Dipeptide ester, sweet taste

During work on a series of aspartyl dipeptides containing ACC 71 (vide supra, Eq. (28), Sect. 4) at the carboxyl terminus, it was reported that dispartame Asp-ACC-OMe had a distinct sweet taste [302] and that the corresponding n-propyl ester had 250-300 times the sweetness of sucrose [303]. However, replacement of phenylalanine by 2,3-methanophenylalanine gave tasteless analogues of aspartame [293, 304], and some dimethyl-ACC 214 (methanovaline) and tri-methyl-ACC 215 aspartame analogues [Asp-(Me)n-ACC-OMe] have a bitter taste. These taste properties, which depend on the number and position of the methyl substituents, have been explained on the basis of topochemical models thus, a L-shaped conformation of the dipeptide is necessary for sweet taste, Eq. (86) [3051. 

Aspartame. Aspartame [22839-47-0] [53906-69-1] (APM, L-aspartyl-L-phenylalanine methyl ester) (1), also known under the trade names of NutraSweet and EQUAL, is the most widely used nonnutritive sweetener worldwide. This dipeptide ester was synthesized as an intermediate for an antiulcer peptide at G. D. Searle in 1965. Although this compound was known in the literature, its sweet taste was serendipitously discovered when a chemist licked his finger which was contaminated with it. Many analogues, especially the more stable esters, were made (6) and their taste qualities and potencies determined. It was the first compound to be chosen for commercial development. Following the purchase of G. D. Searle by Monsanto, the aspartame business was split off to become a separate Monsanto subsidiary called the NutraSweet Company. 

Other peptides, such as L-aspartyl-L-phenylalanine methyl ester (aspartame), have a sweet taste. Several studies have been carried out to relate the structure and taste of analogs of this dipeptide (25). Tsang et al. (26) reported that the analogs at the lower end of the L-aspartyl-a-aminocycloalkanecarboxylic acid methyl ester series were sweet, the dipeptides containing a-... 

The sweet dipeptide esters of the L-aspartic acid and the L-amino malonic acid (15-21) are interesting exceptions to the bitter taste shared by all other members of the peptide series. Fig. 

After the finding of a sweet taste in L-Asp-L-Phe-OMe (aspartame) by Mazur et at. (6), a number of aspartyl dipeptide esters were synthesized by several groups in order to deduce structure-taste relationships, and to obtain potent sweet peptides. In the case of the peptides, the configuration and the conformation of the molecule are important in connection with the space-filling properties. The preferred conformations of amino acids can be shown by application of the extended Hiickel theory calculation. However, projection of reasonable conformations for di- and tripeptide molecules is not easily accomplished. 

In the course of investigations of aspartyl dipeptide esters, we had to draw their chemical structures in a unified formula. In an attempt to find a convenient method for predicting the sweettasting property of new peptides and, in particular, to elucidate more definite structure-taste relationships for aspartyl dipeptide esters, we previously applied the Fischer projection technique in drawing sweet molecules in a unified formula 04). 

The sweet-tasting property of aspartyl dipeptide esters has been successfully explained on the basis of the general structures shown in Figure 1 (4). A peptide will taste sweet when it takes... 

The structure-taste relationships will be discussed in detail. Dipeptide esters are closely related to amino acids in chemical structure and properties. Hence, we selected amino acids as the standard to which sweet peptides were related. The structural features of sweet-tasting amino acids have been best explained by Kaneko (12) as shown in Figure 2, in which an amino acid will taste sweet when R2 is H, CH3 or C2H5, whereas the size of Ri is not restricted if the amino acid is soluble in water. 

Therefore, we have concluded that sweet-tasting aspartyl dipeptide esters can be drawn as the unified formula (A), whereas nonsweet peptides as (B) as shown in Figure 1. 

In Ama-L-Phe-OMe (47) (14, 15), it is also not known whether the sweet-tasting isomer has the L-L(or S-S) or the D-L(or R-S) configuration. In the case of aspartyl dipeptide esters, the L-L isomer was sweet. By analogy, other researchers deduced that the L-L(or S-S) isomer ((47b) in Figure 4) would be sweet. However, it seemed to us that the D(or i )-configuration would be preferred for the aminomalonic acid because the D-L(or R-S) isomer ((47a) in Figure 4) was compatible with the sweet formula and could also fit the spatial barrier model (13), whereas the L-L(or S-S) isomer could neither fit the receptor model nor meet the sweet formula. 

Finally, L-Asp-D-Val-Gly-OMe (41) was synthesized in order to see whether it remained sweet. The peptide was devoid of sweetness and almost tasteless, though D-valine-containing aspartyl dipeptide esters such as L-Asp-D-Val-0Pr (17) and L-Asp-D-Val-OPrt (8, 17), which are similar to the tripeptide ester in size and shape and have potent sweet taste. 

Aspartame (Nutrasweet ) is a remarkably sweet-tasting dipeptide ester. Complete hydrolysis of aspartame gives phenyl alanine, aspartic acid, and methanol. Mild incubation with carboxypeptidase has no effect on aspartame. Treatment of aspartame with phenyl isothiocyanate, followed by mild hydrolysis, gives the phenylthiohydantoin of aspartic acid. 

