Drug screening identifies tazarotene and bexarotene as therapeutic agents in multiple sulfatase deficiency

Lars Schlotawa; Karolina Tyka; Matthias Kettwig; Rebecca C Ahrens‐Nicklas; Matthias Baud; Tea Berulava; Nicola Brunetti‐Pierri; Alyssa Gagne; Zackary M Herbst; Jean A Maguire; Jlenia Monfregola; Tonatiuh Pena; Karthikeyan Radhakrishnan; Sophie Schröder; Elisa A Waxman; Andrea Ballabio; Thomas Dierks; André Fischer; Deborah L French; Michael H Gelb; Jutta Gärtner

doi:10.15252/emmm.202114837

EMBO Molecular Medicine (Mar 2023)

Drug screening identifies tazarotene and bexarotene as therapeutic agents in multiple sulfatase deficiency

Lars Schlotawa,
Karolina Tyka,
Matthias Kettwig,
Rebecca C Ahrens‐Nicklas,
Matthias Baud,
Tea Berulava,
Nicola Brunetti‐Pierri,
Alyssa Gagne,
Zackary M Herbst,
Jean A Maguire,
Jlenia Monfregola,
Tonatiuh Pena,
Karthikeyan Radhakrishnan,
Sophie Schröder,
Elisa A Waxman,
Andrea Ballabio,
Thomas Dierks,
André Fischer,
Deborah L French,
Michael H Gelb,
Jutta Gärtner

Affiliations

Lars Schlotawa: Department of Paediatrics and Adolescent Medicine University Medical Centre Göttingen Göttingen Germany
Karolina Tyka: Department of Paediatrics and Adolescent Medicine University Medical Centre Göttingen Göttingen Germany
Matthias Kettwig: Department of Paediatrics and Adolescent Medicine University Medical Centre Göttingen Göttingen Germany
Rebecca C Ahrens‐Nicklas: Division of Human Genetics and Metabolism The Children's Hospital of Philadelphia Philadelphia PA USA
Matthias Baud: School of Chemistry and Institute for Life Sciences University of Southampton Southampton UK
Tea Berulava: Department for Epigenetics and Systems Medicine in Neurodegenerative Diseases German Centre for Neurodegenerative Diseases Göttingen Germany
Nicola Brunetti‐Pierri: Telethon Institute of Genetics and Medicine Pozzuoli Italy
Alyssa Gagne: Center for Cellular and Molecular Therapeutics The Children's Hospital of Philadelphia Philadelphia PA USA
Zackary M Herbst: Department of Chemistry University of Washington Seattle WA USA
Jean A Maguire: Center for Cellular and Molecular Therapeutics The Children's Hospital of Philadelphia Philadelphia PA USA
Jlenia Monfregola: Telethon Institute of Genetics and Medicine Pozzuoli Italy
Tonatiuh Pena: Department for Epigenetics and Systems Medicine in Neurodegenerative Diseases German Centre for Neurodegenerative Diseases Göttingen Germany
Karthikeyan Radhakrishnan: Faculty of Chemistry, Biochemistry I Bielefeld University Bielefeld Germany
Sophie Schröder: Department for Epigenetics and Systems Medicine in Neurodegenerative Diseases German Centre for Neurodegenerative Diseases Göttingen Germany
Elisa A Waxman: Center for Cellular and Molecular Therapeutics The Children's Hospital of Philadelphia Philadelphia PA USA
Andrea Ballabio: Telethon Institute of Genetics and Medicine Pozzuoli Italy
Thomas Dierks: Faculty of Chemistry, Biochemistry I Bielefeld University Bielefeld Germany
André Fischer: Department for Epigenetics and Systems Medicine in Neurodegenerative Diseases German Centre for Neurodegenerative Diseases Göttingen Germany
Deborah L French: Center for Cellular and Molecular Therapeutics The Children's Hospital of Philadelphia Philadelphia PA USA
Michael H Gelb: Department of Chemistry University of Washington Seattle WA USA
Jutta Gärtner: Department of Paediatrics and Adolescent Medicine University Medical Centre Göttingen Göttingen Germany

DOI: https://doi.org/10.15252/emmm.202114837
Journal volume & issue: Vol. 15, no. 3
pp. n/a – n/a

Abstract

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Abstract Multiple sulfatase deficiency (MSD, MIM #272200) results from pathogenic variants in the SUMF1 gene that impair proper function of the formylglycine‐generating enzyme (FGE). FGE is essential for the posttranslational activation of cellular sulfatases. MSD patients display reduced or absent sulfatase activities and, as a result, clinical signs of single sulfatase disorders in a unique combination. Up to date therapeutic options for MSD are limited and mostly palliative. We performed a screen of FDA‐approved drugs using immortalized MSD patient fibroblasts. Recovery of arylsulfatase A activity served as the primary readout. Subsequent analysis confirmed that treatment of primary MSD fibroblasts with tazarotene and bexarotene, two retinoids, led to a correction of MSD pathophysiology. Upon treatment, sulfatase activities increased in a dose‐ and time‐dependent manner, reduced glycosaminoglycan content decreased and lysosomal position and size normalized. Treatment of MSD patient derived induced pluripotent stem cells (iPSC) differentiated into neuronal progenitor cells (NPC) resulted in a positive treatment response. Tazarotene and bexarotene act to ultimately increase the stability of FGE variants. The results lay the basis for future research on the development of a first therapeutic option for MSD patients.

Published in EMBO Molecular Medicine

ISSN: 1757-4676 (Print); 1757-4684 (Online)
Publisher: Springer Nature
Country of publisher: United Kingdom
LCC subjects: Medicine: Medicine (General); Science: Biology (General): Genetics
Website: https://www.embopress.org/journal/17574684

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Abstract

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