Pan-cancer multi-omics profiling of MS4A2 unveils its functional landscape in lung adenocarcinoma

医学 肺癌 腺癌 癌症研究 趋化因子 免疫系统 免疫学 癌症 肿瘤科 内科学
作者
Bitian Zhang,William C. Cho,Ping‐Chung Leung,Chris K.C. Wong,Dongjie Wang
出处
期刊:International Journal of Surgery [Wolters Kluwer]
标识
DOI:10.1097/js9.0000000000002903
摘要

Background: The membrane-spanning 4-domains subfamily A member 2 (MS4A2), a mast cell-specific IgE receptor component, exhibits paradoxical roles in cancer progression. While pan-cancer analyses suggest its context-dependent duality, its prognostic hierarchy across survival metrics—overall survival (OS), disease-specific survival (DSS), progression-free interval (PFI), and disease-free interval (DFI)—remains uncharacterized in lung adenocarcinoma (LUAD). Materials and Methods: We integrated bulk RNA-seq (TCGA/GTEx, 33 cancers) and single-cell transcriptomics (NSCLC cohorts) to map MS4A2’s expression dynamics. Prognostic impacts were quantified through Cox regression and Kaplan-Meier modeling for all four survival endpoints (OS/DSS/PFI/DFI), complemented by immune infiltration and methylation-epigenetic correlation analyses. Drug sensitivity associations were evaluated using GDSC pharmacogenomics. Results: Pan-cancer stratification revealed LUAD-specific prognostic dominance of MS4A2, with elevated expression reducing mortality risk (OS HR = 0.58, DSS HR = 0.61; all p<0.05) and prolonging disease control (PFI HR = 0.59, DFI HR = 0.59; all p<0.05). Single-cell mapping localized MS4A2 to tumor-associated mast cells, where its bidirectional chemokine regulation—suppressing lymphoid homing (CCL19/CCL21) while amplifying myeloid recruitment (CCL20/CXCL8)—orchestrated leukocyte transendothelial migration. Clinically, MS4A2 exhibited female-biased expression (p<0.01) and stage-dependent attenuation (p<0.01), correlating with enhanced sensitivity to 5-fluorouracil and axitinib (p<0.05) in high-expressing tumors despite their immune-evasive traits. Conclusion: By converging multi-omics evidence across four prognostic axes (OS/DSS/PFI/DFI), we redefine MS4A2 as a mast cell-driven gatekeeper of LUAD progression. Its dual chemokine polarization establishes an immunosuppressive niche paradoxically susceptible to cytotoxic agents, proposing a precision stratification framework: MS4A2 high tumors for 5-FU/axitinib regimens combined with immunotherapies to counterbalance microenvironmental resistance. This quad-metric prognostic model advances LUAD management by linking mast cell biology to clinically actionable survival endpoints.
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