Engineered Platelet‐Derived Growth Factor‐Releasing Hydrogels Promote Fetal Membrane Healing In Vivo

Author:

Avilla‐Royo Eva12ORCID,Vonzun Ladina13ORCID,Seehusen Frauke4,Vallmajo‐Martin Queralt15ORCID,Famos Flurina1,Moser Lukas1ORCID,Gegenschatz‐Schmid Katharina1ORCID,Krattiger Lisa Amanda1ORCID,Strübing Nele13ORCID,Weisskopf Miriam6ORCID,Moehrlen Ueli378,Ochsenbein‐Kölble Nicole13ORCID,Ehrbar Martin1ORCID

Affiliation:

1. Department of Obstetrics University Hospital Zurich University of Zurich Schmelzbergstrasse 12 8091 Zurich Switzerland

2. Department of Health Sciences and Technology ETH Zurich Universitätstrasse 2 8092 Zurich Switzerland

3. The Zurich Center for Fetal Diagnosis and Therapy Frauenklinikstrasse 10 8091 Zurich Switzerland

4. Laboratory for Animal Model Pathology Institute of Veterinary Pathology University of Zurich Winterthurerstrasse 268 8057 Zurich Switzerland

5. Gene Expression Laboratory Salk Institute for Biological Studies 10010 N Torrey Pines Road La Jolla 92037 USA

6. Center for Surgical Research University Hospital Zurich University of Zurich Sternwartstrasse 14 8091 Zurich Switzerland

7. Department of Pediatric Surgery University Children's Hospital Zurich University of Zurich Steinwiesstrasse 75 8032 Zurich Switzerland

8. Children's Research Center University Children's Hospital Zurich University of Zurich Steinwiesstrasse 75 8032 Zurich Switzerland

Abstract

AbstractFetoscopic interventions to treat fetal anomalies are currently performed for a variety of conditions. Depending on the procedure, preterm rupture of the fetal membranes (FMs) happens in around 30% of the cases, potentially leading to preterm birth and fetal morbidity and mortality. Here, the capacity of modular transglutaminase crosslinked poly(ethylene glycol) (TG‐PEG) hydrogels that release platelet‐derived growth factor (PDGF)‐BB to promote FM healing is described. In vitro, such growth factor‐loaded hydrogels are able to stimulate amniotic cell migration and proliferation. When applied in vivo, these TG‐PEG hydrogels tightly seal the FM and uterus defects created by a fetoscope and remain stable for 10 days. The migration of healing‐related cells into such hydrogels in the myometrium, endometrium, and FM areas is only possible in soft TG‐PEG hydrogels. Importantly, bioengineered hydrogels releasing PDGF‐BB promote recruitment of host cells from the myometrium and the endometrium, and to a lesser extent from FM areas. In such hydrogels, the potent proliferation and matrix production of the recruited cells at the site of treatment into the biomaterial initiates a robust early healing response. PDGF‐BB‐loaded TG‐PEG hydrogels hold great promise for the treatment of fetoscopy‐induced FM defects and for the prevention of preterm birth.

Funder

UniversitätsSpital Zürich

Publisher

Wiley

Subject

Electrochemistry,Condensed Matter Physics,Biomaterials,Electronic, Optical and Magnetic Materials

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