Thoracic Cancer (May 2022)

Intratumoral genetic and immune microenvironmental heterogeneity in T4N0M0 (diameter ≥ 7 cm) non‐small cell lung cancers

  • Jia−Tao Zhang,
  • Song Dong,
  • Li−Yan Ji,
  • Jia−Ying Zhou,
  • Zhi− Hong Chen,
  • Jian Su,
  • Qing−Ge Zhu,
  • Meng−Min Wang,
  • E−E. Ke,
  • Hao Sun,
  • Xue−Tao Li,
  • Jin−Ji Yang,
  • Qing Zhou,
  • Xu− Chao Zhang,
  • Xuan Gao,
  • Xue−Ning Yang,
  • Xuefeng Xia,
  • Xin Yi,
  • Wen−Zhao Zhong,
  • Yi−Long Wu

DOI
https://doi.org/10.1111/1759-7714.14393
Journal volume & issue
Vol. 13, no. 9
pp. 1333 – 1341

Abstract

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Abstract Background Starting with low metastatic capability, T4N0M0 (diameter ≥ 7 cm) non‐small cell lung cancers (NSCLCs) constitute a unique tumor subset, as with a large tumor size but no regional or distant metastases. We systematically investigated intratumoral heterogeneity, clonal structure, chromosomal instability (CIN), and immune microenvironment in T4N0M0 (≥7 cm) NSCLCs. Methods Whole‐exome sequencing, RNA sequencing, and multiplex immunohistochemistry (mIHC) staining were conducted to analyze 24 spatially segregated tumor samples from eight patients who were pathologically diagnosed with T4N0M0 (diameter ≥ 7 cm) NSCLCs. The adjacent normal tissues and peripheral blood served as controls. Results In total, 35.2% of mutations and 91.1% of somatic copy number alterations were classified as subclonal events, which exhibited widespread genetic intratumoral heterogeneity. In contrast, a low degree of CIN was observed. None of the patients had genome doubling. The burden of loss of heterozygosity, aneuploidy, and the genome instability index of these tumors were significantly lower than those in the TRACERx cohort. Expression profiles revealed significantly upregulated expression of cell division‐related signals and the G2/M checkpoint pathway. In addition, a similar expression pattern of the immune microenvironment was observed in different regions of the tumor, which was confirmed by mIHC profiles. Conclusions Our study indicates the presence of intratumoral genetic heterogeneity and immune microenvironmental heterogeneity features in T4N0M0 NSCLCs, and the low degree of CIN may be related to the low metastatic capability.

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