RISS 학술연구정보서비스

검색
자동완성 버튼
다국어입력
다국어 입력

http://chineseinput.net/에서 pinyin(병음)방식으로 중국어를 변환할 수 있습니다.

변환된 중국어를 복사하여 사용하시면 됩니다.

예시)
  • 中文 을 입력하시려면 zhongwen을 입력하시고 space를누르시면됩니다.
  • 北京 을 입력하시려면 beijing을 입력하시고 space를 누르시면 됩니다.
Α Β Γ Δ Ε Ζ Η Θ Ι Κ Λ Μ Ν Ξ Ο Π Ρ Σ Τ Υ Φ Χ Ψ Ω α β γ δ ε ζ η θ ι κ λ μ ν ξ ο π ρ σ τ υ φ χ ψ ω
á à Á À é è É È ç Ç ê
Ä Ö Ü ä ö ü ß
ְ ֳ ֲ ֱ ָ ַ ֵ ֶ ִ ֹ ּ ֻ ׂ ׁ ּ פ ם ן ו ט א ר ק ף ך ל ח י ע כ ג ד ש ץ ת צ מ נ ה ב
± × ÷
· ¨ ´ ˇ ˘ ˝ ˚ ˙ ¸ ˛ ¡ ¿ ː _
½ ¼ ¾ ¹ ² ³
Æ Ð Ħ IJ Ł Ø Œ Þ Ŧ Ŋ æ đ ð ħ ı ij ĸ ŀ ł ø œ ß þ ŧ ŋ ʼn
А Б В Г Д Е Ё Ж З И Й К Л М Н О П Р С Т У Ф Х Ц Ч Ш Щ Ъ Ы Ь Э Ю Я а б в г д е ё ж з и й к л м н о п р с т у ф х ц ч ш щ ъ ы ь э ю я
¤
§ ª º
ا ب ت ث ج ح خ د ذ ر ز س ش ص ض ط ظ ع غ ف ق ک ل م ن ه و ی
닫기
    인기검색어 순위 펼치기

    RISS 인기검색어

      검색결과 좁혀 보기

      선택해제

      오늘 본 자료

      • 오늘 본 자료가 없습니다.
      더보기
      검색키워드
      저자 : ve-Quelquejeu, Mé (검색결과 1 건)
      • 무료
      • 기관 내 무료
      • 유료

      • Inactivation of Mycobacterium tuberculosis l,d-Transpeptidase Ldt<sub>Mt1</sub>by Carbapenems and Cephalosporins

        Dubé,e, Vincent,Triboulet, Sé,bastien,Mainardi, Jean-Luc,Ethè,ve-Quelquejeu, Mé,lanie,Gutmann, Laurent,Marie, Arul,Dubost, Lionel,Hugonnet, Jean-Emmanuel,Arthur, Michel American Society for Microbiology 2012 Antimicrobial agents and chemotherapy Vol.56 No.8

        <B>ABSTRACT</B><P>The structure ofMycobacterium tuberculosispeptidoglycan is atypical since it contains a majority of 3→3 cross-links synthesized byl,d-transpeptidases that replace 4→3 cross-links formed by thed,d-transpeptidase activity of classical penicillin-binding proteins. Carbapenems inactivate thesel,d-transpeptidases, and meropenem combined with clavulanic acid is bactericidal against extensively drug-resistantM. tuberculosis. Here, we used mass spectrometry and stopped-flow fluorimetry to investigate the kinetics and mechanisms of inactivation of the prototypicM. tuberculosisl,d-transpeptidase LdtMt1by carbapenems (meropenem, doripenem, imipenem, and ertapenem) and cephalosporins (cefotaxime, cephalothin, and ceftriaxone). Inactivation proceeded through noncovalent drug binding and acylation of the catalytic Cys of LdtMt1, which was eventually followed by hydrolysis of the resulting acylenzyme. Meropenem rapidly inhibited LdtMt1, with a binding rate constant of 0.08 μM<SUP>−1</SUP>min<SUP>−1</SUP>. The enzyme was unable to recover from this initial binding step since the dissociation rate constant of the noncovalent complex was low (<0.1 min<SUP>−1</SUP>) in comparison to the acylation rate constant (3.1 min<SUP>−1</SUP>). The covalent adduct resulting from enzyme acylation was stable, with a hydrolysis rate constant of 1.0 × 10<SUP>−3</SUP>min<SUP>−1</SUP>. Variations in the carbapenem side chains affected both the binding and acylation steps, ertapenem being the most efficient LdtMt1inactivator. Cephalosporins also formed covalent adducts with LdtMt1, although the acylation reaction was 7- to 1,000-fold slower and led to elimination of one of the drug side chains. Comparison of kinetic constants for drug binding, acylation, and acylenzyme hydrolysis indicates that carbapenems and cephems can both be tailored to optimize peptidoglycan synthesis inhibition inM. tuberculosis.</P>

      맨처음 페이지로1맨끝 페이지로

      연관 검색어 추천

      이 검색어로 많이 본 자료

      활용도 높은 자료

      해외이동버튼