2005
DOI: 10.1074/jbc.m500031200
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Structural Studies of a Stabilized Phosphoenzyme Intermediate of Ca2+-ATPase

Abstract: Ca2؉ -ATPase belongs to the family of P-type ATPases and maintains low concentrations of intracellular Ca 2؉ . Its reaction cycle consists of four main intermediates that alternate ion binding in the transmembrane domain with phosphorylation of an aspartate residue in a cytoplasmic domain. Previous work characterized an ultrastable phosphoenzyme produced first by labeling with fluorescein isothiocyanate, then by allowing this labeled enzyme to establish a maximal Ca 2؉ gradient, and finally by removing Ca 2؉ f… Show more

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Cited by 19 publications
(20 citation statements)
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“…It indicates that V 10 as a reversible mixed inhibitor of Na + /K + -ATPase activity binds to enzyme sites participating in both substrate binding and catalysis. Obtained mixed inhibition is in agreement with previously reported results that there are two binding sites for V 10 on Ca 2+ -ATPase which belongs, as well as Na + /K + -ATPase, to P-type of ATPases Stokes et al 2005). Decrease in apparent affinity for MgATP 2-is in agreement with competition of V 10 with fluorescein isothocyanate for ATP binding site of Ca 2+ -ATPase .…”
Section: Discussionsupporting
confidence: 91%
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“…It indicates that V 10 as a reversible mixed inhibitor of Na + /K + -ATPase activity binds to enzyme sites participating in both substrate binding and catalysis. Obtained mixed inhibition is in agreement with previously reported results that there are two binding sites for V 10 on Ca 2+ -ATPase which belongs, as well as Na + /K + -ATPase, to P-type of ATPases Stokes et al 2005). Decrease in apparent affinity for MgATP 2-is in agreement with competition of V 10 with fluorescein isothocyanate for ATP binding site of Ca 2+ -ATPase .…”
Section: Discussionsupporting
confidence: 91%
“…It could be summarized that the obtained dose-dependent inhibition of PMCA and sodium pump by V 10 , as well as kinetic analysis, is in agreement with previously reported findings that decameric vanadate species block the active side of P-type ATPases and consequently affect phosphorylation step in the enzyme cycle of P-type ATPases (sodium and calcium pump) (Stokes et al 2005). However, this mechanism could not be responsible for obtained ecto-ATPase inhibition (a member of ecto-NTPDases) and probably occurs via different mechanism resulting in less sensitivity compared to P-type ATPases (sodium and calcium pump).…”
Section: Discussionsupporting
confidence: 91%
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“…In previous work, we followed the conventional strategies of Fourier-Bessel reconstruction, increasing the numbers of tubular crystals in several symmetry groups and using real-space averaging in order to maximize the resolution. In contrast to Ca 2+ -ATPase where we were able to achieve 7 Å resolution with as few as 13 tubes (Stokes et al, 2005), a 12 Å structure of Na + /K + -ATPase required 27 tubes (Rice et al, 2001) and further increases in this number have not improved this resolution significantly (unpublished results). This suggests the presence of disorder such as short range bending or variable twist that cannot be compensated by Fourier-Bessel methods, but may be tractable by IHRSR.…”
Section: Na + K + -Atpase Tubular Crystalsmentioning
confidence: 91%
“…This data set consisted of 635 subimages with dimensions of 360×120 pixels, a relative shift of 4 pixels, and comprising a total of ~1500 unit cells. Initially, we used a reference from a Fourier-Bessel reconstruction from 13 tubular crystals with the same helical symmetry and with an estimated resolution of ~7 Å (Stokes et al, 2005). We easily obtained a well-defined minimum at the expected helical parameters Δφ and Δz during the first round of refinement, even though we did not employ layer line filtering for this data set.…”
Section: Rabbit Sr Ca 2+ -Atpase Tubular Crystalsmentioning
confidence: 99%