[Translated article] Genetic variants and enzyme activity in citidin deaminase: Relationship with capecitabine toxicity and recommendation for dose adjustment

Paula Castro-Sánchez; Mª Amparo Talens-Bolós; María José Prieto-Castelló; Loreto Pitaluga-Poveda; Juan Antonio Barrera-Ramírez; Andrés Corno-Caparrós

doi:10.1016/j.farma.2023.03.004

[Translated article] Genetic variants and enzyme activity in citidin deaminase: Relationship with capecitabine toxicity and recommendation for dose adjustment

Farm Hosp. 2023 May-Jun;47(3):T127-T132. doi: 10.1016/j.farma.2023.03.004. Epub 2023 May 3.

[Article in English, Spanish]

Authors

Paula Castro-Sánchez¹, Mª Amparo Talens-Bolós², María José Prieto-Castelló³, Loreto Pitaluga-Poveda³, Juan Antonio Barrera-Ramírez², Andrés Corno-Caparrós⁴

Affiliations

¹ Universidad Miguel Hernández de Elche, San Juan de Alicante, Spain. Electronic address: paulacastrosanchez90@gmail.com.
² Hospital General Universitario de Elda, Elda, Spain.
³ Universidad Miguel Hernández de Elche, San Juan de Alicante, Spain.
⁴ Laboratorio de Análisis Genéticos ANCOR, Alicante, Spain.

PMID: 37147242
DOI: 10.1016/j.farma.2023.03.004

Abstract

Objective: Capecitabine, an antineoplastic drug used in the treatment of breast and colon cancer, can cause severe, even fatal toxicity in some patients. The interindividual variability of this toxicity is largely due to genetic variations in target genes and enzymes of metabolism of this drug, such as Thymidylate Synthase (TS) and Dihydropyrimidine Dehydrogenase (DPD). The enzyme Cytidine Deaminase (CDA), involved in the activation of capecitabine, also has several variants associated with an increased risk of toxicity to treatment, although its role as a biomarker is not yet clearly defined. Therefore, our main objective is to study the association between the presence of genetic variants in CDA gen, CDA enzymatic activity and the development of severe toxicity in patients treated with capecitabine whose initial dose was adjusted based on the genetic profile of the DPD gen (DPYD).

Method: Prospective multicenter observational cohort study, focused on the analysis of the genotype-phenotype association of the CDA enzyme. After the experimental phase, an algorithm will be developed to determine the dose adjustment needed to reduce the risk of treatment toxicity according to CDA genotype, developing a Clinical Guide for capecitabine dosing according to genetic variants in DPYD and CDA. Based on this guide, a Bioinformatics Tool will be created to generate the pharmacotherapeutic report automatically, facilitating the implementation of pharmacogenetic advice in clinical practice. This tool will be a great support in making pharmacotherapeutic decisions based on the patient's genetic profile, incorporating precision medicine into clinical routine. Once the usefulness of this tool has been validated, it will be offered free of charge to facilitate the implementation of pharmacogenetics in hospital centers and equitably benefit all patients on capecitabine treatment.

Keywords: Capecitabina; Capecitabine; Citidin deaminase; Citidin desaminasa; Clinical protocols; Farmacogenética; Medicina de precisión; Pharmacogenetics; Precision medicine; Protocolos clínicos; Toxicidad; Toxicity.

Publication types

Observational Study
Multicenter Study

MeSH terms

Antimetabolites, Antineoplastic* / therapeutic use
Capecitabine
Dihydrouracil Dehydrogenase (NADP) / genetics
Fluorouracil* / adverse effects
Genotype
Prospective Studies

Substances

Capecitabine
Antimetabolites, Antineoplastic
Fluorouracil
Dihydrouracil Dehydrogenase (NADP)