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HIV-1 integrase: From biology to chemotherapeuticsAAA

dc.contributor.authorZeinalipour-Loizidou, E.en
dc.contributor.authorNicolaou, Charalambos P.en
dc.contributor.authorNicolaïdes, Andrew N.en
dc.contributor.authorKostrikis, Leontios G.en
dc.creatorZeinalipour-Loizidou, E.en
dc.creatorNicolaou, Charalambos P.en
dc.creatorNicolaïdes, Andrew N.en
dc.creatorKostrikis, Leontios G.en
dc.date.accessioned2019-11-21T06:23:35Z
dc.date.available2019-11-21T06:23:35Z
dc.date.issued2007
dc.identifier.issn1570-162X
dc.identifier.urihttp://gnosis.library.ucy.ac.cy/handle/7/56297
dc.description.abstractAIDS has claimed the lives of 25 million people worldwide, an additional 40 million people are HIV-infected and new cases are being diagnosed every year. Despite the fact that HAART has moved AIDS from the category of terminal diseases to that of treatable chronic illnesses, its long-term therapeutic success may be compromised by the development of resistance to the currently used drugs. Despite the availability of RT, PR and fusion inhibitors, the development of further drugs such as inhibitors that target the third enzyme IN is essential for the clinical management of HIV-infected patients. The absence of cellular homolgues to IN and the unique nature of the reactions catalyzed by IN, make it an ideal target for drug design. Considerable progress towards designing HIV-1 IN inhibitors has been made over the last years and several lead compounds have been identified, synthesized and clinically studied. This review focuses on the existing knowledge of the biology of HIV-1 IN with emphasis on the mechanism of integration, structure and function and the technologies for measuring IN activity. This is followed by the current trends on designing HIV-1 IN inhibitors with the aid of molecular informatics and a review on the main classes of HIV-1 IN inhibitors reported this far with special emphasis on the clinical candidates. © 2007 Bentham Science Publishers Ltd.en
dc.sourceCurrent HIV Researchen
dc.source.urihttps://www.scopus.com/inward/record.uri?eid=2-s2.0-34447280643&doi=10.2174%2f157016207781023965&partnerID=40&md5=63ed1ea3a93cd2761111607c25abdc93
dc.subjecthumanen
dc.subjectHumansen
dc.subjectclinical trialen
dc.subjectreviewen
dc.subjectunindexed drugen
dc.subjectunclassified drugen
dc.subjectnonhumanen
dc.subjectdrug withdrawalen
dc.subjectdrug potentiationen
dc.subjectdrug targetingen
dc.subjectantiinfective agenten
dc.subjecthighly active antiretroviral therapyen
dc.subjectvirus loaden
dc.subjectvirus RNAen
dc.subjectenzyme activityen
dc.subjectHuman immunodeficiency virus 1en
dc.subjectantiretrovirus agenten
dc.subjectvirus replicationen
dc.subjectantivirus agenten
dc.subjectHuman immunodeficiency virus 1 infectionen
dc.subjectvirus DNAen
dc.subjectantiviral activityen
dc.subjectreal time polymerase chain reactionen
dc.subjectmolecular mechanicsen
dc.subjectAnti-Retroviral Agentsen
dc.subjectX ray crystallographyen
dc.subjectdrug designen
dc.subjectDNA integrationen
dc.subjectHIV Integraseen
dc.subjectHIV Integrase Inhibitorsen
dc.subjectintegraseen
dc.subjectintegrase inhibitoren
dc.subjectdrug potencyen
dc.subjecthigh throughput screeningen
dc.subjectquantitative structure activity relationen
dc.subjectHIV-1 integraseen
dc.subjectInhibitorsen
dc.subject1 [5 (4 fluorobenzyl) 2 furyl] 3 (1,2,4 triazol 3 yl) 1,3 propanedioneen
dc.subjectcichoric aciden
dc.subjectcomputer aided designen
dc.subjectComputer-Aided Designen
dc.subjectComputer-aided drug designen
dc.subjectcurcuminen
dc.subjectdicaffeoylquinic aciden
dc.subjectDNA bindingen
dc.subjectenzyme structureen
dc.subjectfz 41en
dc.subjectgs 1937en
dc.subjectgs 9137en
dc.subjectindolicidinen
dc.subjectindolicidin derivativeen
dc.subjectl 870712en
dc.subjectl 870812en
dc.subjectl 900612en
dc.subjectlife cycleen
dc.subjectmercaptosalicylhydrazideen
dc.subjectn (4 fluorobenzyl) 8 hydroxy 5 (tetrahydro 2h 1,2 thiazin 2 yl) 1,6 naphthyridine 7 carboxamide s,s dioxideen
dc.subjectprotein GAP31en
dc.subjectprotein K159en
dc.subjectprotein MAP30en
dc.subjectsalicylhydrazideen
dc.subjectsuraminen
dc.subjectthalassiolin aen
dc.subjectthalassiolin Ben
dc.subjectthalassiolin Cen
dc.subjectv 165en
dc.subjectzinteviren
dc.titleHIV-1 integrase: From biology to chemotherapeuticsAAAen
dc.typeinfo:eu-repo/semantics/article
dc.identifier.doi10.2174/157016207781023965
dc.description.volume5
dc.description.issue4
dc.description.startingpage365
dc.description.endingpage388
dc.author.faculty002 Σχολή Θετικών και Εφαρμοσμένων Επιστημών / Faculty of Pure and Applied Sciences
dc.author.departmentΤμήμα Χημείας / Department of Chemistry
dc.type.uhtypeArticleen
dc.description.notes<p>Tradenames: ar 177en
dc.description.notesfz 41en
dc.description.notesgs 9137en
dc.description.notesl 870712en
dc.description.notesl 870810en
dc.description.notesl 900612, Mercken
dc.description.notess 1360en
dc.description.notest 30177en
dc.description.notesv 165en
dc.description.notesManufacturers: Mercken
dc.description.notesCited By :25</p>en
dc.source.abbreviationCurr.HIV Res.en


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