Lineage tracing reveals the phylodynamics, plasticity, and paths of tumor evolution
Author(s) -
Dian Yang,
Matthew G. Jones,
Santiago Naranjo,
William M. Rideout,
Kyung Hoi Min,
Raymond Ho,
Wei Wu,
Joseph M. Replogle,
Jennifer L. Page,
Jeffrey J. Quinn,
Felix Horns,
Xiaojie Qiu,
Michael Z. Chen,
William A. Freed-Pastor,
Christopher S. McGinnis,
David M. Patterson,
Zev J. Gartner,
Eric D. Chow,
Trever G. Bivona,
Michelle M. Chan,
Nir Yosef,
Tyler Jacks,
Jonathan S. Weissman
Publication year - 2022
Publication title -
cell
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 26.304
H-Index - 776
eISSN - 1097-4172
pISSN - 0092-8674
DOI - 10.1016/j.cell.2022.04.015
Subject(s) - biology , somatic evolution in cancer , lineage (genetic) , viral phylodynamics , epigenetics , tumor progression , epigenome , phenotype , kras , evolutionary biology , phylogenetic tree , computational biology , genetics , cancer , mutation , gene , dna methylation , gene expression
Tumor evolution is driven by the progressive acquisition of genetic and epigenetic alterations that enable uncontrolled growth and expansion to neighboring and distal tissues. The study of phylogenetic relationships between cancer cells provides key insights into these processes. Here, we introduced an evolving lineage-tracing system with a single-cell RNA-seq readout into a mouse model of Kras;Trp53(KP)-driven lung adenocarcinoma and tracked tumor evolution from single-transformed cells to metastatic tumors at unprecedented resolution. We found that the loss of the initial, stable alveolar-type2-like state was accompanied by a transient increase in plasticity. This was followed by the adoption of distinct transcriptional programs that enable rapid expansion and, ultimately, clonal sweep of stable subclones capable of metastasizing. Finally, tumors develop through stereotypical evolutionary trajectories, and perturbing additional tumor suppressors accelerates progression by creating novel trajectories. Our study elucidates the hierarchical nature of tumor evolution and, more broadly, enables in-depth studies of tumor progression.
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