Vorinostat in the acute neuroinflammatory form of X‐linked adrenoleukodystrophy

Bettina Zierfuss; Isabelle Weinhofer; Jörn‐Sven Kühl; Wolfgang Köhler; Annette Bley; Katharina Zauner; Johannes Binder; Ksenija Martinović; Christian Seiser; Christoph Hertzberg; Stephan Kemp; Gerda Egger; Gerda Leitner; Jan Bauer; Christoph Wiesinger; Markus Kunze; Sonja Forss‐Petter; Johannes Berger

doi:10.1002/acn3.51015

Annals of Clinical and Translational Neurology (May 2020)

Vorinostat in the acute neuroinflammatory form of X‐linked adrenoleukodystrophy

Bettina Zierfuss,
Isabelle Weinhofer,
Jörn‐Sven Kühl,
Wolfgang Köhler,
Annette Bley,
Katharina Zauner,
Johannes Binder,
Ksenija Martinović,
Christian Seiser,
Christoph Hertzberg,
Stephan Kemp,
Gerda Egger,
Gerda Leitner,
Jan Bauer,
Christoph Wiesinger,
Markus Kunze,
Sonja Forss‐Petter,
Johannes Berger

Affiliations

Bettina Zierfuss: Department of Pathobiology of the Nervous System Center for Brain Research Medical University of Vienna Vienna Austria
Isabelle Weinhofer: Department of Pathobiology of the Nervous System Center for Brain Research Medical University of Vienna Vienna Austria
Jörn‐Sven Kühl: Department of Pediatric Oncology, Hematology, and Hemostaseology University Hospital Leipzig Leipzig Germany
Wolfgang Köhler: Department of Neurology University of Leipzig Medical Center Leukodystrophy Clinic Leipzig Germany
Annette Bley: Department of Pediatrics University Medical Center Hamburg Eppendorf Hamburg Germany
Katharina Zauner: Department of Pathobiology of the Nervous System Center for Brain Research Medical University of Vienna Vienna Austria
Johannes Binder: Department of Pathobiology of the Nervous System Center for Brain Research Medical University of Vienna Vienna Austria
Ksenija Martinović: Department of Pathobiology of the Nervous System Center for Brain Research Medical University of Vienna Vienna Austria
Christian Seiser: Division of Cell and Developmental Biology Center for Anatomy and Cell Biology Medical University of Vienna Vienna Austria
Christoph Hertzberg: Vivantes Klinikum Neukölln Berlin Germany
Stephan Kemp: Department of Genetic Metabolic Diseases Amsterdam UMC University of Amsterdam Amsterdam The Netherlands
Gerda Egger: Department of Pathology Medical University of Vienna Vienna Austria
Gerda Leitner: Department of Blood Group Serology and Transfusion Medicine Medical University of Vienna Vienna Austria
Jan Bauer: Department of Neuroimmunology Center for Brain Research Medical University of Vienna Vienna Austria
Christoph Wiesinger: Department of Pathobiology of the Nervous System Center for Brain Research Medical University of Vienna Vienna Austria
Markus Kunze: Department of Pathobiology of the Nervous System Center for Brain Research Medical University of Vienna Vienna Austria
Sonja Forss‐Petter: Department of Pathobiology of the Nervous System Center for Brain Research Medical University of Vienna Vienna Austria
Johannes Berger: Department of Pathobiology of the Nervous System Center for Brain Research Medical University of Vienna Vienna Austria

DOI: https://doi.org/10.1002/acn3.51015
Journal volume & issue: Vol. 7, no. 5
pp. 639 – 652

Abstract

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Abstract Objective To identify a pharmacological compound targeting macrophages, the most affected immune cells in inflammatory X‐linked adrenoleukodystrophy (cerebral X‐ALD) caused by ABCD1 mutations and involved in the success of hematopoietic stem cell transplantation and gene therapy. Methods A comparative database analysis elucidated the epigenetic repressing mechanism of the related ABCD2 gene in macrophages and identified the histone deacetylase (HDAC) inhibitor Vorinostat as a compound to induce ABCD2 in these cells to compensate for ABCD1 deficiency. In these cells, we investigated ABCD2 and pro‐inflammatory gene expression, restoration of defective peroxisomal β‐oxidation activity, accumulation of very long‐chain fatty acids (VLCFAs) and their differentiation status. We investigated ABCD2 and pro‐inflammatory gene expression, restoration of defective peroxisomal ß‐oxidation activity, accumulation of very long‐chain fatty acids (VLCFA) and differentiation status. Three advanced cerebral X‐ALD patients received Vorinostat and CSF and MRI diagnostics was carried out in one patient after 80 days of treatment. Results Vorinostat improved the metabolic defects in X‐ALD macrophages by stimulating ABCD2 expression, peroxisomal ß‐oxidation, and ameliorating VLCFA accumulation. Vorinostat interfered with pro‐inflammatory skewing of X‐ALD macrophages by correcting IL12B expression and further reducing monocyte differentiation. Vorinostat normalized the albumin and immunoglobulin CSF‐serum ratios, but not gadolinium enhancement upon 80 days of treatment. Interpretation The beneficial effects of HDAC inhibitors on macrophages in X‐ALD and the improvement of the blood‐CSF/blood‐brain barrier are encouraging for future investigations. In contrast with Vorinostat, less toxic macrophage‐specific HDAC inhibitors might improve also the clinical state of X‐ALD patients with advanced inflammatory demyelination.

Published in Annals of Clinical and Translational Neurology

ISSN: 2328-9503 (Online)
Publisher: Wiley
Country of publisher: United States
LCC subjects: Medicine: Internal medicine: Neurosciences. Biological psychiatry. Neuropsychiatry: Neurology. Diseases of the nervous system
Website: https://onlinelibrary.wiley.com/journal/23289503

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