Nomenclature for the description of sequence variations; History

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Draft 3; 29Nov96

RECOMMENDATIONS FOR A NOMENCLATURE SYSTEM FOR HUMAN GENE MUTATIONS

Prepared by Stylianos E Antonarakis

Introduction

This document is created as a result of the meeting on "locus-specific mutation databases" held on March 24, 1996 in Heidelberg, Germany and the "Mutation Database" meeting on October 29, 1996 in San Francisco, California. As a chairperson of the Nomenclature committee, I had accepted the task preparing and circulating a document with recommendations for debate, further discussions and most importantly for final approval / acceptance at the October 1996 meeting in San Francisco. The first draft of this document (5 Aug 96) was distributed to a number of investigators, the majority of which are co-authors in the Beaudet et al and Beutler et al papers (see below). This second draft (5 Sep 96) contained modifications according to their suggestions, opinions and criticisms. Furthermore, many colleagues had offered suggestions, criticisms, and ideas through electronic communication. During the October 29, 1996 meeting in San Francisco, there was a sufficient discussion of these recommendations and it was agreed that another, further modified draft of the document would be posted on the "World Wide Web" for final debate for a period of 6 weeks. Then, this set of initial recommendations would be published as guidelines for mutation nomenclature.

Two manuscripts were recently published in the journal "Human Mutation" that contain mutation nomenclature recommendations: "Update on nomenclature for human gene mutations" by Beaudet et al., Hum.Mut. 8: 197-202, 1996 and "Mutation nomenclature: nicknames, systematic names and unique identifiers" by Beutler et al., Hum.Mut. 8: 203-206, 1996. These documents present the views of the authors after discussions during the October 19, 1994, Montreal and the October 24-25, 1995 Minneapolis meetings. Other published papers/letters on nomenclature issues include the following: Beaudet & Tsui, Hum.Mut. 2: 245, 1993; Beutler, Am.J.Hum.Genet. 53: 783, 1993; Antonarakis & McKusick, Hum.Mut. 4: 166, 1994.

It is obvious that the most unambiguous nomenclature system is that based on genomic DNA. Even in that case, however, length polymorphisms create a problem in the numbering of nucleotides and therefore a standard, reference sequence ought to be established, preferably by the experts. Unfortunately, the entire genomic sequence is only known for a minority of human genes. For the vast majority of genes, the known sequence is that of cDNA. The existence of more than one transcription start site, alternative splicing and utilization of alternative exons and variable number of repeats complicate the nucleotide numbering and here too a reference sequence needs to be established. The nomenclature, at least in the present state of the human genome development, needs to be accurate, unambiguous, but flexible. The nucleotide change must always be included in the original report; however other names, for example based on amino acid changes, may be used. The genomic DNA-based nomenclature was termed "systematic" by Beutler at al, while all other mutation names were considered as "trivial" or "common" by these authors.

A list of recommendations follows:

For genomic DNA and cDNA , the A of the ATG of the initiator Met codon is nucleotide +1. There is no nucleotide zero (0). The nucleotide 5' to +1 is numbered -1. If there is more than one potential ATG, a reference consensus may be used. The numbering of nucleotides in the reference sequence in the databases should not be changed and will always be associated with the same (original) accession number.
The use of lower case g for genomic or c for cDNA in front of the nucleotide number is recommended. To avoid confusion, a dot should separate these from the nucleotide number (g. or c. for genomic or cDNA respectively). The reference sequence Genbank number should also be included in the original publication/database submission.
Nucleotide changes start with the nucleotide number and the change follows this number. 1996G>T denotes that at nucleotide 1996 of the reference sequence, G is replaced by a T.
Deletions are designated by del after the nucleotide number. 1996delT denotes the deletion of T at nt 1996. 1996-1998del denotes the deletion of 3 nts. Alternatively this mutation can be denoted as 1996-1998delTTC. For deletions in short tandem repeats the most 3' nt is arbitrarily assigned; eg. a TG deletion in the sequence AATGTGTGCC is designated 1996-1997delTG or 1996-1997del (where 1996 is the first T before C).
Insertions are designated by ins after the nucleotide interval number. 1996-1997insT denotes that T was inserted in the interval between nts 1996 and 1997. For insertions in short repeats the most 3' nt interval is arbitrarily assigned; eg. a TG insertion in the sequence AATGTGTGCC is designated 1996-1997insTG (where 1996 is the last G of the short TG repeat).
DNA polymorphic variants may be designated as alternative possibilities by an /. For example, 1996G/A denotes that in a given normal population there is either G or A at nt 1996. The system can accommodate short sequence repeat polymorphisms; eg 1996(GT)6-22. In this case, 1996 is the first nucleotide of the dinucleotide repeat.
A unique identifier per mutation should be obtained. The OMIM unique identifier can be used, or database curators may assign such unique identifiers.
Intron mutations when the full genomic sequence is not known can be designated by the intron (IVS) number, positive numbers starting from the G of the donor site invariant GT, negative numbers starting from the G of the acceptor site invariant AG. IVS4+1G>T denotes the G to T substitution at nt +1 of intron 4. IVS4-2A>C denotes the A to C substitution at nt -2 of intron 4. When the full length genomic sequence
is known, the mutation can also be simply designated by the nt number of the reference sequence.
Two mutations in the same allele can be listed within brackets as follows: [1996G>T; 2001A>C]. This will also allow the (i) designation of mutations that are only deleterious when they occur in the same allele with additional nucleotide substitutions; (ii) designation of haplotypes of different alleles.
For amino acid-based systems, the codon for the initiator Methionine is codon 1.
The single letter amino acid code is recommended. However the three letter code is also acceptable.
For amino acid nomenclature, the format is Y96S (Tyrosine at codon 96 substituted by Serine). The "wild type" amino acid is given before and the mutant amino acid after the codon number. Therefore there is no confusion for the significance of G,C,T and A in the nomenclature.
Stop codons are designated by X. For example R96X (Arginine codon 96 substituted by a termination codon).
Deletions of amino acids are designated as: T96del denotes that the codon 96 for Threonine is deleted.
Insertions of amino acids are designated as: T96-97ins denotes that a codon for Threonine is inserted at the interval between codons 96 and 97 of the reference sequence of the protein.
Normal amino acid polymorphic variants may be designated as alternative possibilities by an /. For example, G/A96 denotes that in a given normal population there is either Glycine or Alanine at codon 96.
The first report of a mutation in the literature should contain both a nucleotide and amino acid based name when appropriate.

No recommendations are made at this time for more complex mutations. Detailed description for such mutations and nomenclature proposals can be usually found in the original reference or by the unique identifier. A second phase of recommendations will deal with such issues in the future. In addition, the consequence of a mutation (frameshift, particular splicing abnormality, exon skipping etc) is not included in the mutation name. However, investigators that maintain mutation databases are encouraged to include a field of mutation consequence or mutation mechanism (if known) in their databases.

This version of this document will be posted for 6 weeks starting 2nd December, 1996.

After this date the recommendations will be published as guidelines for investigators.

Please forward to my email address (sea@medsun.unige.ch) your comments, suggestions, criticisms.

We would also invite you to co-sign this document (if you do not have major disagreements with its content). Your participation and names will appear in the published version of these recommendations. Please include your institution, address, and email coordinates.

Stylianos E. Antonarakis MD, DSc
Professor of Medical Genetics
University of Geneva Medical School
9 avenue de Champel
1211 Geneva
SWITZERLAND

Tel. +41-22-702.57.07
Fax: +41-22-702.57.06
E-mail: sea@medsun.unige.ch