Simple Summary In-depth knowledge of non-neoplastic patterns is fundamental when diagnosing neoplasia. In the present study, we described the flow cytometric (FC) features of B- and T-lymphocytes in 42 canine reactive lymph nodes and 36 lymphomas. Proliferative activity (Ki67%) in reactive lymph nodes was also reported. Reactive lymph nodes were composed of a mixed population of small and large T (CD5+) and B (CD21+) cells. Small T-cells were larger in size than small B-cells and large T-cells were larger than large B-cells. Large B-cells were 20% in B-cell lymphomas and showed a larger size in lymphomas than in reactive lymph nodes. Large T-cells were & LE;4% in reactive lymph nodes and >4% in T-cell lymphomas and showed higher CD5 expression in lymphomas compared to reactive lymph nodes. We report, for the first time, a subset of small CD5+CD21+dim cells in reactive lymph nodes, whose biological role has yet to be defined. Ki-67% values were higher than those reported in normal lymph nodes, and largely overlapped with those reported in lymphomas. An in-depth knowledge of non-neoplastic patterns is fundamental to diagnose neoplasia. In the present study, we described the flow cytometric (FC) cell size (FSC) and fluorescence intensity (MFI) of B- and T-lymphocytes in 42 canine reactive lymph nodes and 36 lymphomas. Proliferative activity (Ki67%) in reactive lymph nodes was also reported. Reactive lymph nodes were composed of a mixed population of small and large T (CD5+) and B (CD21+) cells. Small T-cells were larger in size than small B-cells, and large T-cells were larger than large B-cells. Small T-cells were composed of CD5+CD21- and CD5+CD21+dim subpopulations. Large B-cells were 20% in lymphomas and showed a higher FSC in lymphomas than in reactive lymph nodes. Large T-cells were 4% in lymphomas and showed a higher CD5 MFI in lymphomas (if expressed) compared to reactive lymph nodes. A subset of CD5+CD21+dim lymphocytes was recognized in addition to CD5+CD21- and CD5-CD21+ cells. In T-zone lymphomas, neoplastic cells had higher FSC and CD21 MFI values than small CD5+CD21+dim cells in reactive lymph nodes. Ki67% values were higher than those reported in normal lymph nodes, and largely overlapped with those reported in low-grade lymphomas and partially in high-grade lymphomas. Our results may contribute to making a less operator-dependent FC differential between lymphoma and reactive lymph nodes.
Flow Cytometric Features of B- and T-Lmphocytes in Reactive Lymph Nodes Compared to Their Neoplastic Counterparts in Dogs
Riondato, FulvioFirst
;Poggi, Alessia;Miniscalco, Barbara;Sini, Federica;Martini, ValeriaLast
2023-01-01
Abstract
Simple Summary In-depth knowledge of non-neoplastic patterns is fundamental when diagnosing neoplasia. In the present study, we described the flow cytometric (FC) features of B- and T-lymphocytes in 42 canine reactive lymph nodes and 36 lymphomas. Proliferative activity (Ki67%) in reactive lymph nodes was also reported. Reactive lymph nodes were composed of a mixed population of small and large T (CD5+) and B (CD21+) cells. Small T-cells were larger in size than small B-cells and large T-cells were larger than large B-cells. Large B-cells were 20% in B-cell lymphomas and showed a larger size in lymphomas than in reactive lymph nodes. Large T-cells were & LE;4% in reactive lymph nodes and >4% in T-cell lymphomas and showed higher CD5 expression in lymphomas compared to reactive lymph nodes. We report, for the first time, a subset of small CD5+CD21+dim cells in reactive lymph nodes, whose biological role has yet to be defined. Ki-67% values were higher than those reported in normal lymph nodes, and largely overlapped with those reported in lymphomas. An in-depth knowledge of non-neoplastic patterns is fundamental to diagnose neoplasia. In the present study, we described the flow cytometric (FC) cell size (FSC) and fluorescence intensity (MFI) of B- and T-lymphocytes in 42 canine reactive lymph nodes and 36 lymphomas. Proliferative activity (Ki67%) in reactive lymph nodes was also reported. Reactive lymph nodes were composed of a mixed population of small and large T (CD5+) and B (CD21+) cells. Small T-cells were larger in size than small B-cells, and large T-cells were larger than large B-cells. Small T-cells were composed of CD5+CD21- and CD5+CD21+dim subpopulations. Large B-cells were 20% in lymphomas and showed a higher FSC in lymphomas than in reactive lymph nodes. Large T-cells were 4% in lymphomas and showed a higher CD5 MFI in lymphomas (if expressed) compared to reactive lymph nodes. A subset of CD5+CD21+dim lymphocytes was recognized in addition to CD5+CD21- and CD5-CD21+ cells. In T-zone lymphomas, neoplastic cells had higher FSC and CD21 MFI values than small CD5+CD21+dim cells in reactive lymph nodes. Ki67% values were higher than those reported in normal lymph nodes, and largely overlapped with those reported in low-grade lymphomas and partially in high-grade lymphomas. Our results may contribute to making a less operator-dependent FC differential between lymphoma and reactive lymph nodes.
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