Primary Structure of the γ Subunit of the DHP-Sensitive Calcium Channel from Skeletal Muscle

Jay, Scott D.; Ellis, Steven B.; McCue, Ann F.; Williams, Mark E.; Vedvick, Thomas S.; Harpold, Michael M.; Campbell, Kevin P.

doi:10.1126/science.2158672

Cited by 257 publications

(123 citation statements)

References 29 publications

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“…We found expressed sequences corresponding to CACNG5 by PCR amplification of a human fetal kidney cDNA library but did not exclude the possibility of CACNG5 expression in the brain or other tissues. It is worth noting that several tissues that express multiple ␣ 1 , ␤, and ␣ 2 ␦ subunit isoforms, including testes, ovary, lung, pancreas, spleen, liver, and kidney, do not express ␥ 1 or ␥ 2 (Biel et al 1990;Jay et al 1990;Castellano and Perez-Reyes 1994;Yu 1995;Williams et al 1999). The ␥ 3 , ␥ 4 , and ␥ 5 isoforms are possible components of Ca 2+ channels in these tissues.…”

Section: Role Of ␥ Subunits In Ca 2+ Channel Functionmentioning

confidence: 99%

“…Expression of a single isoform in neurons distinguishes the ␥ subunit from other Ca 2+ channel subunits, which utilize genetic heterogeneity as an important mechanism for generating functional diversity in these cells. In addition, the expression of significant levels of either CACNG1 or CACNG2 mRNA has not been reported in tissues such as heart, kidney, and testis, which express high levels of other Ca 2+ channel subunits and produce measurable Ca 2+ currents (Jay et al 1990; Letts et al 1998). We therefore hypothesized the existence of additional ␥ subunit genes.…”

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confidence: 99%

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Identification of Three Novel Ca²⁺ Channel γ Subunit Genes Reveals Molecular Diversification by Tandem and Chromosome Duplication

Burgess¹,

Davis²,

Gefrides³

et al. 1999

Genome Res.

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Gene duplication is believed to be an important evolutionary mechanism for generating functional diversity within genomes. The accumulated products of ancient duplication events can be readily observed among the genes encoding voltage-dependent Ca2+ ion channels. Ten paralogous genes have been identified that encode isoforms of the α1 subunit, four that encode β subunits, and three that encode α2δ subunits. Until recently, only a single gene encoding a muscle-specific isoform of the Ca2+ channel γ subunit (CACNG1) was known. Expression of a distantly related gene in the brain was subsequently demonstrated upon isolation of the Cacng2 gene, which is mutated in the mouse neurological mutant stargazer (stg). In this study, we sought to identify additional genes that encoded γ subunits. Because gene duplication often generates paralogs that remain in close syntenic proximity (tandem duplication) or are copied onto related daughter chromosomes (chromosome or whole-genome duplication), we hypothesized that the known positions of CACNG1 andCACNG2 could be used to predict the likely locations of additional γ subunit genes. Low-stringency genomic sequence analysis of targeted regions led to the identification of three novel Ca2+ channel γ subunit genes, CACNG3,CACNG4, and CACNG5, on chromosomes 16 and 17. These results demonstrate the value of genome evolution models for the identification of distantly related members of gene families.[The sequence data described in this paper have been submitted to the GenBank data library under accession numbersAF142618–AF142625 and AF148220.]

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Section: Role Of ␥ Subunits In Ca 2+ Channel Functionmentioning

confidence: 99%

mentioning

confidence: 99%

Identification of Three Novel Ca²⁺ Channel γ Subunit Genes Reveals Molecular Diversification by Tandem and Chromosome Duplication

Burgess¹,

Davis²,

Gefrides³

et al. 1999

Genome Res.

