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Solid Phase Synthesis of Novel Fullerene Nucleotides Conjugates

机译:新型富勒烯核苷酸缀合物的固相合成

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N-substituted 3, 4-fullero pyrrolidine was synthesized according to 1, 3-dipolar cycloaddition of the azomethine ylide. Aspartic acid with protected a-amino and α-carboxyl groups was reacted with the activated hydroxyl group of N-substituted 3,4-fullero pyrrolidine. The products were deprotected, affording the monofullerene aspartic acid (mFas). The conjugate FasT was synthesized by reaction of mFas containing protected amino group with the thymidylic acid derivatived controlled pore glass (CPG) using solid phase synthesis. All of the above fullerene derivatives were characterized by UV-vis, ~1H NMR, IR and MS spectrometric analysis, giving the correct spectra with regard to their chemical structure. The chemical structures of fullerene nucleotides conjugate FasT is different from previous reports and may have novel biological properties. Moreover, they are more suitable for applications in biomedical research due to their solubilization in THF and DMSO. They have a potential to be used as monomer for the automatic synthesis. It allows further conjugation with specific biomolecules including amino acids, peptides, nucleotides and nucleic acids. A novel method has been developed to synthesize fullerene nucleotides conjugate. Their unique chemical structures make them very interesting for their potential use in medicine and biology.
机译:根据氮杂甲酸甲吡啶的1,3-偶极环加成合成N-取代的3,4- Fulerors吡咯烷。具有保护A-氨基和α-羧基的天冬氨酸与N-取代的3,4- Fuleroro吡咯烷的活化羟基反应。将产品脱保护,得到Monofullerene天冬氨酸(MFA)。通过使用固相合成的含有保护氨基的MFA的MFA反应来合成缀合物,通过使用固相合成的胸苷酰基酸衍生的控制孔玻璃(CPG)来合成。所有上述富勒烯衍生物都是通过UV-Vis,〜1H NMR,IR和MS光谱分析的特征,给出了其化学结构的正确光谱。富勒烯核苷酸缀合物的化学结构与先前的报道不同,并且可以具有新的生物学性质。此外,由于它们在THF和DMSO中的溶解,它们更适合于生物医学研究的应用。它们有可能用作自动合成的单体。它允许与包括氨基酸,肽,核苷酸和核酸的特定生物分子进行进一步缀合。已经开发了一种新的方法来合成富勒烯核苷酸缀合物。它们独特的化学结构使它们非常有趣的是他们在医学和生物学中的潜在使用。

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