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p-Nitrobenzyloxycarbonyl (pNZ) as Temporary Na-Protecting Group for Mild Solid-Phase Peptide Synthesis. Avoiding Diketopiperazine and Aspartimide Formation

机译：对硝基苄氧基羰基（pNZ）作为温和固相肽合成的临时Na保护基。避免形成二酮哌嗪和天冬酰胺

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摘要

p-Nitrobenzyloxycarbonyl was used as temporary protecting group for the -amino function in solid-phase peptide synthesis. The corresponding derivatives are solids, easy to be synthesized, and perform well in the solid-phase mode. pNZ is removed in practical neutral conditions in the presence of catalytic amounts of acid. They are orthogonal with the most common protecting groups used in peptide chemistry. They are specially useful in combination with Fmoc chemistry to overcome those side reactions associated with the used of the piperidine such DKP and aspartiimide formation. The flexibility of pNZ can be very useful for the preparation of libraries of small organic molecules.

机译：对硝基苄氧羰基用作固相肽合成中α-氨基官能团的临时保护基。相应的衍生物是固体，易于合成，并且在固相模式下表现良好。在实际中性条件下，在催化量的酸存在下，pNZ被去除。它们与肽化学中使用的最常见的保护基团正交。它们特别适合与Fmoc化学结合使用，以克服与哌啶的使用相关的那些副反应，例如DKP和天冬酰胺的形成。 pNZ的灵活性对于有机小分子文库的制备非常有用。

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Isidro Llobet Albert; Guasch Camell Judit; Álvarez Domingo Mercedes; Albericio Palomera Fernando;
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年度 2013
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1. p-Nitrobenzyloxycarbonyl(pNZ)as a Temporary N~alpha-Protecting Group in Orthogonal Solid-Phase Peptide Synthesis-Avoiding Diketopiperazine and Aspartimide Formation [J] . Albert Isidro-Llobet, Judit Guasch-Camell, Mercedes Alvarez, European journal of organic chemistry . 2005,第14期

机译：对硝基苄氧基羰基（pNZ）作为正交固相肽合成中的N-α保护临时基团，避免了二酮哌嗪和天冬酰胺的形成
2. Semipermanent p-nitrobenzyloxycarbonyl (pNZ) protection of Orn and Lys side chains:prevention of undesired alpha-Fmoc removal and application to the synthesis of cyclic peptides [J] . Albert Isidro-Llobet, Mercedes Alvarez, Fernando Albericio Tetrahedron letters: The International Journal for the Rapid Publication of Preliminary Communications in Organic Chemistry . 2005,第45期

机译：Orn和Lys侧链的半永久对硝基苄氧基羰基（pNZ）保护：防止不期望的α-Fmoc去除并应用于环肽的合成
3. Problem of aspartimide formation in Fmoc-based solid-phase peptide synthesis using Dmab group to protect side chain of aspartic acid [J] . Ruczynski J, Lewandowska B, Mucha P, Journal of peptide science: An official publication of the European Peptide Society . 2008,第3期

机译：使用Dmab基团保护天冬氨酸侧链的基于Fmoc的固相肽合成中天冬酰胺形成的问题
4. p-NitrobenzyIoxycarbonyl (pNZ) as an Alternative to Fmoc for the Protection of Amines in Solid-Phase Peptide Synthesis [C] . Albert Isidro-Llobet, Pilar E. Lopez, Judit Guasch-Camell American Peptide Symposium . 2006

机译：P-NITROBENZYIOXYCARONOLYL（PNZ）作为FMOC在固相肽合成中保护胺的替代方法
5. Peptide synthesis and characterization: Part 1. Synthesis and characterization of cyclic pseudopeptide analogs of endothelin antagonist BQ-123. Part 2. Comparative study of mild cleavage techniques for solid-phase synthesis of penta-, tetra-, and tri-peptides. [D] . Ingram, Darlene D. 2004

机译：肽的合成和表征：第1部分。内皮素拮抗剂BQ-123的环状假肽类似物的合成和表征。第2部分。五肽，四肽和三肽固相合成的轻度裂解技术的比较研究。
6. The aspartimide problem persists: Fluorenylmethyloxycarbonyl‐solid‐phase peptide synthesis (Fmoc‐SPPS) chain termination due to formation of N‐terminal piperazine‐25‐diones [O] . Daniel Samson, Daniel Rentsch, Marco Minuth, -1

机译：天冬酰胺的问题仍然存在：由于形成了N-末端哌嗪-25-二酮导致芴基甲氧基羰基固相肽合成（Fmoc-SPPS）链终止
7. "Difficult Sequences" and Solvation of Peptide Chains in Solid-Phase Peptide Synthesis. [O] . Mitsuaki NARITA, Shôkichi ÔUCHI 1994

机译：固相肽合成中的“难度序列”和肽链的溶剂化。

p-Nitrobenzyloxycarbonyl (pNZ) as Temporary Na-Protecting Group for Mild Solid-Phase Peptide Synthesis. Avoiding Diketopiperazine and Aspartimide Formation

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