SEQUENCE SLIDER: expanding polyalanine fragments for phasing with multiple side-chain hypotheses

Fragment-based molecular-replacement methods can solve a macromolecular structure quasi-ab initio. ARCIMBOLDO, using a common secondary-structure or tertiary-structure template or a library of folds, locates these with Phaser and reveals the rest of the structure by density modification and autotrac...

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Autores principales: Borges, Rafael Junqueira, Meindl, Kathrin, Triviño, Josep, Sammito, Massimo, Medina, Ana, Millán, Claudia, Alcorlo, Martin, Hermoso, Juan A., Fontes, Marcos Roberto de Mattos, Usón, Isabel
Formato: Online Artículo Texto
Lenguaje:English
Publicado: International Union of Crystallography 2020
Materias:
Ccp4
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7057211/
https://www.ncbi.nlm.nih.gov/pubmed/32133987
http://dx.doi.org/10.1107/S2059798320000339
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author Borges, Rafael Junqueira
Meindl, Kathrin
Triviño, Josep
Sammito, Massimo
Medina, Ana
Millán, Claudia
Alcorlo, Martin
Hermoso, Juan A.
Fontes, Marcos Roberto de Mattos
Usón, Isabel
author_facet Borges, Rafael Junqueira
Meindl, Kathrin
Triviño, Josep
Sammito, Massimo
Medina, Ana
Millán, Claudia
Alcorlo, Martin
Hermoso, Juan A.
Fontes, Marcos Roberto de Mattos
Usón, Isabel
author_sort Borges, Rafael Junqueira
collection PubMed
description Fragment-based molecular-replacement methods can solve a macromolecular structure quasi-ab initio. ARCIMBOLDO, using a common secondary-structure or tertiary-structure template or a library of folds, locates these with Phaser and reveals the rest of the structure by density modification and autotracing in SHELXE. The latter stage is challenging when dealing with diffraction data at lower resolution, low solvent content, high β-sheet composition or situations in which the initial fragments represent a low fraction of the total scattering or where their accuracy is low. SEQUENCE SLIDER aims to overcome these complications by extending the initial polyalanine fragment with side chains in a multisolution framework. Its use is illustrated on test cases and previously unknown structures. The selection and order of fragments to be extended follows the decrease in log-likelihood gain (LLG) calculated with Phaser upon the omission of each single fragment. When the starting substructure is derived from a remote homolog, sequence assignment to fragments is restricted by the original alignment. Otherwise, the secondary-structure prediction is matched to that found in fragments and traces. Sequence hypotheses are trialled in a brute-force approach through side-chain building and refinement. Scoring the refined models through their LLG in Phaser may allow discrimination of the correct sequence or filter the best partial structures for further density modification and autotracing. The default limits for the number of models to pursue are hardware dependent. In its most economic implementation, suitable for a single laptop, the main-chain trace is extended as polyserine rather than trialling models with different sequence assignments, which requires a grid or multicore machine. SEQUENCE SLIDER has been instrumental in solving two novel structures: that of MltC from 2.7 Å resolution data and that of a pneumococcal lipoprotein with 638 residues and 35% solvent content.
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spelling pubmed-70572112020-03-06 SEQUENCE SLIDER: expanding polyalanine fragments for phasing with multiple side-chain hypotheses Borges, Rafael Junqueira Meindl, Kathrin Triviño, Josep Sammito, Massimo Medina, Ana Millán, Claudia Alcorlo, Martin Hermoso, Juan A. Fontes, Marcos Roberto de Mattos Usón, Isabel Acta Crystallogr D Struct Biol Ccp4 Fragment-based molecular-replacement methods can solve a macromolecular structure quasi-ab initio. ARCIMBOLDO, using a common secondary-structure or tertiary-structure template or a library of folds, locates these with Phaser and reveals the rest of the structure by density modification and autotracing in SHELXE. The latter stage is challenging when dealing with diffraction data at lower resolution, low solvent content, high β-sheet composition or situations in which the initial fragments represent a low fraction of the total scattering or where their accuracy is low. SEQUENCE SLIDER aims to overcome these complications by extending the initial polyalanine fragment with side chains in a multisolution framework. Its use is illustrated on test cases and previously unknown structures. The selection and order of fragments to be extended follows the decrease in log-likelihood gain (LLG) calculated with Phaser upon the omission of each single fragment. When the starting substructure is derived from a remote homolog, sequence assignment to fragments is restricted by the original alignment. Otherwise, the secondary-structure prediction is matched to that found in fragments and traces. Sequence hypotheses are trialled in a brute-force approach through side-chain building and refinement. Scoring the refined models through their LLG in Phaser may allow discrimination of the correct sequence or filter the best partial structures for further density modification and autotracing. The default limits for the number of models to pursue are hardware dependent. In its most economic implementation, suitable for a single laptop, the main-chain trace is extended as polyserine rather than trialling models with different sequence assignments, which requires a grid or multicore machine. SEQUENCE SLIDER has been instrumental in solving two novel structures: that of MltC from 2.7 Å resolution data and that of a pneumococcal lipoprotein with 638 residues and 35% solvent content. International Union of Crystallography 2020-02-25 /pmc/articles/PMC7057211/ /pubmed/32133987 http://dx.doi.org/10.1107/S2059798320000339 Text en © Borges et al. 2020 http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution (CC-BY) Licence, which permits unrestricted use, distribution, and reproduction in any medium, provided the original authors and source are cited.http://creativecommons.org/licenses/by/4.0/
spellingShingle Ccp4
Borges, Rafael Junqueira
Meindl, Kathrin
Triviño, Josep
Sammito, Massimo
Medina, Ana
Millán, Claudia
Alcorlo, Martin
Hermoso, Juan A.
Fontes, Marcos Roberto de Mattos
Usón, Isabel
SEQUENCE SLIDER: expanding polyalanine fragments for phasing with multiple side-chain hypotheses
title SEQUENCE SLIDER: expanding polyalanine fragments for phasing with multiple side-chain hypotheses
title_full SEQUENCE SLIDER: expanding polyalanine fragments for phasing with multiple side-chain hypotheses
title_fullStr SEQUENCE SLIDER: expanding polyalanine fragments for phasing with multiple side-chain hypotheses
title_full_unstemmed SEQUENCE SLIDER: expanding polyalanine fragments for phasing with multiple side-chain hypotheses
title_short SEQUENCE SLIDER: expanding polyalanine fragments for phasing with multiple side-chain hypotheses
title_sort sequence slider: expanding polyalanine fragments for phasing with multiple side-chain hypotheses
topic Ccp4
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7057211/
https://www.ncbi.nlm.nih.gov/pubmed/32133987
http://dx.doi.org/10.1107/S2059798320000339
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