Authors
Francis Blokzijl, Joep De Ligt, Myrthe Jager, Valentina Sasselli, Sophie Roerink, Nobuo Sasaki, Meritxell Huch, Sander Boymans, Ewart Kuijk, Pjotr Prins, Isaac J Nijman, Inigo Martincorena, Michal Mokry, Caroline L Wiegerinck, Sabine Middendorp, Toshiro Sato, Gerald Schwank, Edward ES Nieuwenhuis, Monique MA Verstegen, Luc JW Van Der Laan, Jeroen De Jonge, Jan NM IJzermans, Robert G Vries, Marc Van De Wetering, Michael R Stratton, Hans Clevers, Edwin Cuppen, Ruben Van Boxtel
Publication date
2016/10/13
Journal
Nature
Volume
538
Issue
7624
Pages
260-264
Publisher
Nature Publishing Group UK
Description
The gradual accumulation of genetic mutations in human adult stem cells (ASCs) during life is associated with various age-related diseases, including cancer,. Extreme variation in cancer risk across tissues was recently proposed to depend on the lifetime number of ASC divisions, owing to unavoidable random mutations that arise during DNA replication. However, the rates and patterns of mutations in normal ASCs remain unknown. Here we determine genome-wide mutation patterns in ASCs of the small intestine, colon and liver of human donors with ages ranging from 3 to 87 years by sequencing clonal organoid cultures derived from primary multipotent cells,,. Our results show that mutations accumulate steadily over time in all of the assessed tissue types, at a rate of approximately 40 novel mutations per year, despite the large variation in cancer incidence among these tissues. Liver ASCs, however, have …
Scholar articles
F Blokzijl, J De Ligt, M Jager, V Sasselli, S Roerink… - Nature, 2016