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通过表观遗传印迹工程化选择性地分离痤疮丙酸杆菌噬菌体。

Engineering selectivity of Cutibacterium acnes phages by epigenetic imprinting.

机构信息

Department of Medicine and Life Sciences, Universitat Pompeu Fabra, Barcelona, Spain.

Sbiomedic, Beerse, Belgium.

出版信息

PLoS Pathog. 2022 Mar 28;18(3):e1010420. doi: 10.1371/journal.ppat.1010420. eCollection 2022 Mar.

Abstract

Cutibacterium acnes (C. acnes) is a gram-positive bacterium and a member of the human skin microbiome. Despite being the most abundant skin commensal, certain members have been associated with common inflammatory disorders such as acne vulgaris. The availability of the complete genome sequences from various C. acnes clades have enabled the identification of putative methyltransferases, some of them potentially belonging to restriction-modification (R-M) systems which protect the host of invading DNA. However, little is known on whether these systems are functional in the different C. acnes strains. To investigate the activity of these putative R-M and their relevance in host protective mechanisms, we analyzed the methylome of six representative C. acnes strains by Oxford Nanopore Technologies (ONT) sequencing. We detected the presence of a 6-methyladenine modification at a defined DNA consensus sequence in strain KPA171202 and recombinant expression of this R-M system confirmed its methylation activity. Additionally, a R-M knockout mutant verified the loss of methylation properties of the strain. We studied the potential of one C. acnes bacteriophage (PAD20) in killing various C. acnes strains and linked an increase in its specificity to phage DNA methylation acquired upon infection of a methylation competent strain. We demonstrate a therapeutic application of this mechanism where phages propagated in R-M deficient strains selectively kill R-M deficient acne-prone clades while probiotic ones remain resistant to phage infection.

摘要

痤疮丙酸杆菌(C. acnes)是一种革兰氏阳性菌,也是人类皮肤微生物组的成员。尽管它是最丰富的皮肤共生菌,但某些成员与常见的炎症性疾病有关,如寻常痤疮。各种 C. acnes 进化枝的完整基因组序列的可用性使得能够鉴定假定的甲基转移酶,其中一些可能属于限制修饰(R-M)系统,这些系统可以保护宿主免受入侵 DNA 的侵害。然而,关于这些系统在不同 C. acnes 菌株中是否具有功能,人们知之甚少。为了研究这些假定的 R-M 系统的活性及其在宿主保护机制中的相关性,我们通过牛津纳米孔技术(ONT)测序分析了六种代表性 C. acnes 菌株的甲基组。我们在 KPA171202 菌株中检测到在定义的 DNA 共有序列处存在 6-甲基腺嘌呤修饰,并且该 R-M 系统的重组表达证实了其甲基化活性。此外,R-M 敲除突变体验证了该菌株失去了甲基化特性。我们研究了一种 C. acnes 噬菌体(PAD20)在杀死各种 C. acnes 菌株中的潜力,并将其特异性的增加与感染具有甲基化能力的菌株时获得的噬菌体 DNA 甲基化联系起来。我们证明了这种机制的一种治疗应用,其中在 R-M 缺陷菌株中繁殖的噬菌体选择性地杀死 R-M 缺陷的易长粉刺的进化枝,而益生菌则对噬菌体感染保持抗性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0f0d/8989293/3123d682079d/ppat.1010420.g001.jpg

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