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dc.contributor.authorBodo, S.
dc.contributor.authorColas, C.
dc.contributor.authorBuhard, O.
dc.contributor.authorCollura, A.
dc.contributor.authorTinat, J.
dc.contributor.authorLavoine, N.
dc.contributor.authorGuilloux, A.
dc.contributor.authorChalastanis, A.
dc.contributor.authorLafitte, P.
dc.contributor.authorCoulet, F.
dc.contributor.authorBuisine, M. P.
dc.contributor.authorIlencikova, D.
dc.contributor.authorRuiz Ponte, Clara
dc.contributor.authorKinzel, M.
dc.contributor.authorGrandjouan, S.
dc.contributor.authorBrems, H.
dc.contributor.authorLejeune, S.
dc.contributor.authorBlanché, H.
dc.contributor.authorWang, Q.
dc.contributor.authorCaron, O.
dc.contributor.authorCabaret, O.
dc.contributor.authorSvrcek, M.
dc.contributor.authorVidaud, D.
dc.contributor.authorParfait, B.
dc.contributor.authorVerloes, A.
dc.contributor.authorKnappe, U. J.
dc.contributor.authorSoubrier, F.
dc.contributor.authorMortemousque, I.
dc.contributor.authorLeis, A.
dc.contributor.authorAuclair-Perrossier, J.
dc.contributor.authorFrébourg, T.
dc.contributor.authorFléjou, J. F.
dc.contributor.authorEntz-Werle, N.
dc.contributor.authorLeclerc, J.
dc.contributor.authorMalka, D.
dc.contributor.authorCohen-Haguenauer, O.
dc.contributor.authorGoldberg, Y.
dc.contributor.authorGerdes, A. M.
dc.contributor.authorFedhila, F.
dc.contributor.authorMathieu-Dramard, M.
dc.contributor.authorHamelin, R.
dc.contributor.authorWafaa, B.
dc.contributor.authorGauthier-Villars, M.
dc.contributor.authorBourdeaut, F.
dc.contributor.authorSheridan, E.
dc.contributor.authorVasen, H.
dc.contributor.authorBrugières, L.
dc.contributor.authorWimmer, K.
dc.contributor.authorMuleris, M.
dc.contributor.authorDuval, A.
dc.date.accessioned2017-06-07T07:34:42Z
dc.date.available2017-06-07T07:34:42Z
dc.date.issued2015
dc.identifier.issn0016-5085
dc.identifier.urihttp://hdl.handle.net/20.500.11940/8152
dc.description.abstractBACKGROUND & AIMS: Patients with bi-allelic germline mutations in mismatch repair (MMR) genes (MLH1, MSH2, MSH6, or PMS2) develop a rare but severe variant of Lynch syndrome called constitutional MMR deficiency (CMMRD). This syndrome is characterized by early-onset colorectal cancers, lymphomas or leukemias, and brain tumors. There is no satisfactory method for diagnosis of CMMRD because screens for mutations in MMR genes are noninformative for 30% of patients. MMR-deficient cancer cells are resistant to genotoxic agents and have microsatellite instability (MSI), due to accumulation of errors in repetitive DNA sequences. We investigated whether these features could be used to identify patients with CMMRD. METHODS: We examined MSI by PCR analysis and tolerance to methylating or thiopurine agents (functional characteristics of MMR-deficient tumor cells) in lymphoblastoid cells (LCs) from 3 patients with CMMRD and 5 individuals with MMR-proficient LCs (controls). Using these assays, we defined experimental parameters that allowed discrimination of a series of 14 patients with CMMRD from 52 controls (training set). We then used the same parameters to assess 23 patients with clinical but not genetic features of CMMRD. RESULTS: In the training set, we identified parameters, based on MSI and LC tolerance to methylation, that detected patients with CMMRD vs controls with 100% sensitivity and 100% specificity. Among 23 patients suspected of having CMMRD, 6 had MSI and LC tolerance to methylation (CMMRD highly probable), 15 had neither MSI nor LC tolerance to methylation (unlikely to have CMMRD), and 2 were considered doubtful for CMMRD based on having only 1 of the 2 features. CONCLUSION: The presence of MSI and tolerance to methylation in LCs identified patients with CMMRD with 100% sensitivity and specificity. These features could be used in diagnosis of patients.
