Topographically designed analogs of [cyclic] [D-Pen2,D-Pen5]enkephalin

Hruby, Victor J.; Tóth, Géza; Gehrig, Catherine A.; Kao, Lung Fa; Knapp, Richard J.; Lui, George K.; Yamamura, Henry I.; Kramer, Thomas H.; Davis, Peg; Burks, Thomas F.

doi:10.1021/jm00110a010

Cited by 109 publications

(80 citation statements)

References 8 publications

(17 reference statements)

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“…The up to 5-fold difference in the gauche (+) population is unexpected since DPDPE and compound 1 have similar structures; both are 14-membered cyclic disulfides with aromatic residues at positions 1 and 4. Furthermore, a comparison against the potent (2S,3S)-isomer of [β-Me-p-NO 2 Phe 4 ]DPDPE with 10% gauche (+) population for Tyr, also can be made [22,45]. In this case, the increase in the gauche (+) may be a result of a substitution of a constrained aromatic residue at position 4.…”

Section: Compound 1 Has Unique Conformational Features As An Opioid Lmentioning

confidence: 99%

Structure–activity relationships of bifunctional cyclic disulfide peptides based on overlapping pharmacophores at opioid and cholecystokinin receptors

et al. 2008

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Prolonged opioid exposure increases the expression of cholecystokinin (CCK) and its receptors in the central nervous system, where CCK may attenuate the antinociceptive effects of opioids. The complex interactions between opioid and CCK may play a role in the development of opioid tolerance. We designed and synthesized cyclic disulfide peptides and determined their agonist properties at opioid receptors and antagonist properties at CCK receptors. Compound 1 (Tyr-c[DCys-Gly-Trp-Cys]-Asp-Phe-NH 2 ) showed potent binding and agonist activities at δ and µ opioid receptors while displaying some binding to CCK receptors. The NMR structure of the lead compound displayed similar conformational features of opioid and CCK ligands.

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Section: Compound 1 Has Unique Conformational Features As An Opioid Lmentioning

confidence: 99%

Structure–activity relationships of bifunctional cyclic disulfide peptides based on overlapping pharmacophores at opioid and cholecystokinin receptors

et al. 2008

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“…First, the receptorligand interactions (structure-activity relationships) for these compounds have been well studied (1,2,(24)(25)(26)(27)30 f3-D-glucoside moiety, were chosen for further study to see whether analgesia (peptide transport) could be demonstrated in live mice.…”

mentioning

confidence: 99%

Glycopeptide enkephalin analogues produce analgesia in mice: evidence for penetration of the blood-brain barrier.

Polt

Porreca²,

Szabó

et al. 1994

Proc. Natl. Acad. Sci. U.S.A.

222

154

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Most peptides have not proved useful as neuroactive drugs because they are blocked by the blood-brain barrier and do not reach their receptors within the brain.Intraperitoneally administered L-serinyl JD-glucosde aalgues of [Metslenkephaln (glycopeptides) have been shown to be transported across the blood-brain barrier to bind with targeted p and &oplod receptors in the mouse brain. The opioid nature of the bing has been demonstrated with intracerebroventricularly a ered naloxone. Paradoxically, glucosylation decreases the ipophlt of the peptides while promoting transport across the phc endothe layer. It is suggested that glucose transporter GLUT-1 is responsible for the transport of the peptide message. Profound and long-lasting anesla has been observed in mice (tail-ck and hot-plate assays) with two of the glycopeptide a ues when administered intraperitoneally.

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“…The free amino groups on the side chains of 5-aminovaleric acid, b-alanine, 4-aminobutyric acid, 6-aminohexanoic acid and p-aminobenzoic acid were protected before peptide synthesis with a Boc (N-tert-butoxycarbonyl) group as previously reported (11).…”

Section: Amine Protectionmentioning

confidence: 99%

Structure‐Based Design of Residue 1 Analogs of the Direct Thrombin Inhibitor Pentapeptide FM 19

Girnys

Sobczyk-Kojiro

Mosberg³

2009

Chem Biol Drug Des

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Myocardial ischemia and other acute coronary syndromes are leading causes of death worldwide, and often result from a thrombus that blocks an atherosclerotic coronary artery. A key enzyme in thrombus formation is the serine protease thrombin, which is responsible for both the conversion of soluble fibrinogen into insoluble fibrin, as well as the activation of the GPCRs, PAR1 and PAR4, which stimulate platelet aggregation. Thus, thrombin is an attractive target for anticoagulant and antithrombotic therapy. Previous studies in our laboratory led to the development of lead compound FM 19 (D-Arg-Oic-Pro-D-Ala-Phe(p-Me)-NH 2 ), which shows modest potency as a thrombin inhibitor. The recently determined X-ray structure of FM 19 in the active site of thrombin has revealed potential sites for modification to improve potency. This study reports replacements to the first residue (D-Arg 1 ) of FM 19, which seek to improve potency by removing the N-terminal amine to eliminate an adverse electrostatic interaction, and alterations to the length of the side chain to eliminate an unfavorable eclipsed conformation observed in the X-ray structure. This study produced two compounds, 1 and 9, with improved a-thrombin inhibition (IC 50 values of 0.66 ± 0.20 lM and 0.57 ± 0.12 lM, respectively).

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Topographically designed analogs of [cyclic] [D-Pen2,D-Pen5]enkephalin

Cited by 109 publications

References 8 publications

Structure–activity relationships of bifunctional cyclic disulfide peptides based on overlapping pharmacophores at opioid and cholecystokinin receptors

Structure–activity relationships of bifunctional cyclic disulfide peptides based on overlapping pharmacophores at opioid and cholecystokinin receptors

Glycopeptide enkephalin analogues produce analgesia in mice: evidence for penetration of the blood-brain barrier.

Structure‐Based Design of Residue 1 Analogs of the Direct Thrombin Inhibitor Pentapeptide FM 19

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