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根据结核病疾病状态影响感染患者循环外泌体的蛋白质和脂质含量。

Affects Protein and Lipid Content of Circulating Exosomes in Infected Patients Depending on Tuberculosis Disease State.

作者信息

Biadglegne Fantahun, Schmidt Johannes R, Engel Kathrin M, Lehmann Jörg, Lehmann Robert T, Reinert Anja, König Brigitte, Schiller Jürgen, Kalkhof Stefan, Sack Ulrich

机构信息

College of Medicine and Health Sciences, Bahir Dar University, Bahir Dar P.O. Box 79, Ethiopia.

Institute of Medical Microbiology and Epidemiology of Infectious Diseases, Faculty of Medicine, Leipzig University, 04103 Leipzig, Germany.

出版信息

Biomedicines. 2022 Mar 27;10(4):783. doi: 10.3390/biomedicines10040783.

Abstract

Tuberculosis (TB), which is caused by the bacterium (), is still one of the deadliest infectious diseases. Understanding how the host and pathogen interact in active TB will have a significant impact on global TB control efforts. Exosomes are increasingly recognized as a means of cell-to-cell contact and exchange of soluble mediators. In the case of TB, exosomes are released from the bacillus and infected cells. In the present study, a comprehensive lipidomics and proteomics analysis of size exclusion chromatography-isolated plasma-derived exosomes from patients with TB lymphadenitis (TBL) and treated as well as untreated pulmonary TB (PTB) was performed to elucidate the possibility to utilize exosomes in diagnostics and knowledge building. According to our findings, exosome-derived lipids and proteins originate from both the host and in the plasma of active TB patients. Exosomes from all patients are mostly composed of sphingomyelins (SM), phosphatidylcholines, phosphatidylinositols, free fatty acids, triacylglycerols (TAG), and cholesterylesters. Relative proportions of, e.g., SMs and TAGs, vary depending on the disease or treatment state and could be linked to pathogenesis and dormancy. We identified three proteins of origin: DNA-directed RNA polymerase subunit beta (RpoC), Diacyglycerol O-acyltransferase (Rv2285), and Formate hydrogenase (HycE), the latter of which was discovered to be differently expressed in TBL patients. Furthermore, we discovered that infection alters the host protein composition of circulating exosomes, significantly affecting a total of 37 proteins. All TB patients had low levels of apolipoproteins, as well as the antibacterial proteins cathelicidin, Scavenger Receptor Cysteine Rich Family Member (SSC5D), and Ficolin 3 (FCN3). When compared to healthy controls, the protein profiles of PTB and TBL were substantially linked, with 14 proteins being co-regulated. However, adhesion proteins (integrins, Intercellular adhesion molecule 2 (ICAM2), CD151, Proteoglycan 4 (PRG4)) were shown to be more prevalent in PTB patients, while immunoglobulins, Complement component 1r (C1R), and Glutamate receptor-interacting protein 1 (GRIP1) were found to be more abundant in TBL patients, respectively. This study could confirm findings from previous reports and uncover novel molecular profiles not previously in focus of TB research. However, we applied a minimally invasive sampling and analysis of circulating exosomes in TB patients. Based on the findings given here, future studies into host-pathogen interactions could pave the way for the development of new vaccines and therapies.

摘要

结核病(TB)由结核杆菌引起,仍然是最致命的传染病之一。了解宿主与病原体在活动性结核病中如何相互作用,将对全球结核病防控工作产生重大影响。外泌体越来越被认为是细胞间接触和可溶性介质交换的一种方式。就结核病而言,外泌体从杆菌和受感染细胞中释放出来。在本研究中,对结核性淋巴结炎(TBL)患者以及治疗和未治疗的肺结核(PTB)患者经尺寸排阻色谱分离的血浆来源外泌体进行了全面的脂质组学和蛋白质组学分析,以阐明在外泌体用于诊断和知识构建方面的可能性。根据我们的研究结果,外泌体衍生的脂质和蛋白质源自活动性结核病患者血浆中的宿主和结核杆菌。所有患者的外泌体主要由鞘磷脂(SM)、磷脂酰胆碱、磷脂酰肌醇、游离脂肪酸、三酰甘油(TAG)和胆固醇酯组成。例如,SM和TAG的相对比例因疾病或治疗状态而异,可能与结核杆菌的发病机制和休眠有关。我们鉴定出三种结核杆菌来源的蛋白质:DNA指导的RNA聚合酶亚基β(RpoC)、二酰甘油O-酰基转移酶(Rv2285)和甲酸氢化酶(HycE),其中后者在TBL患者中发现表达不同。此外,我们发现结核杆菌感染会改变循环外泌体的宿主蛋白质组成,显著影响总共37种蛋白质。所有结核病患者的载脂蛋白水平较低,以及抗菌蛋白cathelicidin、富含半胱氨酸的清道夫受体家族成员(SSC5D)和纤维胶凝蛋白3(FCN3)水平也较低。与健康对照相比,PTB和TBL的蛋白质谱有显著关联,有14种蛋白质共同调控。然而,粘附蛋白(整合素、细胞间粘附分子2(ICAM2)、CD151、蛋白聚糖4(PRG4))在PTB患者中更为普遍,而免疫球蛋白、补体成分1r(C1R)和谷氨酸受体相互作用蛋白1(GRIP1)分别在TBL患者中更为丰富。本研究可以证实先前报告的结果,并揭示结核病研究之前未关注的新分子谱。然而,我们对结核病患者的循环外泌体进行了微创采样和分析。基于此处给出的研究结果,未来对宿主-病原体相互作用的研究可能为新疫苗和治疗方法的开发铺平道路。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/feff/9025801/b5fa12a95060/biomedicines-10-00783-g001.jpg

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