Omange Robert Were, Kim Samuel C, Kolhatkar Nikita S, Plott Tempest, Van Trump Will, Zhang Kenneth, O'Donnell Hope, Chen Daniel, Hosny Ahmed, Wiest Michael, Barry Zach, Addiego Elisa Cambronero, Mengistu Meron, Odorizzi Pamela M, Cai Yanhui, Jacobson Rachel, Wallin Jeffrey J
Biomarker Sciences and Diagnostics, Gilead Sciences, Inc., Foster City, CA, United States.
Spring Science, San Carlos, CA, United States.
Front Immunol. 2025 Mar 25;16:1541152. doi: 10.3389/fimmu.2025.1541152. eCollection 2025.
Selective and potent Toll-like receptor (TLR) agonists are currently under evaluation in preclinical models and clinical studies to understand how the innate immune system can be harnessed for therapeutic potential. These molecules are designed to modulate innate and adaptive immune responses, making them promising therapeutic candidates for treating diseases such as cancer or chronic viral infections. Much is known about the expression and signaling of TLRs which varies based on cell type, cellular localization, and tissue distribution. However, the downstream effects of different TLR agonists on cellular populations and phenotypes are not well understood. This study aimed to investigate the impact of TLR pathway stimulation on peripheral blood mononuclear cell (PBMC) cultures from people living with HIV (PLWH) and healthy donors.
The effects of TLR4, TLR7, TLR7/8, TLR8 and TLR9 agonists were evaluated on cytokine production, cell population frequencies, and morphological characteristics of PBMC cultures over time. Changes in the proportions of different cell populations in blood and morphological features were assessed using high-content imaging and analyzed using an AI-driven approach.
TLR4 and TLR8 agonists promoted a compositional shift and accumulation of small round (lymphocyte-like) PBMCs, whereas TLR9 agonists led to an accumulation of large round (myeloid-like) PBMCs. A related increase was observed in markers of cell death, most prominently with TLR4 and TLR8 agonists. All TLR agonists were shown to promote some features associated with cellular migration. Furthermore, a comparison of TLR agonist responses in healthy and HIV-positive PBMCs revealed pronounced differences in cytokine/chemokine responses and morphological cellular features. Most notably, higher actin contraction and nuclear fragmentation was observed in response to TLR4, TLR7, TLR7/8 and TLR9 agonists for antiretroviral therapy (ART)-suppressed PLWH versus healthy PBMCs.
These data suggest that machine learning, combined with cell imaging and cytokine quantification, can be used to better understand the cytological and soluble immune responses following treatments with immunomodulatory agents In addition, comparisons of these responses between disease states are possible with the appropriate patient samples.
目前正在临床前模型和临床研究中评估选择性和强效的Toll样受体(TLR)激动剂,以了解如何利用先天免疫系统发挥治疗潜力。这些分子旨在调节先天和适应性免疫反应,使其成为治疗癌症或慢性病毒感染等疾病的有前景的治疗候选物。关于TLR的表达和信号传导,我们已知很多,其会因细胞类型、细胞定位和组织分布而有所不同。然而,不同TLR激动剂对细胞群体和表型的下游影响尚不清楚。本研究旨在调查TLR途径刺激对来自艾滋病毒感染者(PLWH)和健康供体的外周血单核细胞(PBMC)培养物的影响。
随着时间的推移,评估TLR4、TLR7、TLR7/8、TLR8和TLR9激动剂对PBMC培养物的细胞因子产生、细胞群体频率和形态特征的影响。使用高内涵成像评估血液中不同细胞群体比例和形态特征的变化,并使用人工智能驱动的方法进行分析。
TLR4和TLR8激动剂促进了小圆形(淋巴细胞样)PBMC的组成性转变和积累,而TLR9激动剂导致大圆形(髓样样)PBMC的积累。在细胞死亡标志物中观察到相关增加,最明显的是TLR4和TLR8激动剂。所有TLR激动剂均显示出促进一些与细胞迁移相关的特征。此外,对健康和HIV阳性PBMC中TLR激动剂反应的比较揭示了细胞因子/趋化因子反应和细胞形态特征的明显差异。最值得注意的是,与健康PBMC相比,接受抗逆转录病毒治疗(ART)的PLWH对TLR4、TLR7、TLR7/8和TLR9激动剂的反应中观察到更高的肌动蛋白收缩和核碎裂。
这些数据表明,机器学习与细胞成像和细胞因子定量相结合,可用于更好地理解免疫调节剂治疗后的细胞学和可溶性免疫反应。此外,使用适当的患者样本可以比较不同疾病状态下的这些反应。
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