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首页> 外文期刊>Biosensors & Bioelectronics: The International Journal for the Professional Involved with Research, Technology and Applications of Biosensers and Related Devices >Functionalized aptamer with an antiparallel G-quadruplex: Structural remodeling, recognition mechanism, and diagnostic applications targeting CTGF
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Functionalized aptamer with an antiparallel G-quadruplex: Structural remodeling, recognition mechanism, and diagnostic applications targeting CTGF

机译:具有反平行G-Quadruplex的功能化适体:结构重塑,识别机制和靶向CTGF的诊断应用

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摘要

Connective tissue growth factor (CTGF), a widely used biomarker, is involved in many diseases, such as diabetic retinopathy, diabetic nephropathy, and rheumatoid arthritis, and it is often over-expressed in human malignant tumors. Therefore, sensitive, specific and efficient detection methods for CTGF are needed for the early diagnosis and assessment of prognosis. In this study, an aptamer, APT1, that specifically binds to CTGF was obtained by SELEX technology. Circular dichroism spectroscopy indicated that APT1 formed interconvertible parallel and antiparallel G-quadruplexes. Mutation and truncation strategies optimized APT1 and improved its functions, yielding APT1M6T, which folded into an antiparallel G-quadruplex with higher targeting affinity. A stable APT1M6T-CTGF complex model was established by molecular simulation, which helped elucidate the molecular recognition mechanism of APT1M6T and CTGF and also provided experimental guidance for rational site-directed modification of APT1M6T. A locked nucleic acid sequence was then integrated into APT1M6T to generate APT1M6TL, which had higher structural stability. A BLI-based enzyme-linked aptamer sandwich assay (BLI-ELASA) was successfully developed. The method exhibited a broad detection range from 0.05 to 50 nM with a low detection limit of 0.02 nM. The method showed high selectivity, reproducibility, and stability for analysis of CTGF in spiked serum and urine samples. This developed BLI-ELASA is promising and enables real-time, sensitive and rapid detection of the disease-specific biomarker CTGF.
机译:结缔组织生长因子(CTGF)是广泛使用的生物标志物,涉及许多疾病,例如糖尿病视网膜病,糖尿病肾病和类风湿性关节炎,并且通常在人体恶性肿瘤中过度表达。因此,早期诊断和评估预后需要对CTGF进行敏感,具体和有效的检测方法。在该研究中,通过SELEX技术获得特异性结合CTGF的适体APT1。圆形二色谱表明APT1形成相互渗透并联和反平行的G-四边形。突变和截断策略优化APT1并改善其功能,产生APT1M6T,其折叠成具有更高靶向亲和力的反平行G-Quadruple。通过分子模拟建立了稳定的APT1M6T-CTGF复杂模型,这有助于阐明APT1M6T和CTGF的分子识别机制,并为APT1M6T的理性部位导向修饰提供了实验指导。然后将锁定的核酸序列集成到APT1M6T中以产生APT1M6T1,其具有更高的结构稳定性。成功开发了一种基于BLI的酶联Aptamer Sandwich测定(Bli-Elasa)。该方法具有0.05至50nm的宽检测范围,检测限为0.02nm。该方法显示出高的选择性,再现性和用于分析尖刺血清和尿液样品的CTGF的稳定性。这种发达的Bli-Elasa是有前途的,并且能够进行实时,敏感和快速地检测疾病特异性生物标志物CTGF。

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