Julie Thompson scite author profile

The sensitivity of the commonly used progressive multiple sequence alignment method has been greatly improved for the alignment of divergent protein sequences. Firstly, individual weights are assigned to each sequence in a partial alignment in order to down-weight near-duplicate sequences and up-weight the most divergent ones. Secondly, amino acid substitution matrices are varied at different alignment stages according to the divergence of the sequences to be aligned. Thirdly, residue-specific gap penalties and locally reduced gap penalties in hydrophilic regions encourage new gaps in potential loop regions rather than regular secondary structure. Fourthly, positions in early alignments where gaps have been opened receive locally reduced gap penalties to encourage the opening up of new gaps at these positions. These modifications are incorporated into a new program, CLUSTAL W which is freely available.

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Clustal W and Clustal X version 2.0

Larkin

et al. 2007

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The CLUSTAL_X windows interface: flexible strategies for multiple sequence alignment aided by quality analysis tools

et al. 1997

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CLUSTAL X is a new windows interface for the widely-used progressive multiple sequence alignment program CLUSTAL W. The new system is easy to use, providing an integrated system for performing multiple sequence and profile alignments and analysing the results. CLUSTAL X displays the sequence alignment in a window on the screen. A versatile sequence colouring scheme allows the user to highlight conserved features in the alignment. Pull-down menus provide all the options required for traditional multiple sequence and profile alignment. New features include: the ability to cut-and-paste sequences to change the order of the alignment, selection of a subset of the sequences to be realigned, and selection of a sub-range of the alignment to be realigned and inserted back into the original alignment. Alignment quality analysis can be performed and low-scoring segments or exceptional residues can be highlighted. Quality analysis and realignment of selected residue ranges provide the user with a powerful tool to improve and refine difficult alignments and to trap errors in input sequences. CLUSTAL X has been compiled on SUN Solaris, IRIX5.3 on Silicon Graphics, Digital UNIX on DECstations, Microsoft Windows (32 bit) for PCs, Linux ELF for x86 PCs, and Macintosh PowerMac.

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Fast, scalable generation of high‐quality protein multiple sequence alignments using Clustal Omega

Sievers

Wilm

Dineen

et al. 2011

Molecular Systems Biology

12,648

9,521

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Multiple sequence alignment with the Clustal series of programs

Ramu

Sugawara²,

Koike³

et al. 2003

Nucleic Acids Research

4,316

2,998

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The Clustal series of programs are widely used in molecular biology for the multiple alignment of both nucleic acid and protein sequences and for preparing phylogenetic trees. The popularity of the programs depends on a number of factors, including not only the accuracy of the results, but also the robustness, portability and user-friendliness of the programs. New features include NEXUS and FASTA format output, printing range numbers and faster tree calculation. Although, Clustal was originally developed to run on a local computer, numerous Web servers have been set up, notably at the EBI (European Bioinformatics Institute) (http://www.ebi.ac.uk/clustalw/).

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Multiple Sequence Alignment Using ClustalW and ClustalX

Thompson

Gibson

Higgins

2002

CP in Bioinformatics

2,013

1,569

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The Clustal programs are widely used for carrying out automatic multiple alignment of nucleotide or amino acid sequences. The most familiar version is ClustalW, which uses a simple text menu system that is portable to more or less all computer systems. ClustalX features a graphical user interface and some powerful graphical utilities for aiding the interpretation of alignments and is the preferred version for interactive usage. Users may run Clustal remotely from several sites using the Web or the programs may be downloaded and run locally on PCs, Macintosh, or Unix computers. The protocols in this unit discuss how to use ClustalX and ClustalW to construct an alignment, and create profile alignments by merging existing alignments.

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Multiple sequence alignment with Clustal X

Jeanmougin¹,

Thompson²,

Gouy³

et al. 1998

Trends in Biochemical Sciences

2,457

1,519

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[22] Using CLUSTAL for multiple sequence alignments

Higgins¹,

Thompson²,

Gibson³

1996

1,485

956

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Julie Thompson

CLUSTAL W: improving the sensitivity of progressive multiple sequence alignment through sequence weighting, position-specific gap penalties and weight matrix choice

Clustal W and Clustal X version 2.0

The CLUSTAL_X windows interface: flexible strategies for multiple sequence alignment aided by quality analysis tools

Fast, scalable generation of high‐quality protein multiple sequence alignments using Clustal Omega

Multiple sequence alignment with the Clustal series of programs

Multiple Sequence Alignment Using ClustalW and ClustalX

Multiple sequence alignment with Clustal X

[22] Using CLUSTAL for multiple sequence alignments

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