Conformational comparison of µ‐selective endomorphin‐2 with its C‐terminal free acid in DMSO solution, by ¹H NMR spectroscopy and molecular modeling calculation

Abstract: In order to make clear the structural role of the C-terminal amide group of endomorphin-2 (EM2, H-Tyr-Pro-Phe-Phe-NH2), an endogenous mu-receptor ligand, in the biological function, the solution conformations of endomorphin-2 and its C-terminal free acid (EM2OH, H-Tyr-Pro-Phe-Phe-OH), studied using two-dimensional 1H NMR measurements and molecular modeling calculations, were compared. Both peptides were in equilibrium between the cis and trans isomers around the Tyr-Pro omega bond in a population ratio of appr… Show more

“…In contrast, this conformational feature of cis-EM1 was not observed during the MD calculation performed in H 2 O and in vacuo [25]. Similarly as for the cis-isomer of EM1, based on the NMR data, a compact sandwich structure with stacking of the Tyr 1 , Pro 2 , and Phe 3 rings was also detected for cis-EM2 in DMSO and in TFE [27] [29]. Moreover, the results of the RS calculations indicated the presence of compact conformations created by the packing of the side chains of aromatic amino acids around the Pro 2 residue in the case of the cis-isomers of EMs (Fig.…”

“…These results indicated that the replacement of the C-terminal amide group by a carboxy group resulted in a higher flexibility for EM2OH. The subsequent structural examination of EM2 and its C-terminal free-acid analog carried out in different media (i.e., H 2 O, DMSO, TFE, and DPC micelles) by In et al [27] led to the similar observations regarding the backbone structure of the cisand trans-isomers of both tetrapeptides, as described in [29]. In this latter study, four different types of backbone conformation were distinguished, namely the rS-and n7-type open conformers, as well as the F1-and F2-type folded conformers, whose population ratios depended on the solvent type and pH.…”

“…For EM2 and EM2OH, In et al [29] performed NMR measurements, followed by SA and MD simulations. On the basis of their results, it was concluded that all conformers of the cis-and trans-isomers of EM2 assumed a similar extended conformation with a twisted backbone at the Pro 2 -Phe 3 region (Fig.…”

“…Nevertheless, almost exclusively the trans-isomer of EM2 was observed in DPC micelles (pH 3.5 and 5.2) [27]. In the case of C-terminal free-acid analog (EM2OH), the NMR studies led to population ratios of cis-and trans-isomers which proved to be equivalent to those of EM2 in H 2 O (pH 2.7), DMSO, and DPC micelles (pH 3.5) [27] [29], but different proportions of the two isomers were detected in H 2 O (pH 5.2), TFE, and DPC micelles (pH 5.2) compared to those found for the parent peptide [27].…”

Structural Investigation of Endomorphins by Experimental and Theoretical Methods: Hunting for the Bioactive Conformation

“…In contrast, this conformational feature of cis-EM1 was not observed during the MD calculation performed in H 2 O and in vacuo [25]. Similarly as for the cis-isomer of EM1, based on the NMR data, a compact sandwich structure with stacking of the Tyr 1 , Pro 2 , and Phe 3 rings was also detected for cis-EM2 in DMSO and in TFE [27] [29]. Moreover, the results of the RS calculations indicated the presence of compact conformations created by the packing of the side chains of aromatic amino acids around the Pro 2 residue in the case of the cis-isomers of EMs (Fig.…”

“…These results indicated that the replacement of the C-terminal amide group by a carboxy group resulted in a higher flexibility for EM2OH. The subsequent structural examination of EM2 and its C-terminal free-acid analog carried out in different media (i.e., H 2 O, DMSO, TFE, and DPC micelles) by In et al [27] led to the similar observations regarding the backbone structure of the cisand trans-isomers of both tetrapeptides, as described in [29]. In this latter study, four different types of backbone conformation were distinguished, namely the rS-and n7-type open conformers, as well as the F1-and F2-type folded conformers, whose population ratios depended on the solvent type and pH.…”

“…For EM2 and EM2OH, In et al [29] performed NMR measurements, followed by SA and MD simulations. On the basis of their results, it was concluded that all conformers of the cis-and trans-isomers of EM2 assumed a similar extended conformation with a twisted backbone at the Pro 2 -Phe 3 region (Fig.…”

“…Nevertheless, almost exclusively the trans-isomer of EM2 was observed in DPC micelles (pH 3.5 and 5.2) [27]. In the case of C-terminal free-acid analog (EM2OH), the NMR studies led to population ratios of cis-and trans-isomers which proved to be equivalent to those of EM2 in H 2 O (pH 2.7), DMSO, and DPC micelles (pH 3.5) [27] [29], but different proportions of the two isomers were detected in H 2 O (pH 5.2), TFE, and DPC micelles (pH 5.2) compared to those found for the parent peptide [27].…”

Structural Investigation of Endomorphins by Experimental and Theoretical Methods: Hunting for the Bioactive Conformation

“…This may be related to the fact that amidation brings the C-terminal group to a neutral state, which in turn decreases the repulsion of carboxyl groups in the aspartic acid. This is known to play a key role in preventing the formation of a folded conformation for the C-terminal amidated peptide (46). An open conformation for OSN would allow more side chain interaction with calcium and phosphate ions (35).…”

C-terminal Amidation of an Osteocalcin-derived Peptide Promotes Hydroxyapatite Crystallization

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