QSAR for RNases and theoretic–experimental study of molecular diversity on peptide mass fingerprints of a new Leishmania infantum protein

The toxicity and low success of current treatments for Leishmaniosis determines the search of new peptide drugs and/or molecular targets in Leishmania pathogen species (L. infantum and L. major). For example, Ribonucleases (RNases) are enzymes relevant to several biologic processes; then, theoretica...

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Autores principales: González-Díaz, Humberto, Dea-Ayuela, María A., Pérez-Montoto, Lázaro G., Prado-Prado, Francisco J., Agüero-Chapín, Guillermín, Bolas-Fernández, Francisco, Vazquez-Padrón, Roberto I., Ubeira, Florencio M.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Springer Netherlands 2009
Materias:
Full-Length Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7088557/
https://www.ncbi.nlm.nih.gov/pubmed/19578942
http://dx.doi.org/10.1007/s11030-009-9178-0
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author González-Díaz, Humberto
Dea-Ayuela, María A.
Pérez-Montoto, Lázaro G.
Prado-Prado, Francisco J.
Agüero-Chapín, Guillermín
Bolas-Fernández, Francisco
Vazquez-Padrón, Roberto I.
Ubeira, Florencio M.
author_facet González-Díaz, Humberto
Dea-Ayuela, María A.
Pérez-Montoto, Lázaro G.
Prado-Prado, Francisco J.
Agüero-Chapín, Guillermín
Bolas-Fernández, Francisco
Vazquez-Padrón, Roberto I.
Ubeira, Florencio M.
author_sort González-Díaz, Humberto
collection PubMed
description The toxicity and low success of current treatments for Leishmaniosis determines the search of new peptide drugs and/or molecular targets in Leishmania pathogen species (L. infantum and L. major). For example, Ribonucleases (RNases) are enzymes relevant to several biologic processes; then, theoretical and experimental study of the molecular diversity of Peptide Mass Fingerprints (PMFs) of RNases is useful for drug design. This study introduces a methodology that combines QSAR models, 2D-Electrophoresis (2D-E), MALDI-TOF Mass Spectroscopy (MS), BLAST alignment, and Molecular Dynamics (MD) to explore PMFs of RNases. We illustrate this approach by investigating for the first time the PMFs of a new protein of L. infantum. Here we report and compare new versus old predictive models for RNases based on Topological Indices (TIs) of Markov Pseudo-Folding Lattices. These group of indices called Pseudo-folding Lattice 2D-TIs include: Spectral moments π (k)(x,y), Mean Electrostatic potentials ξ (k)(x,y), and Entropy measures θ (k)(x,y). The accuracy of the models (training/cross-validation) was as follows: ξ (k)(x,y)-model (96.0%/91.7%)>π (k)(x,y)-model (84.7/83.3) > θ (k)(x,y)-model (66.0/66.7). We also carried out a 2D-E analysis of biological samples of L. infantum promastigotes focusing on a 2D-E gel spot of one unknown protein with M<20, 100 and pI <7. MASCOT search identified 20 proteins with Mowse score >30, but not one >52 (threshold value), the higher value of 42 was for a probable DNA-directed RNA polymerase. However, we determined experimentally the sequence of more than 140 peptides. We used QSAR models to predict RNase scores for these peptides and BLAST alignment to confirm some results. We also calculated 3D-folding TIs based on MD experiments and compared 2D versus 3D-TIs on molecular phylogenetic analysis of the molecular diversity of these peptides. This combined strategy may be of interest in drug development or target identification. ELECTRONIC SUPPLEMENTARY MATERIAL: The online version of this article (doi:10.1007/s11030-009-9178-0) contains supplementary material, which is available to authorized users.
