Translational research in neuroendocrine tumors: pitfalls and opportunities

Fecha de publicación: 06/04/2017

Autores de IIS La Fe

Ángel Agustín Segura Huerta

Autor

Participantes ajenos a IIS La Fe

Capdevila, J
Casanovas, O
Salazar, R
Castellano, D
Fuster, P
Aller, J
Garcia-Carbonero, R
Jimenez-Fonseca, P
Grande, E
Castano, JP

Grupos

Investigación Clínica y Traslacional en Cáncer

Leader

José Gómez Codina

Abstract

Interest in research on neuroendocrine tumors (NETs) has grown in the past 10 years, coinciding with improvements in our understanding of the molecular pathogenesis of NETs. In addition, NETs have become one of the most exciting settings for drug development. Two targeted agents for the management of advanced pancreatic NETs have been approved, but the development of targeted agents for NETs is limited by problems with both patient selection and demonstration of activity. In this review, we analyze these limitations and discuss ways to increase the predictive value of preclinical models for target discovery and drug development. The role of translational research and 'omics' methodologies is emphasized, with the final aim of developing personalized medicine. Because NETs usually grow slowly and metastatic tumors are found at easily accessible locations, and owing to improvements in techniques for liquid biopsies, NETs provide a unique opportunity to obtain tumor samples at all stages of the evolution of the disease and to adapt treatment to changes in tumor biology. Combining clinical and translational research is essential to achieve progress in the NET field. Slow growth and genetic stability limit and challenge both the availability and further development of preclinical models of NETs, one of the most crucial unmet research needs in the field. Finally, we suggest some useful approaches for improving clinical drug development for NETs: moving from classical RECIST-based response end points to survival parameters; searching for different criteria to define response rates (for example, antiangiogenic effects and metabolic responses); implementing randomized phase II studies to avoid single-arm phase II studies that produce limited data on drug efficacy; and using predictive biomarkers for patient selection.

Datos de la publicación

ISSN/ISSNe:: 0950-9232, 1476-5594
Tipo:: Review
Páginas:: 1899-1907
DOI:: 10.1038/onc.2016.316
Factor de Impacto:: 3,235 SCImago ℠
Cuartil:: Q1 SCImago ℠

Documentos

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Métricas

Filiaciones

Capdevila, J:: Univ Autonoma Barcelona, Vall dHebron Univ Hosp, VHIO, Med Oncol Dept, Passeig Vall dHebron 119-129, Barcelona 08035, Spain
Casanovas, O:: Inst Catalan Oncol IDIBELL, ProCURE Res Program, Barcelona, Spain
Salazar, R:: Univ Barcelona, Catalan Inst Oncol IDIBELL, Oncol Dept, Barcelona, Spain
Castellano, D:: Hosp Univ 12 Octubre, Oncol Dept, Madrid, Spain
Segura, A:: Hosp Univ & Politecn La Fe, Oncol Dept, Valencia, Spain
Fuster, P:: Hosp Univ Son Espases, Oncol Dept, Palma De Mallorca, Spain
Aller, J:: Puerta de Hierro Univ Hosp, Dept Endocrinol, Madrid, Spain
Garcia-Carbonero, R:: Hosp Univ Doce Octubre Ctr, Spanish Minist Sci & Innovat, Med Oncol Dept, RTICC,Inst Salud Carlos 3, Madrid, Spain
Jimenez-Fonseca, P:: Cent Asturias Univ Hosp, Dept Med Oncol, Oviedo, Spain
Grande, E:: Hosp Univ Ramon y Cajal, Oncol Dept, Madrid, Spain
Castano, JP:: Maimonides Inst Biomed Res Cordoba IMIBIC, Cordoba, Spain

Reina Sofia Univ Hosp, Cordoba, Spain

Univ Cordoba, Dept Cell Biol Physiol & Immunol, Cordoba, Spain

CIBER Fisiopatol Obesidad & Nutr, Cordoba, Spain