Strukturna i funkcionalna analiza gena za alfa-1-antitripsin u bolestima pluća čoveka

Structural and functional analysis of alpha-1-antitrypsin gene in human lung diseases

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2012
Author
Ljujić, Mila V.
Mentor
Radojković, Dragica
Committee members
Matić, Gordana
Divac, Aleksandra
Topić, Aleksandra
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Abstract
Alfa-1-antitripsin je inhibitor serin proteaza čija je osnovna biološka funkcija inhibicija elastaze neutrofila – enzima koji učestvuje u degradaciji elastina i koji dovodi do oštećenja tkiva pluća. Deficijencija i disfunkcija alfa-1-antitripsina leže u osnovi više oboljenja od kojih su najčešći emfizem pluća i oboljenja jetre, a mogu predstavljati i faktor rizika za nastanak karcinoma pluća. Ovaj rad je imao za cilj da ispita postojanje strukturnih promena u kodirajućim egzonima gena za alfa-1-antitripsin kod ispitanika sa emfizemom pluća i kod ispitanika sa karcinomom pluća, kao i da istraži funkcionalne posledice otkrivenih promena i njihov eventualni značaj u nastanku i razvoju bolesti. Strukturnom analizom gena za alfa-1-antitripsin DGGE metodom i DNK sekvenciranjem detektovano je prisustvo deficijentnih varijanti Z, S i Mmalton, kao i dve nove varijante označene kao G320R i V321F. Elektroforezom u denaturišućem poliakrilamidnom gelu uočeno je da varijante G320R i V321F migriraju ...

Alpha-1-antitrypsin is a serine protease inhibitor whose main biological function is inhibition of neutrophil elastase – enzyme capable of digestion of elastin and involved in lung tissue destruction. Deficiency and disfunction of alpha-1-antitrypsin is associated with emphysema and liver disease, and can represent a risk factor for development of lung cancer. The objective of this work was to perform structural analysis of alpha-1-antitrypsin gene in subjects with emphysema and lung cancer, as well as to perform functional analysis of discovered variants in order to estimate their role in disease development. Structural analysis of alpha-1-antitrypsin gene, using DGGE and DNA sequencing, revealed presence of deficient variants Z, S and Mmalton, as well as two novel variants – G320R and V321F. Denaturing PAGE analysis showed that variants G320R and V321F exibited increased gel mobility compared to WT variant, and electrophoresis in the presence of 5M urea showed that these variants eff...

Faculty:
Универзитет у Београду, Биолошки факултет
Date:
12-07-2012
Keywords:
Alfa-1-antitripsin / Alpha-1-antitrypsin / emfizem pluća / karcinom pluća / retke varijante / G320R / V321F / inhibitorna aktivnost / polimerizacija / termostabilnost / emphysema / lung cancer / rare variants / G320R / V321F / inhibitory activity / polymerization / thermostability

DOI: 10.2298/bg20120712ljujic

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Handle
https://hdl.handle.net/21.15107/rcub_nardus_2015
URI
http://eteze.bg.ac.rs/application/showtheses?thesesId=34
https://nardus.mpn.gov.rs/handle/123456789/2015
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