A Retrospective Multicentric Study of 34 Patients with Niemann–Pick Type C Disease and Early Liver Involvement in France

医学 肝脾肿大 胃肠病学 肝活检 新生儿胆汁淤积症 胆汁淤积 内科学 肝病 病理 活检 肝移植 疾病 胆道闭锁 移植
作者
Antoine Gardin,Charlotte Mussini,Bénédicte Héron,Manuel Schiff,Anaïs Brassier,Dries Dobbelaere,Pierre Broué,Caroline Sevin,Marie T. Vanier,Dalila Habès,Emmanuel Jacquemin,Emmanuel Gonzalès
出处
期刊:The Journal of Pediatrics [Elsevier BV]
卷期号:254: 75-82.e4 被引量:4
标识
DOI:10.1016/j.jpeds.2022.10.015
摘要

To describe the clinical features and course of liver involvement in a cohort of patients with Niemann-Pick type C disease (NP-C), a severe lysosomal storage disorder.Patients with genetically confirmed NP-C (NPC1, n = 31; NPC2, n = 3) and liver involvement before age 6 months were retrospectively included. Clinical, laboratory test, and imaging data were collected until the last follow-up or death; available liver biopsy specimens were studied using anti-CD68 immunostaining.At initial evaluation (median age, 17 days of life), all patients had hepatomegaly, 33 had splenomegaly, and 30 had neonatal cholestasis. Portal hypertension and liver failure developed in 9 and 4 patients, respectively. Liver biopsy studies, performed in 16 patients, revealed significant fibrosis in all 16 and CD68+ storage cells in 15. Serum alpha-fetoprotein concentration measured in 21 patients was elevated in 17. Plasma oxysterol concentrations were increased in the 16 patients tested. Four patients died within 6 months of life, including 3 from liver involvement. In patients who survived beyond age 6 months (median follow-up, 6.1 years), cholestasis regressed in all, and portal hypertension regressed in all but 1; 25 patients developed neurologic involvement, which was fatal in 16 patients.Liver involvement in NP-C consisted of transient neonatal cholestasis with hepatosplenomegaly, was associated with liver fibrosis, and was responsible for death in 9% of patients. The combination of liver anti-CD68 immunostaining, serum alpha-fetoprotein measurement, and studies of plasma biomarkers should facilitate early identification of NP-C.

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