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Voltage sensor

Ca2+ Channel Blockers. Figure 1 Most voltage-gated Ca2+ channels exist as a hetero-oligomeric complex of several subunits, a 1 subunits form the Ca2+-selective ion pore and contain the voltage-sensors of the channel. [Pg.296]

DICR (depolarization-induced Ca2+ release) is Ca2+ release triggered by depolarization of the sarcolemma. In skeletal muscle, conformational change in the voltage sensor (a 1S subunit of the dihydropyridine receptor) in the T-tubule is directly transmitted to the... [Pg.426]

Dihydropyridine receptor (DHPR) is a member of voltage-dqiendent Ca2+ channels (CaVi, L-type), which specifically binds to dihydropyridine derivatives, a group of the Ca2+ channel blockers. Cav 1.1 works as the voltage sensor for skeletal muscle contraction, and Cay 1.2, as Ca2+-influx channel for cardiac muscle contraction. [Pg.427]

HVA calcium channels are biochemically hetero-oligomeric complexes of five proteins encoded by four gene families (Fig. 1) The ax subunits of 190-250 kDa contain the voltage-sensor, the selectivity filter, the ion-conducting pore, the binding sites for most calcium... [Pg.1302]

The voltage sensor is the part of a channel protein responsible for detection of the membrane potential. A voltage sensor of the voltage-dependent Na+ channel was predicted by Hodgkin and Huxley in 1952. Positively charged amino acid residues in S4 of each repeat play an essential role as the voltage sensor. [Pg.1313]

According to Schneider and Chandler (1973), depolarization of the T-tubules affects sensors which open Ca " channels in the SR. The sensors are modified Ca channels which act as voltage sensors (Tanabe et al., 1987). The signal from the sensor reaches the SR and opens the Ca channels with the release of Ca to the myoplasm. The Ca channels in the SR system are opened by micromolar [Ca ], mM [ATP], and caffeine but are inhibited by Mg (Smith et al., 1986 Rosseau et al., 1988). The channels are closed in resting muscle and are opened when the voltage sensor is activated. [Pg.247]

Possible mechanisms responsible for the decreased Ca release are changes in the sensitivity of the voltage sensor in the T-tubular system or in the SR Ca channel to the sensor stimulus. A third possibility would be a decreased availability... [Pg.247]

Fig. 16.1 Sodium channel structure. Schematic representation of the sodium channel subunits, a, ySl and / 2. (A) The a-subunit consists of four homologous intracelIularly linked domains (I—IV) each consisting of six connected segments (1-6). The segment 4 of each of the domains acts as the voltage sensor, physically moving out in response to depolarization resulting in activation of the sodium channel. The channel is inactivated rapidly by the linker region between III and IV docking on to the acceptor site formed by the cytoplasmic ends of S5 and S6 of domain IV. The / -subunits have a common structure, with the / 1 non-covalently bound, and f 2 linked by disulfide bonds to the a-channel... Fig. 16.1 Sodium channel structure. Schematic representation of the sodium channel subunits, a, ySl and / 2. (A) The a-subunit consists of four homologous intracelIularly linked domains (I—IV) each consisting of six connected segments (1-6). The segment 4 of each of the domains acts as the voltage sensor, physically moving out in response to depolarization resulting in activation of the sodium channel. The channel is inactivated rapidly by the linker region between III and IV docking on to the acceptor site formed by the cytoplasmic ends of S5 and S6 of domain IV. The / -subunits have a common structure, with the / 1 non-covalently bound, and f 2 linked by disulfide bonds to the a-channel...
Structural models for voltage-dependent gating of ion channels must identify the voltage-sensors or gating charges (Fig. 6-5A) within the channel structure and suggest a plausible mechanism for transmembrane movement... [Pg.105]

Bezanilla, F. The voltage sensor in voltage dependent ion channels. Physiol. Rev. 80, 555-592, 2000. [Pg.109]


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See also in sourсe #XX -- [ Pg.21 , Pg.22 ]

See also in sourсe #XX -- [ Pg.21 , Pg.22 ]




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