Subcutaneous Administration of a Zwitterionic Chitosan‐Based Hydrogel for Controlled Spatiotemporal Release of Monoclonal Antibodies-Reference-Cited by-同舟云学术

Subcutaneous Administration of a Zwitterionic Chitosan‐Based Hydrogel for Controlled Spatiotemporal Release of Monoclonal Antibodies

Published:2023-12-17 Issue: Volume: Page:
ISSN:0935-9648
Container-title:Advanced Materials
language:en
Short-container-title:Advanced Materials

Author:

Gréa Thomas¹²,Jacquot Guillaume³⁴⁵,Durand Arthur¹⁶,Mathieu Clélia³⁵,Gasser Adeline³⁵,Zhu Chen³⁵⁷,Banerjee Mainak³⁵⁷,Hucteau Elyse³⁸,Mallard Joris³⁸,Lopez Navarro Pedro³⁵,Popescu Bogdan V.³⁵,Thomas Eloise⁹,Kryza David⁹¹⁰,Sidi‐Boumedine Jacqueline⁹¹⁰,Ferrauto Giuseppe¹¹,Gianolio Eliana¹¹,Fleith Guillaume¹²,Combet Jérôme¹²,Brun Susana¹³,Erb Stéphane⁵¹⁴¹⁵,Cianferani Sarah⁵¹⁴¹⁵,Charbonnière Loïc J.⁷^ORCID,Fellmann Lyne¹⁶,Mirjolet Céline¹⁷¹⁸,David Laurent²,Tillement Olivier¹,Lux François¹¹⁹,Harlepp Sébastien³⁵,Pivot Xavier³⁵^ORCID,Detappe Alexandre³⁵⁷^ORCID

Affiliation:

1. Institut Lumière Matière UMR 5306 Université Claude Bernard Lyon1‐CNRS University of Lyon Villeurbanne Cedex 69622 France

2. Université Claude Bernard Lyon 1 INSA Lyon Jean Monnet University CNRS, UMR 5223 Ingénierie des Matériaux Polymères (IMP) Villeurbanne Cedex 69622 France

3. Institute of Cancerology Strasbourg Europe (ICANS) Strasbourg 67000 France

4. Nano‐H St Quentin Fallavier 38070 France

5. Strasbourg Drug Discovery and Development Institute (IMS) Strasbourg 67000 France

6. MexBrain 13 avenue Albert Einstein Villeurbanne 69100 France

7. Equipe de Synthèse Pour l'Analyse Institut Pluridisciplinaire Hubert Curien (IPHC) UMR 7178 CNRS/University of Strasbourg Strasbourg Cedex 2 67087 France

8. Biomedicine Research Centre of Strasbourg (CRBS) Mitochondria, oxidative stress and muscular protection laboratory (UR 3072) Strasbourg 67000 France

9. LAGEPP University Claude Bernard Lyon 1 CNRS UMR 5007 Villeurbanne Cedex 69622 France

10. Imthernat Plateform Hospices Civils of Lyon Lyon 69002 France

11. Molecular Imaging Center Department of Molecular Biotechnology and Health Sciences University of Turin Turin 10124 Italy

12. Université de Strasbourg CNRS, Institut Charles Sadron (UPR 22) 23 rue du Loess, 67034 Strasbourg Cedex 2 BP 84047 France

13. Poly‐Dtech Strasbourg 67100 France

14. Laboratoire de Spectrométrie de Masse BioOrganique IPHC UMR 7178 University of Strasbourg CNRS Strasbourg 67087 France

15. Infrastructure Nationale de Protéomique ProFI – FR2048 Strasbourg 67087 France

16. SILABE Université of Strasbourg fort Foch Niederhausbergen 67207 France

17. Radiation Oncology Department Preclinical Radiation Therapy and Radiobiology Unit Centre Georges‐François Leclerc Unicancer Dijon 21000 France

18. TIReCS team INSERM UMR 1231 Dijon 21000 France

19. University Institute of France (IUF) Paris 75231 France

Abstract

AbstractSubcutaneous (SC) administration of monoclonal antibodies (mAbs) is a proven strategy for improving therapeutic outcomes and patient compliance. The current FDA‐/EMA‐approved enzymatic approach, utilizing recombinant human hyaluronidase (rHuPH20) to enhance mAbs SC delivery, involves degrading the extracellular matrix's hyaluronate to increase tissue permeability. However, this method lacks tunable release properties, requiring individual optimization for each mAb. Seeking alternatives, physical polysaccharide hydrogels emerge as promising candidates due to their tunable physicochemical and biodegradability features. Unfortunately, none have demonstrated simultaneous biocompatibility, biodegradability, and controlled release properties for large proteins (≥150 kDa) after SC delivery in clinical settings. Here, a novel two‐component hydrogel comprising chitosan and chitosan@DOTAGA is introduced that can be seamlessly mixed with sterile mAbs formulations initially designed for intravenous (IV) administration, repurposing them as novel tunable SC formulations. Validated in mice and nonhuman primates (NHPs) with various mAbs, including trastuzumab and rituximab, the hydrogel exhibited biodegradability and biocompatibility features. Pharmacokinetic studies in both species demonstrated tunable controlled release, surpassing the capabilities of rHuPH20, with comparable parameters to the rHuPH20+mAbs formulation. These findings signify the potential for rapid translation to human applications, opening avenues for the clinical development of this novel SC biosimilar formulation.

Funder

H2020 European Research Council

Agence Nationale de la Recherche

Publisher

Wiley

Subject

Mechanical Engineering,Mechanics of Materials,General Materials Science

Link

https://onlinelibrary.wiley.com/doi/pdf/10.1002/adma.202308738

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