Figure 1
Figure 1. EBV-infected cell phenotypes of EBV+ T/NK lymphoproliferative diseases. (A) Age distribution of patients with T-cell and NK-cell types. (B) EBV-infected cells among categories of clinical groups. Infected T cells were further divided into CD4+ T cells, CD8+ T cells, γδ T cells, and “other T cells.“ The 25 cases of “other T cells” were defined as either phenotypically different T-cell subsets (2 patients were CD4−CD8−, 1 patient was CD4+CD8+, and 1 patient had 2 lineages consisting of CD4+CD8− and CD4−CD8+ cells) or ill-defined T cells (n = 21). In the majority of the ill-defined T-cell patients, Abs against CD4 or CD8 could not be used to define their CD4/CD8 phenotype because the number of recovered PBMCs was not sufficient. SMBA indicates severe mosquito bite allergy; and HV, hydroa vacciniforme. (C) The 4th WHO pathologic classification of each clinical group at the time of diagnosis. SETLPD indicates systemic EBV+ T-cell lymphoproliferative disease of childhood; and HVL, hydroa vacciniforme–like lymphoma. (D) EBV-infected cells among categories of the pathologic classification at diagnosis and at the last follow-up or death. Patients in CR were classified according to the data and status before remission.

EBV-infected cell phenotypes of EBV+ T/NK lymphoproliferative diseases. (A) Age distribution of patients with T-cell and NK-cell types. (B) EBV-infected cells among categories of clinical groups. Infected T cells were further divided into CD4+ T cells, CD8+ T cells, γδ T cells, and “other T cells.“ The 25 cases of “other T cells” were defined as either phenotypically different T-cell subsets (2 patients were CD4CD8, 1 patient was CD4+CD8+, and 1 patient had 2 lineages consisting of CD4+CD8 and CD4CD8+ cells) or ill-defined T cells (n = 21). In the majority of the ill-defined T-cell patients, Abs against CD4 or CD8 could not be used to define their CD4/CD8 phenotype because the number of recovered PBMCs was not sufficient. SMBA indicates severe mosquito bite allergy; and HV, hydroa vacciniforme. (C) The 4th WHO pathologic classification of each clinical group at the time of diagnosis. SETLPD indicates systemic EBV+ T-cell lymphoproliferative disease of childhood; and HVL, hydroa vacciniforme–like lymphoma. (D) EBV-infected cells among categories of the pathologic classification at diagnosis and at the last follow-up or death. Patients in CR were classified according to the data and status before remission.

Close Modal
This Feature Is Available To Subscribers Only

or Create an Account

Close Modal
Close Modal