AI Article Synopsis
- Sperm capacitation involves rearranging the actin cytoskeleton, which is critical for acrosomal exocytosis (AR) in mice.
- The activity of small GTPases RHOA/C and RAC1 is crucial in the initial stages, facilitating phosphorylation of LIMK1 and COFILIN, with RAC1 and PAK4 primarily regulating actin polymerization in the sperm head for AR.
- The Slingshot family of protein phosphatases (SSH1) also plays a role in COFILIN phosphorylation, with its activity regulated by the opposing actions of RHOA/C, RAC1, and certain phosphatases, marking a unique regulatory mechanism in mouse sperm.
Article Abstract
The actin cytoskeleton reorganization during sperm capacitation is essential for the occurrence of acrosomal exocytosis (AR) in several mammalian species. Here, we demonstrate that in mouse sperm, within the first minutes of exposure upon capacitating conditions, the activity of RHOA/C and RAC1 is essential for LIMK1 and COFILIN phosphorylation. However, we observed that the signaling pathway involving RAC1 and PAK4 is the main player in controlling actin polymerization in the sperm head necessary for the occurrence of AR. Moreover, we show that the transient phosphorylation of COFILIN is also influenced by the Slingshot family of protein phosphatases (SSH1). The activity of SSH1 is regulated by the dual action of two pathways. On one hand, RHOA/C and RAC1 activity promotes SSH1 phosphorylation (inactivation). On the other hand, the activating dephosphorylation is driven by okadaic acid-sensitive phosphatases. This regulatory mechanism is independent of the commonly observed activating mechanisms involving PP2B and emerges as a new finely tuned modulation that is, so far, exclusively observed in mouse sperm. However, persistent phosphorylation of COFILIN by SSH1 inhibition or okadaic acid did not altered actin polymerization and the AR. Altogether, our results highlight the role of small GTPases in modulating actin dynamics required for AR.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC9142561 | PMC |
| http://dx.doi.org/10.1016/j.jbc.2022.101988 | DOI Listing |
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