A-amino group, protection

Amino acid 1 with a-amino group protected by Fmoc group... 

The efficiency of this method was demonstrated by the elegant two-step synthesis of aspartame [87], Protection of the a-amino group and activation of the a-carboxylic group are accomplished in only one step Deprotection of the amino functionality occurs during aminolysis, such as with methyl phenylalaninate (H-Phe-OMe in equation 15)... 

Peptide synthesis was amenable to solid-phase techniques since the process was repetitive. The C-terminal amino acid is attached to polymeric surface and the peptide chain is assembled via a two-step process coupling of the incoming amino acid that has the alpha-amino group protected... 

The masking of the normal reaetions of simple ligands, such as the nitro, cyano, and ammonia groups, by coordination to a metal is a phenomenon encountered early by a chemist. One of the first examples of masking in a chelate complex was reported, signifieantly, in biological journals. It involves the protection by copper ion of the a-amino group in ornithine and lysine ... 

Many different approaches have been developed for peptide synthesis, and it is not the intention to cover more than the basic principles here, with a suitable example. The philosophy to convert two amino acids into a dipeptide is to transform each difunctional amino acid into a monofunctional compound, one of which has the amino group protected, whilst the other has the carboxyl group protected. This allows... 

Amino group protection may be achieved by converting the amine into its Al-tert-butyloxycarbonyl (tBOC or just BOC) derivative, by reaction with di-tert-butyl dicarbonate. This reagent should be considered as a variant of a carboxylic acid... 

It has also been suggested to reduce the nitro group to an amino group, protect it with an acetyl protection, oxidize the sulfur atom to a sulfone using potassium dichromate, and then remove the protective acetyl group by hydrolysis [48-50]. 

Piperazine-2,5-diones can be symmetric or asymmetric. Symmetric DKPs are readily obtained by heating amino acid esters,1179-181 whereas asymmetric DKPs are obtained directly from the related dipeptides under basic or, more properly, acid catalysis, or by cyclocondensation of dipeptide esters.1182-185 As an alternative procedure hexafluoroacetone can be used to protect/activate the amino acid for the synthesis of symmetric DKPs or of the second amino acid residue for synthesis of the dipeptide ester and subsequent direct cyclocondensation to DKPs.1186 The use of active esters for the cyclocondensation is less appropriate since it may lead to epimerization when a chiral amino acid is involved as the carboxy component in the cyclization reaction. Resin-bound DKPs as scaffolds for further on-resin transformations are readily prepared using the backbone amide linker (BAL) approach, where the amino acid ester is attached to the BAL resin by its a-amino group and then acylated with a Fmoc-protected amino acid by the HATU procedure, N -deprotection leads to on-resin DKP formation1172 (see Section 6.8.3.2.2.3). 

There are two principal modes for introducing the photophore into a peptide (1) Coupling a photoreactive N-protected amino acid during the stepwise assembly of the peptide e.g. in Scheme 3, the amino acid 4-benzoylphenylalanine (3) is incorporated into position 8 of substance P (9). (2) Post-synthetic modification of a fully assembled peptide, at either a free N-terminal a-amino group or a side-chain functionality, by the photophore in a site-specific or nonspecific manner e.g. in Scheme 3, treatment of cyclic R-G-D-containing peptide 10 with 4-benzoylbenzoic anhydride (11) gives the modified peptide 12. 

The synthesis uses Evans chemistry to introduce enantioselectively an azide group, which is then reduced to the a-amino group (Scheme 16). Note that in all cases, the phosphinyl group is protected as its sulfide during the synthesis to avoid complication (oxidation) observed with the phosphine. The phosphine sulfide is compatible with Fmoc- and Boc-peptide synthesis conditions. The free phosphine can later be regenerated by treating the sulfide with Raney nickel in MeOH (as shown in Scheme 15) or by methylation followed by treatment with HMPTJ50 This reduction was even applied successfully to sulfide-protected phosphine peptides still attached to the solid support.151 ... 

Houghten and co-workers[145] introduced a method for combinatorial synthesis of a per-alkylated peptide library using nonspecific N-alkylation. The peptides were synthesized by SMPS methodology 146 in combination with repetitive amide N-alkylation on the solid support after each coupling step. Peptides were synthesized on MBHA-PSty resin using Fmoc chemistry. After Fmoc deprotection the a-amino group was protected by Trt to prevent N -alkylation and to allow only amide alkylation. The on-resin amide alkylation was achieved by amide proton abstraction using LiOtBu in THF followed by nonfunctionalized alkyl and aryl halides in DMSO. 

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