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利用铬化聚二乙炔组装体作为平台来探测药物与RNA之间的特异性结合。

Utilization of chromic polydiacetylene assemblies as a platform to probe specific binding between drug and RNA.

作者信息

Kamphan Anothai, Gong Changjun, Maiti Krishnagopal, Sur Souvik, Traiphol Rakchart, Arya Dev P

机构信息

Department of Chemistry, Faculty of Science, Naresuan University, Phitsanulok 65000, Thailand.

Laboratory of Advanced Polymers and Nanomaterials, School of Materials Science and Engineering and Center of Excellence for Innovation in Chemistry, Faculty of Science, Mahidol University at Salaya, Phuttamonthon 4 Road, Salaya, Nakhon Pathom 73170, Thailand.

出版信息

RSC Adv. 2017;7(66):41435-41443. doi: 10.1039/C7RA07178G. Epub 2017 Aug 24.

Abstract

Recognition of nucleic acids remains an important endeavor in biology. Nucleic acids adopt shapes ranging from A-form (RNA and GC rich DNA) to B-form (AT rich DNA). We show, in this contribution, shape-specific recognition of A-U rich RNA duplex by a neomycin (Neo)-polydiacetylene (PDA) complex. PDA assemblies are fabricated by using a well-known diacetylene (DA) monomer, 10,12-pentacosadiynoic acid (PCDA). The response of poly(PCDA) assemblies is generated by mixing with a modified neomycin-PCDA monomer (Neo-PCDA). The functionalization by neomycin moiety provides specific binding with homopolyribonucleotide poly (rA) - poly (rU) stimulus. Various types of alcohols are utilized as additives to enhance the sensitivity of poly(PCDA)/Neo-PCDA assemblies. A change of absorption spectra is clearly observed when a relatively low concentration of poly (rA)-poly (rU) is added into the system. Furthermore, poly(PCDA)/Neo-PCDA shows a clear specificity for poly (rA)-poly (rU) over the corresponding DNA duplex. The variation of linker between neomycin moiety and conjugated PDA backbone is found to significantly affect its sensitivity. We also investigate other parameters including the concentration of Neo-PCDA and the DA monomer structure. Our results provide here preliminary data for an alternative approach to improve the sensitivity of PDA utilized in biosensing and diagnostic applications.

摘要

核酸识别仍然是生物学中的一项重要工作。核酸具有从A-型(RNA和富含GC的DNA)到B-型(富含AT的DNA)等多种形状。在本论文中,我们展示了新霉素(Neo)-聚二乙炔(PDA)复合物对富含A-U的RNA双链体的形状特异性识别。PDA组装体是通过使用一种著名的二乙炔(DA)单体——10,12-二十五碳二炔酸(PCDA)制备而成。聚(PCDA)组装体的响应是通过与一种修饰的新霉素-PCDA单体(Neo-PCDA)混合产生的。新霉素部分的功能化提供了与同聚核糖核苷酸聚(rA)-聚(rU)刺激物的特异性结合。使用各种类型的醇作为添加剂来提高聚(PCDA)/Neo-PCDA组装体的灵敏度。当向系统中加入相对低浓度的聚(rA)-聚(rU)时,可以清楚地观察到吸收光谱的变化。此外,聚(PCDA)/Neo-PCDA对聚(rA)-聚(rU)表现出明显高于相应DNA双链体的特异性。发现新霉素部分与共轭PDA主链之间连接子的变化会显著影响其灵敏度。我们还研究了其他参数,包括Neo-PCDA的浓度和DA单体结构。我们的结果为提高用于生物传感和诊断应用的PDA灵敏度的替代方法提供了初步数据。

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