The Influence of the COVID-19 Pandemic in NK Cell Subpopulations from CML Patients Enrolled in the Argentina Stop Trial
María Belén Sanchez, Bianca Vasconcelos Cordoba, Carolina Pavlovsky, Beatriz Moiraghi, Ana Ines Varela, Isabel Giere, Mariana Juni, Nicolas Flaibani, José Mordoh, Julio Cesar Sanchez Avalos, Estrella Mariel Levy, Michele Bianchini

TL;DR
The study found that the immune profiles of CML patients attempting treatment-free remission changed during the pandemic, possibly due to the impact of COVID-19 on NK cells.
Contribution
The study identifies immune differences in CML patients before and during the pandemic, suggesting a potential impact of COVID-19 on NK cell profiles.
Findings
Non-relapsing patients in 2019 had NK cells with memory features and high cytotoxicity markers.
In 2022-2023, NK cells showed reduced CD16/CD57 but increased NKp44/PD-1 expression and higher functionality.
Serum samples from 2022-2023 confirmed anti-SARS-CoV-2 IgG, suggesting a link between the pandemic and immune changes.
Abstract
Treatment-free remission (TFR) is a key therapeutic goal for chronic myeloid leukemia (CML) patients in deep molecular response (DMR). While predicting patient outcome remains challenging, different NK cell populations seem crucial. We conducted an immunological sub-study from the Argentina Stop Trial (AST), including 46 patients in 2019 (AST I) and 35 new patients between 2022 and 2023 (AST II). To characterize NK cell subsets in patients attempting TFR, peripheral blood mononuclear cell samples were collected before stopping treatment and phenotype and functional characteristics were assessed by flow cytometry. Non-relapsing patients from AST I exhibited NK cell subpopulations with cytomegalovirus-related memory features, high expression of cytotoxicity markers, and robust functionality. Remarkably, though clinical variables were very similar between cohorts, significant immune…
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Taxonomy
TopicsChronic Myeloid Leukemia Treatments · Immune Cell Function and Interaction · CAR-T cell therapy research
