<scp><i>Kinesin family member 12</i></scp>‐related hepatopathy: A generally indolent disorder with elevated gamma‐glutamyl‐transferase activity-Reference-Cited by-同舟云学术

Kinesin family member 12‐related hepatopathy: A generally indolent disorder with elevated gamma‐glutamyl‐transferase activity

Published:2024-03-29 Issue:3 Volume:106 Page:224-233
ISSN:0009-9163
Container-title:Clinical Genetics
language:en
Short-container-title:Clinical Genetics

Author:

Vogel Georg‐Friedrich¹²^ORCID,Podpeskar Alexandra¹,Rieder Dietmar³,Salzer Helin¹,Garczarczyk‐Asim Dorota¹,Wang Li⁴,Abuduxikuer Kuerbanjiang⁴,Wang Jian‐She⁴,Scharrer Anke⁵,Faqeih Eissa Ali⁶,Aseeri Ali T.⁷,Vodopiutz Julia⁸^ORCID,Heilos Andreas⁹,Pichler Judith⁹,Huber Wolf‐Dietrich⁹,Müller Thomas¹,Knisely A. S.¹⁰,Janecke Andreas R.¹¹¹^ORCID

Affiliation:

1. Department of Paediatrics I Medical University of Innsbruck Innsbruck Austria

2. Institute of Cell Biology Medical University of Innsbruck Innsbruck Austria

3. Division of Bioinformatics Medical University of Innsbruck Innsbruck Austria

4. The Center for Pediatric Liver Diseases Children's Hospital of Fudan University, National Children's Medical Center Shanghai China

5. Department of Pathology Medical University Vienna Vienna Austria

6. Section of Medical Genetics, King Fahad Medical City Children's Specialist Hospital Riyadh Kingdom of Saudi Arabia

7. Section of Gastroenterology and Hepatology, King Fahad Medical City Children's Specialist Hospital Riyadh Kingdom of Saudi Arabia

8. Department of Pediatrics and Adolescent Medicine, Division of Pediatric Pulmonology, Allergology and Endocrinology, Comprehensive Center for Pediatrics Medical University of Vienna Vienna Austria

9. Department of Pediatric Nephrology and Gastroenterology Medical University Vienna Vienna Austria

10. Diagnostik‐ und Forschungsinstitut für Pathologie Medizinische Universität Graz Graz Austria

11. Division of Human Genetics Medical University of Innsbruck Innsbruck Austria

Abstract

AbstractExome sequencing (ES) has identified biallelic kinesin family member 12 (KIF12) mutations as underlying neonatal cholestatic liver disease. We collected information on onset and progression of this entity. Among consecutively referred pediatric patients at our centers, diagnostic ES identified 4 patients with novel, biallelic KIF12 variants using the human GRCh38 reference sequence, as KIF12 remains incompletely annotated in the older reference sequence GRCh37. A review of these and of 21 reported patients with KIF12 variants found that presentation with elevated serum transaminase activity in the context of trivial respiratory infection, without clinical features of liver disease, was more common (n = 18) than manifest cholestatic disease progressing rapidly to liver transplantation (LT; n = 7). Onset of liver disease was at age <1 year in 15 patients; LT was more common in this group. Serum gamma‐glutamyl transpeptidase activity (GGT) was elevated in all patients, and total bilirubin was elevated in 15 patients. Liver fibrosis or cirrhosis was present in 14 of 18 patients who were biopsied. The 16 different pathogenic variants and 11 different KIF12 genotypes found were not correlated with age of onset or progression to LT. Identification of biallelic pathogenic KIF12 variants distinguishes KIF12‐related disease from other entities with elevated GGT.

Publisher

Wiley

Link

https://onlinelibrary.wiley.com/doi/pdf/10.1111/cge.14524

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