Assessment of immunoglobulin heavy chain, immunoglobulin light chain, and T‐cell receptor clonality testing in the diagnosis of feline lymphoid neoplasia

Rout, Emily D.; Burnett, Robert; Yoshimoto, Janna; Avery, P.; Avery, Anne C.

doi:10.1111/vcp.12767

Cited by 32 publications

(47 citation statements)

References 44 publications

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“…We previously determined that our IGH‐VDJ PARR reaction only detected 50% of feline B‐cell neoplasms, but targeting additional IG gene rearrangements increased B‐cell PARR sensitivity from 50% to 87% . The sensitivity of our TRG PARR primers to detect clonality in T‐cell neoplasms was 97%.…”

Section: Methodsmentioning

confidence: 87%

“…Polymerase chain reaction for antigen receptor rearrangements was performed on DNA extracted from blood samples, as previously described, to assess clonality of immunoglobulin (IG) and T‐cell receptor gamma (TRG) gene rearrangements. All 146 cases in the definition cohort and a subset of cases in the outcome cohort had PARR with primers targeting complete IG heavy chain V‐D‐J (IGH‐VDJ) and TRG gene rearrangements.…”

Section: Methodsmentioning

confidence: 99%

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Immunophenotypic characterization and clinical outcome in cats with lymphocytosis

Rout

Labadie

Curran

et al. 2019

Veterinary Internal Medicne

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Background: Lymphocytosis is relatively common in cats, but few studies describe lymphocyte populations or the clinical course associated with different immunophenotypic expansions.Hypothesis/Objectives: We hypothesized that cats frequently develop nonneoplastic lymphocytosis and that different neoplastic immunophenotypes have variable prognoses. We aimed to characterize the lymphocyte expansions in a large population of cats with lymphocytosis and to assess clinical presentation and outcome in a subset.Animals: Three cohorts of cats older than 1 year with lymphocytosis (>6000/μL) were examined to define immunophenotypic categories (n = 146), evaluate outcome (n = 94), and determine prevalence of immunophenotypes (n = 350).Methods: Retrospective study of cats with blood submitted for flow cytometry.Medical records (n = 94) were reviewed for clinical data, treatment, and survival information. Results: Five major immunophenotypic categories were identified: B cell, heterogeneous (≥2 lineages expanded), CD4+ T cell, CD4−CD8− (double negative [DN]) T cell, and CD5-low-expressing T cell. B-cell and heterogeneous phenotypes were more consistent with a non-neoplastic process, having polyclonal antigen receptor gene rearrangements, younger age at presentation, lower lymphocyte counts, and prolonged survival. The neoplastic phenotypes, CD4+ T cell, DN T cell, and CD5 low T cell, had different median survival times (752 days [n = 37], 271 days [n = 7], 27.5 days [n = 12], respectively). Among CD4+ T-cell cases, cats with abdominal lymphadenopathy, intestinal involvement, or both and females had shorter survival. Among 350 cats with lymphocytosis, CD4+ T-cell lymphocytosis was most common, followed by heterogeneous and B-cell phenotypes. Conclusions and Clinical Importance: Neoplastic CD4+ T-cell lymphocytosis is common in cats and has a prolonged clinical course compared to aberrant T-cell

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Section: Methodsmentioning

confidence: 87%

Section: Methodsmentioning

confidence: 99%

Immunophenotypic characterization and clinical outcome in cats with lymphocytosis

Rout

Labadie

Curran

et al. 2019

Veterinary Internal Medicne

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“…DNA quantity and quality were determined to be sufficient based on PARR results, as previously described. 17 PARR results were independently interpreted by the authors (E.D. Rout, A.C. Avery), blinded to the signalment and flow cytometry data.…”

