Potent inhibition of cholesterol biosynthesis in 3T3 fibroblasts by N-[(1,5,9)-trimethyldecyl]-4α, 10-dimethyl-8-AZA-trans-decal-3β-OL, a new 2,3-oxidosqualene cyclase inhibitor

“…From our cellular data it does not seem that fenpropimorph is a good inhibitor of the mammalian cyclase. In contrast with results obtained recently with specific cyclase inhibitors in the same cellular system (Gerst et al, 1986(Gerst et al, , 1988), the levels of 2,3-oxidosqualene and 2,3:22,23-dioxidosqualene in the fenpropimorphtreated cells represent only minor amounts of the total non-saponifiable fraction. Moreover, when tested in vitro on a pig liver microsomal 2,3-oxidosqualene:lanosterol cyclase, this fungicide was found to be a poor inhibitor, i.e.…”

“…were performed according to published procedures (Gerst et al, 1986;Costet et al, 1987). Analysis of the C27-sterol fractions by thin-layer argentation chromatography has been described elsewhere (Gerst et al, 1988). Separation of the polar sterols was performed by t.l.c.…”

“…The HMG-CoA reductase activity of cell extracts was measured as described previously (Gerst et al, 1988); the effect of fenpropimorph on the 2,3-oxidosqualene: lanosterol cyclase activity, associated to pig liver microsomes (microsomal fractions), was determined as described previously (Duriatti et al, 1985).…”

Inhibition by the fungicide fenpropimorph of cholesterol biosynthesis in 3T3 fibroblasts

“…From our cellular data it does not seem that fenpropimorph is a good inhibitor of the mammalian cyclase. In contrast with results obtained recently with specific cyclase inhibitors in the same cellular system (Gerst et al, 1986(Gerst et al, , 1988), the levels of 2,3-oxidosqualene and 2,3:22,23-dioxidosqualene in the fenpropimorphtreated cells represent only minor amounts of the total non-saponifiable fraction. Moreover, when tested in vitro on a pig liver microsomal 2,3-oxidosqualene:lanosterol cyclase, this fungicide was found to be a poor inhibitor, i.e.…”

“…were performed according to published procedures (Gerst et al, 1986;Costet et al, 1987). Analysis of the C27-sterol fractions by thin-layer argentation chromatography has been described elsewhere (Gerst et al, 1988). Separation of the polar sterols was performed by t.l.c.…”

“…The HMG-CoA reductase activity of cell extracts was measured as described previously (Gerst et al, 1988); the effect of fenpropimorph on the 2,3-oxidosqualene: lanosterol cyclase activity, associated to pig liver microsomes (microsomal fractions), was determined as described previously (Duriatti et al, 1985).…”

Inhibition by the fungicide fenpropimorph of cholesterol biosynthesis in 3T3 fibroblasts

“…MDL28,815, a rationally designed inhibitor of sterol biosynthesis, resembles cholesterol and mimics the high energy reaction intermediates of several of the late steps of sterol modification (Gerst et al , 1988). Despite a chemical structure different from that of morpholines its affinity for the (+)‐[ 3 H]‐pentazocine labelled sigma 1 ‐site of guinea‐pig brain microsomes was close ( K i 0.16 ± 0.04 n m ( n = 3)) to that of tridemorph (Table 1).…”

“…The ultrahigh affinity of fenpropimorph for the brain α 1 ‐site ( K i 5 p m ) suggests that this morpholine might be a valuable tool for studies on sigma 1 ‐mediated effects. The haloperidol congener trifluperidol ( K i 1.3 n m ) inhibits the sterol C 8 –C 7 isomerase of yeast (Sobus et al , 1977) whereas the azadecalin MDL28,815 ( K i 0.16 n m ) inhibits the mammalian sterol C 8 –C 7 isomerase in 3T3 mouse fibroblasts (Gerst et al , 1988) as well as in the human hepatoma cell line HepG2 (van Sickle et al , 1993). The anti‐hypercholesteraemic drug AY‐9944 ( K i 0.46 n m ) reduces sterol C 8 –C 7 isomerization in yeast (Pereira et al , 1983) and rat adrenal gland (Givner et al , 1967).…”

High affinity of sigma₁‐binding sites for sterol isomerization inhibitors: evidence for a pharmacological relationship with the yeast sterol C₈–C₇ isomerase

Rationally Designed Inhibitors of Sterol Biosynthesis