lidorestat   Click here for help

GtoPdb Ligand ID: 7411

Synonyms: IDD-000676-01 | IDD-676
PDB Ligand
Compound class: Synthetic organic
Comment: Lidorestat is an experimental aldose reductase inhibitor. [1-2].
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2D Structure
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Physico-chemical Properties
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Hydrogen bond acceptors 3
Hydrogen bond donors 1
Rotatable bonds 4
Topological polar surface area 83.36
Molecular weight 376.05
XLogP 3.6
No. Lipinski's rules broken 0
SMILES / InChI / InChIKey
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Canonical SMILES OC(=O)Cn1cc(c2c1cccc2)Cc1sc2c(n1)c(F)c(cc2F)F
Isomeric SMILES OC(=O)Cn1cc(c2c1cccc2)Cc1sc2c(n1)c(F)c(cc2F)F
InChI InChI=1S/C18H11F3N2O2S/c19-11-6-12(20)18-17(16(11)21)22-14(26-18)5-9-7-23(8-15(24)25)13-4-2-1-3-10(9)13/h1-4,6-7H,5,8H2,(H,24,25)
InChI Key KYHVTMFADJNSGS-UHFFFAOYSA-N
References
1. Maccari R, Ciurleo R, Giglio M, Cappiello M, Moschini R, Corso AD, Mura U, Ottanà R. (2010)
Identification of new non-carboxylic acid containing inhibitors of aldose reductase.
Bioorg Med Chem, 18 (11): 4049-55. [PMID:20452228]
2. Maccari R, Ottanà R, Ciurleo R, Rakowitz D, Matuszczak B, Laggner C, Langer T. (2008)
Synthesis, induced-fit docking investigations, and in vitro aldose reductase inhibitory activity of non-carboxylic acid containing 2,4-thiazolidinedione derivatives.
Bioorg Med Chem, 16 (11): 5840-52. [PMID:18492610]
3. Srivastava SK, Ramana KV, Bhatnagar A. (2005)
Role of aldose reductase and oxidative damage in diabetes and the consequent potential for therapeutic options.
Endocr Rev, 26 (3): 380-92. [PMID:15814847]
4. Van Zandt MC, Doan B, Sawicki DR, Sredy J, Podjarny AD. (2009)
Discovery of [3-(4,5,7-trifluoro-benzothiazol-2-ylmethyl)-pyrrolo[2,3-b]pyridin-1-yl]acetic acids as highly potent and selective inhibitors of aldose reductase for treatment of chronic diabetic complications.
Bioorg Med Chem Lett, 19 (7): 2006-8. [PMID:19250825]
5. Van Zandt MC, Jones ML, Gunn DE, Geraci LS, Jones JH, Sawicki DR, Sredy J, Jacot JL, Dicioccio AT, Petrova T et al.. (2005)
Discovery of 3-[(4,5,7-trifluorobenzothiazol-2-yl)methyl]indole-N-acetic acid (lidorestat) and congeners as highly potent and selective inhibitors of aldose reductase for treatment of chronic diabetic complications.
J Med Chem, 48 (9): 3141-52. [PMID:15857120]