Discovery of a new selective ERAP1 inhibitor for Hedgehog-dependent cancer treatment

Francesca Bufalieri; Antonino Cucinotta; Silvia Cammarone; Francesca Agnoli; Irene Basili; Giulia Ferri; Deborah Quaglio; Miriam Caimano; Anna Laura Capriotti; Carmela Maria Montone; Ludovica Lospinoso Severini; Patrizia Tempora; Silvia D’Amico; Francesca Juretich; Marta S. Semrau; Shirin Navacci; Marilisa Conenna; Rosa Bordone; Francesco Spallotta; Silvia Garavaglia; Paola Storici; Francesca Ghirga; Aldo Laganà; Franco Locatelli; Olivier Ayrault; Paola Infante; Bruno Botta; Mattia Mori; Doriana Fruci; Lucia Di Marcotullio

doi:10.1016/j.ymthe.2025.10.036

Discovery of a new selective ERAP1 inhibitor for Hedgehog-dependent cancer treatment

Francesca Bufalieri
, Antonino Cucinotta
, Silvia Cammarone
, Francesca Agnoli
, Irene Basili
, Giulia Ferri
, Deborah Quaglio
, Miriam Caimano
, Anna Laura Capriotti
, Carmela Maria Montone
, Ludovica Lospinoso Severini
, Patrizia Tempora
, Silvia D’Amico
, Francesca Juretich
, Marta S. Semrau
, Shirin Navacci
, Marilisa Conenna
, Rosa Bordone
, Francesco Spallotta
, Silvia Garavaglia

Paola Storici, Francesca Ghirga, Aldo Laganà, Franco Locatelli, Olivier Ayrault, Paola Infante, Bruno Botta, Mattia Mori, Doriana Fruci, Lucia Di Marcotullio

Dipartimento di Scienze del Farmaco

Risultato della ricerca: Contributo su rivista › Articolo in rivista › peer review

Abstract

Inappropriate activation of the Hedgehog (HH) signaling pathway drives the pathogenesis of several cancers, including medulloblastoma (MB), the most common malignant brain tumor in children. HH group MB (HH-MB) is highly heterogeneous and resistant to current treatments. Understanding the molecular events underlying the control of the HH pathway is critical for the development of more effective and tailored interventions. Endoplasmic reticulum aminopeptidase 1 (ERAP1), a key regulator of the immune response, has emerged as a promising therapeutic target for HH-MB, but the lack of clinically viable ERAP1 inhibitors has hindered progress in this area. Here, we identify canthin-6-one (N1) as a selective ERAP1 inhibitor. N1 binds directly to ERAP1 and disrupts its function in the HH pathway, resulting in reduced signaling. Specifically, N1 impairs the association of ERAP1 with the deubiquitinase USP47, promoting βTrCP protein stability and Gli1 degradation. Notably, HH-dependent cells genetically depleted for ERAP1 are insensitive to N1, confirming its specificity. Remarkably, N1 inhibits HH-MB growth in vitro and in vivo , crosses the blood-brain barrier, and improves survival in an HH-MB mouse model. These findings highlight N1 as a breakthrough ERAP1 inhibitor and provide a promising therapeutic option for the treatment of HH-dependent cancers.

Lingua originale	Inglese
pagine (da-a)	582-605
Numero di pagine	24
Rivista	Molecular Therapy
Volume	34
Numero di pubblicazione	1
DOI	https://doi.org/10.1016/j.ymthe.2025.10.036
Stato di pubblicazione	Pubblicato - 7 gen 2026

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10.1016/j.ymthe.2025.10.036

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Bufalieri, F., Cucinotta, A., Cammarone, S., Agnoli, F., Basili, I., Ferri, G., Quaglio, D., Caimano, M., Capriotti, A. L., Montone, C. M., Lospinoso Severini, L., Tempora, P., D’Amico, S., Juretich, F., Semrau, M. S., Navacci, S., Conenna, M., Bordone, R., Spallotta, F., ... Di Marcotullio, L. (2026). Discovery of a new selective ERAP1 inhibitor for Hedgehog-dependent cancer treatment. Molecular Therapy, 34(1), 582-605. https://doi.org/10.1016/j.ymthe.2025.10.036

