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<li><a href="/genbank/htgs">About HTGs</a></li>
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<!-- was itemctrl -->
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<div class="container">
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<div id="maincontent" class="content col twelve_col last">
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<div class="col1">
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<h1 id="common-discrepancy-reports">Common Discrepancy Reports</h1>
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<h3 id="introduction">Introduction</h3>
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<p>The Discrepancy Report is an evaluation of a single or multiple ASN.1
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files, looking for suspicious annotation or annotation discrepancies
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that NCBI staff has noticed commonly occur in genome submissions, both
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complete and incomplete (WGS). A few of the problems that this
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function was written to find include inconsistent locus_tag prefixes,
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missing protei_id's, missing gene features, and suspect product
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names. </p>
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<p>This page shows common reports generated by tbl2asn, so has the older test names. The <a href="/genbank/new_asndisc_examples">newer test names</a> are generated by table2asn or the newest version of the command-line program asndisc.</p>
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<p>If you have questions about the Discrepancy Report, please contact us by email at <a href="mailto:genomes@ncbi.nlm.nih.gov">genomes@ncbi.nlm.nih.gov</a> prior to sending us your submission.</p>
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<p>For more information about annotation requirements, be sure to read the appropriate annotation guidelines:</p>
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<ul>
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<li><a href="/genbank/genomesubmit">Prokaryotic Genome Guidelines</a></li>
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<li><a href="/genbank/eukaryotic_genome_submission">Eukaryotic Genome Guidelines</a></li>
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</ul>
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<p>You may be interested to know that NCBI has a publicly available
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<a href="/genome/annotation_prok/">Prokaryotic Genomes Annotation Pipeline</a>.
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This pipeline generates files that are ready for submission to
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GenBank, although the submitter is welcome to edit them before
|
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submission to GenBank.</p>
|
|
|
|
|
|
<h3 id="common-discrepancy-report-catego">Common Discrepancy Report Categories</h3>
|
|
|
|
|
|
<pre><code>MISSING_GENES
|
|
- every CDS, rRNA, tRNA and ncRNA must have a gene feature with a locus\_tag. This report
|
|
may also occur if the gene is present, but the nucleotide spans do not completely
|
|
contain the corresponding feature.
|
|
|
|
EXTRA_GENES
|
|
- Looks for genes that do not have corresponding features. This may be OK if these
|
|
represent pseudogenes that are not translated. If this is the case, be sure to
|
|
include a brief note with the gene. For example "similar to protein X; may
|
|
contain a frameshift"
|
|
|
|
BAD_LOCUS\_TAG_FORMAT
|
|
- The correct format for a locus\_tag is prefix_uniqueID (i.e. ABC_0001). See
|
|
the [Prokaryotic Genome Annotation Guide for more about locus\_tag](/genbank/genomesubmit_annotation/#locus\_tag)
|
|
If you haven't already, register your project and a locus\_tag prefix
|
|
at <https://submit.ncbi.nlm.nih.gov/subs/bioproject/>.
|
|
|
|
MISSING_LOCUS\_TAGS
|
|
- every gene must have a locus\_tag
|
|
|
|
DUPLICATE_LOCUS\_TAGS
|
|
- every locus\_tag should be unique. The only exception is if a gene is split across a gap.
|
|
|
|
INCONSISTENT_LOCUS\_TAG_PREFIX
|
|
- All of the locus\_tags must have the same prefix, before the underscore. If you would
|
|
like to differentiate RNA genes or plasmid genes, you could add a letter after the
|
|
underscore (i.e ABC_r0001 or ABC_p0001). The only punctuation allowed in a locus\_tag
|
|
is the underscore.
