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Immobilized stem–loop structured probes as conformational switches for enzymatic detection of microbial 16S rRNA

机译:固定的茎环结构探针作为构象开关用于酶法检测微生物16S rRNA

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摘要

We have designed and evaluated novel DNA stem–loop structured probes for enzymatic detection of nucleic acid targets. These probes constitute a novel class of conformational switches for enzymatic activity, which in the absence of a target sterically shield an affinity label and upon hybridization of the target to the recognition sequence that forms the loop of the probe restore accessibility of the label for the binding of a reporter enzyme. Analysis of probe characteristics revealed stem stability as the most important parameter governing detection functionality, while other factors such as the length of linker molecules attaching the label to the stem–loop structure and the nature of the solid support proved to be less critical. Apparently, the bulky nature of the reporter enzyme facilitates shielding of the label in the absence of the target, thereby conferring considerable structural tolerance to the conformational switch system. The stem–loop structured probes allow sensitive detection of unlabeled nucleic acid targets. Employing a microtiter assay format, 4 ng of bacterial 16S ribosomal RNA corresponding to 8 fmol could be detected, which can be compared favorably with current immobilized molecular beacon concepts based on fluorescence detection.
机译:我们已经设计和评估了用于酶促检测核酸靶标的新型DNA茎环结构探针。这些探针构成用于酶活性的新型构象开关,其在没有靶标的情况下在空间上屏蔽亲和标记,并且在靶标与形成探针环的识别序列杂交后,恢复了标记物与结合的可及性。报告酶。探针特性分析表明,茎的稳定性是支配检测功能的最重要参数,而其他因素(例如,将标记附加至茎-环结构的接头分子的长度和固体支持物的性质)就不那么重要了。显然,报告酶的庞大性质有助于在不存在靶标的情况下屏蔽标记,从而赋予构象转换系统相当大的结构耐受性。茎环结构的探针可以灵敏地检测未标记的核酸靶标。采用微量滴定分析法,可以检测到4 ng细菌细菌16S核糖体RNA,对应于8 fmol,可以与当前基于荧光检测的固定分子信标概念相媲美。

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