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来自异戊二烯和异戊二烯单环氧化物的血红蛋白加合物。

Haemoglobin adducts from isoprene and isoprene monoepoxides.

作者信息

Tareke E, Golding B T, Small R D, Törnqvist M

机构信息

Department of Environmental Chemistry, Stockholm University, Sweden.

出版信息

Xenobiotica. 1998 Jul;28(7):663-72. doi: 10.1080/004982598239245.

Abstract
  1. Isoprene is metabolised in vitro by oxygenation of either double bond to 2-ethenyl-2-methyloxirane (epoxide A) and 2-(1'-methylethenyl)oxirane (epoxide B). The reactivity in vitro and formation in vivo of the monoepoxides of isoprene were studied by the formation of adducts to N-terminal valines in haemoglobin (Hb). These adducts were analysed by mass spectrometry after cleavage and derivatization by a modified Edman degradation method. 2. When red blood cells were incubated with commercial isoprene oxide (about 95% epoxide A, < or = 5% epoxide B) adducts from both epoxides were formed. 3. It is confirmed that epoxide A is hydrolysed much faster than epoxide B. The rates are enhanced by phosphate buffer (epoxide A), probably through acid catalysis, and by the presence of red blood cells (both epoxides), due to enzymatic detoxification. 4. Comparison of total valine adduct levels in Hb from isoprene and isoprene oxide injected i.p. led to the conclusion that 23 and 1% of injected isoprene was metabolized to the epoxides in mouse and rat, respectively.
摘要
  1. 异戊二烯在体外通过将任何一个双键氧化为2-乙烯基-2-甲基环氧乙烷(环氧化物A)和2-(1'-甲基乙烯基)环氧乙烷(环氧化物B)进行代谢。通过血红蛋白(Hb)中N端缬氨酸形成加合物的方式,研究了异戊二烯单环氧化物的体外反应性和体内形成情况。这些加合物在通过改良的埃德曼降解法进行裂解和衍生化后,用质谱法进行分析。2. 当红细胞与市售氧化异戊二烯(约95%环氧化物A,≤5%环氧化物B)一起孵育时,两种环氧化物的加合物均会形成。3. 已证实环氧化物A的水解速度比环氧化物B快得多。磷酸盐缓冲液(环氧化物A)可能通过酸催化提高了水解速率,而红细胞的存在(两种环氧化物)则由于酶解毒作用提高了水解速率。4. 对腹腔注射异戊二烯和氧化异戊二烯后Hb中总缬氨酸加合物水平进行比较,得出的结论是,在小鼠和大鼠中分别有23%和1%的注射异戊二烯代谢为环氧化物。

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