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Site isolation of emitters within cross-linked polymer nanoparticles for white electroluminescence.交联聚合物纳米粒子内辐射体的站点隔离实现白色电致发光。
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Azlactone-functionalized polymers as reactive templates for parallel polymer synthesis: synthesis and screening of a small library of cationic polymers in the context of DNA delivery.氮丙啶功能化聚合物作为用于平行聚合反应的活性模板:在 DNA 递送背景下阳离子聚合物的小文库的合成和筛选。
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用于细胞内递送的化学多样性核壳纳米粒子的组合合成。

Combinatorial synthesis of chemically diverse core-shell nanoparticles for intracellular delivery.

机构信息

David H Koch Institute for Integrative Cancer Research, Massachusetts Institute of Technology, Cambridge, MA 02139, USA.

出版信息

Proc Natl Acad Sci U S A. 2011 Aug 9;108(32):12996-3001. doi: 10.1073/pnas.1106379108. Epub 2011 Jul 22.

DOI:10.1073/pnas.1106379108
PMID:21784981
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3156157/
Abstract

Analogous to an assembly line, we employed a modular design for the high-throughput study of 1,536 structurally distinct nanoparticles with cationic cores and variable shells. This enabled elucidation of complexation, internalization, and delivery trends that could only be learned through evaluation of a large library. Using robotic automation, epoxide-functionalized block polymers were combinatorially cross-linked with a diverse library of amines, followed by measurement of molecular weight, diameter, RNA complexation, cellular internalization, and in vitro siRNA and pDNA delivery. Analysis revealed structure-function relationships and beneficial design guidelines, including a higher reactive block weight fraction, stoichiometric equivalence between epoxides and amines, and thin hydrophilic shells. Cross-linkers optimally possessed tertiary dimethylamine or piperazine groups and potential buffering capacity. Covalent cholesterol attachment allowed for transfection in vivo to liver hepatocytes in mice. The ability to tune the chemical nature of the core and shell may afford utility of these materials in additional applications.

摘要

类似于装配线,我们采用模块化设计,对具有阳离子核和可变壳的 1536 种结构独特的纳米颗粒进行高通量研究。这使得我们能够阐明通过评估大型文库才能获得的复杂、内化和递药趋势。通过使用机器人自动化技术,将环氧化物功能化的嵌段聚合物与胺的多样化文库进行组合交联,然后测量分子量、直径、RNA 复合物形成、细胞内化以及体外 siRNA 和 pDNA 递药。分析揭示了结构-功能关系和有益的设计准则,包括更高的反应性嵌段重量分数、环氧化物和胺之间的化学计量等效性以及薄的亲水性壳。交联剂最好具有叔二甲胺或哌嗪基团和潜在的缓冲能力。共价胆固醇附着允许在体内转染小鼠肝脏中的肝细胞。调节核和壳的化学性质的能力可能为这些材料在其他应用中提供了实用性。