|
|
|
|
DUPLICATE_GENE_LOCUS
|
|
- more than one gene includes the same biological gene name. This may be Ok if there
|
|
are multiple copies of the same gene in the genome
|
|
|
|
NON_GENE_LOCUS\_TAG
|
|
- locus\_tags should only be used on gene features
|
|
|
|
DISC_COUNT_NUCLEOTIDES
|
|
- counts the number of nucleotide sequences
|
|
|
|
MISSING_PROTEIN_ID
|
|
- every CDS feature (unless they are labeled as pseudo) must have a protein_id. The basic
|
|
format is:
|
|
protein_id gnl|dbname|OBB_0001
|
|
where dbname is an abbreviation for your lab or institute and OBB_0001 is a unique
|
|
identifier (usually the same as the locus\_tag)
|
|
|
|
INCONSISTENT_PROTEIN_ID
|
|
- all of the protein_ids should include the same dbname
|
|
|
|
FEATURE_LOCATION_CONFLICT
|
|
- the nucleotide location of the gene feature does not match the nucleotide location of
|
|
the corresponding rRNA, TRNA, tmRNA, or ncRNA
|
|
|
|
EC_NUMBER_NOTE
|
|
- EC numbers should be annotated as EC_number qualifiers on the CDS feature, not as notes
|
|
or product names. However an EC number may be included in a note if it refers to
|
|
another protein.
|
|
|
|
EC_NUMBER_ON_UNKNOWN_PROTEIN
|
|
- We do not expect to see the EC numbers on proteins named "hypothetical protein". If
|
|
there is enough information to add an EC number, please use a more informative
|
|
product name. Otherwise, remove the EC number.
|
|
|
|
PSEUDO_MISMATCH
|
|
- a feature includes a pseudo qualifier but the corresponding gene feature is not labeled.
|
|
The pseudo qualifier is required on the gene feature.
|
|
|
|
JOINED_FEATURES
|
|
- Joined features are not expected in prokaryotic submissions since introns are rare
|
|
in bacteria. This may be OK if the CDS includes an exception (e.g., ribosomal slippage).
|
|
Joined features are expected in eukaryotic submissions.
|
|
|
|
OVERLAPPING_CDS
|
|
- indicates that two CDS features overlap and have similar product names, suggesting
|
|
that they may represent a frameshifted gene that is annotated in two separate genes.
|
|
[Since ABC-type transporter genes often overlap, they are not reported.] If these
|
|
genes are not found biologically as two separate proteins, then they should be annotated
|
|
as a single gene with a /pseudo qualifier to indicate the gene is non-functional. The
|
|
product name would be entered in the gene_description and a brief note describing the
|
|
problem ("frameshift") added. For example:
|
|
1 200 gene
|
|
gene phoA
|
|
gene_desc alkaline phosphatase
|
|
locus\_tag OBB_0001
|
|
pseudo
|
|
note nonfunctional due to frameshift
|
|
|
|
If the situation is unclear and you want to keep the two genes in draft annotation, then
|
|
a note can be added to each CDS, "overlaps another CDS with the same product name", as a
|
|
flag to database users. This note can be added automatically when the .sqn files are made,
|
|
using the "-c b" argument of tbl2asn.
|
|
|
|
OVERLAPPING_GENES
|
|
- similar to OVERLAPPING_CDS. The nucleotide location of one gene overlaps an adjacent
|
|
gene. This may be OK or it may indicate a gene with a frameshift. If this is a
|
|
frameshifted gene, annotate one gene feature across the entire span, include a
|
|
pseudo qualifier, and include a brief note.
|
|
|
|
ADJACENT_PSEUDOGENES
|
|
- adjacent pseudogenes have the same gene name. This may indicate a frameshifted gene
|
|
that should be combined into a single gene feature. This can be ignored if there really
|
|
are two separate genes.
|
|
|
|
CONTAINED_CDS
|
|
- One CDS feature completely contains another CDS feature. This may be OK in a eukaryote
|
|
If there is a gene inside the intron of a longer gene. However, this is not expected
|
|
in a prokaryote. Often, this indicates short open reading frames that do not encode
|
|
REAL proteins were annotated as hypothetical proteins. Please remove any CDS features
|
|
that do not represent translated proteins.
