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小肠结肠炎耶尔森菌在三维胶原蛋白凝胶中不寻常的、毒力质粒依赖性生长行为。

Unusual, virulence plasmid-dependent growth behavior of Yersinia enterocolitica in three-dimensional collagen gels.

作者信息

Freund Sandra, Czech Beate, Trülzsch Konrad, Ackermann Nikolaus, Heesemann Jürgen

机构信息

Max von Pettenkofer Institute for Hygiene and Medical Microbiology, Ludwig Maximilians University, D-80336 Munich, Germany.

出版信息

J Bacteriol. 2008 Jun;190(12):4111-20. doi: 10.1128/JB.00156-08. Epub 2008 Apr 11.

Abstract

As a first approach to establishing a three-dimensional culture infection model, we studied the growth behavior of the extracellular pathogen Yersinia enterocolitica in three-dimensional collagen gels (3D-CoG). Surprisingly, we observed that plasmidless Y. enterocolitica was motile in the 3D-CoG in contrast to its growth in traditional motility agar at 37 degrees C. Motility at 37 degrees C was abrogated in the presence of the virulence plasmid pYV or the exclusive expression of the pYV-located Yersinia adhesion gene yadA. YadA-producing yersiniae formed densely packed (dp) microcolonies, whereas pYVDelta yadA-carrying yersiniae formed loosely packed microcolonies at 37 degrees C in 3D-CoG. Furthermore, we demonstrated that the packing density of the microcolonies was dependent on the head domain of YadA. Moreover, dp microcolony formation did not depend on the capacity of YadA to bind to collagen fibers, as demonstrated by the use of yersiniae producing collagen nonbinding YadA. By using a yopE-gfp reporter, we demonstrated Ca(2+)-dependent expression of this pYV-localized virulence gene by yersiniae in 3D-CoG. In conclusion, this study revealed unique plasmid-dependent growth behavior of yersiniae in a three-dimensional matrix environment that resembles the behavior of yersiniae (e.g., formation of microcolonies) in infected mouse tissue. Thus, this 3D-CoG model may be a first step to a more complex level of in vitro infection models that mimic living tissue, enabling us to study the dynamics of pathogen-host cell interactions.

摘要

作为建立三维培养感染模型的第一步,我们研究了细胞外病原体小肠结肠炎耶尔森菌在三维胶原蛋白凝胶(3D-CoG)中的生长行为。令人惊讶的是,我们观察到无质粒的小肠结肠炎耶尔森菌在3D-CoG中具有运动性,这与其在37℃传统运动性琼脂中的生长情况形成对比。在毒力质粒pYV存在或pYV定位的耶尔森菌粘附基因yadA单独表达时,37℃下的运动性被消除。产生YadA的耶尔森菌形成紧密堆积(dp)的微菌落,而携带pYVDelta yadA的耶尔森菌在37℃的3D-CoG中形成松散堆积的微菌落。此外,我们证明微菌落的堆积密度取决于YadA的头部结构域。而且,如使用产生不结合胶原蛋白的YadA的耶尔森菌所证明的,dp微菌落的形成不依赖于YadA结合胶原蛋白纤维的能力。通过使用yopE-gfp报告基因,我们证明了耶尔森菌在3D-CoG中Ca(2+)依赖的该pYV定位毒力基因的表达。总之,本研究揭示了耶尔森菌在三维基质环境中独特的质粒依赖性生长行为,这种行为类似于耶尔森菌在感染小鼠组织中的行为(例如微菌落的形成)。因此,这种3D-CoG模型可能是迈向更复杂的体外感染模型的第一步,该模型可模拟活组织,使我们能够研究病原体与宿主细胞相互作用的动态过程。

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