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dc.contributor.authorTajada, Sendoa
dc.contributor.authorCidad, Pilar
dc.contributor.authorColinas, Olaia
dc.contributor.authorSantana, L. Fernando
dc.contributor.authorLópez‐López, José R.
dc.contributor.authorPérez‐García, M. Teresa
dc.date.accessioned2024-02-06T09:36:36Z
dc.date.available2024-02-06T09:36:36Z
dc.date.issued2013
dc.identifier.citationJ Physiol. 2013 Dec 15;591(24):6175-91es
dc.identifier.issn0022-3751es
dc.identifier.urihttps://uvadoc.uva.es/handle/10324/65780
dc.description.abstractHypertension is a clinical syndrome characterized by increased arterial tone. Although the mechanisms are varied, the generally accepted view is that increased CaV1.2 channel function is a common feature of this pathological condition. Here, we investigated the mechanisms underlying vascular dysfunction in a mouse model of genetic hypertension. Contrary to expectation, we found that whole-cell CaV1.2 currents (ICa) were lower in hypertensive (BPH line) than normotensive (BPN line) myocytes. However, local CaV1.2 sparklet activity was higher in BPH cells, suggesting that the relatively low ICa in these cells was produced by a few hyperactive CaV1.2 channels. Furthermore, our data suggest that while the lower expression of the pore-forming α1c subunit of CaV1.2 currents underlies the lower ICa in BPH myocytes, the increased sparklet activity was due to a different composition in the auxiliary subunits of the CaV1.2 complexes. ICa currents in BPN cells were produced by channels composed of α1c/α2δ/β3 subunits, while in BPH myocytes currents were probably generated by the opening of channels formed by α1c/α2δ/β2 subunits. In addition, Ca(2+) sparks evoked large conductance, Ca(2+)-activated K(+) (BK) currents of lower magnitude in BPH than in BPN myocytes, because BK channels were less sensitive to Ca(2+). Our data are consistent with a model in which a decrease in the global number of CaV1.2 currents coexist with the existence of a subpopulation of highly active channels that dominate the resting Ca(2+) influx. The decrease in BK channel activity makes the hyperpolarizing brake ineffective and leads BPH myocytes to a more contracted resting state.es
dc.format.mimetypeapplication/pdfes
dc.language.isospaes
dc.rights.accessRightsinfo:eu-repo/semantics/openAccesses
dc.titleDown‐regulation of CaV1.2 channels during hypertension: how fewer CaV1.2 channels allow more Ca2+ into hypertensive arterial smooth musclees
dc.typeinfo:eu-repo/semantics/articlees
dc.identifier.doi10.1113/JPHYSIOL.2013.265751es
dc.identifier.publicationfirstpage6175es
dc.identifier.publicationissue24es
dc.identifier.publicationlastpage6191es
dc.identifier.publicationtitleThe Journal of Physiologyes
dc.identifier.publicationvolume591es
dc.peerreviewedSIes
dc.identifier.essn1469-7793es
dc.type.hasVersioninfo:eu-repo/semantics/draftes


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