Conformational ensembles, signal transduction and residue hot spots: Application to drug discovery

Author:

Ozbabacan, S. E. A.

Gursoy, A.

Keskin, O.

Nussinov, R.
Author Address

[Nussinov, Ruth] NCI, SAIC Frederick Inc, Basic Sci Program, Ctr Canc Res Nanobiol Program, Frederick, MD 21702 USA. [Ozbabacan, Saliha Ece Acuner; Gursoy, Attila; Keskin, Ozlem] Koc Univ, Ctr Computat Biol & Bioinformat, TR-34450 Istanbul, Turkey. [Ozbabacan, Saliha Ece Acuner; Gursoy, Attila; Keskin, Ozlem] Koc Univ, Coll Engn, TR-34450 Istanbul, Turkey. [Nussinov, Ruth] Tel Aviv Univ, Sackler Inst Mol Med, Dept Human Genet & Mol Med, Sackler Sch Med, IL-69978 Tel Aviv, Israel.;Nussinov, R, NCI, SAIC Frederick Inc, Basic Sci Program, Ctr Canc Res Nanobiol Program, 1050 Boyles St, Frederick, MD 21702 USA.;ruthnu@helix.nih.gov

Abstract:

A key step in drug development is the identification of both a protein target and its topological cellular network location and interactions, with regard to information flow in disease-causing events and to medication effects. Information flow involves a cascade of binding or covalent modification processes, with each step being affected by those that occur previously. Proteins are flexible, and information flows via dynamic changes in the distribution of conformational protein ensembles; molecular recognition is mainly determined by these changes. Drug discovery often focuses on signaling proteins situated at the crossroads of cellular networks; such signaling proteins have multiple partners that bind through shared binding sites. This review highlights these shared binding sites, and describes research to suggest that partners binding at these sites could at least partly interact via different energetically dominant 'hot-spot' residues. The data also indicate that, despite dynamic changes in the distribution of the conformational ensembles, the hot-spot conformations are retained in their pre-organized states.

See More

Author Address