首页> 外文期刊>The Journal of Experomental Medicine >Targeted Gene Disruption Reveals an Adhesin Indispensable for Pathogenicity of Blastomyces dermatitidis
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Targeted Gene Disruption Reveals an Adhesin Indispensable for Pathogenicity of Blastomyces dermatitidis

机译:靶向的基因破坏揭示了皮肤芽孢杆菌的致病性必不可少的粘附素。

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Systemic fungal infections are becoming more common and difficult to treat, yet the pathogenesis of these infectious diseases remains poorly understood. In many cases, pathogenicity can be attributed to the ability of the fungi to adhere to target tissues, but the lack of tractable genetic systems has limited progress in understanding and interfering with the offending fungal products. In Blastomyces dermatitidis , the agent of blastomycosis, a respiratory and disseminated mycosis of people and animals worldwide, expression of the putative adhesin encoded by the WI-1 gene was investigated as a possible virulence factor. DNA-mediated gene transfer was used to disrupt the WI-1 locus by allelic replacement, resulting in impaired binding and entry of yeasts into macrophages, loss of adherence to lung tissue, and abolishment of virulence in mice; each of these properties was fully restored after reconstitution of WI-1 by means of gene transfer. These findings establish the pivotal role of WI-1 in adherence and virulence of B . dermatitidis yeasts. To our knowledge, they offer the first example of a genetically proven virulence determinant among systemic dimorphic fungi, and underscore the value of reverse genetics for studies of pathogenesis in these organisms.
机译:全身性真菌感染正变得越来越普遍且难以治疗,但对这些传染病的发病机理仍知之甚少。在许多情况下,致病性可以归因于真菌粘附至目标组织的能力,但是缺乏易处理的遗传系统限制了在了解和干扰有害真菌产品方面的进展。在皮肤病菌Blastomyces dermatitidis中,作为一种可能的致病因子,研究了WI-1基因编码的假定黏附素的表达。 DNA介导的基因转移被用于通过等位基因置换破坏WI-1基因座,导致酵母的结合减弱和进入巨噬细胞,丧失对肺组织的附着力,并消除小鼠的毒力。通过基因转移,WI-1重组后,所有这些特性都得到了完全恢复。这些发现建立了WI-1在B的粘附和毒力中的关键作用。皮肤病酵母。据我们所知,它们提供了遗传证明的系统性双态真菌中毒力决定因素的第一个例子,并强调了反向遗传学在这些生物发病机理研究中的价值。

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