Genomic Landscape of Vinflunine Response in Metastatic Urothelial Cancer

Alejandra Bernardini; Marta Dueñas; María Cruz Martín-Soberon; Carolina Rubio; Cristian Suarez-Cabrera; Raquel Ruiz-Palomares; Ester Munera-Maravilla; Sara Lázaro; Iris Lodewijk; Daniel Rueda; David Gómez-Sánchez; Teresa Alonso-Gordoa; Javier Puente; Álvaro Pinto; Pilar González-Peramato; Carlos Aguado; Mercedes Herrera; Flora López; Victor M. G. Martinez; Lucía Morales; Daniel Castellano; Jesús M. Paramio; Guillermo de Velasco

doi:10.3390/cancers14020378

Cancers (Jan 2022)

Genomic Landscape of Vinflunine Response in Metastatic Urothelial Cancer

Alejandra Bernardini,
Marta Dueñas,
María Cruz Martín-Soberon,
Carolina Rubio,
Cristian Suarez-Cabrera,
Raquel Ruiz-Palomares,
Ester Munera-Maravilla,
Sara Lázaro,
Iris Lodewijk,
Daniel Rueda,
David Gómez-Sánchez,
Teresa Alonso-Gordoa,
Javier Puente,
Álvaro Pinto,
Pilar González-Peramato,
Carlos Aguado,
Mercedes Herrera,
Flora López,
Victor M. G. Martinez,
Lucía Morales,
Daniel Castellano,
Jesús M. Paramio,
Guillermo de Velasco

Affiliations

Alejandra Bernardini: Instituto de Investigación i+12, Hospital University “12 de Octubre”, 28040 Madrid, Spain
Marta Dueñas: Instituto de Investigación i+12, Hospital University “12 de Octubre”, 28040 Madrid, Spain
María Cruz Martín-Soberon: Instituto de Investigación i+12, Hospital University “12 de Octubre”, 28040 Madrid, Spain
Carolina Rubio: Instituto de Investigación i+12, Hospital University “12 de Octubre”, 28040 Madrid, Spain
Cristian Suarez-Cabrera: Instituto de Investigación i+12, Hospital University “12 de Octubre”, 28040 Madrid, Spain
Raquel Ruiz-Palomares: Instituto de Investigación i+12, Hospital University “12 de Octubre”, 28040 Madrid, Spain
Ester Munera-Maravilla: Instituto de Investigación i+12, Hospital University “12 de Octubre”, 28040 Madrid, Spain
Sara Lázaro: Unidad de Oncología Molecular, CIEMAT, 28045 Madrid, Spain
Iris Lodewijk: Instituto de Investigación i+12, Hospital University “12 de Octubre”, 28040 Madrid, Spain
Daniel Rueda: Instituto de Investigación i+12, Hospital University “12 de Octubre”, 28040 Madrid, Spain
David Gómez-Sánchez: Instituto de Investigación i+12, Hospital University “12 de Octubre”, 28040 Madrid, Spain
Teresa Alonso-Gordoa: Departamento de Oncología Médica, Hospital Ramón y Caja, 28034 Madrid, Spain
Javier Puente: Departamento de Oncología Médica, Hospital Clínico San Carlos, 28040 Madrid, Spain
Álvaro Pinto: Departamento de Oncología Médica, Hospital La Paz, 28046 Madrid, Spain
Pilar González-Peramato: Departamento de Oncología Médica, Hospital La Paz, 28046 Madrid, Spain
Carlos Aguado: Departamento de Oncología Médica, Hospital Clínico San Carlos, 28040 Madrid, Spain
Mercedes Herrera: Departamento de Oncología Médica, Hospital 12 de Octubre, 28040 Madrid, Spain
Flora López: Departamento de Oncología Médica, Hospital 12 de Octubre, 28040 Madrid, Spain
Victor M. G. Martinez: Instituto de Investigación i+12, Hospital University “12 de Octubre”, 28040 Madrid, Spain
Lucía Morales: Instituto de Investigación i+12, Hospital University “12 de Octubre”, 28040 Madrid, Spain
Daniel Castellano: Instituto de Investigación i+12, Hospital University “12 de Octubre”, 28040 Madrid, Spain
Jesús M. Paramio: Instituto de Investigación i+12, Hospital University “12 de Octubre”, 28040 Madrid, Spain
Guillermo de Velasco: Instituto de Investigación i+12, Hospital University “12 de Octubre”, 28040 Madrid, Spain

DOI: https://doi.org/10.3390/cancers14020378
Journal volume & issue: Vol. 14, no. 2
p. 378

Abstract

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Background and Aims: Metastatic urothelial carcinoma (mUC) remains an incurable disease with limited treatment options after platinum-based chemotherapy and immune checkpoint blockade (ICB). Vinflunine has shown a modest increase in overall survival and remains a therapeutic option for chemo- and immunotherapy refractory tumours. However, biomarkers that could identify responding patients to vinflunine and possible alternative therapies after failure to treatment are still missing. In this study, we aimed to identify potential genomic biomarkers of vinflunine response in mUC patient samples and potential management alternatives. Methods: Formalin-fixed paraffin-embedded samples of mUC patients (n = 23) from three university hospitals in Spain were used for genomic targeted-sequencing and transcriptome (using the Immune Profile panel by NanoString) analyses. Patients who received vinflunine after platinum-based chemotherapy failure were classified in non-responders (NR: progressive disease ≤ 3 months; n= 11) or responders (R: response ≥ 6 months; n = 12). Results: Genomic characterization revealed that the most common alteration, TP53 mutations, had comparable frequency in R (6/12; 50%) and NR (4/11; 36%). Non-synonymous mutations in KTM2C (4/12; 33.3%), PIK3CA (3/12; 25%) and ARID2 (3/12; 25%) were predominantly associated with response. No significant difference was observed in tumour mutational burden (TMB) between R and NR patients. The NR tumours showed increased expression of diverse immune-related genes and pathways, including various interferon gamma-related genes. We also identified increased MAGEA4 expression as a potential biomarker of non-responding tumours to vinflunine treatment. Conclusions: Our data may help to identify potential genomic biomarkers of response to vinflunine. Moreover, tumours refractory to vinflunine showed immune signatures potentially associated with response to ICB. Extensive validation studies, including longitudinal series, are needed to corroborate these findings.

Published in Cancers

ISSN: 2072-6694 (Online)
Publisher: MDPI AG
Country of publisher: Switzerland
LCC subjects: Medicine: Internal medicine: Neoplasms. Tumors. Oncology. Including cancer and carcinogens
Website: https://www.mdpi.com/journal/cancers/

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