Impact of genetic and non-genetic factors on phenotypic diversity in NBAS-associated disease

Nicole Hammann; Dominic Lenz; Ivo Baric; Ellen Crushell; Carlo Dionisi Vici; Felix Distelmaier; Francois Feillet; Peter Freisinger; Maja Hempel; Anna L Khoreva; Martin W Laass; Yves Lacassie; Elke Lainka; Catherine Larson-Nath; Zhongdie Li; Patryk Lipiński; Eberhard Lurz; André Mégarbané; Susana Nobre; Giorgia Olivieri; Bianca Peters; Paolo Prontera; Lea D Schlieben; Christine M Seroogy; Cristina Sobacchi; Shigeru Suzuki; Christel Tran; Jerry Vockley; Jian-She Wang; Matias Wagner; Holger Prokisch; Sven F Garbade; Stefan Kölker; Georg F Hoffmann; Christian Staufner

doi:10.1016/j.ymgme.2023.108118

Impact of genetic and non-genetic factors on phenotypic diversity in NBAS-associated disease

Mol Genet Metab. 2024 Mar;141(3):108118. doi: 10.1016/j.ymgme.2023.108118. Epub 2024 Jan 11.

Authors

Nicole Hammann¹, Dominic Lenz¹, Ivo Baric², Ellen Crushell³, Carlo Dionisi Vici⁴, Felix Distelmaier⁵, Francois Feillet⁶, Peter Freisinger⁷, Maja Hempel⁸, Anna L Khoreva⁹, Martin W Laass¹⁰, Yves Lacassie¹¹, Elke Lainka¹², Catherine Larson-Nath¹³, Zhongdie Li¹⁴, Patryk Lipiński¹⁵, Eberhard Lurz¹⁶, André Mégarbané¹⁷, Susana Nobre¹⁸, Giorgia Olivieri⁴, Bianca Peters¹, Paolo Prontera¹⁹, Lea D Schlieben²⁰, Christine M Seroogy²¹, Cristina Sobacchi²², Shigeru Suzuki²³, Christel Tran²⁴, Jerry Vockley²⁵, Jian-She Wang¹⁴, Matias Wagner²⁰, Holger Prokisch²⁰, Sven F Garbade¹, Stefan Kölker¹, Georg F Hoffmann¹, Christian Staufner²⁶