Section: Pcr For Antigen Receptor Rearrangementsmentioning

confidence: 99%

“…Detection of incomplete IGH-DJ and IG light-chain rearrangements increases sensitivity in detecting B-cell and plasma cell neoplasms in humans, cats and dogs, as compared to complete IGH-VDJ rearrangements alone. 16,17,22,23 Incomplete IGH-DJ and Kde rearrangements are less prone to somatic hypermutation, and analysis of the IG kappa locus is useful in detecting clonality in canine tumors with somatic hypermutation, such as plasmacytomas. 16,22 The [25][26][27] Familial cases suggest a genetic predisposition and many cases have an isochromosome (3q) abnormality and chromosomal instability.…”

Section: Sequential Sample Analysismentioning

confidence: 99%

Polyclonal B‐cell lymphocytosis in English bulldogs

Rout

Moore

Burnett

et al. 2020

Veterinary Internal Medicne

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Background: English bulldogs disproportionally develop an expansion of small B-cells, which has been interpreted as B-cell chronic lymphocytic leukemia (BCLL). However, clonality testing in these cases has often not been supportive of neoplasia. Hypothesis: English bulldogs have a syndrome of nonneoplastic B-cell expansion. Animals: Eighty-four English bulldogs with small-sized CD21+ B-cell lymphocytosis in the blood as determined by flow cytometry. Methods: This is a retrospective study. We characterized this syndrome by assessing B-cell clonality, clinical presentation, flow cytometric features, and immunoglobulin gammopathy patterns. We identified 84 cases with CD21+ lymphocytosis among 195 English bulldogs with blood samples submitted to the Colorado State University-Clinical Immunology laboratory for immunophenotyping between 2010 and 2019. Flow cytometry features were compared to normal B-cells and BCLL cases. PCR for antigen receptor rearrangements (PARR) by multiple immunoglobulin primers was performed to assess B-cell clonality. A subset of cases with gammopathy were examined by protein electrophoresis, immunofixation, and immunoglobulin subclass ELISA quantification. Results: Seventy percent (58/83) of cases had polyclonal or restricted polyclonal immunoglobulin gene rearrangements, suggesting nonmalignant B-cell expansion. The median age of all dogs in the study was 6.8 years and 74% were male. The median (range) lymphocyte count was 22 400/μL (2000-384 400/μL) and B-cells had low expression of class II MHC and CD25. Splenomegaly or splenic masses were detected in 57% (26/46) of cases and lymphadenopathy in 11% (7/61). Seventy-one percent (52/73) of cases had hyperglobulinemia and 77% (23/30) with globulin characterization had IgA ± IgM polyclonal or restricted polyclonal gammopathy patterns. Conclusions and Clinical Importance: Polyclonal B-cell lymphocytosis in English bulldogs is characterized by low B-cell class II MHC and CD25 expression, splenomegaly

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“…MacNeill et al tackle the challenge of diagnostic testing for immune‐mediated hemolytic anemia, and LeVine et al review the pathophysiology and diagnostic dilemmas of immune thrombocytopenia . Electrophoresis and immunofixation techniques to characterize serum proteins are reviewed by Moore et al Harris et al validate a densitometric assay to quantify monoclonal proteins in canine sera, and Rout et al assess immunoglobulin heavy and light chain, and T‐cell receptor clonality to diagnose feline lymphoid neoplasia . Bergman et al investigate interferences from canine anti‐mouse antibodies in hormone immunoassays, and Irvine et al assess and compare two immunoassays to measure serum cardiac Troponin I in dogs and cats .…”

mentioning

confidence: 99%

An introduction for the Veterinary Clinical Pathology Special Issue on clinical immunology

Sprague

Radin

2019

Veterinary Clinical Pathol

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Assessment of immunoglobulin heavy chain, immunoglobulin light chain, and T‐cell receptor clonality testing in the diagnosis of feline lymphoid neoplasia

Cited by 32 publications

References 44 publications

Immunophenotypic characterization and clinical outcome in cats with lymphocytosis

Immunophenotypic characterization and clinical outcome in cats with lymphocytosis

Polyclonal B‐cell lymphocytosis in English bulldogs

An introduction for the Veterinary Clinical Pathology Special Issue on clinical immunology

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