Your search keyword '"Peptide YY chemistry"' showing total 84 results

1. Binding of Natural Peptide Ligands to the Neuropeptide Y 5 Receptor.

Author

Rudolf S, Kaempf K, Vu O, Meiler J, Beck-Sickinger AG, and Coin I

Subjects

Ligands, Humans, Peptides chemistry, Peptides metabolism, Protein Binding, Peptide YY metabolism, Peptide YY chemistry, Binding Sites, Pancreatic Polypeptide metabolism, Pancreatic Polypeptide chemistry, Models, Molecular, Receptors, Neuropeptide Y metabolism, Receptors, Neuropeptide Y chemistry

Abstract

The binding mode of natural peptide ligands to the Y 5 G protein-coupled receptor (Y 5 R), an attractive therapeutic target for the treatment of obesity, is largely unknown. Here, we apply complementary biochemical and computational approaches, including scanning of the receptor surface with a genetically encoded crosslinker, Ala-scanning of the ligand and double-cycle mutagenesis, to map interactions in the ligand-receptor interface and build a structural model of the NPY-Y 5 R complex guided by the experimental data. In the model, the carboxyl (C)-terminus of bound NPY is placed close to the extracellular loop (ECL) 3, whereas the characteristic α-helical segment of the ligand drapes over ECL1 and is tethered towards ECL2 by a hydrophobic cluster. We further show that the other two natural ligands of Y 5 R, peptide YY (PYY) and pancreatic polypeptide (PP) dock to the receptor in a similar pose., (© 2021 The Authors. Angewandte Chemie International Edition published by Wiley-VCH GmbH.)

Published

2022

2. The effect of fatty diacid acylation of human PYY 3-36 on Y 2 receptor potency and half-life in minipigs.

Author

Østergaard S, Paulsson JF, Kofoed J, Zosel F, Olsen J, Jeppesen CB, Spetzler J, Ynddal L, Schleiss LG, Christoffersen BØ, Raun K, Sensfuss U, Nielsen FS, Jørgensen R, and Wulff BS

Subjects

Acetylation, Animals, Anti-Obesity Agents administration & dosage, Anti-Obesity Agents therapeutic use, CHO Cells, Cricetinae, Cricetulus, Drug Combinations, Fatty Acids chemistry, Female, HEK293 Cells, Half-Life, Humans, Liraglutide administration & dosage, Liraglutide therapeutic use, Obesity drug therapy, Oligopeptides administration & dosage, Oligopeptides chemistry, Oligopeptides therapeutic use, Protein Binding, Swine, Swine, Miniature, Oligopeptides pharmacokinetics, Peptide YY chemistry, Receptors, Neuropeptide Y metabolism

Abstract

Peptides are notoriously known to display very short in vivo half-lives often measured in minutes which in many cases greatly reduces or eliminates sufficient in vivo efficacy. To obtain long half-lives allowing for up to once-weekly dosing regimen, fatty acid acylation (lipidation) have been used to non-covalently associate the peptide to serum albumin thus serving as a circulating depot. This approach is generally considered in the scientific and patent community as a standard approach to protract almost any given peptide. However, it is not trivial to prolong the half-life of peptides by lipidation and still maintain high potency and good formulation properties. Here we show that attaching a fatty acid to the obesity-drug relevant peptide PYY 3-36 is not sufficient for long pharmacokinetics (PK), since the position in the backbone, but also type of fatty acid and linker strongly influences PK and potency. Furthermore, understanding the proteolytic stability of the backbone is key to obtain long half-lives by lipidation, since backbone cleavage still occurs while associated to albumin. Having identified a PYY analogue with a sufficient half-life, we show that in combination with a GLP-1 analogue, liraglutide, additional weight loss can be achieved in the obese minipig model., (© 2021. The Author(s).)

Published

2021

3. Rational Development of Stable PYY 3-36 Peptide Y 2 Receptor Agonists.

Author

Poulsen C, Pedersen MØ, Wahlund PO, Sjölander A, Thomsen JK, Conde-Frieboes KW, Paulsson JF, Wulff BS, and Østergaard S

Subjects

Asparagine chemistry, Drug Development, HEK293 Cells, Humans, Peptide Fragments pharmacology, Peptide YY pharmacology, Peptide Fragments chemistry, Peptide YY chemistry, Receptors, Neuropeptide Y agonists

Abstract

Purpose: The anorectic effect of PYY 3-36 makes it a potential pharmacological weight loss treatment. Modifications of the endogenous peptide to obtain commercially attractive pharmacological and biophysical stability properties are examined., Methods: Half-life extended PYY 3-36 analogues were prepared and examined regarding Y 2 -receptor potency as well as biophysical and stability properties., Results: Deamidation of asparagine in position 18 and 29 was observed upon incubation at 37°C. Asparagine in position 18 - but not position 29 - could be substituted to glutamine without detrimental effects on Y 2 -receptor potency. Covalent dimers were formed via the phenol impurity benzoquinone reacting with two N-terminal residues (Isoleucine-Lysine). Both residues had to be modified to suppress dimerization, which could be done without negatively affecting Y 2 -receptor potency or other stability/biophysical properties. Introduction of half-life extending modifications in position 30 and 35 eliminated aggregation at 37°C without negatively affecting other stability properties. Placement of a protracting moiety (fatty acid) in the receptor-binding C-terminal region reduced Y 2 -receptor potency substantially, whereas only minor effects of protractor position were observed on structural, biophysical or stability properties. Lipidated PYY 3-36 analogues formed oligomers of various sizes depending on primary structure and solution conditions., Conclusions: By rational design, a chemically and physically stable Y 2 -receptor selective, half-life extended PYY 3-36 peptide has been developed., (© 2021. The Author(s), under exclusive licence to Springer Science+Business Media, LLC, part of Springer Nature.)

Published

2021

4. The Design of a GLP-1/PYY Dual Acting Agonist.

Author

Østergaard S, Paulsson JF, Kjaergaard Gerstenberg M, and Wulff BS

Subjects

Crystallography, X-Ray, Glucagon-Like Peptide 1 chemical synthesis, Glucagon-Like Peptide 1 chemistry, Humans, Models, Molecular, Peptide Fragments chemical synthesis, Peptide Fragments chemistry, Peptide YY chemical synthesis, Peptide YY chemistry, Drug Design, Glucagon-Like Peptide 1 pharmacology, Glucagon-Like Peptide-1 Receptor agonists, Peptide Fragments pharmacology, Peptide YY pharmacology, Receptors, Gastrointestinal Hormone agonists

Abstract

The two gut hormones GLP-1 and PYY 3-36 , which are both secreted from the L-cells upon food stimuli, have a stronger inhibitory effect on food intake when they are combined, compared to their individual effects as single agonists. Although they are not homologous and share no sequence similarity, we show that a GLP-1 analogue can be designed to exhibit potent activity on both the Y 2 and GLP-1 receptors. Dual acting hybrid analogues were realized by designing truncated and potent Y 2 receptor PYY analogues, followed by integrating the critical residues into GLP-1. In this study, we show that one of these dual acting agonists acutely reduces food intake significantly more than the respective mono-agonist counterparts., (© 2021 Wiley-VCH GmbH.)

Published

2021

5. Design and Evaluation of Peptide Dual-Agonists of GLP-1 and NPY2 Receptors for Glucoregulation and Weight Loss with Mitigated Nausea and Emesis.

Author

Milliken BT, Elfers C, Chepurny OG, Chichura KS, Sweet IR, Borner T, Hayes MR, De Jonghe BC, Holz GG, Roth CL, and Doyle RP

Subjects

Animals, Binding, Competitive, Blood Glucose metabolism, Exenatide chemistry, Humans, Insulin Secretion drug effects, Islets of Langerhans drug effects, Islets of Langerhans metabolism, Male, Microsomes, Liver metabolism, Models, Molecular, Molecular Docking Simulation, Peptide YY chemistry, Rats, Rats, Sprague-Dawley, Shrews, Structure-Activity Relationship, Glucagon-Like Peptide-1 Receptor agonists, Glucose metabolism, Nausea drug therapy, Receptors, Neuropeptide Y agonists, Vomiting drug therapy, Weight Loss drug effects

Abstract

There is a critical unmet need for therapeutics to treat the epidemic of comorbidities associated with obesity and type 2 diabetes, ideally devoid of nausea/emesis. This study developed monomeric peptide agonists of glucagon-like peptide 1 receptor (GLP-1R) and neuropeptide Y2 receptor (Y2-R) based on exendin-4 (Ex-4) and PYY 3-36 . A novel peptide, GEP44, was obtained via in vitro receptor screens, insulin secretion in islets, stability assays, and in vivo rat and shrew studies of glucoregulation, weight loss, nausea, and emesis. GEP44 in lean and diet-induced obese rats produced greater reduction in body weight compared to Ex-4 without triggering nausea associated behavior. Studies in the shrew demonstrated a near absence of emesis for GEP44 in contrast to Ex-4. Collectively, these data demonstrate that targeting GLP-1R and Y2-R with chimeric single peptides offers a route to new glucoregulatory treatments that are well-tolerated and have improved weight loss when compared directly to Ex-4.

Published

2021

6. Bioimaging and Biodistribution of the Metal-Ion-Controlled Self-Assembly of PYY 3-36 Studied by SPECT/CT.

Author

Kalomoiri P, Rodríguez-Rodríguez C, Sørensen KK, Bergamo M, Saatchi K, Häfeli UO, and Jensen KJ

Subjects

2,2'-Dipyridyl chemistry, 2,2'-Dipyridyl pharmacokinetics, Animals, Coordination Complexes chemical synthesis, Coordination Complexes chemistry, Coordination Complexes pharmacokinetics, Copper chemistry, Female, Kidney Cortex chemistry, Kidney Cortex metabolism, Ligands, Mice, Mice, Inbred C57BL, Peptide YY chemical synthesis, Peptide YY chemistry, Renal Elimination, Tissue Distribution, Copper pharmacokinetics, Peptide YY pharmacokinetics, Tomography, Emission-Computed, Single-Photon, Tomography, X-Ray Computed

Abstract

The controlled self-assembly of peptide- and protein-based pharmaceuticals is of central importance for their mode of action and tuning of their properties. Peptide YY 3-36 (PYY 3-36 ) is a 36-residue peptide hormone that reduces food intake when peripherally administered. Herein, we describe the synthesis of a PYY 3-36 analogue functionalized with a metal-ion-binding 2,2'-bipyridine ligand that enables self-assembly through metal complexation. Upon addition of Cu II , the bipyridine-modified PYY 3-36 peptide binds stoichiometric quantities of metal ions in solution and contributes to the organization of higher-order assemblies. In this study, we aimed to explore the size effect of the self-assembly in vivo by using non-invasive quantitative single-photon emission computed tomography/computed tomography (SPECT/CT) imaging. For this purpose, bipyridine-modified PYY 3-36 was radiolabeled with a chelator holding 111 In III , followed by the addition of Cu II to the bipyridine ligand. SPECT/CT imaging and biodistribution studies showed fast renal clearance and accumulation in the kidney cortex. The radiolabeled bipyridyl-PYY 3-36 conjugates with and without Cu II presented a slightly slower excretion 1 h post injection compared to the unmodified-PYY 3-36 , thus demonstrating that higher self-assemblies of the peptide might have an effect on the pharmacokinetics., (© 2020 Wiley-VCH GmbH.)

Published

2020

7. Engineering of a Potent, Long-Acting NPY2R Agonist for Combination with a GLP-1R Agonist as a Multi-Hormonal Treatment for Obesity.

Author

Lear S, Pflimlin E, Zhou Z, Huang D, Weng S, Nguyen-Tran V, Joseph SB, Roller S, Peterson S, Li J, Tremblay M, Schultz PG, and Shen W

Subjects

Amino Acid Sequence, Animals, Body Weight drug effects, Drug Interactions, Eating drug effects, Half-Life, Models, Molecular, Peptide YY pharmacokinetics, Polyethylene Glycols chemistry, Protein Conformation, Rats, Engineering, Glucagon-Like Peptide-1 Receptor agonists, Obesity drug therapy, Peptide YY chemistry, Peptide YY pharmacology, Receptors, Neuropeptide Y agonists

Abstract

Bariatric surgery results in increased intestinal secretion of hormones GLP-1 and anorexigenic PYY, which is believed to contribute to the clinical efficacy associated with the procedure. This observation raises the question whether combination treatment with gut hormone analogs might recapitulate the efficacy and mitigate the significant risks associated with surgery. Despite PYY demonstrating excellent efficacy and safety profiles with regard to food intake reduction, weight loss, and glucose control in preclinical animal models, PYY-based therapeutic development remains challenging given a low serum stability and half-life for the native peptide. Here, combined peptide stapling and PEG-fatty acid conjugation affords potent PYY analogs with >14 h rat half-lives, which are expected to translate into a human half-life suitable for once-weekly dosing. Excellent efficacy in glucose control, food intake reduction, and weight loss for lead candidate 22 in combination with our previously reported long-acting GLP-1 analog is demonstrated in a diet-induced obesity mouse model.

