Sex, Genotype, and Liver Volume Progression as Risk of Hospitalization Determinants in Autosomal Dominant Polycystic Liver Disease

Ria Schönauer; Dana Sierks; Melissa Boerrigter; Tabinda Jawaid; Lea Caroff; Marie-Pierre Audrezet; Anja Friedrich; Melissa Shaw; Jan Degenhardt; Mirjam Forberger; Jonathan de Fallois; Hendrik Bläker; Carsten Bergmann; Juliana Gödiker; Philipp Schindler; Bernhard Schlevogt; Roman-U Müller; Thomas Berg; Ilse Patterson; William J Griffiths; John A Sayer; Genomics England Research Consortium; Bernt Popp; Vicente E Torres; Marie C Hogan; Stefan Somlo; Terry J Watnick; Frederik Nevens; Whitney Besse; Emilie Cornec-Le Gall; Peter C Harris; Joost P H Drenth; Jan Halbritter

doi:10.1053/j.gastro.2023.12.007

Sex, Genotype, and Liver Volume Progression as Risk of Hospitalization Determinants in Autosomal Dominant Polycystic Liver Disease

Gastroenterology. 2024 May;166(5):902-914. doi: 10.1053/j.gastro.2023.12.007. Epub 2023 Dec 13.

Authors

Ria Schönauer¹, Dana Sierks², Melissa Boerrigter³, Tabinda Jawaid⁴, Lea Caroff⁵, Marie-Pierre Audrezet⁶, Anja Friedrich⁷, Melissa Shaw⁸, Jan Degenhardt⁹, Mirjam Forberger¹⁰, Jonathan de Fallois¹¹, Hendrik Bläker¹⁰, Carsten Bergmann⁷, Juliana Gödiker¹², Philipp Schindler¹³, Bernhard Schlevogt¹⁴, Roman-U Müller¹⁵, Thomas Berg¹⁶, Ilse Patterson¹⁷, William J Griffiths¹⁸, John A Sayer¹⁹; Genomics England Research Consortium; Bernt Popp²², Vicente E Torres⁴, Marie C Hogan⁴, Stefan Somlo⁸, Terry J Watnick²³, Frederik Nevens²⁴, Whitney Besse⁸, Emilie Cornec-Le Gall⁵, Peter C Harris⁴, Joost P H Drenth²⁵, Jan Halbritter²⁶

Collaborators

Genomics England Research Consortium:
John C Ambrose²⁰, Prabhu Arumugam²⁰, Roel Bevers²⁰, Marta Bleda²⁰, Freya Boardman-Pretty²¹, Christopher R Boustred²⁰, Helen Brittain²⁰, Mark J Caulfield²¹, Georgia C Chan²⁰, Greg Elgar²¹, Tom Fowler²⁰, Adam Giess²⁰, Angela Hamblin²⁰, Shirley Henderson²¹, Tim J P Hubbard²⁰, Rob Jackson²⁰, Louise J Jones²¹, Dalia Kasperaviciute²¹, Melis Kayikci²⁰, Athanasios Kousathanas²⁰, Lea Lahnstein²⁰, Sarah E A Leigh²⁰, Ivonne U S Leong²⁰, Javier F Lopez²⁰, Fiona Maleady-Crowe²⁰, Meriel McEntagart²⁰, Federico Minneci²⁰, Loukas Moutsianas²¹, Michael Mueller²¹, Nirupa Murugaesu²⁰, Anna C Need²¹, Peter O'Donovan²⁰, Chris A Odhams²⁰, Christine Patch²¹, Mariana Buongermino Pereira²⁰, Daniel Perez-Gil²⁰, John Pullinger²⁰, Tahrima Rahim²⁰, Augusto Rendon²⁰, Tim Rogers²⁰, Kevin Savage²⁰, Kushmita Sawant²⁰, Richard H Scott²⁰, Afshan Siddiq²⁰, Alexander Sieghart²⁰, Samuel C Smith²⁰, Alona Sosinsky²¹, Alexander Stuckey²⁰, Mélanie Tanguy²⁰, Ana Lisa Taylor Tavares²⁰, Ellen R A Thomas²¹, Simon R Thompson²⁰, Arianna Tucci²¹, Matthew J Welland²⁰, Eleanor Williams²⁰, Katarzyna Witkowska²¹, Suzanne M Wood²¹

