Pesquisa | Biblioteca Virtual em Saúde

RarÎ³ -Foxa1 signaling promotes luminal identity in prostate progenitors and is disrupted in prostate cancer.

Felice, Dario De; Alaimo, Alessandro; Bressan, Davide; Genovesi, Sacha; Marmocchi, Elisa; Annesi, Nicole; Beccaceci, Giulia; Dalfovo, Davide; Cutrupi, Federico; Foletto, Veronica; Lorenzoni, Marco; Gandolfi, Francesco; Kannan, Srinivasaraghavan; Verma, Chandra S; Vasciaveo, Alessandro; Shen, Michael M; Romanel, Alessandro; Chiacchiera, Fulvio; Cambuli, Francesco; Lunardi, Andrea.

bioRxiv ; 2024 Mar 08.

Artigo em Inglês | MEDLINE | ID: mdl-38496627

RESUMO

Retinoic acid (RA) signaling is a master regulator of vertebrate development with crucial roles in directing body axis orientation and tissue differentiation, including in the reproductive system. However, a mechanistic understanding of how RA signaling promotes cell lineage identity in different tissues is often missing. Here, leveraging prostate organoid technology, we demonstrated that RA signaling orchestrates the commitment of adult mouse prostate progenitors to glandular identity, epithelial barrier integrity, and ultimately, proper specification of the prostatic lumen. Mechanistically, RA-dependent RARÎ³ activation promotes the expression of the pioneer factor Foxa1, which synergizes with the androgen pathway for proper luminal expansion, cytoarchitecture and function. FOXA1 nucleotide variants are common in human prostate and breast cancers and considered driver mutations, though their pathogenic mechanism is incompletely understood. Combining functional genetics experiments with structural modeling of FOXA1 folding and chromatin binding analyses, we discovered that FOXA1 F254E255 is a loss-of-function mutation leading to compromised transcriptional function and lack of luminal fate commitment of prostate progenitors. Overall, we define RA as a crucial instructive signal for glandular identity in adult prostate progenitors. We propose deregulation of vitamin A metabolism as a risk factor for benign and malignant prostate disease, and identified cancer associated FOXA1 indels affecting residue F254 as loss-of-function mutations promoting dedifferentiation of adult prostate progenitors. Summary: Retinoic acid signaling orchestrates luminal differentiation of adult prostate progenitors.

Sterile inflammation via TRPM8 RNA-dependent TLR3-NF-kB/IRF3 activation promotes antitumor immunity in prostate cancer.

Alaimo, Alessandro; Genovesi, Sacha; Annesi, Nicole; De Felice, Dario; Subedi, Saurav; Macchia, Alice; La Manna, Federico; Ciani, Yari; Vannuccini, Federico; Mugoni, Vera; Notarangelo, Michela; Libergoli, Michela; Broso, Francesca; Taulli, Riccardo; Ala, Ugo; Savino, Aurora; Cortese, Martina; Mirzaaghaei, Somayeh; Poli, Valeria; Bonapace, Ian Marc; Papotti, Mauro Giulio; Molinaro, Luca; Doglioni, Claudio; Caffo, Orazio; Anesi, Adriano; Nagler, Michael; Bertalot, Giovanni; Carbone, Francesco Giuseppe; Barbareschi, Mattia; Basso, Umberto; Dassi, Erik; Pizzato, Massimo; Romanel, Alessandro; Demichelis, Francesca; Kruithof-de Julio, Marianna; Lunardi, Andrea.

EMBO J ; 43(5): 780-805, 2024 Mar.

Artigo em Inglês | MEDLINE | ID: mdl-38316991

RESUMO

Inflammation is a common condition of prostate tissue, whose impact on carcinogenesis is highly debated. Microbial colonization is a well-documented cause of a small percentage of prostatitis cases, but it remains unclear what underlies the majority of sterile inflammation reported. Here, androgen- independent fluctuations of PSA expression in prostate cells have lead us to identify a prominent function of the Transient Receptor Potential Cation Channel Subfamily M Member 8 (TRPM8) gene in sterile inflammation. Prostate cells secret TRPM8 RNA into extracellular vesicles (EVs), which primes TLR3/NF-kB-mediated inflammatory signaling after EV endocytosis by epithelial cancer cells. Furthermore, prostate cancer xenografts expressing a translation-defective form of TRPM8 RNA contain less collagen type I in the extracellular matrix, significantly more infiltrating NK cells, and larger necrotic areas as compared to control xenografts. These findings imply sustained, androgen-independent expression of TRPM8 constitutes as a promoter of anticancer innate immunity, which may constitute a clinically relevant condition affecting prostate cancer prognosis.

Assuntos

Neoplasias da Próstata , Canais de Cátion TRPM , Humanos , Masculino , Androgênios , Inflamação/genética , Fator Regulador 3 de Interferon , Proteínas de Membrana , NF-kappa B/genética , Neoplasias da Próstata/genética , Receptor 3 Toll-Like/genética , Canais de Cátion TRPM/genética , Animais

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