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Targeting androgen receptor stability and degradation: approaches for developing a therapy for spinal and bulbar muscular atrophy

Articolo
Data di Pubblicazione:
2025
Citazione:
Targeting androgen receptor stability and degradation: approaches for developing a therapy for spinal and bulbar muscular atrophy / R. Cristofani, B. Tedesco, V. Ferrari, M. Chierichetti, M. Cozzi, P. Pramaggiore, L. Cornaggia, A. Mohamed, E. Casarotto, M. Brodnanova, R. Magdalena, P. Koshal, M. Piccolella, V. Crippa, M. Galbiati, A. Poletti, P. Rusmini. - In: CELL COMMUNICATION AND SIGNALING. - ISSN 1478-811X. - 23:1(2025 Jul 17), pp. 1-15. [10.1186/s12964-025-02351-4]
Abstract:
: Conformational changes of proteins can occur due to mutations or stress conditions, altering their functionality through loss of physiological or gain of pathological function. A Protein Quality Control (PQC) system exists in cells to deal with the accumulation of misfolded proteins and aggregates, comprising a network of chaperones and degradative pathways to refold or remove the aberrant proteins. Protein misfolding and PQC system impairment lead to a broad range of diseases, including neurodegenerative and neuromuscular disorders, among them spinal and bulbar muscular atrophy (SBMA). SBMA is a neuromuscular disorder caused by a polyglutamine expansion (polyQ) in the androgen receptor (AR) protein. Expanded AR (ARexp) is highly prone to misfolding and aggregation, leading to its accumulation in affected tissues. Here, we summarise the dynamics that control AR protein stability and its degradation in physiological conditions. Next, we recapitulate the current knowledge of the molecular mechanisms of SBMA pathogenesis involving the PQC system. Finally, we provide an overview of promising approaches to SBMA intervention involving the modulation of PQC system functions to reduce ARexp accumulation and its toxic effects in affected cells.
Tipologia IRIS:
01 - Articolo su periodico
Keywords:
Androgen receptor; Autophagy; Degradation; Polyglutamine
Elenco autori:
R. Cristofani, B. Tedesco, V. Ferrari, M. Chierichetti, M. Cozzi, P. Pramaggiore, L. Cornaggia, A. Mohamed, E. Casarotto, M. Brodnanova, R. Magdalena, P. Koshal, M. Piccolella, V. Crippa, M. Galbiati, A. Poletti, P. Rusmini
Autori di Ateneo:
CHIERICHETTI MARTA ( autore )
CORNAGGIA LAURA ( autore )
COZZI MARTA ( autore )
CRIPPA VALERIA ( autore )
CRISTOFANI RICCARDO MARIA ( autore )
FERRARI VERONICA ( autore )
GALBIATI MARIARITA ( autore )
MAGDALENA PARRA ROCIO FERNANDA ( autore )
MOHAMED ALI AHMED MOHAMED ( autore )
POLETTI ANGELO ( autore )
PRAMAGGIORE PAOLA ( autore )
RUSMINI PAOLA ( autore )
TEDESCO BARBARA ( autore )
Link alla scheda completa:
https://air.unimi.it/handle/2434/1176336
Link al Full Text:
https://air.unimi.it/retrieve/handle/2434/1176336/3113634/s12964-025-02351-4.pdf
Progetto:
Alternative translation initiation as a novel strategy to block toxicity of the mutant Androgen Receptor in SBMA
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Settori (2)


Settore BIOS-06/A - Fisiologia

Settore BIOS-10/A - Biologia cellulare e applicata
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Realizzato con VIVO | Progettato da Cineca | 25.11.5.0