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title = "Discovery of a new selective ERAP1 inhibitor for Hedgehog-dependent cancer treatment",

abstract = "Inappropriate activation of the Hedgehog (HH) signaling pathway drives the pathogenesis of several cancers, including medulloblastoma (MB), the most common malignant brain tumor in children. HH group MB (HH-MB) is highly heterogeneous and resistant to current treatments. Understanding the molecular events underlying the control of the HH pathway is critical for the development of more effective and tailored interventions. Endoplasmic reticulum aminopeptidase 1 (ERAP1), a key regulator of the immune response, has emerged as a promising therapeutic target for HH-MB, but the lack of clinically viable ERAP1 inhibitors has hindered progress in this area. Here, we identify canthin-6-one (N1) as a selective ERAP1 inhibitor. N1 binds directly to ERAP1 and disrupts its function in the HH pathway, resulting in reduced signaling. Specifically, N1 impairs the association of ERAP1 with the deubiquitinase USP47, promoting βTrCP protein stability and Gli1 degradation. Notably, HH-dependent cells genetically depleted for ERAP1 are insensitive to N1, confirming its specificity. Remarkably, N1 inhibits HH-MB growth in vitro and in vivo , crosses the blood-brain barrier, and improves survival in an HH-MB mouse model. These findings highlight N1 as a breakthrough ERAP1 inhibitor and provide a promising therapeutic option for the treatment of HH-dependent cancers.",

keywords = "ERAP1, Hedgehog pathway, cancer, chemical biology, medulloblastoma",

author = "Francesca Bufalieri and Antonino Cucinotta and Silvia Cammarone and Francesca Agnoli and Irene Basili and Giulia Ferri and Deborah Quaglio and Miriam Caimano and Capriotti, \{Anna Laura\} and Montone, \{Carmela Maria\} and \{Lospinoso Severini\}, Ludovica and Patrizia Tempora and Silvia D{\textquoteright}Amico and Francesca Juretich and Semrau, \{Marta S.\} and Shirin Navacci and Marilisa Conenna and Rosa Bordone and Francesco Spallotta and Silvia Garavaglia and Paola Storici and Francesca Ghirga and Aldo Lagan{\`a} and Franco Locatelli and Olivier Ayrault and Paola Infante and Bruno Botta and Mattia Mori and Doriana Fruci and \{Di Marcotullio\}, Lucia",

note = "Publisher Copyright: {\textcopyright} 2025 The American Society of Gene and Cell Therapy.",

year = "2026",

month = jan,

day = "7",

doi = "10.1016/j.ymthe.2025.10.036",

language = "English",

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pages = "582--605",

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Bufalieri, F, Cucinotta, A, Cammarone, S, Agnoli, F, Basili, I, Ferri, G, Quaglio, D, Caimano, M, Capriotti, AL, Montone, CM, Lospinoso Severini, L, Tempora, P, D’Amico, S, Juretich, F, Semrau, MS, Navacci, S, Conenna, M, Bordone, R, Spallotta, F, Garavaglia, S, Storici, P, Ghirga, F, Laganà, A, Locatelli, F, Ayrault, O, Infante, P, Botta, B, Mori, M, Fruci, D & Di Marcotullio, L 2026, 'Discovery of a new selective ERAP1 inhibitor for Hedgehog-dependent cancer treatment', Molecular Therapy, vol. 34, n. 1, pagg. 582-605. https://doi.org/10.1016/j.ymthe.2025.10.036

TY - JOUR

T1 - Discovery of a new selective ERAP1 inhibitor for Hedgehog-dependent cancer treatment

AU - Bufalieri, Francesca

AU - Cucinotta, Antonino

AU - Cammarone, Silvia

AU - Agnoli, Francesca

AU - Basili, Irene

AU - Ferri, Giulia

AU - Quaglio, Deborah

AU - Caimano, Miriam

AU - Capriotti, Anna Laura

AU - Montone, Carmela Maria

AU - Lospinoso Severini, Ludovica

AU - Tempora, Patrizia

AU - D’Amico, Silvia

AU - Juretich, Francesca

AU - Semrau, Marta S.

