SPATA33 localizes calcineurin to the mitochondria and regulates sperm motility in mice

Author:

Miyata HaruhikoORCID,Oura SeiyaORCID,Morohoshi AkaneORCID,Shimada KeisukeORCID,Mashiko Daisuke,Oyama Yuki,Kaneda Yuki,Matsumura Takafumi,Abbasi Ferheen,Ikawa MasahitoORCID

Abstract

Calcineurin is a calcium-dependent phosphatase that plays roles in a variety of biological processes including immune responses. In spermatozoa, there is a testis-enriched calcineurin composed of PPP3CC and PPP3R2 (sperm calcineurin) that is essential for sperm motility and male fertility. Because sperm calcineurin has been proposed as a target for reversible male contraceptives, identifying proteins that interact with sperm calcineurin widens the choice for developing specific inhibitors. Here, by screening the calcineurin-interacting PxIxIT consensus motif in silico and analyzing the function of candidate proteins through the generation of gene-modified mice, we discovered that SPATA33 interacts with sperm calcineurin via a PQIIIT sequence. Spata33 knockout mice exhibit reduced sperm motility because of an inflexible midpiece, leading to impaired male fertility, which phenocopies Ppp3cc and Ppp3r2 knockout mice. Further analysis reveals that sperm calcineurin disappears from the mitochondria in the Spata33 knockout testis. In addition, immunoprecipitation analysis indicates that sperm calcineurin interacts with not only SPATA33 but also the mitochondrial protein VDAC2. These results indicate that SPATA33 localizes calcineurin to the mitochondria and regulates sperm motility.

Funder

HHS | NIH | Eunice Kennedy Shriver National Institute of Child Health and Human Development

Takeda Science Foundation

Bill and Melinda Gates Foundation

Japan Agency for Medical Research and Development

MEXT | Japan Society for the Promotion of Science

Publisher

Proceedings of the National Academy of Sciences

Subject

Multidisciplinary

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