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在深层组织部位生长过程中发现的病原体社交行为的拓扑正确合成重建。

Topologically correct synthetic reconstruction of pathogen social behavior found during growth in deep tissue sites.

机构信息

Department of Molecular Biology and Microbiology, Tufts University Graduate School of Biomedical Sciences, Boston, United States.

Graduate Program in Molecular Microbiology, Tufts University Graduate School of Biomedical Sciences, Boston, United States.

出版信息

Elife. 2020 Jun 16;9:e58106. doi: 10.7554/eLife.58106.

Abstract

Within deep tissue sites, extracellular bacterial pathogens often replicate in clusters that are surrounded by immune cells. Disease is modulated by interbacterial interactions as well as bacterial-host cell interactions resulting in microbial growth, phagocytic attack and secretion of host antimicrobial factors. To overcome the limited ability to manipulate these infection sites, we established a system for ( growth in microfluidics-driven microdroplets that regenerates microbial social behavior in tissues. Chemical generation of nitric oxide (NO) in the absence of immune cells was sufficient to reconstruct microbial social behavior, as witnessed by expression of the NO-inactivating protein Hmp on the extreme periphery of microcolonies, mimicking spatial regulation in tissues. Similarly, activated macrophages that expressed inducible NO synthase (iNOS) drove peripheral expression of Hmp, allowing regeneration of social behavior observed in tissues. These results argue that topologically correct microbial tissue growth and associated social behavior can be reconstructed in culture.

摘要

在深部组织部位,细胞外细菌病原体通常在被免疫细胞包围的集群中复制。疾病的发生受到细菌间相互作用以及细菌-宿主细胞相互作用的调节,导致微生物生长、吞噬作用和宿主抗菌因子的分泌。为了克服对这些感染部位的有限操纵能力,我们建立了一种在微流控驱动的微滴中生长的系统,该系统在组织中再生微生物的社会行为。在没有免疫细胞的情况下,化学产生一氧化氮(NO)足以重建微生物的社会行为,这可以从微菌落极端外围的 NO 失活蛋白 Hmp 的表达中得到证明,这模拟了组织中的空间调节。同样,表达诱导型一氧化氮合酶(iNOS)的活化巨噬细胞驱动 Hmp 的外周表达,从而允许在组织中观察到的社会行为的再生。这些结果表明,可以在培养物中重建拓扑正确的微生物组织生长和相关的社会行为。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/939d/7316508/77e5d64bdbd3/elife-58106-fig1.jpg

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