Clinico-biological refinement of BCL11B-related disorder and identification of an episignature: A series of 20 unreported individuals

Ange‐Line Bruel ,Roberta Zuntini,Elodie Sanchez,Claire Lozano,Frédéric Tran Mau‐Them ,Laurence Perrin,Mevyn Nizard,Nicolas Chatron,Jennifer Kerkhof,Vincent Gatinois,Kévin Yauy,Julien Van Gils,Juliette Piard,William Dufour,Matthew L Tedder ,Jeanne Amiel,A Crastes De Paulet ,Sophie Rondeau,Patrick Edery,Quentin Sabbagh,Anne‐Marie Guerrot ,Evan Gouy,Vincent Michaud,David Geneviève,Arthur Sorlin,Chin-To Fong,Sandra Whalen,Marion Lesieur-Sebellin,Carlo Fusco,Odile Boute,Francesca Peluso,Henri Margot,Tugce B Balci ,Madhavi Prasad,Alyce Belonis,Stanislas Lyonnet,Sadegheh Haghshenas,Liselot Van Der Laan,Chloé Trouvé,Vincent Pernin,Pauline Marzin,Tania Attié‐Bitach ,Debbie Shears,Stefano Giuseppe Caraffi,Haley Mcconkey,Diana S Brightman,Chitra Prasad,Mouna Barat‐Houari ,Marlène Rio,Nathalie Ruiz-Pallares,Bekim Sadiković ,Jonathan Levy,Gaël Nicolas,Solveig Heide,Christophe Philippe,Boris Keren,Alain Verloès ,Marjolaine Willems,Natalya Karp,Mylène Tharreau,Michael A Levy,Corinne Collet,Victoria Mok Siu,Anjali Joshi ,Raissa Relator,Valentin Ruault

doi:10.1016/j.gim.2023.101007

Abstract

PurposeBCL11B-related disorder (BCL11B-RD) arises from rare genetic variants within the BCL11B gene, resulting in a distinctive clinical spectrum encompassing syndromic neurodevelopmental disorder, with or without intellectual disability, associated with facial features and impaired immune function. This study presents an in-depth clinico-biological analysis of 20 newly reported individuals with BCL11B-RD, coupled with a characterization of genome-wide DNA methylation patterns of this genetic condition. MethodsThrough an international collaboration, clinical and molecular data from 20 individuals were systematically gathered, and a comparative analysis was conducted between this series and existing literature. We further scrutinized peripheral blood DNA methylation profile of individuals with BCL11B-RD, contrasting them with healthy controls and other neurodevelopmental disorders marked by established episignature. ResultsOur findings unveil rarely documented clinical manifestations, notably including Rubinstein-Taybi-like facial features, craniosynostosis, and autoimmune disorders, all manifesting within the realm of BCL11B-RD. We refine the intricacies of T cell compartment alterations of BCL11B-RD, revealing decreased levels naive CD4+ T cells and recent thymic emigrants while concurrently observing an elevated proportion of effector-memory expressing CD45RA CD8+ T cells (TEMRA). Finally, a distinct DNA methylation episignature exclusive to BCL11B-RD is unveiled. ConclusionThis study serves to enrich our comprehension of the clinico-biological landscape of BCL11B-RD, potentially furnishing a more precise framework for diagnosis and follow-up of individuals carrying pathogenic BCL11B variant. Moreover, the identification of a unique DNA methylation episignature offers a valuable diagnosis tool for BCL11B-RD, thereby facilitating routine clinical practice by empowering physicians to reevaluate variants of uncertain significance within the BCL11B gene.

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