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细菌在体内的部分重编程促进成年肝脏器官生长而无纤维化和肿瘤发生。

In vivo partial reprogramming by bacteria promotes adult liver organ growth without fibrosis and tumorigenesis.

机构信息

Institute for Regeneration and Repair, The University of Edinburgh, Edinburgh, UK; Centre for Regenerative Medicine, The University of Edinburgh, Edinburgh, UK.

Institute for Regeneration and Repair, The University of Edinburgh, Edinburgh, UK; Centre for Inflammation Research, The University of Edinburgh, Edinburgh, UK; Edinburgh Pathology, The University of Edinburgh, Edinburgh, UK.

出版信息

Cell Rep Med. 2022 Nov 15;3(11):100820. doi: 10.1016/j.xcrm.2022.100820.

Abstract

Ideal therapies for regenerative medicine or healthy aging require healthy organ growth and rejuvenation, but no organ-level approach is currently available. Using Mycobacterium leprae (ML) with natural partial cellular reprogramming capacity and its animal host nine-banded armadillos, we present an evolutionarily refined model of adult liver growth and regeneration. In infected armadillos, ML reprogram the entire liver and significantly increase total liver/body weight ratio by increasing healthy liver lobules, including hepatocyte proliferation and proportionate expansion of vasculature, and biliary systems. ML-infected livers are microarchitecturally and functionally normal without damage, fibrosis, or tumorigenesis. Bacteria-induced reprogramming reactivates liver progenitor/developmental/fetal genes and upregulates growth-, metabolism-, and anti-aging-associated markers with minimal change in senescence and tumorigenic genes, suggesting bacterial hijacking of homeostatic, regeneration pathways to promote de novo organogenesis. This may facilitate the unraveling of endogenous pathways that effectively and safely re-engage liver organ growth, with broad therapeutic implications including organ regeneration and rejuvenation.

摘要

理想的再生医学或健康衰老疗法需要健康的器官生长和 rejuvenation,但目前没有器官水平的方法。利用分枝杆菌(ML)具有天然的部分细胞重编程能力及其动物宿主九带犰狳,我们提出了一种进化上成熟的成年肝脏生长和再生模型。在受感染的犰狳中,ML 对整个肝脏进行重编程,并通过增加健康的肝小叶(包括肝细胞增殖和血管系统以及胆管系统的比例性扩张),显著增加总肝/体重比。受 ML 感染的肝脏在微观结构和功能上正常,没有损伤、纤维化或肿瘤发生。细菌诱导的重编程激活了肝祖细胞/发育/胎儿基因,并上调了与生长、代谢和抗衰老相关的标志物,衰老和致瘤基因的变化最小,这表明细菌劫持了维持平衡、再生途径以促进新器官发生。这可能有助于揭示有效的、安全地重新激活肝脏器官生长的内源性途径,具有广泛的治疗意义,包括器官再生和 rejuvenation。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a76b/9729881/4007564ac486/fx1.jpg

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