Nariman Deravi scite author profile

BackgroundEvolution of indolent to aggressive lymphoma has been described in dogs but is difficult to distinguish from the de novo development of a second, clonally distinct lymphoma. Differentiation of these scenarios can be aided by next generation sequencing (NGS)-based assessment of clonality of lymphocyte antigen receptor genes.Case presentationAn 8-year-old male intact Mastiff presented with generalized lymphadenomegaly was diagnosed with nodal T zone lymphoma (TZL) based on cytology, histopathology, immunohistochemistry and flow cytometry. Thirteen months later, the dog re-presented with progressive lymphadenomegaly, and based on cytology and flow cytometry, a large B cell lymphoma (LBCL) was diagnosed. Sequencing-based clonality testing confirmed the de novo development of a LBCL and the persistence of a TZL.ConclusionsThe occurrence of two distinct lymphoid neoplasms should be considered if patient features and tumor cytomorphology or immunophenotype differ among sequential samples. Sequencing-based clonality testing may provide conclusive evidence of two concurrent and distinct clonal lymphocyte populations, termed most appropriately “composite lymphoma”.

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T‐Cell Tumors

Deravi¹,

Keller²,

Bienzle³

2022

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What is your diagnosis? A pigmented round cell tumor

Quiroz-Rocha¹,

Deravi

Knight

et al. 2017

Veterinary Clinical Pathol

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Nariman Deravi

Specific immunotypes of canine T cell lymphoma are associated with different outcomes

Composite lymphoma of concurrent T zone lymphoma and large cell B cell lymphoma in a dog

T‐Cell Tumors

What is your diagnosis? A pigmented round cell tumor

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