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Activation of cAMP‐dependent phosphorylation pathways is independent of ROS production during mouse sperm capacitation

Gen L. Takei, Darya A. Tourzani, Bidur Paudel, Pablo E. Visconti

2021Molecular Reproduction and Development28 citationsDOI

Abstract

Abstract Mammalian sperm have to undergo capacitation to fertilize the egg. At the molecular level, capacitation involves cAMP synthesis, protein kinase A activation, and downstream increase in tyrosine phosphorylation. In addition, during capacitation, mammalian sperm actively generate reactive oxygen species (ROS). It has been proposed that ROS modulate phosphorylation pathways; however, the crosstalk between these signaling processes is not well‐understood. In the present study, we used loss‐ and gain‐of‐function approaches to evaluate the interconnection between ROS and phosphorylation. We showed that BSA and HCO 3 − , but not Ca 2+ , in the capacitation media are required for ROS production. The synergic effect of these compounds was neither mediated by HCO 3 − stimulation of cAMP synthesis nor by BSA‐induced cholesterol efflux. The capacitation‐induced ROS generation was blocked in the presence of superoxide dismutase (SOD), catalase, and apocynin. However, none of these compounds affected cAMP‐dependent or tyrosine phosphorylation. On the other hand, the addition of NADPH to the media induced ROS generation in sperm incubated in the absence of BSA and HCO 3 − without upregulating cAMP‐dependent or tyrosine phosphorylation signaling. Most interestingly, catalase, but not SOD, blocked in vitro fertilization suggesting a role for H 2 O 2 in this process.

Topics & Concepts

CapacitationPhosphorylationTyrosine phosphorylationCell biologyBiologyReactive oxygen speciesSignal transductionSuperoxide dismutaseSpermCrosstalkProtein phosphorylationCatalaseBiochemistryProtein kinase AOxidative stressMotilityBotanyPhysicsOpticsSperm and Testicular FunctionReproductive Biology and FertilityOvarian function and disorders