Affiliations

¹ Heidelberg University, Medical Faculty Heidelberg, Center for Pediatric and Adolescent Medicine, Department I, Division of Pediatric Neurology and Metabolic Medicine, Heidelberg, Germany.
² Department of Paediatrics, University Hospital Center Zagreb, University of Zagreb, School of Medicine, Zagreb, Croatia.
³ National Centre for Inherited Metabolic Disorders, Childrens Health Ireland, Temple Street, Dublin 1, Ireland.
⁴ Division of Metabolism, Bambino Gesù Children's Research Hospital, Rome, Italy.
⁵ Department of General Paediatrics, Neonatology and Paediatric Cardiology, University Children's Hospital, Heinrich-Heine-University, Düsseldorf, Germany.
⁶ Department of Paediatrics, Hôpital d'Enfants Brabois, CHU Nancy, Vandoeuvre les Nancy, France.
⁷ Children's Hospital Reutlingen, Germany.
⁸ Institute of Human Genetics, Heidelberg University Hospital, Heidelberg, Germany.
⁹ Dmitry Rogachev National Research Center for Pediatric Hematology, Oncology, Immunology Moscow, Russia.
¹⁰ Department of Pediatrics, Faculty of Medicine and University Hospital Carl Gustav Carus, Technische Universität Dresden, Dresden, Germany.
¹¹ Department of Pediatrics, Division of Genetics, LSU Health Sciences Center and Children's Hospital, New Orleans, Louisiana, USA.
¹² Pediatrics II, Department for Pediatric Nephrology, Gastroenterology, Endocrinology and Transplant Medicine, University Hospital Essen, University of Duisburg-Essen, Essen, Germany.
¹³ Pediatric Gastroenterology, University of Minnesota Medical School, Minneapolis, MN, USA.
¹⁴ Center for Pediatric Liver Diseases, Children's Hospital of Fudan University, Shanghai, China.
¹⁵ Department of Pediatrics, Nutrition and Metabolic Diseases, The Children's Memorial Health Institute, Warsaw, Poland.
¹⁶ Department of Pediatrics, Dr. von Hauner Children's Hospital, University Hospital, LMU Munich, Munich, Germany.
¹⁷ Department of Human Genetics Gilbert and Rose-Marie Chagoury School of Medicine, Lebanese American University, Byblos, Lebanon; Institut Jérôme Lejeune, Paris, France.
¹⁸ Pediatric Hepatology and Liver Transplantation Unit, Pediatric Department, Coimbra Hospital and Universitary Centre, Coimbra, Portugal.
¹⁹ Medical Genetics Unit, Maternal-Infantile Department, Hospital and University of Perugia, Perugia, Italy.
²⁰ School of Medicine, Institute of Human Genetics, Technische Universität München, Munich, Germany; Department Computational Health, Institute of Neurogenomics, Helmholtz Zentrum München, Munich, Germany.
²¹ Division of Allergy, Immunology and Rheumatology, Department of Pediatrics, University of Wisconsin-Madison, USA.
²² Humanitas Research Hospital IRCCS, Rozzano, Italy; Institute for Genetic and Biomedical Research-National Research Council, Milan Unit, Milan, Italy.
²³ Department of Pediatrics, Asahikawa Medical University, Asahikawa, Japan.
²⁴ Division of Genetic Medicine, Lausanne University Hospital and University of Lausanne, Lausanne, Switzerland.
²⁵ University of Pittsburgh School of Medicine, UPMC Children's Hospital of Pittsburgh, Pittsburgh, PA, USA.
²⁶ Heidelberg University, Medical Faculty Heidelberg, Center for Pediatric and Adolescent Medicine, Department I, Division of Pediatric Neurology and Metabolic Medicine, Heidelberg, Germany. Electronic address: Christian.Staufner@med.uni-heidelberg.de.

PMID: 38244286
DOI: 10.1016/j.ymgme.2023.108118

Abstract

Biallelic pathogenic variants in neuroblastoma-amplified sequence (NBAS) cause a pleiotropic multisystem disorder. Three clinical subgroups have been defined correlating with the localisation of pathogenic variants in the NBAS gene: variants affecting the C-terminal region of NBAS result in SOPH syndrome (short stature, optic atrophy, Pelger-Huët anomaly), variants affecting the Sec 39 domain are associated with infantile liver failure syndrome type 2 (ILFS2) and variants affecting the ß-propeller domain give rise to a combined phenotype. However, there is still unexplained phenotypic diversity across the three subgroups, challenging the current concept of genotype-phenotype correlations in NBAS-associated disease. Therefore, besides examining the genetic influence, we aim to elucidate the potential impact of pre-symptomatic diagnosis, emergency management and other modifying variables on the clinical phenotype. We investigated genotype-phenotype correlations in individuals sharing the same genotypes (n = 30 individuals), and in those sharing the same missense variants with a loss-of-function variant in trans (n = 38 individuals). Effects of a pre-symptomatic diagnosis and emergency management on the severity of acute liver failure (ALF) episodes also were analysed, comparing liver function tests (ALAT, ASAT, INR) and mortality. A strong genotype-phenotype correlation was demonstrated in individuals sharing the same genotype; this was especially true for the ILFS2 subgroup. Genotype-phenotype correlation in patients sharing only one missense variant was still high, though at a lower level. Pre-symptomatic diagnosis in combination with an emergency management protocol leads to a trend of reduced severity of ALF. High genetic impact on clinical phenotype in NBAS-associated disease facilitates monitoring and management of affected patients sharing the same genotype. Pre-symptomatic diagnosis and an emergency management protocol do not prevent ALF but may reduce its clinical severity.

Keywords: Genotype-phenotype correlation; ILFS2; NBAS; Recurrent acute liver failure; SOPH.

MeSH terms

Humans
Liver Failure, Acute* / genetics
Mutation, Missense
Neuroblastoma* / complications
Pelger-Huet Anomaly* / complications
Pelger-Huet Anomaly* / genetics
Pelger-Huet Anomaly* / pathology
Phenotype