TY - JOUR
T1 - TRIB3 silencing promotes the downregulation of Akt pathway and PAX3-FOXO1 in high-risk rhabdomyosarcoma
AU - Gallo-Oller, Gabriel
AU - Pons, Guillem
AU - Sansa-Girona, Júlia
AU - Navarro, Natalia
AU - Zarzosa, Patricia
AU - García-Gilabert, Lia
AU - Cabré-Fernandez, Paula
AU - Guillén Burrieza, Gabriela
AU - Valero-Arrese, Lorena
AU - Segura, Miguel F
AU - Lizcano, José M
AU - Sánchez de Toledo, José
AU - Moreno, Lucas
AU - Gallego, Soledad
AU - Roma, Josep
N1 - © 2024. The Author(s).
PY - 2024/4/5
Y1 - 2024/4/5
N2 - Rhabdomyosarcoma (RMS), such as other childhood tumors, has witnessed treatment advancements in recent years. However, high-risk patients continue to face poor survival rates, often attributed to the presence of the PAX3/7-FOXO1 fusion proteins, which has been associated with metastasis and treatment resistance. Despite efforts to directly target these chimeric proteins, clinical success remains elusive. In this study, the main aim was to address this challenge by investigating regulators of FOXO1. Specifically, we focused on TRIB3, a potential regulator of the fusion protein in RMS. Our findings revealed a prominent TRIB3 expression in RMS tumors, highlighting its correlation with the presence of fusion protein. By conducting TRIB3 genetic inhibition experiments, we observed an impairment on cell proliferation. Notably, the knockdown of TRIB3 led to a decrease in PAX3-FOXO1 and its target genes at protein level, accompanied by a reduction in the activity of the Akt signaling pathway. Additionally, inducible silencing of TRIB3 significantly delayed tumor growth and improved overall survival in vivo. Based on our analysis, we propose that TRIB3 holds therapeutic potential for treating the most aggressive subtype of RMS. The findings herein reported contribute to our understanding of the underlying molecular mechanisms driving RMS progression and provide novel insights into the potential use of TRIB3 as a therapeutic intervention for high-risk RMS patients.
AB - Rhabdomyosarcoma (RMS), such as other childhood tumors, has witnessed treatment advancements in recent years. However, high-risk patients continue to face poor survival rates, often attributed to the presence of the PAX3/7-FOXO1 fusion proteins, which has been associated with metastasis and treatment resistance. Despite efforts to directly target these chimeric proteins, clinical success remains elusive. In this study, the main aim was to address this challenge by investigating regulators of FOXO1. Specifically, we focused on TRIB3, a potential regulator of the fusion protein in RMS. Our findings revealed a prominent TRIB3 expression in RMS tumors, highlighting its correlation with the presence of fusion protein. By conducting TRIB3 genetic inhibition experiments, we observed an impairment on cell proliferation. Notably, the knockdown of TRIB3 led to a decrease in PAX3-FOXO1 and its target genes at protein level, accompanied by a reduction in the activity of the Akt signaling pathway. Additionally, inducible silencing of TRIB3 significantly delayed tumor growth and improved overall survival in vivo. Based on our analysis, we propose that TRIB3 holds therapeutic potential for treating the most aggressive subtype of RMS. The findings herein reported contribute to our understanding of the underlying molecular mechanisms driving RMS progression and provide novel insights into the potential use of TRIB3 as a therapeutic intervention for high-risk RMS patients.
KW - TRIB3
KW - Fusion protein
KW - PAX3-FOXO1
KW - Akt
KW - Rhabdomyosarcoma
KW - Pax3-foxo1
KW - Trib3
KW - TRIB3
KW - Fusion protein
KW - PAX3-FOXO1
KW - Akt
KW - Rhabdomyosarcoma
KW - TRIB3
KW - Fusion protein
KW - PAX3-FOXO1
KW - Akt
KW - Rhabdomyosarcoma
UR - https://www.mendeley.com/catalogue/7cda97ec-12f1-3e54-bd22-ce228195a4dd/
UR - http://www.scopus.com/inward/record.url?scp=85203339855&partnerID=8YFLogxK
UR - https://portalrecerca.uab.cat/en/publications/82b9e27b-30bf-43fc-8ac9-cd6d5013bd3d
U2 - 10.1186/s40164-024-00503-9
DO - 10.1186/s40164-024-00503-9
M3 - Article
C2 - 38581035
SN - 2162-3619
VL - 13
JO - Experimental Hematology & Oncology
JF - Experimental Hematology & Oncology
IS - 1
M1 - 38
ER -