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黄酮类化合物对酪氨酸酶酶促氧化诱导褐变的促进作用:构效关系

Promotion effects of flavonoids on browning induced by enzymatic oxidation of tyrosinase: structure-activity relationship.

作者信息

Lu Yao, Xu Yi, Song Meng-Ting, Qian Ling-Ling, Liu Xiao-Lin, Gao Rong-Yao, Han Rui-Min, Skibsted Leif H, Zhang Jian-Ping

机构信息

Department of Chemistry, Renmin University of China Beijing 100872 China

Department of Food Science, University of Copenhagen Rolighedsvej 30 DK-1958 Frederiksberg C Denmark

出版信息

RSC Adv. 2021 Apr 13;11(23):13769-13779. doi: 10.1039/d1ra01369f.

Abstract

Tyrosinase, widely distributed in nature, is a copper-containing polyphenol oxidase involved in the formation of melanin. Flavonoids are most often considered as tyrosinase inhibitors but have also been confirmed to be tyrosinase substrates. Four structure-related flavonoids including flavones (apigenin and luteolin) and flavonols (kaempferol and quercetin) are found to promote not inhibit browning induced by tyrosinase catalyzed oxidation both in model systems and in mushrooms under aerobic conditions. A comparison with enzymatic oxidation and autooxidation of flavonoids alone has helped to clarify why flavonoids function as a substrate rather than an inhibitor. Flavonoids almost do not affect the kinetics of melanin formation from enzymatic oxidation of l-dopa in excess. In addition, a new brown complex formed during the reaction of flavonoid quinone and dopaquinone is suggested to enhance the browning effects by competing with isomerization and autooxidation. Structure-activity relationships of the four flavonoids in melanin formation leading to browning induced by autooxidation and enzymatic oxidation confirm the enzymatic nature of the browning.

摘要

酪氨酸酶广泛存在于自然界,是一种参与黑色素形成的含铜多酚氧化酶。黄酮类化合物通常被认为是酪氨酸酶抑制剂,但也已被证实是酪氨酸酶的底物。研究发现,包括黄酮(芹菜素和木犀草素)和黄酮醇(山奈酚和槲皮素)在内的四种结构相关的黄酮类化合物,在有氧条件下,无论是在模型体系还是蘑菇中,都能促进而非抑制酪氨酸酶催化氧化诱导的褐变。将黄酮类化合物单独的酶促氧化和自氧化进行比较,有助于阐明黄酮类化合物为何作为底物而非抑制剂发挥作用。黄酮类化合物几乎不影响过量左旋多巴酶促氧化形成黑色素的动力学。此外,有人提出,在黄酮醌与多巴醌反应过程中形成的一种新的棕色复合物,通过与异构化和自氧化竞争来增强褐变效应。这四种黄酮类化合物在自氧化和酶促氧化诱导褐变的黑色素形成过程中的构效关系,证实了褐变的酶促性质。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/fbdb/8697750/28802398fee0/d1ra01369f-s1.jpg

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