Literature DB >> 27914300

Structure-based analysis of Bacilli and plasmid dihydrofolate reductase evolution.

Mona Alotaibi1, Ben Delos Reyes2, Tin Le2, Phuong Luong2, Faramarz Valafar3, Robert P Metzger4, Gary B Fogel5, David Hecht6.   

Abstract

Dihydrofolate reductase (DHFR), a key enzyme in tetrahydrofolate-mediated biosynthetic pathways, has a structural motif known to be highly conserved over a wide range of organisms. Given its critical role in purine and amino acid synthesis, DHFR is a well established therapeutic target for treating a wide range of prokaryotic and eukaryotic infections as well as certain types of cancer. Here we present a structural-based computer analysis of bacterial (Bacilli) and plasmid DHFR evolution. We generated a structure-based sequence alignment using 7 wild-type DHFR x-ray crystal structures obtained from the RCSB Protein Data Bank and 350 chromosomal and plasmid homology models we generated from sequences obtained from the NCBI Protein Database. We used these alignments to compare active site and non-active site conservation in terms of amino acid residues, secondary structure and amino acid residue class. With respect to amino acid sequences and residue classes, active-site positions in both plasmid and chromosomal DHFR are significantly more conserved than non-active site positions. Secondary structure conservation was similar for active site and non-active site positions. Plasmid-encoded DHFR proteins have greater degree of sequence and residue class conservation, particularly in sequence positions associated with a network of concerted protein motions, than chromosomal-encoded DHFR proteins. These structure-based were used to build DHFR specific phylogenetic trees from which evidence for horizontal gene transfer was identified.
Copyright © 2016 Elsevier Inc. All rights reserved.

Entities:  

Keywords:  DHFR; Dihydrofolate Reductase; Evolution; Horizontal Gene Transfer; Network of Coupled Protein Motion; Phylogeny; Plasmid evolution; Structure-based Alignment

Mesh:

Substances:

Year:  2016        PMID: 27914300      PMCID: PMC5203806          DOI: 10.1016/j.jmgm.2016.10.011

Source DB:  PubMed          Journal:  J Mol Graph Model        ISSN: 1093-3263            Impact factor:   2.518


  70 in total

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Review 2.  Relating protein motion to catalysis.

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3.  Structural-based analysis of dihydrofolate reductase evolution.

Authors:  David Hecht; Jonathan Tran; Gary B Fogel
Journal:  Mol Phylogenet Evol       Date:  2011-06-17       Impact factor: 4.286

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5.  Iron requirement of Lactobacillus spp. in completely chemically defined growth media.

Authors:  M Elli; R Zink; A Rytz; R Reniero; L Morelli
Journal:  J Appl Microbiol       Date:  2000-04       Impact factor: 3.772

6.  Trimethoprim resistance determined by R factors.

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7.  Investigation of the structural basis for thermostability of DNA-binding protein HU from Bacillus stearothermophilus.

Authors:  S Kawamura; Y Abe; T Ueda; K Masumoto; T Imoto; N Yamasaki; M Kimura
Journal:  J Biol Chem       Date:  1998-08-07       Impact factor: 5.157

8.  Modeling the evolution of drug resistance in malaria.

Authors:  David Hecht; Gary B Fogel
Journal:  J Comput Aided Mol Des       Date:  2012-11-21       Impact factor: 3.686

9.  Protein Homeostasis Imposes a Barrier on Functional Integration of Horizontally Transferred Genes in Bacteria.

Authors:  Shimon Bershtein; Adrian W R Serohijos; Sanchari Bhattacharyya; Michael Manhart; Jeong-Mo Choi; Wanmeng Mu; Jingwen Zhou; Eugene I Shakhnovich
Journal:  PLoS Genet       Date:  2015-10-20       Impact factor: 5.917

Review 10.  The genus Weissella: taxonomy, ecology and biotechnological potential.

Authors:  Vincenzina Fusco; Grazia M Quero; Gyu-Sung Cho; Jan Kabisch; Diana Meske; Horst Neve; Wilhelm Bockelmann; Charles M A P Franz
Journal:  Front Microbiol       Date:  2015-03-17       Impact factor: 5.640

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