Affiliations

¹ Department of Nephrology and Internal Intensive Care Medicine, Charité Universitätsmedizin Berlin (corporate member of Freie Universität Berlin and Humboldt-Universität zu Berlin), Berlin, Germany; Division of Nephrology, Department of Internal Medicine, University of Leipzig Medical Center, Leipzig, Germany.
² Division of Nephrology, Department of Internal Medicine, University of Leipzig Medical Center, Leipzig, Germany; Department of Pediatric Surgery, Universitätsklinikum Leipzig, Leipzig, Germany.
³ Department of Gastroenterology and Hepatology, Radboud University Medical Center, Nijmegen, The Netherlands.
⁴ Division of Nephrology and Hypertension, Mayo Clinic, Rochester, Minnesota.
⁵ University of Brest, Institut National de la Santé et de la Recherche Médicale, UMR 1078, Génétique, Génomique Fonctionnelle et Biotechnologies, Brest, France; Centre Hospitalier Universitaire Brest, Service de Néphrologie, Centre de Référence Maladies Rénales Héréditaires de l'Enfant et de l'Adulte, Brest, France.
⁶ Centre Hospitalier Universitaire Brest, Service de Génétique Moléculaire, Brest, France.
⁷ Medizinische Genetik Mainz, Limbach Genetics, Mainz, Germany.
⁸ Departments of Internal Medicine and Nephrology, Yale University School of Medicine, New Haven, Connecticut.
⁹ Department 2 of Internal Medicine, University of Cologne, Faculty of Medicine, University Hospital Cologne, Cologne, Germany.
¹⁰ Department of Pathology, University of Leipzig Medical Center, Leipzig, Germany.
¹¹ Division of Nephrology, Department of Internal Medicine, University of Leipzig Medical Center, Leipzig, Germany.
¹² Department of Internal Medicine B, University Hospital Münster, Münster, Germany.
¹³ Clinic for Radiology, University Hospital Münster, Münster, Germany.
¹⁴ Department of Internal Medicine B, University Hospital Münster, Münster, Germany; Department of Gastroenterology, Medical Center Osnabrück, Osnabrück, Germany.
¹⁵ Department 2 of Internal Medicine, University of Cologne, Faculty of Medicine, University Hospital Cologne, Cologne, Germany; Cologne Excellence Cluster on Cellular Stress Responses in Aging-Associated Diseases (CECAD) University of Cologne, Faculty of Medicine and University Hospital Cologne, Cologne, Germany.
¹⁶ Division of Hepatology, Department of Medicine II, University of Leipzig Medical Center, Leipzig, Germany.
¹⁷ Department of Radiology, Cambridge University Hospitals, Cambridge, United Kingdom.
¹⁸ Department of Hepatology, Cambridge Liver Unit, Cambridge University Hospitals, Cambridge, United Kingdom.
¹⁹ Translational and Clinical Research Institute, Faculty of Medical Sciences, Newcastle University, Newcastle upon Tyne, United Kingdom; Renal Services, Newcastle upon Tyne National Health Service Foundation Trust, Newcastle upon Tyne, United Kingdom; National Institute for Health Research Newcastle Biomedical Research Centre, Newcastle upon Tyne, United Kingdom.
²⁰ Genomics England, London, United Kingdom.
²¹ Genomics England, London, United Kingdom; William Harvey Research Institute, Queen Mary University of London, London, United Kingdom.
²² Berlin Institute of Health at Charité, Universitätsmedizin Berlin, Center of Functional Genomics, Berlin, Germany.
²³ Department of Medicine, University of Maryland School of Medicine, Baltimore, Maryland.
²⁴ Department of Hepatology and Liver Transplantation Unit, University Hospitals Katholieke Universiteit Leuven, Leuven, Belgium.
²⁵ Department of Gastroenterology and Hepatology, Radboud University Medical Center, Nijmegen, The Netherlands. Electronic address: joostphdrenth@cs.com.
²⁶ Department of Nephrology and Internal Intensive Care Medicine, Charité Universitätsmedizin Berlin (corporate member of Freie Universität Berlin and Humboldt-Universität zu Berlin), Berlin, Germany; Division of Nephrology, Department of Internal Medicine, University of Leipzig Medical Center, Leipzig, Germany. Electronic address: jan.halbritter@charite.de.

PMID: 38101549
DOI: 10.1053/j.gastro.2023.12.007

Abstract

Background & aims: Autosomal dominant polycystic liver disease is a rare condition with a female preponderance, based mainly on pathogenic variants in 2 genes, PRKCSH and SEC63. Clinically, autosomal dominant polycystic liver disease is characterized by vast heterogeneity, ranging from asymptomatic to highly symptomatic hepatomegaly. To date, little is known about the prediction of disease progression at early stages, hindering clinical management, genetic counseling, and the design of randomized controlled trials. To improve disease prognostication, we built a consortium of European and US centers to recruit the largest cohort of patients with PRKCSH and SEC63 liver disease.

Methods: We analyzed an international multicenter cohort of 265 patients with autosomal dominant polycystic liver disease harboring pathogenic variants in PRKCSH or SEC63 for genotype-phenotype correlations, including normalized age-adjusted total liver volumes and polycystic liver disease-related hospitalization (liver event) as primary clinical end points.

Results: Classifying individual total liver volumes into predefined progression groups yielded predictive risk discrimination for future liver events independent of sex and underlying genetic defects. In addition, disease severity, defined by age at first liver event, was considerably more pronounced in female patients and patients with PRKCSH variants than in those with SEC63 variants. A newly developed sex-gene score was effective in distinguishing mild, moderate, and severe disease, in addition to imaging-based prognostication.

Conclusions: Both imaging and clinical genetic scoring have the potential to inform patients about the risk of developing symptomatic disease throughout their lives. The combination of female sex, germline PRKCSH alteration, and rapid total liver volume progression is associated with the greatest odds of polycystic liver disease-related hospitalization.

Keywords: ADPLD; PCLD; PRKCSH; SEC63; TLV.

Publication types

Research Support, Non-U.S. Gov't
Multicenter Study

MeSH terms

Adult
Calcium-Binding Proteins*
Cysts* / diagnostic imaging
Cysts* / genetics
Cysts* / pathology
Disease Progression*
Europe
Female
Genetic Association Studies
Genetic Predisposition to Disease
Genotype
Glucosidases* / genetics
Hepatomegaly / diagnostic imaging
Hepatomegaly / genetics
Hospitalization* / statistics & numerical data
Humans
Liver / diagnostic imaging
Liver / pathology
Liver Diseases* / diagnostic imaging
Liver Diseases* / genetics
Liver Diseases* / pathology
Male
Middle Aged
Molecular Chaperones*
Organ Size
Prognosis
RNA-Binding Proteins*
Risk Assessment
Risk Factors
Severity of Illness Index
Sex Factors
United States / epidemiology

Substances

Glucosidases
SEC63 protein, human
PRKCSH protein, human
Calcium-Binding Proteins
RNA-Binding Proteins
Molecular Chaperones

Supplementary concepts

Polycystic liver disease