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Peer-reviewed veterinary case report

New genetic changes found in dog large B-cell lymphoma by genome

By Fanelli, Antonella et al.·Published in Veterinary and Comparative Oncology·2025·Department of Veterinary Sciences University of Turin Grugliasco Turin Italy, Italy·View original on Crossref

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Original publication title: Expanding the Spectrum of Canine Diffuse Large B‐Cell Lymphoma Genetic Aberrations Through Whole Genome Sequencing Analysis

Species:
dog

Plain-English summary

A group of dogs diagnosed with diffuse large B-cell lymphoma (DLBCL), a type of cancer, were treated with a combination of chemotherapy and immunotherapy. Despite having similar symptoms, some dogs responded well to treatment while others did not, leading to different survival outcomes. Researchers used advanced genetic testing to identify unique genetic changes in the dogs, which may help explain why some dogs had better responses than others. This study highlights the complexity of DLBCL in dogs and suggests that more research is needed to understand the genetic factors involved in treatment success.

People also search for: dog lymphoma treatment · diffuse large B-cell lymphoma in dogs · dog cancer survival rates

Abstract

ABSTRACTDiffuse large B‐cell lymphoma (DLBCL) is one of the most prevalent haematological malignancies in both humans and dogs, characterised in both species by significant clinical heterogeneity and limited prognostic predictability. With the introduction of next‐generation sequencing (NGS) technologies in veterinary medicine over the past decade, researchers have begun to elucidate the molecular basis of canine DLBCL (cDLBCL); however, much of the clinical heterogeneity associated with this tumour remains unexplained. In this study, we performed whole genome sequencing on 10 cDLBCL cases, all treated with chemo‐immunotherapy, which exhibited similar clinico‐pathological features but markedly different outcomes. Cases were classified as “poor” or “good” responders based on whether their lymphoma‐specific survival fell below or above the cohort's median. Protein‐coding variants and copy number aberrations unique to poor or good responders revealed novel candidate genes not previously identified in cDLBCL studies, while splicing, untranslated regions, and intronic variants were detected in genes already known to be recurrently mutated. In conclusion, our investigation has broadened the spectrum of potentially pathogenic variants implicated in cDLBCL, though further studies with larger cohorts are necessary to validate these findings.

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Original publication on Crossref: https://doi.org/10.1111/vco.13059