Circulating tumor DNA for monitoring classic Hodgkin lymphoma patients: Correlation with FDG‐PET/CT

Sara Fernández; Laura Cereceda; Eva Díaz; Sasha Figueroa; Laura Reguera; Victoria Menéndez; José L. Solórzano; Carlos Montalbán; Mónica Estévez; Juan F. García

doi:10.1002/jha2.826

eJHaem (Feb 2024)

Circulating tumor DNA for monitoring classic Hodgkin lymphoma patients: Correlation with FDG‐PET/CT

Sara Fernández,
Laura Cereceda,
Eva Díaz,
Sasha Figueroa,
Laura Reguera,
Victoria Menéndez,
José L. Solórzano,
Carlos Montalbán,
Mónica Estévez,
Juan F. García

Affiliations

Sara Fernández: Translational Research, Fundación MD Anderson International España S.L. Madrid Madrid Spain
Laura Cereceda: Translational Research, Fundación MD Anderson International España S.L. Madrid Madrid Spain
Eva Díaz: Translational Research, Fundación MD Anderson International España S.L. Madrid Madrid Spain
Sasha Figueroa: Translational Research, Fundación MD Anderson International España S.L. Madrid Madrid Spain
Laura Reguera: Nuclear Medicine Department MD Anderson Cancer Center Madrid Madrid Spain
Victoria Menéndez: Translational Research, Fundación MD Anderson International España S.L. Madrid Madrid Spain
José L. Solórzano: Pathology Department MD Anderson Cancer Center Madrid Madrid Spain
Carlos Montalbán: Hematology Department MD Anderson Cancer Center Madrid Madrid Spain
Mónica Estévez: Hematology Department MD Anderson Cancer Center Madrid Madrid Spain
Juan F. García: Translational Research, Fundación MD Anderson International España S.L. Madrid Madrid Spain

DOI: https://doi.org/10.1002/jha2.826
Journal volume & issue: Vol. 5, no. 1
pp. 70 – 75

Abstract

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Abstract The value of circulating tumor DNA (ctDNA) as a biomarker of disease activity in classic Hodgkin lymphoma (cHL) patients has not yet been well established. By profiling primary tumors and ctDNA, we identified common variants between primary tumors and longitudinal plasma samples in most of the cases, confirming high spatial and temporal heterogeneity. Although ctDNA analyses mirrored HRS cell genetics overall, the prevalence of variants shows that none of them can be used as a single biomarker. Conversely, the estimation of hGE/mL, based on measures of total ctDNA, reflects disease activity and is almost perfectly correlated with standard parameters such as PET/CT that are associated with refractoriness.

Published in eJHaem

ISSN: 2688-6146 (Online)
Publisher: Wiley
Country of publisher: United Kingdom
LCC subjects: Medicine: Internal medicine: Specialties of internal medicine: Diseases of the blood and blood-forming organs
Website: https://onlinelibrary.wiley.com/journal/26886146

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