Quantitative flow cytometric identification of aberrant T cell clusters in erythrodermic cutaneous T cell lymphoma. Implications for staging and prognosis

Aims Assessment of peripheral blood tumour burden for staging of cutaneous T cells lymphoma is most often accomplished by flow cytometry (FC) using various non-standarised strategies. We report the results of calculating absolute Sezary cell counts (SCCs) by FC, based on the identification of aberrant T cell clusters on a virtual 6-dimensional space and independently of the expected immunophenotype (6D-FC SCC). Methods 6D-FC SCCs were calculated on 65 peripheral blood specimens from 28 patients with erythrodermic cutaneous T cells lymphoma (stage III or IV). Comparisons were made with recommended FC strategies and correlations with overall mortality were studied. Results At first visit, 17 of 28 patients (61%) had 6D-FC SCCs meeting current criteria for Stage IV disease (≥1000 SC/μL); while only 2 patients (7%) met Stage IV criteria on other tissues. As defined by comprehensive staging using clinicomorphological criteria and 6D-FC SCCs, Stage IV disease identified a subgroup of patients with worse overall survival (p=0.0227). Residual non-aberrant CD4 T cells were markedly decreased in Stage IV disease (p=0.018). Among 65 specimens, discrepancies were observed between 6D-FC SCCs and usual FC thresholds for Stage IV disease, namely a CD4:CD8 ratio ≥10:1 (9 discrepancies, 14%), and ≥40% aberrant CD4 T cells (4 discrepancies, 6%). Surprisingly, 8 cases (12%) from 6 patients exhibited two distinctively separate clusters of aberrant CD4 T cells with different CD7 and/or CD26 expression. Conclusions Visual 6-dimensional identification of aberrant T cell clusters by FC allows for the calculation of clinically significant SCCs. Simplified gating strategies and relative quantitative values might underestimate the immunophenotypical complexity of Sezary cells.

[1]  Greg Finak,et al.  Critical assessment of automated flow cytometry data analysis techniques , 2013, Nature Methods.

[2]  P. Hari,et al.  Immunophenotypic stability of Sézary cells by flow cytometry: usefulness of flow cytometry in assessing response to and guiding alemtuzumab therapy. , 2012, American journal of clinical pathology.

[3]  M. Borowitz,et al.  Simplified flow cytometric assessment in mycosis fungoides and Sézary syndrome. , 2011, American journal of clinical pathology.

[4]  J. Scarisbrick,et al.  Survival outcomes and prognostic factors in mycosis fungoides/Sézary syndrome: validation of the revised International Society for Cutaneous Lymphomas/European Organisation for Research and Treatment of Cancer staging proposal. , 2010, Journal of clinical oncology : official journal of the American Society of Clinical Oncology.

[5]  L. Medeiros,et al.  Flow cytometric detection of peripheral blood involvement by mycosis fungoides and Sézary syndrome using T-cell receptor Vβ chain antibodies and its application in blood staging , 2010, Modern Pathology.

[6]  J. Katzmann,et al.  A comparison of morphologic features, flow cytometry, TCR-Vbeta analysis, and TCR-PCR in qualitative and quantitative assessment of peripheral blood involvement by Sézary syndrome. , 2006, American journal of clinical pathology.

[7]  P. Nowell,et al.  Sézary cell counts in erythrodermic cutaneous T-cell lymphoma: Implications for prognosis and staging , 2006, Leukemia & lymphoma.

[8]  Nicola Pimpinelli,et al.  WHO-EORTC classification for cutaneous lymphomas. , 2005, Blood.

[9]  David A Jones,et al.  Profound loss of T-cell receptor repertoire complexity in cutaneous T-cell lymphoma. , 2003, Blood.

[10]  A. Varghese,et al.  Long-term outcome of 525 patients with mycosis fungoides and Sezary syndrome: clinical prognostic factors and risk for disease progression. , 2003, Archives of dermatology.

[11]  Anthony D. Kelleher,et al.  Characterization of CD4+ CTLs Ex Vivo1 , 2002, The Journal of Immunology.

[12]  M. Huentelman,et al.  Gene Therapy for Cardiovascular Disorders , 2001 .

[13]  M. Nikolova,et al.  Crosstalk between Tumor T Lymphocytes and Reactive T Lymphocytes in Cutaneous T Cell Lymphomas , 2001, Annals of the New York Academy of Sciences.

[14]  N. Dang,et al.  Absence of CD26 expression is a useful marker for diagnosis of T-cell lymphoma in peripheral blood. , 2001, American journal of clinical pathology.

[15]  J. Scarisbrick,et al.  Prognostic significance of tumor burden in the blood of patients with erythrodermic primary cutaneous T-cell lymphoma. , 2001, Blood.

[16]  A. de Matteis,et al.  The relevance of the CD4+ CD26– subset in the identification of circulating Sézary cells , 2001, The British journal of dermatology.

[17]  F. Foss,et al.  Immunophenotypic identification of Sezary cells in peripheral blood. , 1996, American journal of clinical pathology.

[18]  J. Katzmann,et al.  Detection of circulating T cells with CD4+CD7- immunophenotype in patients with benign and malignant lymphoproliferative dermatoses. , 1996, Journal of the American Academy of Dermatology.

[19]  W. P. Mak,et al.  Lymphocyte subpopulation reference ranges for monitoring human immunodeficiency virus-infected Chinese adults , 1996, Clinical and diagnostic laboratory immunology.

[20]  R. Edelson,et al.  Profound deficiency in normal circulating T cells in erythrodermic cutaneous T-cell lymphoma. , 1994, Archives of dermatology.

[21]  E. Vonderheid,et al.  Infections complicating mycosis fungoides and Sézary syndrome. , 1992, JAMA.

[22]  P. Nowell,et al.  Diagnostic and prognostic significance of Sézary cells in peripheral blood smears from patients with cutaneous T cell lymphoma. , 1985, Blood.

[23]  L. Peterson,et al.  The usefulness of CD26 in flow cytometric analysis of peripheral blood in Sézary syndrome. , 2008, American journal of clinical pathology.

[24]  B. Thiers Revisions to the staging and classification of mycosis fungoides and Sézary syndrome: a proposal of the International Society for Cutaneous Lymphomas (ISCL) and the cutaneous lymphoma task force of the European Organization of Research and Treatment of Cancer (EORTC) , 2008 .

[25]  G. Burg,et al.  Update on erythrodermic cutaneous T-cell lymphoma: report of the International Society for Cutaneous Lymphomas. , 2002, Journal of the American Academy of Dermatology.

[26]  A. Pistorio,et al.  An Italian national multicenter study for the definition of reference ranges for normal values of peripheral blood lymphocyte subsets in healthy adults. , 1999, Haematologica.