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T cell subtypes and reciprocal inflammatory mediator expression differentiate P. falciparum memory recall responses in asymptomatic and symptomatic malaria patients in southeastern Haiti

机译:海地东南部无症状和有症状疟疾患者的T细胞亚型和相互的炎症介质表达可区分恶性疟原虫记忆回想

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摘要

Asymptomatic Plasmodium falciparum infection is responsible for maintaining malarial disease within human populations in low transmission countries such as Haiti. Investigating differential host immune responses to the parasite as a potential underlying mechanism could help provide insight into this highly complex phenomenon and possibly identify asymptomatic individuals. We performed a cross-sectional analysis of individuals who were diagnosed with malaria in Sud-Est, Haiti by comparing the cellular and humoral responses of both symptomatic and asymptomatic subjects. Plasma samples were analyzed with a P. falciparum protein microarray, which demonstrated serologic reactivity to 3,877 P. falciparum proteins of known serologic reactivity; however, no antigen-antibody reactions delineating asymptomatics from symptomatics were identified. In contrast, differences in cellular responses were observed. Flow cytometric analysis of patient peripheral blood mononuclear cells co-cultured with P. falciparum infected erythrocytes demonstrated a statistically significant increase in the proportion of T regulatory cells (CD4+ CD25+ CD127-), and increases in unique populations of both NKT-like cells (CD3+ CD8+ CD56+) and CD8mid T cells in asymptomatics compared to symptomatics. Also, CD38+/HLA-DR+ expression on γδ T cells, CD8mid (CD56-) T cells, and CD8mid CD56+ NKT-like cells decreased upon exposure to infected erythrocytes in both groups. Cytometric bead analysis of the co-culture supernatants demonstrated an upregulation of monocyte-activating chemokines/cytokines in asymptomatics, while immunomodulatory soluble factors were elevated in symptomatics. Principal component analysis of these expression values revealed a distinct clustering of individual responses within their respective phenotypic groups. This is the first comprehensive investigation of immune responses to P. falciparum in Haiti, and describes unique cell-mediated immune repertoires that delineate individuals into asymptomatic and symptomatic phenotypes. Future investigations using large scale biological data sets analyzing multiple components of adaptive immunity, could collectively define which cellular responses and molecular correlates of disease outcome are malaria region specific, and which are truly generalizable features of asymptomatic Plasmodium immunity, a research goal of critical priority.
机译:无症状的恶性疟原虫感染负责在低传播国家(例如海地)的人群中维持疟疾。将宿主对寄生虫的不同免疫反应作为潜在的潜在机制进行调查,可能有助于深入了解这一高度复杂的现象,并可能确定无症状的个体。通过比较有症状和无症状受试者的细胞和体液反应,我们对在海地南部苏伊斯特被诊断出患有疟疾的个体进行了横断面分析。用恶性疟原虫蛋白质微阵列分析血浆样品,证明其对已知血清反应性的3,877种恶性疟原虫蛋白质具有血清反应性。但是,没有鉴定出从症状到症状的抗原抗体反应。相反,观察到细胞反应的差异。与恶性疟原虫感染的红细胞共培养的患者外周血单核细胞的流式细胞术分析表明,T调节细胞(CD4 + CD25 + CD127 -),并且两个NKT样细胞(CD3 + CD8 + CD56 + )的唯一种群都增加和有症状的CD8 mid T细胞无症状。此外,γδT细胞,CD8 mid (CD56 -)T上的CD38 + / HLA-DR + 表达两组中,CD8 mid CD56 + NKT样细胞均减少。共培养上清液的细胞计数珠分析显示无症状的单核细胞激活趋化因子/细胞因子上调,而有症状的免疫调节可溶性因子升高。这些表达值的主成分分析表明,在它们各自的表型组中,各个响应具有明显的聚集性。这是对海地对恶性疟原虫免疫反应的首次全面研究,描述了独特的细胞介导的免疫谱,将个体分为无症状和有症状的表型。未来使用大规模生物学数据集进行的研究将分析适应性免疫的多个组成部分,可以共同确定哪些细胞反应和疾病结局的分子相关性是疟疾区域特有的,而哪些才是无症状性疟原虫免疫的真正普遍化特征,这是至关重要的研究目标。

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