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dc.contributor.author Chang, Iksoo -
dc.contributor.author Park, Seong Jun -
dc.contributor.author Lee, Hye-Jin -
dc.contributor.author Kim, Inki -
dc.contributor.author Park, Sojung -
dc.contributor.author Ahn, Mi Kyoung -
dc.contributor.author Lee, Juhwan -
dc.contributor.author Kang, Moo Seok -
dc.contributor.author Baek, In-jeoung -
dc.contributor.author Sung, Young Hoon -
dc.contributor.author Pack, Chan-Gi -
dc.contributor.author Kang, Hyo-jeong -
dc.contributor.author Lee, Kunsong -
dc.contributor.author Im, Ho Joon -
dc.contributor.author Seo, Eul Ju -
dc.contributor.author Kim, Kyung Mo -
dc.contributor.author Yang, Suk-Kyun -
dc.contributor.author Song, Kyuyoung -
dc.contributor.author Oh, Seak Hee -
dc.date.accessioned 2021-10-19T08:00:02Z -
dc.date.available 2021-10-19T08:00:02Z -
dc.date.created 2021-10-14 -
dc.date.issued 2021-08 -
dc.identifier.issn 1876-4479 -
dc.identifier.uri http://hdl.handle.net/20.500.11750/15618 -
dc.description.abstract BACKGROUND AND AIMS: Mutations in XIAP can lead to the development of treatment-refractory severe paediatric Crohn's disease [CD], for which haematopoietic stem cell transplantation is the primary therapeutic option. The interpretation of variants of uncertain significance [VUSs] in XIAP needs to be scrutinized. METHODS: Targeted next-generation sequencing was performed for 33 male paediatric patients with refractory CD admitted at a tertiary referral hospital. To obtain functional data, biomolecular cell assays and supercomputing molecular dynamics simulations were performed. RESULTS: Nine unrelated male patients harboured hemizygous XIAP variants. Four known pathogenic variants and one novel pathogenic variant [p.Lys168Serfs*12] were identified in five patients, and two novel VUSs [p.Gly205del and p.Pro260Ser] and one known VUS [p.Glu350del] were identified in the remaining four. Among children with VUSs, only the subject with p.Gly205del exhibited defective NOD2 signalling. Using molecular dynamics simulation, we determined that the altered backbone torsional energy of C203 in XIAP of p.G205del was ~2 kcal/mol, suggesting loss of zinc binding in the mutant XIAP protein and poor coordination between the mutant XIAP and RIP2 proteins. Elevated auto-ubiquitination of zinc-depleted p.G205del XIAP protein resulted in XIAP protein deficiency. CONCLUSION: A high prevalence of XIAP deficiency was noted among children with refractory CD. Advanced functional studies decreased the subjectivity in the case-level interpretation of XIAP VUSs and directed consideration of haematopoietic stem cell transplantation. © The Author(s) 2021. Published by Oxford University Press on behalf of European Crohn’s and Colitis Organisation. All rights reserved. For permissions, please email: journals.permissions@oup.com. -
dc.language English -
dc.publisher Oxford University Press -
dc.title Interpretation of XIAP Variants of Uncertain Significance in Paediatric Patients with Refractory Crohn's Disease -
dc.type Article -
dc.identifier.doi 10.1093/ecco-jcc/jjab013 -
dc.identifier.wosid 000730897800007 -
dc.identifier.scopusid 2-s2.0-85113715461 -
dc.identifier.bibliographicCitation Journal of Crohn's and Colitis, v.15, no.8, pp.1291 - 1304 -
dc.description.isOpenAccess FALSE -
dc.subject.keywordAuthor XIAP -
dc.subject.keywordAuthor Crohn’s disease -
dc.subject.keywordAuthor molecular dynamics -
dc.subject.keywordAuthor variant of uncertain significance -
dc.subject.keywordPlus X-LINKED INHIBITOR -
dc.subject.keywordPlus INFLAMMATORY-BOWEL-DISEASE -
dc.subject.keywordPlus AMBER FORCE-FIELD -
dc.subject.keywordPlus SEQUENCE VARIANTS -
dc.subject.keywordPlus APOPTOSIS IAPS -
dc.subject.keywordPlus DEFICIENCY -
dc.subject.keywordPlus REFINEMENT -
dc.subject.keywordPlus MANAGEMENT -
dc.subject.keywordPlus GENETICS -
dc.subject.keywordPlus MUTATION -
dc.citation.endPage 1304 -
dc.citation.number 8 -
dc.citation.startPage 1291 -
dc.citation.title Journal of Crohn's and Colitis -
dc.citation.volume 15 -
dc.description.journalRegisteredClass scie -
dc.description.journalRegisteredClass scopus -
dc.relation.journalResearchArea Gastroenterology & Hepatology -
dc.relation.journalWebOfScienceCategory Gastroenterology & Hepatology -
dc.type.docType Article -
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Department of Brain Sciences Theoretical and Computational Biophysics Laboratory 1. Journal Articles

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