Communications Biology (Jan 2024)

Single-cell transcriptomics enable the characterization of local extension in retinoblastoma

  • Yaoming Liu,
  • Wei Hu,
  • Yanjie Xie,
  • Junjie Tang,
  • Huan Ma,
  • Jinmiao Li,
  • Jiahe Nie,
  • Yinghao Wang,
  • Yang Gao,
  • Chao Cheng,
  • Cheng Li,
  • Yujun Ma,
  • Shicai Su,
  • Zhihui Zhang,
  • Yuekun Bao,
  • Yi Ren,
  • Xinyue Wang,
  • Fengyu Sun,
  • Shengli Li,
  • Rong Lu

DOI
https://doi.org/10.1038/s42003-023-05732-y
Journal volume & issue
Vol. 7, no. 1
pp. 1 – 12

Abstract

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Abstract Retinoblastoma (RB) is the most prevalent ocular tumor of childhood, and its extraocular invasion significantly increases the risk of metastasis. Nevertheless, a single-cell characterization of RB local extension has been lacking. Here, we perform single-cell RNA sequencing on four RB samples (two from intraocular and two from extraocular RB patients), and integrate public datasets of five normal retina samples, four intraocular samples, and three extraocular RB samples to characterize RB local extension at the single-cell level. A total of 128,454 qualified cells are obtained in nine major cell types. Copy number variation inference reveals chromosome 6p amplification in cells derived from extraocular RB samples. In cellular heterogeneity analysis, we identified 10, 8, and 7 cell subpopulations in cone precursor like cells, retinoma like cells, and MKI67+ photoreceptorness decreased (MKI67+ PhrD) cells, respectively. A high expression level of SOX4 was detected in cells from extraocular samples, especially in MKI67+ PhrD cells, which was verified in additional clinical RB samples. These results suggest that SOX4 might drive RB local extension. Our study presents a single-cell transcriptomic landscape of intraocular and extraocular RB samples, improving our understanding of RB local extension at the single-cell resolution and providing potential therapeutic targets for RB patients.