Published

2020

8. Modified Peptide YY Molecule Attenuates the Activity of NPY/AgRP Neurons and Reduces Food Intake in Male Mice.

Author

Jones ES, Nunn N, Chambers AP, Østergaard S, Wulff BS, and Luckman SM

Subjects

Animals, Arcuate Nucleus of Hypothalamus cytology, Ghrelin, Male, Mice, Neurons drug effects, Peptide Fragments pharmacology, Peptide YY pharmacology, Arcuate Nucleus of Hypothalamus drug effects, Eating drug effects, Peptide Fragments chemistry, Peptide YY chemistry, Receptors, Neuropeptide Y agonists, Satiety Response drug effects

Abstract

To study the effects of an analog of the gut-produced hormone peptide YY (PYY3-36), which has increased selectivity for the Y2 receptor; specifically, to record its effects on food intake and on hypothalamic neuropeptide Y/agouti-related peptide (NPY/AgRP) neuron activity. NNC0165-1273, a modified form of the peptide hormone PYY3-36 with potent selectivity at Y2 receptor (>5000-fold over Y1, 1250-fold over Y4, and 650-fold over Y5 receptor), was tested in vivo and in vitro in mouse models. NNC0165-1273 has fivefold lower relative affinity for Y2 compared with PYY3-36, but >250-, 192-, and 400-fold higher selectivity, respectively, for the Y1, Y4, and Y5 receptors. NNC0165-1273 produced a reduction in nighttime feeding at a dose at which PYY3-36 loses efficacy. The normal behavioral satiety sequence observed suggests that NNC0165-1273 is not nauseating and, instead, reduces food intake by producing early satiety. Additionally, NNC0165-1273 blocked ghrelin-induced cFos expression in NPY/AgRP neurons. In vitro electrophysiological recordings showed that, opposite to ghrelin, NNC0165-1273 hyperpolarized NPY/AgRP neurons and reduced action potential frequency. Administration of NNC0165-1273 via subcutaneous osmotic minipump caused a dose-dependent decrease in body weight and fat mass in an obese mouse model. Finally, NNC0165-1273 attenuated the feeding response when NPY/AgRP neurons were activated using ghrelin or more selectively with designer receptors. NNC0165-1273 is nonnauseating and stimulates a satiety response through, at least in part, a direct action on hypothalamic NPY/AgRP neurons. Modification of PYY3-36 to produce compounds with increased affinity to Y2 receptors may be useful as antiobesity therapies in humans., (Copyright © 2019 Endocrine Society.)

Published

2019

9. Half-Life Extending Modifications of Peptide YY 3-36 Direct Receptor-Mediated Internalization.

Author

Bech EM, Kaiser A, Bellmann-Sickert K, Nielsen SS, Sørensen KK, Elster L, Hatzakis N, Pedersen SL, Beck-Sickinger AG, and Jensen KJ

Subjects

Anti-Obesity Agents chemistry, Anti-Obesity Agents therapeutic use, Arrestins metabolism, HEK293 Cells, Half-Life, Humans, Intravital Microscopy, Lipids chemistry, Liposomes, Models, Biological, Models, Chemical, Molecular Structure, Obesity drug therapy, Obesity metabolism, Peptide Fragments chemistry, Peptide Fragments therapeutic use, Peptide YY chemistry, Peptide YY therapeutic use, Polyethylene Glycols chemistry, Structure-Activity Relationship, Anti-Obesity Agents pharmacology, Drug Design, Peptide Fragments pharmacology, Peptide YY pharmacology, Receptors, Neuropeptide Y metabolism

Abstract

Peptide YY 3-36 (PYY 3-36 ) is an endogenous ligand of the neuropeptide Y 2 receptor (Y 2 R), on which it acts to reduce food intake. Chemically modified PYY 3-36 analogues with extended half-lives are potential therapeutics for the treatment of obesity. Here we show that the common half-life extending strategies PEGylation and lipidation not only control PYY 3-36 's pharmacokinetics but also affect central aspects of its pharmacodynamics. PEGylation of PYY 3-36 inhibited endocytosis by increasing receptor dissociation rates ( k off ), which reduced arrestin-3 (Arr3) activity. This is the first link between Arr3 recruitment and Y 2 R residence time. C16-lipidation of PYY 3-36 had a negligible impact on Y 2 R signaling, binding, and endocytosis. In contrast, C18acid-lipidation minimized endocytosis, which indicated a decreased internalization through non-arrestin-related mechanisms. We propose a temporal model that connects the properties and position of the half-life extender with receptor G i versus Arr3 signaling bias. We believe that this will be important for future design of peptide therapeutics.

Published

2019

10. Melanin production by tyrosinase activity on a tyrosine-rich peptide fragment and pH-dependent self-assembly of its lipidated analogue.

Author

Hutchinson JA, Hamley IW, Edwards-Gayle CJC, Castelletto V, Piras C, Cramer R, Kowalczyk R, Seitsonen J, Ruokolainen J, and Rambo RP

Subjects

Amino Acid Sequence, Fluorescent Dyes chemistry, Hydrogels chemistry, Hydrogen-Ion Concentration, Lipopeptides metabolism, Micelles, Oligopeptides metabolism, Peptide Fragments metabolism, Peptide YY metabolism, Protein Conformation, beta-Strand, Protein Multimerization, Pyrenes chemistry, Tyrosine chemistry, Lipopeptides chemistry, Melanins chemical synthesis, Monophenol Monooxygenase chemistry, Oligopeptides chemistry, Peptide Fragments chemistry, Peptide YY chemistry

Abstract

We investigate the self-assembly of a palmitoylated (C16-chain at the N terminus) peptide fragment in comparison to the unlipidated peptide EELNRYY, a fragment of the gut hormone peptide PYY3-36. The lipopeptide C16-EELNRYY shows remarkable pH-dependent self-assembly above measured critical aggregation concentrations, forming fibrils at pH 7, but micelles at pH 10. The parent peptide does not show self-assembly behaviour. The lipopeptide forms hydrogels at sufficiently high concentration at pH 7, the dynamic mechanical properties of which were measured. We also show that the tyrosine functionality at the C terminus of EELNRYY can be used to enzymatically produce the pigment melanin. The enzyme tyrosinase oxidises tyrosine into 3,4-dihydroxyphenylalanine (DOPA), DOPA-quinone and further products, eventually forming eumelanin. This is a mechanism of photo-protection in the skin, for this reason controlling tyrosinase activity is a major target for skin care applications and EELNRYY has potential to be developed for such uses.

Published

2019

11. A Long-Acting PYY 3-36 Analog Mediates Robust Anorectic Efficacy with Minimal Emesis in Nonhuman Primates.

Author

Rangwala SM, D'Aquino K, Zhang YM, Bader L, Edwards W, Zheng S, Eckardt A, Lacombe A, Pick R, Moreno V, Kang L, Jian W, Arnoult E, Case M, Jenkinson C, Chi E, Swanson RV, Kievit P, Grove K, Macielag M, Erion MD, SinhaRoy R, and Leonard JN

Subjects

Animals, CHO Cells, Cricetulus, Glucagon-Like Peptide-1 Receptor agonists, Glucagon-Like Peptide-1 Receptor metabolism, HEK293 Cells, Humans, Liraglutide pharmacology, Macaca mulatta, Mice, Mice, Inbred C57BL, Obesity drug therapy, Obesity metabolism, Peptide YY administration & dosage, Anorexia chemically induced, Peptide YY chemistry, Peptide YY pharmacology, Vomiting chemically induced

Abstract

The gut hormone PYY 3-36 reduces food intake in humans and exhibits at least additive efficacy in combination with GLP-1. However, the utility of PYY analogs as anti-obesity agents has been severely limited by emesis and rapid proteolysis, a profile similarly observed with native PYY 3-36 in obese rhesus macaques. Here, we found that antibody conjugation of a cyclized PYY 3-36 analog achieved high NPY2R selectivity, unprecedented in vivo stability, and gradual infusion-like exposure. These properties permitted profound reduction of food intake when administered to macaques for 23 days without a single emetic event in any animal. Co-administration with the GLP-1 receptor agonist liraglutide for an additional 5 days further reduced food intake with only one animal experiencing a single bout of emesis. This antibody-conjugated PYY analog therefore may enable the long-sought potential of GLP-1/PYY-based combination treatment to achieve robust, well-tolerated weight reduction in obese patients., (Copyright © 2019 Elsevier Inc. All rights reserved.)

Published

2019

12. Self-Assembly of Lipopeptides Containing Short Peptide Fragments Derived from the Gastrointestinal Hormone PYY 3-36 : From Micelles to Amyloid Fibrils.

Author

Hutchinson JA, Hamley IW, Torras J, Alemán C, Seitsonen J, and Ruokolainen J

Subjects

Hydrogen-Ion Concentration, Molecular Dynamics Simulation, Protein Conformation, beta-Strand, Temperature, Amyloid chemistry, Lipopeptides chemistry, Micelles, Peptide Fragments chemistry, Peptide YY chemistry

Abstract

We investigate the impact of lipidation on the self-assembly of two peptide fragments from the gastrointestinal peptide hormone PYY 3-36 . The lipopeptides C 16 IKPEAP and C 16 IKPEAPGE contain the first 6 and 8 amino acid residues, respectively, from the PYY 3-36 peptide sequence, with a palmitoyl C 16 tail attached at the N-terminus. These lipopeptides form spherical micelles in aqueous solution, above a critical micelle concentration (cmc), which is pH-dependent. Modeling of small-angle X-ray scattering data along with molecular dynamics simulations shows the formation of micelles with a hydrophobic interior and a well-hydrated exterior. The lipopeptides have a disordered conformation over the pH and temperature ranges studied. The cmc is found to be independent of temperature, pointing to athermal micellization. In contrast to the presence of hydrated micelles in solution, β-sheet amyloid fibrils form in dried samples. Thus, the nanostructure of lipidated PYY 3-36 fragment peptides can be tuned by control of pH or concentration, for future applications.

Published

2019

13. Design of Y 2 Receptor Selective and Proteolytically Stable PYY 3-36 Analogues.

Author

Østergaard S, Kofoed J, Paulsson JF, Madsen KG, Jorgensen R, and Wulff BS

Subjects

Amino Acid Sequence, HEK293 Cells, Humans, Models, Molecular, Protein Conformation, beta-Strand, Protein Stability, Proteolysis, Substrate Specificity, Peptide YY chemistry, Peptide YY metabolism, Receptors, Neuropeptide Y metabolism

Abstract

In recent years peptide YY (PYY) has attracted attention within the area of diabetes and obesity due to its involvement in food intake regulation and glucose homeostasis. It is well-known that PYY 1-36 is rapidly cleaved by dipeptidyl peptidase-4 to the more Y 2 receptor selective analogue PYY 3-36 , which is further cleaved to the inactive analogue PYY 3-34 . In order to improve the selectivity and proteolytic stability of the C-terminus, we synthesized several analogues incorporating N-methyl amino acids or β-homo amino acids and other non-natural amino acids. These were tested against all four NPY receptors, and highly potent and Y 2 receptor selective analogues were identified by combining a tryptophan residue in position 30 with either N-methyl or β-homo arginine in position 35. We also identified an analogue with a MeGln 34 substitution that surprisingly displayed high affinity toward all four receptors. In addition, these analogues displayed improved stability toward C-terminal proteolysis compared to native PYY 3-36 .