AU - Navacci, Shirin

AU - Conenna, Marilisa

AU - Bordone, Rosa

AU - Spallotta, Francesco

AU - Garavaglia, Silvia

AU - Storici, Paola

AU - Ghirga, Francesca

AU - Laganà, Aldo

AU - Locatelli, Franco

AU - Ayrault, Olivier

AU - Infante, Paola

AU - Botta, Bruno

AU - Mori, Mattia

AU - Fruci, Doriana

AU - Di Marcotullio, Lucia

PY - 2026/1/7

Y1 - 2026/1/7

N2 - Inappropriate activation of the Hedgehog (HH) signaling pathway drives the pathogenesis of several cancers, including medulloblastoma (MB), the most common malignant brain tumor in children. HH group MB (HH-MB) is highly heterogeneous and resistant to current treatments. Understanding the molecular events underlying the control of the HH pathway is critical for the development of more effective and tailored interventions. Endoplasmic reticulum aminopeptidase 1 (ERAP1), a key regulator of the immune response, has emerged as a promising therapeutic target for HH-MB, but the lack of clinically viable ERAP1 inhibitors has hindered progress in this area. Here, we identify canthin-6-one (N1) as a selective ERAP1 inhibitor. N1 binds directly to ERAP1 and disrupts its function in the HH pathway, resulting in reduced signaling. Specifically, N1 impairs the association of ERAP1 with the deubiquitinase USP47, promoting βTrCP protein stability and Gli1 degradation. Notably, HH-dependent cells genetically depleted for ERAP1 are insensitive to N1, confirming its specificity. Remarkably, N1 inhibits HH-MB growth in vitro and in vivo , crosses the blood-brain barrier, and improves survival in an HH-MB mouse model. These findings highlight N1 as a breakthrough ERAP1 inhibitor and provide a promising therapeutic option for the treatment of HH-dependent cancers.

AB - Inappropriate activation of the Hedgehog (HH) signaling pathway drives the pathogenesis of several cancers, including medulloblastoma (MB), the most common malignant brain tumor in children. HH group MB (HH-MB) is highly heterogeneous and resistant to current treatments. Understanding the molecular events underlying the control of the HH pathway is critical for the development of more effective and tailored interventions. Endoplasmic reticulum aminopeptidase 1 (ERAP1), a key regulator of the immune response, has emerged as a promising therapeutic target for HH-MB, but the lack of clinically viable ERAP1 inhibitors has hindered progress in this area. Here, we identify canthin-6-one (N1) as a selective ERAP1 inhibitor. N1 binds directly to ERAP1 and disrupts its function in the HH pathway, resulting in reduced signaling. Specifically, N1 impairs the association of ERAP1 with the deubiquitinase USP47, promoting βTrCP protein stability and Gli1 degradation. Notably, HH-dependent cells genetically depleted for ERAP1 are insensitive to N1, confirming its specificity. Remarkably, N1 inhibits HH-MB growth in vitro and in vivo , crosses the blood-brain barrier, and improves survival in an HH-MB mouse model. These findings highlight N1 as a breakthrough ERAP1 inhibitor and provide a promising therapeutic option for the treatment of HH-dependent cancers.

KW - ERAP1

KW - Hedgehog pathway

KW - cancer

KW - chemical biology

KW - medulloblastoma

UR - https://www.scopus.com/pages/publications/105024998751

U2 - 10.1016/j.ymthe.2025.10.036

DO - 10.1016/j.ymthe.2025.10.036

M3 - Article

SN - 1525-0016

VL - 34

SP - 582

EP - 605

JO - Molecular Therapy

JF - Molecular Therapy

IS - 1

ER -

Discovery of a new selective ERAP1 inhibitor for Hedgehog-dependent cancer treatment

Abstract

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