KRAP tethers IP3 receptors to actin and licenses them to evoke cytosolic Ca2+ signals
Author | Thillaiappan, Nagendra Babu |
Author | Smith, Holly A. |
Author | Atakpa-Adaji, Peace |
Author | Taylor, Colin W. |
Available date | 2023-08-28T09:09:49Z |
Publication Date | 2021 |
Publication Name | Nature Communications |
Resource | Scopus |
ISSN | 20411723 |
Abstract | Regulation of IP3 receptors (IP3Rs) by IP3 and Ca2+ allows regenerative Ca2+ signals, the smallest being Ca2+ puffs, which arise from coordinated openings of a few clustered IP3Rs. Cells express thousands of mostly mobile IP3Rs, yet Ca2+ puffs occur at a few immobile IP3R clusters. By imaging cells with endogenous IP3Rs tagged with EGFP, we show that KRas-induced actin-interacting protein (KRAP) tethers IP3Rs to actin beneath the plasma membrane. Loss of KRAP abolishes Ca2+ puffs and the global increases in cytosolic Ca2+ concentration evoked by more intense stimulation. Over-expressing KRAP immobilizes additional IP3R clusters and results in more Ca2+ puffs and larger global Ca2+ signals. Endogenous KRAP determines which IP3Rs will respond: it tethers IP3R clusters to actin alongside sites where store-operated Ca2+ entry occurs, licenses IP3Rs to evoke Ca2+ puffs and global cytosolic Ca2+ signals, implicates the actin cytoskeleton in IP3R regulation and may allow local activation of Ca2+ entry. 2021, The Author(s). |
Sponsor | The authors thank Martyn Reynolds and Stephen Tovey (Cairn, UK) for help with super-resolution confocal microscopy. Supported by a Wellcome Senior Investigator Award (grant no. 101844), and by a grant (grant no. BB/T012986/1) and studentship (to H.A.S) from the Biotechnology and Biological Sciences Research Council UK. P.A.-A. is a research fellow of Emmanuel College, Cambridge. |
Language | en |
Publisher | Nature Research |
Subject | Actin Calcium signalling Cytoskeletal proteins Endoplasmic reticulum Super-resolution microscopy |
Type | Article |
Issue Number | 1 |
Volume Number | 12 |
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