Published

2018

14. Conformation and Aggregation of Selectively PEGylated and Lipidated Gastric Peptide Hormone Human PYY 3-36 .

Author

Castelletto V, Hamley IW, Seitsonen J, Ruokolainen J, Harris G, Bellmann-Sickert K, and Beck-Sickinger AG

Subjects

Humans, Lipids chemistry, Peptide YY chemistry, Peptide YY metabolism, Polyethylene Glycols chemistry, Protein Multimerization, Protein Structure, Secondary

Abstract

The gastric peptide hormone human PYY 3-36 is a target for the development of therapeutics, especially for treatment of obesity. The conformation and aggregation behavior of PEGylated and lipidated derivatives of this peptide are examined using a combination of fluorescence dye assays, circular dichroism (CD) spectroscopy, analytical ultracentrifugation (AUC) measurements, small-angle X-ray scattering (SAXS) and cryogenic-transmission electron microscopy (cryo-TEM). The behavior of two PYY 3-36 derivatives lipidated (with octyl chains) in different positions is compared to that of two derivatives with PEG attached at different residues and to that of the native peptide. We find that, unexpectedly, PYY 3-36 forms amyloid fibril structures above a critical aggregation concentration. Formation of these structures is suppressed by PEGylation or lipidation. PEGylation significantly reduces the (reversible) loss of α-helix content observed on heating PYY 3-36 . The PEG conjugates form mainly monomeric structures in solution- coiled-coil formation, and other aggregation presumably being sterically hindered by swollen PEG chains. However, some small aggregates are detected by AUC. In complete contrast, both of the two lipidated peptides show the formation of spherical micelle-like structures which are small oligomeric aggregates. Our findings show that PEGylation and lipidation are complementary strategies to tune the conformation and aggregation of the important gastric peptide hormone human PYY 3-36 .

Published

2018

15. The anorectic effect of central PYY 1-36 treatment in rainbow trout (Oncorhynchus mykiss) is associated with changes in mRNAs encoding neuropeptides and parameters related to fatty acid sensing and metabolism.

Author

Velasco C, Blanco AM, Unniappan S, and Soengas JL

Subjects

Amino Acid Sequence, Animals, Appetite Depressants chemistry, Eating physiology, Female, Fish Proteins genetics, Fish Proteins metabolism, Gene Expression Regulation drug effects, Neuropeptides metabolism, Peptide YY chemistry, RNA, Messenger genetics, RNA, Messenger metabolism, Appetite Depressants pharmacology, Fatty Acids metabolism, Neuropeptides genetics, Oncorhynchus mykiss genetics, Peptide YY pharmacology

Abstract

We hypothesized that peptide YY (PYY) is involved in the metabolic regulation of food intake in fish. Therefore, we assessed in rainbow trout (Oncorhynchus mykiss) the effects of intracerebroventricular treatment with 10 ng/g PYY 1-36 on food intake, expression of neuropeptides involved in food intake control, and the activity of fatty acid-sensing systems. The administration of PYY 1-36 caused a significant reduction in food intake up to 24 h post-treatment. This anorectic action was associated with changes 2 h after treatment in mRNA abundance of neuropeptides involved in metabolic regulation of food intake in hypothalamus (decreased NPY and raised CART values) and hindbrain (increased POMCa1 values). We also observed that PYY 1-36 treatment induced changes in mRNA abundance of parameters related to fatty acid sensing and metabolism in hypothalamus (decreased values of ACLY, PPARγ, and SREBP1c) and hindbrain (increased values of LPL, FAT/CD36, PPARα, PPARγ, and SREBP1c and decreased values of UCP2a). PYY 1-36 treatment also increased mRNA abundance of mTOR. In general, it seems that mRNAs encoding some components of the machinery required for fatty acid sensing and metabolism are activated by PYY 1-36 . The response observed was higher in the hindbrain than in the hypothalamus, supporting the greater importance of this brain area in mediating the modulatory effects of gastrointestinal hormones on feeding regulation., (Copyright © 2018 Elsevier Inc. All rights reserved.)

Published

2018

16. Elucidation of the Binding Mode of the Carboxyterminal Region of Peptide YY to the Human Y 2 Receptor.

Author

Xu B, Vasile S, Østergaard S, Paulsson JF, Pruner J, Åqvist J, Wulff BS, Gutiérrez-de-Terán H, and Larhammar D

Subjects

Amino Acid Sequence, Animals, Binding Sites physiology, HEK293 Cells, Humans, Peptide Fragments chemistry, Peptide Fragments genetics, Peptide Fragments metabolism, Peptide YY chemistry, Protein Structure, Secondary, Receptors, Neuropeptide Y chemistry, Swine, Peptide YY genetics, Peptide YY metabolism, Receptors, Neuropeptide Y genetics, Receptors, Neuropeptide Y metabolism

Abstract

Understanding the agonist-receptor interactions in the neuropeptide Y (NPY)/peptide YY (PYY) signaling system is fundamental for the design of novel modulators of appetite regulation. We report here the results of a multidisciplinary approach to elucidate the binding mode of the native peptide agonist PYY to the human Y 2 receptor, based on computational modeling, peptide chemistry and in vitro pharmacological analyses. The preserved binding orientation proposed for full-length PYY and five analogs, truncated at the amino terminus, explains our pharmacological results where truncations of the N-terminal proline helix showed little effect on peptide affinity. This was followed by receptor mutagenesis to investigate the roles of several receptor positions suggested by the modeling. As a complement, PYY-(3-36) analogs were synthesized with modifications at different positions in the common PYY/NPY C-terminal fragment ( 32 TRQRY 36 -amide). The results were assessed and interpreted by molecular dynamics and Free Energy Perturbation (FEP) simulations of selected mutants, providing a detailed map of the interactions of the PYY/NPY C-terminal fragment with the transmembrane cavity of the Y 2 receptor. The amidated C-terminus would be stabilized by polar interactions with Gln288 6.55 and Tyr219 5.39 , while Gln130 3.32 contributes to interactions with Q 34 in the peptide and T 32 is close to the tip of TM7 in the receptor. This leaves the core, α -helix of the peptide exposed to make potential interactions with the extracellular loops. This model agrees with most experimental data available for the Y 2 system and can be used as a basis for optimization of Y 2 receptor agonists., (Copyright © 2018 by The Author(s).)

Published

2018

17. Antiobesity and emetic effects of a short-length peptide YY analog and its PEGylated and alkylated derivatives.

Author

Niida A, Kanematsu-Yamaki Y, Asakawa T, Ishimura Y, Fujita H, Matsumiya K, Nishizawa N, Adachi Y, Mochida T, Tsuchimori K, Yoneyama-Hirozane M, Sakamoto J, Hirabayashi H, Fukui H, Takekawa S, and Asami T

Subjects

Alkylation, Amino Acid Sequence, Animals, Anti-Obesity Agents pharmacokinetics, Anti-Obesity Agents therapeutic use, Dogs, Emetics chemistry, Emetics therapeutic use, Emetics toxicity, Half-Life, Infusions, Subcutaneous, Mice, Mice, Inbred C57BL, Mice, Obese, Obesity pathology, Peptide YY pharmacokinetics, Peptide YY therapeutic use, Receptors, Neuropeptide Y agonists, Receptors, Neuropeptide Y metabolism, Vomiting etiology, Anti-Obesity Agents chemistry, Obesity drug therapy, Peptide YY chemistry, Polyethylene Glycols chemistry

Abstract

Neuropeptide Y2 receptor (Y2R) agonism is an important anorectic signal and a target of antiobesity drug discovery. Recently, we synthesized a short-length Y2R agonist, PYY-1119 (4-imidazolecarbonyl-[d-Hyp 24 ,Iva 25 ,Pya(4) 26 ,Cha 27,36 ,γMeLeu 28 ,Lys 30 ,Aib 31 ]PYY(23-36), 1) as an antiobesity drug candidate. Compound 1 induced marked body weight loss in diet-induced obese (DIO) mice; however, 1 also induced severe vomiting in dogs at a lower dose than the minimum effective dose administered to DIO mice. The rapid absorption of 1 after subcutaneous administration caused the severe vomiting. Polyethylene glycol (PEG)- and alkyl-modified derivatives of 1 were synthesized to develop Y2R agonists with improved pharmacokinetic profiles, i.e., lower maximum plasma concentration (C max ) and longer time at maximum concentration (T max ). Compounds 5 and 10, modified with 20 kDa PEG at the N-terminus and eicosanedioic acid at the Lys 30 side chain of 1, respectively, showed high Y2R binding affinity and induced significant body weight reduction upon once-daily administration to DIO mice. Compounds 5 and 10, with their relatively low C max and long T max , partially attenuated emesis in dogs compared with 1. These results indicate that optimization of pharmacokinetic properties of Y2R agonists is an effective strategy to alleviate emesis induced by Y2R agonism., (Copyright © 2017 Elsevier Ltd. All rights reserved.)

Published

2018

18. Highly potent antiobesity effect of a short-length peptide YY analog in mice.

Author

Nishizawa N, Niida A, Adachi Y, Kanematsu-Yamaki Y, Masuda Y, Kumano S, Yokoyama K, Noguchi Y, Asakawa T, Hirabayashi H, Amano N, Takekawa S, Ohtaki T, and Asami T

Subjects

Amino Acid Sequence, Animals, Anti-Obesity Agents chemistry, Anti-Obesity Agents pharmacology, Diet, Inhibitory Concentration 50, Male, Mice, Mice, Knockout, Molecular Structure, Peptide YY agonists, Body Weight drug effects, Peptide YY chemistry, Peptide YY pharmacology

Abstract

Continuous administration of a 14-amino acid peptide YY (PYY) analog, Ac-[d-Pro 24 ,Pya(4) 26 ,Cha 27,36 ,Aib 28,31 ,Lys 30 ]PYY(23-36) (4), which has a high binding affinity and agonist activity for the neuropeptide Y2 receptor (Y2R), has previously shown an antiobesity effect in a 2-week diet-induced obesity (DIO) study in mice. However, there remained a possibility to obtain more potent analogs by further improving its pharmacokinetic profile. A combination of the N-terminal 4-imidazolecarbonyl moiety and three amino acid substitutions, trans-4-hydroxy-d-proline (d-Hyp) 24 , isovaline (Iva) 25 , and γ-methylleucine (γMeLeu) 28 , not only improved the binding affinity of the peptide for Y2R but also increased its anorectic activity in lean mice. In a 2-week DIO study in mice, continuous administration of 4-imidazolecarbonyl-[d-Hyp 24 ,Iva 25 ,Pya(4) 26 ,Cha 27,36 ,γMeLeu 28 ,Lys 30 ,Aib 31 ]PYY(23-36) (31, PYY-1119) at a dose of 0.03mg/kg/day showed a highly potent antiobesity effect, with more than 10% body weight reduction., (Copyright © 2017 Elsevier Ltd. All rights reserved.)

Published

2017

19. Potent antiobesity effect of a short-length peptide YY-analogue continuously administered in mice.

Author

Nishizawa N, Niida A, Adachi Y, Masuda Y, Kumano S, Yokoyama K, Asakawa T, Hirabayashi H, Amano N, Takekawa S, Ohtaki T, and Asami T

Subjects

Animals, Anti-Obesity Agents administration & dosage, Anti-Obesity Agents chemistry, Dose-Response Relationship, Drug, Injections, Intravenous, Injections, Subcutaneous, Mice, Mice, Inbred C57BL, Mice, Obese, Molecular Structure, Peptide YY administration & dosage, Peptide YY chemistry, Receptors, Neuropeptide Y agonists, Structure-Activity Relationship, Anti-Obesity Agents pharmacology, Eating drug effects, Obesity drug therapy, Peptide YY pharmacology

Abstract

The gastrointestinal peptide, peptide YY 3-36 (PYY 3-36 ) and its shorter peptide analogues have been reported to reduce appetite by activating the neuropeptide Y2 receptor (Y2R), which is associated with obesity and other metabolic diseases. A 14-amino acid PYY analogue, Ac-[d-Pro 24 ,Cha 27,28,36 ,Aib 31 ]PYY(23-36) (3), showed high binding affinity and agonist activity for the Y2R, similar to that of PYY 3-36 , but had weak anorectic activity upon continuous administration in lean mice. Three amino acid substitutions [Pya(4) 26 , Aib 28 , Lys 30 ], which contributed to the decreased hydrophobicity of 3, efficiently increased its anorectic activity. The compound containing these three amino acids, Ac-[d-Pro 24 ,Pya(4) 26 ,Cha 27,36 ,Aib 28,31 ,Lys 30 ]PYY(23-36) (22), exerted more potent and durable food intake suppression than that by PYY 3-36 in lean mice, as well as excellent Y2R agonist activity (EC 50 : 0.20nM) and good subcutaneous bioavailability (66.6%). The 11-day continuous administration of 22 at 1mg/kg/day successfully produced antiobese and antidiabetic effects, with more than 20% body weight loss in obese and Type 2 diabetes ob/ob model mice., (Copyright © 2017 Elsevier Ltd. All rights reserved.)

Published

2017

20. Solution Structure and Constrained Molecular Dynamics Study of Vitamin B12 Conjugates of the Anorectic Peptide PYY(3-36).

