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合成和修饰肽以进行化学选择性连接,并组装成量子点-肽生物共轭物。

Synthesizing and modifying peptides for chemoselective ligation and assembly into quantum dot-peptide bioconjugates.

作者信息

Algar W Russ, Blanco-Canosa Juan B, Manthe Rachel L, Susumu Kimihiro, Stewart Michael H, Dawson Philip E, Medintz Igor L

机构信息

Naval Research Laboratory, Washington, DC, USA.

出版信息

Methods Mol Biol. 2013;1025:47-73. doi: 10.1007/978-1-62703-462-3_5.

DOI:10.1007/978-1-62703-462-3_5
PMID:23918329
Abstract

Quantum dots (QDs) are well-established as photoluminescent nanoparticle probes for in vitro or in vivo imaging, sensing, and even drug delivery. A critical component of this research is the need to reliably conjugate peptides, proteins, oligonucleotides, and other biomolecules to QDs in a controlled manner. In this chapter, we describe the conjugation of peptides to CdSe/ZnS QDs using a combination of polyhistidine self-assembly and hydrazone ligation. The former is a high-affinity interaction with the inorganic surface of the QD; the latter is a highly efficient and chemoselective reaction that occurs between 4-formylbenzoyl (4FB) and 2-hydrazinonicotinoyl (HYNIC) moieties. Two methods are presented for modifying peptides with these functional groups: (1) solid phase peptide synthesis; and (2) solution phase modification of pre-synthesized, commercial peptides. We further describe the aniline-catalyzed ligation of 4FB- and HYNIC-modified peptides, in the presence of a fluorescent label on the latter peptide, as well as subsequent assembly of the ligated peptide to water-soluble QDs. Many technical elements of these protocols can be extended to labeling peptides with other small molecule reagents. Overall, the bioconjugate chemistry is robust, selective, and modular, thereby potentiating the controlled conjugation of QDs with a diverse array of biomolecules for various applications.

摘要

量子点(QDs)作为用于体外或体内成像、传感甚至药物递送的光致发光纳米颗粒探针已得到广泛认可。这项研究的一个关键组成部分是需要以可控的方式将肽、蛋白质、寡核苷酸和其他生物分子可靠地偶联到量子点上。在本章中,我们描述了使用多组氨酸自组装和腙连接相结合的方法将肽偶联到CdSe/ZnS量子点上。前者是与量子点无机表面的高亲和力相互作用;后者是在4-甲酰基苯甲酰基(4FB)和2-肼基烟酰基(HYNIC)部分之间发生的高效且化学选择性反应。介绍了两种用这些官能团修饰肽的方法:(1)固相肽合成;(2)对预先合成的商业肽进行溶液相修饰。我们进一步描述了在后者肽上存在荧光标记的情况下,苯胺催化的4FB和HYNIC修饰肽的连接,以及随后将连接的肽组装到水溶性量子点上。这些方案的许多技术要素可以扩展到用其他小分子试剂标记肽。总体而言,生物共轭化学是稳健、选择性和模块化的,从而增强了量子点与各种生物分子的可控偶联,以用于各种应用。

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