The Ca
            <sub>V</sub>
            3.2 T-Type Ca
            <sup>2+</sup>
            Channel Is Required for Pressure Overload–Induced Cardiac Hypertrophy in Mice

Chiang, Chien-Sung; Huang, C. C.; Chieng, Hockling; Chang, Yao-Tang; Chang, Dory; Chen, Ji-Jr; Chen, Yong-Cyuan; Chen, Yen‐Hui; Shin, Hee‐Sup; Campbell, Kevin P.; Chen, Chien‐Chang

doi:10.1161/circresaha.108.184051

Cited by 143 publications

(131 citation statements)

References 51 publications

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“…Ca V 3.2 is also preferentially expressed in fetal ventricles, but less so in adult ventricles, and therefore the T-type Ca 21 current is very small or even undetectable in adult ventricular myocytes (Perez-Reyes 2003;Chiang et al 2009). ACMs from both day-1 (Figures 6A-6C) and aged ( Figures 6D-6F) hearts also expressed Ca V 3.2 predominantly in the intracellular space rather than the cell periphery, whereas very weak signals were detected near the plasma membrane in adult cardiac ventricular myocytes ( Figures 6G-6I).…”

Section: Expression Of Fetal Cardiac Gene Products Anp and Ca V 32 Imentioning

confidence: 99%

Self-beating Atypically Shaped Cardiomyocytes Survive a Long-term Postnatal Development While Preserving the Expression of Fetal Cardiac Genes in Mice

Omatsu‐Kanbe

Yamamoto

Mori

et al. 2010

J Histochem Cytochem.

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S U M M A R Y The present study was designed to examine the postnatal developmental changes of atypically shaped cardiomyocytes (ACMs) prepared from the heart of newborn [postnatal day 1 (day-1)] through aged (12-month-old) mice. ACMs were identified as a novel type of self-beating cardiomyocyte with a peculiar morphology in mouse cardiac ventricles. The cell length of ACMs significantly increased during the first three postnatal months and further increased over the following 9 months. In contrast, the population of ACMs was significantly decreased within the first 5 weeks and reached a plateau in the adult stage. ACMs obtained from newborn and adult mice exhibited similar spontaneous action potentials. The expression of the fetal cardiac gene products atrial natriuretic peptide and voltage-gated T-type Ca 21 channel Ca V 3.2 was confirmed by immunostaining in ACMs obtained from both newborn and aged mice. These observations provide evidence that ACMs that exhibit spontaneous beating survive the long-term postnatal development of cardiac ventricles while preserving the expression of fetal cardiac genes. This manuscript contains online supplemental material at http://www.jhc.org. Please visit this article online to view these materials. (J Histochem Cytochem 58:543-551, 2010)

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Section: Expression Of Fetal Cardiac Gene Products Anp and Ca V 32 Imentioning

confidence: 99%

Self-beating Atypically Shaped Cardiomyocytes Survive a Long-term Postnatal Development While Preserving the Expression of Fetal Cardiac Genes in Mice

Omatsu‐Kanbe

Yamamoto

Mori

et al. 2010

J Histochem Cytochem.

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“…23 It has been recently reported that CaV3.2 (Cacna1h) is required for cardiac hypertrophy induced by pressure overload. 24 Likewise, crossbreeding of dnNRSF mice with transgenic mice lacking the target genes of REST/NRSF might provide a clue.…”

Section: Study Limitationsmentioning

confidence: 99%

Pathophysiological Remodeling of Mouse Cardiac Myocytes Expressing Dominant Negative Mutant of Neuron Restrictive Silencing Factor

Takano

Kinoshita

Shioya

et al. 2010

Circ J

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“…However, Ca V 3.1 and Ca V 3.2 channels are also expressed in the heart where they are involved in pacemaking in the sinoatrial node (Ca V 3.1; 43 ) as well as in ventricular hypertrophy where Ca V 3.1 and Ca V 3.2 channels seem to play opposite roles. 44,45 Moreover, in resistance vessels Ca V 3.1 and Ca V 3.2 T-type channel protein expression has been demonstrated by immunolocalization to VSMCs 46-51 as well as ECs. 48,49,51,52 Interestingly, in human cerebral arteries the T-type isoforms expressed are the Ca V 3.2 and Ca V 3.3 channels, with no expression of Ca V 3.1 channels.…”

mentioning

confidence: 99%

T-type Ca²⁺channels and autoregulation of local blood flow

et al. 2017

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L-type voltage gated Ca2C channels are considered to be the primary source of calcium influx during the myogenic response. However, many vascular beds also express T-type voltage gated Ca 2C channels. Recent studies suggest that these channels may also play a role in autoregulation. At low pressures (40-80 mmHg) T-type channels affect myogenic responses in cerebral and mesenteric vascular beds. T-type channels also seem to be involved in skeletal muscle autoregulation. This review discusses the expression and role of T-type voltage gated Ca 2C channels in the autoregulation of several different vascular beds. Lack of specific pharmacological inhibitors has been a huge challenge in the field. Now the research has been strengthened by genetically modified models such as mice lacking expression of T-type voltage gated Ca 2C channels (Ca V 3.1 and Ca V 3.2). Hopefully, these new tools will help further elucidate the role of voltage gated T-type Ca 2C channels in autoregulation and vascular function.

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The Ca _V 3.2 T-Type Ca ²⁺ Channel Is Required for Pressure Overload–Induced Cardiac Hypertrophy in Mice

Cited by 143 publications

References 51 publications

Self-beating Atypically Shaped Cardiomyocytes Survive a Long-term Postnatal Development While Preserving the Expression of Fetal Cardiac Genes in Mice

Self-beating Atypically Shaped Cardiomyocytes Survive a Long-term Postnatal Development While Preserving the Expression of Fetal Cardiac Genes in Mice

Pathophysiological Remodeling of Mouse Cardiac Myocytes Expressing Dominant Negative Mutant of Neuron Restrictive Silencing Factor

T-type Ca²⁺channels and autoregulation of local blood flow

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The Ca V 3.2 T-Type Ca 2+ Channel Is Required for Pressure Overload–Induced Cardiac Hypertrophy in Mice

Cited by 143 publications

References 51 publications

Self-beating Atypically Shaped Cardiomyocytes Survive a Long-term Postnatal Development While Preserving the Expression of Fetal Cardiac Genes in Mice

Self-beating Atypically Shaped Cardiomyocytes Survive a Long-term Postnatal Development While Preserving the Expression of Fetal Cardiac Genes in Mice

Pathophysiological Remodeling of Mouse Cardiac Myocytes Expressing Dominant Negative Mutant of Neuron Restrictive Silencing Factor

T-type Ca2+channels and autoregulation of local blood flow

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Product

Resources

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The Ca _V 3.2 T-Type Ca ²⁺ Channel Is Required for Pressure Overload–Induced Cardiac Hypertrophy in Mice

T-type Ca²⁺channels and autoregulation of local blood flow