Zohreh Sajjadi scite author profile

Zohreh Sajjadi

3Publications

65Citation Statements Received

104Citation Statements Given

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103

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Université de Montréal

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Selective tert-Butyl Ester Deprotection in the Presence of Acid Labile Protecting Groups with Use of ZnBr₂

et al. 2004

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Chemoselective hydrolysis of tert-butyl esters in the presence of other acid-labile groups has been explored by employing alpha-amino esters and ZnBr(2) in DCM. Although N-Boc and N-trityl groups were found to be labile, PhF protected amines were compatible with these Lewis acid deprotection conditions such that a variety of N-(PhF)amino acids were prepared in good yields from their corresponding tert-butyl esters.

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Amino acid–azetidine chimeras: synthesis of enantiopure 3‐substituted azetidine‐2‐carboxylic acids

Sajjadi

Lubell

2005

The Journal of Peptide Research

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Azetidine-2-carboxylic acid (Aze) analogs possessing various heteroatomic side chains at the 3-position have been synthesized by modification of 1-9-(9-phenylfluorenyl) (PhF)-3-allyl-Aze tert-butyl ester (2S,3S)-1. 3-Allyl-Aze 1 was synthesized by regioselective allylation of alpha-tert-butyl beta-methyl N-(PhF)aspartate 13, followed by selective omega-carboxylate reduction, tosylation, and intramolecular N-alkylation. Removal of the PhF group and olefin reduction by hydrogenation followed by Fmoc protection produced nor-leucine-Aze chimera 2. Regioselective olefin hydroboration of (2S,3S)-1 produced primary alcohol 23, which was protected as a silyl ether, hydrogenated and N-protected to give 1-Fmoc-3-hydroxypropyl-Aze 26. Enantiopure (2S,3S)-3-(3-azidopropyl)-1-Fmoc-azetidine-2-carboxylic acid tert-butyl ester 3 was prepared as a Lys-Aze chimera by activation of 3-hydroxypropyl-Aze 26 as a methanesulfonate and displacement with sodium azide. Moreover, orthogonally protected azetidine dicarboxylic acid 4 was synthesized as an alpha-aminoadipate-Aze chimera by oxidation of alcohol 26. These orthogonally protected amino acid-Aze chimeras are designed to serve as tools for studying the influence of conformation on peptide activity.

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Selective tert‐Butyl Ester Deprotection in the Presence of Acid Labile Protecting Groups with Use of ZnBr₂.

et al. 2004

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Selective tert-Butyl Ester Deprotection in the Presence of Acid Labile Protecting Groups with Use of ZnBr2. -In the presence of ZnBr2, tert-butyl esters containing N-Fmoc or N-Flu protected amino groups can undergo selective deprotection. Methyl esters and allyl esters as well as some other functional groups are not affected under these conditions, but N-Boc and N-trityl groups are cleaved. Interestingly, starting from the diester (Id) selective hydrolysis of the α-tert-butyl ester is possible. -(KAUL, R.; BROUILLETTE, Y.; SAJJADI, Z.; HANSFORD, K. A.; LUBELL*, W. D.; J.

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Zohreh Sajjadi

Selective tert-Butyl Ester Deprotection in the Presence of Acid Labile Protecting Groups with Use of ZnBr₂

Amino acid–azetidine chimeras: synthesis of enantiopure 3‐substituted azetidine‐2‐carboxylic acids

Selective tert‐Butyl Ester Deprotection in the Presence of Acid Labile Protecting Groups with Use of ZnBr₂.

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Zohreh Sajjadi

Selective tert-Butyl Ester Deprotection in the Presence of Acid Labile Protecting Groups with Use of ZnBr2

Amino acid–azetidine chimeras: synthesis of enantiopure 3‐substituted azetidine‐2‐carboxylic acids

Selective tert‐Butyl Ester Deprotection in the Presence of Acid Labile Protecting Groups with Use of ZnBr2.

Contact Info

Product

Resources

About

Selective tert-Butyl Ester Deprotection in the Presence of Acid Labile Protecting Groups with Use of ZnBr₂

Selective tert‐Butyl Ester Deprotection in the Presence of Acid Labile Protecting Groups with Use of ZnBr₂.