首页> 外文OA文献 >Blood Myeloid Dendritic Cells from HIV-1-Infected Individuals Display a Proapoptotic Profile Characterized by Decreased Bcl-2 Levels and by Caspase-3+ Frequencies That Are Associated with Levels of Plasma Viremia and T Cell Activation in an Exploratory Study ▿
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Blood Myeloid Dendritic Cells from HIV-1-Infected Individuals Display a Proapoptotic Profile Characterized by Decreased Bcl-2 Levels and by Caspase-3+ Frequencies That Are Associated with Levels of Plasma Viremia and T Cell Activation in an Exploratory Study ▿

机译:在一项探索性研究中,来自HIV-1感染者的血液髓样树突状细胞显示出以Bcl-2水平降低和Caspase-3 +频率降低与血浆病毒血症水平和T细胞活化相关的凋亡特征。

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摘要

Reduced frequencies of myeloid and plasmacytoid dendritic cell (DC) subsets (mDCs and pDCs, respectively) have been observed in the peripheral blood of HIV-1-infected individuals throughout the course of disease. Accumulation of DCs in lymph nodes (LNs) may partly account for the decreased numbers observed in blood, but increased DC death may also be a contributing factor. We used multiparameter flow cytometry to evaluate pro- and antiapoptotic markers in blood mDCs and pDCs from untreated HIV-1-infected donors, from a subset of infected donors before and after receiving antiretroviral therapy (ART), and from uninfected control donors. Blood mDCs, but not pDCs, from untreated HIV-1-infected donors expressed lower levels of antiapoptotic Bcl-2 than DCs from uninfected donors. A subset of HIV-1-infected donors had elevated frequencies of proapoptotic caspase-3+ blood mDCs, and positive correlations were observed between caspase-3+ mDC frequencies and plasma viral load and CD8+ T-cell activation levels. Caspase-3+ mDC frequencies, but not mDC Bcl-2 expression, were reduced with viral suppression on ART. Apoptosis markers on DCs in blood and LN samples from a cohort of untreated, HIV-1-infected donors with chronic disease were also evaluated. LN mDCs displayed higher levels of Bcl-2 and lower caspase-3+ frequencies than did matched blood mDCs. Conversely, LN pDCs expressed lower Bcl-2 levels than their blood counterparts. In summary, blood mDCs from untreated HIV-1-infected subjects displayed a proapoptotic profile that was partially reversed with viral suppression, suggesting that DC death may be a factor contributing to blood DC depletion in the setting of chronic, untreated HIV disease.
机译:在整个病程中,HIV-1感染者的外周血中髓样和浆细胞样树突状细胞(DC)子集(分别为mDC和pDC)的频率降低。 DC在淋巴结(LN)中的积累可能部分解释了血液中观察到的数量减少,但DC死亡增加也可能是一个因素。我们使用多参数流式细胞术评估未经治疗的HIV-1感染供体,接受抗逆转录病毒治疗(ART)前后的部分感染供体以及未感染对照供体的血液mDC和pDC中的促凋亡和抗凋亡标记。未经治疗的HIV-1感染供者的血液mDC,而非pDC,其抗凋亡Bcl-2水平低于未感染供者的DC。一部分被HIV-1感染的供体的促凋亡caspase-3 +血液mDC频率升高,并且在caspase-3 + mDC频率与血浆病毒载量和CD8 + T细胞活化水平之间观察到正相关。 Caspase-3 + mDC的频率,但不是mDC Bcl-2的表达,被ART上的病毒抑制所降低。还评估了未经治疗的HIV-1感染的慢性病供体队列中血液和LN样品中DC的凋亡标记。与匹配的血液mDC相比,LN mDC显示出更高的Bcl-2水平和更低的caspase-3 +频率。相反,LN pDCs表达的Bcl-2水平低于其血液对应物。总之,未经治疗的HIV-1感染者的血液mDCs显示出凋亡的特征,其部分被病毒抑制所逆转,这表明在慢性未经治疗的HIV疾病中,DC死亡可能是导致血液中DC耗竭的因素。

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