Table 9.
P450 17A1
| Properties | References |
|---|---|
| Physiological substrates; Progesterone, 17α-hydroxyprogesterone,17α-hydroxypregnenolone, 16α-hydroxyprogesterone | (Pikuleva et al. 2008; Petrunak et al. 2014; Pan et al. 2016; Gonzalez and Guengerich 2017; Yadav et al. 2017; Gonzalez et al. 2018) |
|
Function: Biosynthesis of androgens and estrogens (cortisol), 16α-hydroxylase, 17α-hydroxylase, 17,20-lyase (Figs. 4, 11); controls the levels of mineralocorticoids influencing blood pressure, glucocorticoids involved in immune and stress responses, as well as androgens and estrogens involved in development and homeostasis of reproductive tissues |
|
|
Inhibition: Lower androgen level and production in prostate cancer, treating diseases caused by cortisol overproduction; increases the pool of precursors for mineralocorticoid production and blocks P450 17A1-mediated production of glucocorticoids (Leroux 2005; Bird and Abbott 2016; Bonomo et al. 2016) | |
|
Inhibitors: (Ahmed 1999; Clement et al. 2003) | |
|
Drugs: | |
|
Abiraterone and analogsa (Pinto-Bazurco Mendieta et al. 2008; Ferraldeschi and de Bono 2013; Auchus R. J. et al. 2014; Petrunak et al. 2014; Yin and Hu 2014; Schroeder et al. 2016; Malikova et al. 2017) | |
| Abiraterone, galeterone, seviteronel, orteronela (Yamaoka et al. 2012; Stein et al. 2014; Bird and Abbott 2016; Petrunak et al. 2017) | |
| Azole drugsa (e.g., ketoconazole, liarozole—weak inhibitors) (Ayub and Levell 1989; Ideyama et al. 1998; Ahmed 1999; Clement et al. 2003; Bird and Abbott 2016) Ketoconazole (at high concentrations) (De Coster et al. 1986; Ayub and Levell 1989; Engelhardt and Weber 1994; Johansson et al. 2002) | |
| Rifampicinb (Kim et al. 2013) | |
| Valproic acidc (at high concentrations) (Glister et al. 2012) | |
|
Natural compounds: | |
|
1α,25-Dihydroxyvitamin D3 d (Lundqvist et al. 2010) | |
| Daidzein, hesperitin, resveratrol d (Lin et al. 2014) | |
| Polyphenols d (e.g., apigenin, aringenin, eriodictyol, genistein) d (Hasegawa et al. 2013) | |
|
Physiological compounds: | |
|
Bone morphogenetic protein 4 c (Rege et al. 2015) | |
| Epidermal growth factorc (Doi et al. 2001) | |
| Interferon-βc (van Koetsveld et al. 2013) | |
|
Other compounds, including drug candidates: | |
|
16- and 17-Azolyl steroids a (Njar et al. 1998) | |
| 5-(Phenoxymethyl)-1,3-dioxane analogs d (Schroeder et al. 2016) | |
| 6-Hydroxy-2,2´,4,4´-tetrabromodiphenyl ether d, bromodiphenyl ether-183 d (Canton et al. 2006; Song et al. 2008) | |
| Biphenylmethylene 4-pyridines d (Hu et al. 2010) | |
| Bisphenol A d (Niwa et al. 2001) | |
| Imidazole, pyridine, 1,2,4- and 1,2,3-triazole, pyrazine, pyrimidine, pyrazole, oxazole, thiazole, isoxazole, 1,2,3,4- and 1,2,3,5-tetrazole and isothiazole containing compounds d (Bonomo et al. 2016) | |
| Methoxy- and hydroxy-substituted methyleneimidazolyl biphenylsa (Hille et al. 2009) | |
| α-Naphthoflavonec (Lin et al. 2014) | |
| Nitrophenols d (Furuta et al. 2008) | |
| Prochloraz d (Ohlsson et al. 2009) | |
| Steroidal C-17 benzoazoles d (Handratta et al. 2005) | |
| Vioxx (rofecoxib)-related lactones d (van Duursen et al. 2010) | |
| YM116 d (Ideyama et al. 1998) | |
|
Induction: stimulation of androgen biosynthesis in man and risk of development of prostate cancer, or enhanced estrogen biosynthesis and risk of breast cancer | |
|
Inducers: | |
|
Drugs: | |
|
Cycloheximidee (Doi et al. 2001) | |
| Valproic acidf (Nelson-DeGrave et al. 2004) | |
|
Natural compounds: | |
|
Retinoids e (Wickenheisser et al. 2005) | |
| Forskolin e (Sawetawan et al. 1996; Nelson-DeGrave et al. 2004; Asif et al. 2006; Lin et al. 2014) | |
|
Physiological compounds: | |
|
Adrenocorticotropic hormone (ACTH) e (Di Blasio et al. 1987) | |
| Cardiolipin g (Kisselev et al. 1999) | |
| Cortisol e (Hsu et al. 2001; Auchus R. J. et al. 2014) | |
| Insulin-like growth factors I and II e (Mesiano et al. 1997) | |
|
Other compounds: | |
|
PD98059 (MAPK kinase (MEK) inhibitor) e (Doi et al. 2001) | |
| Polybrominated diphenyl ethers f (e.g. 2´-hydroxybromodiphenyl ether-68) (Song et al. 2008) | |
Footnotes:
a
Competitive inhibition, ligand binding
b
Competitive inhibition, binding to enzyme active site
c
Reduced/suppressed mRNA and/or protein level/expression and activity
d
Decreased/suppressed/inhibited activity/product formation
e
Increased transcription/mRNA/protein expression/levels /and/or catalytic activity
f
Up-regulation of biosynthesis, increased expression of protein
g
Increased activity, and/or increased product formation