Your search keyword '"Muttenthaler, Markus"' showing total 14 results

1. Improving the Gastrointestinal Stability of Linaclotide.

Author

Braga Emidio N, Tran HNT, Andersson A, Dawson PE, Albericio F, Vetter I, and Muttenthaler M

Subjects

Cell Line, Drug Design, Drug Stability, Gastrointestinal Agents chemical synthesis, Guanylyl Cyclase C Agonists chemical synthesis, Humans, Peptides chemical synthesis, Proteolysis, Gastrointestinal Agents metabolism, Guanylyl Cyclase C Agonists metabolism, Peptides metabolism

Abstract

High susceptibility to proteolytic degradation in the gastrointestinal tract limits the therapeutic application of peptide drugs in gastrointestinal disorders. Linaclotide is an orally administered peptide drug for the treatment of irritable bowel syndrome with constipation (IBS-C) and abdominal pain. Linaclotide is however degraded in the intestinal environment within 1 h, and improvements in gastrointestinal stability might enhance its therapeutic application. We therefore designed and synthesized a series of linaclotide analogues employing a variety of strategic modifications and evaluated their gastrointestinal stability and pharmacological activity at its target receptor guanylate cyclase-C. All analogues had substantial improvements in gastrointestinal half-lives (>8 h vs linaclotide 48 min), and most remained active at low nanomolar concentrations. This work highlights strategic approaches for the development of gut-stable peptides toward the next generation of orally administered peptide drugs for the treatment of gastrointestinal disorders.

Published

2021

2. Trends in peptide drug discovery.

Author

Muttenthaler M, King GF, Adams DJ, and Alewood PF

Subjects

Animals, Chemistry, Pharmaceutical methods, Drug Design, Humans, Peptide Library, Drug Development, Drug Discovery, Peptides pharmacology

Abstract

Since the introduction of insulin almost a century ago, more than 80 peptide drugs have reached the market for a wide range of diseases, including diabetes, cancer, osteoporosis, multiple sclerosis, HIV infection and chronic pain. In this Perspective, we summarize key trends in peptide drug discovery and development, covering the early efforts focused on human hormones, elegant medicinal chemistry and rational design strategies, peptide drugs derived from nature, and major breakthroughs in molecular biology and peptide chemistry that continue to advance the field. We emphasize lessons from earlier approaches that are still relevant today as well as emerging strategies such as integrated venomics and peptide-display libraries that create new avenues for peptide drug discovery. We also discuss the pharmaceutical landscape in which peptide drugs could be particularly valuable and analyse the challenges that need to be addressed for them to reach their full potential.

Published

2021

3. Neuropeptide signalling systems - An underexplored target for venom drug discovery.

Author

Mendel HC, Kaas Q, and Muttenthaler M

Subjects

Animals, Heart Failure metabolism, Humans, Ligands, Neuropeptides chemistry, Obesity metabolism, Peptides chemistry, Venoms chemistry, Venoms metabolism, Drug Discovery methods, Neuropeptides metabolism, Peptides metabolism, Signal Transduction

Abstract

Neuropeptides are signalling molecules mainly secreted from neurons that act as neurotransmitters or peptide hormones to affect physiological processes and modulate behaviours. In humans, neuropeptides are implicated in numerous diseases and understanding their role in physiological processes and pathologies is important for therapeutic development. Teasing apart the (patho)physiology of neuropeptides remains difficult due to ligand and receptor promiscuity and the complexity of the signalling pathways. The current approach relies on a pharmacological toolbox of agonists and antagonists displaying high selectivity for independent receptor subtypes, with the caveat that only few selective ligands have been discovered or developed. Animal venoms represent an underexplored source for novel receptor subtype-selective ligands that could aid in dissecting human neuropeptide signalling systems. Multiple endogenous-like neuropeptides as well as peptides acting on neuropeptide receptors are present in venoms. In this review, we summarise current knowledge on neuropeptides and discuss venoms as a source for ligands targeting neuropeptide signalling systems., (Copyright © 2020 Elsevier Inc. All rights reserved.)

