首页> 外文期刊>Journal of Clinical Pathology >Loss of BCL-2 in the progression of oral cancer is not attributable to mutations.
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Loss of BCL-2 in the progression of oral cancer is not attributable to mutations.

机译:口腔癌进展过程中BCL-2的丢失并非归因于突变。

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BACKGROUND: BCL-2 and BAX are important in the regulation of apoptosis. There have been reports of loss of BCL-2 in basal cells of oral epithelial dysplasia (OED) and in oral squamous cell carcinoma (OSCC), and suppression of BAX in poorly differentiated OSCC. AIM: To investigate whether loss of BCL-2 in OED and OSCC, and of BAX in poorly differentiated OSCC could be attributed to BCL-2 and BAX mutations. METHODS: Immunohistochemistry and in situ hybridisation were used to confirm BCL-2 and BAX expression. DNA was extracted from archival samples of OED (n = 22) and OSCC (n = 28). The connective tissue part from each section was collected separately and used as the normal reference. RESULTS: No mutations were detected in BCL-2 or BAX that could explain their aberrant expression at the mRNA and protein levels in OED and OSCC. The reported A/G polymorphism at codon 7 of BCL-2 was detected in 18 of 50 samples and a novel C/T polymorphism at codon 100 was detected in three of 50 samples. CONCLUSIONS: No mutations were found that could explain loss of BCL-2 in oral dysplasia and carcinoma. An unreported C/T polymorphism in BCL-2 was detected. Downregulation of BCL-2 in OED and OSCC may be the result of transcriptional regulation.
机译:背景:BCL-2和BAX在细胞凋亡的调控中很重要。有报告说口腔上皮发育不良(OED)和口腔鳞状细胞癌(OSCC)的基底细胞中BCL-2的丢失,以及在分化较差的OSCC中BAX的抑制。目的:研究OED和OSCC中BCL-2的丢失以及低分化OSCC中BAX的丢失是否可归因于BCL-2和BAX突变。方法:采用免疫组织化学和原位杂交技术确定BCL-2和BAX的表达。从OED(n = 22)和OSCC(n = 28)的存档样本中提取DNA。分别收集每个切片的结缔组织部分,并用作正常参考。结果:在BCL-2或BAX中未检测到任何突变,可以解释它们在OED和OSCC的mRNA和蛋白水平上的异常表达。在50个样品中的18个中检测到报告的BCL-2密码子7位的A / G多态性,在50个样品中的三个中检测到100个密码子的新C / T多态性。结论:没有发现突变可以解释口腔发育不良和癌中BCL-2的丢失。在BCL-2中检测到未报告的C / T多态性。 OED和OSCC中BCL-2的下调可能是转录调控的结果。

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