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人端粒酶逆转录酶调控树突状细胞治疗脓毒症的免疫功能及机制研究

Study on the functions and mechanism of immune functions of human telomerase reverse transcriptase regulating dendritic cells treating sepsis.

作者信息

Chen H-M, Wang L-Q, Wan H-P, Wei H-Z, Ke L-C, Liu C-Y, Tan Q-Y

机构信息

Department of Emergency Surgery, First Affiliated Hospital of Nanchang University, Nanchang, China.

出版信息

Eur Rev Med Pharmacol Sci. 2016 Nov;20(21):4500-4507.

Abstract

OBJECTIVE

We analyzed the functions and mechanisms of immune functions of human telomerase reverse transcriptase regulating dendritic cells (DC) treating sepsis of mice models.

MATERIALS AND METHODS

Eighty clean grade Balb/c animals aged from 6 to 8 weeks, weighted from 18 g to 22 g were selected for this study. The DC cells were harvested from the animals and cultivated to transfect with the recombinant eukaryotic expression plasmid hTERT-IRES2-EGFP construct. The LPS (E. coli 0111:B4, 5 mg/kg) was injected into the abdominal cavity of mice to establish sepsis models. Afterwards, animals were divided randomly into the sepsis group (A group), the group of hTERT transfecting DC (B group), the group of DC un-transfected (C group) with 25 mice in each group. 5 mice were in the normal control group (D group), without any treatment. An equivalent volume of normal saline was injected into the abdominal cavity of A group. Subsequently, 1 ml of cell suspension (105/ml) was transfected into B and C groups respectively. Five animals from A, B, C groups and one animal from group D were sacrificed after 24h, 48h, 72d, 7d and 10d respectively.

RESULTS

It was found that median survival time of the group of hTERT transfecting DC was remarkably higher than that of the untransfected group and the sepsis group. The average scores of the pathology of kidney and intestine at each time were significantly lower than that of the other two groups (p<0.05). At each time point, in the group of hTERT transfecting DC, levels of CRP and Cr were remarkably lower than that of the other two groups; HLA-DR, CD40 of immune phenotype and the expression level of peripheral blood T cells MHC-II molecules were significantly higher than that of the other two groups; the expression level of IL-12 and TNF-a were significantly lower than that of the other two groups; apoptosis rate of DC were significantly lower than that of the other two groups; the content and activity of NF-κB were significantly higher than that of the other two groups (p<0.05).

CONCLUSIONS

The telomerase reverse transcriptase gene can raise the expression and maturity of DC, reduce apoptosis, induce cytokine secretion, reduce the inflammatory response and increase the survival time.

摘要

目的

分析人端粒酶逆转录酶调控树突状细胞(DC)治疗小鼠脓毒症模型的免疫功能及机制。

材料与方法

选取80只6至8周龄、体重18至22克的清洁级Balb/c动物用于本研究。从动物体内获取DC细胞并培养,用重组真核表达质粒hTERT-IRES2-EGFP构建体进行转染。将脂多糖(大肠杆菌0111:B4,5毫克/千克)注入小鼠腹腔以建立脓毒症模型。之后,将动物随机分为脓毒症组(A组)、hTERT转染DC组(B组)、未转染DC组(C组),每组25只。正常对照组(D组)5只,不做任何处理。向A组腹腔注射等量生理盐水。随后,分别向B组和C组转染1毫升细胞悬液(10⁵/毫升)。分别在24小时、48小时、72小时、7天和10天后,处死A、B、C组各5只动物以及D组1只动物。

结果

发现hTERT转染DC组的中位生存时间显著高于未转染组和脓毒症组。各时间点肾脏和肠道病理平均评分显著低于其他两组(p<0.05)。在每个时间点,hTERT转染DC组中,CRP和Cr水平显著低于其他两组;免疫表型的HLA-DR、CD40以及外周血T细胞MHC-II分子表达水平显著高于其他两组;IL-12和TNF-α表达水平显著低于其他两组;DC凋亡率显著低于其他两组;NF-κB含量和活性显著高于其他两组(p<0.05)。

结论

端粒酶逆转录酶基因可提高DC的表达和成熟度,减少凋亡,诱导细胞因子分泌,减轻炎症反应并延长生存时间。

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