The WNK1–ERK5 route plays a pathophysiological role in ovarian cancer and limits therapeutic efficacy of trametinib-Reference-Cited by-同舟云学术

The WNK1–ERK5 route plays a pathophysiological role in ovarian cancer and limits therapeutic efficacy of trametinib

Published:2023-04 Issue:4 Volume:13 Page:
ISSN:2001-1326
Container-title:Clinical and Translational Medicine
language:en
Short-container-title:Clinical & Translational Med

Author:

Sánchez‐Fdez Adrián¹²³⁴^ORCID,Matilla‐Almazán Sofía¹²³^ORCID,Montero Juan Carlos¹²³⁵,Del Carmen Sofía²⁵,Abad Mar²⁵,García‐Alonso Sara¹²³,Bhattacharya Somshuvra⁶,Calar Kristin⁶,de la Puente Pilar⁶⁷,Ocaña Alberto⁸⁹,Pandiella Atanasio¹²³^ORCID,Esparís‐Ogando Azucena¹²³^ORCID

Affiliation:

1. Instituto de Biología Molecular y Celular del Cáncer‐CSIC Salamanca Spain

2. Instituto de Investigación Biomédica de Salamanca (IBSAL) Salamanca Spain

3. Centro de Investigación Biomédica en Red de Cáncer (CIBERONC) Salamanca Spain

4. Moores Cancer Center, University of California San Diego La Jolla CA USA

5. Department of Pathology University Hospital of Salamanca Salamanca Spain

6. Cancer Biology and Immunotherapies Group Sanford Research Sioux Falls South Dakota USA

7. Department of Surgery Sanford School of Medicine, University of South Dakota Sioux Falls South Dakota USA

8. Experimental Therapeutics Unit CRIS‐Cancer Hospital Clínico San Carlos and CIBERONC Madrid Spain

9. Universidad de Castilla La Mancha, Castilla La Mancha Albacete Spain

Abstract

AbstractBackgroundThe dismal prognosis of advanced ovarian cancer calls for the development of novel therapies to improve disease outcome. In this regard, we set out to discover new molecular entities and to assess the preclinical effectiveness of their targeting.MethodsCell lines, mice and human ovarian cancer samples were used. Proteome profiling of human phosphokinases, in silico genomic analyses, genetic (shRNA and CRISPR/Cas9) and pharmacological strategies as well as an ex vivo human preclinical model were performed.ResultsWe identified WNK1 as a highly phosphorylated protein in ovarian cancer and found that its activation or high expression had a negative impact on patients’ survival. Genomic analyses showed amplification of WNK1 in human ovarian tumours. Mechanistically, we demonstrate that WNK1 exerted its action through the MEK5–ERK5 signalling module in ovarian cancer. Loss of function, genetic or pharmacological experiments, demonstrated anti‐proliferative and anti‐tumoural effects of the targeting of the WNK1–MEK5–ERK5 route. Additional studies showed that this pathway modulated the anti‐tumoural properties of the MEK1/2 inhibitor trametinib. Thus, treatment with trametinib activated the WNK1–MEK5–ERK5 route, raising the possibility that this effect may limit the therapeutic benefit of ERK1/2 targeting in ovarian cancer. Moreover, in different experimental settings, including an ex vivo patient‐derived model consisting of ovarian cancer cells cultured with autologous patient sera, we show that inhibition of WNK1 or MEK5 increased the anti‐proliferative and anti‐tumour efficacy of trametinib.ConclusionsThe present study uncovers the participation of WNK1–MEK5–ERK5 axis in ovarian cancer pathophysiology, opening the possibility of acting on this pathway with therapeutic purposes. Another important finding of the present study was the activation of that signalling axis by trametinib, bypassing the anti‐tumoural efficacy of this drug. That fact should be considered in the context of the use of trametinib in ovarian cancer.

Funder

National Institute of General Medical Sciences

Junta de Castilla y León

Publisher

Wiley

Subject

Molecular Medicine,Medicine (miscellaneous)

Link

https://onlinelibrary.wiley.com/doi/pdf/10.1002/ctm2.1217

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