Genetics, Vol. 163, 1527-1532, April 2003, Copyright © 2003

Patterns of Cell Division and the Risk of Cancer

Steven A. Franka, Yoh Iwasab, and Martin A. Nowakc
a Department of Ecology and Evolutionary Biology, University of California, Irvine, California 92697-2525,
b Department of Biology, Kyushu University, Fukuoka 8128581, Japan
c Institute for Advanced Study, Princeton, New Jersey 08540

Corresponding author: Steven A. Frank, University of California, Irvine, CA 92697-2525., safrank{at}uci.edu (E-mail)

Communicating editor: J. B. WALSH

Epidermal and intestinal tissues divide throughout life to replace lost surface cells. These renewing tissues have long-lived basal stem cell lineages that divide many times, each division producing one stem cell and one transit cell. The transit cell divides a limited number of times, producing cells that move up from the basal layer and eventually slough off from the surface. If mutation rates are the same in stem and transit divisions, we show that minimal cancer risk is obtained by using the fewest possible stem divisions subject to the constraints imposed by the need to renew the tissue. In this case, stem cells are a necessary risk imposed by the constraints of tissue architecture. Cairns suggested that stem cells may have lower mutation rates than transit cells do. We develop a mathematical model to study the consequences of different stem and transit mutation rates. Our model shows that stem cell mutation rates two or three orders of magnitude less than transit mutation rates may favor relatively more stem divisions and fewer transit divisions, perhaps explaining how renewing tissues allocate cell divisions between long stem and short transit lineages.





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