Ca(2+) and Membrane Potential Transitions During Action Potentials Are Self-Similar to Each Other and to Variability of AP Firing Intervals Across the Broad Physiologic Range of AP Intervals During Autonomic Receptor Stimulation

Ca(2+) and V(m) transitions occurring throughout action potential (AP) cycles in sinoatrial nodal (SAN) cells are cues that (1) not only regulate activation states of molecules operating within criticality (Ca(2+) domain) and limit-cycle (V(m) domain) mechanisms of a coupled-clock system that underl...

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Autores principales: Yang, Dongmei, Morrell, Christopher H., Lyashkov, Alexey E., Tagirova Sirenko, Syevda, Zahanich, Ihor, Yaniv, Yael, Vinogradova, Tatiana M., Ziman, Bruce D., Maltsev, Victor A., Lakatta, Edward G.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2021
Materias:
Physiology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8456031/
https://www.ncbi.nlm.nih.gov/pubmed/34566668
http://dx.doi.org/10.3389/fphys.2021.612770
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author Yang, Dongmei
Morrell, Christopher H.
Lyashkov, Alexey E.
Tagirova Sirenko, Syevda
Zahanich, Ihor
Yaniv, Yael
Vinogradova, Tatiana M.
Ziman, Bruce D.
Maltsev, Victor A.
Lakatta, Edward G.
author_facet Yang, Dongmei
Morrell, Christopher H.
Lyashkov, Alexey E.
Tagirova Sirenko, Syevda
Zahanich, Ihor
Yaniv, Yael
Vinogradova, Tatiana M.
Ziman, Bruce D.
Maltsev, Victor A.
Lakatta, Edward G.
author_sort Yang, Dongmei
collection PubMed
description Ca(2+) and V(m) transitions occurring throughout action potential (AP) cycles in sinoatrial nodal (SAN) cells are cues that (1) not only regulate activation states of molecules operating within criticality (Ca(2+) domain) and limit-cycle (V(m) domain) mechanisms of a coupled-clock system that underlies SAN cell automaticity, (2) but are also regulated by the activation states of the clock molecules they regulate. In other terms, these cues are both causes and effects of clock molecular activation (recursion). Recently, we demonstrated that Ca(2+) and V(m) transitions during AP cycles in single SAN cells isolated from mice, guinea pigs, rabbits, and humans are self-similar (obey a power law) and are also self-similar to trans-species AP firing intervals (APFIs) of these cells in vitro, to heart rate in vivo, and to body mass. Neurotransmitter stimulation of β-adrenergic receptor or cholinergic receptor–initiated signaling in SAN cells modulates their AP firing rate and rhythm by impacting on the degree to which SAN clocks couple to each other, creating the broad physiologic range of SAN cell mean APFIs and firing interval variabilities. Here we show that Ca(2+) and V(m) domain kinetic transitions (time to AP ignition in diastole and 90% AP recovery) occurring within given AP, the mean APFIs, and APFI variabilities within the time series of APs in 230 individual SAN cells are self-similar (obey power laws). In other terms, these long-range correlations inform on self-similar distributions of order among SAN cells across the entire broad physiologic range of SAN APFIs, regardless of whether autonomic receptors of these cells are stimulated or not and regardless of the type (adrenergic or cholinergic) of autonomic receptor stimulation. These long-range correlations among distributions of Ca(2+) and V(m) kinetic functions that regulate SAN cell clock coupling during each AP cycle in different individual, isolated SAN cells not in contact with each other. Our numerical model simulations further extended our perspectives to the molecular scale and demonstrated that many ion currents also behave self-similar across autonomic states. Thus, to ensure rapid flexibility of AP firing rates in response to different types and degrees of autonomic input, nature “did not reinvent molecular wheels within the coupled-clock system of pacemaker cells,” but differentially engaged or scaled the kinetics of gears that regulate the rate and rhythm at which the “wheels spin” in a given autonomic input context.
