Proliferative, pro-inflammatory, and angiogenesis regulator gene expression profile defines prognosis in different histopathological subtypes of nodal peripheral T-cell lymphoma

Nodal peripheral T-cell lymphoma (PTCL) is an aggressive and heterogeneous malignancy with poor prognosis. We studied the prognostic impact of the expression profile of genes related to cell proliferation ( , , and ), pro-inflammatory activity ( and ), and angiogenesis ( ) in nodal PTCL outcomes, as...

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Veröffentlicht in:Oncotarget 2019-08, Vol.10 (50), p.5136-5151
Hauptverfasser: de Pádua Covas Lage, Luís Alberto, Levy, Débora, Xavier, Flávia Dias, Reis, Diego Cândido, de Oliveira Costa, Renata, Gonçalves, Marianne Castro, Rocha, Vanderson, Zerbini, Maria Cláudia Nogueira, Pereira, Juliana
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container_title Oncotarget
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creator de Pádua Covas Lage, Luís Alberto
Levy, Débora
Xavier, Flávia Dias
Reis, Diego Cândido
de Oliveira Costa, Renata
Gonçalves, Marianne Castro
Rocha, Vanderson
Zerbini, Maria Cláudia Nogueira
Pereira, Juliana
description Nodal peripheral T-cell lymphoma (PTCL) is an aggressive and heterogeneous malignancy with poor prognosis. We studied the prognostic impact of the expression profile of genes related to cell proliferation ( , , and ), pro-inflammatory activity ( and ), and angiogenesis ( ) in nodal PTCL outcomes, as well as the ability of this genomic panel to discriminate different histological subtypes. We investigated the relative expression of regulator genes in 63 nodal PTCL patients. CCNA2, TOP2A, CHEK1, and NF-kB1 proteins were also assessed by immunohistochemistry. The median patient age was 47 years, 57.1% were male, 34.9% were diagnosed with PTCL-NOS, 28.6% with ALK-/ALCL, 22.2% with ALK+/ALCL, and 14.3% with AITL. The proliferative genes were associated with worse 3-year OS and PFS in PTCL-NOS and better 3-year PFS in ALK-/ALCL. Expression of CCNA2≥median and overexpression of CHEK1 protein (HR 3.793; = 0.007) were associated with worse OS for all the cohort of nodal PTCL (HR 1.418; = 0.001). The genomic expression profile tested in this study was not able to discriminate the different subtypes of nodal PTCL, although it showed a distinct prognostic significance between PTCL-NOS and ALCL-ALK. Overexpression of the CCNA2 gene and CHEK1 protein were associated with poor prognosis in the total nodal PTCL cohort.
doi_str_mv 10.18632/oncotarget.27098
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We studied the prognostic impact of the expression profile of genes related to cell proliferation ( , , and ), pro-inflammatory activity ( and ), and angiogenesis ( ) in nodal PTCL outcomes, as well as the ability of this genomic panel to discriminate different histological subtypes. We investigated the relative expression of regulator genes in 63 nodal PTCL patients. CCNA2, TOP2A, CHEK1, and NF-kB1 proteins were also assessed by immunohistochemistry. The median patient age was 47 years, 57.1% were male, 34.9% were diagnosed with PTCL-NOS, 28.6% with ALK-/ALCL, 22.2% with ALK+/ALCL, and 14.3% with AITL. The proliferative genes were associated with worse 3-year OS and PFS in PTCL-NOS and better 3-year PFS in ALK-/ALCL. Expression of CCNA2≥median and overexpression of CHEK1 protein (HR 3.793; = 0.007) were associated with worse OS for all the cohort of nodal PTCL (HR 1.418; = 0.001). The genomic expression profile tested in this study was not able to discriminate the different subtypes of nodal PTCL, although it showed a distinct prognostic significance between PTCL-NOS and ALCL-ALK. 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The genomic expression profile tested in this study was not able to discriminate the different subtypes of nodal PTCL, although it showed a distinct prognostic significance between PTCL-NOS and ALCL-ALK. Overexpression of the CCNA2 gene and CHEK1 protein were associated with poor prognosis in the total nodal PTCL cohort.</abstract><cop>United States</cop><pub>Impact Journals LLC</pub><pmid>31497245</pmid><doi>10.18632/oncotarget.27098</doi><tpages>16</tpages><oa>free_for_read</oa></addata></record>
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title Proliferative, pro-inflammatory, and angiogenesis regulator gene expression profile defines prognosis in different histopathological subtypes of nodal peripheral T-cell lymphoma
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