Author

Henry KE, Kerwood DJ, Allis DG, Workinger JL, Bonaccorso RL, Holz GG, Roth CL, Zubieta J, and Doyle RP

Subjects

Binding Sites, Cycloaddition Reaction, Fluorescence Resonance Energy Transfer, HEK293 Cells, Humans, Hydrogen Bonding, Magnetic Resonance Spectroscopy, Molecular Dynamics Simulation, Peptide YY chemistry, Protein Structure, Tertiary, Peptide YY metabolism, Solutions chemistry, Vitamin B 12 metabolism

Abstract

Vitamin B12 -peptide conjugates have considerable therapeutic potential through improved pharmacokinetic and/or pharmacodynamic properties imparted on the peptide upon covalent attachment to vitamin B12 (B12 ). There remains a lack of structural studies investigating the effects of B12 conjugation on peptide secondary structure. Determining the solution structure of a B12 -peptide conjugate or conjugates and measuring functions of the conjugate(s) at the target peptide receptor may offer considerable insight concerning the future design of fully optimized conjugates. This methodology is especially useful in tandem with constrained molecular dynamics (MD) studies, such that predictions may be made about conjugates not yet synthesized. Focusing on two B12 conjugates of the anorectic peptide PYY(3-36), one of which was previously demonstrated to have improved food intake reduction compared with PYY(3-36), we performed NMR structural analyses and used the information to conduct MD simulations. The study provides rare structural insight into vitamin B12 conjugates and validates the fact that B12 can be conjugated to a peptide without markedly affecting peptide secondary structure., (© 2016 WILEY-VCH Verlag GmbH & Co. KGaA, Weinheim.)

Published

2016

21. In vivo and in vitro degradation of peptide YY3-36 to inactive peptide YY3-34 in humans.

Author

Toräng S, Bojsen-Møller KN, Svane MS, Hartmann B, Rosenkilde MM, Madsbad S, and Holst JJ

Subjects

Animals, Blood Glucose, Blood Pressure, COS Cells, Chlorocebus aethiops, Humans, Male, Peptide Fragments chemistry, Peptide YY chemistry, Proteolysis, Single-Blind Method, Young Adult, Peptide Fragments metabolism, Peptide YY metabolism

Abstract

Peptide YY (PYY) is a 36-amino-acid peptide released from enteroendocrine cells upon food intake. The NH2 terminally truncated metabolite, PYY3-36, exerts anorexic effects and has received considerable attention as a possible antiobesity drug target. The kinetics and degradation products of PYY metabolism are not well described. A related peptide, neuropeptide Y, may be degraded from the COOH terminus, and in vivo studies in pigs revealed significant COOH-terminal degradation of PYY. We therefore investigated PYY metabolism in vitro after incubation in human blood and plasma and in vivo after infusion of PYY1-36 and PYY3-36 in eight young, healthy men. A metabolite, corresponding to PYY3-34, was formed after incubation in plasma and blood and during the infusion of PYY. PYY3-34 exhibited no agonistic or antagonistic effects on the Y2 receptor. PYY1-36 infused with and without coadministration of sitagliptin was eliminated with half-lives of 10.1 ± 0.5 and 9.4 ± 0.8 min (means ± SE) and metabolic clearance rates of 15.7 ± 1.5 and 14.1 ± 1.1 ml·kg(-1)·min(-1) after infusion, whereas PYY3-36 was eliminated with a significantly longer half-life of 14.9 ± 1.3 min and a metabolic clearance rate of 9.4 ± 0.6 ml·kg(-1)·min(-1) We conclude that, upon intravenous infusion in healthy men, PYY is inactivated by cleavage of the two COOH-terminal amino acids. In healthy men, PYY3-36 has a longer half-life than PYY1-36., (Copyright © 2016 the American Physiological Society.)

Published

2016

22. Nanocarrier for Oral Peptide Delivery Produced by Polyelectrolyte Complexation in Nanoconfinement.

Author

He W, Parowatkin M, Mailänder V, Flechtner-Mors M, Graf R, Best A, Koynov K, Mohr K, Ziener U, Landfester K, and Crespy D

Subjects

Alginates chemistry, Chitosan therapeutic use, Electrolytes chemistry, Hexuronic Acids chemistry, Humans, Hydrophobic and Hydrophilic Interactions, Peptide YY therapeutic use, Polymers chemistry, Polymers therapeutic use, Chitosan chemistry, Drug Carriers, Obesity drug therapy, Peptide YY chemistry

Abstract

The hydrophilic peptide YY (PYY) is a promising hormone-based antiobesity drug. We present a new concept for the delivery of PYY from pH-responsive chitosan-based nanocarriers. To overcome the drawbacks while retaining the merits of the polyelectrolyte complex (PEC) method, we propose a one-pot approach for the encapsulation of a hydrophilic peptide drug in cross-linked PEC nanocarriers. First, the hydrophilic peptide is encapsulated via polyelectrolyte complexation within water-in-oil miniemulsion droplets. In a second step, the PEC surface is reinforced by controlled interfacial cross-linking. PYY is efficiently encapsulated and released upon pH change. Such nanocarriers are promising candidates for the fight against obesity and, in general, for the oral delivery of protein drugs.

Published

2015

23. Preparation and characterization of albumin conjugates of a truncated peptide YY analogue for half-life extension.

Author

Ehrlich GK, Michel H, Truitt T, Riboulet W, Pop-Damkov P, Goelzer P, Hainzl D, Qureshi F, Lueckel B, Danho W, Conde-Knape K, and Konkar A

Subjects

Amino Acid Sequence, Animals, Binding Sites, Eating drug effects, Half-Life, Humans, Male, Mice, Mice, Inbred C57BL, Models, Molecular, Molecular Sequence Data, Molecular Weight, Peptide YY chemistry, Protein Binding, Protein Conformation, Serum Albumin chemistry, Serum Albumin pharmacology, Substrate Specificity, Peptide YY metabolism, Serum Albumin metabolism

Abstract

Recombinant human serum albumin (HSA) conjugates of a 15-amino-acid truncated peptide YY (PYY) analogue were prepared using three heterobifunctional linkers [succinimidyl 4-[N-maleimidomethyl]cyclohexane-1-carboxylate (SMCC), 6-maleimidohexanoic acid N-hydroxysuccinimide ester (MHS), and N-[γ-maleimidobutyryloxy]sulfosuccinimide ester (GMBS)] in 2 synthetic steps involving (1) reaction of succinimidyl ester on linker with ε-amine of Lys2 on the peptide and (2) reaction of maleimide on peptide linker with free thiol of Cysteine 34 (Cys34) on albumin. In-process controls using ESI LC-MS were used to follow reactions and identify reaction products. Proteolytic digests of the conjugate revealed that peptide conjugation occurs at Cys34 on HSA. Conjugates were assayed in cell-based assays to determine potency at the human Y2-receptor, and selectivity at the human Y1-, Y4-, and Y5-receptors using a calcium flux assay. All three conjugates assayed were selective agonists of the Y2-receptor, and displayed nanomolar potencies. MCC and MH conjugates were selected for acute PK/PD studies in DIO mice. Significant reduction in food intake was observed with the MH conjugate, which lasted for 24 h at the 10 mg (or 4 μmol)/kg dose. While the MCC conjugate exhibited greater potency in vitro, it was slightly less effective than the MH conjugate in vivo with respect to reduction in food intake. Both conjugates were significantly less active than the peptide coupled to a 30 kDa PEG. The observed T1/2 (8-9 h) for both conjugates was significantly lower than that observed for the PEGylated peptide (∼25 h). These results suggest that, as compared with the unmodified and PEGylated peptide, the extended circulation half-life of albumin conjugates is mediated through uptake and recirculation by FcRn, and allometric scaling methods are necessary to account for interspecies variation in pharmacokinetic properties.

Published

2013

24. Detecting ligand interactions with G protein-coupled receptors in real-time on living cells.

Author

Xu B, Varasteh Z, Orlova A, Andersson K, Larhammar D, and Björkelund H

Subjects

Animals, Bombesin analogs & derivatives, HEK293 Cells, Humans, Ligands, Peptide YY chemistry, Peptide YY metabolism, Radioactive Tracers, Receptors, Neuropeptide Y genetics, Receptors, Neuropeptide Y metabolism, Swine, Time Factors, Transfection, Radioligand Assay, Receptors, G-Protein-Coupled metabolism

Abstract

G protein-coupled receptors (GPCRs) are a large group of receptors of great biological and clinical relevance. Despite this, the tools for a detailed analysis of ligand-GPCR interactions are limited. The aim of this paper was to demonstrate how ligand binding to GPCRs can be followed in real-time on living cells. This was conducted using two model systems, the radiolabeled porcine peptide YY (pPYY) interacting with transfected human Y2 receptor (hY2R) and the bombesin antagonist RM26 binding to the naturally expressed gastrin-releasing peptide receptor (GRPR). By following the interaction over time, the affinity and kinetic properties such as association and dissociation rate were obtained. Additionally, data were analyzed using the Interaction Map method, which can evaluate a real-time binding curve and present the number of parallel interactions contributing to the curve. It was found that pPYY binds very slowly with an estimated time to equilibrium of approximately 12h. This may be problematic in standard end-point assays where equilibrium is required. The RM26 binding showed signs of heterogeneity, observed as two parallel interactions with unique kinetic properties. In conclusion, measuring binding in real-time using living cells opens up for a better understanding of ligand interactions with GPCRs., (Copyright © 2013 Elsevier Inc. All rights reserved.)

Published

2013

25. Salivary peptide tyrosine-tyrosine 3-36 modulates ingestive behavior without inducing taste aversion.

Author

Hurtado MD, Sergeyev VG, Acosta A, Spegele M, La Sala M, Waler NJ, Chiriboga-Hurtado J, Currlin SW, Herzog H, Dotson CD, Gorbatyuk OS, and Zolotukhin S

Subjects

Aminophylline, Animals, Conditioning, Psychological drug effects, Eating drug effects, Extracellular Signal-Regulated MAP Kinases metabolism, Gene Expression Regulation drug effects, Gene Expression Regulation genetics, Glucagon-Like Peptide 1 metabolism, Humans, Iodine Isotopes pharmacokinetics, Male, Mice, Mice, Inbred C57BL, Oxytocin metabolism, Peptide YY chemistry, Proto-Oncogene Proteins c-fos metabolism, Satiation drug effects, Tyrosine 3-Monooxygenase metabolism, Vasopressins metabolism, alpha-MSH metabolism, Feeding Behavior drug effects, Peptide Fragments pharmacology, Peptide YY deficiency, Saliva enzymology

Abstract

Hormone peptide tyrosine-tyrosine (PYY) is secreted into circulation from the gut L-endocrine cells in response to food intake, thus inducing satiation during interaction with its preferred receptor, Y2R. Clinical applications of systemically administered PYY for the purpose of reducing body weight were compromised as a result of the common side effect of visceral sickness. We describe here a novel approach of elevating PYY in saliva in mice, which, although reliably inducing strong anorexic responses, does not cause aversive reactions. The augmentation of salivary PYY activated forebrain areas known to mediate feeding, hunger, and satiation while minimally affecting brainstem chemoreceptor zones triggering nausea. By comparing neuronal pathways activated by systemic versus salivary PYY, we identified a metabolic circuit associated with Y2R-positive cells in the oral cavity and extending through brainstem nuclei into hypothalamic satiety centers. The discovery of this alternative circuit that regulates ingestive behavior without inducing taste aversion may open the possibility of a therapeutic application of PYY for the treatment of obesity via direct oral application.

