TMEM176A基因甲基化是胃癌诊断的分子标志物

目的研究TMEM176A基因在人胃癌中的甲基化情况及其临床意义。方法应用甲基化特异性PCR技术对209例胃癌组织进行分析。用癌症基因组图谱(TCGA)数据库进一步分析TMEM176A的表达受甲基化调控。结果TCGA数据库分析发现,TMEM176A的表达与K450甲基化芯片结果显示的启动子区的18个CpG位点甲基化呈负相关(R=-0.622,P<0.0001)。甲基化特异性PCR检测发现,TMEM176A在胃癌中的甲基化率为68.42%(143/209),TMEM176A甲基化与淋巴结转移相关(P<0.05)。结论TMEM176A在胃癌中频繁发生甲基化,TMEM176A基因的表达受启动子区甲基化的调控,TMEM176A基因是潜在的胃癌诊断和预后标志物。

TMEM176B调控乳腺癌凋亡作用及机制研究

目的:研究跨膜蛋白176B (Transmembrane protein 176B, TMEM176B)在乳腺癌中凋亡作用及机制。方法:qRT-PCR、western blot法检测乳腺癌组织中TMEM176B表达;小分子干扰RNA和干扰TMEM176B后研究其作用和分子机制。MTT法和CCK8实验检测乳腺癌细胞生长情况;流式细胞实验检测乳腺癌凋亡作用。结果:干扰TMEM176B后明显抑制乳腺癌活力和诱导乳腺癌凋亡,抑制细胞增殖蛋白Ki67表达,且下调抑凋亡蛋白Bcl-2和上调促凋亡蛋白Bax表达水平。在机制方面,我们发现干扰TMEM176B后下调p53表达和p-AKT水平。结论:TMEM176B通过调控p53表达和p-AKT水平进而调控乳腺癌凋亡作用。

A subpopulation of CD146^(+) macrophages enhances antitumor immunity by activating the NLRP3 inflammasome

As one of the main tumor-infiltrating immune cell types, tumor-associated macrophages (TAMs) determine the efficacy of immunotherapy. However, limited knowledge about their phenotypically and functionally heterogeneous nature restricts their application in tumor immunotherapy. In this study, we identified a subpopulation of CD146+ TAMs that exerted antitumor activity in both human samples and animal models. CD146 expression in TAMs was negatively controlled by STAT3 signaling. Reducing this population of TAMs promoted tumor development by facilitating myeloid-derived suppressor cell recruitment via activation of JNK signaling. Interestingly, CD146 was involved in the NLRP3 inflammasome-mediated activation of macrophages in the tumor microenvironment, partially by inhibiting transmembrane protein 176B (TMEM176B), an immunoregulatory cation channel. Treatment with a TMEM176B inhibitor enhanced the antitumor activity of CD146+ TAMs. These data reveal a crucial antitumor role of CD146+ TAMs and highlight the promising immunotherapeutic approach of inhibiting CD146 and TMEM176B.