Molecular origin of the L-type Ca2+ current of skeletal muscle myotubes selectively deficient in dihydropyridine receptor beta1a subunit - Wikidata - awgldk - TriplyDB

Molecular origin of the L-type Ca2+ current of skeletal muscle myotubes selectively deficient in dihydropyridine receptor beta1a subunit

Molecular origin of the L-type Ca2+ current of skeletal muscle myotubes selectively deficient in dihydropyridine receptor beta1a subunit

http://www.wikidata.org/entity/Q34168362

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Functional analysis of a frame-shift mutant of the dihydropyridine receptor pore subunit (alpha1S) expressing two complementary protein fragments A component of excitation-contraction coupling triggered in the absence of the T671-L690 and L720-Q765 regions of the II-III loop of the dihydropyridine receptor alpha(1s) pore subunit.Ca2+ sparks in embryonic mouse skeletal muscle selectively deficient in dihydropyridine receptor alpha1S or beta1a subunits.Mutations of calcium channel beta subunit genes in mice The beta 1a subunit is essential for the assembly of dihydropyridine-receptor arrays in skeletal muscle.Differential regulation of skeletal muscle L-type Ca2+ current and excitation-contraction coupling by the dihydropyridine receptor beta subunit.Involvement of the carboxy-terminus region of the dihydropyridine receptor beta1a subunit in excitation-contraction coupling of skeletal muscle Functional expression of the L-type calcium channel in mice skeletal muscle during prenatal myogenesis.Ca2+ current and charge movements in skeletal myotubes promoted by the beta-subunit of the dihydropyridine receptor in the absence of ryanodine receptor type 1.Ca2+-dependent excitation-contraction coupling triggered by the heterologous cardiac/brain DHPR beta2a-subunit in skeletal myotubes Intramembrane charge movements and excitation- contraction coupling expressed by two-domain fragments of the Ca2+ channel.Functional impact of the ryanodine receptor on the skeletal muscle L-type Ca(2+) channel Proper restoration of excitation-contraction coupling in the dihydropyridine receptor beta1-null zebrafish relaxed is an exclusive function of the beta1a subunit.Effects of mutations causing hypokalaemic periodic paralysis on the skeletal muscle L-type Ca2+ channel expressed in Xenopus laevis oocytes.

P2860

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P2860

Molecular origin of the L-type Ca2+ current of skeletal muscle myotubes selectively deficient in dihydropyridine receptor beta1a subunit

http://www.wikidata.org/entity/Q34168362

description

1998 nî lūn-bûn

@nan

1998 թուականի Յուլիսին հրատարակուած գիտական յօդուած

@hyw

1998 թվականի հուլիսին հրատարակված գիտական հոդված

@hy

1998年の論文

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1998年論文

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1998年論文

@zh-hant

1998年論文

@zh-hk

1998年論文

@zh-mo

1998年論文

@zh-tw

1998年论文

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name

Molecular origin of the L-type ...... ridine receptor beta1a subunit

@ast

Molecular origin of the L-type ...... ridine receptor beta1a subunit

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Molecular origin of the L-type ...... ridine receptor beta1a subunit

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type

label

Molecular origin of the L-type ...... ridine receptor beta1a subunit

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Molecular origin of the L-type ...... ridine receptor beta1a subunit

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Molecular origin of the L-type ...... ridine receptor beta1a subunit

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prefLabel

Molecular origin of the L-type ...... ridine receptor beta1a subunit

@ast

Molecular origin of the L-type ...... ridine receptor beta1a subunit

@en

Molecular origin of the L-type ...... ridine receptor beta1a subunit

@nl

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P1433

Biophysical Journal

P1476

Molecular origin of the L-type ...... ridine receptor beta1a subunit

@en

P2093

C A Ahern

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C Strube

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J A Powell

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M Beurg

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M Sukhareva

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P A Powers

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R Coronado

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R G Gregg

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P2860

Absence of the beta subunit (cchb1) of the skeletal muscle dihydropyridine receptor alters expression of the alpha 1 subunit and eliminates excitation-contraction coupling

Cloning and expression of a cardiac/brain beta subunit of the L-type calcium channel

Endogenous cardiac Ca2+ channels do not overcome the E-C coupling defect in immortalized dysgenic muscle cells: evidence for a missing link

Barium currents in developing skeletal muscle cells of normal and mutant mice foetuses with 'muscular dysgenesis'

A single nucleotide deletion in the skeletal muscle-specific calcium channel transcript of muscular dysgenesis (mdg) mice

Heterologous regulation of the cardiac Ca2+ channel alpha 1 subunit by skeletal muscle beta and gamma subunits. Implications for the structure of cardiac L-type Ca2+ channels.

Recovery of Ca2+ current, charge movements, and Ca2+ transients in myotubes deficient in dihydropyridine receptor beta 1 subunit transfected with beta 1 cDNA.

Calcium channel beta subunit heterogeneity: functional expression of cloned cDNA from heart, aorta and brain

Reduced Ca2+ current, charge movement, and absence of Ca2+ transients in skeletal muscle deficient in dihydropyridine receptor beta 1 subunit.

The beta subunit controls the gating and dihydropyridine sensitivity of the skeletal muscle Ca2+ channel.

P304

207-217

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10.1016/S0006-3495(98)77507-1

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1

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75

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13636154

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9649380

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1299692

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