Aurum Institute, Johannesburg, South Africa.
School of Medicine, Vanderbilt University, Nashville, Tennessee, United States of America.
PLoS One. 2022 Feb 4;17(2):e0252097. doi: 10.1371/journal.pone.0252097. eCollection 2022.
Current tuberculosis treatments leave most patients with bronchiectasis and fibrosis, permanent conditions that impair lung function and increase all-cause post-TB mortality. Host-directed therapies (HDTs) may reduce lung inflammation and hasten eradication of infection. Biomarkers can accelerate tuberculosis regimen development, but no studies have yet examined early biomarkers of TB-HDTs.
Biomarkers of inflammation and microbicidal activity were evaluated as a part of a recent phase-2 randomized controlled trial of four HDTs in 200 patients with pulmonary tuberculosis and baseline predictors of poor outcome, including CC-11050 (PDE4i), everolimus (mTORi), auranofin (oral gold salt), and ergocalciferol (vitamin D). Two of the 4 arms (CC-11050 and everolimus) showed superior recovery of lung function at day 180 compared to control; none showed accelerated eradication of MTB infection. Patients underwent 18F-fluorodeoxyglucose positron emission tomography/computed tomography (PET/CT) on entry and day 56. PET signals were analyzed according to total, maximal, and peak glycolytic activity; CT was analyzed according to total modified Hounsfield units to assess radiodensity. Mycobactericidal activity in ex vivo whole blood culture was measured on days 42, 84, and 140. C-reactive protein (CRP) was measured at multiple time points.
All PET/CT parameters showed highly significant reductions from baseline to day 56; however, only maximal or peak glycolytic activity showed further experimental reduction compared to controls, and only in everolimus recipients. CRP dropped precipitously during early treatment, but did so equally in all arms; over the entire period of treatment, the rate of decline of CRP tended to be greater in CC-11050 recipients than in controls but this fell short of statistical significance. Whole blood mycobactericidal activity in ex-vivo culture was enhanced by auranofin compared to controls, but not by other HDTs.
None of these early biomarkers correctly predicted HDT effects on inflammation or infection across all four experimental arms. Instead, they each appear to show highly specific responses related to HDT mechanisms of action.
目前的结核病治疗方法会使大多数患者留下支气管扩张和纤维化等永久性疾病,这些疾病会损害肺功能并增加结核病治疗后的全因死亡率。宿主导向疗法(HDTs)可能会减少肺部炎症并加速感染的清除。生物标志物可以加速结核病治疗方案的开发,但尚无研究检查过 TB-HDTs 的早期生物标志物。
作为最近一项针对 200 例肺结核患者的四项 HDTs 的随机对照 2 期临床试验的一部分,评估了炎症和杀菌活性的生物标志物,以及包括 CC-11050(PDE4i)、依维莫司(mTORi)、金诺芬(口服金盐)和胆钙化醇(维生素 D)在内的基线预测不良预后的标志物。与对照组相比,四项治疗组中的两项(CC-11050 和依维莫司)在第 180 天显示出更好的肺功能恢复;但均未显示加速结核分枝杆菌感染的清除。患者在入组时和第 56 天进行 18F-氟脱氧葡萄糖正电子发射断层扫描/计算机断层扫描(PET/CT)。根据总、最大和峰值糖酵解活性分析 PET 信号;根据总改良的亨斯菲尔德单位(HU)分析 CT,以评估放射密度。在第 42、84 和 140 天测量了体外全血培养中的杀菌活性。在多个时间点测量 C 反应蛋白(CRP)。
所有 PET/CT 参数均显示从基线到第 56 天显著降低;然而,只有最大或峰值糖酵解活性与对照组相比显示出进一步的实验性降低,并且仅在依维莫司组中观察到。CRP 在早期治疗期间急剧下降,但在所有治疗组中均相同;在整个治疗期间,CC-11050 组的 CRP 下降速度比对照组更快,但无统计学意义。与对照组相比,金诺芬增强了体外全血培养中的杀菌活性,但其他 HDTs 则没有。
这些早期生物标志物均不能正确预测四种实验性治疗组中 HDT 对炎症或感染的影响。相反,它们似乎都显示出与 HDT 作用机制高度相关的高度特异性反应。
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