Author
Listed:
- Kasper Karlsson
(Stanford University School of Medicine
Stanford University School of Medicine
Stanford University School of Medicine
Karolinska Institutet)
- Moritz J. Przybilla
(Stanford University School of Medicine
Wellcome Sanger Institute & University of Cambridge)
- Eran Kotler
(Stanford University School of Medicine
Stanford University School of Medicine)
- Aziz Khan
(Stanford University School of Medicine)
- Hang Xu
(Stanford University School of Medicine
Stanford University School of Medicine
Stanford University School of Medicine)
- Kremena Karagyozova
(Stanford University School of Medicine)
- Alexandra Sockell
(Stanford University School of Medicine)
- Wing H. Wong
(Stanford University School of Medicine)
- Katherine Liu
(Stanford University School of Medicine
Stanford University School of Medicine)
- Amanda Mah
(Stanford University School of Medicine)
- Yuan-Hung Lo
(Stanford University School of Medicine)
- Bingxin Lu
(University College London)
- Kathleen E. Houlahan
(Stanford University School of Medicine
Stanford University School of Medicine
Stanford University School of Medicine)
- Zhicheng Ma
(Stanford University School of Medicine)
- Carlos J. Suarez
(Stanford University School of Medicine)
- Chris P. Barnes
(University College London)
- Calvin J. Kuo
(Stanford University School of Medicine)
- Christina Curtis
(Stanford University School of Medicine
Stanford University School of Medicine
Stanford University School of Medicine
Stanford University School of Medicine)
Abstract
The earliest events during human tumour initiation, although poorly characterized, may hold clues to malignancy detection and prevention1. Here we model occult preneoplasia by biallelic inactivation of TP53, a common early event in gastric cancer, in human gastric organoids. Causal relationships between this initiating genetic lesion and resulting phenotypes were established using experimental evolution in multiple clonally derived cultures over 2 years. TP53 loss elicited progressive aneuploidy, including copy number alterations and structural variants prevalent in gastric cancers, with evident preferred orders. Longitudinal single-cell sequencing of TP53-deficient gastric organoids similarly indicates progression towards malignant transcriptional programmes. Moreover, high-throughput lineage tracing with expressed cellular barcodes demonstrates reproducible dynamics whereby initially rare subclones with shared transcriptional programmes repeatedly attain clonal dominance. This powerful platform for experimental evolution exposes stringent selection, clonal interference and a marked degree of phenotypic convergence in premalignant epithelial organoids. These data imply predictability in the earliest stages of tumorigenesis and show evolutionary constraints and barriers to malignant transformation, with implications for earlier detection and interception of aggressive, genome-instable tumours.
Suggested Citation
Kasper Karlsson & Moritz J. Przybilla & Eran Kotler & Aziz Khan & Hang Xu & Kremena Karagyozova & Alexandra Sockell & Wing H. Wong & Katherine Liu & Amanda Mah & Yuan-Hung Lo & Bingxin Lu & Kathleen E, 2023.
"Deterministic evolution and stringent selection during preneoplasia,"
Nature, Nature, vol. 618(7964), pages 383-393, June.
Handle:
RePEc:nat:nature:v:618:y:2023:i:7964:d:10.1038_s41586-023-06102-8
DOI: 10.1038/s41586-023-06102-8
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