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spelling pubmed-84560312021-09-23 Ca(2+) and Membrane Potential Transitions During Action Potentials Are Self-Similar to Each Other and to Variability of AP Firing Intervals Across the Broad Physiologic Range of AP Intervals During Autonomic Receptor Stimulation Yang, Dongmei Morrell, Christopher H. Lyashkov, Alexey E. Tagirova Sirenko, Syevda Zahanich, Ihor Yaniv, Yael Vinogradova, Tatiana M. Ziman, Bruce D. Maltsev, Victor A. Lakatta, Edward G. Front Physiol Physiology Ca(2+) and V(m) transitions occurring throughout action potential (AP) cycles in sinoatrial nodal (SAN) cells are cues that (1) not only regulate activation states of molecules operating within criticality (Ca(2+) domain) and limit-cycle (V(m) domain) mechanisms of a coupled-clock system that underlies SAN cell automaticity, (2) but are also regulated by the activation states of the clock molecules they regulate. In other terms, these cues are both causes and effects of clock molecular activation (recursion). Recently, we demonstrated that Ca(2+) and V(m) transitions during AP cycles in single SAN cells isolated from mice, guinea pigs, rabbits, and humans are self-similar (obey a power law) and are also self-similar to trans-species AP firing intervals (APFIs) of these cells in vitro, to heart rate in vivo, and to body mass. Neurotransmitter stimulation of β-adrenergic receptor or cholinergic receptor–initiated signaling in SAN cells modulates their AP firing rate and rhythm by impacting on the degree to which SAN clocks couple to each other, creating the broad physiologic range of SAN cell mean APFIs and firing interval variabilities. Here we show that Ca(2+) and V(m) domain kinetic transitions (time to AP ignition in diastole and 90% AP recovery) occurring within given AP, the mean APFIs, and APFI variabilities within the time series of APs in 230 individual SAN cells are self-similar (obey power laws). In other terms, these long-range correlations inform on self-similar distributions of order among SAN cells across the entire broad physiologic range of SAN APFIs, regardless of whether autonomic receptors of these cells are stimulated or not and regardless of the type (adrenergic or cholinergic) of autonomic receptor stimulation. These long-range correlations among distributions of Ca(2+) and V(m) kinetic functions that regulate SAN cell clock coupling during each AP cycle in different individual, isolated SAN cells not in contact with each other. Our numerical model simulations further extended our perspectives to the molecular scale and demonstrated that many ion currents also behave self-similar across autonomic states. Thus, to ensure rapid flexibility of AP firing rates in response to different types and degrees of autonomic input, nature “did not reinvent molecular wheels within the coupled-clock system of pacemaker cells,” but differentially engaged or scaled the kinetics of gears that regulate the rate and rhythm at which the “wheels spin” in a given autonomic input context. Frontiers Media S.A. 2021-09-08 /pmc/articles/PMC8456031/ /pubmed/34566668 http://dx.doi.org/10.3389/fphys.2021.612770 Text en Copyright © 2021 Yang, Morrell, Lyashkov, Tagirova Sirenko, Zahanich, Yaniv, Vinogradova, Ziman, Maltsev and Lakatta. https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Physiology
Yang, Dongmei
Morrell, Christopher H.
Lyashkov, Alexey E.
Tagirova Sirenko, Syevda
Zahanich, Ihor
Yaniv, Yael
Vinogradova, Tatiana M.
Ziman, Bruce D.
Maltsev, Victor A.
Lakatta, Edward G.
Ca(2+) and Membrane Potential Transitions During Action Potentials Are Self-Similar to Each Other and to Variability of AP Firing Intervals Across the Broad Physiologic Range of AP Intervals During Autonomic Receptor Stimulation
title Ca(2+) and Membrane Potential Transitions During Action Potentials Are Self-Similar to Each Other and to Variability of AP Firing Intervals Across the Broad Physiologic Range of AP Intervals During Autonomic Receptor Stimulation
title_full Ca(2+) and Membrane Potential Transitions During Action Potentials Are Self-Similar to Each Other and to Variability of AP Firing Intervals Across the Broad Physiologic Range of AP Intervals During Autonomic Receptor Stimulation
title_fullStr Ca(2+) and Membrane Potential Transitions During Action Potentials Are Self-Similar to Each Other and to Variability of AP Firing Intervals Across the Broad Physiologic Range of AP Intervals During Autonomic Receptor Stimulation
title_full_unstemmed Ca(2+) and Membrane Potential Transitions During Action Potentials Are Self-Similar to Each Other and to Variability of AP Firing Intervals Across the Broad Physiologic Range of AP Intervals During Autonomic Receptor Stimulation
title_short Ca(2+) and Membrane Potential Transitions During Action Potentials Are Self-Similar to Each Other and to Variability of AP Firing Intervals Across the Broad Physiologic Range of AP Intervals During Autonomic Receptor Stimulation
title_sort ca(2+) and membrane potential transitions during action potentials are self-similar to each other and to variability of ap firing intervals across the broad physiologic range of ap intervals during autonomic receptor stimulation
topic Physiology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8456031/
https://www.ncbi.nlm.nih.gov/pubmed/34566668
http://dx.doi.org/10.3389/fphys.2021.612770
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