Studies on the catalytic function of aromatase: aromatization of 6-alkoxy-substituted androgens

Numazawa, Mitsuteru; Ando, Momoko; Zennyoji, Rika

doi:10.1016/s0960-0760(02)00148-6

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Journal Article

Studies on the catalytic function of aromatase: aromatization of 6-alkoxy-substituted androgens
Citation	Numazawa M, Ando M, Zennyoji R. J. Steroid Biochem. Mol. Biol. 2002; 82(1): 65-73.
Copyright	(Copyright © 2002, Elsevier Publishing)
DOI	10.1016/s0960-0760(02)00148-6
PMID	12429140
Abstract	To gain insight into the catalytic function of aromatase, we studied aromatization of a series of 6alpha- and 6beta-ether-substituted (methoxy, ethoxy, and n-butoxy) androst-4-ene-3,17-dione (AD) steroids (1 and 2) and their androsta-1,4-diene-3,17-dione (ADD) derivatives (3 and 4) with human placental aromatase by gas chromatography-mass spectrometry (GC-MS). Among the steroids examined, 6beta-methoxy and 6beta-ethoxyADDs (4a and 4b) are suicide substrates of aromatase. All of the steroids were found to be converted into the corresponding 6-alkoxy estrogens. Introduction of the alkoxy groups at C-6 of AD or ADD decreased the ability of these to serve as a substrate of aromatase. In 6alpha-alkoxy steroid series, compounds 1 and 3, the aromatization rate increased by elongating the 6-methoxy group up to the n-butoxy group whereas, in the 6beta-isomers series, 2 and 4, the rate decreased due to this structural modification. 6beta-Alkoxy steroids, 2 and 4, including the suicide substrates, were extremely poor substrates for the aromatization reaction. Apparent K(m) values obtained for 6alpha-alkoxy compounds 1 and 3 were similar to each other, ranging from 92 to 111nM, as shown by their previously-obtained K(i) values. The findings indicate that the stereochemistry as well as the bulkiness of the 6-ether-substituent play an important role in the ability to serve as a substrate. It is also predicted that the aromatization reaction and the mechanism-based inactivation reaction would be related and have a definite partition number which is characteristic to the compound in a series of suicide substrates. Language: en
Keywords	Androstenedione; Aromatase; Catalysis; Enzyme Inhibitors; Female; Gas Chromatography-Mass Spectrometry; Humans; Kinetics; Microsomes; Molecular Structure; Placenta; Pregnancy; Structure-Activity Relationship