Please use this identifier to cite or link to this item: http://hdl.handle.net/10553/106862
Title: Cystathionine β-synthase deficiency in the E-HOD registry-part I: pyridoxine responsiveness as a determinant of biochemical and clinical phenotype at diagnosis
Authors: Kožich, Viktor
Sokolová, Jitka
Morris, Andrew A. M.
Pavlíková, Markéta
Gleich, Florian
Kölker, Stefan
Krijt, Jakub
Dionisi‐Vici, Carlo
Baumgartner, Matthias R.
Blom, Henk J.
Huemer, Martina
Aldámiz‐Echevarría, Luis
Arantes, Rodrigo Rezende
Arrieta, Francisco
Blasco‐Alonso, Javier
Brouwers, Martijn
Brunner‐Krainz, Michaela
Bueno, María
Peláez, Rosa Burgos
Cano, Aline
Couce, María‐Luz
Crushell, Ellen
Ficicioglu, Can
Forny, Patrick
García Jiménez, María Concepción
Gaspar, Ana
González‐Lamuño Leguina, Domingo
Chapman, Kimberly A.
Chien, Yin‐Hsiu
Janssen, Mirian C.H.
Ješina, Pavel
Lachmann, Robin
Lavigne, Christian
Lund, Allan M.
Lüsebrink, Natalia
Maillot, Francois
Martins, Ana Maria
Olivas, Silvia Meavilla
Mention, Karine
Mochel, Fanny
Monavari, Ahmad
Moreira, Sónia
Moreno, Carolina Araujo
Muačević‐Katanec, Diana
Mundy, Helen
Murphy, Elaine
Olivieri, Giorgia
Paquay, Stéphanie
Pedrón‐Giner, Consuelo
Peña Quintana, Luis 
Porras‐Hurtado, Gloria L.
Fraile, Pilar Quijada
Redonnet‐Vernhet, Isabelle
Rennings, Alexander J.M.
Pons, Mònica Ruiz
Santra, Saikat
Servais, Aude
Schiaffino, Maria Cristina
Schiff, Manuel
Schwahn, Bernd C.
Schwartz, Ida V.D.
Sremba, Leighann J.
Stainforth, Collette
Stepien, Karolina M.
Sykut‐Cegielska, Jolanta
Terry, Allyson
Tran, Christel
Miñana, Isidro Vitoria
Vives‐Piñera, Inmaculada
Williams, Monique
Zeman, Jiří
Zielonka, Matthias
UNESCO Clasification: 32 Ciencias médicas
320503 Gastroenterología
3207 Patología
Keywords: Homocystinuria
Patient registry
Natural history
Methionine
Thromboembolism, et al
Issue Date: 2021
Journal: Journal of Inherited Metabolic Disease 
Abstract: Cystathionine β‐synthase (CBS) deficiency has a wide clinical spectrum, ranging from neurodevelopmental problems, lens dislocation and marfanoid features in early childhood to adult onset disease with predominantly thromboembolic complications. We have analysed clinical and laboratory data at the time of diagnosis in 328 patients with CBS deficiency from the E‐HOD (European network and registry for Homocystinurias and methylation Defects) registry. We developed comprehensive criteria to classify patients into four groups of pyridoxine responsivity: non‐responders (NR), partial, full and extreme responders (PR, FR and ER, respectively). All groups showed overlapping concentrations of plasma total homocysteine while pyridoxine responsiveness inversely correlated with plasma/serum methionine concentrations. The FR and ER groups had a later age of onset and diagnosis and a longer diagnostic delay than NR and PR patients. Lens dislocation was common in all groups except ER but the age of dislocation increased with increasing responsiveness. Developmental delay was commonest in the NR group while no ER patient had cognitive impairment. Thromboembolism was the commonest presenting feature in ER patients, whereas it was least likely at presentation in the NR group. This probably is due to the differences in ages at presentation: all groups had a similar number of thromboembolic events per 1000 patient‐years. Clinical severity of CBS deficiency depends on the degree of pyridoxine responsiveness. Therefore, a standardised pyridoxine‐responsiveness test in newly diagnosed patients and a critical review of previous assessments is indispensable to ensure adequate therapy and to prevent or reduce long‐term complications
URI: http://hdl.handle.net/10553/106862
ISSN: 0141-8955
DOI: 10.1002/jimd.12338
Source: Journal of Inherited Metabolic Disease [ISSN 0141-8955], v. 44(3), p. 677-692, (Mayo 2021)
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