|
|
|
|
RNA_CDS_OVERLAP and CDS_TRNA_OVERLAP
|
|
- similar to CONTAINED_CDS. A CDS feature overlaps an RNA feature. This is unusual
|
|
and may indicate a feature(s) needs to be removed.
|
|
|
|
SHORT_CONTIG and SHORT_SEQUENCES
|
|
- We prefer not to include contigs shorter than 200 nucleotides
|
|
|
|
INCONSISTENT_BIOSOURCE
|
|
- The organism information is not identical on all of the contigs.
|
|
|
|
PARTIAL_CDS_COMPLETE_SEQUENCE
|
|
- Every CDS feature in a prokaryotic sequence should be complete unless it abuts the
|
|
end of the sequence or a gap.
|
|
|
|
TAX_LOOKUP_MISSING and TAX_LOOKUP_MISMATCH
|
|
- Taxonomy errors can generally be ignored because they will be fixed during processing.
|
|
|
|
SUSPECT_PHRASES and DISC_SUSPICIOUS_NOTE_TEXT
|
|
- looks for phrases in a note that may indicate a problem. For example, 'fragment' may
|
|
indicate this should be a pseudogene. We also prefer not to include percent similarity
|
|
information because this information is time sensitive and may change as more data
|
|
is added/updated.
|
|
|
|
RNA_NO_PRODUCT
|
|
- every rRNA and tRNA should have a product name. If you do not know the product, then
|
|
use "Xxx" or "tRNA-Xxx". For example:
|
|
100 180 gene
|
|
locus\_tag ABC_xxxx
|
|
100 180 tRNA
|
|
product Xxx
|
|
|
|
DISC_PERCENT_N
|
|
- an unusually large number of ambiguous bases is present. This may indicate a low quality
|
|
sequence that should be trimmed or removed.
|
|
|
|
N_RUNS
|
|
- There should not be any gaps in the individual contigs in your submission. WGS projects
|
|
consist of only contigs (overlapping reads), not any supercontigs/scaffolds (assembled
|
|
contigs separated by gaps). If these are gaps, you will need to split the sequences at
|
|
the gaps and submit each contig as a separate record. We prefer not to include contigs
|
|
that are shorter than 200 nucleotides unless they are part of multi-component scaffolds.
|
|
If you have super-contig/assembly information, you can send it to us as an AGP file to
|
|
indicate how the pieces of the WGS submission are assembled together. We will use the AGP
|
|
file to create CON records of the scaffolds and/or chromosomes.
|
|
For more information about AGP files see: <https://www.ncbi.nlm.nih.gov/genbank/wgs.submit/#agp>
|
|
|
|
ZERO_BASECOUNT
|
|
- A sequence does not include a particular nucleotide; may indicate a low quality sequence;
|
|
could be OK if it's a short repetitive sequence.
|
|
|
|
NO_ANNOTATION
|
|
- Typos in table headers may lead to lost annotation. Check to be sure this is the expected
|
|
number of unannotated sequences.
|
|
|
|
DISC_SHORT_INTRON
|
|
- Detects introns shorter than 10bp, which are usually not biologically correct, but are
|
|
present to adjust for a frameshift in the sequence. If this is a frameshifted gene,
|
|
then the recommended approach is to annotate one gene feature across the entire span,
|
|
include a pseudo qualifier, and a brief note.
|
|
|
|
DISC_CDS_WITHOUT_MRNA
|
|
- In eukaryotic annotation, every CDS feature should have a corresponding mRNA feature.
|
|
However, mRNAs are not usually included in prokaryotic annotation.
|
|
|
|
DISC_FEATURE_COUNT
|
|
- counts the number of each feature type. Check to be sure this is correct
|
|
|
|
DISC_GENE_PARTIAL_CONFLICT
|
|
- if a CDS is partial, the corresponding gene feature should also be partial. [For
|
|
eukaryotes if there is no UTR information, then the mRNA and gene will agree with
|
|
the CDS but will be partial at both ends.]
