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Immunity in young adult survivors of childhood leukemia is similar to the elderly rather than age-matched controls: Role of cytomegalovirus

机译:免疫成年幸存者的童年白血病是类似于老年人而不是年龄组:巨细胞病毒的作用

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Many treatment complications that occur late in childhood cancer survivors resemble age-related comorbidities observed in the elderly. An immune phenotype characterized by increased immune activation, systemic inflammation, and accumulation of late-differentiated memory CD57(+) CD28(-) T cells has been associated with comorbidities in the elderly. Here, we explored if this phenotype was present in young adult leukemia survivors following an average of 19 years from chemotherapy and/or radiotherapy completion, and compared this with that in age-matched controls. We found that markers of systemic inflammation-IL-6 and human C-reactive protein and immune activation-CD38 and HLA-DR on T cells, soluble CD (sCD) 163 from monocytes and macrophages-were increased in survivors compared to controls. T-cell responses specific to cytomegalovirus (CMV) were also increased in survivors compared to controls while CMV IgG levels in survivors were comparable to levels measured in the elderly (>50years) and correlated with IL-6, human C-reactive protein, sCD163, and CD57(+) CD28(-) memory T cells. Immune activation and inflammation markers correlated poorly with prior chemotherapy and radiotherapy exposure. These data suggest that CMV infection/reactivation is strongly correlated with the immunological phenotype seen in young childhood leukemia survivors and these changes may be associated with the early onset of age-related comorbidities in this group.
机译:许多治疗晚期发生的并发症儿童癌症幸存者与年龄相关并发症观察老年人。增加免疫表型特征激活、系统性炎症和积累late-differentiated记忆T细胞CD28 CD57(+)(-)有关并发症的老人。如果这种表型出现在年轻的成年人白血病幸存者后平均19年从化疗或放疗完成,而这个的年龄组。系统性inflammation-IL-6和人类c反应蛋白和免疫activation-CD38 HLA-DRT细胞,从单核细胞和可溶性CD (sCD) 163macrophages-were增加幸存者相比来控制。巨细胞病毒(CMV)也在增加幸存者相比控制而巨细胞病毒免疫球蛋白幸存者与水平的水平以老年人(> 50年)和相关的与il - 6、人类的c反应蛋白,sCD163,CD57 CD28(+)(-)记忆T细胞。和炎症标记相关差之前的化疗和放疗。这些数据表明,巨细胞病毒感染/复活强烈相关与免疫表型在年轻儿童白血病幸存者和这些变化可能与早期发病有关的在这组与年龄相关的并发症。

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