DSP missense variant in a Scottish Highland calf with congenital ichthyosis, alopecia, acantholysis of the tongue and corneal defects.
Cattle
Corneal ulcers
Dermatology
Genetic disorder
Genodermatosis
Hyperkeratosis
Precision medicine
Skin
Journal
BMC veterinary research
ISSN: 1746-6148
Titre abrégé: BMC Vet Res
Pays: England
ID NLM: 101249759
Informations de publication
Date de publication:
07 Jan 2022
07 Jan 2022
Historique:
received:
29
07
2021
accepted:
13
12
2021
entrez:
8
1
2022
pubmed:
9
1
2022
medline:
25
2
2022
Statut:
epublish
Résumé
Ichthyosis describes a localized or generalized hereditary cornification disorder caused by an impaired terminal keratinocyte differentiation resulting in excessive stratum corneum with the formation of more or less adherent scales. Ichthyosis affects humans and animals. Two rare bovine forms are reported, the severe harlequin ichthyosis and the less severe congenital ichthyosis, both characterized by a severe orthokeratotic lamellar hyperkeratosis. A 2-weeks-old purebred Scottish Highland calf was referred because of a syndrome resembling congenital ichthyosis. The clinical phenotype included diffuse alopecia and a markedly lichenified skin covered with large and excessive scales. Additionally, conjunctivitis and ulceration of the cornea were noted. Post-mortem examination revealed deep fissures in the diffusely thickened tongue and histopathological findings in the skin confirmed the clinical diagnosis. Whole-genome sequencing of the affected calf and comparison of the data with control genomes was performed. A search for private variants in known candidate genes for skin phenotypes including genes related with erosive and hyperkeratotic lesions revealed a single homozygous protein-changing variant, DSP: c.6893 C>A, or p.Ala2298Asp. The variant is predicted to change a highly conserved residue in the C-terminal plakin domain of the desmoplakin protein, which represents a main intracellular component of desmosomes, important intercellular adhesion molecules in various tissues including epidermis. Sanger sequencing confirmed the variant was homozygous in the affected calf and heterozygous in both parents. Further genotyping of 257 Scottish Highland animals from Switzerland revealed an estimated allele frequency of 1.2%. The mutant allele was absent in more than 4800 controls from various other cattle breeds. This study represents the first report of combined lesions compatible with congenital ichthyosis, alopecia, acantholysis of the tongue and corneal defects associated with a DSP missense variant as the most likely underlying cause. To the best of our knowledge, this study is also the first report of a DSP-related syndromic form of congenital ichthyosis in domestic animals. The results of our study enable genetic testing to avoid the unintentional occurrence of further affected cattle. The findings were added to the Online Mendelian Inheritance in Animals (OMIA) database (OMIA 002243-9913).
Sections du résumé
BACKGROUND
BACKGROUND
Ichthyosis describes a localized or generalized hereditary cornification disorder caused by an impaired terminal keratinocyte differentiation resulting in excessive stratum corneum with the formation of more or less adherent scales. Ichthyosis affects humans and animals. Two rare bovine forms are reported, the severe harlequin ichthyosis and the less severe congenital ichthyosis, both characterized by a severe orthokeratotic lamellar hyperkeratosis.
RESULTS
RESULTS
A 2-weeks-old purebred Scottish Highland calf was referred because of a syndrome resembling congenital ichthyosis. The clinical phenotype included diffuse alopecia and a markedly lichenified skin covered with large and excessive scales. Additionally, conjunctivitis and ulceration of the cornea were noted. Post-mortem examination revealed deep fissures in the diffusely thickened tongue and histopathological findings in the skin confirmed the clinical diagnosis. Whole-genome sequencing of the affected calf and comparison of the data with control genomes was performed. A search for private variants in known candidate genes for skin phenotypes including genes related with erosive and hyperkeratotic lesions revealed a single homozygous protein-changing variant, DSP: c.6893 C>A, or p.Ala2298Asp. The variant is predicted to change a highly conserved residue in the C-terminal plakin domain of the desmoplakin protein, which represents a main intracellular component of desmosomes, important intercellular adhesion molecules in various tissues including epidermis. Sanger sequencing confirmed the variant was homozygous in the affected calf and heterozygous in both parents. Further genotyping of 257 Scottish Highland animals from Switzerland revealed an estimated allele frequency of 1.2%. The mutant allele was absent in more than 4800 controls from various other cattle breeds.
