口服重组人或小鼠乳铁蛋白可减少结核分枝杆菌TDM诱导的肉芽肿性肺病理。

Shen-An Hwang, M. Kruzel, J. Actor
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引用次数: 16

摘要

海藻糖6′6-二mycolate (TDM)是结核分枝杆菌(MTB)细胞壁上最丰富的糖脂。TDM能够在小鼠模型中诱导肉芽肿病理,类似于结核分枝杆菌感染诱导的肉芽肿病理。利用急性TDM模型,研究重组人和小鼠乳铁蛋白减少肉芽肿病理的作用。给C57BL/6小鼠静脉注射TDM,剂量为25 μg·mouse-1。在第4天和第6天,灌胃给予重组人或小鼠乳铁蛋白(1 mg·(100 μL)-1·mouse-1)。注射TDM后第7天,对小鼠肺病理、细胞因子产生和白细胞数量进行评估。给予人乳铁蛋白或小鼠乳铁蛋白的小鼠肺部IL-12p40的产生减少。小鼠乳铁蛋白增加肺组织IL-6和KC (CXCL1)。在注射tdm的小鼠中观察到巨噬细胞数量增加,这些小鼠分别给予人或小鼠乳铁蛋白。肉芽肿病理主要由迁移的白细胞组成,在接受人或小鼠乳铁蛋白治疗的小鼠中,肉芽肿病理明显减少。肉芽肿病理定量显示,与TDM对照小鼠相比,给予人或小鼠乳铁蛋白的小鼠肉芽肿明显减少。本报告首次直接比较了异源重组人和同源小鼠乳铁蛋白对tdm诱导肉芽肿发展的免疫调节作用。
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Oral recombinant human or mouse lactoferrin reduces Mycobacterium tuberculosis TDM induced granulomatous lung pathology.
Trehalose 6'6-dimycolate (TDM) is the most abundant glycolipid on the cell wall of Mycobacterium tuberculosis (MTB). TDM is capable of inducing granulomatous pathology in mouse models that resembles those induced by MTB infection. Using the acute TDM model, this work investigates the effect of recombinant human and mouse lactoferrin to reduce granulomatous pathology. C57BL/6 mice were injected intravenously with TDM at a dose of 25 μg·mouse-1. At day 4 and 6, recombinant human or mouse lactoferrin (1 mg·(100 μL)-1·mouse-1) were delivered by gavage. At day 7 after TDM injection, mice were evaluated for lung pathology, cytokine production, and leukocyte populations. Mice given human or mouse lactoferrin had reduced production of IL-12p40 in their lungs. Mouse lactoferrin increased IL-6 and KC (CXCL1) in lung tissue. Increased numbers of macrophages were observed in TDM-injected mice given human or mouse lactoferrin. Granulomatous pathology, composed of mainly migrated leukocytes, was visually reduced in mice that received human or mouse lactoferrin. Quantitation of granulomatous pathology demonstrated a significant decrease in mice given human or mouse lactoferrin compared with TDM control mice. This report is the first to directly compare the immune modulatory effects of both heterologous recombinant human and homologous mouse lactoferrin on the development of TDM-induced granulomas.
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