Pleiotropic constraints promote the evolution of cooperation in cellular groups.
Michael A BentleyChristian A YatesJotun HeinGail M PrestonKevin R FosterPublished in: PLoS biology (2022)
The evolution of cooperation in cellular groups is threatened by lineages of cheaters that proliferate at the expense of the group. These cell lineages occur within microbial communities, and multicellular organisms in the form of tumours and cancer. In contrast to an earlier study, here we show how the evolution of pleiotropic genetic architectures-which link the expression of cooperative and private traits-can protect against cheater lineages and allow cooperation to evolve. We develop an age-structured model of cellular groups and show that cooperation breaks down more slowly within groups that tie expression to a private trait than in groups that do not. We then show that this results in group selection for pleiotropy, which strongly promotes cooperation by limiting the emergence of cheater lineages. These results predict that pleiotropy will rapidly evolve, so long as groups persist long enough for cheater lineages to threaten cooperation. Our results hold when pleiotropic links can be undermined by mutations, when pleiotropy is itself costly, and in mixed-genotype groups such as those that occur in microbes. Finally, we consider features of multicellular organisms-a germ line and delayed reproductive maturity-and show that pleiotropy is again predicted to be important for maintaining cooperation. The study of cancer in multicellular organisms provides the best evidence for pleiotropic constraints, where abberant cell proliferation is linked to apoptosis, senescence, and terminal differentiation. Alongside development from a single cell, we propose that the evolution of pleiotropic constraints has been critical for cooperation in many cellular groups.
Keyphrases
- single cell
- cell proliferation
- healthcare
- poor prognosis
- genome wide
- oxidative stress
- magnetic resonance
- papillary thyroid
- endothelial cells
- young adults
- gene expression
- dna methylation
- gram negative
- cell cycle
- long non coding rna
- signaling pathway
- squamous cell
- mesenchymal stem cells
- bone marrow
- multidrug resistant
- cell cycle arrest
- pi k akt
- contrast enhanced