Role of Flexibility in Protein-DNA-Drug Recognition: The Case of Asp677Gly-Val703Ile Topoisomerase Mutant Hypersensitive to Camptothecin

Author:

D'Annessa Ilda1,Tesauro Cinzia1,Fiorani Paola1,Chillemi Giovanni2,Castelli Silvia1,Vassallo Oscar1,Capranico Giovanni3,Desideri Alessandro1

Affiliation:

1. National Research Council (CNR) and Department of Biology, University of Rome Tor Vergata, Via Della Ricerca Scientifica, Rome 00133, Italy

2. CASPUR, Via dei Tizii 6b, Rome 00185, Italy

3. Department of Biochemistry “Giovanni Moruzzi,” University of Bologna, Via Irnerio 48, 40126 Bologna, Italy

Abstract

Topoisomerases I are ubiquitous enzymes that control DNA topology within the cell. They are the unique target of the antitumor drug camptothecin that selectively recognizes the DNA-topoisomerase covalent complex and reversibly stabilizes it. The biochemical and structural-dynamical properties of the Asp677Gly-Val703Ile double mutant with enhanced CPT sensitivity have been investigated. The mutant displays a lower religation rate of the DNA substrate when compared to the wild-type protein. Analyses of the structural dynamical properties by molecular dynamics simulation show that the mutant has reduced flexibility and an active site partially destructured at the level of the Lys532 residue. These results demonstrate long-range communication mechanism where reduction of the linker flexibility alters the active site geometry with the consequent lowering of the religation rate and increase in drug sensitivity.

Funder

American International Recruitment Council

Publisher

Hindawi Limited

Subject

Molecular Biology,Biochemistry,Molecular Biology,Biochemistry

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