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阴道毛滴虫蛋氨酸 γ-裂合酶对氟化蛋氨酸类似物酶促加工的机制研究。

Mechanistic studies on the enzymatic processing of fluorinated methionine analogues by Trichomonas vaginalis methionine γ-lyase.

机构信息

Department of Chemistry, University of Waterloo, 200 University Avenue West, Waterloo, Ontario N2L 3G1, Canada.

出版信息

Biochem J. 2011 Sep 15;438(3):513-21. doi: 10.1042/BJ20101986.

Abstract

TFM (L-trifluoromethionine), a potential prodrug, was reported to be toxic towards human pathogens that express MGL (L-methionine γ-lyase; EC 4.4.1.11), a pyridoxal phosphate-containing enzyme that converts L-methionine into α-oxobutyrate, ammonia and methyl mercaptan. It has been hypothesized that the extremely reactive thiocarbonyl difluoride is produced when the enzyme acts upon TFM, resulting in cellular toxicity. The potential application of the fluorinated thiomethyl group in other areas of biochemistry and medicinal chemistry requires additional studies. Therefore a detailed investigation of the theoretical and experimental chemistry and biochemistry of these fluorinated groups (CF₃S⁻ and CF₂HS⁻) has been undertaken to trap and identify chemical intermediates produced by enzyme processing of molecules containing these fluorinated moieties. TvMGL (MGL from Trichomonas vaginalis) and a chemical model system of the reaction were utilized in order to investigate the cofactor-dependent activation of TFM and previously uninvestigated DFM (L-difluoromethionine). The differences in toxicity between TFM and DFM were evaluated against Escherichia coli expressing TvMGL1, as well as the intact human pathogen T. vaginalis. The relationship between the chemical structure of the reactive intermediates produced from the enzymatic processing of these analogues and their cellular toxicity are discussed.

摘要

TFM(L-三氟甲硫氨酸),一种潜在的前药,据报道对表达 MGL(L-蛋氨酸 γ-裂解酶;EC 4.4.1.11)的人体病原体有毒,该酶含有吡哆醛磷酸盐,可将 L-蛋氨酸转化为α-氧代丁酸、氨和甲硫醇。据推测,当该酶作用于 TFM 时,会产生极活泼的硫羰基二氟化物,导致细胞毒性。氟代硫甲基基团在生物化学和药物化学的其他领域的潜在应用需要进一步的研究。因此,对这些氟代基团(CF₃S⁻和 CF₂HS⁻)的理论和实验化学和生物化学进行了详细的研究,以捕获和鉴定含这些氟代部分的分子经酶处理产生的化学中间产物。TvMGL(阴道毛滴虫的 MGL)和反应的化学模型系统被用于研究 TFM 和以前未研究过的 DFM(L-二氟甲硫氨酸)的辅因子依赖性激活。评估了 TFM 和 DFM 对表达 TvMGL1 的大肠杆菌以及完整的人体病原体阴道毛滴虫的毒性差异。讨论了这些类似物酶促处理产生的反应性中间产物的化学结构与其细胞毒性之间的关系。

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