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Literature DB >> 31418572

O-GlcNAc Engineering of GPCR Peptide-Agonists Improves Their Stability and in Vivo Activity.

Paul M Levine, Aaron T Balana, Emmanuel Sturchler¹, Cassandra Koole², Hiroshi Noda³, Barbara Zarzycka, Eileen J Daley³, Tin T Truong², Vsevolod Katritch⁴, Thomas J Gardella³, Denise Wootten², Patrick M Sexton², Patricia McDonald¹, Matthew R Pratt⁴.

Abstract

Peptide agonists of GPCRs and other receptors are powerful signaling molecules with high potential as biological tools and therapeutics, but they are typically plagued by instability and short half-lives in vivo. Nature uses protein glycosylation to increase the serum stability of secreted proteins. However, these extracellular modifications are complex and heterogeneous in structure, making them an impractical solution. In contrast, intracellular proteins are subjected to a simple version of glycosylation termed O-GlcNAc modification. In our studies of this modification, we found that O-GlcNAcylation inhibits proteolysis, and strikingly, this stabilization occurs despite large distances in primary sequence (10-15 amino acids) between the O-GlcNAc and the site of cleavage. We therefore hypothesized that this "remote stabilization" concept could be useful to engineer the stability and potentially additional properties of peptide or protein therapeutics. Here, we describe the application of O-GlcNAcylation to two clinically important peptides: glucagon-like peptide-1 (GLP-1) and the parathyroid hormone (PTH), which respectively help control glucose and calcium levels in the blood. For both peptides, we found O-GlcNAcylated analogs that are equipotent to unmodified peptide in cell-based activation assays, while several GLP-1 analogs were biased agonists relative to GLP-1. As we predicted, O-GlcNAcylation can improve the stability of both GLP-1 and PTH in serum despite the fact that the O-GlcNAc can be quite remote from characterized sites of peptide cleavage. The O-GlcNAcylated GLP-1 and PTH also displayed significantly improved in vivo activity. Finally, we employed structure-based molecular modeling and receptor mutagenesis to predict how O-GlcNAcylation can be accommodated by the receptors and the potential interactions that contribute to peptide activity. This approach demonstrates the potential of O-GlcNAcylation for generating analogs of therapeutic peptides with enhanced proteolytic stability.

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Year: 2019 PMID： 31418572 PMCID： PMC6860926 DOI： 10.1021/jacs.9b05365

Source DB: PubMed Journal: J Am Chem Soc ISSN： 0002-7863 Impact factor: 15.419

37 in total

1. Serum stability of peptides.

Authors: Håvard Jenssen; Stein Ivar Aspmo
Journal: Methods Mol Biol Date: 2008

Review 2. Pursuit of a perfect insulin.

Authors: Alexander N Zaykov; John P Mayer; Richard D DiMarchi
Journal: Nat Rev Drug Discov Date: 2016-03-18 Impact factor: 84.694

3. Phase-plate cryo-EM structure of a biased agonist-bound human GLP-1 receptor-Gs complex.

Authors: Yi-Lynn Liang; Maryam Khoshouei; Alisa Glukhova; Sebastian G B Furness; Peishen Zhao; Lachlan Clydesdale; Cassandra Koole; Tin T Truong; David M Thal; Saifei Lei; Mazdak Radjainia; Radostin Danev; Wolfgang Baumeister; Ming-Wei Wang; Laurence J Miller; Arthur Christopoulos; Patrick M Sexton; Denise Wootten
Journal: Nature Date: 2018-02-21 Impact factor: 49.962

4. Dipeptidyl peptidase IV resistant analogues of glucagon-like peptide-1 which have extended metabolic stability and improved biological activity.

Authors: C F Deacon; L B Knudsen; K Madsen; F C Wiberg; O Jacobsen; J J Holst
Journal: Diabetologia Date: 1998-03 Impact factor: 10.122

Review 5. PTH receptor-1 signalling-mechanistic insights and therapeutic prospects.

Authors: Ross W Cheloha; Samuel H Gellman; Jean-Pierre Vilardaga; Thomas J Gardella
Journal: Nat Rev Endocrinol Date: 2015-08-25 Impact factor: 43.330

6. N-terminal His(7)-modification of glucagon-like peptide-1(7-36) amide generates dipeptidyl peptidase IV-stable analogues with potent antihyperglycaemic activity.

