Multivalent γ‐PGA‐Exendin‐4 Conjugates to Target Pancreatic β‐Cells

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Abstract: Targeting of glucagon‐like peptide 1 receptor (GLP‐1R), expressed on the surface of pancreatic β‐cells, is of great interest for the development of advanced therapies for diabetes and diagnostics for insulinoma. We report the conjugation of exendin‐4 (Ex‐4), an approved drug to treat type 2 diabetes, to poly‐γ‐glutamic acid (γ‐PGA) to obtain more stable and effective GLP‐1R ligands. Exendin‐4 modified at Lysine‐27 with PEG4‐maleimide was conjugated to γ‐PGA functionalized with furan, in different molar ratios, exploiting a chemoselective Diels‐Alder cycloaddition. The γ‐PGA presenting the highest number of conjugated Ex‐4 molecules (average 120 per polymeric chain) showed a double affinity towards GLP‐1R with respect to exendin per se, paving the way to improved therapeutic and diagnostic applications.

Standort
Deutsche Nationalbibliothek Frankfurt am Main
Umfang
Online-Ressource
Sprache
Englisch

Erschienen in
Multivalent γ‐PGA‐Exendin‐4 Conjugates to Target Pancreatic β‐Cells ; day:13 ; month:07 ; year:2022 ; extent:1
ChemBioChem ; (13.07.2022) (gesamt 1)

Urheber
Rossi, Lorenzo
Kerekes, Krisztina
Kovács‐Kocsi, Judit
Körhegyi, Zoltán
Bodnár, Magdolna
Fazekas, Erika
Prépost, Eszter
Pignatelli, Cataldo
Caneva, Enrico
Nicotra, Francesco
Russo, Laura

DOI
10.1002/cbic.202200196
URN
urn:nbn:de:101:1-2022071315170113858742
Rechteinformation
Open Access; Der Zugriff auf das Objekt ist unbeschränkt möglich.
Letzte Aktualisierung
15.08.2025, 07:34 MESZ

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Beteiligte

  • Rossi, Lorenzo
  • Kerekes, Krisztina
  • Kovács‐Kocsi, Judit
  • Körhegyi, Zoltán
  • Bodnár, Magdolna
  • Fazekas, Erika
  • Prépost, Eszter
  • Pignatelli, Cataldo
  • Caneva, Enrico
  • Nicotra, Francesco
  • Russo, Laura

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