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“…The first γ 1 subunit was cloned from skeletal muscle [44,45], whereas it was not expressed in cardiac muscle [46]. The γ subunit distinguishingly modulates the functions by altering both activation and inactivation properties of LTCC [46].…”

Section: Molecular Basis Of L-type Calcium Channelmentioning

confidence: 99%

Mutations in voltage-gated L-type calcium channel: implications in cardiac arrhythmia

et al. 2018

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The voltage-gated L-type calcium channel (LTCC) is essential for multiple cellular processes. In the heart, calcium influx through LTCC plays an important role in cardiac electrical excitation. Mutations in LTCC genes, including CACNA1C, CACNA1D, CACNB2 and CACNA2D, will induce the dysfunctions of calcium channels, which result in the abnormal excitations of cardiomyocytes, and finally lead to cardiac arrhythmias. Nevertheless, the newly found mutations in LTCC and their functions are continuously being elucidated. This review summarizes recent findings on the mutations of LTCC, which are associated with long QT syndromes, Timothy syndromes, Brugada syndromes, short QT syndromes, and some other cardiac arrhythmias. Indeed, we describe the gain/loss-of-functions of these mutations in LTCC, which can give an explanation for the phenotypes of cardiac arrhythmias. Moreover, we present several challenges in the field at present, and propose some diagnostic or therapeutic approaches to these mutation-associated cardiac diseases in the future.

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“…2) (Ruth et al 1989), whereas the g subunit is a glycoprotein with four transmembrane segments ( Fig. 2) (Jay et al 1990). The cloned a2 subunit has many glycosylation sites and several hydrophobic sequences (Ellis et al 1988), but biosynthesis studies indicate that it is an extracellular, extrinsic membrane glycoprotein, attached to the membrane through disulfide linkage to the d subunit ( Fig.…”

Section: Molecular Properties Of Ca 2þ Channels Subunit Structurementioning

confidence: 99%

Voltage-Gated Calcium Channels

Zamponi

2015

Encyclopedia of Psychopharmacology

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Voltage-gated calcium (Ca 2þ ) channels are key transducers of membrane potential changes into intracellular Ca 2þ transients that initiate many physiological events. There are ten members of the voltage-gated Ca 2þ channel family in mammals, and they serve distinct roles in cellular signal transduction. The Ca V 1 subfamily initiates contraction, secretion, regulation of gene expression, integration of synaptic input in neurons, and synaptic transmission at ribbon synapses in specialized sensory cells. The Ca V 2 subfamily is primarily responsible for initiation of synaptic transmission at fast synapses. The Ca V 3 subfamily is important for repetitive firing of action potentials in rhythmically firing cells such as cardiac myocytes and thalamic neurons. This article presents the molecular relationships and physiological functions of these Ca 2þ channel proteins and provides information on their molecular, genetic, physiological, and pharmacological properties.

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Primary Structure of the γ Subunit of the DHP-Sensitive Calcium Channel from Skeletal Muscle

Cited by 257 publications

References 29 publications

Identification of Three Novel Ca²⁺ Channel γ Subunit Genes Reveals Molecular Diversification by Tandem and Chromosome Duplication

Identification of Three Novel Ca²⁺ Channel γ Subunit Genes Reveals Molecular Diversification by Tandem and Chromosome Duplication

Mutations in voltage-gated L-type calcium channel: implications in cardiac arrhythmia

Voltage-Gated Calcium Channels

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Primary Structure of the γ Subunit of the DHP-Sensitive Calcium Channel from Skeletal Muscle

Cited by 257 publications

References 29 publications

Identification of Three Novel Ca2+ Channel γ Subunit Genes Reveals Molecular Diversification by Tandem and Chromosome Duplication

Identification of Three Novel Ca2+ Channel γ Subunit Genes Reveals Molecular Diversification by Tandem and Chromosome Duplication

Mutations in voltage-gated L-type calcium channel: implications in cardiac arrhythmia

Voltage-Gated Calcium Channels

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Identification of Three Novel Ca²⁺ Channel γ Subunit Genes Reveals Molecular Diversification by Tandem and Chromosome Duplication

Identification of Three Novel Ca²⁺ Channel γ Subunit Genes Reveals Molecular Diversification by Tandem and Chromosome Duplication