4.6 Article

VAMPs sensitive to tetanus toxin are required for cortical granule exocytosis in mouse oocytes

Journal

EXPERIMENTAL CELL RESEARCH
Volume 405, Issue 1, Pages -

Publisher

ELSEVIER INC
DOI: 10.1016/j.yexcr.2021.112629

Keywords

Cortical granule exocytosis; VAMP; R-SNARE; Cortical reaction; Mouse oocyte

Funding

  1. Fogarty International Center from NIH, USA (GRIP) [R01 TW007571]
  2. Agencia Nacional de Promoci on Cientifica y Tecnologica [PICT 2012-0218]
  3. Universidad Nacional de Cuyo, Argentina [06/M071, 06/M093]

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The fusion of cortical granules with oocyte plasma membrane is crucial for preventing polyspermy during oocyte activation. Cortical granule exocytosis (CGE) is unique because cortical granules are not replenished after secretion. Research demonstrates that R-SNAREs proteins VAMP1 and VAMP3 are essential for CGE in mouse oocytes, highlighting the importance of the SNARE complex in this process.
Fusion of cortical granules with oocyte plasma membrane is one of the most significant secretory events to prevent polyspermy during oocyte activation. Cortical granule exocytosis (CGE) is distinct from most other exocytosis because cortical granules are not renewed after secretion. However, it is thought to be mediated by SNARE complex, which mediates membrane fusion in other exocytoses. SNAREs proteins are divided into Q (glutamine)- and R (arginine)-SNAREs. Q-SNAREs include Syntaxins and SNAP25 family, and R-SNAREs include VAMPs family. In mouse oocytes, Syntaxin4 and SNAP23 have been involved in CGE; nevertheless, it is unknown if VAMP is required. Here, we demonstrated by RT-PCR and immunoblotting that VAMP1 and VAMP3 are expressed in mouse oocyte, and they localized in the cortical region of this cell. Using a functional assay to quantify CGE, we showed that tetanus toxin -which specifically cleavages VAMP1, VAMP2 or VAMP3-inhibited CGE suggesting that at least one VAMP was necessary. Function blocking assays demonstrated that only the microinjection of anti-VAMP1 or anti-VAMP3 antibodies abolished CGE in activated oocytes. These findings demonstrate that R-SNAREs sensitive to tetanus toxin, VAMP1 and VAMP3 -but not VAMP2-, are required for CGE and demonstrate that CGE is mediated by the SNARE complex.

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