Authors: B D Green; M H Mooney; V A Gault; N Irwin; C J Bailey; P Harriott; B Greer; F P M O'Harte; P R Flatt
Journal: J Endocrinol Date: 2004-03 Impact factor: 4.286

7. Comparison of the pharmacokinetics of parenteral parathyroid hormone-(1-34) [PTH-(1-34)] and PTH-related peptide-(1-34) in healthy young humans.

Authors: L J Fraher; K Klein; R Marier; D Freeman; G N Hendy; D Goltzman; A B Hodsman
Journal: J Clin Endocrinol Metab Date: 1995-01 Impact factor: 5.958

Review 8. Tools for GPCR drug discovery.

Authors: Ru Zhang; Xin Xie
Journal: Acta Pharmacol Sin Date: 2012-01-23 Impact factor: 6.150

9. Autocrine selection of a GLP-1R G-protein biased agonist with potent antidiabetic effects.

Authors: Hongkai Zhang; Emmanuel Sturchler; Jiang Zhu; Ainhoa Nieto; Philip A Cistrone; Jia Xie; LinLing He; Kyungmoo Yea; Teresa Jones; Rachel Turn; Peter S Di Stefano; Patrick R Griffin; Philip E Dawson; Patricia H McDonald; Richard A Lerner
Journal: Nat Commun Date: 2015-12-01 Impact factor: 14.919

10. High-resolution crystal structure of parathyroid hormone 1 receptor in complex with a peptide agonist.

Authors: Janosch Ehrenmann; Jendrik Schöppe; Christoph Klenk; Mathieu Rappas; Lutz Kummer; Andrew S Doré; Andreas Plückthun
Journal: Nat Struct Mol Biol Date: 2018-11-19 Impact factor: 15.369

8 in total

1. Spatial and temporal proteomics reveals the distinct distributions and dynamics of O-GlcNAcylated proteins.

Authors: Senhan Xu; Ming Tong; Suttipong Suttapitugsakul; Ronghu Wu
Journal: Cell Rep Date: 2022-06-14 Impact factor: 9.995

2. Generation of Potent and Stable GLP-1 Analogues Via "Serine Ligation".

Authors: Paul M Levine; Timothy W Craven; Xinting Li; Aaron T Balana; Gregory H Bird; Marina Godes; Patrick J Salveson; Patrick W Erickson; Mila Lamb; Maggie Ahlrichs; Michael Murphy; Cassandra Ogohara; Meerit Y Said; Loren D Walensky; Matthew R Pratt; David Baker
Journal: ACS Chem Biol Date: 2022-03-23 Impact factor: 4.634

O-GlcNAc Engineering of GPCR Peptide-Agonists Improves Their Stability and in Vivo Activity.

1. Serum stability of peptides.

Review 2. Pursuit of a perfect insulin.

3. Phase-plate cryo-EM structure of a biased agonist-bound human GLP-1 receptor-Gs complex.

4. Dipeptidyl peptidase IV resistant analogues of glucagon-like peptide-1 which have extended metabolic stability and improved biological activity.

Review 5. PTH receptor-1 signalling-mechanistic insights and therapeutic prospects.

6. N-terminal His(7)-modification of glucagon-like peptide-1(7-36) amide generates dipeptidyl peptidase IV-stable analogues with potent antihyperglycaemic activity.

7. Comparison of the pharmacokinetics of parenteral parathyroid hormone-(1-34) [PTH-(1-34)] and PTH-related peptide-(1-34) in healthy young humans.

Review 8. Tools for GPCR drug discovery.

9. Autocrine selection of a GLP-1R G-protein biased agonist with potent antidiabetic effects.

10. High-resolution crystal structure of parathyroid hormone 1 receptor in complex with a peptide agonist.

1. Spatial and temporal proteomics reveals the distinct distributions and dynamics of O-GlcNAcylated proteins.

2. Generation of Potent and Stable GLP-1 Analogues Via "Serine Ligation".

Review 3. Molecular Interrogation to Crack the Case of O-GlcNAc.

Review 4. O-GlcNAcylated peptides and proteins for structural and functional studies.

5. The activity of sulfono-γ-AApeptide helical foldamers that mimic GLP-1.

6. PTHG2 Reduces Bone Loss in Ovariectomized Mice by Directing Bone Marrow Mesenchymal Stem Cell Fate.

Review 7. Helical sulfono-γ-AApeptides with predictable functions in protein recognition.

Review 8. The therapeutic potential of GLP-1 receptor biased agonism.