but also to the profile of normal Kit + ICC in the mouse small intestine. Spry4 and Tpbg/5T4 may represent candidates for targeted therapeutic approaches in GIST with oncogenic KIT mutations.
机译:胃肠道间质瘤(GIST)被认为是来自Cajal(ICC)或ICC前体的间质细胞。大多数GIST中都存在受体酪氨酸激酶KIT的致癌突变。 KIT K642E最初在零星的GIST中鉴定,后来在家族GIST队列的种系中发现。创建了带有种系试剂盒K641E突变体的小鼠模型来模拟家族性GIST。用芯片,定量PCR和免疫荧光技术研究了 K641E Kit GIST小鼠胃窦的表达情况。发现Gja1 / Cx43,Gpc6,Gpr133,Pacrg,Pde3a,Prkar2b,Prkcq / Pkce,Rasd2,Spry4和Tpbg / 5T4被上调。 Gja1 / Cx43,Pde3a,Prkcq / Pkce编码的蛋白位于野生型和Kit K641E 动物的Kit-ir ICC中,而仅在Kit-ir细胞中检测到Spry4和Tpbg / 5T4。套件 K641E ,但不适用于套件 WT / WT 动物。该小鼠模型中大多数上调的基因属于人GIST的基因表达谱,也属于小鼠小肠中正常Kit + ICC的谱。 Spry4和Tpbg / 5T4可能代表具有致癌性KIT突变的GIST靶向治疗方法的候选人。

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