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杀伤细胞凝集素样受体 G2 通过双重激活 ERK1/2 和 JAK/STAT 通路促进胃癌细胞的侵袭表型。

Killer cell lectin-like receptor G2 facilitates aggressive phenotypes of gastric cancer cells via dual activation of the ERK1/2 and JAK/STAT pathways.

机构信息

Department of Gastroenterological Surgery, Nagoya University Graduate School of Medicine, 65 Tsurumai-Cho, Showa-Ku, Nagoya, 466-8550, Japan.

出版信息

Gastric Cancer. 2024 May;27(3):506-518. doi: 10.1007/s10120-024-01480-y. Epub 2024 Feb 22.

DOI:10.1007/s10120-024-01480-y
PMID:38386237
Abstract

BACKGROUND

Advanced gastric cancer (GC) has a poor prognosis. This study aimed to identify novel GC-related genes as potential therapeutic targets.

METHODS

Killer cell lectin-like receptor G2 (KLRG2) was identified as a candidate gene by transcriptome analysis of metastatic GC tissues. Small interfering RNA-mediated KLRG2 knockdown in human GC cell lines was used to investigate KLRG2 involvement in signaling pathways and functional behaviors in vitro and in vivo. Clinicopathological data were analyzed in patients stratified according to tumor KLRG2 mRNA expression.

RESULTS

KLRG2 knockdown in GC cells decreased cell proliferation, migration, and invasion; caused cell cycle arrest in G/M phase; induced apoptosis via caspase activation; suppressed JAK/STAT and MAPK-ERK1/2 pathway activities; and upregulated p53 and p38 MAPK activities. In mouse xenograft models of peritoneal metastasis, the number and weight of disseminated GC nodules were decreased by KLRG2 knockdown. High tumor levels of KLRG2 mRNA were significantly associated with lower 5-year overall survival (OS) and relapse-free survival (RFS) rates in patients with Stage I-III GC (5-year OS rate: 64.4% vs. 80.0%, P = 0.009; 5-year RFS rate: 62.8% vs. 78.1%, P = 0.030).

CONCLUSIONS

KLRG2 knockdown attenuated the malignant phenotypes of GC cells via downregulation of JAK/STAT and MAPK-ERK1/2 pathway activity and upregulation of p38 MAPK and p53. Targeted suppression of KLRG2 may serve as a new treatment approach for GC.

摘要

背景

晚期胃癌(GC)预后较差。本研究旨在寻找新的 GC 相关基因作为潜在的治疗靶点。

方法

通过对转移性 GC 组织的转录组分析,确定杀伤细胞凝集素样受体 G2(KLRG2)为候选基因。使用小干扰 RNA 介导的人 GC 细胞系中 KLRG2 敲低,研究 KLRG2 参与体外和体内信号通路和功能行为。根据肿瘤 KLRG2 mRNA 表达对患者进行分层,分析临床病理数据。

结果

GC 细胞中 KLRG2 的敲低降低了细胞增殖、迁移和侵袭能力;导致细胞周期停滞在 G/M 期;通过半胱氨酸天冬氨酸蛋白酶激活诱导细胞凋亡;抑制 JAK/STAT 和 MAPK-ERK1/2 通路活性;并上调 p53 和 p38 MAPK 活性。在 GC 腹膜转移的小鼠异种移植模型中,KLRG2 敲低可减少播散性 GC 结节的数量和重量。肿瘤中 KLRG2 mRNA 水平高与 I-III 期 GC 患者的 5 年总生存率(OS)和无复发生存率(RFS)显著降低相关(5 年 OS 率:64.4%比 80.0%,P=0.009;5 年 RFS 率:62.8%比 78.1%,P=0.030)。

结论

KLRG2 敲低通过下调 JAK/STAT 和 MAPK-ERK1/2 通路活性以及上调 p38 MAPK 和 p53,减弱 GC 细胞的恶性表型。靶向抑制 KLRG2 可能成为 GC 的一种新治疗方法。

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