Published

2013

26. Mutagenesis and computational modeling of human G-protein-coupled receptor Y2 for neuropeptide Y and peptide YY.

Author

Xu B, Fällmar H, Boukharta L, Pruner J, Lundell I, Mohell N, Gutiérrez-de-Terán H, Aqvist J, and Larhammar D

Subjects

Humans, Mutagenesis, Site-Directed, Neuropeptide Y chemistry, Peptide YY chemistry, Protein Structure, Secondary, Receptors, G-Protein-Coupled chemistry, Receptors, G-Protein-Coupled genetics, Receptors, Neuropeptide Y chemistry, Receptors, Neuropeptide Y genetics, Receptors, Peptide chemistry, Receptors, Peptide genetics, Neuropeptide Y metabolism, Peptide YY metabolism, Receptors, G-Protein-Coupled metabolism, Receptors, Neuropeptide Y metabolism, Receptors, Peptide metabolism

Abstract

Neuropeptide Y and peptide YY receptor type 2 (Y2) is involved in appetite regulation and several other physiological processes. We have investigated the structure of the human Y2 receptor. Computational modeling of receptor-agonist interactions was used as a guide to design a series of receptor mutants, followed by binding assays using full-length and truncated peptide agonists and the Y2-specific antagonist BIIE0246. Our model suggested a hydrogen bond network among highly conserved residues Thr2.61, Gln3.32, and His7.39, which could play roles in ligand binding and/or receptor structure. In addition, the C-terminus of the peptide could make contact with residues Tyr5.38 and Leu6.51. Mutagenesis of all these positions, followed by binding assays, provides experimental support for our computational model: most of the mutants for the residues forming the proposed hydrogen bond network displayed reduced peptide agonist affinities as well as reduced hPYY3-36 potency in a functional assay. The Ala and Leu mutants of Gln3.32 and His7.39 disrupted membrane expression of the receptor. Combined with the modeling, the experimental results support roles for these hydrogen bond network residues in peptide binding as well as receptor architecture. The reduced agonist affinity for mutants of Tyr5.38 and Leu6.51 supports their role in a binding pocket surrounding the invariant tyrosine at position 36 of the peptide ligands. The results for antagonist BIIE0246 suggest several differences in interactions compared to those of the peptides. Our results lead to a new structural model for NPY family receptors and peptide binding.

Published

2013

27. Co-delivery of a hydrophobic small molecule and a hydrophilic peptide by porous silicon nanoparticles.

Author

Liu D, Bimbo LM, Mäkilä E, Villanova F, Kaasalainen M, Herranz-Blanco B, Caramella CM, Lehto VP, Salonen J, Herzig KH, Hirvonen J, and Santos HA

Subjects

Animals, Anti-Inflammatory Agents, Non-Steroidal administration & dosage, Anti-Inflammatory Agents, Non-Steroidal chemistry, Caco-2 Cells, Cell Line, Cell Survival drug effects, Coculture Techniques, Drug Carriers chemistry, HT29 Cells, Hep G2 Cells, Humans, Hydrophobic and Hydrophilic Interactions, Indomethacin administration & dosage, Indomethacin chemistry, Mice, Nanoparticles chemistry, Peptide Fragments administration & dosage, Peptide Fragments chemistry, Peptide YY administration & dosage, Peptide YY chemistry, Permeability, Porosity, Silicon chemistry, Drug Carriers administration & dosage, Nanoparticles administration & dosage, Silicon administration & dosage

Abstract

Nanoparticulate drug delivery systems offer remarkable opportunities for clinical treatment. However, there are several challenges when they are employed to deliver multiple cargos/payloads, particularly concerning the synchronous delivery of small molecular weight drugs and relatively larger peptides. Since porous silicon (PSi) nanoparticles (NPs) can easily contain high payloads of drugs with various properties, we evaluated their carrier potential in multi-drug delivery for co-loading of the hydrophobic drug indomethacin and the hydrophilic human peptide YY3-36 (PYY3-36). Sequential loading of these two drugs into the PSi NPs enhanced the drug release rate of each drug and also their amount permeated across Caco-2 and Caco-2/HT29 cell monolayers. Regardless of the loading approach used, dual or single, the drug permeation profiles were in good correlation with their drug release behaviour. Furthermore, the permeation studies indicated the critical role of the mucus intestinal layer and the paracellular resistance in the permeation of the therapeutic compounds across the intestinal wall. Loading with PYY3-36 also greatly improved the cytocompatibility of the PSi NPs. Conformational analysis indicated that the PYY3-36 could still display biological activity after release from the PSi NPs and permeation across the intestinal cell monolayers. These results are the first demonstration of the promising potential of PSi NPs for simultaneous multi-drug delivery of both hydrophobic and hydrophilic compounds., (Copyright © 2013 Elsevier B.V. All rights reserved.)

Published

2013

28. A parallel semisynthetic approach for structure-activity relationship studies of peptide YY.

Author

Albertsen L, Østergaard S, Paulsson JF, Norrild JC, and Strømgaard K

Subjects

Amino Acid Sequence, Escherichia coli metabolism, Molecular Sequence Data, Oligopeptides chemical synthesis, Peptide YY genetics, Peptide YY metabolism, Protein Binding, Receptors, Neuropeptide Y chemistry, Receptors, Neuropeptide Y metabolism, Recombinant Fusion Proteins biosynthesis, Recombinant Fusion Proteins chemistry, Recombinant Fusion Proteins genetics, Solid-Phase Synthesis Techniques, Structure-Activity Relationship, Oligopeptides chemistry, Peptide YY chemistry

Abstract

The gut hormone peptide YY (PYY) is postprandially secreted from enteroendocrine L cells and is involved in the regulation of energy homeostasis. The N-terminal truncated version PYY(3-36) decreases food intake and has potential as an anti-obesity agent. The anorectic effect of PYY(3-36) is mediated through Y₂ receptors in the hypothalamus, vagus, and brainstem regions, and it is well known that the C-terminal tetrapeptide sequence of PYY(3-36) is crucial for Y2 receptor activation. The aim of this work was to develop a semisynthetic methodology for the generation of a library of C-terminally modified PYY(3-36) analogues. By using an intein-based expression system, PYY(3-29) was generated as a C-terminal peptide α-thioester. Heptapeptides bearing an N-terminal cysteine and modifications at one of the four C-terminal positions were synthesized in a 96-well plate by parallel solid-phase synthesis. In the plate format, an array of [Ala30]PYY(3-36) analogues were generated by ligation, desulfurization, and subsequent solid-phase extraction. The generated analogues, in which either Arg33, Gln34, Arg35, or Tyr36 had been substituted with proteinogenic or non-proteinogenic amino acids, were tested in a functional Y₂ receptor assay. Generally, substitutions of Tyr36 were better tolerated than modifications of Arg33, Gln34, and Arg35. Two analogues showed significantly improved Y₂ receptor selectivity; therefore, these results could be used to design new drug candidates for the treatment of obesity., (Copyright © 2013 WILEY-VCH Verlag GmbH & Co. KGaA, Weinheim.)

Published

2013

29. Presence and dynamics of leptin, GLP-1, and PYY in human breast milk at early postpartum.

Author

Schueler J, Alexander B, Hart AM, Austin K, and Larson-Meyer DE

Subjects

Absorptiometry, Photon, Adiposity, Adult, Appetite physiology, Body Mass Index, Female, Humans, Radioimmunoassay, Weight Gain physiology, Young Adult, Glucagon-Like Peptide 1 chemistry, Leptin chemistry, Milk, Human chemistry, Peptide YY chemistry, Postpartum Period physiology

Abstract

Objective: The presence of appetite hormones, namely glucagon-like peptide-1 (GLP-1), peptide YY (PYY), and leptin in breast milk may be important in infant feeding regulation and infant growth. This study evaluated whether concentrations of GLP-1, PYY, and leptin change across a single feeding (from fore- to hindmilk), and are associated with maternal and infant anthropometrics., Design and Methods: Thirteen postpartum women (mean ± SD: 25.6 ± 4.5 years, 72.0 ± 11.9 kg) provided fore- and hindmilk samples 4-5 weeks after delivery and underwent measurements of body weight and composition by Dual X-ray Absorptiometry. GLP-1, PYY, and leptin concentrations were measured using radioimmunoassay, and milk fat content was determined by creamatocrit., Results: Concentration of GLP-1 and content of milk fat was higher in hindmilk than foremilk (P ≤ 0.05). PYY and leptin concentrations did not change between fore- and hindmilk. Both leptin concentration and milk fat content were correlated with indices of maternal adiposity, including body mass index (r = 0.65-0.85, P < 0.02), and fat mass (r = 0.65-0.84, P < 0.02). Hindmilk GLP-1 was correlated with infant weight gain from birth to 6 months (r = -0.67, P = 0.034)., Conclusion: The presence of appetite hormones in breast milk may be important in infant appetite and growth regulation., (Copyright © 2013 The Obesity Society.)

Published

2013

30. Effects of fasting and feeding on the brain mRNA expressions of orexin, tyrosine hydroxylase (TH), PYY and CCK in the Mexican blind cavefish (Astyanax fasciatus mexicanus).

Author

Wall A and Volkoff H

Subjects

Amino Acid Sequence, Animals, Characidae metabolism, Characidae physiology, Cholecystokinin chemistry, Cholecystokinin genetics, Cholecystokinin metabolism, Cloning, Molecular, Fish Proteins chemistry, Fish Proteins genetics, Intracellular Signaling Peptides and Proteins chemistry, Intracellular Signaling Peptides and Proteins genetics, Intracellular Signaling Peptides and Proteins metabolism, Molecular Sequence Data, Neuropeptides chemistry, Neuropeptides genetics, Neuropeptides metabolism, Orexins, Peptide YY chemistry, Peptide YY genetics, Peptide YY metabolism, RNA, Messenger metabolism, Sequence Alignment, Tyrosine 3-Monooxygenase chemistry, Tyrosine 3-Monooxygenase genetics, Tyrosine 3-Monooxygenase metabolism, Brain metabolism, Characidae genetics, Fasting, Feeding Behavior, Fish Proteins metabolism, Gene Expression Regulation

Abstract

The effects of fasting and feeding on the brain expression of orexin (OX), tyrosine hydroxylase (TH), peptide Y (PY) and cholecystokinin (CCK) were examined in the blind cavefish Astyanax fasciatus mexicanus. A 10-days fasting period induced increases in both OX and TH brain mRNA expression but had no effect on PYY and CCK expression. Periprandial changes in expression were seen for OX, TH and PYY but not for CCK. OX brain expression peaked 1h prior to a scheduled meal and decreased 1h post feeding in fed fish. A peak in TH expression was seen 1h post feeding in unfed fish whereas a peak in PYY expression was seen 1h post feeding in fed fish. Our result indicates that brain OX, TH and PYY might be involved in the central regulation of feeding of blind cavefish., (Copyright © 2013 Elsevier Inc. All rights reserved.)

Published

2013

31. Development of porous silicon nanocarriers for parenteral peptide delivery.

Author

Kovalainen M, Mönkäre J, Kaasalainen M, Riikonen J, Lehto VP, Salonen J, Herzig KH, and Järvinen K

Subjects

Administration, Cutaneous, Administration, Intravenous, Animals, Biological Availability, Delayed-Action Preparations administration & dosage, Delayed-Action Preparations chemistry, Drug Carriers administration & dosage, Drug Delivery Systems, Mice, Mice, Inbred BALB C, Porosity, Silicon administration & dosage, Drug Carriers chemistry, Nanoparticles administration & dosage, Nanoparticles chemistry, Peptide Fragments administration & dosage, Peptide Fragments chemistry, Peptide YY administration & dosage, Peptide YY chemistry, Silicon chemistry

Abstract

Porous silicon (PSi) is receiving growing attention in biomedical research, for example, in drug and peptide delivery. Inspired by several advantages of PSi, herein, thermally oxidized (TOPSi, hydrophilic), undecylenic acid-treated thermally hydrocarbonized (UnTHCPSi, moderately hydrophilic), and thermally hydrocarbonized (THCPSi, hydrophobic) PSi nanocarriers are investigated for sustained subcutaneous (sc) and intravenous (iv) peptide delivery. The route of administration is shown to affect drastically peptide YY3-36 (PYY3-36) release from the PSi nanocarriers in mice. Subcutaneous nanocarriers are demonstrated to be capable to sustain PYY3-36 delivery over 4 days, with the high absolute bioavailability values of PYY3-36. The pharmacokinetic parameters of PYY3-36 are presented to be similar between the sc PSi nanocarriers despite surface chemistry. In contrast, iv-delivered PSi nanocarriers display significant differences between the surface types. Overall, these results demonstrate the feasibility of PSi nanocarriers for the sustained sc delivery of peptides.

