Targeting S100A4 with niclosamide attenuates inflammatory and profibrotic pathways in models of amyotrophic lateral sclerosis

Martina Milani; Eleonora Mammarella; Simona Rossi; Chiara Miele; Serena Lattante; Mario Sabatelli; Mauro Cozzolino; Nadia D’Ambrosi; Savina Apolloni

doi:10.1186/s12974-021-02184-1

Journal of Neuroinflammation (Jun 2021)

Targeting S100A4 with niclosamide attenuates inflammatory and profibrotic pathways in models of amyotrophic lateral sclerosis

Martina Milani,
Eleonora Mammarella,
Simona Rossi,
Chiara Miele,
Serena Lattante,
Mario Sabatelli,
Mauro Cozzolino,
Nadia D’Ambrosi,
Savina Apolloni

Affiliations

Martina Milani: Department of Biology, University of Rome “Tor Vergata”
Eleonora Mammarella: Department of Biology, University of Rome “Tor Vergata”
Simona Rossi: Institute of Translational Pharmacology, CNR
Chiara Miele: Department of Biology, University of Rome “Tor Vergata”
Serena Lattante: Unità Operativa Complessa di Genetica Medica, Fondazione Policlinico Universitario A. Gemelli IRCCS
Mario Sabatelli: Unità Operativa Complessa di Neurologia, Fondazione Policlinico Universitario A. Gemelli IRCCS
Mauro Cozzolino: Institute of Translational Pharmacology, CNR
Nadia D’Ambrosi: Department of Biology, University of Rome “Tor Vergata”
Savina Apolloni: Department of Biology, University of Rome “Tor Vergata”

DOI: https://doi.org/10.1186/s12974-021-02184-1
Journal volume & issue: Vol. 18, no. 1
pp. 1 – 16

Abstract

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Abstract Background An increasing number of studies evidences that amyotrophic lateral sclerosis (ALS) is characterized by extensive alterations in different cell types and in different regions besides the CNS. We previously reported the upregulation in ALS models of a gene called fibroblast-specific protein-1 or S100A4, recognized as a pro-inflammatory and profibrotic factor. Since inflammation and fibrosis are often mutual-sustaining events that contribute to establish a hostile environment for organ functions, the comprehension of the elements responsible for these interconnected pathways is crucial to disclose novel aspects involved in ALS pathology. Methods Here, we employed fibroblasts derived from ALS patients harboring the C9orf72 hexanucleotide repeat expansion and ALS patients with no mutations in known ALS-associated genes and we downregulated S100A4 using siRNA or the S100A4 transcriptional inhibitor niclosamide. Mice overexpressing human FUS were adopted to assess the effects of niclosamide in vivo on ALS pathology. Results We demonstrated that S100A4 underlies impaired autophagy and a profibrotic phenotype, which characterize ALS fibroblasts. Indeed, its inhibition reduces inflammatory, autophagic, and profibrotic pathways in ALS fibroblasts, and interferes with different markers known as pathogenic in the disease, such as mTOR, SQSTM1/p62, STAT3, α-SMA, and NF-κB. Importantly, niclosamide in vivo treatment of ALS-FUS mice reduces the expression of S100A4, α-SMA, and PDGFRβ in the spinal cord, as well as gliosis in central and peripheral nervous tissues, together with axonal impairment and displays beneficial effects on muscle atrophy, by promoting muscle regeneration and reducing fibrosis. Conclusion Our findings show that S100A4 has a role in ALS-related mechanisms, and that drugs such as niclosamide which are able to target inflammatory and fibrotic pathways could represent promising pharmacological tools for ALS.

Published in Journal of Neuroinflammation

ISSN: 1742-2094 (Online)
Publisher: BMC
Country of publisher: United Kingdom
LCC subjects: Medicine: Internal medicine: Neurosciences. Biological psychiatry. Neuropsychiatry: Neurology. Diseases of the nervous system
Website: https://jneuroinflammation.biomedcentral.com/

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