PICK1 deficiency causes male infertility in mice by disrupting acrosome formation
Nan Xiao, … , Liwen Jiang, Jun Xia
Nan Xiao, … , Liwen Jiang, Jun Xia
Published March 2, 2009
Citation Information: J Clin Invest. 2009;119(4):802-812. https://doi.org/10.1172/JCI36230.
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Research Article Reproductive biology

PICK1 deficiency causes male infertility in mice by disrupting acrosome formation

Abstract

Protein interacting with C kinase 1 (PICK1) is a peripheral membrane protein involved in protein trafficking, a function that has been well characterized in neurons. Here, we report that male mice deficient in PICK1 are infertile and have a phenotype resembling the human disease globozoospermia. The primary defect in the testes of Pick1-knockout mice was fragmentation of acrosomes in the early stages of spermiogenesis. This fragmentation was followed by defects in nuclear elongation and mitochondrial sheath formation, leading to round-headed sperm, reduced sperm count, and severely impaired sperm motility. We found that PICK1 interacted with Golgi-associated PDZ- and coiled-coil motif–containing protein (GOPC) and the primary catalytic subunit of protein kinase 2 (CK2α′), proteins whose deficiencies lead to globozoospermia in mice. PICK1 was highly expressed in round spermatids and localized to Golgi-derived proacrosomal granules. GOPC colocalized with PICK1 in the Golgi region and facilitated formation of PICK1-positive clusters. Furthermore, there was an increase in apoptosis in the seminiferous tubules of Pick1–/– mice, a phenotype also seen in CK2α′-deficient mice. Our results suggest that PICK1 is involved in vesicle trafficking from the Golgi apparatus to the acrosome and cooperates with other proteins such as GOPC and CK2α′ in acrosome biogenesis.

Authors

Nan Xiao, Chuen Kam, Chong Shen, Wenying Jin, Junqi Wang, Kwong Man Lee, Liwen Jiang, Jun Xia

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Figure 7

PICK1 and GOPC partially colocalize around the Golgi apparatus, and GOPC increases PICK1 clusters.

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PICK1 and GOPC partially colocalize around the Golgi apparatus, and GOPC...
(A) Immunofluorescence staining showed that PICK1 (red) and GOPC (green) are both expressed in the perinuclear region on the round spermatids and they partially colocalize with the Golgi marker GM130 (blue). (B) In the rat testis smear, 5 ng/μl BFA treatment for 5 minutes leads to better colocalization of PICK1, GOPC, and TGN38, as indicated by the arrows. (C) GFP-PICK1 and myc-GOPC or the empty myc vector were cotransfected into 293T cells. GOPC increased the number of PICK1 clusters, and some of these clusters overlapped with the GOPC signal, as indicated by the arrows. (D) GOPC increases the percentage of HEK293T cells with PICK1 self-clusters to 76.1% ± 3.8% from 55.0% ± 0.8% in the vector control group (mean ± SEM; n = 3 experiments; *P < 0.05). (E) GST-GOPC was mixed with liposome and subjected to high-speed centrifugation. Equal amounts of pellet and supernatant were loaded and resolved by SDS-PAGE. GOPC was found to associate with liposomes and appeared in the pellet (top). In the control experiments, GOPC was not found in the pellet without liposomes, and GST itself did not bind to liposomes. Scale bars: 10 μm.