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Introduction: KCTD15 encodes an oligomeric BTB domain protein reported to inhibit neural crest formation through repression of Wnt/beta-catenin signalling, as well as transactivation by TFAP2. Heterozygous missense variants in the closely related paralogue KCTD1 cause scalp-ear-nipple syndrome.

Methods: Exome sequencing was performed on a two-generation family affected by a distinctive phenotype comprising a lipomatous frontonasal malformation, anosmia, cutis aplasia of the scalp and/or sparse hair, and congenital heart disease. Identification of a de novo missense substitution within KCTD15 led to targeted sequencing of DNA from a similarly affected sporadic patient, revealing a different missense mutation. Structural and biophysical analyses were performed to assess the effects of both amino acid substitutions on the KCTD15 protein.

Results: A heterozygous c.310G>C variant encoding p.(Asp104His) within the BTB domain of KCTD15 was identified in an affected father and daughter and segregated with the phenotype. In the sporadically affected patient, a de novo heterozygous c.263G>A variant encoding p.(Gly88Asp) was present in KCTD15. Both substitutions were found to perturb the pentameric assembly of the BTB domain. A crystal structure of the BTB domain variant p.(Gly88Asp) revealed a closed hexameric assembly, whereas biophysical analyses showed that the p.(Asp104His) substitution resulted in a monomeric BTB domain likely to be partially unfolded at physiological temperatures.

Conclusion: BTB domain substitutions in KCTD1 and KCTD15 cause clinically overlapping phenotypes involving craniofacial abnormalities and cutis aplasia. The structural analyses demonstrate that missense substitutions act through a dominant negative mechanism by disrupting the higher order structure of the KCTD15 protein complex.

Competing Interests: Competing interests: None declared.

