Craniopharyngiomas are rare benign pathologies but clinically challenging tumours because of their intimate relationship with critical brain structures, leading to severe endocrine-deficiencies/comorbidities. Therefore, identifying alternative prognostic/therapeutic tools is crucial. Although dysregulated splicing is a molecular feature that characterizes almost all tumour/cancer types, the dysregulation of the components belonging to the molecular machinery controlling the splicing-process (spliceosome) remains unknown in craniopharyngiomas. Here, we uncover a profound dysregulation in the expression of relevant spliceosome-components and splicing-factors in craniopharyngiomas versus control non-tumour tissues, identifying PRPF8 and RAVER1 as key tumour suppressor factors associated with relevant oncogenic processes. Moreover, we demonstrate that the spliceosome activity inhibition using pladienolide-B in primary patient´s derived cell-cultures might serve as a potential therapeutic tool worth to be explored in humans. Altogether, our results demonstrate a drastic and clinically relevant spliceosome-associated molecular dysregulation in craniopharyngiomas, which could serve as a potential source of novel diagnostic/prognostic biomarkers and therapeutic targets.
Impaired splicing machinery in craniopharyngiomas unveils PRPF8 and RAVER1 as novel biomarkers and therapeutic targets.
颅咽管瘤中受损的剪接机制揭示了 PRPF8 和 RAVER1 作为新的生物标志物和治疗靶点
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作者:Fuentes-Fayos Antonio C, G-GarcÃa Miguel E, Sánchez-Medianero Teresa, Apps John, Flores-MartÃnez Ãlvaro, De la Rosa-Herencia Ana S, Gil-Duque Ignacio, Otto Georg, Venegas-Moreno Eva, Ruiz-Valdepeñas Eugenio Cárdenas, Herrera-MartÃnez Aura D, Solivera Juan, Gahete Manuel D, Cano David A, Ortega Rosa, Soto-Moreno Alfonso, Gálvez-Moreno MarÃa A, MartÃnez-Barberá Juan Pedro, Luque Raúl M
| 期刊: | Acta Neuropathologica Communications | 影响因子: | 5.700 |
| 时间: | 2025 | 起止号: | 2025 Jun 28; 13(1):142 |
| doi: | 10.1186/s40478-025-02040-w | 研究方向: | 肿瘤 |
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