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首页> 外文期刊>Progress in Artificial Intelligence >Lipophilicity of Bacteriochlorin-Based Photosensitizers as a Determinant for PDT Optimization through the Modulation of the Inflammatory Mediators
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Lipophilicity of Bacteriochlorin-Based Photosensitizers as a Determinant for PDT Optimization through the Modulation of the Inflammatory Mediators

机译:通过调节炎症介质的PDT优化的抗精菌性光敏剂的亲脂性

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摘要

Photodynamic therapy (PDT) augments the host antitumor immune response, but the role of the PDT effect on the tumor microenvironment in dependence on the type of photosensitizer and/or therapeutic protocols has not been clearly elucidated. We employed three bacteriochlorins (F2BOH, F(2)BMet and Cl(2)BHep) of different polarity that absorb near-infrared light (NIR) and generated a large amount of reactive oxygen species (ROS) to compare the PDT efficacy after various drug-to-light intervals: 15 min. (V-PDT), 3h (E-PDT) and 72h (C-PDT). We also performed the analysis of the molecular mechanisms of PDT crucial for the generation of the long-lasting antitumor immune response. PDT-induced damage affected the integrity of the host tissue and developed acute (protocol-dependent) local inflammation, which in turn led to the infiltration of neutrophils and macrophages. In order to further confirm this hypothesis, a number of proteins in the plasma of PDT-treated mice were identified. Among a wide range of cytokines (IL-6, IL-10, IL-13, IL-15, TNF-alpha, GM-CSF), chemokines (KC, MCP-1, MIP1 alpha, MIP1 beta, MIP2) and growth factors (VEGF) released after PDT, an important role was assigned to IL-6. PDT protocols optimized for studied bacteriochlorins led to a significant increase in the survival rate of BALB/c mice bearing CT26 tumors, but each photosensitizer (PS) was more or less potent, depending on the applied DLI (15 min, 3 h or 72 h). Hydrophilic (F2BOH) and amphiphilic (F(2)BMet) PSs were equally effective in V-PDT (>80 cure rate). F(2)BMet was the most efficient in E-PDT (DLI = 3h), leading to a cure of 65 % of the animals. Finally, the most powerful PS in the C-PDT (DLI = 72 h) regimen turned out to be the most hydrophobic compound (Cl(2)BHep), allowing 100 % of treated animals to be cured at a light dose of only 45 J/cm(2).
机译:光动力疗法(PDT)增强了宿主抗肿瘤免疫应答,但PDT影响依赖于光敏剂和/或治疗方案类型的肿瘤微环境的作用并未明确阐明。我们使用三种菌种(F2BOH,F(2)Bmet和Cl(2)BHEP)的不同极性,其吸收近红外光(NIR)并产生大量的反应性氧物质(ROS)以比较各种后的PDT功效药物到光间隔:15分钟。 (V-PDT),3H(E-PDT)和72h(C-PDT)。我们还表现了对PDT的分子机制对持久抗肿瘤免疫反应产生的关键。 PDT诱导的损伤影响了宿主组织的完整性,并且发育了急性(方案依赖性)局部炎症,这又导致了中性粒细胞和巨噬细胞的渗透。为了进一步证实该假设,鉴定了PDT处理的小鼠血浆中的许多蛋白质。在各种各样的细胞因子(IL-6,IL-10,IL-13,IL-15,TNF-α,GM-CSF)中,趋化因子(KC,MCP-1,MIP1α,MIP1β,MIP2)和生长PDT后释放的因素(VEGF),将重要作用分配给IL-6。优化用于研究的菌氯的PDT方案导致含CT26肿瘤的BALB / C小鼠的存活率的显着增加,但是每个光敏剂(PS)或多或少有效,这取决于所施加的DLI(15分钟,3小时或72小时)。亲水性(F2BOH)和两亲(F(2)Bmet)PSS在V-PDT(> 80固化率)中同样有效。 F(2)Bmet在E-PDT(DLI = 3H)中最有效,导致65%的动物的固化。最后,C-PDT(DLI = 72h)方案中最强大的PS是最疏水的化合物(CL(2)BHEP),允许100%的处理动物以45的轻剂量固化J / CM(2)。

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