STIM1 signalling controls store-operated calcium entry required for development and contractile function in skeletal muscle

Stiber, Jonathan A.; Hawkins, April; Zhang, Zhu-Shan; Sunny, Wang,; Burch, Jarrett; Graham, Victoria; Ward, Cary; Seth, Malini; Finch, Elizabeth A.; Malouf, Nadia N.; Williams, R. Sanders; Eu, Jerry P.; Rosenberg, Paul B.

doi:10.1038/ncb1731

Cited by 337 publications

(558 citation statements)

References 49 publications

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“…It has been previously reported by our group and others that actin-binding proteins provide a physical linkage between Cx43 and the cortical cytoskeleton and that these interactions are required for maintaining functional Cx43-formed gap junctions in differentiating myoblasts [6,58]. Among the different proteins interacting with connexins are the ZO proteins, vinculin, ezrin, a-actin and cortactin [6,47,58]. In this study we showed that TRPC1 channels could regulate the remodeling of a specific pool of Cx43 protein, likely through the stabilization and coordination of its interaction with cortactin.…”

Section: Discussionmentioning

confidence: 98%

“…depends upon the activation of peculiar channels which belong to the TRPC family, and function as storedependent and mechanosensitive channels [4,13,34,46]. Of interest, these channels have been recently implicated in the regulation of numerous physiological and pathological processes, such as skeletal muscle differentiation and Duchenne muscular dystrophy [4,30,46,47]. An open question in the field of TRPC signaling is the identification of specific targets by which these Ca 2? gates can affect cell differentiation.…”

Section: Discussionmentioning

confidence: 99%

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Functional interaction between TRPC1 channel and connexin-43 protein: a novel pathway underlying S1P action on skeletal myogenesis

Meacci

Bini

Sassoli

et al. 2010

Cell. Mol. Life Sci.

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We recently demonstrated that skeletal muscle differentiation induced by sphingosine 1-phosphate (S1P) requires gap junctions and transient receptor potential canonical 1 (TRPC1) channels. Here, we searched for the signaling pathway linking the channel activity with Cx43 expression/function, investigating the involvement of the Ca 2? -sensitive protease, m-calpain, and its targets in S1P-induced C2C12 myoblast differentiation. Gene silencing and pharmacological inhibition of TRPC1 significantly reduced Cx43 up-regulation and Cx43/cytoskeletal interaction elicited by S1P. TRPC1-dependent functions were also required for the transient increase of m-calpain activity/expression and the subsequent decrease of PKCa levels. Remarkably, Cx43 expression in S1P-treated myoblasts was reduced by m-calpain-siRNA and enhanced by pharmacological inhibition of classical PKCs, stressing the relevance for calpain/PKCa axis in Cx43 protein remodeling. The contribution of this pathway in myogenesis was also investigated. In conclusion, these findings provide novel mechanisms by which S1P regulates myoblast differentiation and offer interesting therapeutic options to improve skeletal muscle regeneration.

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Section: Discussionmentioning

confidence: 98%

Section: Discussionmentioning

confidence: 99%

Functional interaction between TRPC1 channel and connexin-43 protein: a novel pathway underlying S1P action on skeletal myogenesis

Meacci

Bini

Sassoli

et al. 2010

Cell. Mol. Life Sci.

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“…Fast-twitch fibers are known to operate with a ∼30% partially filled SR only, whereas slow-twitch fibers are almost completely filled under resting conditions (Fryer and Stephenson 1996). Whether SR depletion even in exercised fast-twitch muscle would be severe enough to trigger SOCE could not be answered in intact muscle, especially in view of mechanisms that counteract fatigue ) and given the fact that SOCE operates mostly at negative membrane potentials (Stiber et al 2008;Kurebayashi and Ogawa 2001).…”

