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非肥胖型糖尿病小鼠的高血糖与唾液腺功能障碍:干燥综合征临床前研究的注意事项。

Hyperglycemia and Salivary Gland Dysfunction in the Non-obese Diabetic Mouse: Caveats for Preclinical Studies in Sjögren's Syndrome.

机构信息

Arthritis and Clinical Immunology Program, Oklahoma Medical Research Foundation, Oklahoma City, OK, USA.

出版信息

Sci Rep. 2019 Nov 29;9(1):17969. doi: 10.1038/s41598-019-54410-9.

Abstract

The Non-obese Diabetic (NOD) mouse model for type I diabetes also develops some features of Sjögren's syndrome (SS). Since the source of the mice and the environment exert a strong influence on diabetes, this study investigated SS development in NOD mice obtained from two vendors. Female NOD mice from The Jackson Laboratory (JAX) and Taconic Biosciences were monitored for blood glucose and pilocarpine-induced salivation. The gut microbiome was analyzed by 16S rRNA sequencing of stool DNA. At euthanasia, serum cytokines and sialoadenitis severity were evaluated. The onset of diabetes was significantly accelerated in JAX mice compared to Taconic mice. Although the gut microbiome between the two groups was distinct, both groups developed sialoadenitis. There was no correlation between the severity of sialoadenitis and reduced saliva production. Instead, salivary gland dysfunction was associated with hyperglycemia and elevation of serum IL1β, IL16, and CXCL13. Our data suggest that inflammatory pathways linked with hyperglycemia are confounding factors for salivary gland dysfunction in female NOD mice, and might not be representative of the mechanisms operative in SS patients. Considering that NOD mice have been used to test numerous experimental therapies for SS, caution needs to be exerted before advancing these therapeutics for human trials.

摘要

非肥胖型糖尿病(NOD)小鼠模型也会发展出一些干燥综合征(SS)的特征。由于小鼠的来源和环境对糖尿病有很大的影响,因此本研究调查了从两家供应商获得的 NOD 小鼠的 SS 发展情况。监测雌性 NOD 小鼠(来自杰克逊实验室(JAX)和塔科尼克生物科学公司)的血糖和毛果芸香碱诱导的唾液分泌情况。通过对粪便 DNA 的 16S rRNA 测序分析肠道微生物组。安乐死后,评估血清细胞因子和唾液腺炎严重程度。与 Taconic 小鼠相比,JAX 小鼠的糖尿病发病明显加快。尽管两组之间的肠道微生物组存在差异,但两组均发生唾液腺炎。唾液腺炎的严重程度与唾液分泌减少之间没有相关性。相反,唾液腺功能障碍与高血糖以及血清 IL1β、IL16 和 CXCL13 的升高有关。我们的数据表明,与高血糖相关的炎症途径是雌性 NOD 小鼠唾液腺功能障碍的混杂因素,并且可能不能代表 SS 患者的机制。考虑到 NOD 小鼠已被用于测试 SS 的许多实验性治疗方法,在将这些治疗方法推进到人体试验之前,需要谨慎行事。

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