CONCLUSIONS
CONCLUSIONS
This study represents the first report of combined lesions compatible with congenital ichthyosis, alopecia, acantholysis of the tongue and corneal defects associated with a DSP missense variant as the most likely underlying cause. To the best of our knowledge, this study is also the first report of a DSP-related syndromic form of congenital ichthyosis in domestic animals. The results of our study enable genetic testing to avoid the unintentional occurrence of further affected cattle. The findings were added to the Online Mendelian Inheritance in Animals (OMIA) database (OMIA 002243-9913).
Identifiants
pubmed: 34996433
doi: 10.1186/s12917-021-03113-3
pii: 10.1186/s12917-021-03113-3
pmc: PMC8739657
doi:
Substances chimiques
Desmoplakins
0
Types de publication
Case Reports
Journal Article
Langues
eng
Sous-ensembles de citation
IM
Pagination
20Subventions
Organisme : Schweizerischer Nationalfonds zur Förderung der Wissenschaftlichen Forschung
ID : 31003A_172911
Organisme : Schweizerischer Nationalfonds zur Förderung der Wissenschaftlichen Forschung
ID : 31003A_172911
Informations de copyright
© 2022. The Author(s).
Références
Anim Genet. 2020 Oct;51(5):837-838
pubmed: 32567073
J Med Genet. 2016 May;53(5):289-95
pubmed: 26399581
Animals (Basel). 2020 Oct 30;10(11):
pubmed: 33143196
Annu Rev Anim Biosci. 2019 Feb 15;7:89-102
pubmed: 30508490
J Vet Intern Med. 2020 Nov;34(6):2800-2807
pubmed: 33135329
F1000Res. 2016 Jun 24;5:
pubmed: 27408699
Nat Genet. 2008 Apr;40(4):449-54
pubmed: 18344998
BMC Genet. 2020 May 24;21(1):55
pubmed: 32448141
J Am Acad Dermatol. 2010 Oct;63(4):607-41
pubmed: 20643494
Acta Derm Venereol. 2020 Mar 25;100(7):adv00096
pubmed: 32147747
J Vet Med Sci. 2007 May;69(5):553-5
pubmed: 17551233
J Invest Dermatol. 2002 Feb;118(2):232-8
pubmed: 11841538
Am J Hum Genet. 2005 Oct;77(4):653-60
pubmed: 16175511
Nature. 2020 May;581(7809):434-443
pubmed: 32461654
Bioinformatics. 2015 Aug 15;31(16):2745-7
pubmed: 25851949
Sci Rep. 2017 Sep 13;7(1):11466
pubmed: 28904385
Vet Rec. 2001 Nov 3;149(18):563
pubmed: 11720213
Am J Clin Dermatol. 2018 Feb;19(1):51-66
pubmed: 28815464
J Invest Dermatol. 2010 Apr;130(4):968-78
pubmed: 19924139
Fly (Austin). 2012 Apr-Jun;6(2):80-92
pubmed: 22728672
Br Vet J. 1985 Jan-Feb;141(1):1-8
pubmed: 3995245
Exp Eye Res. 2020 Nov;200:108206
pubmed: 32882212
Anim Genet. 2019 Dec;50(6):749-752
pubmed: 31568573
Vet Rec. 2006 Mar 25;158(12):412-4
pubmed: 16565341
Acta Derm Venereol. 2015 Mar;95(3):337-40
pubmed: 25227139
BMC Vet Res. 2015 Mar 04;11:48
pubmed: 25890340
Gigascience. 2020 Mar 1;9(3):
pubmed: 32191811
Dtsch Tierarztl Wochenschr. 2006 Sep;113(9):351-4
pubmed: 17009813
Clin Dermatol. 2016 Mar-Apr;34(2):242-75
pubmed: 26903188
Mol Genet Genomics. 2021 Nov;296(6):1313-1322
pubmed: 34599683