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细菌病原体汉氏巴尔通体的 VirB/VirD4 型 IV 型分泌系统将共轭 DNA 转移到人类细胞中。

Conjugative DNA transfer into human cells by the VirB/VirD4 type IV secretion system of the bacterial pathogen Bartonella henselae.

机构信息

Biozentrum, University of Basel, 4056 Basel, Switzerland.

出版信息

Proc Natl Acad Sci U S A. 2011 Aug 30;108(35):14643-8. doi: 10.1073/pnas.1019074108. Epub 2011 Aug 15.

Abstract

Bacterial type IV secretion systems (T4SS) mediate interbacterial conjugative DNA transfer and transkingdom protein transfer into eukaryotic host cells in bacterial pathogenesis. The sole bacterium known to naturally transfer DNA into eukaryotic host cells via a T4SS is the plant pathogen Agrobacterium tumefaciens. Here we demonstrate T4SS-mediated DNA transfer from a human bacterial pathogen into human cells. We show that the zoonotic pathogen Bartonella henselae can transfer a cryptic plasmid occurring in the bartonellae into the human endothelial cell line EA.hy926 via its T4SS VirB/VirD4. DNA transfer into EA.hy926 cells was demonstrated by using a reporter derivative of this Bartonella-specific mobilizable plasmid generated by insertion of a eukaryotic egfp-expression cassette. Fusion of the C-terminal secretion signal of the endogenous VirB/VirD4 protein substrate BepD with the plasmid-encoded DNA-transport protein Mob resulted in a 100-fold increased DNA transfer rate. Expression of the delivered egfp gene in EA.hy926 cells required cell division, suggesting that nuclear envelope breakdown may facilitate passive entry of the transferred ssDNA into the nucleus as prerequisite for complementary strand synthesis and transcription of the egfp gene. Addition of an eukaryotic neomycin phosphotransferase expression cassette to the reporter plasmid facilitated selection of stable transgenic EA.hy926 cell lines that display chromosomal integration of the transferred plasmid DNA. Our data suggest that T4SS-dependent DNA transfer into host cells may occur naturally during human infection with Bartonella and that these chronically infecting pathogens have potential for the engineering of in vivo gene-delivery vectors with applications in DNA vaccination and therapeutic gene therapy.

摘要

细菌 IV 型分泌系统 (T4SS) 在细菌发病机制中介导细菌间的共轭 DNA 转移和跨王国蛋白转移到真核宿主细胞中。已知唯一通过 T4SS 将 DNA 自然转移到真核宿主细胞中的细菌是植物病原体根癌农杆菌。在这里,我们证明了 T4SS 介导的从人类病原体细菌向人类细胞的 DNA 转移。我们表明,人畜共患病病原体汉赛巴尔通体可以通过其 T4SS VirB/VirD4 将发生在巴尔通体中的隐秘质粒转移到人类内皮细胞系 EA.hy926 中。通过插入真核 egfp 表达盒生成的这种巴尔通体特异性可移动质粒的报告衍生质粒,证明了 DNA 转移到 EA.hy926 细胞中。内源性 VirB/VirD4 蛋白底物 BepD 的 C 末端分泌信号与质粒编码的 DNA 转运蛋白 Mob 的融合导致 DNA 转移率提高了 100 倍。在 EA.hy926 细胞中表达递送的 egfp 基因需要细胞分裂,这表明核膜破裂可能促进转移的 ssDNA 被动进入细胞核,作为互补链合成和 egfp 基因转录的前提。向报告质粒中添加真核新霉素磷酸转移酶表达盒,有助于选择稳定的转基因 EA.hy926 细胞系,这些细胞系显示转移的质粒 DNA 已整合到染色体中。我们的数据表明,在人类感染巴尔通体期间,T4SS 依赖性 DNA 转移到宿主细胞中可能自然发生,并且这些慢性感染的病原体具有在体内基因传递载体工程中的潜力,可应用于 DNA 疫苗接种和治疗性基因治疗。

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