CD133+外泌体对2型糖尿病小鼠中风后肝功能的治疗作用
Therapeutic effects of CD133 + Exosomes on liver function after stroke in type 2 diabetic mice.
作者信息
Venkat Poornima, Gao Huanjia, Findeis Elizabeth L, Chen Zhili, Zacharek Alex, Landschoot-Ward Julie, Powell Brianna, Lu Mei, Liu Zhongwu, Zhang Zhenggang, Chopp Michael
机构信息
Department of Neurology, Henry Ford Hospital, Detroit, MI, United States.
Department of Public Health Sciences, Henry Ford Hospital, Detroit, MI, United States.
出版信息
Front Neurosci. 2023 Mar 9;17:1061485. doi: 10.3389/fnins.2023.1061485. eCollection 2023.
BACKGROUND AND PURPOSE
Non-alcoholic fatty liver disease (NAFLD) is known to adversely affect stroke recovery. However, few studies investigate how stroke elicits liver dysfunction, particularly, how stroke in type 2 diabetes mellitus (T2DM) exacerbates progression of NAFLD. In this study, we test whether exosomes harvested from human umbilical cord blood (HUCBC) derived CD133 + cells (CD133 + Exo) improves neuro-cognitive outcome as well as reduces liver dysfunction in T2DM female mice.
METHODS
Female, adult non-DM and T2DM mice subjected to stroke presence or absence were considered. T2DM-stroke mice were randomly assigned to receive PBS or Exosome treatment group. CD133 + Exo (20 μg/200 μl PBS, i.v.) was administered once at 3 days after stroke. Evaluation of neurological (mNSS, adhesive removal test) and cognitive function [novel object recognition (NOR) test, odor test] was performed. Mice were sacrificed at 28 days after stroke and brain, liver, and serum were harvested.
RESULTS
Stroke induces severe and significant short-term and long-term neurological and cognitive deficits which were worse in T2DM mice compared to non-DM mice. CD133 + Exo treatment of T2DM-stroke mice significantly improved neurological function and cognitive outcome indicated by improved discrimination index in the NOR and odor tests compared to control T2DM-stroke mice. CD133 + Exo treatment of T2DM stroke significantly increased vascular and white matter/axon remodeling in the ischemic brain compared to T2DM-stroke mice. However, there were no differences in the lesion volume between non-DM stroke, T2DM-stroke and CD133 + Exo treated T2DM-stroke mice. In T2DM mice, stroke induced earlier and higher TLR4, NLRP3, and cytokine expression (SAA, IL1β, IL6, TNFα) in the liver compared to heart and kidney, as measured by Western blot. T2DM-stroke mice exhibited worse NAFLD progression with increased liver steatosis, hepatocellular ballooning, fibrosis, serum ALT activity, and higher NAFLD Activity Score compared to T2DM mice and non-DM-stroke mice, while CD133 + Exo treatment significantly attenuated the progression of NAFLD in T2DM stroke mice.
CONCLUSION
Treatment of female T2DM-stroke mice with CD133 + Exo significantly reduces the progression of NAFLD/NASH and improves neurological and cognitive function compared to control T2DM-stroke mice.
背景与目的
已知非酒精性脂肪性肝病(NAFLD)会对中风恢复产生不利影响。然而,很少有研究调查中风如何引发肝功能障碍,特别是2型糖尿病(T2DM)患者的中风如何加剧NAFLD的进展。在本研究中,我们测试了从人脐带血(HUCBC)来源的CD133 +细胞中收获的外泌体(CD133 + Exo)是否能改善T2DM雌性小鼠的神经认知结果并减轻肝功能障碍。
方法
考虑纳入成年非糖尿病和T2DM雌性小鼠,使其经历有无中风的情况。T2DM中风小鼠被随机分配到接受PBS或外泌体治疗组。在中风后3天静脉注射一次CD133 + Exo(20μg/200μl PBS)。进行神经功能(mNSS、粘胶去除试验)和认知功能[新物体识别(NOR)试验、嗅觉试验]评估。中风后28天处死小鼠,采集脑、肝和血清。
结果
中风会导致严重且显著的短期和长期神经及认知缺陷,与非糖尿病小鼠相比,T2DM小鼠的这些缺陷更严重。与对照T2DM中风小鼠相比,用CD133 + Exo治疗T2DM中风小鼠可显著改善神经功能和认知结果,这通过NOR和嗅觉试验中改善的辨别指数得以体现。与T2DM中风小鼠相比,用CD133 + Exo治疗T2DM中风可显著增加缺血脑中的血管和白质/轴突重塑。然而,非糖尿病中风小鼠、T2DM中风小鼠和接受CD133 + Exo治疗的T2DM中风小鼠之间的梗死体积没有差异。通过蛋白质印迹法检测发现,与心脏和肾脏相比,在T2DM小鼠中,中风诱导肝脏中TLR4、NLRP3和细胞因子表达(SAA、IL1β、IL6、TNFα)更早且更高。与T2DM小鼠和非糖尿病中风小鼠相比,T2DM中风小鼠表现出更严重的NAFLD进展,伴有肝脏脂肪变性增加、肝细胞气球样变、纤维化、血清ALT活性升高以及更高的NAFLD活动评分,而CD133 + Exo治疗可显著减轻T2DM中风小鼠的NAFLD进展。
结论
与对照T2DM中风小鼠相比,用CD133 + Exo治疗雌性T2DM中风小鼠可显著降低NAFLD/NASH的进展,并改善神经和认知功能。
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