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3,5-二乙氧羰基-1,4-二氢可力丁处理的大鼠体内N-烷基原卟啉IX的形成。烷基从底物向卟啉的转移。

N-Alkylprotoporphyrin IX formation in 3,5-dicarbethoxy-1,4-dihydrocollidine-treated rats. Transfer of the alkyl group from the substrate to the porphyrin.

作者信息

Ortiz de Montellano P R, Beilan H S, Kunze K L

出版信息

J Biol Chem. 1981 Jul 10;256(13):6708-13.

PMID:6894597
Abstract

Administration of 3,5-dicarbethoxy-1,4-dihydrocollidine (DDC) to rats causes the accumulation of N-methylprotoporphyrin IX, a potent inhibitor of ferrochelatase. To clarify the origin of the porphyrin N-methyl group, we have synthesized and administered to rats N-ethyl-3,5-dicarbethoxy-1,4-dihydrocollidine (N-ethyl DDC) and 3,5-dicarbethoxy-2,6-dimethyl-4-ethyl-1,4-dihydropyridine (DDEP), the DDC analogue with a 4-ethyl rather than 4-methyl group. Only N-methylprotoporphyrin IX is isolated from rats treated with the former agent, and only N-ethylprotoporphyrin IX from those treated with the latter. All four isomers of N-ethylprotoporphyrin IX are formed biologically. The structure of the isolated porphyrins has been confirmed by complete spectroscopic comparison with the four synthetic isomers of N-ethylprotoporphyrin IX. DDEP has been shown to cause NADPH- and time-dependent in vitro loss of hepatic microsomal cytochrome P-450. These results unequivocally establish that the 4-alkyl groups in DDC and dDEP are the source of the N-alkyl group in N-methyl- and N-ethylprotoporphyrin IX, respectively, and strongly suggest that the alkyl group is transferred to the prosthetic heme of cytochrome P-450 during catalytic processing of the substrate by the enzyme. The mechanism of the group transfer is discussed.

摘要

给大鼠施用3,5 - 二乙氧羰基 - 1,4 - 二氢可力丁(DDC)会导致N - 甲基原卟啉IX的积累,N - 甲基原卟啉IX是一种有效的亚铁螯合酶抑制剂。为了阐明卟啉N - 甲基基团的来源,我们合成了N - 乙基 - 3,5 - 二乙氧羰基 - 1,4 - 二氢可力丁(N - 乙基DDC)并将其施用于大鼠,还合成了3,5 - 二乙氧羰基 - 2,6 - 二甲基 - 4 - 乙基 - 1,4 - 二氢吡啶(DDEP),即具有4 - 乙基而非4 - 甲基基团的DDC类似物。从用前一种试剂处理的大鼠中仅分离出N - 甲基原卟啉IX,而从用后一种试剂处理的大鼠中仅分离出N - 乙基原卟啉IX。N - 乙基原卟啉IX的所有四种异构体都是生物合成形成的。通过与N - 乙基原卟啉IX的四种合成异构体进行完整的光谱比较,已证实了分离出的卟啉的结构。已表明DDEP会导致肝微粒体细胞色素P - 450在体外发生NADPH和时间依赖性损失。这些结果明确证实,DDC和DDEP中的4 - 烷基分别是N - 甲基和N - 乙基原卟啉IX中N - 烷基的来源,并有力地表明在酶对底物进行催化加工过程中,烷基被转移到细胞色素P - 450的辅基血红素上。讨论了基团转移的机制。

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