Reconstitution of local Ca<sup>2+</sup> signaling between cardiac L-type Ca<sup>2+</sup> channels and ryanodine receptors: insights into regulation by FKBP12.6

Chen, S. R. Wayne; Dirksen, Robert T.

doi:10.1152/ajpcell.00250.2005

Cited by 13 publications

(16 citation statements)

References 47 publications

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“…FKBP12 failed to modulate recombinant RyR2 when co-expressed in CHO cells or skeletal myotubes (George et al, 2003;Goonasekera et al, 2005). Similarly, exogenous FKBP12 had no effects in permeabilised cardiomyocytes (Guo et al, 2010).…”

Section: Ryr-fkbp Association In Heart 1765mentioning

confidence: 98%

“…FKBP12.6 is considered to inhibit RyR2 activity, mediating channel closure. These FKBP12.6 effects have been investigated in heterologous systems expressing recombinant RyR2 channels, where FKBP12.6 coexpression suppressed spontaneous or agonist-induced Ca 2+ release (George et al, 2003;Goonasekera et al, 2005). FKBP12.6 deficiency in cardiomyocytes (upon FK506 or rapamycin treatment, or gene-targeted deletion) results in increased intracellular Ca 2+ transients and contractions, and also increased Ca 2+ spark frequency, amplitude and duration (McCall et al, 1996;Xiao et al, 1997;Xin et al, 2002).…”

Section: Introductionmentioning

confidence: 99%

“…Adenovirusmediated FKBP12 overexpression in isolated cardiomyocytes increases SR Ca 2+ content and decreases Ca 2+ spark frequency (Seidler et al, 2007). However, FKBP12 fails to modulate recombinant RyR2 in heterologous expression systems (George et al, 2003;Goonasekera et al, 2005) or in permeabilised cardiomyocytes (Guo et al, 2010).…”

Section: Introductionmentioning

confidence: 99%

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Disparate Ryanodine Receptor Association with the FK506-binding Proteins in Mammalian Heart

Zissimopoulos¹,

Seifan²,

Maxwell³

et al. 2012

Journal of Cell Science

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SummaryThe FK506-binding proteins (FKBP12 and FKBP12.6; also known as FKBP1A and FKBP1B, respectively) are accessory subunits of the ryanodine receptor (RyR) Ca 2+ release channel. Aberrant RyR2-FKBP12.6 interactions have been proposed to be the underlying cause of channel dysfunction in acquired and inherited cardiac disease. However, the stoichiometry of the RyR2 association with FKBP12 or FKBP12.6 in mammalian heart is currently unknown. Here, we describe detailed quantitative analysis of cardiac stoichiometry between RyR2 and FKBP12 or FKBP12.6 using immunoblotting and [3 H]ryanodine-binding assays, revealing striking disparities between four mammalian species. In mouse and pig heart, RyR2 is found complexed with both FKBP12 and FKBP12.6, although the former is the most abundant isoform. In rat heart, RyR2 is predominantly associated with FKBP12.6, whereas in rabbit it is associated with FKBP12 only. Co-immunoprecipitation experiments demonstrate RyR2-specific interaction with both FKBP isoforms in native cardiac tissue. Assuming four FKBP-binding sites per RyR2 tetramer, only a small proportion of available sites are occupied by endogenous FKBP12.6. FKBP interactions with RyR2 are very strong and resistant to drug (FK506, rapamycin and cyclic ADPribose) and redox (H 2 O 2 and diamide) treatment. By contrast, the RyR1-FKBP12 association in skeletal muscle is readily disrupted under oxidative conditions. This is the first study to directly assess association of endogenous FKBP12 and FKBP12.6 with RyR2 in native cardiac tissue. Our results challenge the widespread perception that RyR2 associates exclusively with FKBP12.6 to near saturation, with important implications for the role of the FK506-binding proteins in RyR2 pathophysiology and cardiac disease.

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Section: Ryr-fkbp Association In Heart 1765mentioning

confidence: 98%

Section: Introductionmentioning

confidence: 99%

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Disparate Ryanodine Receptor Association with the FK506-binding Proteins in Mammalian Heart

Zissimopoulos¹,

Seifan²,

Maxwell³

et al. 2012

Journal of Cell Science

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“…The additional variable k' is a scaling factor that varies with (∆F/F) max (Sheridan et al, 2003;Goonasekera et al, 2005). Pooled current-voltage (I-V) and fl uorescence-voltage (∆F/F-V) data in Table I are expressed as mean ± SEM.…”

Section: Simultaneous Measurements Of Macroscopic Ca 2+ Currents and mentioning

confidence: 99%

Triadin Binding to the C-Terminal Luminal Loop of the Ryanodine Receptor is Important for Skeletal Muscle Excitation–Contraction Coupling

Beard¹,

Groom²,

Kimura³

et al. 2007

J Cell Biol

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“…The ensuing increase in intracellular calcium concentrations gives rise to a wide range of physiological responses, including calcium-dependent gene transcription, calcium release from internal stores, excitation contraction coupling, and secretion/neurotransmitter release [1][2][3][4][5][6][7][8]. Physiological roles of voltage-gated calcium channels are well summarized in other reviews [9].…”

Section: Introductionmentioning

confidence: 99%

Trafficking and stability of voltage-gated calcium channels

Simms

Zamponi

2011

Cell. Mol. Life Sci.

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Voltage-gated calcium channels are important mediators of calcium influx into electrically excitable cells. The amount of calcium entering through this family of channel proteins is not only determined by the functional properties of channels embedded in the plasma membrane but also by the numbers of channels that are expressed at the cell surface. The trafficking of channels is controlled by numerous processes, including co-assembly with ancillary calcium channel subunits, ubiquitin ligases, and interactions with other membrane proteins such as G protein coupled receptors. Here we provide an overview about the current state of knowledge of calcium channel trafficking to the cell membrane, and of the mechanisms regulating the stability and internalization of this important ion channel family.

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Reconstitution of local Ca²⁺ signaling between cardiac L-type Ca²⁺ channels and ryanodine receptors: insights into regulation by FKBP12.6

Cited by 13 publications

References 47 publications

Disparate Ryanodine Receptor Association with the FK506-binding Proteins in Mammalian Heart

Disparate Ryanodine Receptor Association with the FK506-binding Proteins in Mammalian Heart

Triadin Binding to the C-Terminal Luminal Loop of the Ryanodine Receptor is Important for Skeletal Muscle Excitation–Contraction Coupling

Trafficking and stability of voltage-gated calcium channels

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Reconstitution of local Ca2+ signaling between cardiac L-type Ca2+ channels and ryanodine receptors: insights into regulation by FKBP12.6

Cited by 13 publications

References 47 publications

Disparate Ryanodine Receptor Association with the FK506-binding Proteins in Mammalian Heart

Disparate Ryanodine Receptor Association with the FK506-binding Proteins in Mammalian Heart

Triadin Binding to the C-Terminal Luminal Loop of the Ryanodine Receptor is Important for Skeletal Muscle Excitation–Contraction Coupling

Trafficking and stability of voltage-gated calcium channels

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Product

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Reconstitution of local Ca²⁺ signaling between cardiac L-type Ca²⁺ channels and ryanodine receptors: insights into regulation by FKBP12.6