The Polemic Diagnostic Role of TP53 Mutations in Liquid Biopsies from Breast, Colon and Lung Cancers
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Garrido Navas, María del Carmen; García Díaz, Abel; Molina Vallejo, María Pilar; González Martínez, Coral; Alcaide Lucena, Miriam; Cañas García, Inés; Bayarri, Clara; Delgado, Juan Ramón; González Rodríguez, Encarnación; Lorente Acosta, José Antonio; Serrano, María JoséEditorial
Mdpi
Materia
TP53 mutations Liquid biopsies cfDNA CTC Issue Concordances
Date
2020-11-12Referencia bibliográfica
Garrido-Navas, M. C., García-Díaz, A., Molina-Vallejo, M. P., González-Martínez, C., Alcaide Lucena, M., Cañas-García, I., ... & Serrano, M. J. (2020). The Polemic Diagnostic Role of TP53 Mutations in Liquid Biopsies from Breast, Colon and Lung Cancers. Cancers, 12(11), 3343. [doi:10.3390/cancers12113343]
Abstract
Simple Summary: Most solid tumors share mutations in TP53 that is thus considered one of the main
cancer driver genes. Mutations in TP53 occur very early during tumor development, so their
identification helps in diagnosing cancer. Furthermore, knowing in advance the TP53 mutation
status might help guiding targeted treatments against this gene. However, this analysis is mainly
performed in tissue samples, that is, solid biopsies, being an invasive technique. Contrarily, liquid
biopsies, consisting of the analysis of blood samples, are non-invasive, can be performed repeatedly,
helping in monitoring the patient evolution, and might be useful in early stages when the tumor is
not yet detected by other technologies. Here, we review the main studies conducted on two types of
liquid biopsies: circulating tumor cells and cell-free DNA.We discuss the main findings regarding
TP53 mutation analysis, the clinical utility of this information and some controversies arising from
the study of liquid biopsies compared to tissue samples, and we finish by suggesting future directions
within this field.
Abstract: Being minimally invasive and thus allowing repeated measures over time, liquid biopsies
are taking over traditional solid biopsies in certain circumstances such as those for unreachable
tumors, very early stages or treatment monitoring. However, regarding TP53 mutation status analysis,
liquid biopsies have not yet substituted tissue samples, mainly due to the lack of concordance between
the two types of biopsies. This needs to be examined in a study-dependent manner, taking into
account the particular type of liquid biopsy analyzed, that is, circulating tumor cells (CTCs) or cell-free
DNA (cfDNA), its involvement in the tumor biology and evolution and, finally, the technology
used to analyze each biopsy type. Here, we review the main studies analyzing TP53 mutations in either CTCs or cfDNA in the three more prevalent solid tumors: breast, colon and lung cancers.
We evaluate the correlation for mutation status between liquid biopsies and tumor tissue, suggesting
possible sources of discrepancies, as well as evaluating the clinical utility of using liquid biopsies for
the analysis of TP53 mutation status and the future actions that need to be undertaken to make liquid
biopsy analysis a reality for the evaluation of TP53 mutations.