首页> 外文期刊>Journal of Medicinal Chemistry >Inactivation of Purified Human Recombinant Monoamine Oxidases A and B by Rasagiline and Its Analogues
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Inactivation of Purified Human Recombinant Monoamine Oxidases A and B by Rasagiline and Its Analogues

机译:雷沙吉兰及其类似物对纯化的人重组单胺氧化酶A和B的灭活作用

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The inactivation of purified human recombinant monoamine oxidases (MAO) A and B by rasagiline [N-propargyl-1(R)-aminoindan] and four of its analogues [N-propargyl-1(S)-aminoindan (S-PAI), 6-hydroxy-N-propargyl-1(R)-aminoindan (R-HPAI), N-methyl-N-propargyl-1(R)-aminoindan (R-MPAI), and 6-(N-methyl-N-ethyl carbamoyloxy)-N-propargyl-1(R)-aminoindan (R-CPAI)] has been investigated. All compounds tested, with the exception of R-CPAI, form stoichiometric N(5) flavocyanine adducts with the FAD moiety of either enzyme. No H_2O_2 is produced during either MAO A or MAO B inactivation, which demonstrates that covalent addition occurs in a single turnover. Rasagiline has the highest specificity for MAO B, as demonstrated by a 100-fold higher inhibition potency (k_(inact)/K_i) compared to MAO A, with the remaining compounds exhibiting lower isozyme specificities. MAO B and MAO A are more selective for the R-enantiomer (rasagiline) compared to the S-enantiomer (S-PAI) by 2500-fold and 17-fold, respectively. Differences in UV/vis and CD spectral data of the complexes of the studied compounds with both MAO A and MAO B are interpreted in light of crystallographic data of complexes of MAO B with rasagiline and its analogues (Binda, C.; et al. J. Med. Chem. 2004, 47, 1767-1774.
机译:雷沙吉兰[N-炔丙基-1(R)-氨基茚满]及其四个类似物[N-炔丙基-1(S)-氨基茚满(S-PAI),对纯化的人重组单胺氧化酶(MAO)A和B的灭活, 6-羟基-N-炔丙基-1(R)-氨基茚满(R-HPAI),N-甲基-N-炔丙基-1(R)-氨基茚满(R-MPAI)和6-(N-甲基-N-已研究了乙基氨基甲酰氧基)-N-炔丙基-1(R)-氨基茚满(R-CPAI)]。除R-CPAI外,所有测试的化合物均与任一酶的FAD部分形成化学计量的N(5)黄酮花青加合物。在MAO A或MAO B灭活过程中均不产生H_2O_2,这表明共价添加发生在单个周转中。雷沙吉兰对MAO B具有最高的特异性,这是与MAO A相比具有100倍的高抑制力(k_(inact)/ K_i)所证实的,其余化合物表现出较低的同工酶特异性。与S-对映体(S-PAI)相比,MAO B和MAO A对R-对映体(雷沙吉兰)的选择性分别高2500倍和17倍。根据MAO B与雷沙吉兰及其类似物的复合物的晶体学数据解释了所研究化合物与MAO A和MAO B的复合物在UV / vis和CD光谱数据上的差异(Binda,C .; et al。 。Med。Chem。2004,47,1767-1774。

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