Yeast Sterol C<sub>8</sub>−C<sub>7</sub> Isomerase:  Identification and Characterization of a High-Affinity Binding Site for Enzyme Inhibitors

Moebius, Fabian F.; Bermoser, Katrin; Reiter, Raphael; Hanner, Markus; Glossmann, Hartmut

doi:10.1021/bi961996m

Cited by 65 publications

(50 citation statements)

References 34 publications

(48 reference statements)

Supporting

Mentioning

Contrasting

Order By: Relevance

“…However, the IC 50 value deduced from the in vitro assay is much higher. This result is not surprising in the light of the previous results obtained by others [21] and by ourselves [6] with the yeast sterol isomerase. Indeed, a similar discrepancy has already been observed with various inhibitors of the yeast sterol isomerase, including SR31747A.…”

Section: Discussionsupporting

confidence: 82%

“…Inhibition of cholesterol biosynthesis, whether at the early HMG CoA reductase step (by lovastatin or compactin [24]), or at final steps [by 24(R,S),25-iminolanosterol [25], BM 17.766 [26]], has been shown to induce growth inhibition of tumour cells. Although we did not show that SR31747A inhibits liver sterol isomerase in vivo, such an inhibition can be expected as liver sterol isomerase is pharmacologically indistinguishable from the yeast and mammalian enzymes [21]. Furthermore, it is worth noting that tamoxifen is another M1 sterol isomerase inhibitor, which competitively inhibits SR31747A binding to this enzyme [27].…”

Section: Discussionmentioning

confidence: 87%

See 1 more Smart Citation

Antiproliferative effects of SR31747A in animal cell lines are mediated by inhibition of cholesterol biosynthesis at the sterol isomerase step

Bouteiller

Jamme

David

et al. 1998

European Journal of Biochemistry

View full text Add to dashboard Cite

SR31747A is a new sigma ligand exhibiting immunosuppressive properties and antiproliferative activity on lymphocyte cells. Only two subtypes of sigma receptor, namely the sigma 1 receptor and emopamilbinding protein, have been characterised molecularly. Only the σ 1 receptor has been shown to bind (Z)Ncyclohexyl-N-ethyl-3-(3-chloro4-cyclohexylphenyl)propen-2-ylamine hydrochloride (SR31747A) with high affinity. It was demonstrated that the SR31747A effect on the inhibition of T-cell proliferation was consistent with a sigma 1 receptor-mediated event. In this report, binding experiments and sterol isomerase assays, using recombinant yeast strains, indicate that the recently cloned emopamil-binding protein is a new SR31747A-binding protein whose activity is inhibited by SR31747A. Sterol analyses reveal the accumulation of a ∆8-cholesterol isomer at the expense of cholesterol in SR31747A-treated cells, suggesting that cholesterol biosynthesis is inhibited by SR31747A at the ∆8-∆7 sterol isomerase step in animal cells. This observation is consistent with a sterol isomerase role of the emopamil-binding protein in the cholesterol biosynthetic pathway in animal cells. In contrast, there is no evidence for such a role of the sigma 1 receptor, in spite of the structural similarity shared by this protein and yeast sterol isomerase. We have found that SR31747A also exerts anti-proliferative effects at nanomolar concentrations on various established cell lines. The antiproliferative activity of SR31747A is reversed by cholesterol. Sterol-isomerase overproduction enhances resistance of CHO cells. This last observation strongly suggests that sterol isomerase is implicated in the antiproliferative effect of the drug in established cell lines.

show abstract

Section: Discussionsupporting

confidence: 82%

Section: Discussionmentioning

confidence: 87%

Antiproliferative effects of SR31747A in animal cell lines are mediated by inhibition of cholesterol biosynthesis at the sterol isomerase step

Bouteiller

Jamme

David

et al. 1998

European Journal of Biochemistry

View full text Add to dashboard Cite

show abstract

“…This isomerase is a putative target of drugs effective in animal models of stroke (13). Surprisingly, the mammalian genome contains another protein without homology to the human sterol ⌬8-⌬7 isomerase that shows significant pharmacological and structural similarities with the sterol ⌬8-⌬7 isomerase of Saccharomyces cerevisiae (14)(15)(16)(17). We now report the cloning of the ultimate enzyme of mammalian sterol biosynthesis, the ⌬7-sterol reductase.…”

mentioning

confidence: 99%

Molecular cloning and expression of the human Δ7-sterol reductase

Moebius

Fitzky

Lee

et al. 1998

Proc. Natl. Acad. Sci. U.S.A.

