Molecular and Functional Evidence for Multiple Ca2+-binding Domains in the Type 1 Inositol 1,4,5-Trisphosphate Receptor

Sienaert, Ilse; Missiaen, Ludwig; Smedt, Humbert De; Parys, Jan B.; Sipma, Henk; Casteels, Rik

doi:10.1074/jbc.272.41.25899

Cited by 135 publications

(106 citation statements)

References 62 publications

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“…Stimulation of IP 3 R by cytosolic Ca 2þ is universally observed even with purified IP 3 R reconstituted into lipid bilayers (Ferris et al 1989;Hirota et al 1995;Michikawa et al 1999), suggesting that this essential Ca 2þ -binding site probably resides within the primary sequence of the IP 3 R. At least seven cytosolic Ca 2þ -binding sites have been identified within IP 3 R1 (Sienaert et al 1996;Sienaert et al 1997), but the physiological relevance of these sites is unresolved. Two of the sites (residues 304-381 and 378-450) are within the IP 3 -binding core, for which there is a high-resolution structure (Bosanac et al 2002).…”

Section: Regulation Of Ip 3 Receptors By Ca 2þ and Ipmentioning

confidence: 99%

“…However, point mutations of several of these acidic residues had no effect on Ca 2þ -regulation of IP 3 R (Joseph et al 2005). The remaining Ca 2þ -binding sites fall within the central region of the IP 3 R (Sienaert et al 1996;Sienaert et al 1997). The site between residues 1347 -1426 is interesting because its proximity to a calmodulin (CaM)-binding region is reminiscent of RyR, which have two CaM-binding regions within 200 residues of high-affinity Ca 2þ -binding sites, and a third flanked by two high-affinity Ca 2þ -binding sites (Chen and MacLennan 1994).…”

Section: Regulation Of Ip 3 Receptors By Ca 2þ and Ipmentioning

confidence: 99%

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IP3 Receptors: Toward Understanding Their Activation

Taylor¹,

Tovey²

2010

Cold Spring Harbor Perspectives in Biology

250

183

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Inositol 1,4,5-trisphosphate receptors (IP 3 R) and their relatives, ryanodine receptors, are the channels that most often mediate Ca 2þ release from intracellular stores. Their regulation by Ca 2þ allows them also to propagate cytosolic Ca 2þ signals regeneratively. This brief review addresses the structural basis of IP 3 R activation by IP 3 and Ca 2þ . IP 3 initiates IP 3 R activation by promoting Ca 2þ binding to a stimulatory Ca 2þ -binding site, the identity of which is unresolved. We suggest that interactions of critical phosphate groups in IP 3 with opposite sides of the clam-like IP 3 -binding core cause it to close and propagate a conformational change toward the pore via the adjacent N-terminal suppressor domain. The pore, assembled from the last pair of transmembrane domains and the intervening pore loop from each of the four IP 3 R subunits, forms a structure in which a luminal selectivity filter and a gate at the cytosolic end of the pore control cation fluxes through the IP 3 R.

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Section: Regulation Of Ip 3 Receptors By Ca 2þ and Ipmentioning

confidence: 99%

Section: Regulation Of Ip 3 Receptors By Ca 2þ and Ipmentioning

confidence: 99%

IP3 Receptors: Toward Understanding Their Activation

Taylor¹,

Tovey²

2010

Cold Spring Harbor Perspectives in Biology

250

183

View full text Add to dashboard Cite

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“…We have found that the Ca# + -dependent inhibition of InsP $ binding to cerebellar microsomes might result from a direct interaction of Ca# + with InsP $ R1 [29]. Two of the Ca# + -binding regions identified in the cytoplasmic part of InsP $ R1 are located in the InsP $ -binding domain [25], making these sites reasonable candidates for the mediation of the competitive inhibitory effects of Ca# + described here. Recently, biphasic dependence on Ca# + of InsP $ R channel activity was found to occur with cerebellar receptor isolated and reconstituted in lipid bilayers, suggesting direct effects of Ca# + on this protein [44].…”

Section: [$H]inspmentioning

confidence: 67%

“…However, distinct and noninteracting inhibitory sites might also make a significant contribution to the high degree of sigmoidicity of these curves [40]. Several Ca# + -binding sites have been identified in the InsP $ R1 subunit [25].…”

Section: [$H]inspmentioning

confidence: 99%

“…The selectivities of stimulation and inhibition of IICR for bivalent cations differ [20][21][22], suggesting that different sites are involved. Ca# + -binding regions have been identified in type 1 [23][24][25] and type 2 InsP $ Rs [23] but their function is unknown. The molecular basis of the Ca# + -dependence might differ for each receptor.…”

Section: Introductionmentioning

confidence: 99%

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Regulation of cerebellar Ins(1,4,5)P3 receptor by interaction between Ins(1,4,5)P3 and Ca2+

Coquil

Picard

Mauger

1999

Biochemical Journal

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We have characterized in detail the Ca# + -dependent inhibition of [$H]Ins(1,4,5)P $ ([$H]InsP $ ) binding to sheep cerebellar microsomes, over a short duration (3 s), with the use of a perfusion protocol. This procedure prevented artifacts previously identified in studies of this Ca# + effect. In a cytosol-like medium at pH 7.1 and 20 mC, a maximal inhibition of approx. 50 % was measured. Both inhibition and its reversal were complete within 3 s. Ca# + decreased the affinity of the receptor for InsP $ by approx. 50 % (K d 146p24 nM at pCa 9 and 321p56 nM at pCa 5.3), without changing the total number of binding sites. Conversely, increasing the [$H]InsP $ concentration from 30 to 400 nM tripled the IC &! for Ca# + and decreased the maximal inhibition by 63 %. This is similar to a partial competitive inhibition between InsP $ binding and inhibitory Ca# + binding and is consistent with InsP $ and

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The Calcium Signaling Mechanisms in Arterial Smooth Muscle and Endothelial Cells

Ottolini

Sonkusare

2021

Comprehensive Physiology

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Molecular and Functional Evidence for Multiple Ca2+-binding Domains in the Type 1 Inositol 1,4,5-Trisphosphate Receptor

Cited by 135 publications

References 62 publications

IP3 Receptors: Toward Understanding Their Activation

IP3 Receptors: Toward Understanding Their Activation

Regulation of cerebellar Ins(1,4,5)P3 receptor by interaction between Ins(1,4,5)P3 and Ca2+

The Calcium Signaling Mechanisms in Arterial Smooth Muscle and Endothelial Cells

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