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dc.contributor.authorMartín-Nalda, A.
dc.contributor.authorFortuny, C.
dc.contributor.authorRey Cordo, Carmen Lourdes 
dc.contributor.authorBunney, T. D.
dc.contributor.authorAlsina, L.
dc.contributor.authorEsteve-Solé, A.
dc.contributor.authorBull, D.
dc.contributor.authorAnton, M. C.
dc.contributor.authorBasagaña, M.
dc.contributor.authorCasals, F.
dc.contributor.authorDeyá, A.
dc.contributor.authorGarcía-Prat, M.
dc.contributor.authorGimeno, R.
dc.contributor.authorJuan, M.
dc.contributor.authorMartinez-Banaclocha, H.
dc.contributor.authorMartinez-Garcia, J. J.
dc.contributor.authorMensa-Vilaró, A.
dc.contributor.authorRabionet, R.
dc.contributor.authorMartin-Begue, N.
dc.contributor.authorRudilla, F.
dc.contributor.authorYagüe, J.
dc.contributor.authorEstivill, X.
dc.contributor.authorGarcía-Patos, V.
dc.contributor.authorPujol, R. M.
dc.contributor.authorSoler-Palacín, P.
dc.contributor.authorKatan, M.
dc.contributor.authorPelegrín, P.
dc.contributor.authorColobran, R.
dc.contributor.authorVicente, A.
dc.contributor.authorArostegui, J. I.
dc.date.accessioned2022-05-19T08:34:20Z
dc.date.available2022-05-19T08:34:20Z
dc.date.issued2020
dc.identifier.issn0271-9142
dc.identifier.otherhttps://www.ncbi.nlm.nih.gov/pubmed/32671674es
dc.identifier.urihttp://hdl.handle.net/20.500.11940/16751
dc.description.abstractAutoinflammatory diseases (AIDs) were first described as clinical disorders characterized by recurrent episodes of seemingly unprovoked sterile inflammation. In the past few years, the identification of novel AIDs expanded their phenotypes toward more complex clinical pictures associating vasculopathy, autoimmunity, or immunodeficiency. Herein, we describe two unrelated patients suffering since the neonatal period from a complex disease mainly characterized by severe sterile inflammation, recurrent bacterial infections, and marked humoral immunodeficiency. Whole-exome sequencing detected a novel, de novo heterozygous PLCG2 variant in each patient (p.Ala708Pro and p.Leu845_Leu848del). A clear enhanced PLCgamma2 activity for both variants was demonstrated by both ex vivo calcium responses of the patient's B cells to IgM stimulation and in vitro assessment of PLC activity. These data supported the autoinflammation and PLCgamma2-associated antibody deficiency and immune dysregulation (APLAID) diagnosis in both patients. Immunological evaluation revealed a severe decrease of immunoglobulins and B cells, especially class-switched memory B cells, with normal T and NK cell counts. Analysis of bone marrow of one patient revealed a reduced immature B cell fraction compared with controls. Additional investigations showed that both PLCG2 variants activate the NLRP3-inflammasome through the alternative pathway instead of the canonical pathway. Collectively, the evidences here shown expand APLAID diversity toward more severe phenotypes than previously reported including dominantly inherited agammaglobulinemia, add novel data about its genetic basis, and implicate the alternative NLRP3-inflammasome activation pathway in the basis of sterile inflammation.en
dc.rightsAtribución 4.0 Internacional
dc.rights.urihttp://creativecommons.org/licenses/by/4.0/
dc.subject.meshCytokines*
dc.subject.meshInflammasomes*
dc.subject.meshPhospholipase C gamma*
dc.subject.meshAdolescent*
dc.subject.meshPedigree*
dc.subject.meshPhenotype*
dc.subject.meshGenetic Predisposition to Disease*
dc.subject.meshAutoimmunity*
dc.subject.meshDNA Mutational Analysis*
dc.subject.meshHumans*
dc.subject.meshGenetic Association Studies*
dc.subject.meshAgammaglobulinemia*
dc.subject.meshStructure-Activity Relationship*
dc.subject.meshCaspase 1*
dc.subject.meshHereditary Autoinflammatory Diseases*
dc.titleSevere Autoinflammatory Manifestations and Antibody Deficiency Due to Novel Hypermorphic PLCG2 Mutationsen
dc.typeJournal Articlees
dc.authorsophosMartín-Nalda, A.;Fortuny, C.;Rey, L.;Bunney, T. D.;Alsina, L.;Esteve-Solé, A.;Bull, D.;Anton, M. C.;Basagaña, M.;Casals, F.;Deyá, A.;García-Prat, M.;Gimeno, R.;Juan, M.;Martinez-Banaclocha, H.;Martinez-Garcia, J. J.;Mensa-Vilaró, A.;Rabionet, R.;Martin-Begue, N.;Rudilla, F.;Yagüe, J.;Estivill, X.;García-Patos, V.;Pujol, R. M.;Soler-Palacín, P.;Katan, M.;Pelegrín, P.;Colobran, R.;Vicente, A.;Arostegui, J. I.
dc.identifier.doi10.1007/s10875-020-00794-7
dc.identifier.pmid32671674
dc.identifier.sophos40642
dc.issue.number7es
dc.journal.titleJOURNAL OF CLINICAL IMMUNOLOGYes
dc.organizationServizo Galego de Saúde::Estrutura de Xestión Integrada (EOXI)::EOXI de Vigo - Complexo Hospitalario Universitario de Vigo::Pediatríaes
dc.page.initial987es
dc.page.final1000es
dc.rights.accessRightsopenAccess
dc.subject.decsfenotipo*
dc.subject.decsanálisis de mutaciones del ADN*
dc.subject.decscitocinas*
dc.subject.decscaspasa 1*
dc.subject.decspredisposición genética a la enfermedad*
dc.subject.decsagammaglobulinemia*
dc.subject.decsestudios de asociación genética*
dc.subject.decsautoinmunidad*
dc.subject.decsfosfolipasa C gamma*
dc.subject.decshumanos*
dc.subject.decsrelación estructura-actividad*
dc.subject.decslinaje*
dc.subject.decsenfermedades autoinflamatorias hereditarias*
dc.subject.decsinflamasomas*
dc.subject.decsadolescente*
dc.subject.keywordCHUVIes
dc.typefidesArtículo Originales
dc.typesophosArtículo Originales
dc.volume.number40es


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Atribución 4.0 Internacional
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