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March 28, 2026Open Access

Digital Spatial Profiling Uncovers Transcriptomic Features of Distinct Plasma Cell-like Phenotypes in Diffuse Large B-cell Lymphoma

Key Points

To explore the role and transcriptomic features of distinct plasma cell-like phenotypes in diffuse large B-cell lymphoma and their prognostic significance.
Used spatially-resolved transcriptomics to profile four plasma cell-like phenotypes based on specific markers.
Classified patients as DLBCL plasma cell-like phenotype predominant or deficient based on plasma cell-like phenotype cell percentage.
Conducted transcriptomic analyses to assess the correlation with proliferation, immune function, and tumor microenvironment.
Constructed a random forest model to predict response to bortezomib using plasma cell-like phenotype-associated genes.
The non-plasma cell-like phenotype showed better prognosis compared to all plasma cell-like phenotypes.
Patients with >30% plasma cell-like phenotype had higher disease progression rates within 12 months.
Higher plasma cell-like phenotype signatures correlated with poorer progression-free survival but greater benefit from R-CHOP plus bortezomib treatment.

Abstract

Diffuse large B-cell lymphoma (DLBCL) exhibits marked heterogeneity, complicating treatment and prognosis. The role of plasma cell-like phenotypes in DLBCL remains underexplored. Using spatially-resolved transcriptomics, we profiled four distinct plasma cell-like phenotypes in DLBCL based on CD20, HLA-DRA, and PRDM1 markers: CD20(+)HLA-DRA(+)PRDM1(-), CD20(+)HLA-DRA(+)PRDM1(+), CD20(+)HLA-DRA(-)PRDM1(-), and CD20(+)HLA-DRA(-)PRDM1(+). The CD20(+)HLA-DRA(+)PRDM1(-) phenotype (non-plasma cell-like phenotype) was associated with better prognosis whereas the other three phenotypes (plasma cell-like phenotypes) correlated with worse prognosis. Patients with 30% plasma cell-like phenotype cells were classified as DLBCL plasma cell-like phenotype predominant (DLBCLPCPP), and those with ≤30% as DLBCL plasma cell-like phenotype deficient (DLBCLPCPD). Plasma cell-like phenotype cells correlated with reduced proliferation, impaired immune function, and enhanced tumor microenvironment remodeling. DLBCLPCPP demonstrated a lower proportion of patients with Ki-67 ≥85% (29.6% vs. 53.9%, p=0.0198), similar responses to first-line treatment (92.6% vs. 92.6%, p=1.00), but a higher rate of disease progression within 12 months (25.9% vs. 3.7%, p=0.0238) and an increased incidence of B2M alterations (22.2% vs. 3.7%, p=0.0509) compared to DLBCLPCPD. Transcriptomic analyses revealed closer proximity between plasma cell-like phenotype cells and plasmablastic lymphoma. Leveraging plasma cell-like phenotype-associated genes, we constructed a random forest model to predict response to bortezomib. High plasma cell-like phenotype signatures were linked to poorer progression-free survival (PFS) but greater benefit from R-CHOP plus bortezomib, while low-signature patients achieved better PFS with R-CHOP alone. These findings characterize the transcriptomic features of distinct plasma cell-like phenotypes in DLBCL, providing new insights into its prognostic relevance and potential for individualized treatment strategies.

Digital Spatial Profiling Uncovers Transcriptomic Features of Distinct Plasma Cell-like Phenotypes in Diffuse Large B-cell Lymphoma

Key Points

Abstract

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