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Essential role of Fkbp6 in male fertility and homologous chromosome pairing in meiosis
Authors:Crackower Michael A  Kolas Nadine K  Noguchi Junko  Sarao Renu  Kikuchi Kazuhiro  Kaneko Hiroyuki  Kobayashi Eiji  Kawai Yasuhiro  Kozieradzki Ivona  Landers Rushin  Mo Rong  Hui Chi-Chung  Nieves Edward  Cohen Paula E  Osborne Lucy R  Wada Teiji  Kunieda Tetsuo  Moens Peter B  Penninger Josef M
Affiliation:Institute of Molecular Biotechnology of the Austrian Academy of Sciences (IMBA), c/o Dr. Bohrgasse 7, 1030, Vienna, Austria.
Abstract:
Meiosis is a critical stage of gametogenesis in which alignment and synapsis of chromosomal pairs occur, allowing for the recombination of maternal and paternal genomes. Here we show that FK506 binding protein (Fkbp6) localizes to meiotic chromosome cores and regions of homologous chromosome synapsis. Targeted inactivation of Fkbp6 in mice results in aspermic males and the absence of normal pachytene spermatocytes. Moreover, we identified the deletion of Fkbp6 exon 8 as the causative mutation in spontaneously male sterile as/as mutant rats. Loss of Fkbp6 results in abnormal pairing and misalignments between homologous chromosomes, nonhomologous partner switches, and autosynapsis of X chromosome cores in meiotic spermatocytes. Fertility and meiosis are normal in Fkbp6 mutant females. Thus, Fkbp6 is a component of the synaptonemal complex essential for sex-specific fertility and for the fidelity of homologous chromosome pairing in meiosis.
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