Department of Biological Chemistry, University of Michigan, Ann Arbor, MI 48109-0606, USA.
Physical Sciences Division, Pacific Northwest National Laboratory, Post Office Box 999, K1-83, Richland, WA 99352, USA.
Science. 2016 May 20;352(6288):953-8. doi: 10.1126/science.aaf0616.
Methyl-coenzyme M reductase, the rate-limiting enzyme in methanogenesis and anaerobic methane oxidation, is responsible for the biological production of more than 1 billion tons of methane per year. The mechanism of methane synthesis is thought to involve either methyl-nickel(III) or methyl radical/Ni(II)-thiolate intermediates. We employed transient kinetic, spectroscopic, and computational approaches to study the reaction between the active Ni(I) enzyme and substrates. Consistent with the methyl radical-based mechanism, there was no evidence for a methyl-Ni(III) species; furthermore, magnetic circular dichroism spectroscopy identified the Ni(II)-thiolate intermediate. Temperature-dependent transient kinetics also closely matched density functional theory predictions of the methyl radical mechanism. Identifying the key intermediate in methanogenesis provides fundamental insights to develop better catalysts for producing and activating an important fuel and potent greenhouse gas.
甲基辅酶 M 还原酶是产甲烷作用和厌氧甲烷氧化的限速酶,每年负责生物生成超过 10 亿吨甲烷。甲烷合成的机制被认为涉及甲基镍(III)或甲基自由基/Ni(II)-硫醇中间物。我们采用瞬态动力学、光谱和计算方法来研究活性 Ni(I)酶与底物之间的反应。与基于甲基自由基的机制一致,没有证据表明存在甲基镍(III)物种;此外,圆二色性光谱鉴定了 Ni(II)-硫醇中间物。温度依赖的瞬态动力学也与甲基自由基机制的密度泛函理论预测非常吻合。鉴定产甲烷作用中的关键中间物为开发更好的催化剂以生产和激活一种重要燃料和强效温室气体提供了基础见解。
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