Mechanism of beta 4 Subunit Modulation of BK Channels
Large-conductance (BK-type) Ca super(2+)-activated potassium channels are activated by membrane depolarization and cytoplasmic Ca super(2+). BK channels are expressed in a broad variety of cells and have a corresponding diversity in properties. Underlying much of the functional diversity is a family...
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| Veröffentlicht in: | The Journal of general physiology 2006-04, Vol.127 (4), p.449-465 |
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| description | Large-conductance (BK-type) Ca super(2+)-activated potassium channels are activated by membrane depolarization and cytoplasmic Ca super(2+). BK channels are expressed in a broad variety of cells and have a corresponding diversity in properties. Underlying much of the functional diversity is a family of four tissue-specific accessory subunits ( beta 1- beta 4). Biophysical characterization has shown that the beta 4 subunit confers properties of the so-called "type II" BK channel isotypes seen in brain. These properties include slow gating kinetics and resistance to iberiotoxin and charybdotoxin blockade. In addition, the beta 4 subunit reduces the apparent voltage sensitivity of channel activation and has complex effects on apparent Ca super(2+) sensitivity. Specifically, channel activity at low Ca super(2+) is inhibited, while at high Ca super(2+), activity is enhanced. The goal of this study is to understand the mechanism underlying beta 4 subunit action in the context of a dual allosteric model for BK channel gating. We observed that beta 4's most profound effect is a decrease in P sub(o) (at least 11-fold) in the absence of calcium binding and voltage sensor activation. However, beta 4 promotes channel opening by increasing voltage dependence of P sub(o)-V relations at negative membrane potentials. In the context of the dual allosteric model for BK channels, we find these properties are explained by distinct and opposing actions of beta 4 on BK channels. beta 4 reduces channel opening by decreasing the intrinsic gating equilibrium (L sub(0)), and decreasing the allosteric coupling between calcium binding and voltage sensor activation (E). However, beta 4 has a compensatory effect on channel opening following depolarization by shifting open channel voltage sensor activation (Vh sub(o)) to more negative membrane potentials. The consequence is that beta 4 causes a net positive shift of the G-V relationship (relative to alpha subunit alone) at low calcium. At higher calcium, the contribution by Vh sub(o) and an increase in allosteric coupling to Ca super(2+) binding (C) promotes a negative G-V shift of alpha + beta 4 channels as compared to alpha subunits alone. This manner of modulation predicts that type II BK channels are downregulated by beta 4 at resting voltages through effects on L sub(0). However, beta 4 confers a compensatory effect on voltage sensor activation that increases channel opening during depolarization. |
| doi_str_mv | 10.1085/jgp.200509436 |
| format | Article |
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BK channels are expressed in a broad variety of cells and have a corresponding diversity in properties. Underlying much of the functional diversity is a family of four tissue-specific accessory subunits ( beta 1- beta 4). Biophysical characterization has shown that the beta 4 subunit confers properties of the so-called "type II" BK channel isotypes seen in brain. These properties include slow gating kinetics and resistance to iberiotoxin and charybdotoxin blockade. In addition, the beta 4 subunit reduces the apparent voltage sensitivity of channel activation and has complex effects on apparent Ca super(2+) sensitivity. Specifically, channel activity at low Ca super(2+) is inhibited, while at high Ca super(2+), activity is enhanced. The goal of this study is to understand the mechanism underlying beta 4 subunit action in the context of a dual allosteric model for BK channel gating. We observed that beta 4's most profound effect is a decrease in P sub(o) (at least 11-fold) in the absence of calcium binding and voltage sensor activation. However, beta 4 promotes channel opening by increasing voltage dependence of P sub(o)-V relations at negative membrane potentials. In the context of the dual allosteric model for BK channels, we find these properties are explained by distinct and opposing actions of beta 4 on BK channels. beta 4 reduces channel opening by decreasing the intrinsic gating equilibrium (L sub(0)), and decreasing the allosteric coupling between calcium binding and voltage sensor activation (E). However, beta 4 has a compensatory effect on channel opening following depolarization by shifting open channel voltage sensor activation (Vh sub(o)) to more negative membrane potentials. The consequence is that beta 4 causes a net positive shift of the G-V relationship (relative to alpha subunit alone) at low calcium. At higher calcium, the contribution by Vh sub(o) and an increase in allosteric coupling to Ca super(2+) binding (C) promotes a negative G-V shift of alpha + beta 4 channels as compared to alpha subunits alone. This manner of modulation predicts that type II BK channels are downregulated by beta 4 at resting voltages through effects on L sub(0). However, beta 4 confers a compensatory effect on voltage sensor activation that increases channel opening during depolarization.