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MS4A12 表达降低抑制结肠癌分化并预测早期生存。

Decreased expression of MS4A12 inhibits differentiation and predicts early stage survival in colon cancer.

出版信息

Neoplasma. 2017;64(1):65-73. doi: 10.4149/neo_2017_108.

Abstract

Lack of normal differentiation was considered as a common defect in cancer cells. MS4A12, a colon-specific gene, belongs to MS4A family that plays an important role in differentiation, proliferation and cell cycle regulation. The aim of the study was to investigate MS4A12 role in colon cancer cell differentiation and its prognostic value in colon cancer. We used sodium butyrate (BS) to set up differentiated model of colon cancer cell line LoVo. Cell differentiation was evaluated with ALP activity and E-cadherin. We used BS (4 mmol/L) inducing differentiation of LoVo cell and found after BS treated over 48h MS4A12 variant-1 (one of MS4A12 gene transcripts) as well as ALP and E-cadherin of LoVo cells were all increased significantly. When silence MS4A12 variant-1, the elevation of ALP and E-cadherin in BS-treated cells were all inhibited. Besides, after silence MS4A12 variant-1, the cells showed significant resistances to BS function of induction cell cycle arrest and apoptosis. Survival analysis used GEO datasets GSE39582 and GSE38832 that include 681 distinct colon cancer samples. Log-rank test and Cox's proportional hazards regression were applied to analyzing single and multiple prognostic variables, respectively. In early stage colon cancer, the patients with low MS4A12 expression had a poor survival (HR=1.72; p=0.036), while in advanced stage colon cancer MS412 had little prognostic value (HR=0.89; p=0.601). These results indicated MS4A12 might relate to colon cancer cell differentiation and supposed to be a risk classification marker for early stage colon cancer.

摘要

正常分化的缺失被认为是癌细胞的一个常见缺陷。MS4A12 是一种结肠特异性基因,属于 MS4A 家族,该家族在分化、增殖和细胞周期调控中发挥重要作用。本研究旨在探讨 MS4A12 在结肠癌细胞分化中的作用及其在结肠癌中的预后价值。我们使用丁酸钠(BS)建立结肠癌细胞系 LoVo 的分化模型。通过碱性磷酸酶(ALP)活性和 E-钙黏蛋白评估细胞分化。我们使用 BS(4mmol/L)诱导 LoVo 细胞分化,发现 BS 处理超过 48h 后,MS4A12 变体-1(MS4A12 基因转录本之一)以及 ALP 和 E-钙黏蛋白在 LoVo 细胞中均显著增加。当沉默 MS4A12 变体-1 时,BS 处理细胞中 ALP 和 E-钙黏蛋白的升高均被抑制。此外,沉默 MS4A12 变体-1 后,细胞对 BS 诱导细胞周期阻滞和凋亡的功能表现出明显的抗性。使用包含 681 个不同结肠癌样本的 GEO 数据集 GSE39582 和 GSE38832 进行生存分析。对数秩检验和 Cox 比例风险回归分别用于分析单变量和多变量预后变量。在早期结肠癌中,MS4A12 低表达的患者生存较差(HR=1.72;p=0.036),而在晚期结肠癌中 MS412 预后价值不大(HR=0.89;p=0.601)。这些结果表明 MS4A12 可能与结肠癌细胞分化有关,并可能成为早期结肠癌的风险分类标志物。

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