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UniProtKB/Swiss-Prot variant pages

UniProtKB/Swiss-Prot Q14004: Variant p.Asn842Ser

Cyclin-dependent kinase 13
Gene: CDK13
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Variant information Variant position: help 842 The position of the amino-acid change on the UniProtKB canonical protein sequence.
Type of variant: help LP/P [Disclaimer] The variants are classified into three categories: LP/P, LB/B and US.
  • LP/P: likely pathogenic or pathogenic.
  • LB/B: likely benign or benign.
  • US: uncertain significance

Residue change: help From Asparagine (N) to Serine (S) at position 842 (N842S, p.Asn842Ser). Indicates the amino acid change of the variant. The one-letter and three-letter codes for amino acids used in UniProtKB/Swiss-Prot are those adopted by the commission on Biochemical Nomenclature of the IUPAC-IUB.
Physico-chemical properties: help Change from medium size and polar (N) to small size and polar (S) The physico-chemical property of the reference and variant residues and the change implicated.
BLOSUM score: help 1 The score within a Blosum matrix for the corresponding wild-type to variant amino acid change. The log-odds score measures the logarithm for the ratio of the likelihood of two amino acids appearing by chance. The Blosum62 substitution matrix is used. This substitution matrix contains scores for all possible exchanges of one amino acid with another:
  • Lowest score: -4 (low probability of substitution).
  • Highest score: 11 (high probability of substitution).
More information can be found on the following page

Variant description: help In CHDFIDD. Any additional useful information about the variant.
Other resources: help Links to websites of interest for the variant.


Sequence information Variant position: help 842 The position of the amino-acid change on the UniProtKB canonical protein sequence.
Protein sequence length: help 1512 The length of the canonical sequence.
Location on the sequence: help MEGLDYCHKKNFLHRDIKCS N ILLNNRGQIKLADFGLARLY The residue change on the sequence. Unless the variant is located at the beginning or at the end of the protein sequence, both residues upstream (20) and downstream (20) of the variant will be shown.
Residue conservation: help The multiple alignment of the region surrounding the variant against various orthologous sequences.
Human                         MEGLDYCHKKNFLHRDIKCSNILLNNRGQIKLADFGLARLY

Mouse                         MEGLDYCHKKNFLHRDIKCSNILLNNRGQIKLADFGLARLY

Bovine                        MEGLDYCHKKNFLHRDIKCSNILLNNRGQIKLADFGLARLY

Sequence annotation in neighborhood: help The regions or sites of interest surrounding the variant. In general the features listed are posttranslational modifications, binding sites, enzyme active sites, local secondary structure or other characteristics reported in the cited references. The "Sequence annotation in neighborhood" lines have a fixed format:
  • Type: the type of sequence feature.
  • Positions: endpoints of the sequence feature.
  • Description: contains additional information about the feature.
TypePositionsDescription
Chain 1 – 1512 Cyclin-dependent kinase 13
Domain 705 – 998 Protein kinase
Active site 837 – 837 Proton acceptor
Helix 840 – 842



Literature citations
Distinct genetic architectures for syndromic and nonsyndromic congenital heart defects identified by exome sequencing.
Sifrim A.; Hitz M.P.; Wilsdon A.; Breckpot J.; Turki S.H.; Thienpont B.; McRae J.; Fitzgerald T.W.; Singh T.; Swaminathan G.J.; Prigmore E.; Rajan D.; Abdul-Khaliq H.; Banka S.; Bauer U.M.; Bentham J.; Berger F.; Bhattacharya S.; Bu'Lock F.; Canham N.; Colgiu I.G.; Cosgrove C.; Cox H.; Daehnert I.; Daly A.; Danesh J.; Fryer A.; Gewillig M.; Hobson E.; Hoff K.; Homfray T.; Kahlert A.K.; Ketley A.; Kramer H.H.; Lachlan K.; Lampe A.K.; Louw J.J.; Manickara A.K.; Manase D.; McCarthy K.P.; Metcalfe K.; Moore C.; Newbury-Ecob R.; Omer S.O.; Ouwehand W.H.; Park S.M.; Parker M.J.; Pickardt T.; Pollard M.O.; Robert L.; Roberts D.J.; Sambrook J.; Setchfield K.; Stiller B.; Thornborough C.; Toka O.; Watkins H.; Williams D.; Wright M.; Mital S.; Daubeney P.E.; Keavney B.; Goodship J.; Abu-Sulaiman R.M.; Klaassen S.; Wright C.F.; Firth H.V.; Barrett J.C.; Devriendt K.; FitzPatrick D.R.; Brook J.D.; Hurles M.E.;
Nat. Genet. 48:1060-1065(2016)
Cited for: INVOLVEMENT IN CHDFIDD; VARIANTS CHDFIDD ARG-714; ARG-717; GLN-751 AND SER-842; Phenotypic and molecular characterisation of CDK13-related congenital heart defects, dysmorphic facial features and intellectual developmental disorders.
Bostwick B.L.; McLean S.; Posey J.E.; Streff H.E.; Gripp K.W.; Blesson A.; Powell-Hamilton N.; Tusi J.; Stevenson D.A.; Farrelly E.; Hudgins L.; Yang Y.; Xia F.; Wang X.; Liu P.; Walkiewicz M.; McGuire M.; Grange D.K.; Andrews M.V.; Hummel M.; Madan-Khetarpal S.; Infante E.; Coban-Akdemir Z.; Miszalski-Jamka K.; Jefferies J.L.; Rosenfeld J.A.; Emrick L.; Nugent K.M.; Lupski J.R.; Belmont J.W.; Lee B.; Lalani S.R.;
Genome Med. 9:73-73(2017)
Cited for: VARIANTS CHDFIDD GLU-734; ASP-842 AND SER-842;
Disclaimer: Any medical or genetic information present in this entry is provided for research, educational and informational purposes only. They are not in any way intended to be used as a substitute for professional medical advice, diagnostic, treatment or care.