Solid-phase synthesis of neurokinin A antagonists. Comparison of the Boc and Fmoc methods.

P Rovero, L Quartara, G Fabbri
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Abstract

During the preparation of the NK-2 selective tachykinin antagonist MEN 10208 (Thr-Asp-Tyr-D-Trp-Val-D-Trp-D-Trp-Arg-NH2) and its analogs by the solid-phase method employing the Boc strategy routinely used in our laboratory, we encountered difficulties in the coupling of hydrophobic amino acids D-Trp and Val. To study the coupling problems several syntheses of MEN 10208 and analogs were carried out with different activation strategies. These syntheses yielded considerable amounts of deletion sequences even though a negative Kaiser test was obtained after each coupling. Inaccessibility of the free amino group of the growing peptide due to steric hindrance of the hydrophobic residues during coupling, and for the ninhydrin complex during the Kaiser test, may account, at least in part, for the unsatisfactory synthetics results and for the false-negative ninhydrin tests. Repetition of each synthesis with the Fmoc strategy on a newly developed DOD resin for peptide amides using the DCC/HOBt chemistry gave superior results in terms of the yield and purity of the crude peptides. Therefore, the Fmoc strategy appears to offer advantages over the Boc method for the preparation of these peptides containing hydrophobic amino acids.

神经激肽A拮抗剂的固相合成。Boc和Fmoc方法的比较。
在采用本实验室常用的Boc策略固相法制备NK-2选择性速激素拮抗剂MEN 10208 (Thr-Asp-Tyr-D-Trp-Val-D-Trp-D-Trp-Arg-NH2)及其类似物的过程中,我们遇到了疏水氨基酸D-Trp和Val的偶联困难。为了研究偶联问题,我们采用不同的活化策略合成了MEN 10208及其类似物。这些合成产生了相当数量的缺失序列,即使在每次耦合后获得阴性Kaiser试验。由于偶联过程中疏水残基的位阻以及Kaiser试验中茚三酮复合物的位阻,生长中的肽的自由氨基无法接近,这可能至少部分地解释了不令人满意的合成结果和茚三酮试验假阴性的原因。使用DCC/HOBt化学方法,在新开发的肽酰胺DOD树脂上重复Fmoc策略,在粗肽的收率和纯度方面取得了优异的结果。因此,Fmoc策略似乎比Boc方法在制备这些含有疏水氨基酸的肽方面具有优势。
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