|
|
|
|
DISC_BAD_GENE_STRAND
|
|
- a gene and its corresponding feature should be annotated on the same strand
|
|
|
|
SHOW_HYPOTHETICAL_CDS_HAVING_GENE_NAME
|
|
- If there is enough information to assign a gene name, then the CDS needs a
|
|
more informative product name than "hypothetical protein", so improve the
|
|
product name or remove the gene name, as appropriate.
|
|
|
|
TEST_OVERLAPPING_RRNAS
|
|
- rRNA features should not overlap
|
|
|
|
TEST_UNUSUAL_MISC_RNA
|
|
- misc_RNAs are unusual in a genome, consider using ncRNA, misc_binding, or misc_feature,
|
|
as appropriate.
|
|
|
|
DISC_QUALITY_SCORES
|
|
- if you have quality scores, please include them.
|
|
|
|
DISC_PARTIAL_PROBLEMS and DISC_BACTERIAL_PARTIAL_NONEXTENDABLE_PROBLEMS
|
|
- In a eukaryotic sequence, internal partial are expected to end at splice consensus sites.
|
|
However, internal partials should not be present in prokaryotic submissions. The
|
|
only partials expected in a prokaryotic sequence are those that abut the end of the
|
|
sequence or a gap. If an internal partial is within one or two bases of the end of
|
|
a sequence (or a gap) it should be extended to end of the sequence (use codon_start
|
|
to adjust the start codon if extending the 5' end). However, if extending the CDS
|
|
introduces internal stop codons, then annotate as a pseudogene or nonfunctional
|
|
gene with the /pseudo qualifier.
|
|
|
|
DISC_SUSPECT_RRNA_PRODUCTS and DISC_SHORT_RRNA
|
|
- Most often seen when rRNAs are annotated based on similarity to the 5' domain of 16S rRNA.
|
|
Please verify the all of the rRNA is annotated. If only part of the rRNA is present
|
|
because it extends off the end of a contig, the rRNA should be partial at the end of
|
|
the contig. Note that rRNAs should not be partial unless they are at the end of the
|
|
contig. If only a fragment of the rRNA is present, do not use an rRNA feature. Instead,
|
|
either delete the feature or annotate it as a misc_feature (without a gene or locus\_tag)
|
|
|
|
DISC_TRINOMIAL_SHOULD_HAVE_QUALIFIER
|
|
- When an organism name includes qualifiers (i.e strain, subspecies, serovar. forma), the
|
|
qualifier should be included in the source information. The easiest way is to include
|
|
this information in the fasta header. For example:
|
|
|
|
>ContigID [organism=Salmonella enterica subsp. enterica serovar Choleraesuis str. A50] [subspecies=enterica] [serovar=Chloeraesuis] [strain=A50]
|
|
|
|
DISC_SEGSETS_PRESENT
|
|
- When creating a submission in Sequin, segmented sequence is an outdated submission
|
|
format that is no longer accepted. Instead use the Batch option.
|
|
|
|
DISC_MISMATCHED_COMMENTS
|
|
- The information in the comments should be identical for all of the sequences in a
|
|
single submission.
|
|
|
|
DISC_BAD_BACTERIAL_GENE_NAME
|
|
- The standard format for a bacterial gene name is three lowercase letter followed by a
|
|
capital letter (e.g., abcD)
|
|
|
|
SHORT_PROT_SEQUENCES
|
|
- Protein sequences should be at least 50 amino acids, unless they are partial.
|
|
|
|
|
|
|
|
SUSPECT_PRODUCT_NAMES
|
|
|
|
Categories:
|
|
|
|
Remove organism from product name
|
|
Organelles not appropriate in prokaryote
|
|
Implies evolutionary relationship; change to -like protein (homolog, paralog, ortholog)
|
|
Suspicious phrase; should this be nonfunctional?
