4.6 Review

Molecular evolution of hydrogen peroxide degrading enzymes

Journal

ARCHIVES OF BIOCHEMISTRY AND BIOPHYSICS
Volume 525, Issue 2, Pages 131-144

Publisher

ELSEVIER SCIENCE INC
DOI: 10.1016/j.abb.2012.01.017

Keywords

Catalase; Catalase-peroxidase; Manganese catalase; Molecular evolution; Pathogen; Horizontal gene transfer

Funding

  1. Austrian science Fund (FWF Project) [P20996-B11]
  2. Doctoral Program Biomolecular Technology of Proteins - BioToP [FWF W1224]
  3. Austrian Science Fund (FWF) [P20996] Funding Source: Austrian Science Fund (FWF)

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For efficient removal of intra- and/or extracellular hydrogen peroxide by dismutation to harmless dioxygen and water (2H(2)O(2) -> O-2 + 2H(2)O), nature designed three metalloenzyme families that differ in oligomeric organization, monomer architecture as well as active site geometry and catalytic residues. Here we report on the updated reconstruction of the molecular phylogeny of these three gene families. Ubiquitous typical (monofunctional) heme catalases are found in all domains of life showing a high structural conservation. Their evolution was directed from large subunit towards small subunit proteins and further to fused proteins where the catalase fold was retained but lost its original functionality. Bifunctional catalase-peroxidases were at the origin of one of the two main heme peroxidase superfamilies (i.e. peroxidase-catalase superfamily) and constitute a protein family predominantly present among eubacteria and archaea, but two evolutionary branches are also found in the eukaryotic world. Non-heme manganese catalases are a relatively small protein family with very old roots only present among bacteria and archaea. Phylogenetic analyses of the three protein families reveal features typical (i) for the evolution of whole genomes as well as (ii) for specific evolutionary events including horizontal gene transfer, paralog formation and gene fusion. As catalases have reached a striking diversity among prokaryotic and eukaryotic pathogens, understanding their phylogenetic and molecular relationship and function will contribute to drug design for prevention of diseases of humans, animals and plants. (c) 2012 Elsevier Inc. All rights reserved.

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