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The Rationale for Targeting the NAD/NADH Cofactor Binding Site of Parasitic S-Adenosyl-L-homocysteine Hydrolase for the Design of Anti-parasitic Drugs

机译：理瞄准寄生s-腺苷-L-高半胱氨酸水解酶的NaD / NaDH辅助因子结合位点抗寄生虫药物的设计

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Trypanosomal S-adenoyl-L-homocysteine hydrolase (Tc-SAHH), considered as a target for treatment of Chagas disease, has the same catalytic mechanism as human SAHH (Hs-SAHH) and both enzymes have very similar X-ray structures. Efforts toward the design of selective inhibitors against Tc-SAHH targeting the substrate binding site have not to date shown any significant promise. Systematic kinetic and thermodynamic studies on association and dissociation of cofactor NAD/H for Tc-SAHH and Hs-SAHH provide a rationale for the design of anti-parasitic drugs directed toward cofactor-binding sites. Analogues of NAD and their reduced forms show significant selective inactivation of Tc-SAHH, confirming that this design approach is rational.

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Sumin Cai; Qing-Shan Li; Jianwen Fang; Ronald T. Borchardt; Krzysztof Kuczera; C. Russell Middaugh; Richard L. Schowen;
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年(卷),期 -1(28),5
年度 -1
页码 485–503
总页数 20
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专利

1. THE RATIONALE FOR TARGETING THE NAD/NADH COFACTOR BINDING SITE OF PARASITIC S-ADENOSYL-L-HOMOCYSTEINE HYDROLASE FOR THE DESIGN OF ANTI-PARASITIC DRUGS [J] . Sumin Cai, Qing Shan Li, Jianwen Fang Nucleosides, nucleotides and nucleic acids . 2009,第5a7期

机译：靶向抗寄生虫药物S-腺苷基-L-半胱氨酸水解酶NAD / NADH结合位点的合理性
2. Adenosine binding sites at S-adenosylhomocysteine hydrolase are controlled by the NAD(+)/NADH ratio of the enzyme. [J] . Kloor D, Ludtke A, Stoeva S, Biochemical Pharmacology . 2003,第11期

机译：S-腺苷同型半胱氨酸水解酶上的腺苷结合位点由该酶的NAD（+）/ NADH比值控制。
3. Verification of a novel NADH-binding motif: Combinatorial mutagenesis of three amino acids in the cofactor-binding pocket of Corynebacterium 2,5-diketo-D-gluconic acid reductase [J] . Banta S, Anderson S Journal of Molecular Evolution . 2002,第6期

机译：一个新的NADH结合基序的验证：棒状杆菌2，5-二酮-D-葡萄糖酸还原酶的辅因子结合口袋中的三个氨基酸的组合诱变
4. Two-photon excited-state and conformation dynamics of NADH binding with dehydrogenases [C] . Yuexin Liv, Florly S. Ariola, Hye-Ryong Kim, International Conference on Femtochemistry . 2006

机译：与脱氢酶结合NADH结合的双光子激发状态和构象动态
5. Kinetic mechanism and quaternary structure of Aminobacter aminovorans NADH:Flavin oxidoreductase: An unusual flavin reductase with bound flavin. Aminobacter aminovorans NADH:Flavin oxidoreductase His140: A highly conserved residue critical for NADH binding and utilization. [D] . Russell, Thomas Randolph. 2004

机译：氨基噬菌体NADH：黄素氧化还原酶的动力学机理和季结构：一种与黄素结合的异常黄素还原酶。氨基杆菌氨基乙酸NADH：黄素氧化还原酶His140：高度保守的残基，对NADH的结合和利用至关重要。
6. Design of anti-parasitic and anti-fungal hydroxy-naphthoquinones that are less susceptible to drug resistance [O] . Louise M. Hughes, Charlotte A. Lanteri, Michael T. O’Neil, -1

机译：抗寄生和抗真菌羟基 - 萘醌的设计不易抗药性
7. Site-directed mutagenesis of the NADH binding site of prokaryotic Complex I (NADH:ubiquinone oxidoreductase) affects generation of reactive oxygen species [O] . Aierstock K.M., Morina K., Fiegen D., 2012

机译：原核复合体I（NADH：泛醌氧化还原酶）NADH结合位点的定点诱变影响活性氧的产生
8. S-Adenosyl-L-homocysteine hydrolase as a potential target for diagnosis with radiohalogenated nucleosides. [R] . P. C. Srivastava A. Hasan 1991

机译：s-腺苷-L-高半胱氨酸水解酶作为放射性卤化核苷诊断的潜在靶标。

The Rationale for Targeting the NAD/NADH Cofactor Binding Site of Parasitic S-Adenosyl-L-homocysteine Hydrolase for the Design of Anti-parasitic Drugs

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