Please use this identifier to cite or link to this item: http://hdl.handle.net/10553/48717
DC FieldValueLanguage
dc.contributor.authorRodriguezPerez, JCen_US
dc.contributor.authorLosada, Antonioen_US
dc.contributor.authorAnabitarte, Aranzazuen_US
dc.contributor.authorCabrera, Juanen_US
dc.contributor.authorLlobet, Javieren_US
dc.contributor.authorPalop, Leocadiaen_US
dc.contributor.authorPlaza, Celiaen_US
dc.contributor.otherRodriguez-Perez, J.C.-
dc.contributor.otherCabrera-Galvan, Juan Jose-
dc.date.accessioned2018-11-24T00:19:21Z-
dc.date.available2018-11-24T00:19:21Z-
dc.date.issued1997en_US
dc.identifier.issn0022-3565en_US
dc.identifier.urihttp://hdl.handle.net/10553/48717-
dc.description.abstractAntihypertensive drugs have differing effects on renal hemodynamics and morphology. We analyzed whether the use of a new beta adrenoceptor antagonist and vasodilator, carvedilol (CVD), slows the progression of nephrosclerosis and whether the renoprotective effect as well as reduction in cardiac hypertrophy is dependent on the degree of blood pressure reduction. Fifty-four adult male Sprague-Dawley rats were distributed among five groups: group I served as untreated controls with 5/6 nephrectomy (Nx); group II, sham (no renal ablation or drug treatment); group III, CVD 5 (5/6 Nx and treatment with oral CVD at 5 mg/kg/day); group IV, CVD 10 (5/6 Nx and treatment with oral CVD at 10 mg/kg/day); and group V, CVD 20 (5/6 Nx and treatment with oral CVD at 20 mg/kg/day). Tail-cuff blood pressure and 24-hr urine samples were obtained before and at 3, 5 and II weeks of treatment with CVD. At the end of the study period, blood was taken to measure serum creatinine, plasma renin activity and CVD levels, as well as the remnant kidney and heart for morphological studies. There was a significant reduction in 24-hr U-ProtV in all the CVD-treated groups, and it was increasingly evident with the highest dose used. However, only rats receiving doses of 10 and 20 mg/kg/day of CVD exhibited significant decreases in blood pressure. Elevated serum creatinine levels seen in untreated controls were significantly decreased by CVD in treated rats (P < .01), indicating that. glomerular filtration rate was improved by this drug. This was associated with a significant increase in U-NaV. Concomitant and significant (P < .01) decreases in plasma renin activity were observed in sham and CVD-treated rats. CVD-treated animals had considerably reduced renal damage (P < .01) and cardiac hypertrophy (P < .01) compared with untreated controls. These data indicate that CVD is effective in delaying progression of renal damage and provides beneficial effects in the remnant kidney and cardiac hypertrophy, even at nonhypotensive doses.en_US
dc.languageengen_US
dc.relation.ispartofJournal of Pharmacology and Experimental Therapeuticsen_US
dc.sourceJournal Of Pharmacology And Experimental Therapeutics[ISSN 0022-3565],v. 283 (1), p. 336-344en_US
dc.subject32 Ciencias médicasen_US
dc.subject3209 Farmacologíaen_US
dc.subject.otherRemnant Kidney Modelen_US
dc.subject.otherGlomerular Injuryen_US
dc.subject.otherSegmental Glomerulosclerosisen_US
dc.subject.otherCell-Proliferationen_US
dc.subject.otherHypertensionen_US
dc.subject.otherDiseaseen_US
dc.subject.otherAngiotensinen_US
dc.subject.otherProteinuriaen_US
dc.subject.otherProgressionen_US
dc.subject.otherAldosteroneen_US
dc.titleEffects of the novel multiple-action agent carvedilol on severe nephrosclerosis in renal ablated ratsen_US
dc.typeinfo:eu-repo/semantics/Articleen_US
dc.typeArticleen_US
dc.identifier.scopus0030803698-
dc.identifier.isiA1997YC30100041-
dcterms.isPartOfJournal Of Pharmacology And Experimental Therapeutics-
dcterms.sourceJournal Of Pharmacology And Experimental Therapeutics[ISSN 0022-3565],v. 283 (1), p. 336-344-
dc.contributor.authorscopusid7005446255-
dc.contributor.authorscopusid16223508500-
dc.contributor.authorscopusid6505823547-
dc.contributor.authorscopusid6602257053-
dc.contributor.authorscopusid57197368765-
dc.contributor.authorscopusid7004690031-
dc.contributor.authorscopusid7005227541-
dc.description.lastpage344en_US
dc.description.firstpage336en_US
dc.relation.volume283en_US
dc.investigacionCiencias de la Saluden_US
dc.type2Artículoen_US
dc.identifier.wosWOS:A1997YC30100041-
dc.contributor.daisngid245684-
dc.contributor.daisngid13476259-
dc.contributor.daisngid612527-
dc.contributor.daisngid3092642-
dc.contributor.daisngid1841045-
dc.contributor.daisngid101887-
dc.contributor.daisngid14385204-
dc.contributor.daisngid751953-
dc.contributor.daisngid1265413-
dc.contributor.daisngid315895-
dc.identifier.investigatorRIDC-1247-2010-
dc.identifier.investigatorRIDNo ID-
dc.description.numberofpages9en_US
dc.utils.revisionen_US
dc.contributor.wosstandardWOS:RodriguezPerez, JC-
dc.contributor.wosstandardWOS:Losada, A-
dc.contributor.wosstandardWOS:Anabitarte, A-
dc.contributor.wosstandardWOS:Cabrera, J-
dc.contributor.wosstandardWOS:Llobet, J-
dc.contributor.wosstandardWOS:Palop, L-
dc.contributor.wosstandardWOS:Plaza, C-
dc.date.coverdateOctubre 1997en_US
dc.identifier.ulpgcen_US
dc.contributor.buulpgcBU-MEDen_US
dc.description.jcr3,227-
dc.description.jcrqQ1-
dc.description.scieSCIE-
item.grantfulltextnone-
item.fulltextSin texto completo-
crisitem.author.deptGIR IUIBS: Patología y Tecnología médica-
crisitem.author.deptIU de Investigaciones Biomédicas y Sanitarias-
crisitem.author.deptGIR IUIBS: Farmacología Molecular y Traslacional-
crisitem.author.deptIU de Investigaciones Biomédicas y Sanitarias-
crisitem.author.orcid0000-0003-0023-1063-
crisitem.author.orcid0000-0002-4184-6403-
crisitem.author.parentorgIU de Investigaciones Biomédicas y Sanitarias-
crisitem.author.parentorgIU de Investigaciones Biomédicas y Sanitarias-
crisitem.author.fullNameRodríguez Pérez,José Carlos-
crisitem.author.fullNameCabrera Galván,Juan José-
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