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Developmentally acquired PKA localisation in mouse oocytes and embryos
Authors:Webb Rachel J  Tinworth Lorna  Thomas Geraint M H  Zaccolo Manuela  Carroll John
Institution:a Department of Physiology, University College London, Gower Street, London, WC1E 6BT, UK
b School of Biosciences, University of Westminster, 115 New Cavendish St, London, W1W 6UW, UK
c Dulbecco Telethon Institute at the Venetian Institute of Molecular Medicine, via Orus 2, 35100 Padova, Italy
Abstract:Localisation of Protein Kinase A (PKA) by A-Kinase Anchoring Proteins (AKAPs) is known to coordinate localised signalling complexes that target cAMP-mediated signalling to specific cellular sub-domains. The cAMP PKA signalling pathway is implicated in both meiotic arrest and meiotic resumption, thus spatio-temporal changes in PKA localisation during development may determine the oocytes response to changes in cAMP. In this study we aim to establish whether changes in PKA localisation occur during oocyte and early embryo development.Using fluorescently-labelled PKA constructs we show that in meiotically incompetent oocytes PKA is distributed throughout the cytoplasm and shows no punctuate localisation. As meiotic competence is acquired, PKA associates with mitochondria. Immature germinal vesicle (GV) stage oocytes show an aggregation of PKA around the GV and PKA remains co-localised with mitochondria throughout oocyte maturation. After fertilisation, the punctuate, mitochondrial distribution was lost, such that by the 2-cell stage there was no evidence of PKA localisation. RT-PCR and Western blotting revealed two candidate AKAPs that are known to be targeted to mitochondria, AKAP1 and D-AKAP2. In summary these data show a dynamic regulation of PKA localisation during oocyte and early embryo development.
Keywords:PKA  AKAP  cAMP  Meiosis  Oocyte  D-AKAP2  AKAP1  Oocyte maturation
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