[ABSTRACT]AIM:Toestablishatransgenicheterozygousmousemodelofprecancerouslesionsofcolorectal cancer with p110δmutation in the C57BL/6J background for serving the studies on colorectal cancer research mediated by p110δ.METHODS:The transgenic heterozygous mice were generated by crossing in p110δD910A/D910A mouse and ApcMin/+mouse, and the genotype was detected by PCR .Compared with ApcMin/+mice, transgenic heterozygous mice ( ApcMin/+;p110δD910A/D910A)were counted, and the number and size of intestine polyps were analyzed after methylene blue staining . The intestinal tissue structure was assessed by HE staining .RESULTS:The transgenic heterozygous mouse model of pre-cancerous lesions of colorectal cancer with p 110δmutation was established .The number and size of polyps in the transgenic heterozygous mice were declined .CONCLUSION: A transgenic heterozygous mouse model of precancerous lesions of colorectal cancer with p 110δmutation was successfully established .The initial phenotype of intestinal tumors in transgenic mice was observed .This model will greatly contribute to the related research of colorectal cancer in mice .%目的:建立p110δ突变失活的ApcMin/+结直肠癌癌前病变小鼠模型,为研究p110δ在小鼠结直肠癌癌前病变中的作用提供实验模型。方法:将C57BL/6J背景的ApcMin/+结直肠癌癌前病变小鼠与p110δ突变失活小鼠(p110δD910A/D910A)进行杂交建系,通过PCR技术鉴定子代小鼠基因型,获得p110δ突变失活的ApcMin/+小鼠。对适龄小鼠进行肠道取材,亚甲蓝染色后,观察肠道结构,对腺瘤和微腺瘤进行统计。肠道组织进行石蜡包埋、切片,做HE染色进行进一步观察。结果:获得p110δ突变失活的ApcMin/+杂交鼠( ApcMin/+;p110δD910A/D910A )并得以稳定传代。 ApcMin/+;p110δD910A/D910A杂交小鼠的肠道组织中,腺瘤数目和体积比ApcMin/+结直肠癌癌前病变小鼠均有减少。结论:成功建立p110δ突变失活的ApcMin/+结直肠癌癌前病变小鼠模型,并得到小鼠肠道肿瘤的初步表型,为进一步研究p110δ在肠道肿瘤发生发展中的作用提供重要的工具动物。
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