</description><identifier>ISSN: 0022-1295</identifier><identifier>DOI: 10.1085/jgp.200509436</identifier><language>eng</language><ispartof>The Journal of general physiology, 2006-04, Vol.127 (4), p.449-465</ispartof><lds50>peer_reviewed</lds50><oa>free_for_read</oa><woscitedreferencessubscribed>false</woscitedreferencessubscribed></display><links><openurl>$$Topenurl_article</openurl><openurlfulltext>$$Topenurlfull_article</openurlfulltext><thumbnail>$$Tsyndetics_thumb_exl</thumbnail><link.rule.ids>314,776,780,27901,27902</link.rule.ids></links><search><creatorcontrib>Wang, Bin</creatorcontrib><creatorcontrib>Rothberg, Brad S</creatorcontrib><creatorcontrib>Brenner, Robert</creatorcontrib><title>Mechanism of beta 4 Subunit Modulation of BK Channels</title><title>The Journal of general physiology</title><description>Large-conductance (BK-type) Ca super(2+)-activated potassium channels are activated by membrane depolarization and cytoplasmic Ca super(2+). BK channels are expressed in a broad variety of cells and have a corresponding diversity in properties. Underlying much of the functional diversity is a family of four tissue-specific accessory subunits ( beta 1- beta 4). Biophysical characterization has shown that the beta 4 subunit confers properties of the so-called "type II" BK channel isotypes seen in brain. These properties include slow gating kinetics and resistance to iberiotoxin and charybdotoxin blockade. In addition, the beta 4 subunit reduces the apparent voltage sensitivity of channel activation and has complex effects on apparent Ca super(2+) sensitivity. Specifically, channel activity at low Ca super(2+) is inhibited, while at high Ca super(2+), activity is enhanced. The goal of this study is to understand the mechanism underlying beta 4 subunit action in the context of a dual allosteric model for BK channel gating. We observed that beta 4's most profound effect is a decrease in P sub(o) (at least 11-fold) in the absence of calcium binding and voltage sensor activation. However, beta 4 promotes channel opening by increasing voltage dependence of P sub(o)-V relations at negative membrane potentials. In the context of the dual allosteric model for BK channels, we find these properties are explained by distinct and opposing actions of beta 4 on BK channels. beta 4 reduces channel opening by decreasing the intrinsic gating equilibrium (L sub(0)), and decreasing the allosteric coupling between calcium binding and voltage sensor activation (E). However, beta 4 has a compensatory effect on channel opening following depolarization by shifting open channel voltage sensor activation (Vh sub(o)) to more negative membrane potentials. The consequence is that beta 4 causes a net positive shift of the G-V relationship (relative to alpha subunit alone) at low calcium. At higher calcium, the contribution by Vh sub(o) and an increase in allosteric coupling to Ca super(2+) binding (C) promotes a negative G-V shift of alpha + beta 4 channels as compared to alpha subunits alone. This manner of modulation predicts that type II BK channels are downregulated by beta 4 at resting voltages through effects on L sub(0). 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BK channels are expressed in a broad variety of cells and have a corresponding diversity in properties. Underlying much of the functional diversity is a family of four tissue-specific accessory subunits ( beta 1- beta 4). Biophysical characterization has shown that the beta 4 subunit confers properties of the so-called "type II" BK channel isotypes seen in brain. These properties include slow gating kinetics and resistance to iberiotoxin and charybdotoxin blockade. In addition, the beta 4 subunit reduces the apparent voltage sensitivity of channel activation and has complex effects on apparent Ca super(2+) sensitivity. Specifically, channel activity at low Ca super(2+) is inhibited, while at high Ca super(2+), activity is enhanced. The goal of this study is to understand the mechanism underlying beta 4 subunit action in the context of a dual allosteric model for BK channel gating. We observed that beta 4's most profound effect is a decrease in P sub(o) (at least 11-fold) in the absence of calcium binding and voltage sensor activation. However, beta 4 promotes channel opening by increasing voltage dependence of P sub(o)-V relations at negative membrane potentials. In the context of the dual allosteric model for BK channels, we find these properties are explained by distinct and opposing actions of beta 4 on BK channels. beta 4 reduces channel opening by decreasing the intrinsic gating equilibrium (L sub(0)), and decreasing the allosteric coupling between calcium binding and voltage sensor activation (E). However, beta 4 has a compensatory effect on channel opening following depolarization by shifting open channel voltage sensor activation (Vh sub(o)) to more negative membrane potentials. The consequence is that beta 4 causes a net positive shift of the G-V relationship (relative to alpha subunit alone) at low calcium. At higher calcium, the contribution by Vh sub(o) and an increase in allosteric coupling to Ca super(2+) binding (C) promotes a negative G-V shift of alpha + beta 4 channels as compared to alpha subunits alone. This manner of modulation predicts that type II BK channels are downregulated by beta 4 at resting voltages through effects on L sub(0). However, beta 4 confers a compensatory effect on voltage sensor activation that increases channel opening during depolarization.</abstract><doi>10.1085/jgp.200509436</doi><tpages>17</tpages><oa>free_for_read</oa></addata></record> |
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| title | Mechanism of beta 4 Subunit Modulation of BK Channels |
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