Published

2013

32. Analogs of pancreatic polypeptide and peptide YY with a locked PP-fold structure are biologically active.

Author

Germain N, Minnion JS, Tan T, Shillito J, Gibbard C, Ghatei M, and Bloom S

Subjects

Animals, Cystine chemical synthesis, Food Deprivation, HEK293 Cells, Humans, Mice, Mice, Inbred C57BL, Pancreatic Polypeptide pharmacology, Peptide YY pharmacology, Peptides, Cyclic chemical synthesis, Peptides, Cyclic pharmacology, Protein Binding, Protein Structure, Secondary, Protein Structure, Tertiary, Receptors, Neuropeptide Y chemistry, Cystine chemistry, Eating drug effects, Pancreatic Polypeptide chemistry, Peptide YY chemistry, Peptides, Cyclic chemistry

Abstract

Pancreatic polypeptide (PP), peptide YY (PYY) and neuropeptide Y (NPY), members of the PP-fold family share a high degree of sequence homology. Nuclear magnetic resonance (NMR) and X-ray crystallography studies have shown these peptides can adopt a tightly organized tertiary structure called the PP-fold, which has long been assumed to be the active structure of this family of peptides. To date, however, no studies have been completed with PYY and PP which confirm if the PP-fold structure is important for their physiological actions. The aim of the study was to test if PYY and PP locked into the PP-fold maintained biological activity. Therefore, we designed and produced analogs of PP and PYY in a cyclic conformation with two cysteine amino acid substitutions at the N-terminus and at position 27. These were oxidized to form a cysteine disulfide bond locking the peptides into the PP-fold structure. Studies demonstrate that the cyclic analogs have both similar in vivo activity to their parent molecules, and affinity for the Y2 and Y4 receptors. Results suggest that the proposed PP and PYY-fold is likely to be their biologically active conformation., (Copyright © 2012 Elsevier Inc. All rights reserved.)

Published

2013

33. Expression and purification of human PYY(3-36) in Escherichia coli using a His-tagged small ubiquitin-like modifier fusion.

Author

Fazen CH, Kahkoska AR, and Doyle RP

Subjects

Amino Acid Sequence, Chromatography, Affinity, Chromatography, High Pressure Liquid, Circular Dichroism, Electrophoresis, Polyacrylamide Gel, Histidine chemistry, Humans, Molecular Sequence Data, Peptide YY chemistry, Peptide YY isolation & purification, Protein Conformation, Recombinant Fusion Proteins chemistry, Recombinant Fusion Proteins isolation & purification, Small Ubiquitin-Related Modifier Proteins chemistry, Small Ubiquitin-Related Modifier Proteins isolation & purification, Spectrometry, Mass, Matrix-Assisted Laser Desorption-Ionization, Cloning, Molecular methods, Escherichia coli genetics, Peptide YY genetics, Recombinant Fusion Proteins genetics, Small Ubiquitin-Related Modifier Proteins genetics

Abstract

Human PYY(3-36) (hPYY3-36) is a 34 amino acid hormone that has received a great deal of attention due to its effects on appetite regulation. hPYY(3-36) was modified at the N-terminus with an octahistidine tag and factor Xa protease sequence along with the small ubiquitin-like modifier (SUMO) tag and expressed in Escherichia coli. The protein was purified from clarified E. coli lysate by immobilized metal affinity chromatography (IMAC) with a yield of 30±7 mg/L of induced culture returned as an average over seven runs, and its identity was confirmed by Western blot and hPYY antibody recognition. The SUMO-tagged hPYY(3-36) was digested with two different proteases to return either His-tagged hPYY(3-36) or unmodified hPYY(3-36): (1) digestion with SUMO protease proceeded at about 50% efficiency yielding His-tagged hPYY(3-36); (2) digestion with factor Xa protease proceeded at greater than 90% efficiency yielding final hPYY(3-36). Products were purified from the digestion mixtures by reverse-phase high-performance liquid chromatography (C(18)) or IMAC, respectively, the identities were confirmed by mass spectrometry and hPYY antibody recognition, and the folded state of His-tagged hPYY(3-36) was investigated by circular dichroism spectroscopy., (Copyright © 2012 Elsevier Inc. All rights reserved.)

Published

2012

34. Improving membrane binding as a design strategy for amphipathic peptide hormones: 2-helix variants of PYY3-36.

Author

Pedersen SL, Bhatia VK, Jurt S, Paulsson JF, Pedersen MH, Jorgensen R, Holst B, Stamou D, Vrang N, Zerbe O, and Jensen KJ

Subjects

Amino Acid Sequence, Magnetic Resonance Spectroscopy, Molecular Sequence Data, Peptide Hormones chemistry, Protein Binding, Protein Structure, Secondary, Structure-Activity Relationship, Cell Membrane metabolism, Peptide Hormones chemical synthesis, Peptide Hormones metabolism, Peptide YY chemistry

Abstract

It has been hypothesized that amphipathic peptides might bind to membranes prior to activating their cognate receptors, but this has proven difficult to test. The peptide hormone PYY3-36 is believed to perform its appetite-suppressing actions through binding to hypothalamic Y2 receptors. It has been proposed that PYY3-36 via its amphipathic α-helix binds to the plasma membrane prior to receptor docking. Here, our aim was to study the implication of this hypothesis using new analogs of PYY3-36. We first studied membrane binding of PYY3-36. Next, we designed a series of PYY3-36 analogs to increase membrane-binding affinity by substituting the N-terminal segment with a de novo designed α-helical, amphipathic sequence. These 2-helix variants of PYY3-36 were assembled by solid-phase peptide synthesis. Pharmacological studies demonstrated that even though the native peptide sequence was radically changed, highly active Y2 receptor agonists were generated. A potent analog, with a Kd of 4 nM for membranes, was structurally characterized by NMR in the membrane-bound state, which clearly showed that it formed the expected 2-helix. The topology of the peptide-micelle association was studied by paramagnetic relaxation enhancement using a spin label, which confirmed that the hydrophobic residues bound to the membrane. Our studies further support the hypothesis that PYY3-36 associates with the membrane and indicate that this can be used in the design of novel molecules with high receptor binding potency. These observations are likely to be generally important for peptide hormones and biopharmaceutical drugs derived from them. This new 2-helix variant of PYY3-36 will be useful as a tool compound for studying peptide-membrane interactions., (Copyright © 2012 European Peptide Society and John Wiley & Sons, Ltd.)

Published

2012

35. Effect of isotonic solutions and peptide adsorption on zeta potential of porous silicon nanoparticle drug delivery formulations.

Author

Kaasalainen M, Mäkilä E, Riikonen J, Kovalainen M, Järvinen K, Herzig KH, Lehto VP, and Salonen J

Subjects

Adsorption, Isotonic Solutions, Particle Size, Porosity, Drug Carriers chemistry, Glucagon-Like Peptide 1 chemistry, Nanoparticles chemistry, Peptide Fragments chemistry, Peptide YY chemistry, Silicon chemistry

Abstract

Recently, highly promising results considering the use of porous silicon (PSi) nanoparticles as a controlled and targeted drug delivery system have been published. Drugs are typically loaded into PSi nanoparticles by electrostatic interactions, and the drug-loaded nanoparticles are then administered parenterally in isotonic solutions. Zeta potential has an important role in drug adsorption and overall physical stability of nanosuspensions. In the present study, we used zeta potential measurements to study the impact of the formulation components to the nanosuspension stability. The impact of medium was studied by measuring isoelectric points (IEP) and zeta potentials in isotonic media. The role of drug adsorption was demonstrated with gastrointestinal peptides GLP-1(7-37) and PYY (3-36) and the selection of isotonic additive was demonstrated with peptide-loaded PSi nanoparticles. The results show the notable effect of isotonic solutions and peptide adsorption on zeta potential of PSi nanosuspensions. As a rule of thumb, the sugars (sucrose, dextrose and mannitol) seem to be good media for negatively charged peptide-loaded particles and weak acids (citric- and lactic acid) for positively charged particles. Nevertheless, perhaps the most important rule can be given for isotonic salt solutions which all are very poor media when the stability of nanosuspension is considered., (Copyright © 2012 Elsevier B.V. All rights reserved.)

Published

2012

36. Mesoporous silicon (PSi) for sustained peptide delivery: effect of psi microparticle surface chemistry on peptide YY3-36 release.

Author

Kovalainen M, Mönkäre J, Mäkilä E, Salonen J, Lehto VP, Herzig KH, and Järvinen K

Subjects

Amino Acid Sequence, Animals, Humans, Injections, Subcutaneous, Mice, Mice, Inbred BALB C, Molecular Sequence Data, Peptide YY chemistry, Porosity, Delayed-Action Preparations chemistry, Peptide YY administration & dosage, Peptide YY blood, Silicon chemistry

Abstract

Purpose: To achieve sustained peptide delivery via mesoporous silicon (PSi) microparticles and to evaluate the effects of different surface chemistries on peptide YY3-36 (PYY3-36) delivery., Methods: PYY3-36 was loaded into thermally oxidized (TOPSi), thermally hydrocarbonized (THCPSi) and undecylenic acid treated THCPSi (UnTHCPSi) microparticles with comparable porous properties. In vitro, PYY3-36 release was investigated by centrifuge. In vivo, PYY3-36 plasma concentrations were analyzed after delivery in microparticles or solution., Results: Achieved loading degrees were high (12.2 - 16.0% w/w). PYY3-36 release was sustained from all microparticles; order of PYY3-36 release was TOPSi > THCPSi > UnTHCPSi both in vitro and in vivo. In mice, PSi microparticles achieved sustained PYY3-36 release over 4 days, whereas PYY3-36 solution was eliminated in 12 h. In vitro, only 27.7, 14.5 and 6.2% of loaded PYY3-36 was released from TOPSi, THCPSi and UnTHCPSi, respectively. Absolute PYY3-36 bioavailabilities were 98, 13, 9 and 38% when delivered subcutaneously in TOPSi, THCPSi, UnTHCPSi and solution, respectively. The results clearly demonstrate improved bioavailability of PYY3-36 via TOPSi and the importance of surface chemistry of PSi on peptide release., Conclusions: PSi represents a promising sustained and tailorable release system for PYY3-36.

Published

2012

37. Challenges in mass spectrometry-based quantification of bioactive peptides: a case study exploring the neuropeptide Y family.

Author

Xi L, Jin Y, Parker EA, Josh P, Jones A, Wijffels G, and Colgrave ML

Subjects

Chromatography, Liquid, Pancreatic Polypeptide chemistry, Peptide YY chemistry, Mass Spectrometry methods, Neuropeptide Y chemistry, Peptides chemistry

Abstract

The study of biologically active peptides is critical to the understanding of physiological pathways, especially those involved in the development of disease. Historically, the measurement of biologically active endogenous peptides has been undertaken by radioimmunoassay, a highly sensitive and robust technique that permits the detection of physiological concentrations in different biofluid and tissue extracts. Over recent years, a range of mass spectrometric approaches have been applied to peptide quantification with limited degrees of success. Neuropeptide Y (NPY), peptide YY (PYY), and pancreatic polypeptide (PP) belong to the NPY family exhibiting regulatory effects on appetite and feeding behavior. The physiological significance of these peptides depends on their molecular forms and in vivo concentrations systemically and at local sites within tissues. In this report, we describe an approach for quantification of individual peptides within mixtures using high-performance liquid chromatography electrospray ionization tandem mass spectrometry analysis of the NPY family peptides. Aspects of quantification including sample preparation, the use of matrix-matched calibration curves, and internal standards will be discussed. This method for the simultaneous determination of NPY, PYY, and PP was accurate and reproducible but lacks the sensitivity required for measurement of their endogenous concentration in plasma. The advantages of mass spectrometric quantification will be discussed alongside the current obstacles and challenges.

Published

2012

38. Photocrosslinked poly(ester anhydride)s for peptide delivery: Effect of oligomer hydrophobicity on PYY3-36 delivery.

Author

Mönkäre J, Hakala RA, Kovalainen M, Korhonen H, Herzig KH, Seppälä JV, and Järvinen K

Subjects

Animals, Biological Availability, Delayed-Action Preparations, Drug Delivery Systems methods, Humans, Hydrophobic and Hydrophilic Interactions, Hypodermoclysis methods, Male, Peptide Fragments, Peptide YY pharmacokinetics, Powders administration & dosage, Powders chemistry, Powders pharmacokinetics, Rats, Rats, Wistar, Succinic Anhydrides chemistry, Peptide YY administration & dosage, Peptide YY chemistry, Polymers administration & dosage, Polymers chemistry

Abstract

The treatment for many diseases can be improved by developing more efficient peptide delivery technologies, for example, biodegradable polymers. In this work, photocrosslinked poly(ester anhydride)s based on functionalized poly(ε-caprolactone) oligomers were investigated for their abilities to achieve controlled peptide delivery. The effect of oligomer hydrophobicity on erosion and peptide release from poly(ester anhydride)s was evaluated by developing a sustained subcutaneous delivery system for an antiobesity drug candidate, peptide YY3-36 (PYY3-36). Oligomer hydrophobicity was modified with alkenylsuccinic anhydrides containing a 12-carbon alkenyl chain. PYY3-36 was mixed as a solid powder with methacrylated poly(ester anhydride) precursors, and this mixture was photocrosslinked at room temperature to form an implant for subcutaneous administration in rats. The oligomer hydrophobicity controlled the polymer erosion and PYY3-36 release as the increased hydrophobicity via the alkenyl chain prolonged polymer erosion in vitro and sustained in vivo release of PYY3-36. In addition, photocrosslinked poly(ester anhydride)s increased the bioavailability of PYY3-36 by up to 20-fold in comparison with subcutaneous administration of solution, evidence of remarkably improved delivery. In conclusion, this work demonstrates the suitability of photocrosslinked poly(ester anhydride)s for use in peptide delivery., (Copyright © 2011 Elsevier B.V. All rights reserved.)

