Deficient LRRC8A-dependent volume-regulated anion channel activity is associated with male infertility in mice
Jianqiang Bao, Carlos J. Perez, Jeesun Kim, Huan Zhang, Caitlin J. Murphy, Tewfik Hamidi, Jean Jaubert, Craig D. Platt, Janet Chou, Meichun Deng, Meng-Hua Zhou, Yuying Huang, Héctor Gaitán-Peñas, Jean-Louis Guénet, Kevin Lin, Yue Lu, Taiping Chen, Mark T. Bedford, Sharon Y.R. Dent, John H. Richburg, Raúl Estévez, Hui-Lin Pan, Raif S. Geha, Qinghua Shi, Fernando Benavides
Jianqiang Bao, Carlos J. Perez, Jeesun Kim, Huan Zhang, Caitlin J. Murphy, Tewfik Hamidi, Jean Jaubert, Craig D. Platt, Janet Chou, Meichun Deng, Meng-Hua Zhou, Yuying Huang, Héctor Gaitán-Peñas, Jean-Louis Guénet, Kevin Lin, Yue Lu, Taiping Chen, Mark T. Bedford, Sharon Y.R. Dent, John H. Richburg, Raúl Estévez, Hui-Lin Pan, Raif S. Geha, Qinghua Shi, Fernando Benavides
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Research Article Genetics Reproductive biology

Deficient LRRC8A-dependent volume-regulated anion channel activity is associated with male infertility in mice

Abstract

Ion channel-controlled cell volume regulation is of fundamental significance to the physiological function of sperm. In addition to volume regulation, LRRC8A-dependent volume-regulated anion channel (VRAC) activity is involved in cell cycle progression, insulin signaling, and cisplatin resistance. Nevertheless, the contribution of LRRC8A and its dependent VRAC activity in the germ cell lineage remain unknown. By utilizing a spontaneous Lrrc8a mouse mutation (c.1325delTG, p.F443*) and genetically engineered mouse models, we demonstrate that LRRC8A-dependent VRAC activity is essential for male germ cell development and fertility. Lrrc8a-null male germ cells undergo progressive degeneration independent of the apoptotic pathway during postnatal testicular development. Lrrc8a-deficient mouse sperm exhibit multiple morphological abnormalities of the flagella (MMAF), a feature commonly observed in the sperm of infertile human patients. Importantly, we identified a human patient with a rare LRRC8A hypomorphic mutation (c.1634G>A, p.Arg545His) possibly linked to Sertoli cell–only syndrome (SCOS), a male sterility disorder characterized by the loss of germ cells. Thus, LRRC8A is a critical factor required for germ cell development and volume regulation in the mouse, and it might serve as a novel diagnostic and therapeutic target for SCOS patients.

Authors

Jianqiang Bao, Carlos J. Perez, Jeesun Kim, Huan Zhang, Caitlin J. Murphy, Tewfik Hamidi, Jean Jaubert, Craig D. Platt, Janet Chou, Meichun Deng, Meng-Hua Zhou, Yuying Huang, Héctor Gaitán-Peñas, Jean-Louis Guénet, Kevin Lin, Yue Lu, Taiping Chen, Mark T. Bedford, Sharon Y.R. Dent, John H. Richburg, Raúl Estévez, Hui-Lin Pan, Raif S. Geha, Qinghua Shi, Fernando Benavides

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Figure 1

Expression and localization of LRRC8A.

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Expression and localization of LRRC8A. (A) Relative median expression le...
(A) Relative median expression levels of LRRC8A mRNA in different human tissues as detected by RNA-seq according to the GTEx database. Tissues were collected from 570 adult postmortem individual donors. RPKM, reads per kilobase of transcript per million. (B) Relative mRNA expression levels of Lrrc8 paralogs (Lrrc8a–e) in the developing mouse testis during postnatal development (calculated from Gene Expression Omnibus [GEO] accession number GSE44346). (C) qPCR analysis of Lrrc8a mRNA levels among the purified Sertoli cells and different subtypes of germ cells inside the seminiferous tubules from 3 biological replicates. Spg, spermatogonia; Spc, spermatocyte; RS, round spermatid; ES, elongating spermatid. Data were presented as mean ± SD (n = 3). (D) LRRC8A protein expression during postnatal testicular development in mice. Protein lysates from homozygous Lrrc8aF443*/F443* mice testes were used as negative controls. The arrow points to the LRRC8A-specific protein band of expected size, which is absent in the Lrrc8aF443*/F443* lanes. NS, nonspecific band. ACTIN serves as an internal control. (E) Representative immunofluorescence (IF) images of LRRC8A in germ cell spreads of the seminiferous tubules by squash preparation. LRRC8A protein is present in the plasma membrane of Spc and spermatids (Spd). Testis from F443*/F443* mice were used as negative controls. Scale bar: 20 μm. (F) LRRC8A protein localization by immunofluorescence in mature sperm from WT and F443*/F443* cauda epididymis. LRRC8A is intensively labeled in the midpiece, with weak labeling in the head and principal piece of mature sperm. Sperm from F443*/F443* cauda served as negative controls. Scale bar: 5 μm. DIC, differential interference contrast.