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dc.contributor.advisor이동윤-
dc.contributor.author민재홍-
dc.date.accessioned2023-05-11T12:03:27Z-
dc.date.available2023-05-11T12:03:27Z-
dc.date.issued2023. 2-
dc.identifier.urihttp://hanyang.dcollection.net/common/orgView/200000652137en_US
dc.identifier.urihttps://repository.hanyang.ac.kr/handle/20.500.11754/180110-
dc.description.abstractObesity-induced inflammation is a major cause of complications of obesity and is mainly induced by obese white adipose tissue (WAT) caused by hypertrophy of adipocyte due to overnutrition. Treatment of such obesity-induced inflammation is difficult because it requires both targeted delivery to obese WAT and anti-inflammatory treatment at the same time. In this paper, glycyrrhizin (GL), which shows an anti-hypertrophic effect on adipocyte, and adipose tissue homing peptide (AHP), which has a target on adipocytes are conjugated through an amine poly-ethylene-glycol thiol (PEG) linkage to treat obesity-induced inflammation occurred from obese WAT through anti-hypertrophic effect on adipocyte. Glycyrrhizin- amine poly-ethylene-glycol thiol-homing peptide (GL-PEG-AHP) conjugates appear anti-hypertrophic effects on adipocytes and anti-inflammatory effects in obesity WAT mimicking environment. Mechanistically, these effects are presumed to occur through the expression of the ATP Binding Cassette subfamily A 1 transporter (ABCA1) in the adipocyte plasma membrane. Finally, GL-PEG-AHP is expected to be a next-generation anti-obesity and obesity-induced inflammatory drug that can expect not only anti-inflammatory effects on obese adipose tissue but also anti-obesity effects in animal models.-
dc.publisher한양대학교-
dc.titleAnti-obesity-induced inflammation treatment study using adipose tissue homing glycyrrhizin derivative-
dc.typeTheses-
dc.contributor.googleauthor민재홍-
dc.sector.campusS-
dc.sector.daehak대학원-
dc.sector.department생명공학과-
dc.description.degreeMaster-
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GRADUATE SCHOOL[S](대학원) > BIOENGINEERING(생명공학과) > Theses (Master)
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