Spatial multi-omics unveils the monoclonal origin, neuroendocrine plasticity, and microenvironment niches in combined small-cell lung cancer.

Publication Title

Cell Rep Med

Authors

• Zhuo Wang
• Qing Luo
• Jie Wu
• Li Lu
• Wenjie Ding
• Yichun Zhao
• Yongfeng Yu
• Ruoran Qiu
• Ling Zhu
• Xinxing Ouyang
• Wendi Xuzhang
• Shun Lu
• Wei Wei, Institute for Systems Biology, Seattle, WA USAFollow
• Qihui Shi
• Ziming Li

Document Type

Article

Publication Date

4-21-2026

Keywords

washington; isb

Abstract

Combined small-cell lung cancer (cSCLC) is an aggressive subtype of SCLC with mixed histologic components. Despite heterogeneity and poorer prognosis than de novo SCLC, cSCLC is managed as SCLC because molecular insight into biology, lineage plasticity, and tumor microenvironment (TME) is limited. We perform spatial whole-exome sequencing, spatial transcriptomics, and single-nucleus RNA sequencing across 19 treatment-naive cSCLC tumors. Different histologic components share a monoclonal origin, whereas divergence associates with distinct mutation and copy-number alteration patterns. Our results define spatially exclusive or interspersed tumor domains with distinct TME and immune landscapes; fibroblast-rich boundaries enriched for an aggressive fibroblast subtype may shape TME and treatment responses. We identify lineage plasticity, including adenocarcinoma-to-SCLC transdifferentiation and SCLC-subtype coexistence, and develop cSCLC Detector, a sensitive mutation-based assay improving cSCLC detection in tissue and liquid biopsies. These findings illuminate cSCLC evolution and heterogeneity, underscoring the need for tailored diagnostic and therapeutic strategies for this aggressive subtype.

Area of Special Interest

Cancer

Specialty/Research Institute

Institute for Systems Biology

Specialty/Research Institute

Oncology

DOI

10.1016/j.xcrm.2026.102741