Enhancement of streptokinase activity by directed evolution인위적 분자 진화에 의한 스트렙토키나제 활성 증진

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dc.contributor.advisorByun, Si-Myung-
dc.contributor.advisor변시명-
dc.contributor.authorSo, Young-Sun-
dc.contributor.author소영선-
dc.date.accessioned2011-12-12T08:53:13Z-
dc.date.available2011-12-12T08:53:13Z-
dc.date.issued2002-
dc.identifier.urihttp://library.kaist.ac.kr/search/detail/view.do?bibCtrlNo=177026&flag=dissertation-
dc.identifier.urihttp://hdl.handle.net/10203/27978-
dc.description학위논문(석사) - 한국과학기술원 : 생물과학과, 2002.8, [ iv, 47 p. ]-
dc.description.abstractA bacterial plasminogen activator, streptokinase is widely used as a thrombolytic agent in the treatment of myocardial infarction. In this study, streptokinase was modified by directed evolution. Through six rounds of random mutagenesis and three rounds of error-prone PCR, over 50 thousands of clones were screened by skim milk-plasminogen overlay test and plasminogen activation assay in 96-well plates. As a result, seven mutants with amino acid substitution were selected. Among them, S221F was purified and its amidolytic activity and plasminogen activation activity were analyzed at pH 7.4 and 37℃ with a chromogenic substrate, $NH_{2-D}-Val-Leu-Lys-p-nitroanilide. The S221F showed the 7.7-fold increased specific activity than wild-type SK owing to the decreased Michaelis constant for the substrate plasminogen. The evolved F221 may contribute to a hydrophobic core of SK β domain for substrate plasminogen binding.eng
dc.languageeng-
dc.publisher한국과학기술원-
dc.subjectplasminogen-
dc.subjectstreptokinase-
dc.subjectplasminogen activation-
dc.subject방향성 있는 인위적 분자 진화-
dc.subject플라스미노젠-
dc.subject스트렙토키나제-
dc.subjectdirected evolution-
dc.titleEnhancement of streptokinase activity by directed evolution-
dc.title.alternative인위적 분자 진화에 의한 스트렙토키나제 활성 증진-
dc.typeThesis(Master)-
dc.identifier.CNRN177026/325007-
dc.description.department한국과학기술원 : 생물과학과, -
dc.identifier.uid020003247-
dc.contributor.localauthorByun, Si-Myung-
dc.contributor.localauthor변시명-
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