|
|
Consider adding 'protein' to the end of the product name (e.g., ends with domain, fold, motif)
|
|
May contain database identifier more appropriate in note; remove from product name
|
|
Use short product name instead of descriptive phrase
|
|
Possible parsing error or incorrect formatting; remove inappropriate symbols (punctuation symbols)
|
|
Correct the name or use 'hypothetical protein'
|
|
Typo (includes replace predicted, possible, probable, candidate with 'putative')
|
|
Use American spelling
|
|
Putative typo
|
|
Use 'protein' instead of 'gene' as appropriate
|
|
|
|
Details:
|
|
Typos
|
|
- list of commonly seen typos, eg 'proteine'. Fixed by -c f and -M arguments of tbl2asn
|
|
|
|
Use American spelling
|
|
- list of commonly seen words, e.g., 'sulfur' rather than 'sulphur'. Fixed by -c f and -M arguments of tbl2asn
|
|
|
|
Possible parsing error or incorrect formatting; remove inappropriate symbols
|
|
|
|
Organelles not appropriate in prokaryote
|
|
- Prokaryotic product name should not include organelle names (i.e. mitochondria,
|
|
golgi, chloroplast)
|
|
|
|
Suspicious phrase may indicate this is a pseudogene
|
|
- if you do not believe a CDS is translated into a functional protein, do not use
|
|
a CDS feature. Similarly, if a CDS feature contains a frameshift, do not
|
|
annotate the N-terminal fragment and the C-terminal fragment as separate features.
|
|
It would be better to use a single gene feature with pseudo qualifier and a
|
|
brief note.
|
|
- If a feature is partial, use the appropriate partial symbol. Do not include the
|
|
word partial in the product name.
|
|
|
|
May contain database identifier more appropriate in note; remove from product name
|
|
- locus\_tags, accession numbers, database identifiers, COG names, EC_number etc
|
|
should not be included in product names. Use the appropriate qualifier (e.g.,
|
|
EC_number, inference, db_xref) or use a note.
|
|
|
|
Implies evolutionary relationship; change to "xyz-like protein"
|
|
- Do not use homolog, paralog, or ortholog in a protein name as this infers an
|
|
evolutionary relationship that has generally not been determined. Instead of
|
|
"protein X homolog" use "protein X-like protein", "putative protein X", or
|
|
just "protein X" depending on how certain you are of the protein's identity.
|
|
|
|
Better as hypothetical protein
|
|
- While we prefer to have biological product names, if you don't have a better
|
|
name use "hypothetical protein". However, not EVERY product name in the genome
|
|
is allowed to be "hypothetical protein"
|
|
|
|
Domain name, descriptive phrase or truncated name; need concise product name
|
|
- Product names should be concise protein names, not descriptions or a domain
|
|
names. If a domain name is all you have (e.g., zinc finger) then use
|
|
`zinc finger domain-containing protein`. In addition, use protein names instead
|
|
of gene names (i.e. `ABC protein` *not* `ABC gene`).
|
|
|
|
Brackets or parenthesis `[] ()`
|
|
- Brackets or parenthesis may be OK if they are part of a protein name, e.g.,
|
|
`3-oxoacyl-(acyl-carrier-protein) reductase` and
|
|
`tRNA (5-methylaminomethyl-2-thiouridylate)-methyltransferase` are valid names.
|
|
However, synonyms or descriptive phrases should not be included in product
|
|
names. This information should be moved to a note.
|
|
</code></pre>
|
|
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<h2 id="genome-resources">Genome Resources</h2>
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<li><a href="/genbank/wgs/">About WGS</a></li>
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|
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|
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|
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|
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|
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<li><a href="/genbank/genome_validation">Validation Error Explanations for Genomes</a></li>
|
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<li><a href="/genbank/asndisc/">Discrepancy Report</a></li>
|
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<li><a href="https://www.ncbi.nlm.nih.gov/genome/annotation_prok/">NCBI Prokaryotic Genome Annotation Pipeline</a></li>
|
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<li><a href="https://www.ncbi.nlm.nih.gov/assembly/agp/AGP_Specification/">AGP Format</a></li>
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