Self Cite

212

166

View full text Add to dashboard Cite

Inhibitors of the last steps of cholesterol biosynthesis such as AY9944 and BM15766 severely impair brain development. Their molecular target is the ⌬7-sterol reductase (EC 1.3.1.21), suspected to be defective in the Smith-Lemli-Opitz syndrome, a frequent inborn disorder of sterol metabolism. Molecular cloning of the cDNA revealed that the human enzyme is a membrane-bound protein with a predicted molecular mass of 55 kDa and six to nine putative transmembrane segments. The protein is structurally related to plant and yeast sterol reductases. In adults the ubiquitously transcribed mRNA is most abundant in adrenal gland, liver, testis, and brain. The ⌬7-sterol reductase is the ultimate enzyme of cholesterol biosynthesis in vertebrates and is absent from yeast. Microsomes from Saccharomyces cerevisiae strains heterologously expressing the human cDNA remove the C 7-8 double bond in 7-dehydrocholesterol. The conversion to cholesterol depends on NADPH and is potently inhibited by AY9944 (IC 50 0.013 M), BM15766 (IC 50 1.2 M), and triparanol (IC 50 14 M). Our work paves the way to clarify whether a defect in the ⌬7-sterol reductase gene underlies the Smith-Lemli-Opitz syndrome.

show abstract

“…Sigma 1 receptor (Sig-1R), a promising target for the treatment of neurodegenerative disease because of its multifaceted roles in cellular survival (6)(7)(8), is a unique membrane protein with no homology to other mammalian proteins (9,10). N,N-dimethyltryptamine is the only endogenous Sig1R ligand identified (11).…”

mentioning

confidence: 99%

Activation of the molecular chaperone, sigma 1 receptor, preserves cone function in a murine model of inherited retinal degeneration

Wang

Saul

Roon

et al. 2016

Proc. Natl. Acad. Sci. U.S.A.

119

View full text Add to dashboard Cite

Retinal degenerative diseases are major causes of untreatable blindness, and novel approaches to treatment are being sought actively. Here we explored the activation of a unique protein, sigma 1 receptor (Sig1R), in the treatment of PRC loss because of its multifaceted role in cellular survival. We used Pde6β rd10 (rd10) mice, which harbor a mutation in the rod-specific phosphodiesterase gene Pde6β and lose rod and cone photoreceptor cells (PRC) within the first 6 wk of life, as a model for severe retinal degeneration. Systemic administration of the high-affinity Sig1R ligand (+)-pentazocine [(+)-PTZ] to rd10 mice over several weeks led to the rescue of cone function as indicated by electroretinographic recordings using natural noise stimuli and preservation of cone cells upon spectral domain optical coherence tomography and retinal histological examination. The protective effect appears to result from the activation of Sig1R, because rd10/Sig1R

show abstract

Yeast Sterol C₈−C₇ Isomerase: Identification and Characterization of a High-Affinity Binding Site for Enzyme Inhibitors

Cited by 65 publications

References 34 publications

Antiproliferative effects of SR31747A in animal cell lines are mediated by inhibition of cholesterol biosynthesis at the sterol isomerase step

Antiproliferative effects of SR31747A in animal cell lines are mediated by inhibition of cholesterol biosynthesis at the sterol isomerase step

Molecular cloning and expression of the human Δ7-sterol reductase

Activation of the molecular chaperone, sigma 1 receptor, preserves cone function in a murine model of inherited retinal degeneration

Contact Info

Product

Resources

About

Yeast Sterol C8−C7 Isomerase: Identification and Characterization of a High-Affinity Binding Site for Enzyme Inhibitors

Cited by 65 publications

References 34 publications

Antiproliferative effects of SR31747A in animal cell lines are mediated by inhibition of cholesterol biosynthesis at the sterol isomerase step

Antiproliferative effects of SR31747A in animal cell lines are mediated by inhibition of cholesterol biosynthesis at the sterol isomerase step

Molecular cloning and expression of the human Δ7-sterol reductase

Activation of the molecular chaperone, sigma 1 receptor, preserves cone function in a murine model of inherited retinal degeneration

Contact Info

Product

Resources

About

Yeast Sterol C₈−C₇ Isomerase: Identification and Characterization of a High-Affinity Binding Site for Enzyme Inhibitors