m6A-modified exosome-derived circHIF1α binding to KH domain of IGF2BP3 mediates DNA damage and arrests G1/S transition phase to resists bacterial infection in bacteremia.

IF 10.6 1区 生物学 Q1 BIOTECHNOLOGY & APPLIED MICROBIOLOGY
Jiang Yu, Yidan Gao, Fei Liu, Yuyu Zhang, Jianda Li, Luogang Ding, Sufang Ren, Jie Yang, Jian Jiao, Gong Feng, Zhi Chen, Wenbo Sun, Jiaqiang Wu
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引用次数: 0

Abstract

Background: Animal and human health are seriously threatened by bacterial infections, which can lead to bacteremia and extremely high rates of morbidity and mortality. Recently, there have been reports indicating the involvement of exosomal circular RNAs (circRNAs) in a range of human disorders and tumor types. However, the role of exosomal circRNAs in bacterial infection remains elusive.

Methods: We extracted and identified exosomes from the culture medium of PIEC cells infected with or without Glaesserella parasuis. RNA sequencing analysis was performed on the exosomes to screen and identify circRNAs (circHIF1α) associated with Glaesserella parasuis infection. PIEC cells were infected with Staphylococcus aureus or Streptococcus suis 2 to further determine whether exosome-derived circHIF1α was the crucial circHIF1α associated with bacterial infections. The transmission process of exosomes and their circHIF1α between cells was clarified via exosome tracing and co-culture assay. Moreover, the mechanism of circHIF1α being packaged into exosomes was explored, and the effects of exosomes and their circHIF1α on cell proliferation, DNA damage and cell cycle were analyzed. In addition, the binding mode and site of interacting proteins with circHIF1α were further determined. In vivo and in vitro, the role of exosomes and their circHIF1α in host resistance to bacterial infection was confirmed.

Results: We first discovered a new circHIF1α that was very stable and detectable, encapsulated into exosomes by hnRNPA2B1, and whose expression in exosomes of bacterially infected PIEC cells significantly decreased. Additionally, exosomal circHIF1α reduced bacterial infection both in vitro and in vivo and suppressed the growth of reception cells. Mechanistically, the circHIF1α interacted with the KH domain of IGF2BP3 in an m6A-modified manner, which mediated DNA damage to arrest the cells at the G1/S phase through the interaction between the regulator of Chromosome Condensation 2 (RCC2) and γ-H2AX protein. Exosomal circHIF1α is a unique therapeutic target for bacterial infection since this work highlights its critical function in fighting bacterial infection.

m6A修饰的外泌体衍生的circHIF1α与IGF2BP3的KH结构域结合可介导DNA损伤并阻止G1/S转换期,从而在菌血症中抵抗细菌感染。
背景:细菌感染严重威胁着动物和人类的健康,可导致菌血症以及极高的发病率和死亡率。最近有报告表明,外泌体循环 RNA(circRNA)参与了一系列人类疾病和肿瘤类型。然而,外泌体环状核糖核酸在细菌感染中的作用仍然难以捉摸:方法:我们从感染或未感染寄生璃泽氏菌的 PIEC 细胞的培养液中提取并鉴定了外泌体。我们对外泌体进行了RNA测序分析,以筛选和鉴定与寄生璃泽氏菌感染相关的circRNAs(circHIF1α)。用金黄色葡萄球菌或猪链球菌2感染PIEC细胞,进一步确定外泌体衍生的circHIF1α是否是与细菌感染相关的关键circHIF1α。通过外泌体追踪和共培养试验,阐明了外泌体及其circHIF1α在细胞间的传播过程。此外,还探讨了circHIF1α被包装到外泌体中的机制,分析了外泌体及其circHIF1α对细胞增殖、DNA损伤和细胞周期的影响。此外,还进一步确定了与 circHIF1α 相互作用的蛋白质的结合模式和位点。在体内和体外,外泌体及其circHIF1α在宿主抵抗细菌感染中的作用得到了证实:结果:我们首次发现了一种新的circHIF1α,它非常稳定且可检测,被hnRNPA2B1包裹到外泌体中,其在细菌感染的PIEC细胞外泌体中的表达量显著下降。此外,外泌体 circHIF1α 可减少体外和体内的细菌感染,并抑制接收细胞的生长。从机理上讲,circHIF1α以m6A修饰的方式与IGF2BP3的KH结构域相互作用,通过染色体凝集调节因子2(RCC2)和γ-H2AX蛋白之间的相互作用,介导DNA损伤,使细胞停滞在G1/S期。外泌体circHIF1α是细菌感染的一个独特治疗靶点,因为这项研究强调了它在对抗细菌感染中的关键功能。
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来源期刊
Journal of Nanobiotechnology
Journal of Nanobiotechnology BIOTECHNOLOGY & APPLIED MICROBIOLOGY-NANOSCIENCE & NANOTECHNOLOGY
CiteScore
13.90
自引率
4.90%
发文量
493
审稿时长
16 weeks
期刊介绍: Journal of Nanobiotechnology is an open access peer-reviewed journal communicating scientific and technological advances in the fields of medicine and biology, with an emphasis in their interface with nanoscale sciences. The journal provides biomedical scientists and the international biotechnology business community with the latest developments in the growing field of Nanobiotechnology.
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