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生物生成的二氧化碳:羧化酶的自然多功能化学策略。

Biologically generated carbon dioxide: nature's versatile chemical strategies for carboxy lyases.

机构信息

ChEM-H Institute, Stanford University, Stanford, CA 94305, USA.

出版信息

Nat Prod Rep. 2020 Jan 1;37(1):100-135. doi: 10.1039/c9np00015a. Epub 2019 May 10.

DOI:10.1039/c9np00015a
PMID:31074473
Abstract

Covering: up to 2019Metabolic production of CO is natural product chemistry on a mammoth scale. Just counting humans, among all other respiring organisms, the seven billion people on the planet exhale about 3 billion tons of CO per year. Essentially all of the biogenic CO arises by action of discrete families of decarboxylases. The mechanistic routes to CO release from carboxylic acid metabolites vary with the electronic demands and structures of specific substrates and illustrate the breadth of chemistry employed for C-COO (C-C bond) disconnections. Most commonly decarboxylated are α-keto acid and β-keto acid substrates, the former requiring thiamin-PP as cofactor, the latter typically cofactor-free. The extensive decarboxylation of amino acids, e.g. to neurotransmitter amines, is synonymous with the coenzyme form of vitamin B, pyridoxal-phosphate, although covalent N-terminal pyruvamide residues serve in some amino acid decarboxylases. All told, five B vitamins (B, B, B, B, B), ATP, S-adenosylmethionine, manganese and zinc ions are pressed into service for specific decarboxylase catalyses. There are additional cofactor-independent decarboxylases that operate by distinct chemical routes. Finally, while most decarboxylases use heterolytic ionic mechanisms, a small number of decarboxylases carry out radical pathways.

摘要

涵盖

截至 2019 年,CO 的代谢生成是大规模的天然产物化学。仅以人类为例,在所有其他呼吸生物中,地球上 70 亿人每年呼出约 30 亿吨 CO。基本上所有生物源 CO 都是由离散的脱羧酶家族作用产生的。从羧酸代谢物中释放 CO 的机制途径因特定底物的电子需求和结构而异,展示了用于 C-COO(C-C 键)断裂的广泛化学。最常见的脱羧化底物是α-酮酸和β-酮酸,前者需要硫胺素-PP 作为辅酶,后者通常不需要辅酶。氨基酸的广泛脱羧作用,例如转化为神经递质胺,与辅酶形式的维生素 B、吡哆醛-磷酸同义,尽管在一些氨基酸脱羧酶中,共价 N-端丙酮酸酰胺残基起作用。总的来说,有五种 B 族维生素(B、B、B、B、B)、ATP、S-腺苷甲硫氨酸、锰和锌离子被用于特定的脱羧酶催化。还有一些不依赖辅酶的脱羧酶,它们通过不同的化学途径起作用。最后,虽然大多数脱羧酶使用异裂离子机制,但少数脱羧酶采用自由基途径。

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