Single‐cell analysis of MYD88<sup>L265P</sup> and MYD88<sup>WT</sup> Waldenström macroglobulinemia patients
Article 2024 en
Authors
TB
Tina Bagratuni
FA
Foteini Aktypi
OT
Ourania Theologi
Abstract
1 min read
Waldenström macroglobulinemia (WM) is characterized by the expansion of clonal lymphoplasmacytic cells; the MYD88L265P somatic mutation is found in >90% of patients, but malignant B cells may still display intra-clonal heterogeneity. To assess clonal heterogeneity in WM, we generated and performed single-cell RNA sequencing of CD19<sup>+</sup> sorted cells from five patients with <i>MYD88</i> <sup><i>L265P</i></sup> and two patients with <i>MYD88</i> <sup><i>WT</i></sup> genotype as well as two healthy donors. We identified distinct transcriptional patterns in the clonal subpopulations not only between the two genetically distinct WM subgroups but also among <i>MYD88</i> <sup><i>L265P</i></sup> patients, which affected the B cell composition in the different subgroups. Comparison of clonal and normal/polyclonal B cells within each patient sample enabled the identification of patient-specific transcriptional changes. We identified gene signatures active in a subset of MYD88<sup>L265P</sup> patients, while other signatures were active in <i>MYD88</i> <sup><i>WT</i></sup> patients. Finally, gene expression analysis showed common transcriptional features between patients compared to the healthy control but also differentially expressed genes between <i>MYD88</i> <sup><i>L265P</i></sup> and <i>MYD88</i> <sup><i>WT</i></sup> patients involved in distinct pathways, including NFκΒ, BCL2, and BTK. Overall, our data highlight the intra-tumor clonal heterogeneity in WM with potential prognostic and therapeutic implications.
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