Haploinsufficiency at the protein kinase A RIα Gene Locus leads to fertility defects in male mice and men (PDF)
Burton,Kimberly A.; McDermott,Deborah A.; Wilkes,David; Poulsen,Melissa N.; Nolan,Michael A.; Goldstein,Marc; Basson,Craig T.; McKnight,G.Stanley
Molecular Endocrinology 20(10): 2504-2513
Publication date: 2006
Carney complex (CNC) is a familial multiple neoplasia syndrome characterized by spotty skin pigmentation, cardiac and cutaneous myxomas, and endocrine tumors. CNC is inherited as an autosomal dominant trait and is transmitted with greater frequency by women vs. men. Nearly two-thirds of CNC patients are heterozygous for inactivating mutations in the gene encoding the protein kinase A (PKA) type Ia regulatory subunit (RIa), PRKAR1. We report here that male mice heterozygous for the Prkar 1a gene have severely reduced fertility. Sperm from Prkar 1a heterozygous mice are morphologically abnormal and reduced in number. Genetic rescue experiments reveal that this phenotype results from elevated PKA catalytic activity in germ cells as early as the pachytene stage of spermatogenesis. Consistent with this defect in the male mutant mice, sperm from CNC patients heterozygous for PRKAR1A mutations were also found to be morphologically aberrant and decreased in number. We conclude that unregulated PKA activity in male meiotic or postmeiotic germ cells leads to structural defects in mature sperm and results in reduced fertility in mice and humans, contributing to the strikingly reduced transmission of PRKAR1A inactivating mutations by male patients with CNC.
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