Elevated expression of complement factor I in lung cancer cells associates with shorter survival–Potentially via non-canonical mechanism

IF 6.4 2区 医学 Q1 MEDICAL LABORATORY TECHNOLOGY Translational Research Pub Date : 2024-02-22 DOI:10.1016/j.trsl.2024.02.003
Anna Felberg , Michał Bieńkowski , Tomasz Stokowy , Kamil Myszczyński , Zuzanna Polakiewicz , Kamila Kitowska , Rafał Sądej , Frida Mohlin , Alicja Kuźniewska , Daria Kowalska , Grzegorz Stasiłojć , Ilse Jongerius , Robbert Spaapen , Miguel Mesa-Guzman , Luis M. Montuenga , Anna M. Blom , Ruben Pio , Marcin Okrój
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Abstract

While numerous membrane-bound complement inhibitors protect the body's cells from innate immunity's autoaggression, soluble inhibitors like complement factor I (FI) are rarely produced outside the liver. Previously, we reported the expression of FI in non-small cell lung cancer (NSCLC) cell lines. Now, we assessed the content of FI in cancer biopsies from lung cancer patients and associated the results with clinicopathological characteristics and clinical outcomes. Immunohistochemical staining intensity did not correlate with age, smoking status, tumor size, stage, differentiation grade, and T cell infiltrates, but was associated with progression-free survival (PFS), overall survival (OS) and disease-specific survival (DSS). Multivariate Cox analysis of low vs. high FI content revealed HR 0.55, 95 % CI 0.32-0.95, p=0.031 for PFS, HR 0.51, 95 % CI 0.25-1.02, p=0.055 for OS, and HR 0.32, 95 % CI 0.12-0.84, p=0.021 for DSS. Unfavorable prognosis might stem from the non-canonical role of FI, as the staining pattern did not correlate with C4d - the product of FI-supported degradation of active complement component C4b. To elucidate that, we engineered three human NSCLC cell lines naturally expressing FI with CRISPR/Cas9 technology, and compared the transcriptome of FI-deficient and FI-sufficient clones in each cell line. RNA sequencing revealed differentially expressed genes engaged in intracellular signaling pathways controlling proliferation, apoptosis, and responsiveness to growth factors. Moreover, in vitro colony-formation assays showed that FI-deficient cells formed smaller foci than FI-sufficient NSCLC cells, but their size increased when purified FI protein was added to the medium. We postulate that a non-canonical activity of FI influences cellular physiology and contributes to the poor prognosis of lung cancer patients.

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补体因子 I 在肺癌细胞中的高表达与生存期缩短有关--可能是通过非经典机制。
虽然有许多膜结合的补体结合抑制剂能保护人体细胞免受先天性免疫的自身侵害,但像补体因子 I(FI)这样的可溶性抑制剂却很少在肝脏外产生。此前,我们曾报道过 FI 在非小细胞肺癌(NSCLC)细胞系中的表达。现在,我们评估了肺癌患者癌症活检组织中 FI 的含量,并将评估结果与临床病理特征和临床预后联系起来。免疫组化染色强度与年龄、吸烟状况、肿瘤大小、分期、分化等级和T细胞浸润无关,但与无进展生存期(PFS)、总生存期(OS)和疾病特异性生存期(DSS)相关。FI含量高与低的多变量Cox分析显示,PFS的HR为0.55,95% CI为0.32-0.95,p=0.031;OS的HR为0.51,95% CI为0.25-1.02,p=0.055;DSS的HR为0.32,95% CI为0.12-0.84,p=0.021。不利的预后可能源于FI的非典型作用,因为染色模式与C4d(FI支持的活性补体成分C4b降解产物)不相关。为了阐明这一点,我们利用CRISPR/Cas9技术设计了三种天然表达FI的人类NSCLC细胞系,并比较了每种细胞系中FI缺陷和FI充足克隆的转录组。RNA测序发现了细胞内控制增殖、凋亡和对生长因子反应的信号通路中的不同表达基因。此外,体外集落形成试验表明,FI缺乏的细胞形成的病灶比FI充足的NSCLC细胞小,但当在培养基中加入纯化的FI蛋白时,它们的体积会增大。我们推测,FI的非经典活性会影响细胞生理,并导致肺癌患者预后不良。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Translational Research
Translational Research 医学-医学:内科
CiteScore
15.70
自引率
0.00%
发文量
195
审稿时长
14 days
期刊介绍: Translational Research (formerly The Journal of Laboratory and Clinical Medicine) delivers original investigations in the broad fields of laboratory, clinical, and public health research. Published monthly since 1915, it keeps readers up-to-date on significant biomedical research from all subspecialties of medicine.
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Contents Contents Masthead Lympho-myeloid aggregate-infiltrating CD20+ B cells display a double-negative phenotype and correlate with poor prognosis in esophageal squamous cell carcinoma Editorial Advisory Board
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