Affiliation:
1. Department of Endocrinology and Metabolism Amsterdam UMC, University of Amsterdam Amsterdam The Netherlands
2. Amsterdam Gastroenterology Endocrinology Metabolism, Inborn Errors of Metabolism Amsterdam The Netherlands
3. Department of Pediatric Metabolic Diseases Amsterdam UMC, University of Amsterdam, Emma Children's Hospital Amsterdam The Netherlands
4. Laboratory Genetic Metabolic Diseases Amsterdam UMC, University of Amsterdam Amsterdam Netherlands
5. Department of Medical Biochemistry Leiden Institute of Chemistry, University of Leiden Leiden The Netherlands
6. Department of Internal Medicine Radboud UMC Nijmegen Netherlands
Abstract
AbstractAcid sphingomyelinase deficiency (ASMD) is an ultra‐rare lysosomal storage disease with a broad spectrum of manifestations ranging from severe neuropathic forms to attenuated, chronic visceral forms. Manifestations of the chronic visceral subtype are variable and encompass different degrees of hepatosplenomegaly, pulmonary disease and dyslipidemia. The aim of this study was to provide insights into the natural course of adult patients with the chronic visceral subtype. Based on these insights, we proposed tentative criteria for initiation and follow‐up of enzyme replacement therapy (ERT). The data of 23 adult patients were collected in a prospective study. Clinical, genetic and demographic data, plasma measurements, abdominal imaging, pulmonary imaging, pulmonary function tests and quality of life questionnaires were collected. Stability of disease based on several clinical, biochemical and radiological markers (i.e., spleen volume, platelet levels, liver volume, alanine aminotransferase [ALT] levels, diffusion capacity of the lungs for carbon monoxide [DLCO] chitotriosidase activity and lysosphingomyelin [LSM]) was assessed. Cardiovascular risk was estimated based on sex, age, smoking, systolic blood pressure and lipid profile. Quality of life was evaluated with the 36‐Item Short Form Health Survey and the Health Assessment Questionnaire. Median follow‐up was 6.1 years (range 1.3–19.5 years). The most common manifestations were splenomegaly (100%), decreased high‐density lipoprotein cholesterol (HDL‐C) plasma levels (83%), (signs of) steatosis measured with transient elastography (82%), thrombocytopenia (64%), hepatomegaly (52%) and decreased diffusion capacity (45%). The majority of markers remained stable during follow‐up. Twelve patients showed progression of disease: four for spleen volume, two for liver volume, three for DLCO, seven for chitotriosidase activity and three for LSM. One patient showed progression of disease based on four markers, although this patient did not report any problems at the last visit. Cardiovascular risk was estimated and was increased in half of the patients older than 40 years. Patient‐reported quality of life did not differ from the general population, but differences in median 36‐Item Short Form Health Survey (SF‐36) scores of patients with severe pulmonary involvement and those of patients without pulmonary involvement were observed. Tentative criteria for initiation and effect of therapy were proposed. In conclusion, the chronic visceral subtype of ASMD showed a predominantly stable disease course in this cohort. We propose that ERT should be initiated on an individual basis and only in case of progression or symptomatic disease. Collection and analysis of real world data are necessary to refine start, stop and follow‐up criteria in the future.