Published

2020

4. Anhydrous Hydrogen Fluoride Cleavage in Boc Solid Phase Peptide Synthesis.

Author

Jadhav KB, Woolcock KJ, and Muttenthaler M

Subjects

Peptides chemistry, Hydrofluoric Acid chemistry, Peptides chemical synthesis, Solid-Phase Synthesis Techniques methods

Abstract

Solid phase peptide synthesis using tert-butyloxycarbonyl/benzyl chemistry (Boc-SPPS) is important for producing peptides for fundamental research as well as for clinical use. During Boc-SPPS, liquid anhydrous hydrogen fluoride (HF) is used to remove the side chain protecting groups of the assembled peptide and to release it from the resin. Here, we provide a detailed protocol for "HF cleavage," aiming to improve accessibility and the use of this valuable and well-validated technique.

Published

2020

5. Methods, setup and safe handling for anhydrous hydrogen fluoride cleavage in Boc solid-phase peptide synthesis.

Author

Muttenthaler M, Albericio F, and Dawson PE

Subjects

Humans, Peptides chemistry, Safety Management, Solid-Phase Synthesis Techniques instrumentation, Hydrofluoric Acid chemistry, Hydrofluoric Acid toxicity, Peptides chemical synthesis, Solid-Phase Synthesis Techniques methods

Abstract

Solid-phase peptide synthesis (SPPS) using tert-butyloxycarbonyl (Boc)/benzyl (Bzl) chemistry is an indispensable technique in many laboratories around the globe, and it provides peptides to the pharmaceutical industry and to thousands of scientists working in basic research. The Boc/Bzl strategy has several advantages, including reliability in the synthesis of long and difficult polypeptides, alternative orthogonality regarding protecting groups and ease of producing C-terminal thioesters for native chemical ligation applications. In this process, anhydrous hydrogen fluoride (HF) is used to remove the side chain protecting groups of the assembled peptide and to release the peptide from the resin, a process typically described as 'HF cleavage'. This protocol describes the general methodology, apparatus setup and safe handling of HF, with the aim of providing comprehensive information on the safe use of this valuable, well-studied and validated cleavage technique. We explain the cleavage mechanism, the physicochemical properties and risks of HF, first aid measures and the correct use of the apparatus. In addition, we provide advice on scavenger selection, as well as a troubleshooting section and video material illustrating key steps of the procedure. The protocol comprises precleavage sample preparation (30 min-2.5 h), complete HF cleavage procedure (2 h) and reaction workup (30 min).

Published

2015

6. Evaluation of diverse peptidyl motifs for cellular delivery of semiconductor quantum dots.

Author

Gemmill KB, Muttenthaler M, Delehanty JB, Stewart MH, Susumu K, Dawson PE, and Medintz IL

Subjects

Animals, Biological Transport, COS Cells, Cell Survival, Chlorocebus aethiops, Drug Delivery Systems instrumentation, Endosomes metabolism, Humans, Peptides genetics, Quantum Dots, Semiconductors, Cells metabolism, Drug Delivery Systems methods, Nanoparticles chemistry, Peptides chemistry, Peptides metabolism

Abstract

Cell-penetrating peptides (CPPs) have rapidly become a mainstay technology for facilitating the delivery of a wide variety of nanomaterials to cells and tissues. Currently, the library of CPPs to choose from is still limited, with the HIV TAT-derived motif still being the most used. Among the many materials routinely delivered by CPPs, nanoparticles are of particular interest for a plethora of labeling, imaging, sensing, diagnostic, and therapeutic applications. The development of nanoparticle-based technologies for many of these uses will require access to a much larger number of functional peptide motifs that can both facilitate cellular delivery of different types of nanoparticles to cells and be used interchangeably in the presence of other peptides and proteins on the same surface. Here, we evaluate the utility of four peptidyl motifs for their ability to facilitate delivery of luminescent semiconductor quantum dots (QDs) in a model cell culture system. We find that an LAH4 motif, derived from a membrane-inserting antimicrobial peptide, and a chimeric sequence that combines a sweet arrow peptide with a portion originating from the superoxide dismutase enzyme provide effective cellular delivery of QDs. Interestingly, a derivative of the latter sequence lacking just a methyl group was found to be quite inefficient, suggesting that even small changes can have significant functional outcomes. Delivery was effected using 1 h incubation with cells, and fluorescent counterstaining strongly suggests an endosomal uptake process that requires a critical minimum number or ratio of peptides to be displayed on the QD surface. Concomitant cytoviability testing showed that the QD-peptide conjugates are minimally cytotoxic in the model COS-1 cell line tested. Potential applications of these peptides in the context of cellular delivery of nanoparticles and a variety of other (bio)molecules are discussed.