Section: Store-operated Ca 2+ Entry (Soce) In Skeletal Musclementioning

confidence: 99%

“…This suggested a slow signalling event during which ER Ca 2+ depletion leads to collection and relocation of Stim1 molecules from regions distant from the plasma membrane towards the membrane to interact with the CRAC channels. During myoblast-tomyotube differentiation, an increased expression and redistribution of Stim1 to the cell periphery was observed (Stiber et al 2008). Myotubes lacking Stim1 do not show SOCE, and muscles from Stim1 knockout mice fatigue more quickly (Stiber et al 2008;Lyfenko and Dirksen 2008).…”

Section: Store-operated Ca 2+ Entry (Soce) In Skeletal Musclementioning

confidence: 99%

“…During myoblast-tomyotube differentiation, an increased expression and redistribution of Stim1 to the cell periphery was observed (Stiber et al 2008). Myotubes lacking Stim1 do not show SOCE, and muscles from Stim1 knockout mice fatigue more quickly (Stiber et al 2008;Lyfenko and Dirksen 2008). Here as well, Orai1 and Stim1 are the crucial molecular players of SOCE (Lyfenko and Dirksen 2008).…”

Section: Store-operated Ca 2+ Entry (Soce) In Skeletal Musclementioning

confidence: 99%

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New factors contributing to dynamic calcium regulation in the skeletal muscle triad—a crowded place

2009

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Skeletal muscle is a highly organized tissue that has to be optimized for fast signalling events conveying electrical excitation to contractile response. The site of electro-chemico-mechanical coupling is the skeletal muscle triad where two membrane systems, the extracellular ttubules and the intracellular sarcoplasmic reticulum, come into very close contact. Structure fits function here and the signalling proteins DHPR and RyR1 were the first to be discovered to bridge this gap in a conformational coupling arrangement. Since then, however, new proteins and more signalling cascades have been identified just in the last decade, adding more diversity and fine tuning to the regulation of excitation-contraction coupling (ECC) and control over Ca 2+ store content. The concept of Ca 2+ entry into working skeletal muscle has become attractive again with the experimental evidence summarized in this review. Store-operated Ca 2+ entry (SOCE), excitation-coupled Ca 2+ entry (ECCE), action-potential-activated Ca 2+ current (APACC), and retrograde EC-coupling (ECC) are new concepts additional to the conventional orthograde ECC; they have provided fascinating new insights into muscle physiology. In this review, we discuss the discovery of these pathways, their potential roles, and the signalling proteins involved that show that the triad may become a crowded place in time.

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Store‐Operated Calcium Entry Mediated by ORAI and STIM

Nguyen

Han

Cao

et al. 2018

Comprehensive Physiology

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The calcium release-activated calcium (CRAC) channel, composed of ORAI and stromal interaction molecules (STIM), represents a prototypical example of store-operated calcium entry in mammals. The ORAI-STIM signaling occurs at membrane contact sites formed by close appositions between the endoplasmic reticulum (ER) and the plasma membrane. ORAI1 is a four-pass transmembrane protein that forms a highly calcium-selective ion channel in the plasma membrane. STIM1 is an ER-resident, a single-pass transmembrane protein that serves as a calcium sensor within the ER lumen and a potent activator of ORAI1 calcium channels. The intricate interplay between ORAI and STIM controls calcium entry into cells to regulate a myriad of physiological processes. We highlight herein the current knowledge on the structure-function relationship of CRAC channel, with a focus on key structural elements that mediate STIM1 conformational switch and the dynamic coupling between STIM1 and ORAI1. Furthermore, we discuss the physiological roles of STIM-ORAI signaling in various tissues and organs, as well as major pathological conditions arising from loss- or gain-of-function mutations in human ORAI1 and STIM1. © 2017 American Physiological Society. Compr Physiol 8:981-1002, 2018.

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STIM1 signalling controls store-operated calcium entry required for development and contractile function in skeletal muscle

Cited by 337 publications

References 49 publications

Functional interaction between TRPC1 channel and connexin-43 protein: a novel pathway underlying S1P action on skeletal myogenesis

Functional interaction between TRPC1 channel and connexin-43 protein: a novel pathway underlying S1P action on skeletal myogenesis

New factors contributing to dynamic calcium regulation in the skeletal muscle triad—a crowded place

Store‐Operated Calcium Entry Mediated by ORAI and STIM

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