dc.language.isoeng
dc.subject.meshAdaptor Proteins, Signal Transducing
dc.subject.meshAdenosine Triphosphatases
dc.subject.meshAdult
dc.subject.meshAntineoplastic Agents, Alkylating
dc.subject.meshBiomarkers, Tumor
dc.subject.meshBrain Neoplasms
dc.subject.meshCaco-2 Cells
dc.subject.meshCase-Control Studies
dc.subject.meshColorectal Neoplasms
dc.subject.meshColorectal Neoplasms, Hereditary Nonpolyposis
dc.subject.meshDNA Mutational Analysis
dc.subject.meshDNA Repair Enzymes
dc.subject.meshDNA-Binding Proteins
dc.subject.meshDrug Resistance, Neoplasm
dc.subject.meshFemale
dc.subject.meshGenetic Predisposition to Disease
dc.subject.meshGenetic Testing
dc.subject.meshGerm-Line Mutation
dc.subject.meshHCT116 Cells
dc.subject.meshHeredity
dc.subject.meshHumans
dc.subject.meshLymphocytes
dc.subject.meshMale
dc.subject.meshMethylation
dc.subject.meshMicrosatellite Instability
dc.subject.meshMismatch Repair Endonuclease PMS2
dc.subject.meshMultiplex Polymerase Chain Reaction
dc.subject.meshMutL Protein Homolog 1
dc.subject.meshMutS Homolog 2 Protein
dc.subject.meshNeoplastic Syndromes, Hereditary
dc.subject.meshNuclear Proteins
dc.subject.meshPhenotype
dc.subject.meshPredictive Value of Tests
dc.subject.meshReproducibility of Results
dc.subject.meshTransfection
dc.subject.meshYoung Adult
dc.subject.meshColon Cancer
dc.subject.meshFunctional Tests
dc.subject.meshPredisposition
dc.subject.meshTumor
dc.titleDiagnosis of Constitutional Mismatch Repair-Deficiency Syndrome Based on Microsatellite Instability and Lymphocyte Tolerance to Methylating Agents
dc.typeArtigoes
dc.authorsophosBodo, S.
dc.authorsophosColas, C.
dc.authorsophosBuhard, O.
dc.authorsophosCollura, A.
dc.authorsophosTinat, J.
dc.authorsophosLavoine, N.
dc.authorsophosGuilloux, A.
dc.authorsophosChalastanis, A.
dc.authorsophosLafitte, P.
dc.authorsophosCoulet, F.
dc.authorsophosBuisine, M. P.
dc.authorsophosIlencikova, D.
dc.authorsophosRuiz-Ponte, C.
dc.authorsophosKinzel, M.
dc.authorsophosGrandjouan, S.
dc.authorsophosBrems, H.
dc.authorsophosLejeune, S.
dc.authorsophosBlanché, H.
dc.authorsophosWang, Q.
dc.authorsophosCaron, O.
dc.authorsophosCabaret, O.
dc.authorsophosSvrcek, M.
dc.authorsophosVidaud, D.
dc.authorsophosParfait, B.
dc.authorsophosVerloes, A.
dc.authorsophosKnappe, U. J.
dc.authorsophosSoubrier, F.
dc.authorsophosMortemousque, I.
dc.authorsophosLeis, A.
dc.authorsophosAuclair-Perrossier, J.
dc.authorsophosFrébourg, T.
dc.authorsophosFléjou, J. F.
dc.authorsophosEntz-Werle, N.
dc.authorsophosLeclerc, J.
dc.authorsophosMalka, D.
dc.authorsophosCohen-Haguenauer, O.
dc.authorsophosGoldberg, Y.
dc.authorsophosGerdes, A. M.
dc.authorsophosFedhila, F.
dc.authorsophosMathieu-Dramard, M.
dc.authorsophosHamelin, R.
dc.authorsophosWafaa, B.
dc.authorsophosGauthier-Villars, M.
dc.authorsophosBourdeaut, F.
dc.authorsophosSheridan, E.
dc.authorsophosVasen, H.
dc.authorsophosBrugières, L.
dc.authorsophosWimmer, K.
dc.authorsophosMuleris, M.
dc.authorsophosDuval, A.
dc.identifier.doi10.1053/j.gastro.2015.06.013
dc.identifier.isi361976900037
dc.identifier.pmid26116798
dc.identifier.sophos19495
dc.issue.number4
dc.journal.titleGastroenterology
dc.organizationConsellería de Sanidade::Fundación pública Galega de Medicina Xenómica
dc.organizationServizo Galego de Saúde::Estrutura de Xestión Integrada (EOXI)::EOXI de Santiago::IDIS.- Instituto de investigaciones sanitarias de Santiago
dc.page.initial1017
dc.page.final1029
dc.rights.accessRightsopenAccess
dc.typesophosArtículo Original
dc.volume.number149


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