In nature, the amino acids are combined to give proteins with hundreds or even thousands of amino acids in each one. Small assemblies of amino acids are known as peptides and die amide bond that links them is called a peptide bond. One important dipeptide is the sweetening agent aspartame, whose synthesis was discussed in Chapter 25. It is composed (and made) of the amino acid aspartic acid (Asp) and the methyl ester of phenylalanine. Only this enantiomer has a sweet taste and it is very sweet indeed—about 160 times as sweet as sucrose. 

The sweet taste of aspartic acid dipeptide esters (I) was discovered by chance in 1969 for a-L-aspartyl-L-phenylalanine methyl ester ( Aspartame , NutraSweet ). The corresponding peptide ester of L-aminomalonic acid (II) is also sweet. 

Peptides, Kke amino acids, can taste bitter, sweet, salty or indifferent. Most natural and synthetic oligopeptides have a bitter taste (see Section 2.3.3.2). A sweet taste indicates dipeptides derived from L-aspartic acid (2-91) and others derived from its lower homologue L-aminomalonic acid (2-92). is always a hydrogen atom or a methyl group, substituents are alkyls or aryls and substituents are esterified carboxyl groups (usually methyl esters, but some ethyl, propyl, isopropyl and other esters are also sweet). The best... 

Aspartame is a dipeptide with an immen.se sweet taste. The synthesis of this low-calorie sweetener is performed with the neutral protease (EC 3.4.24.27) from Bacillus thermopro-teolyticus also known as thermolysin. Applied as a reversal of the hydrolytic reaction, the enzyme shows a remarkable specificity in the coupling of N-protected-L-aspartic add and d/l phenylalanine methyl ester. Owing its extreme thermostability, the enzyme is very stable in the high solvent conditions used for... 

Aspartame was discovered by accident by Jim Schlatter, a chemist at G.D. Searle in 1965. Jim Schlatter was working on drugs for the treatment of gastric ulcers when he spilled some aspartyl-phenylalanine on his hand. He later licked his finger and noticed the sweet taste of the compound, which later became aspartame. Aspartame is the methyl ester of the dipeptide of the natural amino acids L-aspartic acid and L-phenylalanine. There are four possible diastereoiso-mers for aspartame but aspartame is the only one having sweetening properties. The taste of aspartame would not have been predictable based on its amino acid constituents. 

The studies on peptides began with a correlation between sweet amino acids and peptides. Since the projection formula of L-Asp-Gly-OMe (4) is similar in size and shape to that of e-Ac-D-Lys (3) which is sweet, we predicted that L-Asp-Gly-OMe would taste sweet in spite of the bitter taste in the literature. Therefore, we synthesized the peptide and tasted it. As expected, it was sweet and its sweetness potency was almost equal to that of e-Ac-D-Lys. Thus, the dipeptide could be correlated to the amino acid. Lengthening (5) or enlargement (6) of the alkyl group of the ester did not affect its sweetness potency (Table 1). 

Further examinations of the molecular features and of the model of receptor have suggested that several aspartyl tripeptide esters may also taste sweet. In confirmation of the idea, several tripeptide esters have been synthesized. In the first place, L-Asp-Gly-Gly-OMe (38) was synthesized as an arbitrarily-selected standard of tripeptides, because it was considered that this peptide ester had the simplest structure, and correlation of other peptides to (38) was easy. The tripeptide ester was predicted that it would be slightly sweet or tasteless because its projection formula was similar in size and shape to that of L-Asp-Gly-0Bum which is 13 times sweeter than sucrose (16) and because it is more hydrophilic than the dipeptide. The tripeptide (38) was devoid of sweetness and almost tasteless. 

The sweetener aspartame was discovered in 1965 and approved by the FDA in 1981. It is the methyl ester of a dipeptide formed from the amino acids aspartic acid and phenylalanine. Because both of these amino acids occur naturally and arc part of nearly every protein, there is much less reason to be concerned about the health effects of this compound. Nevertheless, it has been extensively tested. Aspartame is about 180 times sweeter than sucrose, so the amount that is needed to sweeten a can of a soft drink, for example, is so small that it contributes only negligible calories to the diet. In addition, the taste profile of aspartame is much closer to sugar than is that of saccharin. Aspartame, sold under the brand name NutraSweet, has been an enormous financial success. Sucralose (Splenda) is prepared from sucrose by replacing some of the hydroxy groups with chlorines. Its taste closely resembles sucrose, but it is about 600 times sweeter. Acesulfame K (Sunett, Sweet One) is about 200 times sweeter than sucrose. It is quite stable to heat, so it is potentially very useful in baked goods. 

Aspartame is a relatively new sweetener which is readily available and known commercially as Canderel. It is the methyl ester of the dipeptide L-aspartyl-L-phenylalanine and has a natural sugar-like taste. It is about 200 times as sweet as sucrose and, in addition, has flavour-enhancing... 

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