Prenatal VEGF Nano-Delivery Reverses Congenital Diaphragmatic Hernia-Associated Pulmonary Abnormalities

Author:

Loukogeorgakis Stavros P.,Michielin Federica,Al-Juffali Noura,Jimenez Julio,Shibuya Soichi,Allen-Hyttinen Jessica,Eastwood Patrice,Alhendi Ahmed S.N.,Davidson Joseph,Naldi Eleonora,Maghsoudlou Panagiotis,Tedeschi Alfonso,Khalaf Sahira,Khabbush Aziza,Plate Manuela,Fachin Camila,Dias Andre Dos Santos,Sindhwani Nikhil,Scaglioni Dominic,Xenakis Theodoros,Sebire Neil,Giomo Monica,Eaton Simon,Toelen Jaan,Luni Camilla,Pavan Piero,Carmeliet Peter,Russo Francesca,Janes Samuel,Nikolic Marko Z.,Elvassore Nicola,Deprest Jan,Coppi Paolo De

Abstract

AbstractRationaleCongenital diaphragmatic hernia (CDH) results in lung hypoplasia. In severe cases, tracheal occlusion (TO) can be offered to promote lung growth. However the benefit is limited, and novel treatments are required to supplement TO. Vascular endothelial growth factor (VEGF) is downregulated in animal models of CDH and could be a therapeutic target, but its role in human CDH is not known.ObjectivesTo investigate whether VEGF supplementation could be a suitable treatment for CDH-associated lung pathology.MethodsFetal lungs from CDH patients were used to determine pulmonary morphology and VEGF expression. A novel humanex vivomodel of fetal lung compression recapitulating CDH features was developed and used to determine the effect of exogenous VEGF supplementation (Figure 1A). A nanoparticle-based approach for intra-pulmonary delivery of VEGF was developed by conjugating it on functionalized nanodiamonds (ND-VEGF) and was tested in experimental CDHin vivo.Measurements and Main ResultsVEGF expression was downregulated in distal pulmonary epithelium of human CDH fetuses in conjunction with attenuated cell proliferation. The compression model resulted in impaired branching morphogenesis similar to CDH and downregulation of VEGF expression in conjunction with reduced proliferation of terminal bud epithelial progenitors; these could be reversed by exogenous supplementation of VEGF. Prenatal delivery of VEGF with the ND-VEGF platform in CDH fetal rats resulted in lung growth and pulmonary arterial remodelling that was complementary to that achieved by TO alone with appearances comparable to healthy controls.ConclusionsThis innovative approach could have a significant impact on the treatment of CDH.

Publisher

Cold Spring Harbor Laboratory

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