Neuroinflammation is one of the major players in amyotrophic lateral sclerosis (ALS) pathogenesis, and astrocytes are significantly involved in this process. The astrocytic protein S100B can be released in pathological states activating the receptor for advanced glycation end products (RAGE). Different indications point to an aberrant expression of S100B and RAGE in ALS. In this work, we observed that S100B and RAGE are progressively and selectively upregulated in astrocytes of diseased rats with a tissue-specific timing pattern, correlated to the level of neurodegeneration. The expression of the full-length and soluble RAGE isoforms could also be linked to the degree of tissue damage. The mere presence of mutant SOD1 is able to increase the intracellular levels and release S100B from astrocytes, suggesting the possibility that an increased astrocytic S100B expression might be an early occurring event in the disease. Finally, our findings indicate that the protein may exert a proinflammatory role in ALS, since its inhibition in astrocytes derived from SOD1G93Amice limits the expression of reactivity-linked/proinflammatory genes. Thus, our results propose the S100B-RAGE axis as an effective contributor to the pathogenesis of the disease, suggesting its blockade as a rational target for a therapeutic intervention in ALS.

Serrano, A., Donno, C., Giannetti, S., Perić, M., Andjus, P., D'Ambrosi, N., et al. (2017). The Astrocytic S100B Protein with Its Receptor RAGE Is Aberrantly Expressed in SOD1G93AModels, and Its Inhibition Decreases the Expression of Proinflammatory Genes. MEDIATORS OF INFLAMMATION, 2017 [10.1155/2017/1626204].

The Astrocytic S100B Protein with Its Receptor RAGE Is Aberrantly Expressed in SOD1G93AModels, and Its Inhibition Decreases the Expression of Proinflammatory Genes

D'Ambrosi, Nadia
;
2017-01-01

Abstract

Neuroinflammation is one of the major players in amyotrophic lateral sclerosis (ALS) pathogenesis, and astrocytes are significantly involved in this process. The astrocytic protein S100B can be released in pathological states activating the receptor for advanced glycation end products (RAGE). Different indications point to an aberrant expression of S100B and RAGE in ALS. In this work, we observed that S100B and RAGE are progressively and selectively upregulated in astrocytes of diseased rats with a tissue-specific timing pattern, correlated to the level of neurodegeneration. The expression of the full-length and soluble RAGE isoforms could also be linked to the degree of tissue damage. The mere presence of mutant SOD1 is able to increase the intracellular levels and release S100B from astrocytes, suggesting the possibility that an increased astrocytic S100B expression might be an early occurring event in the disease. Finally, our findings indicate that the protein may exert a proinflammatory role in ALS, since its inhibition in astrocytes derived from SOD1G93Amice limits the expression of reactivity-linked/proinflammatory genes. Thus, our results propose the S100B-RAGE axis as an effective contributor to the pathogenesis of the disease, suggesting its blockade as a rational target for a therapeutic intervention in ALS.
2017
Pubblicato
Rilevanza internazionale
Articolo
Esperti anonimi
Settore BIO/10 - BIOCHIMICA
English
Con Impact Factor ISI
Animals; Animals, Genetically Modified; Astrocytes; Blotting, Western; Cells, Cultured; Electrophoresis, Polyacrylamide Gel; Enzyme-Linked Immunosorbent Assay; Male; Microscopy, Fluorescence; Rats; Receptor for Advanced Glycation End Products; S100 Calcium Binding Protein beta Subunit; Superoxide Dismutase-1; Immunology; Cell Biology
https://www.hindawi.com/journals/mi/2017/1626204/#references
Serrano, A., Donno, C., Giannetti, S., Perić, M., Andjus, P., D'Ambrosi, N., et al. (2017). The Astrocytic S100B Protein with Its Receptor RAGE Is Aberrantly Expressed in SOD1G93AModels, and Its Inhibition Decreases the Expression of Proinflammatory Genes. MEDIATORS OF INFLAMMATION, 2017 [10.1155/2017/1626204].
Serrano, A; Donno, C; Giannetti, S; Perić, M; Andjus, P; D'Ambrosi, N; Michetti, F
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/2108/205553
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