Kinetic processivity of the two-step oxidations of progesterone and pregnenolone to androgens by human cytochrome P450 17A1

Gonzalez, Eric; Guengerich, F. Peter

doi:10.1074/jbc.m117.794917

Cited by 47 publications

(99 citation statements)

References 65 publications

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“…A value much lower than the D k for the intermolecular reaction can be interpreted in this context. However, the results can also be a reflection of the substrate k off (release and rebinding), so this behavior may not be discernable in the absence of other information such as an isotope dilution experiment using a product or non-reactive substrate trap (Gonzalez & Guengerich, 2017). …”

Section: Types Of Experimentsmentioning

confidence: 99%

Kinetic Deuterium Isotope Effects in Cytochrome P450 Reactions

Guengerich

2017

Methods in Enzymology

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Cytochrome P450 (P450, CYP) research provides many opportunities for the application of kinetic isotope effect (KIE) strategies. P450s collectively catalyze oxidations of more substrates than any other group of enzymes, and C-H bond cleavage is a major feature in a large fraction of these reactions. The presence of a significant primary deuterium KIE is evidence that hydrogen abstraction is at least partially rate-limiting in the reactions, and this appears to be the case in many P450 reactions. The first report of a KIE in (P450-linked) drug metabolism appeared in 1961 (for morphine N-demethylation), and in a number of cases it has been possible to modulate the in vivo metabolism or toxicity of chemicals by deuterium substitution. A number of efforts are in progress to utilize deuterium substitution to alter the metabolism of drugs in an advantageous manner.

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Section: Types Of Experimentsmentioning

confidence: 99%

Kinetic Deuterium Isotope Effects in Cytochrome P450 Reactions

Guengerich

2017

Methods in Enzymology

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“…Cholesterol is subsequently converted into pregnenolone by cholesterol side chain cleavage cytochrome P450/CYP11A1. Pregnenolone is transported to the smooth endoplasmic reticulum where it is converted to testosterone by 3b-hydroxysteroid dehydrogenase D5-D4-isomerase (3b-HSD), CYP17, and 17b-hydroxysteroid dehydrogenase (6,7).…”

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confidence: 99%

Smad ubiquitylation regulatory factor 1 promotes LIM‐homeobox gene 9 degradation and represses testosterone production in Leydig cells

Sun

Chu

et al. 2018

FASEB j.

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Testosterone is essential for spermatogenesis and the maintenance of secondary sexual characteristics in males. An important transcription factor, LIM-homeobox gene 9 (Lhx9) is indispensable for testis development and testosterone production; however, post-translational modifications of Lhx9 are largely unknown. Here, for the first time to our knowledge, we demonstrate that the level of Lhx9 protein increases in human chorionic gonadotropin-exposed Leydig cells and can be polyubiquitylated. We found that Smad ubiquitylation regulatory factor 1 (Smurf1), an E3 ubiquitin ligase, targets Lhx9 for ubiquitin-mediated proteasome degradation, thereby negatively modulating its function. Increasing Smurf1 decreases the level of Lhx9 and inhibits the Lhx9 transactivation capacity of steroidogenic factor 1 [nuclear receptor subfamily 5, group A, member 1 (NR5A1)]. In contrast, the depletion of Smurf1 leads to increased expression of Lhx9 protein and enhances testosterone biosynthesis-related gene transcripts [NR5A1, steroidogenic acute regulatory protein, CYP17A1, hydroxy-δ-5-steroid dehydrogenase, hydroxy-δ-5-steroid dehydrogenase isomerase 6, and hydroxysteroid (17-β) dehydrogenase 3] and testosterone production in Leydig cells. Furthermore, we found that Smurf1 knockout mice exhibit higher levels of Lhx9 protein and steroidogenesis, which leads to increased serum testosterone concentration. These findings reveal that Smurf1 promotes Lhx9 ubiquitylation and is involved in testosterone production in Leydig cells directly. Our results provide new insights into the molecular events that play a role in the homeostasis of testosterone levels and may provide a new target for testosterone regulation.-Hu, F., Zhu, Q., Sun, B., Cui, C., Li, C., Zhang, L. Smad ubiquitylation regulatory factor 1 promotes LIM-homeobox gene 9 degradation and represses testosterone production in Leydig cells.

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“…However, human CYP17A1 preferentially processes 3 further into DHEA . Although the enzyme dissociates from the steroid after hydroxylation, relatively little 3 can escape into other tissues before CYP17A1 acts again . CYP7B1 likely does not encounter 3 in nature, but in our system the enzyme is capable of processing this substrate into novel products 4 and 5 .…”

Section: Figurementioning

confidence: 80%

Mammalian Cells Engineered To Produce New Steroids

et al. 2018

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Steroids can be difficult to modify via traditional organic synthesis methods, but many enzymes regio- and stereo-selectively process a wide variety of steroid substrates. We tested whether steroid-modifying enzymes could make novel steroids from non-native substrates. Numerous genes encoding steroid-modifying enzymes, including some bacterial enzymes, were expressed in mammalian cells by transient transfection and found to be active. We made three unusual steroids by stable expression in HEK293 cells of the 7α-hydroxylase CYP7B1, which was selected because of high native product yield. These cells made 7α,17α-dihydroxypregnenolone and 7β,17α-dihydroxypregnenolone from 17α-hydroxypregnenolone, and produced 11α, 16α-dihydroxyprogesterone from 16α-hydroxyprogesterone. The latter two products resulted from previously unobserved CYP7B1 hydroxylation sites. A Rosetta docking model of CYP7B1 suggested that these substrates’ D-ring hydroxylations may prevent them from binding in the same way as the native substrate, bringing different carbons near the active ferryl oxygen. This new approach could use other enzymes and substrates to produce many novel steroids for drug candidate testing.

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Kinetic processivity of the two-step oxidations of progesterone and pregnenolone to androgens by human cytochrome P450 17A1

Cited by 47 publications

References 65 publications

Kinetic Deuterium Isotope Effects in Cytochrome P450 Reactions

Kinetic Deuterium Isotope Effects in Cytochrome P450 Reactions

Smad ubiquitylation regulatory factor 1 promotes LIM‐homeobox gene 9 degradation and represses testosterone production in Leydig cells

Mammalian Cells Engineered To Produce New Steroids

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