Author
Listed:
- Mirazul Islam
(Vanderbilt University Medical Center
Vanderbilt University)
- Yilin Yang
(Vanderbilt University Medical Center
Vanderbilt University)
- Alan J. Simmons
(Vanderbilt University Medical Center
Vanderbilt University)
- Vishal M. Shah
(Vanderbilt University Medical Center
Vanderbilt University)
- Krushna Pavan Musale
(Indian Institute of Technology Kanpur)
- Yanwen Xu
(Vanderbilt University Medical Center
Vanderbilt University)
- Naila Tasneem
(Vanderbilt University Medical Center
Vanderbilt University)
- Zhengyi Chen
(Vanderbilt University Medical Center
Vanderbilt University)
- Linh T. Trinh
(Vanderbilt University
Vanderbilt University)
- Paola Molina
(Vanderbilt University)
- Marisol A. Ramirez-Solano
(Vanderbilt University Medical Center
Vanderbilt University Medical Center)
- Iannish D. Sadien
(University of Cambridge)
- Jinzhuang Dou
(The University of Texas MD Anderson Cancer Center)
- Andrea Rolong
(Vanderbilt University Medical Center
Vanderbilt University)
- Ken Chen
(The University of Texas MD Anderson Cancer Center)
- Mark A. Magnuson
(Vanderbilt University
Vanderbilt University
Vanderbilt University)
- Jeffrey C. Rathmell
(Vanderbilt University Medical Center
Vanderbilt University Medical Center)
- Ian G. Macara
(Vanderbilt University Medical Center
Vanderbilt University)
- Douglas J. Winton
(University of Cambridge)
- Qi Liu
(Vanderbilt University Medical Center
Vanderbilt University Medical Center)
- Hamim Zafar
(Indian Institute of Technology Kanpur
Indian Institute of Technology Kanpur)
- Reza Kalhor
(Johns Hopkins University School of Medicine)
- George M. Church
(Harvard Medical School
Harvard University)
- Martha J. Shrubsole
(Vanderbilt University Medical Center
Vanderbilt University Medical Center)
- Robert J. Coffey
(Vanderbilt University Medical Center
Vanderbilt University
Vanderbilt University
Vanderbilt University Medical Center)
- Ken S. Lau
(Vanderbilt University Medical Center
Vanderbilt University
Vanderbilt University
Vanderbilt University)
Abstract
Temporal ordering of cellular events offers fundamental insights into biological phenomena. Although this is traditionally achieved through continuous direct observations1,2, an alternative solution leverages irreversible genetic changes, such as naturally occurring mutations, to create indelible marks that enables retrospective temporal ordering3–5. Using a multipurpose, single-cell CRISPR platform, we developed a molecular clock approach to record the timing of cellular events and clonality in vivo, with incorporation of cell state and lineage information. Using this approach, we uncovered precise timing of tissue-specific cell expansion during mouse embryonic development, unconventional developmental relationships between cell types and new epithelial progenitor states by their unique genetic histories. Analysis of mouse adenomas, coupled to multiomic and single-cell profiling of human precancers, with clonal analysis of 418 human polyps, demonstrated the occurrence of polyclonal initiation in 15–30% of colonic precancers, showing their origins from multiple normal founders. Our study presents a multimodal framework that lays the foundation for in vivo recording, integrating synthetic or natural indelible genetic changes with single-cell analyses, to explore the origins and timing of development and tumorigenesis in mammalian systems.
Suggested Citation
Mirazul Islam & Yilin Yang & Alan J. Simmons & Vishal M. Shah & Krushna Pavan Musale & Yanwen Xu & Naila Tasneem & Zhengyi Chen & Linh T. Trinh & Paola Molina & Marisol A. Ramirez-Solano & Iannish D. , 2024.
"Temporal recording of mammalian development and precancer,"
Nature, Nature, vol. 634(8036), pages 1187-1195, October.
Handle:
RePEc:nat:nature:v:634:y:2024:i:8036:d:10.1038_s41586-024-07954-4
DOI: 10.1038/s41586-024-07954-4
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