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眼部结核视网膜色素上皮内的休眠与抗生素耐受性

dormancy and antibiotic tolerance within the retinal pigment epithelium of ocular tuberculosis.

作者信息

Liu Rachel, Dang Joshua N, Lee Rhoeun, Lee Jae Jin, Kesavamoorthy Niranjana, Ameri Hossein, Rao Narsing, Eoh Hyungjin

出版信息

bioRxiv. 2024 Mar 19:2024.03.18.585612. doi: 10.1101/2024.03.18.585612.

Abstract

UNLABELLED

Tuberculosis (TB) is a leading cause of death among infectious diseases worldwide due to latent TB infection, which is the critical step for the successful pathogenic cycle. In this stage, resides inside the host in a dormant and antibiotic-tolerant state. Latent TB infection can lead to a multisystemic diseases because invades virtually all organs, including ocular tissues. Ocular tuberculosis (OTB) occurs when the dormant bacilli within ocular tissues reactivate, originally seeded by hematogenous spread from pulmonary TB. Timely and accurate diagnosis as well as efficient chemotherapies are crucial in preventing poor visual outcomes of OTB patients. Histological evidence suggests that retinal pigment epithelium (RPE) cells play a central role in immune privilege and in the protection from the antibiotic effects, making them an anatomical niche for invading . RPE cells exhibit high tolerance to environmental redox stresses, allowing phagocytosed bacilli to maintain viability in a dormant state. However, the microbiological and metabolic mechanisms determining the interaction between the RPE intracellular environment and phagocytosed are largely unknown. Here, liquid chromatography mass spectrometry (LC-MS) metabolomics was used to illuminate the metabolic state within RPE cells reprogrammed to harbor dormant bacilli and enhance the antibiotic tolerance. The results have led to propose a novel therapeutic option to synthetically kill the dormant inside the RPE cells by modulating the phenotypic state of , thus laying the foundation for a new, innovative regimen for treating OTB.

IMPORTANCE

Understanding the metabolic environment within the retinal pigment epithelium (RPE) cells altered by infection with and mycobacterial dormancy is crucial to identify new therapeutic methods to cure OTB. The present study showed that RPE cellular metabolism is altered to foster intracellular M. tuberculosis to enter into the dormant and drug tolerant state, thereby blunting the efficacy of anti-TB chemotherapy. RPE cells serve as an anatomical niche as the cells protect invading bacilli from antibiotic treatment. LC-MS metabolomics of RPE cells after co-treatment with H2O2 and M. tuberculosis infection showed that intracellular environment within RPE cells is enriched with greater level of oxidative stress. The antibiotic tolerance of intracellular within RPE cells can be restored by a metabolic manipulation strategy such as co-treatment of antibiotic with the most downstream glycolysis metabolite, phosphoenolpyruvate.

摘要

未标注

结核病(TB)是全球传染病死亡的主要原因之一,这归因于潜伏性结核感染,它是致病循环成功的关键步骤。在此阶段,结核杆菌以休眠和耐抗生素的状态寄居于宿主体内。潜伏性结核感染可导致多系统疾病,因为结核杆菌几乎可侵入所有器官,包括眼组织。眼结核(OTB)发生于眼组织内休眠的杆菌重新激活时,最初是由肺结核经血液传播播散而来。及时准确的诊断以及有效的化疗对于预防OTB患者视力不佳的结局至关重要。组织学证据表明,视网膜色素上皮(RPE)细胞在免疫特权以及对抗生素作用的保护中起核心作用,使其成为结核杆菌侵入的解剖学微环境。RPE细胞对环境氧化还原应激表现出高度耐受性,使吞噬的结核杆菌能够在休眠状态下维持活力。然而,决定RPE细胞内环境与吞噬的结核杆菌之间相互作用的微生物学和代谢机制在很大程度上尚不清楚。在此,液相色谱质谱联用(LC-MS)代谢组学被用于阐明重新编程以容纳休眠结核杆菌并增强抗生素耐受性的RPE细胞内的代谢状态。这些结果促使提出一种新的治疗选择,即通过调节结核杆菌的表型状态来综合杀死RPE细胞内的休眠结核杆菌,从而为治疗OTB的全新创新方案奠定基础。

重要性

了解因结核杆菌感染和分枝杆菌休眠而改变的视网膜色素上皮(RPE)细胞内的代谢环境对于确定治愈OTB的新治疗方法至关重要。本研究表明,RPE细胞代谢发生改变,以促进细胞内结核分枝杆菌进入休眠和耐药物状态,从而削弱抗结核化疗的疗效。RPE细胞作为一个解剖学微环境,因为这些细胞保护侵入的杆菌免受抗生素治疗。RPE细胞在与过氧化氢和结核杆菌感染共同处理后的LC-MS代谢组学表明,RPE细胞内环境富含更高水平的氧化应激。RPE细胞内结核杆菌的抗生素耐受性可通过代谢操纵策略恢复,例如将抗生素与最下游的糖酵解代谢物磷酸烯醇丙酮酸共同处理。

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