Published

2013

7. Exploring bioactive peptides from natural sources for oxytocin and vasopressin drug discovery.

Author

Gruber CW, Koehbach J, and Muttenthaler M

Subjects

Amino Acid Sequence, Animals, Humans, Oxytocin metabolism, Vasopressins metabolism, Drug Discovery, Oxytocin chemistry, Oxytocin pharmacology, Peptides chemistry, Peptides pharmacology, Vasopressins chemistry, Vasopressins pharmacology

Published

2012

8. Ligand-based peptide design and combinatorial peptide libraries to target G protein-coupled receptors.

Author

Gruber CW, Muttenthaler M, and Freissmuth M

Subjects

Animals, Binding Sites drug effects, Humans, Models, Biological, Models, Molecular, Protein Binding, Signal Transduction drug effects, Combinatorial Chemistry Techniques, Drug Delivery Systems methods, Drug Design, Ligands, Peptide Library, Peptides pharmacology, Receptors, G-Protein-Coupled drug effects

Abstract

G protein-coupled receptors (GPCRs) are considered to represent the most promising drug targets; it has been repeatedly said that a large fraction of the currently marketed drugs elicit their actions by binding to GPCRs (with cited numbers varying from 30-50%). Closer scrutiny, however, shows that only a modest fraction of (≈60) GPCRs are, in fact, exploited as drug targets, only ≈20 of which are peptide-binding receptors. The vast majority of receptors in the humane genome have not yet been explored as sites of action for drugs. Given the drugability of this receptor class, it appears that opportunities for drug discovery abound. In addition, GPCRs provide for binding sites other than the ligand binding sites (referred to as the "orthosteric site"). These additional sites include (i) binding sites for ligands (referred to as "allosteric ligands") that modulate the affinity and efficacy of orthosteric ligands, (ii) the interaction surface that recruits G proteins and arrestins, (iii) the interaction sites of additional proteins (GIPs, GPCR interacting proteins that regulate G protein signaling or give rise to G protein-independent signals). These sites can also be targeted by peptides. Combinatorial and natural peptide libraries are therefore likely to play a major role in identifying new GPCR ligands at each of these sites. In particular the diverse natural peptide libraries such as the venom peptides from marine cone-snails and plant cyclotides have been established as a rich source of drug leads. High-throughput screening and combinatorial chemistry approaches allow for progressing from these starting points to potential drug candidates. This will be illustrated by focusing on the ligand-based drug design of oxytocin (OT) and vasopressin (AVP) receptor ligands using natural peptide leads as starting points.

Published

2010

9. Conopressin-T from Conus tulipa reveals an antagonist switch in vasopressin-like peptides.

Author

Dutertre S, Croker D, Daly NL, Andersson A, Muttenthaler M, Lumsden NG, Craik DJ, Alewood PF, Guillon G, and Lewis RJ

Subjects

Animals, CHO Cells, Cricetinae, Cricetulus, Humans, Inositol Phosphates chemistry, Models, Biological, Oxytocin chemistry, Oxytocin metabolism, Receptors, Oxytocin chemistry, Receptors, Vasopressin chemistry, Vasotocin chemistry, Conus Snail metabolism, Oxytocin analogs & derivatives, Peptides chemistry, Vasopressins chemistry

