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ATP interacts with the CPVT mutation-associated central domain of the cardiac ryanodine receptor.

Lynda Blayney, Konrad Beck, Ewan MacDonald, Leon D'Cruz, Michail Nomikos, Julia Griffiths, Angelos Thanassoulas, George Nounesis, F Anthony Lai

Institute of Molecular and Experimental Medicine, Cardiff University, Cardiff, UK. blayney@cf.ac.uk

Biochimica et biophysica acta 2013 Oct


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This study was designed to determine whether the cardiac ryanodine receptor (RyR2) central domain, a region associated with catecholamine polymorphic ventricular tachycardia (CPVT) mutations, interacts with the RyR2 regulators, ATP and the FK506-binding protein 12.6 (FKBP12.6). Wild-type (WT) RyR2 central domain constructs (G(2236)to G(2491)) and those containing the CPVT mutations P2328S and N2386I, were expressed as recombinant proteins. Folding and stability of the proteins were examined by circular dichroism (CD) spectroscopy and guanidine hydrochloride chemical denaturation. The far-UV CD spectra showed a soluble stably-folded protein with WT and mutant proteins exhibiting a similar secondary structure. Chemical denaturation analysis also confirmed a stable protein for both WT and mutant constructs with similar two-state unfolding. ATP and caffeine binding was measured by fluorescence spectroscopy. Both ATP and caffeine bound with an EC50 of ~200-400μM, and the affinity was the same for WT and mutant constructs. Sequence alignment with other ATP binding proteins indicated the RyR2 central domain contains the signature of an ATP binding pocket. Interaction of the central domain with FKBP12.6 was tested by glutaraldehyde cross-linking and no association was found. The RyR2 central domain, expressed as a 'correctly' folded recombinant protein, bound ATP in accord with bioinformatics evidence of conserved ATP binding sequence motifs. An interaction with FKBP12.6 was not evident. CPVT mutations did not disrupt the secondary structure nor binding to ATP. Part of the RyR2 central domain CPVT mutation cluster, can be expressed independently with retention of ATP binding. Copyright © 2013 Elsevier B.V. All rights reserved.

Citation

Lynda Blayney, Konrad Beck, Ewan MacDonald, Leon D'Cruz, Michail Nomikos, Julia Griffiths, Angelos Thanassoulas, George Nounesis, F Anthony Lai. ATP interacts with the CPVT mutation-associated central domain of the cardiac ryanodine receptor. Biochimica et biophysica acta. 2013 Oct;1830(10):4426-32


PMID: 23747301

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