Extended knowledge of 2,4-Difluorobenzoic acid

If you are interested in 1583-58-0, you can contact me at any time and look forward to more communication. Recommanded Product: 1583-58-0.

In an article, author is Steuber, Holger, once mentioned the application of 1583-58-0, Recommanded Product: 1583-58-0, Name is 2,4-Difluorobenzoic acid, molecular formula is C7H4F2O2, molecular weight is 158.1, MDL number is MFCD00011670, category is isothiazole. Now introduce a scientific discovery about this category.

Evidence for a novel binding site conformer of aldose reductase in ligand-bound state

Human aldose reductase (ALR2) has evolved as a promising therapeutic target for the treatment of diabetic long-term complications. The binding site of this enzyme possesses two main subpockets: the catalytic anion-binding site and the hydrophobic specificity pocket. The latter can be observed in the open or closed state, depending on the bound ligand. Thus, it exhibits a pronounced capability for induced-fit adaptations, whereas the, catalytic pocket exhibits rigid properties throughout all known crystal, structures. Here, we determined two ALR2 crystal structures at 1.55 and 1.65 angstrom resolution, each complexed with an inhibitor of the recently described naphtho[1,2-d]isothiazole acetic acid series. In contrast to the original design hypothesis based on the binding mode of tolrestat (1), both inhibitors leave the specificity pocket in the closed state. Unexpectedly, the more potent ligand (2) extends the catalytic pocket by opening a novel subpocket. Access to this novel subpocket is mainly attributed to the rotation of an indole moiety of Trp 20 by about 35 degrees. The newly formed subpocket provides accommodation of the naphthyl portion of the ligand. The second inhibitor, 3, differs from 2 only by an extended glycolic ester functionality added to one of its carboxylic groups. However, despite this slight structural modification, the binding mode of 3 differs dramatically from that of the first inhibitor, but provokes less pronounced induced-fit adaptations of the binding cavity. Thus, a novel binding site conformation has been identified in a region where previous complex structures suggested only low adaptability of the binding pocket. Furthermore, the two ligand complexes represent an impressive example of how the slight change of a chemically extended side-chain at a given ligand scaffold can result in a dramatically altered binding mode. In addition, our study emphasizes the importance of crystal structure analysis for the translation of affinity data into structure-activity relationships. (c) 2007 Elsevier Ltd. All rights reserved.

If you are interested in 1583-58-0, you can contact me at any time and look forward to more communication. Recommanded Product: 1583-58-0.

Reference:
Isothiazole – Wikipedia,
,Isothiazole – ScienceDirect.com