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利用小鼠粪便悬液建立脓毒症模型的方案:粪便悬液腹腔注射模型

Protocol for a Sepsis Model Utilizing Fecal Suspension in Mice: Fecal Suspension Intraperitoneal Injection Model.

作者信息

Tsuchida Takumi, Wada Takeshi, Mizugaki Asumi, Oda Yoshitaka, Kayano Katsuhide, Yamakawa Kazuma, Tanaka Shinya

机构信息

Division of Acute and Critical Care Medicine, Department of Anesthesiology and Critical Care Medicine, Faculty of Medicine, Hokkaido University, Sapporo, Japan.

Department of Cancer Pathology, Faculty of Medicine, WPI-ICReDD, Hokkaido University, Sapporo, Japan.

出版信息

Front Med (Lausanne). 2022 May 12;9:765805. doi: 10.3389/fmed.2022.765805. eCollection 2022.

Abstract

BACKGROUND

Various animal models of sepsis have been developed to optimize sepsis treatment. However, therapeutic agents that were successful in animal models were rarely effective in human clinical trials. The cecal ligation and puncture (CLP) model is currently the gold standard for sepsis studies. However, its limitations include the high variability among researchers and the difficulty in comparing animals with different cecum shapes and sizes. In this study, we established a protocol for the creation of a simple and accessible sepsis rodent model using fecal suspensions that minimized differences in technical effects among researchers and individual differences in animals.

METHODS

A mouse model of sepsis using fecal suspension intraperitoneal injection (FSI) was created using fresh stool excreted within 24 h. The collected fresh stool was dissolved in saline solution and filtered. The obtained fecal suspension was injected intraperitoneally into the mice. Moreover, fecal suspensions with different concentrations were prepared, and the survival rates were compared among the fecal suspensions for each concentration. To assess the validity of the FSI as a sepsis model, CLP and FSI with similar mortality rates were compared pathologically, physiologically, immunologically, and bacteriologically. Histopathological comparison was evaluated by hematoxylin-eosin and Gram staining of the parenchymal organs. Physiological evaluation was performed by comparing the respiratory rate, body temperature, and blood gas analysis results. Immunological assessment was performed using multiplex analysis. Bacteriological comparisons were performed by culturing ascites fluid.

RESULTS

The FSI model increased mortality in proportion to the fecal suspension concentration. The mortality rate was reduced with antibiotic administration. In various comparative experiments conducted using the FSI and CLP models, both models showed findings consistent with sepsis. Furthermore, the FSI model showed less variability among the individuals in each test.

CONCLUSION

This is the first detailed and accurate report of a protocol for creating a sepsis model using fecal suspension. The FSI model is a minimally invasive and accessible sepsis rodent model. Its clinical validity as a sepsis model was proven via histological, physiological, microbiological, and immunological evaluation methods. The FSI model minimizes individual differences between mice and helps to conduct accurate studies after the onset of sepsis.

摘要

背景

已开发出多种脓毒症动物模型以优化脓毒症治疗。然而,在动物模型中成功的治疗药物在人体临床试验中很少有效。盲肠结扎和穿刺(CLP)模型是目前脓毒症研究的金标准。然而,其局限性包括研究者之间的高变异性以及比较不同盲肠形状和大小的动物的困难。在本研究中,我们建立了一种使用粪便悬液创建简单且易于操作的脓毒症啮齿动物模型的方案,该方案最大限度地减少了研究者之间技术效果的差异以及动物个体差异。

方法

使用24小时内排出的新鲜粪便创建了一种通过腹腔注射粪便悬液(FSI)的小鼠脓毒症模型。将收集的新鲜粪便溶解于盐溶液中并过滤。将获得的粪便悬液腹腔注射到小鼠体内。此外,制备了不同浓度的粪便悬液,并比较了每种浓度粪便悬液的存活率。为评估FSI作为脓毒症模型的有效性,对具有相似死亡率的CLP和FSI进行了病理、生理、免疫和细菌学比较。通过对实质器官进行苏木精 - 伊红染色和革兰氏染色评估组织病理学比较。通过比较呼吸频率、体温和血气分析结果进行生理评估。使用多重分析进行免疫评估。通过腹水培养进行细菌学比较。

结果

FSI模型的死亡率随粪便悬液浓度成比例增加。给予抗生素后死亡率降低。在使用FSI和CLP模型进行的各种比较实验中,两种模型均显示出与脓毒症一致的结果。此外,FSI模型在每个测试中的个体间变异性较小。

结论

这是关于使用粪便悬液创建脓毒症模型方案的第一份详细且准确的报告。FSI模型是一种微创且易于操作的脓毒症啮齿动物模型。通过组织学、生理学、微生物学和免疫学评估方法证明了其作为脓毒症模型的临床有效性。FSI模型最大限度地减少了小鼠之间的个体差异,并有助于在脓毒症发作后进行准确的研究。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e175/9134078/1138599b05ae/fmed-09-765805-g001.jpg

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