Synthesis of Aspartame by Thermolysin: An X-ray Structural Study

被引：19

作者：

Birrane, Gabriel ^{[1
]}

Bhyravbhatla, Balaji ^{[2
]}

Navia, Manuel A. ^{[3
]}

机构：

[1] Beth Israel Deaconess Med Ctr, Div Expt Med, Boston, MA 02215 USA

[2] Xtal BioStruct, Natick, MA 01760 USA

[3] Altus Pharmaceut, Waltham, MA 02451 USA

来源：

ACS MEDICINAL CHEMISTRY LETTERS | 2014年 / 5卷 / 06期

基金：

美国国家卫生研究院;

关键词：

Protease mediated peptide synthesis; aspartame; crystallography; thermolysin; N-(BENZYLOXYCARBONYL)-L-ASPARTYL-L-PHENYLALANINE METHYL-ESTER; TRANSITION-STATE ANALOGS; LINKED ENZYME CRYSTALS; CATALYZED SYNTHESIS; ORGANIC-SOLVENT; PEPTIDE-BONDS; SLOW-BINDING; ACTIVE-SITE; DIPEPTIDES; INHIBITORS;

D O I：

10.1021/ml500101z

中图分类号：

R914 [药物化学];

学科分类号：

100701 ;

摘要：

Protease mediated peptide synthesis (PMPS) was first described in the 1930s but remains underexploited today. In most PMPS, the reaction equilibrium is shifted toward synthesis by the aqueous insolubility of product generated. Substrates and proteases are selected by trial and error, yields are modest, and reaction times are slow. Once implemented, however, PMPS reactions can be simple, environmentally benign, and readily scalable to a commercial level. We examined the PMPS of a precursor of the artificial sweetener aspartame, a multiton peptide synthesis catalyzed by the enzyme thermolysin. X-ray structures of thermolysin in complex with aspartame substrates separately, and after PMPS in a crystal, rationalize the reaction's substrate preferences and reveal an unexpected form of substrate inhibition that explains its sluggishness. Structure guided optimization of this and other PMPS reactions could expand the economic viability of commercial peptides beyond current high-potency, low-volume therapeutics, with substantial green chemistry advantages.

引用

页码：706 / 710

页数：5

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