Molecular Therapy: Oncology (Dec 2024)

Clinical value of circulating splicing factors in prostate cancer: SRRM1 as a novel predictive biomarker and therapeutic target

  • Antonio J. Montero-Hidalgo,
  • Enrique Gómez-Gómez,
  • Manuel Galán-Cañete,
  • Francisco Porcel-Pastrana,
  • Jesús M. Pérez-Gómez,
  • María Ortega-Bellido,
  • Julia Carrasco-Valiente,
  • Laura Chamorro-Castillo,
  • Juan P. Campos-Hernández,
  • Oriol A. Rangel-Zuñiga,
  • Teresa González-Serrano,
  • Rafael Sánchez-Sánchez,
  • André Sarmento-Cabral,
  • Manuel D. Gahete,
  • Juan M. Jiménez-Vacas,
  • Raúl M. Luque

Journal volume & issue
Vol. 32, no. 4
p. 200910

Abstract

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Prostate cancer (PCa) is the second most common cancer among men worldwide. The main screening tool remains the prostate-specific antigen (PSA), which shows significant limitations, including poor sensitivity/specificity. Therefore, establishing accurate non-invasive diagnostic biomarkers remains an unmet clinical need in PCa. In this context, the splicing process dysregulation represents a PCa hallmark. Here, plasma SRRM1, SNRNP200, and SRSF3 levels, previously identified to play a pathophysiological role in PCa, were determined in control individuals (n = 40) and PCa patients (n = 166). We found that plasma SRRM1 and SNRNP200 levels were elevated in PCa patients and discriminated between control individuals and PCa patients. High plasma SRRM1 levels were associated with a shorter castration-resistant PCa-free survival and correlated with androgen-receptor (AR)/AR-splicing variant 7 (AR-V7) expression levels and activity in PCa tissues. Therefore, the functional and molecular effects of in vivo SRRM1 silencing were then tested in 22Rv1-derived xenograft tumors. In vivo SRRM1 silencing reduced aggressiveness features and altered AR/AR-V7 activity. Our data reveal that SRRM1 holds potential as a non-invasive diagnostic and prognostic biomarker and novel therapeutic target in PCa, offering a clinically relevant opportunity worth exploring in humans.

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