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首页> 外文期刊>Journal of immunology research. >The Intracellular Growth of M. tuberculosis Is More Associated with High Glucose Levels Than with Impaired Responses of Monocytes from T2D Patients
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The Intracellular Growth of M. tuberculosis Is More Associated with High Glucose Levels Than with Impaired Responses of Monocytes from T2D Patients

机译:结核病的细胞内生长与高血糖水平高于T2D患者单核细胞的损伤

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Diabetes mellitus, a metabolic disease characterized by hyperglycemia and poor glucose control, is a risk factor for Mycobacterium tuberculosis (M. tuberculosis) infection and the development of active tuberculosis. To evaluate whether M. tuberculosis infection susceptibility is associated with an intrinsic factor in monocytes from type 2 diabetes (T2D) patients or it is associated with hyperglycemia per se, we analyzed TLR-2 and TLR-4 expression by flow cytometry and the cytokines IL-1β, IL-6, IL-8, IL-10, and TNF-α by cytometric bead array assays, either stimulated with TLR-2 and TLR-4 ligands or infected with M. tuberculosis in the whole blood from T2D patients (n=43) and healthy subjects (n=26) or in CD14+ monocytes from healthy subjects cultured in high glucose (HG) (30?mM). The intracellular growth of M. tuberculosis was evaluated by CFU counts at 0, 1, and 3 days in both monocytes from T2D patients and monocytes from healthy subjects cultured in HG. We did not find significant differences in TLR expression, cytokine production, or growth of M. tuberculosis in monocytes from T2D patients compared with those in monocytes from healthy subjects. Despite these results, in vitro assays of monocytes cultured with 30?mM glucose led to significantly increased TLR-2 and TLR-4 basal expression compared to those of monocytes cultured with 11?mM glucose (P0.05). Conversely, the production of IL-6 by TLR-2 ligand stimulation, of IL-1β, IL-6, and IL-8 by TLR-4 ligand stimulation, and of IL-8 by M. tuberculosis infection significantly decreased in monocytes cultured in HG (P0.05). Additionally, the intracellular survival of M. tuberculosis increased in monocytes in HG after day 3 of culture (P0.05). In conclusion, HG decreased IL-8 production and the intracellular growth control of M. tuberculosis by monocytes, supporting the hypothesis that hyperglycemia plays an important role in the impaired immune responses to M. tuberculosis in patients with T2D.
机译:糖尿病,一种由高血糖和葡萄糖控制特征的代谢疾病,是结核分枝杆菌(肺结核)感染和活性结核病的发展的危险因素。为了评估C.Tuberculosis感染易感性是否与来自2型糖尿病(T2D)患者的单核细胞中的内在因子相关,或者与本身的高血糖相关,我们通过流式细胞术和细胞因子IL分析TLR-2和TLR-4表达通过细胞计数珠阵列测定的-1β,IL-6,IL-8,IL-10和TNF-α,用TLR-2和TLR-4配体刺激或在来自T2D患者的全血中感染M.结核病( n = 43)和来自高葡萄糖(Hg)(30Ωmm)培养的健康受试者的健康受试者(n = 26)或CD14 +单核细胞。通过CFU计数在来自T2D患者的单核细胞和HG中培养的健康受试者的单核细胞中的单核细胞中的0,1,3天评估核细胞分枝杆菌的细胞内生长。与来自T2D患者的单核细胞中,与来自健康受试者的单核细胞的单核细胞中,在TLR表达,细胞因子生产或M.Tuberculosis的生长中没有发现显着差异。尽管这些结果,与用11→mm葡萄糖培养的单核细胞相比,用30×mm葡萄糖培养的单核细胞的体外测定结果显着增加了TLR-2和TLR-4基础表达(P <0.05)。相反,通过TLR-4配体刺激的IL-1β,IL-6和IL-8通过TLR-2配体刺激的IL-6的产生,通过M.Tu-8在培养的单核细胞中显着降低在hg(p <0.05)。此外,培养第3天后,肺结核菌的细胞内存活率增加了Hg中的单核细胞(P <0.05)。总之,HG通过单核细胞产生了IL-8的生产和M.结核病的细胞内生长控制,支持高血糖症在T2D患者患者的免疫应答中发挥着重要作用的假设。

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