Published

2012

39. Oral delivery of the appetite suppressing peptide hPYY(3-36) through the vitamin B12 uptake pathway.

Author

Fazen CH, Valentin D, Fairchild TJ, and Doyle RP

Subjects

Administration, Oral, Animals, Appetite Depressants chemistry, Appetite Depressants pharmacokinetics, Humans, Peptide Fragments, Peptide YY blood, Peptide YY chemistry, Rats, Rats, Sprague-Dawley, Signal Transduction, Vitamin B 12 blood, Vitamin B 12 chemistry, Appetite Depressants administration & dosage, Peptide YY administration & dosage, Vitamin B 12 administration & dosage

Abstract

hPYY(3-36) injections have shown positive effects on appetite regulations, sparking increased interest in hPYY(3-36) research. Of great interest is oral delivery of hPYY(3-36) that can achieve clinically relevant weight-loss outcomes in what would be a highly patient compliant route. Successful oral delivery of other peptides utilizing the vitamin B12 pathway has been shown but below clinically relevant levels. Herein, we present clinically relevant in vivo oral delivery of B12-hPYY(3-36) conjugates.

Published

2011

40. Neuropeptide Y/peptide YY receptor Y2 duplicate in zebrafish with unique introns displays distinct peptide binding properties.

Author

Fällmar H, Sundström G, Lundell I, Mohell N, and Larhammar D

Subjects

Amino Acid Sequence, Animals, Binding Sites, Cell Culture Techniques, HEK293 Cells metabolism, Humans, Introns, Molecular Sequence Data, Neuropeptide Y chemistry, Neuropeptide Y metabolism, Oryzias, Peptide YY chemistry, Peptide YY metabolism, Receptors, Gastrointestinal Hormone chemistry, Receptors, Neuropeptide Y chemistry, Receptors, Neuropeptide Y genetics, Sequence Alignment, Biological Evolution, Gene Duplication genetics, Receptors, Gastrointestinal Hormone metabolism, Receptors, Neuropeptide Y metabolism, Zebrafish metabolism

Abstract

The neuropeptide Y-family peptides and receptors are involved in a broad range of functions including appetite regulation. Both the peptide genes and the receptor genes are known to have duplicated in early vertebrate evolution. The ancestral jawed vertebrate had 7 NPY receptors but the number varies between 4 and 7 in extant vertebrates. Herein we describe the identification of an additional NPY receptor in two fish species, zebrafish and medaka. They cluster together with the Y2 receptors in phylogenetic analyses and seem to be orthologous to each other that is why we have named them Y2-2. Their genes differ from Y2 in having introns in the coding region. Binding studies with zebrafish Y2-2 receptors show that the three endogenous peptides NPY, PYYa and PYYb have similar affinities, 0.15-0.66 nM. This is in contrast to the Y2 receptor where they differed considerably from one another. N-terminally truncated NPY binds poorly and the Y2 antagonist BIIE0246 binds well to Y2-2, results that are reversed in comparison to Y2. Zebrafish Y2-2 mRNA was detected by PCR in the intestine and the eye, but not in the brain. In conclusion, we have found a novel Y2-like NPY/PYY receptor that probably arose in early teleost fish evolution., (Copyright © 2011 Elsevier Inc. All rights reserved.)

Published

2011

41. A role for metalloendopeptidases in the breakdown of the gut hormone, PYY 3-36.

Author

Addison ML, Minnion JS, Shillito JC, Suzuki K, Tan TM, Field BC, Germain-Zito N, Becker-Pauly C, Ghatei MA, Bloom SR, and Murphy KG

Subjects

Animals, Anti-Obesity Agents, Enzyme Inhibitors pharmacology, Gastrointestinal Hormones metabolism, Half-Life, Kidney metabolism, Mice, Peptide YY antagonists & inhibitors, Peptide YY blood, Peptide YY chemistry, Protein Stability drug effects, Tiopronin pharmacology, Metalloendopeptidases metabolism, Peptide YY metabolism

Abstract

Peptide YY(3-36) (PYY(3-36)) is a gut hormone that acts on Y2 receptors to reduce appetite. Obese humans are sensitive to the anorectic effects of PYY(3-36) and display a blunted postprandial rise in PYY(3-36). Bariatric surgery results in increased circulating PYY-immunoreactivity, which appears to play a role in postoperative weight loss. The utility of PYY(3-36) as an antiobesity treatment is limited by its short circulating half-life. Insight into the mechanisms by which PYY(3-36) is degraded may aid design of long-acting PYY(3-36) analogues or enzyme inhibitor therapies. We aimed to investigate the role of metalloendopeptidases in PYY(3-36) degradation and determine whether modulation of these enzymes enhanced PYY(3-36) plasma levels and bioactivity in vivo. Degradation and resultant cleavage products of PYY(3-36) were characterized after incubation with neprilysin and meprin β and with a kidney brush border preparation in vitro. Specific metalloendopeptidase inhibitors were coadministered with PYY(3-36) to mice and subsequent PYY(3-36) plasma levels and bioactivity determined. Meprin β cleaves PYY(3-36) at multiple conserved acidic sites. Blocking the actions of meprin β prevents the degradative effect of kidney brush borders on PYY(3-36). In mice, pretreatment with actinonin significantly prolonged the anorectic effect of PYY(3-36) and maintained higher PYY(3-36) plasma levels than treatment with PYY(3-36) alone. These studies suggest that inhibiting the degradation of PYY(3-36) using specific inhibitor therapies and/or the design of analogues resistant to cleavage by meprins may be useful to antiobesity therapeutics.

Published

2011

42. Structural dynamics of neuropeptide hPYY.

Author

Hegefeld WA, Kuczera K, and Jas GS

Subjects

Circular Dichroism, Humans, Molecular Dynamics Simulation, Protein Structure, Secondary, Protein Structure, Tertiary, Spectroscopy, Fourier Transform Infrared, Peptide YY chemistry

Abstract

We have employed a combination of experiment and simulation to characterize the ensemble of structures sampled by human Peptide YY (hPYY), an important member of the neuropeptide Y family. Experimental structural characterization carried out with far UV circular dichroism spectroscopy and Fourier Transform-Infrared measurements confirmed that the major feature of the secondary structure of hPYY is the α-helix, encompassing about half the peptide residues, with smaller contributions from turn and β-sheet like structures. The peptide undergoes thermal denaturation characterized by a melting temperature of 48°C with an enthalpy change of -24.5 kcal/mol and entropy change of -76.2 cal/(mol K). In our computational studies, based on a 4-μsec MD trajectory generated with the AMBER03 potential, we found excellent agreement of the predicted features with experimental data, including a stable C-terminal helix, a central turn and conservation of about 80% of measured long-range NOE contacts. The main structural fluctuations involved partial helix unwinding and large-scale motions of the N-terminal. Our joint experimental/computational approach leads to several insights into the biological function of PYY. We conclude that the C-terminal helix is crucial for the structural integrity of PYY. The structures and motions found in the simulations suggest microscopic explanations for observed changes in biological activity of the peptide upon mutation and truncation. We also performed microsecond-length MD and replica-exchange simulations of hPYY with the OPLS-AA force field, for which computed structures did not agree well with experimental data, predicting significant loss of helicity and NOE contacts., (Copyright © 2011 Wiley Periodicals, Inc., a Wiley company.)

Published

2011

43. Effects of glycine-extended and serine13-phosphorylated forms of peptide YY on food intake in rats.

Author

Reidelberger R, Haver A, Chelikani P, Keire DA, and Reeve JR Jr

Subjects

Animals, Peptide YY chemistry, Phosphorylation, Rats, Feeding Behavior drug effects, Glycine chemistry, Peptide YY pharmacology, Serine chemistry

Abstract

The gut hormone peptide YY(3-36)-amide [PYY(3-36)-NH(2)] is significantly more potent than PYY(1-36)-NH(2) in reducing food intake in rats and humans. Other Gly-extended and Ser(13)-phosphorylated PYY forms have been detected or predicted based upon known cellular processes of PYY synthesis and modification. Here we compared the effects of 3-h IV infusion of PYY(1-36)-NH(2), PYY(3-36)-NH(2), PYY(1-36)-Gly-OH, PYY(3-36)-Gly-OH, Ser(13)(PO(3))-PYY(1-36)-NH(2), Ser(13)(PO(3))-PYY(3-36)-NH(2), Ser(13)(PO(3))-PYY(1-36)-Gly-OH, and Ser(13)(PO(3))-PYY(3-36)-Gly-OH during the early dark period on food intake in freely feeding rats. PYY(3-36)-NH(2) and Ser(13)(PO(3))-PYY(3-36)-NH(2) reduced food intake similarly at 50 pmol/kg/min, while only PYY(3-36)-NH(2) reduced food intake at 15 pmol/kg/min. PYY(1-36)-NH(2) and Ser(13)(PO(3))-PYY(1-36)-NH(2) reduced food intake similarly at 50 and 150 pmol/kg/min. In contrast, PYY(1-36)-Gly-OH, PYY(3-36)-Gly-OH, Ser(13)(PO(3))-PYY(3-36)-Gly-OH, and Ser(13)(PO(3))-PYY(1-36)-Gly-OH had no effect on food intake at doses of 50 or 150 pmol/kg/min. Taken together, these results indicate that (i) PYY(3-36)-NH(2) is significantly more potent than PYY(1-36)-NH(2) in reducing food intake, (ii) Gly-extended forms of PYY are significantly less potent than non-extended forms, and (iii) Ser(13)-phosphorylation of PYY(3-36)-NH(2) decreases the anorexigenic potency PYY(3-36)-NH(2), but not PYY(1-36)-NH(2). Thus, PYY(3-36)-NH(2) appears to be the most potent PYY form for reducing food intake in rats., (Published by Elsevier Inc.)

Published

2011

44. Non-specific binding and general cross-reactivity of Y receptor agonists are correlated and should importantly depend on their acidic sectors.

Author

Parker MS, Sah R, Balasubramaniam A, Sallee FR, Zerbe O, and Parker SL

Subjects

Amino Acid Motifs physiology, Amino Acid Sequence, Animals, Binding Sites physiology, CHO Cells, Cell Membrane drug effects, Cell Membrane metabolism, Cerebral Cortex metabolism, Cricetinae, Cricetulus, Detergents pharmacology, Gastrointestinal Hormones metabolism, HEK293 Cells, Humans, Mice, Molecular Sequence Data, Neuropeptide Y chemistry, Neuropeptide Y metabolism, Neuropeptides chemistry, Pancreatic Polypeptide chemistry, Pancreatic Polypeptide metabolism, Peptide Fragments, Peptide Hormones chemistry, Peptide YY chemistry, Peptide YY metabolism, Perchlorates pharmacology, Protein Binding drug effects, Protein Binding physiology, Protein Structure, Secondary physiology, Rats, Sodium Compounds pharmacology, Sus scrofa, Transfection, Ultracentrifugation, Urea pharmacology, Neuropeptides metabolism, Peptide Hormones metabolism, Receptors, Neuropeptide Y agonists, Receptors, Neuropeptide Y metabolism

Abstract

Non-specific binding of Y receptor agonists to intact CHO cells, and to CHO cell or rat brain particulates, is much greater for human neuropeptide Y (hNPY) compared to porcine peptide Y (pPYY), and especially relative to human pancreatic polypeptide (hPP). This binding of hNPY is reduced by alkali cations in preference to non-ionic chaotrope urea, while the much lower non-specific binding of pPYY is more sensitive to urea. The difference could mainly be due to the 10-16 stretch in 36-residue Y agonists (residues 8-14 in N-terminally clipped 34-peptides), located in the sector that contains all acidic residues of physiological Y agonists. Anionic pairs containing aspartate in the 10-16 zone could be principally responsible for non-specific attachments, but may also aid the receptor site binding. Two such pairs are found in hNPY, one in pPYY, and none in hPP. The hydroxyl amino acid residue at position 13 in mammalian PYY and PP molecules could lower conformational plasticity and the non-selective binding via intrachain hydrogen bonding. The acidity of this tract could also be important in agonist selectivity of the Y receptor subtypes. The differences point to an evolutionary reduction of promiscuous protein binding from NPY to PP, and should also be important for Y agonist selectivity within NPY receptor group, and correlate with partial agonism and out-of group cross-reactivity with other receptors., (Copyright © 2010 Elsevier Inc. All rights reserved.)

