Literature DB >> 30209232

Human-like Cmah inactivation in mice increases running endurance and decreases muscle fatigability: implications for human evolution.

Jonathan Okerblom1,2,3,4, William Fletes2,3,5, Hemal H Patel6,7, Simon Schenk8, Ajit Varki9,2,3,4, Ellen C Breen3.   

Abstract

Compared to other primates, humans are exceptional long-distance runners, a feature that emerged in genus Homo approximately 2 Ma and is classically attributed to anatomical and physiological adaptations such as an enlarged gluteus maximus and improved heat dissipation. However, no underlying genetic changes have currently been defined. Two to three million years ago, an exon deletion in the CMP-Neu5Ac hydroxylase (CMAH) gene also became fixed in our ancestral lineage. Cmah loss in mice exacerbates disease severity in multiple mouse models for muscular dystrophy, a finding only partially attributed to differences in immune reactivity. We evaluated the exercise capacity of Cmah-/- mice and observed an increased performance during forced treadmill testing and after 15 days of voluntary wheel running. Cmah-/- hindlimb muscle exhibited more capillaries and a greater fatigue resistance in situ Maximal coupled respiration was also higher in Cmah null mice ex vivo and relevant differences in metabolic pathways were also noted. Taken together, these data suggest that CMAH loss contributes to an improved skeletal muscle capacity for oxygen use. If translatable to humans, CMAH loss could have provided a selective advantage for ancestral Homo during the transition from forest dwelling to increased resource exploration and hunter/gatherer behaviour in the open savannah.
© 2018 The Author(s).

Entities:  

Keywords:  evolution; human; hunting; running

Mesh:

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Year:  2018        PMID: 30209232      PMCID: PMC6158528          DOI: 10.1098/rspb.2018.1656

Source DB:  PubMed          Journal:  Proc Biol Sci        ISSN: 0962-8452            Impact factor:   5.349


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2.  Human-like Cmah inactivation in mice increases running endurance and decreases muscle fatigability: implications for human evolution.

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