确定 PKC 调节剂艾滋病毒潜伏期逆转剂对自然杀伤细胞的影响

Q1 Medicine Pathogens and Immunity Pub Date : 2024-04-24 DOI:10.20411/pai.v9i1.673
M. Dimapasoc, Jose Moran, Steve Cole, Alok Ranjan, Rami Hourani, Jocelyn Kim, Paul A Wender, Matthew Marsden, Jerome Zack
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引用次数: 0

摘要

背景:蛋白激酶 C(PKC)调节剂等潜伏期逆转剂(LRA)可减少小动物模型中具有反弹能力的艾滋病毒储库。此外,在 LRA 治疗后施用自然杀伤(NK)细胞也能改善储库的减少。目前还不清楚为什么 PKC 调节剂和 NK 细胞的结合会如此有效,也不知道接触 PKC 调节剂是否会以某种方式增强 NK 细胞的功能:用PKC调节剂(bryostatin-1、prostatin或设计合成的bryostatin-1类似物SUW133)处理原代人类NK细胞,并通过流式细胞术检测活化标志物的表达,用RNA测序分析转录组图谱、通过与 K562 细胞共培养测定细胞毒性,通过 Luminex 检测法评估细胞因子的产生,以及通过与 Jurkat-Latency (J-Lat) 细胞共培养检测细胞因子和分泌因子独立逆转 HIV 潜伏期的能力。结果显示PKC 调节剂增加了参与 NK 细胞活化的蛋白质的表达。经 PKC 处理的 NK 细胞的转录组图谱显示了细胞活化的特征,并富集了与 NFκB 通路相关的基因。NK细胞的细胞毒性不受prostratin的影响,但受bryostatin-1和SUW133的影响则明显降低。来自 PKC 刺激的 NK 细胞的细胞因子不能诱导 J-Lat 细胞系的潜伏逆转。结论虽然 PKC 调节剂对 NK 细胞有一些显著影响,但它们在 "踢杀 "策略中的作用可能是上调 CD4+ T 细胞中 HIV 的表达,而不是直接增强 NK 细胞的效应功能。这表明,PKC 调节剂主要是增强这种艾滋病毒治疗方法的 "踢 "而不是 "杀 "的作用。
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Defining the Effects of PKC Modulator HIV Latency-Reversing Agents on Natural Killer Cells
Background: Latency reversing agents (LRAs) such as protein kinase C (PKC) modulators can reduce rebound-competent HIV reservoirs in small animal models. Furthermore, administration of natural killer (NK) cells following LRA treatment improves this reservoir reduction. It is currently unknown why the combination of a PKC modulator and NK cells is so potent and whether exposure to PKC modulators may augment NK cell function in some way. Methods: Primary human NK cells were treated with PKC modulators (bryostatin-1, prostratin, or the designed, synthetic bryostatin-1 analog SUW133), and evaluated by examining expression of activation markers by flow cytometry, analyzing transcriptomic profiles by RNA sequencing, measuring cytotoxicity by co-culturing with K562 cells, assessing cytokine production by Luminex assay, and examining the ability of cytokines and secreted factors to independently reverse HIV latency by co-culturing with Jurkat-Latency (J-Lat) cells. Results: PKC modulators increased expression of proteins involved in NK cell activation. Transcriptomic profiles from PKC-treated NK cells displayed signatures of cellular activation and enrichment of genes associated with the NFκB pathway. NK cell cytotoxicity was unaffected by prostratin but significantly decreased by bryostatin-1 and SUW133. Cytokines from PKC-stimulated NK cells did not induce latency reversal in J-Lat cell lines.  Conclusions: Although PKC modulators have some significant effects on NK cells, their contribution in “kick and kill” strategies is likely due to upregulating HIV expression in CD4+ T cells, not directly enhancing the effector functions of NK cells. This suggests that PKC modulators are primarily augmenting the “kick” rather than the “kill” arm of this HIV cure approach.
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来源期刊
Pathogens and Immunity
Pathogens and Immunity Medicine-Infectious Diseases
CiteScore
10.60
自引率
0.00%
发文量
16
审稿时长
10 weeks
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