Primary HBB gene mutation severity and long-term outcomes in a global cohort of β-thalassaemia

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dc.contributor.authorMusallam, Khaled M.
dc.contributor.authorVitrano, Angela
dc.contributor.authorMeloni, Antonella
dc.contributor.authorPollina Addario, Walter Sebastiano
dc.contributor.authorDi Marco, Vito
dc.contributor.authorAnsari, Saqib Hussain
dc.contributor.authorFilosa, Aldo
dc.contributor.authorRicchi, Paolo
dc.contributor.authorCeci, Adriana
dc.contributor.authorDaar, Shahina F.
dc.contributor.authorVlachaki, Euthymia
dc.contributor.authorSinger, Sylvia Titi
dc.contributor.authorNaserullah, Zaki A.
dc.contributor.authorPepe, Alessia
dc.contributor.authorScondotto, Salvatore Re
dc.contributor.authorDardanoni, Gabriella
dc.contributor.authorKarimi, Mehran A.
dc.contributor.authorEl-Beshlawy, Amal M.
dc.contributor.authorHajipour, Mahmoud
dc.contributor.authorBonifazi, Fedele
dc.contributor.authorVichinsky, Elliott P.
dc.contributor.authorTaher, Ali T.
dc.contributor.authorSankaran, Vijay G.
dc.contributor.authorMaggio, Aurelio M.
dc.contributor.departmentInternal Medicine
dc.contributor.facultyFaculty of Medicine (FM)
dc.contributor.institutionAmerican University of Beirut
dc.date.accessioned2025-01-24T11:44:24Z
dc.date.available2025-01-24T11:44:24Z
dc.date.issued2022
dc.description.abstractIn β-thalassaemia, the severity of inherited β-globin gene mutations determines the severity of the clinical phenotype at presentation and subsequent transfusion requirements. However, data on associated long-term outcomes remain limited. We analysed data from 2109 β-thalassaemia patients with available genotypes in a global database. Genotype severity was grouped as β0/β0, β0/β+, β+/β+, β0/β++, β+/β++, and β++/β++. Patients were followed from birth until death or loss to follow-up. The median follow-up time was 34·1 years. Mortality and multiple morbidity outcomes were analyzed through five different stratification models of genotype severity groups. Interestingly, β0 and β+ mutations showed similar risk profiles. Upon adjustment for demographics and receipt of conventional therapy, patients with β0/β0, β0/β+, or β+/β+ had a 2·104-increased risk of death [95% confidence interval (CI): 1·176–3·763, P = 0·011] and 2·956-increased odds of multiple morbidity (95% CI: 2·310–3·784, P < 0·001) compared to patients in lower genotype severity groups. Cumulative survival estimates by age 65 years were 36·8% for this subgroup compared with 90·2% for patients in lower genotype severity groups (P < 0·001). Our study identified mortality and morbidity risk estimates across various genotype severity groups in patients with β-thalassaemia and suggests inclusion of both β+ and β0 mutations in strata of greatest severity. © 2021 British Society for Haematology and John Wiley & Sons Ltd
dc.identifier.doihttps://doi.org/10.1111/bjh.17897
dc.identifier.eid2-s2.0-85117957604
dc.identifier.pmid34697800
dc.identifier.urihttp://hdl.handle.net/10938/30443
dc.language.isoen
dc.publisherJohn Wiley and Sons Inc
dc.relation.ispartofBritish Journal of Haematology
dc.sourceScopus
dc.subjectAdult
dc.subjectAlleles
dc.subjectBeta-globins
dc.subjectBeta-thalassemia
dc.subjectCohort studies
dc.subjectDisease management
dc.subjectFemale
dc.subjectFollow-up studies
dc.subjectGenotype
dc.subjectGlobal health
dc.subjectHumans
dc.subjectKaplan-meier estimate
dc.subjectMale
dc.subjectMorbidity
dc.subjectMortality
dc.subjectMutation
dc.subjectOdds ratio
dc.subjectPhenotype
dc.subjectPopulation surveillance
dc.subjectPrognosis
dc.subjectProportional hazards models
dc.subjectSeverity of illness index
dc.subjectYoung adult
dc.subjectHemoglobin beta chain
dc.subjectAllele
dc.subjectBeta thalassemia
dc.subjectBlood
dc.subjectCohort analysis
dc.subjectFollow up
dc.subjectGenetics
dc.subjectHealth survey
dc.subjectHuman
dc.subjectKaplan meier method
dc.subjectProportional hazards model
dc.titlePrimary HBB gene mutation severity and long-term outcomes in a global cohort of β-thalassaemia
dc.typeArticle

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