Titel:	BTB domain mutations perturbing KCTD15 oligomerisation cause a distinctive frontonasal dysplasia syndrome.
Autor/in / Beteiligte Person:	Miller, KA ; Cruz Walma, DA ; Pinkas, DM ; Tooze, RS ; Bufton, JC ; Richardson, W ; Manning, CE ; Hunt, AE ; Cros, J ; Hartill, V ; Parker, MJ ; McGowan, SJ ; Twigg, SRF ; Chalk, R ; Staunton, D ; Johnson, D ; Wilkie, AOM ; Bullock, AN
Zeitschrift:	Journal of medical genetics, Jg. 61 (2024-04-19), Heft 5, S. 490-501
Veröffentlichung:	London : British Medical Association, 2024
Medientyp:	academicJournal
ISSN:	1468-6244 (electronic)
DOI:	10.1136/jmg-2023-109531
Schlagwort:	Humans Abnormalities, Multiple Co-Repressor Proteins genetics Ectodermal Dysplasia Mutation, Missense genetics Syndrome BTB-POZ Domain Craniofacial Abnormalities genetics Face abnormalities
Sonstiges:	Nachgewiesen in: MEDLINE Sprachen: English Publication Type: Journal Article Language: English [J Med Genet] 2024 Apr 19; Vol. 61 (5), pp. 490-501. <i>Date of Electronic Publication: </i>2024 Apr 19. MeSH Terms: BTB-POZ Domain* ; Craniofacial Abnormalities* / genetics ; Face* / abnormalities ; Humans ; Abnormalities, Multiple ; Co-Repressor Proteins / genetics ; Ectodermal Dysplasia ; Mutation, Missense / genetics ; Syndrome References: J Mol Biol. 2016 Jan 16;428(1):92-107. (PMID: 26334369) ; Biophys J. 2000 Mar;78(3):1606-19. (PMID: 10692345) ; Acta Crystallogr D Biol Crystallogr. 2008 Jan;64(Pt 1):119-24. (PMID: 18094475) ; Plast Reconstr Surg. 2015 Jan;135(1):187-196. (PMID: 25285685) ; Proc Natl Acad Sci U S A. 2019 Apr 23;116(17):8370-8379. (PMID: 30971491) ; Nat Commun. 2023 Feb 15;14(1):853. (PMID: 36792598) ; Nature. 2019 Mar;567(7746):127-131. (PMID: 30814734) ; Biomolecules. 2021 Dec 10;11(12):. (PMID: 34944504) ; Nat Genet. 2021 Jan;53(1):45-53. (PMID: 33288918) ; Proc Natl Acad Sci U S A. 2013 Feb 19;110(8):2870-5. (PMID: 23382213) ; PLoS One. 2017 Dec 7;12(12):e0189162. (PMID: 29216270) ; Development. 2020 Dec 14;147(23):. (PMID: 33028614) ; J Invest Dermatol. 2015 Mar;135(3):666-672. (PMID: 25355129) ; Bioessays. 2013 Jul;35(7):586-96. (PMID: 23592240) ; Nature. 2020 May;581(7809):434-443. (PMID: 32461654) ; Nat Genet. 2018 Mar;50(3):414-423. (PMID: 29459680) ; J Mol Biol. 2009 Mar 20;387(1):175-91. (PMID: 19361449) ; FEBS Lett. 2016 Jun;590(11):1663-71. (PMID: 27152988) ; Sci Rep. 2021 Sep 14;11(1):18237. (PMID: 34521919) ; Sci Rep. 2019 Jul 19;9(1):10519. (PMID: 31324836) ; J Proteome Res. 2021 Sep 3;20(9):4318-4330. (PMID: 34342229) ; Int J Mol Sci. 2022 Nov 01;23(21):. (PMID: 36362127) ; Eur Biophys J. 2023 Jul;52(4-5):233-266. (PMID: 36792822) ; Diagnostics (Basel). 2022 Feb 25;12(3):. (PMID: 35328144) ; Mol Syndromol. 2016 Nov;7(6):312-321. (PMID: 27920634) ; Proc Natl Acad Sci U S A. 2022 Jan 4;119(1):. (PMID: 34934014) ; J Biol Chem. 2023 Mar;299(3):102924. (PMID: 36736897) ; Nat Genet. 2009 Jan;41(1):25-34. (PMID: 19079261) ; Clin Dysmorphol. 2021 Oct 1;30(4):167-172. (PMID: 34456244) ; Nat Protoc. 2007;2(9):2212-21. (PMID: 17853878) ; Nature. 2020 Apr;580(7803):402-408. (PMID: 32296183) ; Acta Crystallogr D Biol Crystallogr. 2004 Dec;60(Pt 12 Pt 1):2126-32. (PMID: 15572765) ; Acta Crystallogr D Struct Biol. 2019 Oct 1;75(Pt 10):861-877. (PMID: 31588918) ; Clin Genet. 2007 Jun;71(6):558-60. (PMID: 17539905) ; Cell Commun Signal. 2021 May 17;19(1):56. (PMID: 34001146) ; Biotechnol J. 2011 Jan;6(1):96-100. (PMID: 21053335) ; J Med Genet. 2017 Apr;54(4):260-268. (PMID: 27884935) ; Nat Rev Genet. 2023 Jul;24(7):442-463. (PMID: 36806206) ; Mol Med Rep. 2020 Nov;22(5):3895-3903. (PMID: 33000225) ; J Med Chem. 2019 Oct 10;62(19):8819-8830. (PMID: 31509708) ; Development. 2010 Sep;137(18):3013-8. (PMID: 20685732) ; Cell Genom. 2022 Aug 15;2(9):100168. (PMID: 36778668) ; Biochem J. 2017 Nov 1;474(22):3747-3761. (PMID: 28963344) ; J Appl Crystallogr. 2007 Aug 1;40(Pt 4):658-674. (PMID: 19461840) ; J Clin Invest. 2023 Dec 19;134(4):. (PMID: 38113115) ; Acta Crystallogr D Struct Biol. 2018 Feb 1;74(Pt 2):85-97. (PMID: 29533234) ; Am J Hum Genet. 2013 Apr 4;92(4):621-6. (PMID: 23541344) ; Nat Genet. 2009 Jan;41(1):18-24. (PMID: 19079260) ; Pediatr Radiol. 2006 Jul;36(7):647-62; quiz 726-7. (PMID: 16532348) Grant Information: United Kingdom WT_ Wellcome Trust; MC_PC_21044 United Kingdom MRC_ Medical Research Council; MC_PC_21047 United Kingdom MRC_ Medical Research Council Contributed Indexing: Keywords: Congenital, Hereditary, and Neonatal Diseases and Abnormalities; Exome Sequencing; Mutation, Missense; Structural Homology, Protein Substance Nomenclature: 0 (Co-Repressor Proteins) ; 0 (KCTD1 protein, human) SCR Disease Name: Frontonasal dysplasia Entry Date(s): Date Created: 20240131 Date Completed: 20240422 Latest Revision: 20240509 Update Code: 20240509 PubMed Central ID: PMC11041601

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BTB domain mutations perturbing KCTD15 oligomerisation cause a distinctive frontonasal dysplasia syndrome.