通过与马来酰亚胺单体进行RAFT链增长反应制备的端基功能化聚合物和连接功能化二嵌段共聚物。
End-functionalized polymers and junction-functionalized diblock copolymers via RAFT chain extension with maleimido monomers.
作者信息
Henry Scott M, Convertine Anthony J, Benoit Danielle S W, Hoffman Allan S, Stayton Patrick S
机构信息
Department of Bioengineering, University of Washington, Seattle, Washington 98195, USA.
出版信息
Bioconjug Chem. 2009 Jun;20(6):1122-8. doi: 10.1021/bc800426d.
A new strategy is described for functionalizing the omega-terminal end of polymers synthesized by reversible addition-fragmentation chain transfer (RAFT) polymerization that provides spatially controlled bioconjugation sites. Traditional methods for preparing omega-functional polymers require the reduction of the RAFT chain-transfer agent to yield secondary or tertiary thiols of low reactivity or the synthesis of novel chain-transfer agents that contain reactive groups. As an additional strategy, N-substituted maleimido monomers have been used in a modified block polymerization to add a single maleimido unit onto the RAFT polymer with nearly quantitative efficiency. Unique reactive groups contained in the N-substituent are thereby added to the omega-terminal end of the polymer and are subsequently available for conjugation reactions. This technique has been demonstrated using N-(2-aminoethyl)maleimide trifluoroacetate to introduce a single primary amine to the omega-terminus of poly(dimethylaminoethyl methacrylate) and poly(N-isopropyl acrylamide) and to a specialized block copolymer for siRNA delivery. Evidence for retention of functional RAFT endgroups is provided by synthesis results where chain-extended polyDMAEMA (M(n) = 10 600 g/mol, M(w)/M(n) = 1.14) was used as a macro chain transfer agent for the polymerization of styrene, yielding a diblock polymer of low polydispersity (M(n) = 20 300 g/mol, M(w)/M(n) = 1.11). It is thus also possible to construct diblock copolymers with a bioconjugation site precisely located at the junction between the two blocks. The chain-extended polymers are functionalized with an amine-reactive fluorescent dye or folic acid at conjugation efficiencies of 86 and 94%, respectively. The versatile chain-extension technique described here offers unique opportunities for the synthesis of well-defined polymeric conjugates to molecules of biological and targeting interest.
本文描述了一种用于可逆加成-断裂链转移(RAFT)聚合合成聚合物的ω-末端官能化新策略,该策略可提供空间可控的生物共轭位点。制备ω-官能化聚合物的传统方法需要还原RAFT链转移剂以生成低反应活性的仲硫醇或叔硫醇,或者合成含反应性基团的新型链转移剂。作为一种额外的策略,N-取代马来酰亚胺单体已用于改性嵌段聚合,以几乎定量的效率在RAFT聚合物上添加单个马来酰亚胺单元。N-取代基中含有的独特反应性基团因此被添加到聚合物的ω-末端,随后可用于共轭反应。该技术已通过使用N-(2-氨基乙基)马来酰亚胺三氟乙酸酯进行了验证,该试剂可将单个伯胺引入聚(甲基丙烯酸二甲氨基乙酯)和聚(N-异丙基丙烯酰胺)的ω-末端,以及用于siRNA递送的特殊嵌段共聚物的ω-末端。链延伸的聚二甲基氨基乙基甲基丙烯酸酯(M(n)=10600 g/mol,M(w)/M(n)=1.14)用作苯乙烯聚合的大分子链转移剂,合成结果提供了功能性RAFT端基保留的证据,得到了低多分散性的二嵌段聚合物(M(n)=20300 g/mol,M(w)/M(n)=1.11)。因此,也有可能构建一种二嵌段共聚物,其生物共轭位点精确位于两个嵌段之间的连接处。链延伸聚合物分别用胺反应性荧光染料或叶酸进行官能化,共轭效率分别为86%和94%。本文所述的通用链延伸技术为合成具有明确结构的、与生物和靶向相关分子的聚合物共轭物提供了独特的机会。
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