Abstract

We report the discovery of conopressin-T, a novel bioactive peptide isolated from Conus tulipa venom. Conopressin-T belongs to the vasopressin-like peptide family and displays high sequence homology to the mammalian hormone oxytocin (OT) and to vasotocin, the endogenous vasopressin analogue found in teleost fish, the cone snail's prey. Conopressin-T was found to act as a selective antagonist at the human V 1a receptor. All peptides in this family contain two conserved amino acids within the exocyclic tripeptide (Pro7 and Gly9), which are replaced with Leu7 and Val9 in conopressin-T. Whereas conopressin-T binds only to OT and V 1a receptors, an L7P analogue had increased affinity for the V 1a receptor and weak V2 receptor binding. Surprisingly, replacing Gly9 with Val9 in OT and vasopressin revealed that this position can function as an agonist/antagonist switch at the V 1a receptor. NMR structures of both conopressin-T and L7P analogue revealed a marked difference in the orientation of the exocyclic tripeptide that may serve as templates for the design of novel ligands with enhanced affinity for the V 1a receptor.

Published

2008

10. On the Utility of Chemical Strategies to Improve Peptide Gut Stability

Author

Kremsmayr, Thomas, Aljnabi, Aws, Blanco-Canosa, Juan B., Tran, Hue N. T., Emidio, Nayara Braga, Muttenthaler, Markus, and European Commission

Subjects

Scaffolds, Degradation, Chemical Strategies, Cyclization, Monomers, Drug Discovery, Molecular Medicine, Cyclotides, Peptides and proteins, Amino Acid Sequence, Peptides, Stability

Abstract

Inherent susceptibility of peptides to enzymatic degradation in the gastrointestinal tract is a key bottleneck in oral peptide drug development. Here, we present a systematic analysis of (i) the gut stability of disulfide-rich peptide scaffolds, orally administered peptide therapeutics, and well-known neuropeptides and (ii) medicinal chemistry strategies to improve peptide gut stability. Among a broad range of studied peptides, cyclotides were the only scaffold class to resist gastrointestinal degradation, even when grafted with non-native sequences. Backbone cyclization, a frequently applied strategy, failed to improve stability in intestinal fluid, but several site-specific alterations proved efficient. This work furthermore highlights the importance of standardized gut stability test conditions and suggests defined protocols to facilitate cross-study comparison. Together, our results provide a comparative overview and framework for the chemical engineering of gut-stable peptides, which should be valuable for the development of orally administered peptide therapeutics and molecular probes targeting receptors within the gastrointestinal tract., We thank Marina Kujundzic and Johanna Nemec for their help in collecting some of the stability data and peptide synthesis. We are grateful to the laboratory of Prof. David Craik (The University of Queensland) for providing Vc1.1 and cVc1.1. We thank Prof. Christian F.W. Becker (Institute of Biological Chemistry, University of Vienna) for his support of this work. We also thank Dr. Martin Zehl and the Mass Spectrometry Centre at the University of Vienna (a member of Vienna Life-Science Instruments) for assistance with HR-MS analysis. We are grateful to the NIMH PDSP (National Institute of Mental Health’s Psychoactive Drug Screening Program, Contract # HHSN-271-2018-00023-C), which is directed by Bryan L. Roth at the University of North Carolina at Chapel Hill and Project Officer Jamie Driscoll at NIMH, Bethesda MD, USA, for providing agonist functional activity data of OT variants. This research was supported by the European Research Council under the European Union’s Horizon 2020 research and innovation program (grant agreements no. 714366), by the Australian Research Council Discovery Project (DP190101667) and by the Vienna Science and Technology Fund (WWTF) through project LS18-053. T. Kremsmayr was supported by the Austrian Academy of Sciences through a DOC Fellowship (25139). J.B.B.-C. thanks the Spanish Ministry of Science and Innovation (RTI2018-096323-B-100).

