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首页> 外文期刊>European Journal of Nuclear Medicine and Molecular Imaging >Noninvasive PET tracking of post-transplant gut microbiota in living mice
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Noninvasive PET tracking of post-transplant gut microbiota in living mice

机译:移植后肠道微生物在生物小鼠中的非侵入性宠物跟踪

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Purpose The role that gut microbiota plays in determining the efficacy of the anti-tumor effect of immune checkpoint inhibitors is gaining increasing attention, and fecal bacterial transplantation has been recognized as a promising strategy for improving or rescuing the effect of immune checkpoint inhibition. However, techniques for the precise monitoring of in vivo bacterial behaviors after transplantation are limited. In this study, we aimed to use metabolic labeling and subsequent positron emission tomography (PET) imaging to track the in vivo behaviors of gut bacteria that are responsible for the efficacy of anti-PD-1 therapy in living mice. Methods The antitumor effect of anti-PD-1 blockade was tested in a low-response 4T1 syngeneic mouse model with or without fecal transplantation and with or without broad-spectrum antibiotic imipenem treatment. High-throughput sequencing analyses of 16S rRNA gene amplicons in feces of 4T1 tumor-bearing mice pre- and post-anti-PD-1 treatment were performed. The identified bacteria, Bacteroides fragilis (B. fragilis), were labeled with Cu-64 and fluorescence dye by the metabolic labeling of N-3 followed by click chemistry. In vivo PET and optical imaging of B. fragilis were performed in mice after oral gavage. Results The disturbance of gut microbiota reduced the efficacy of anti-PD-1 treatment, and the combination of B. fragilis gavage and PD-1 blockade was beneficial in rescuing the antitumor effect of anti-PD-1 therapy. Metabolic oligosaccharide engineering and biorthogonal click chemistry resulted in successful B. fragilis labeling with Cu-64 and fluorescence dye with high in vitro and in vivo stability and no effect on viability. PET imaging successfully detected the in vivo behaviors of B. fragilis after transplantation. Conclusion PET tracking by metabolic labeling is a powerful, noninvasive tool for the real-time tracking and quantitative imaging of gut microbiota. This strategy is clinically translatable and may also be extended to the PET tracking of other functional cells to guide cell-based adoptive therapies.
机译:目的,肠道微生物群在确定免疫检查点抑制剂的抗肿瘤作用的功效时发挥的作用正在增加注意力,并且粪便细菌移植被认为是改善或拯救免疫检查点抑制作用的有希望的策略。然而,在移植后体内细菌行为的精确监测的技术有限。在这项研究中,我们旨在使用代谢标记和随后的正电子发射断层扫描(PET)成像,以跟踪肠道细菌的体内行为,这些肠道细菌负责抗PD-1治疗在生物小鼠中的疗效。方法使用或不具有粪便移植的低响应4T1同胞小鼠模型测试抗PD-1阻断的抗肿瘤效应,或没有育种抗生素亚胺蛋白治疗。进行了抗PD-1治疗前和抗PD-1后4T1肿瘤小鼠粪便中的16S rRNA基因扩增子的高通量测序分析。通过N-3的代谢标记,用Cu-64和荧光染料标记已鉴定的细菌,用Cu-64和荧光染料标记,然后单击化学。体内PET和B的光学成像。在口腔饲养后在小鼠中进行脆弱。结果肠道微生物的干扰降低了抗PD-1治疗的功效,B.Fragilis Gavage和PD-1阻断的组合是有益的抵御抗PD-1治疗的抗肿瘤效果。代谢寡糖工程和双正交咔哒化学导致成功的B. Fragilis标记用Cu-64和荧光染料,具有高体外和体内稳定性,对活力没有影响。宠物成像在移植后成功地检测到B.Frellilis的体内行为。结论代谢标签的PET跟踪是一种强大的非侵入性工具,用于肠道微生物的实时跟踪和定量成像。该策略在临床上可翻译,也可以扩展到其他功能细胞的宠物跟踪以引导基于细胞的养护疗法。

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