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dc.contributor.authorHussein, D.
dc.contributor.authorDallol, A.
dc.contributor.authorQuintas, R.
dc.contributor.authorSchulten, H.-J.
dc.contributor.authorAlomari, M.
dc.contributor.authorBaeesa, S.
dc.contributor.authorBangash, M.
dc.contributor.authorAlghamdi, F.
dc.contributor.authorKhan, I.
dc.contributor.authorElAssouli, M.-Z.M.
dc.contributor.authorSaka, M.
dc.contributor.authorCarracedo Álvarez, Ángel
dc.contributor.authorChaudhary, A.
dc.contributor.authorAbuzenadah, A.
dc.date.accessioned2022-05-23T08:37:30Z
dc.date.available2022-05-23T08:37:30Z
dc.date.issued2020
dc.identifier.issn2405-8440
dc.identifier.otherhttps://www.ncbi.nlm.nih.gov/pubmed/33305042es
dc.identifier.urihttp://hdl.handle.net/20.500.11940/16791
dc.description.abstractObjective: Bulk tissue genomic analysis of meningiomas identified common somatic mutations, however, it often excluded blood-related variants. In contrast, genomic characterisation of primary cell lines that can provide critical information regarding growth and proliferation, have been rare. In our work, we identified the variants that are present in the blood, tissues and corresponding cell lines that are likely to be predictive, tumorigenic and progressive. Method: Whole-exome sequencing was used to identify variants and distinguish related pathways that exist in 42 blood, tissues and corresponding cell lines (BTCs) samples for patients with intracranial meningiomas. Conventional sequencing was used for the confirmation of variants. Integrative analysis of the gene expression for the corresponding samples was utilised for further interpretations. Results: In total, 926 BTC variants were detected, implicating 845 genes. A pathway analysis of all BTC genes with damaging variants indicated the 'cell morphogenesis involved in differentiation' stem cell-related pathway to be the most frequently affected pathway. Concordantly, five stem cell-related genes, GPRIN2, ALDH3B2, ASPN, THSD7A and SIGLEC6, showed BTC variants in at least five of the patients. Variants that were heterozygous in the blood and homozygous in the tissues or the corresponding cell lines were rare (average: 1.3 +/- 0.3%), and included variants in the RUNX2 and CCDC114 genes. An analysis comparing the variants detected only in tumours with aggressive features indicated a total of 240 BTC genes, implicating the 'homophilic cell adhesion via plasma membrane adhesion molecules' pathway, and identifying the stem cell-related transcription coactivator NCOA3/AIB1/SRC3 as the most frequent BTC gene. Further analysis of the possible impact of the poly-Q mutation present in the NCOA3 gene indicated associated deregulation of 15 genes, including the up-regulation of the stem cell related SEMA3D gene and the angiogenesis related VEGFA gene. Conclusion: Stem cell-related pathways and genes showed high prevalence in the BTC variants, and novel variants in stem cell-related genes were identified for meningioma. These variants can potentially be used as predictive, tumorigenic and progressive biomarkers for meningioma.en
dc.rightsAttribution-NonCommercial-NoDerivatives 4.0 International
dc.rights.urihttps://creativecommons.org/licenses/by-nc-nd/4.0/
dc.subject.meshMeningioma*
dc.subject.meshMolecular Biology*
dc.subject.meshGenetics*
dc.subject.meshCell Biology*
dc.subject.meshBiochemistry*
dc.titleOverlapping variants in the blood, tissues and cell lines for patients with intracranial meningiomas are predominant in stem cell-related genesen
dc.typeJournal Articlees
dc.authorsophosHussein, D.;Dallol, A.;Quintas, R.;Schulten, H.-J.;Alomari, M.;Baeesa, S.;Bangash, M.;Alghamdi, F.;Khan, I.;ElAssouli, M.-Z.M.;Saka, M.;Carracedo, A.;Chaudhary, A.;Abuzenadah, A.
dc.identifier.doi10.1016/j.heliyon.2020.e05632
dc.identifier.pmid33305042
dc.identifier.sophos42877
dc.issue.number11es
dc.journal.titleHeliyones
dc.organizationServizo Galego de Saúde::Dirección Xeral de Asistencia Sanitaria::Fundación Pública Galega de Medicina Xenómicaes
dc.rights.accessRightsopenAccess
dc.subject.decsbioquímica*
dc.subject.decsmeningioma*
dc.subject.decsbiología celular*
dc.subject.decsbiología molecular*
dc.subject.decsgenética*
dc.subject.keywordFPGMXes
dc.typefidesArtículo Originales
dc.typesophosArtículo Originales
dc.volume.number6es


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