Published

2022

11. Chemical strategies to tune potency, selectivity and stability of venom peptides.

Author

Muttenthaler, Markus

Subjects

*PEPTIDES

Published

2024

12. Expanding the versatility and scope of the oxime ligation: rapid bioconjugation to disulfide-rich peptides.

Author

Hering, Anke, Braga Emidio, Nayara, and Muttenthaler, Markus

Subjects

PEPTIDES, CONOTOXINS, DISULFIDES, PROTEINS

Abstract

The oxime ligation is a valuable bioorthogonal conjugation reaction but with limited compatibility with disulfide-rich peptides/proteins and time-sensitive applications. Here we overcome these limitations by introducing a strategy that supports regiospecific control, oxidative folding, production of stable aminooxy-precursors for on-demand modification, and complete ligation within 5 min. [ABSTRACT FROM AUTHOR]

Published

2022

13. Development of a human vasopressin V1a-receptor antagonist from an evolutionary-related insect neuropeptide

Author

Di Giglio, Maria Giulia, Muttenthaler, Markus, Harpsoe, Kasper, Liutkeviciute, Zita, Keov, Peter, Eder, Thomas, Rattei, Thomas, Arrowsmith, Sarah, Wray, Susan, Ales Marek, Elbert, Tomas, Alewood, Paul F., Gloriam, David E., and Gruber, Christian W.

Subjects

592 Invertebrates, 576 Genetics and evolution, Receptor pharmacology, Journal Article, Peptides, Entomology, hormones, hormone substitutes, and hormone antagonists

Abstract

Characterisation of G protein-coupled receptors (GPCR) relies on the availability of a toolbox of ligands that selectively modulate different functional states of the receptors. To uncover such molecules, we explored a unique strategy for ligand discovery that takes advantage of the evolutionary conservation of the 600-million-year-old oxytocin/vasopressin signalling system. We isolated the insect oxytocin/vasopressin orthologue inotocin from the black garden ant (Lasius niger), identified and cloned its cognate receptor and determined its pharmacological properties on the insect and human oxytocin/vasopressin receptors. Subsequently, we identified a functional dichotomy: inotocin activated the insect inotocin and the human vasopressin V1b receptors, but inhibited the human V1aR. Replacement of Arg8 of inotocin by D-Arg8 led to a potent, stable and competitive V1aR-antagonist ([D-Arg8]-inotocin) with a 3,000-fold binding selectivity for the human V1aR over the other three subtypes, OTR, V1bR and V2R. The Arg8/D-Arg8 ligand-pair was further investigated to gain novel insights into the oxytocin/vasopressin peptide-receptor interaction, which led to the identification of key residues of the receptors that are important for ligand functionality and selectivity. These observations could play an important role for development of oxytocin/vasopressin receptor modulators that would enable clear distinction of the physiological and pathological responses of the individual receptor subtypes.

Published

2017

14. Evaluation of Chemical Strategies for Improving the Stability and Oral Toxicity of Insecticidal Peptides.

Author

Herzig, Volker, de Araujo, Aline Dantas, Greenwood, Kathryn P., Chin, Yanni K.-Y., Windley, Monique J., Chong, Youmie, Muttenthaler, Markus, Mobli, Mehdi, Audsley, Neil, Nicholson, Graham M., Alewood, Paul F., and King, Glenn F.

Subjects

SPIDER venom, PEPTIDES, BIOLOGICAL insecticides, RING formation (Chemistry), BLOWFLIES

Abstract

Spider venoms are a rich source of insecticidal peptide toxins. Their development as bioinsecticides has, however, been hampered due to concerns about potential lack of stability and oral bioactivity. We therefore systematically evaluated several synthetic strategies to increase the stability and oral potency of the potent insecticidal spider-venom peptide ω-HXTX-Hv1a (Hv1a). Selective chemical replacement of disulfide bridges with diselenide bonds and N- to C-terminal cyclization were anticipated to improve Hv1a resistance to proteolytic digestion, and thereby its activity when delivered orally. We found that native Hv1a is orally active in blowflies, but 91-fold less potent than when administered by injection. Introduction of a single diselenide bond had no effect on the susceptibility to scrambling or the oral activity of Hv1a. N- to C-terminal cyclization of the peptide backbone did not significantly improve the potency of Hv1a when injected into blowflies and it led to a significant decrease in oral activity. We show that this is likely due to a dramatically reduced rate of translocation of cyclic Hv1a across the insect midgut, highlighting the importance of testing bioavailability in addition to toxin stability. [ABSTRACT FROM AUTHOR]

Published

2018