Published

2011

45. Infrared study of the folding mechanism of a helical hairpin: porcine PYY.

Author

Waegele MM and Gai F

Subjects

Animals, Circular Dichroism, Hydrophobic and Hydrophilic Interactions, Kinetics, Peptide YY metabolism, Protein Folding, Protein Structure, Secondary, Sus scrofa, Temperature, Peptide YY chemistry

Abstract

The helical hairpin motif plays a key role as a receptor site in DNA binding and protein-protein interactions. Thus, various helical hairpins have recently been developed to assess the factors that control the DNA and/or protein binding affinities of this structural motif and to form synthetic templates for protein and drug design. In addition, several lines of evidence suggest that rapid acquisition of a helical hairpin structure from the unfolded ensemble may guide the rapid formation of helical proteins. Despite its importance as a crucial structural element in protein folding and binding, the folding mechanism of the helical hairpin motif has not been thoroughly studied. Herein, we investigate the structural determinants of the folding kinetics of a naturally occurring helical hairpin (porcine PYY) that is free of disulfide bonds and metal ion-induced cross-links using an infrared temperature-jump technique. It is found that mutations in the turn region predominantly increase the barrier of folding irrespective of the temperature, whereas the effect of mutations that perturb the hydrophobic interactions between the two helices is temperature-dependent. At low temperatures, deletion of hydrophobic side chains is found to predominantly affect the unfolding rate, while the opposite is observed at high temperatures. These results are interpreted in terms of a folding mechanism in which the turn is formed in the transition state and also based on the assumption that cross-strand hydrophobic contacts exist in the thermally unfolded state of PYY.

Published

2010

46. Effects of albumin-conjugated PYY on food intake: the respective roles of the circumventricular organs and vagus nerve.

Author

Baraboi ED, Michel C, Smith P, Thibaudeau K, Ferguson AV, and Richard D

Subjects

Animals, Appetite Regulation drug effects, Area Postrema drug effects, Area Postrema physiology, Blood Glucose drug effects, Body Weight drug effects, Brain physiology, Drinking drug effects, Eating drug effects, Humans, Insulin blood, Male, Neurons physiology, Peptide Fragments, Peptide YY chemistry, Rats, Rats, Wistar, Serum Albumin chemistry, Subfornical Organ drug effects, Vagotomy methods, Vagus Nerve physiology, Appetite Depressants pharmacology, Appetite Regulation physiology, Eating physiology, Peptide YY pharmacology, Serum Albumin pharmacology, Subfornical Organ physiology

Abstract

The mechanism and routes through which peptide tyrosine-tyrosine (PYY) exerts its anorectic effects are still largely unknown. In the present study, we investigated the roles of the area postrema (AP), subfornical organ (SFO) and vagus nerve in mediating the anorectic effect of PYY using PYY(3-36) conjugated to human serum albumin (PYY(3-36)-HSA) in rats. PYY(3-36)-HSA is a large molecule that does not penetrate the blood-brain barrier, and thus provides a useful tool to discriminate between the central (brain) and peripheral actions of this peptide. PYY(3-36)-HSA induced significant reductions in food and body weight gain up to 24 h after administration. The anorectic effect of PYY(3-36)-HSA was delayed for 2 h in rats in which both AP and SFO were ablated, while lesion of either of these circumventricular organs in isolation did not influence the feeding responses to PYY(3-36)-HSA. The PYY(3-36)-HSA-induced anorectic effect was also reduced during the 3- to 6-h period following subdiaphragmatic vagotomy. Lesions of AP, SFO and AP/SFO as well as subdiaphragmatic vagotomy blunted PYY(3-36)-HSA-induced expression of c-fos mRNA in specific brain structures including the bed nucleus of stria terminalis, central amygdala, lateral-external parabrachial nucleus and medial nucleus of the solitary tract. In addition, subdiaphragmatic vagotomy inhibited the neuronal activation induced by PYY(3-36)-HSA in AP and SFO. These findings suggest that the anorectic effect and brain neuronal activation induced by PYY(3-36)-HSA are dependent on integrity of AP, SFO and subdiaphragmatic vagus nerve., (© 2010 The Authors. European Journal of Neuroscience © 2010 Federation of European Neuroscience Societies and Blackwell Publishing Ltd.)

Published

2010

47. Mutagenesis of human neuropeptide Y/peptide YY receptor Y2 reveals additional differences to Y1 in interactions with highly conserved ligand positions.

Author

Akerberg H, Fällmar H, Sjödin P, Boukharta L, Gutiérrez-de-Terán H, Lundell I, Mohell N, and Larhammar D

Subjects

Arginine analogs & derivatives, Arginine pharmacology, Benzazepines pharmacology, Binding Sites, Humans, Ligands, Neuropeptide Y chemistry, Neuropeptide Y genetics, Peptide YY chemistry, Peptide YY genetics, Structure-Activity Relationship, Mutagenesis, Site-Directed, Neuropeptide Y metabolism, Peptide YY metabolism, Receptors, Neuropeptide Y genetics, Receptors, Neuropeptide Y metabolism

Abstract

Neuropeptide Y (NPY) and peptide YY (PYY) share approximately 70% of their 36 amino acids and bind to the same three human receptor subtypes, Y1, Y2 and Y5, even though these receptors only share approximately 30% sequence identity. Based on our previous investigation of human Y1 we describe here a mutagenesis study of three corresponding positions in human Y2, i.e. Tyr2.64, Val6.58 and Tyr7.31. Pharmacological characterization was performed with the four peptide agonists PYY, NPY, PYY(3-36) and NPY(13-36) as well as the non-peptide antagonist BIIE0246. Results from mutants where Tyr2.64 has been substituted by Ala suggest that Tyr2.64 is involved in the interaction with all investigated ligands whereas position Tyr7.31 seems to be more important for interaction with the truncated peptide PYY(3-36) than with intact NPY. Surprisingly, substitution of Tyr7.31 with His, the corresponding residue in Y1, resulted in total loss of binding of iodinated porcine PYY. The third position, Val6.58, did not influence binding of any of the ligands. These findings differ from those obtained for Y1 where Ala substitution resulted in lost or changed binding for each of the three positions. Although Tyr2.64 and Tyr7.31 in Y2 are involved in ligand binding, their interactions with the peptide ligands seem to be different from the corresponding positions in Y1. This suggests that the receptor-ligand interactions have changed during evolution after Y1 and Y2 arose from a common ancestral receptor., (Copyright (c) 2010 Elsevier B.V. All rights reserved.)

Published

2010

48. Application of arginine as an efficient eluent in cation exchange chromatographic purification of a PEGylated peptide.

Author

Annathur GV, Buckley JJ, Muthurania K, and Ramasubramanyan N

Subjects

Chromatography, Gel, Chromatography, High Pressure Liquid, Electrophoresis, Polyacrylamide Gel, Histidine chemistry, Humans, Light, Lysine chemistry, Particle Size, Peptide Fragments, Scattering, Radiation, Sodium Chloride chemistry, Urea chemistry, Arginine chemistry, Chromatography, Ion Exchange methods, Peptide YY chemistry, Peptide YY isolation & purification, Polyethylene Glycols chemistry

Abstract

A cation exchange chromatographic purification process step was developed for the purification of human PEGylated PYY 3-36 from the PEGylation reaction mixture. In this publication we describe experiments carried out to evaluate the chromatographic performance of arginine chloride as an effective cation exchange chromatography eluent. Using arginine we obtained improved recovery and resolution during chromatographic purification of a peptide PEGylation reaction mixture. The chromatographic elution performance of arginine was compared to other cationic amino acids and sodium chloride. Arginine provided higher yield and better resolution of product from other process impurities. The process was successfully scaled up to produce clinical supplies. The basis for improvement in process performance with arginine was characterized by examining the effect of buffer and concentration of the PEGylated peptide on hydrodynamic volume of the molecule in solution. These results were used to predict the behavior of the molecule in the chromatography process. The enhanced chromatographic performance could be attributed to changes in molecular size with concentration, higher eluent strength of arginine, and resulting changes in mass transfer resistance., (Copyright 2010 Elsevier B.V. All rights reserved.)

Published

2010

49. Peptide architecture: adding an alpha-helix to the PYY lysine side chain provides nanomolar binding and body-weight-lowering effects.

Author

Pedersen SL, Sasikumar PG, Vrang N, and Jensen KJ

Subjects

Amino Acid Sequence, Animals, Anti-Obesity Agents chemical synthesis, Anti-Obesity Agents pharmacology, Cell Line, Circular Dichroism, Humans, Male, Mice, Molecular Sequence Data, Peptide YY metabolism, Peptides chemical synthesis, Peptides pharmacology, Protein Binding, Protein Structure, Secondary, Structure-Activity Relationship, Weight Loss, Anti-Obesity Agents chemistry, Peptide YY chemistry, Peptides chemistry

Abstract

The gut hormone PYY3-36 influences food intake and body weight via interaction with hypothalamic presynaptic Y2 receptors (Y2R). Novel Y2R-selective analogues of PYY3-36 are therefore potential drug candidates for the treatment of obesity. It has been hypothesized that PYY3-36 and possibly also the related PP-fold peptides, NPY and PP, bind to the membrane via their amphipathic alpha-helix prior to receptor interaction. The PYY3-36 amphipathic alpha-helix causes the peptide to associate with the membrane, making it essential for Y receptor potency as it potentially guides the C-terminal pentapeptide into the correct conformation for receptor activation. Based on this hypothesis, the importance of the amphipathic nature of PYY3-36, as well as the ability of amphipathic alpha-helices to interact in solution to form di- and tetramers, we redesigned the peptide architecture by addition of an amphipathic alpha-helix via the Lys 4 side chain of PYY3-36. Two different amphipathic sequences were introduced; first, PYY17-31, the native alpha-helix of PYY, and secondly, its retro counterpart, PYY31-17, which is also predicted to form an alpha-helix. Moreover, several different turn motifs between the branching point and the additional alpha-helix were tested. Several novel peptides with nanomolar Y2R binding affinities, as well as increased Y receptor selectivity, were identified. CD experiments showed the modifications to be well accepted, and an increase in mean ellipticity (ME) signifying an increased degree of alpha-helicity was observed. Receptor binding experiments indicated that the direction of the additional alpha-helix is less important, in contrast to the turn motifs, which greatly affect the Y1R binding and thus determine the Y1R activity. Conversely, the structure-activity relationships from in vivo data showed that the peptide containing the retro-sequence was inactive, even though the binding data demonstrated high affinity and selectivity. This demonstrates that radical redesign of peptide architecture can provide nanomolar binding with improved subtype selectivity and with in vivo efficacy.

Published

2010

50. Molecular characterization, appetite regulatory effects and feeding related changes of peptide YY in goldfish.

Author

Gonzalez R and Unniappan S

Subjects

Amino Acid Sequence, Animals, Base Sequence, Brain Chemistry, Eating drug effects, Fasting physiology, Food, Gastrointestinal Tract chemistry, Gene Expression Regulation physiology, Injections, Intraperitoneal, Injections, Intraventricular, Peptide YY administration & dosage, Peptide YY chemistry, RNA, Messenger analysis, Appetite Regulation physiology, Eating physiology, Goldfish physiology, Peptide YY genetics, Peptide YY physiology

Abstract

Peptide YY (PYY) is a 36 amino acid multifunctional gut-brain hormone in mammals. PYY has recently raised great interest as it was shown to reduce food intake and body weight of mammals. While PYY and its receptors have been sequenced from many non-mammalian vertebrates, its functional role, especially in the regulation of food intake in lower vertebrates remain unknown. In this study, we identified the gene organization of goldfish PYY (gfPYY) and found abundant expression of PYY mRNA in the brain and digestive tract of goldfish. A 2.5-fold increase at 3h post-feeding and a 1.5-fold decrease in fasted animals was observed of PYY mRNA expression in the brain, suggesting an anorectic role for PYY in goldfish. A single intraperitoneal injection of 10 ng/g body weight gfPYY(1-36) or an intracerebroventricular injection of 5 ng/g body weight gfPYY(1-36) caused a 27% or 30% reduction in food intake in goldfish, respectively. Overall, our results, for the first time provide molecular and functional evidence for anorectic actions of PYY in goldfish., ((c) 2009 Elsevier Inc. All rights reserved.)

Published

2010