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spelling pubmed-70885572020-03-23 QSAR for RNases and theoretic–experimental study of molecular diversity on peptide mass fingerprints of a new Leishmania infantum protein González-Díaz, Humberto Dea-Ayuela, María A. Pérez-Montoto, Lázaro G. Prado-Prado, Francisco J. Agüero-Chapín, Guillermín Bolas-Fernández, Francisco Vazquez-Padrón, Roberto I. Ubeira, Florencio M. Mol Divers Full-Length Paper The toxicity and low success of current treatments for Leishmaniosis determines the search of new peptide drugs and/or molecular targets in Leishmania pathogen species (L. infantum and L. major). For example, Ribonucleases (RNases) are enzymes relevant to several biologic processes; then, theoretical and experimental study of the molecular diversity of Peptide Mass Fingerprints (PMFs) of RNases is useful for drug design. This study introduces a methodology that combines QSAR models, 2D-Electrophoresis (2D-E), MALDI-TOF Mass Spectroscopy (MS), BLAST alignment, and Molecular Dynamics (MD) to explore PMFs of RNases. We illustrate this approach by investigating for the first time the PMFs of a new protein of L. infantum. Here we report and compare new versus old predictive models for RNases based on Topological Indices (TIs) of Markov Pseudo-Folding Lattices. These group of indices called Pseudo-folding Lattice 2D-TIs include: Spectral moments π (k)(x,y), Mean Electrostatic potentials ξ (k)(x,y), and Entropy measures θ (k)(x,y). The accuracy of the models (training/cross-validation) was as follows: ξ (k)(x,y)-model (96.0%/91.7%)>π (k)(x,y)-model (84.7/83.3) > θ (k)(x,y)-model (66.0/66.7). We also carried out a 2D-E analysis of biological samples of L. infantum promastigotes focusing on a 2D-E gel spot of one unknown protein with M<20, 100 and pI <7. MASCOT search identified 20 proteins with Mowse score >30, but not one >52 (threshold value), the higher value of 42 was for a probable DNA-directed RNA polymerase. However, we determined experimentally the sequence of more than 140 peptides. We used QSAR models to predict RNase scores for these peptides and BLAST alignment to confirm some results. We also calculated 3D-folding TIs based on MD experiments and compared 2D versus 3D-TIs on molecular phylogenetic analysis of the molecular diversity of these peptides. This combined strategy may be of interest in drug development or target identification. ELECTRONIC SUPPLEMENTARY MATERIAL: The online version of this article (doi:10.1007/s11030-009-9178-0) contains supplementary material, which is available to authorized users. Springer Netherlands 2009-07-04 2010 /pmc/articles/PMC7088557/ /pubmed/19578942 http://dx.doi.org/10.1007/s11030-009-9178-0 Text en © Springer Science+Business Media B.V. 2009 This article is made available via the PMC Open Access Subset for unrestricted research re-use and secondary analysis in any form or by any means with acknowledgement of the original source. These permissions are granted for the duration of the World Health Organization (WHO) declaration of COVID-19 as a global pandemic.
spellingShingle Full-Length Paper
González-Díaz, Humberto
Dea-Ayuela, María A.
Pérez-Montoto, Lázaro G.
Prado-Prado, Francisco J.
Agüero-Chapín, Guillermín
Bolas-Fernández, Francisco
Vazquez-Padrón, Roberto I.
Ubeira, Florencio M.
QSAR for RNases and theoretic–experimental study of molecular diversity on peptide mass fingerprints of a new Leishmania infantum protein
title QSAR for RNases and theoretic–experimental study of molecular diversity on peptide mass fingerprints of a new Leishmania infantum protein
title_full QSAR for RNases and theoretic–experimental study of molecular diversity on peptide mass fingerprints of a new Leishmania infantum protein
title_fullStr QSAR for RNases and theoretic–experimental study of molecular diversity on peptide mass fingerprints of a new Leishmania infantum protein
title_full_unstemmed QSAR for RNases and theoretic–experimental study of molecular diversity on peptide mass fingerprints of a new Leishmania infantum protein
title_short QSAR for RNases and theoretic–experimental study of molecular diversity on peptide mass fingerprints of a new Leishmania infantum protein
title_sort qsar for rnases and theoretic–experimental study of molecular diversity on peptide mass fingerprints of a new leishmania infantum protein
topic Full-Length Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7088557/
https://www.ncbi.nlm.nih.gov/pubmed/19578942
http://dx.doi.org/10.1007/s11030-009-9178-0
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