Assessment of glucagon-like peptide-1 analogue and renin inhibitor on the binding and regulation of glp-1 receptor in type 1 diabetic rat hearts

Artinian S.B.; Al Lafi S.M.; Boutary S.S.; Bitar K.M.; Zwainy N.S.; Bikhazi A.B.

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dc.contributor.author	Artinian S.B.
dc.contributor.author	Al Lafi S.M.
dc.contributor.author	Boutary S.S.
dc.contributor.author	Bitar K.M.
dc.contributor.author	Zwainy N.S.
dc.contributor.author	Bikhazi A.B.
dc.contributor.editor
dc.date	2011
dc.date.accessioned	2017-10-04T10:31:28Z
dc.date.available	2017-10-04T10:31:28Z
dc.date.issued	2011
dc.identifier	10.1155/2011/489708
dc.identifier.isbn
dc.identifier.issn	16875214
dc.identifier.uri	http://hdl.handle.net/10938/13286
dc.description.abstract	This study focuses on the effects of long-term renin-angiotensin system suppression and-or incretin mimetic therapies on the regulation and binding affinity of GLP-1 to its receptor in the coronary endothelium (CE) and cardiomyocytes (CMs) of type 1 diabetic male Sprague-Dawley rats. The groups assessed are normal (N), streptozotocin-induced diabetic (D), Insulin treated (DI), Exendin-4 treated (DE), Aliskiren treated (DA), cotreated with Insulin and Aliskiren (DIA) and cotreated with exendin-4 and Aliskiren (DEA). Heart perfusion with 125I-GLP-1 was performed to estimate GLP-1 binding affinity (τ=1-k-n) to its receptor in the heart. Western Blotting was assessed to determine the expression variation of GLP-1 receptor in the heart. Plasma GLP-1 levels were measured using Enzyme-Linked Immunosorbent Assay (ELISA). Diabetes decreased the τ value on CE and increased it on CMs compared to normal. The combination of Exendin-4 with Aliskiren showed a normalizing effect on the binding affinity of GLP-1 at the coronary endothelium, while at the cardiomyocyte level Exendin-4 treatment alone was the most effective. Copyright 2011 Shushan B. Artinian et al.
dc.format.extent
dc.language	English
dc.publisher	NEW YORK
dc.relation.ispartof	Publication Name: Experimental Diabetes Research; Publication Year: 2011; Volume: 2011;
dc.relation.ispartofseries
dc.relation.uri
dc.source	Scopus
dc.subject.other
dc.title	Assessment of glucagon-like peptide-1 analogue and renin inhibitor on the binding and regulation of glp-1 receptor in type 1 diabetic rat hearts
dc.type	Article
dc.contributor.affiliation	Artinian, S.B., Department of Physiology, Faculty of Medicine, American University of Beirut, Beirut 11-236, Lebanon
dc.contributor.affiliation	Al Lafi, S.M., Department of Physiology, Faculty of Medicine, American University of Beirut, Beirut 11-236, Lebanon
dc.contributor.affiliation	Boutary, S.S., Department of Physiology, Faculty of Medicine, American University of Beirut, Beirut 11-236, Lebanon
dc.contributor.affiliation	Bitar, K.M., Department of Physics, Faculty of Arts and Sciences, American University of Beirut, Beirut 11-236, Lebanon
dc.contributor.affiliation	Zwainy, N.S., Department of Physiology, Faculty of Medicine, American University of Beirut, Beirut 11-236, Lebanon
dc.contributor.affiliation	Bikhazi, A.B., Department of Physiology, Faculty of Medicine, American University of Beirut, Beirut 11-236, Lebanon
dc.contributor.authorAddress	Bikhazi, A.B.; Department of Physiology, Faculty of Medicine, American University of Beirut, Beirut 11-236, Lebanon; email: ab04@aub.edu.lb
dc.contributor.authorCorporate	University: American University of Beirut; Faculty: Faculty of Arts and Sciences; Department: Physics;
dc.contributor.authorDepartment	Physics
dc.contributor.authorDivision
dc.contributor.authorEmail	ab04@aub.edu.lb
dc.contributor.faculty	Faculty of Arts and Sciences
dc.contributor.authorInitials	Artinian, SB
dc.contributor.authorInitials	Al Lafi, SM
dc.contributor.authorInitials	Boutary, SS
dc.contributor.authorInitials	Bitar, KM
dc.contributor.authorInitials	Zwainy, NS
dc.contributor.authorInitials	Bikhazi, AB
dc.contributor.authorOrcidID
dc.contributor.authorReprintAddress	Bikhazi, AB (reprint author), Amer Univ Beirut, Fac Med, Dept Physiol, Beirut 11236, Lebanon.
dc.contributor.authorResearcherID
dc.contributor.authorUniversity	American University of Beirut
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dc.description.citedCount	2
dc.description.citedTotWOSCount	1
dc.description.citedWOSCount	1
dc.format.extentCount	1
dc.identifier.articleNo	489708
dc.identifier.coden
dc.identifier.pubmedID
dc.identifier.scopusID	80052749880
dc.identifier.url
dc.publisher.address	410 PARK AVENUE, 15TH FLOOR, #287 PMB, NEW YORK, NY 10022 USA
dc.relation.ispartofConference
dc.relation.ispartofConferenceCode
dc.relation.ispartofConferenceDate
dc.relation.ispartofConferenceHosting
dc.relation.ispartofConferenceLoc
dc.relation.ispartofConferenceSponsor
dc.relation.ispartofConferenceTitle
dc.relation.ispartofFundingAgency
dc.relation.ispartOfISOAbbr	Exp. Diabetes Res.
dc.relation.ispartOfIssue
dc.relation.ispartOfPart
dc.relation.ispartofPubTitle	Experimental Diabetes Research
dc.relation.ispartofPubTitleAbbr	Exp. Dia. Res.
dc.relation.ispartOfSpecialIssue
dc.relation.ispartOfSuppl
dc.relation.ispartOfVolume	2011
dc.source.ID	WOS:000293565800001
dc.type.publication	Journal
dc.subject.otherAuthKeyword
dc.subject.otherChemCAS	aliskiren, 173334-57-1, 173334-58-2, 173399-03-6
dc.subject.otherChemCAS	bovine insulin, 11070-73-8
dc.subject.otherChemCAS	exendin 4, 141732-76-5, 141758-74-9
dc.subject.otherChemCAS	insulin glargine, 160337-95-1
dc.subject.otherChemCAS	iodine 125, 14158-31-7, 22822-81-7
dc.subject.otherIndex	aliskiren
dc.subject.otherIndex	bovine insulin
dc.subject.otherIndex	exendin 4
dc.subject.otherIndex	glucagon like peptide 1 derivative
dc.subject.otherIndex	glucagon like peptide 1 receptor
dc.subject.otherIndex	insulin glargine
dc.subject.otherIndex	iodine 125
dc.subject.otherIndex	renin inhibitor
dc.subject.otherIndex	animal cell
dc.subject.otherIndex	animal experiment
dc.subject.otherIndex	animal model
dc.subject.otherIndex	article
dc.subject.otherIndex	binding affinity
dc.subject.otherIndex	body weight
dc.subject.otherIndex	controlled stu
dc.subject.otherKeywordPlus	MELLITUS
dc.subject.otherKeywordPlus	MODEL
dc.subject.otherWOS	Endocrinology and Metabolism
dc.subject.otherWOS	Medicine, Research and Experimental

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