Nature Communications (Oct 2024)

Inferring replication timing and proliferation dynamics from single-cell DNA sequencing data

  • Adam C. Weiner,
  • Marc J. Williams,
  • Hongyu Shi,
  • Ignacio Vázquez-García,
  • Sohrab Salehi,
  • Nicole Rusk,
  • Samuel Aparicio,
  • Sohrab P. Shah,
  • Andrew McPherson

DOI
https://doi.org/10.1038/s41467-024-52544-7
Journal volume & issue
Vol. 15, no. 1
pp. 1 – 19

Abstract

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Abstract Dysregulated DNA replication is a cause and a consequence of aneuploidy in cancer, yet the interplay between copy number alterations (CNAs), replication timing (RT) and cell cycle dynamics remain understudied in aneuploid tumors. We developed a probabilistic method, PERT, for simultaneous inference of cell-specific replication and copy number states from single-cell whole genome sequencing (scWGS) data. We used PERT to investigate clone-specific RT and proliferation dynamics in >50,000 cells obtained from aneuploid and clonally heterogeneous cell lines, xenografts and primary cancers. We observed bidirectional relationships between RT and CNAs, with CNAs affecting X-inactivation producing the largest RT shifts. Additionally, we found that clone-specific S-phase enrichment positively correlated with ground-truth proliferation rates in genomically stable but not unstable cells. Together, these results demonstrate robust computational identification of S-phase cells from scWGS data, and highlight the importance of RT and cell cycle properties in studying the genomic evolution of aneuploid tumors.