CT45A1介导的MLC2 (MYL9)磷酸化促进了细胞内结构中自然杀伤细胞的抵抗力和外层细胞的命运,从而加剧了微卫星不稳定性高的结直肠癌的进展。

IF 6.6 2区 医学 Q1 Biochemistry, Genetics and Molecular Biology Molecular Oncology Pub Date : 2024-09-25 DOI:10.1002/1878-0261.13736
Hao-Wei Teng, Hsiang-Yueh Huang, Chun-Chi Lin, Yuh-Ching Twu, Wen-Hao Yang, Wen-Chun Lin, Hsin-Yi Lan, Yen-Yu Lin, Wei-Lun Hwang
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引用次数: 0

摘要

微卫星不稳定性高(MSI-H)结直肠癌(CRC)患者具有较高的肿瘤突变负荷和肿瘤免疫原性,对免疫疗法的反应率较高,生存率也较高。然而,部分 MSI-H CRC 患者仍会出现不良的疾病预后。我们的目标是找出决定这些异质性临床结果的肿瘤自主调控因子。我们利用癌症基因组图谱(TCGA)数据集来鉴定MSI-H型CRC患者中不良预后的调控因子。建立了表达靶向调节因子的稳定的 CRC 肿瘤克隆,以评估迁移和干性特性、免疫细胞的脆弱性以及细胞内结构(CIC)的形成。利用 RNA 序列分析(RNA-seq)确定了稳定 CRC 肿瘤克隆中富集的生物通路。我们对福尔马林固定石蜡包埋(FFPE)的MSI-H CRC标本进行了临床病理学鉴定,以探索其中的潜在机制。我们发现,癌症/睾丸抗原家族 45 成员 A1(CT45A1)的表达在 MSI-H CRC 患者中上调,而这些患者的生存预后较差。表达 CT45A1 的微卫星稳定(MSS)CRC 细胞显示出更强的迁移能力。然而,表达 CT45A1 的 MSI-H CRC 细胞(而非 MSS CRC 细胞)对自然杀伤细胞(NK)的细胞毒性表现出更强的抵抗力,并在同型 CIC 结构中充当外层细胞,阻止外源性或治疗性抗体进入内部 CRC 细胞。用小分子抑制剂或靶向肌球蛋白轻链激酶(MYLK)的短发夹RNA(shRNA)使RHO-ROCK/MLCK-MLC2信号失活,可消除NK细胞的抗药性,并减少表达CT45A1的MSI-H CRC细胞的外层细胞命运。在MSI-H CRC患者中,CT45A1阳性肿瘤表现出MLC2磷酸化增加、外层细胞命运增加和存活率降低。我们证明了CT45A1能促进MSI-H CRC的晚期进展,而靶向MLC2磷酸化可提高CT45A1阳性MSI-H CRC患者的免疫疗法疗效。
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CT45A1-mediated MLC2 (MYL9) phosphorylation promotes natural killer cell resistance and outer cell fate in a cell-in-cell structure, potentiating the progression of microsatellite instability-high colorectal cancer.

Patients with microsatellite instability-high (MSI-H) colorectal cancer (CRC) have high tumor mutation burden and tumor immunogenicity, exhibiting a higher response rate to immunotherapy and better survival. However, a portion of MSI-H CRC patients still experience adverse disease outcomes. We aimed to identify the tumor-autonomous regulators determining these heterogeneous clinical outcomes. The Cancer Genome Atlas (TCGA) dataset was used to identify regulators in MSI-H CRC patients with unfavorable outcomes. Stable CRC tumor clones expressing targeted regulators were established to evaluate migratory and stemness properties, immune cell vulnerability, and cell-in-cell (CIC) structure formation. RNA-sequencing (RNA-seq) was used to identify enriched biological pathways in stable CRC tumor clones. Clinicopathological characterization of formalin-fixed paraffin-embedded (FFPE) MSI-H CRC specimens was performed to explore the underlying mechanisms involved. We showed that cancer/testis antigen family 45 member A1 (CT45A1) expression was upregulated in MSI-H CRC patients with poor survival outcomes. CT45A1-expressing microsatellite stable (MSS) CRC cells showed enhanced migratory ability. However, CT45A1-expressing MSI-H CRC cells, but not MSS CRC cells, showed higher resistance to natural killer (NK) cell cytotoxicity and served as outer cells in homotypic CIC structures, preventing exogenous or therapeutic antibody access to inner CRC cells. Inactivating RHO-ROCK/MLCK-MLC2 signaling with small-molecule inhibitors or short-hairpin RNAs (shRNAs) targeting myosin light chain kinase (MYLK) abolished NK cell resistance and reduced the outer cell fate of CT45A1-expressing MSI-H CRC cells. In MSI-H CRC patients, CT45A1-positive tumors exhibited increased MLC2 phosphorylation, increased outer cell fate, and decreased survival. We demonstrated that CT45A1 potentiates the advanced progression of MSI-H CRC, and targeting MLC2 phosphorylation may enhance immunotherapy efficacy in CT45A1-positive MSI-H CRC patients.

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来源期刊
Molecular Oncology
Molecular Oncology Biochemistry, Genetics and Molecular Biology-Molecular Medicine
CiteScore
11.80
自引率
1.50%
发文量
203
审稿时长
10 weeks
期刊介绍: Molecular Oncology highlights new discoveries, approaches, and technical developments, in basic, clinical and discovery-driven translational cancer research. It publishes research articles, reviews (by invitation only), and timely science policy articles. The journal is now fully Open Access with all articles published over the past 10 years freely available.
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