Molecules (Sep 2019)

Hyaluronic Acid–Decorated Liposomes as Innovative Targeted Delivery System for Lung Fibrotic Cells

  • Laura Pandolfi,
  • Vanessa Frangipane,
  • Claudia Bocca,
  • Alessandro Marengo,
  • Erika Tarro Genta,
  • Sara Bozzini,
  • Monica Morosini,
  • Maura D’Amato,
  • Simone Vitulo,
  • Manuela Monti,
  • Giuditta Comolli,
  • Maria Teresa Scupoli,
  • Elias Fattal,
  • Silvia Arpicco,
  • Federica Meloni

DOI
https://doi.org/10.3390/molecules24183291
Journal volume & issue
Vol. 24, no. 18
p. 3291

Abstract

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Collagen Tissue Disease−associated Interstitial Lung Fibrosis (CTD-ILDs) and Bronchiolitis Obliterans Syndrome (BOS) represent severe lung fibrogenic disorders, characterized by fibro-proliferation with uncontrolled extracellular matrix deposition. Hyaluronic acid (HA) plays a key role in fibrosis with its specific receptor, CD44, overexpressed by CTD-ILD and BOS cells. The aim is to use HA-liposomes to develop an inhalatory treatment for these diseases. Liposomes with HA of two molecular weights were prepared and characterized. Targeting efficiency was assessed toward CTD-ILD and BOS cells by flow cytometry and confocal microscopy and immune modulation by RT-PCR and ELISA techniques. HA-liposomes were internalized by CTD-ILD and BOS cells expressing CD44, and this effect increased with higher HA MW. In THP-1 cells, HA-liposomes decreased pro-inflammatory cytokines IL-1β, IL-12, and anti-fibrotic VEGF transcripts but increased TGF-β mRNA. However, upon analyzing TGF-β release from healthy donors-derived monocytes, we found liposomes did not alter the release of active pro-fibrotic cytokine. All liposomes induced mild activation of neutrophils regardless of the presence of HA. HA liposomes could be also applied for lung fibrotic diseases, being endowed with low pro-inflammatory activity, and results confirmed that higher MW HA are associated to an increased targeting efficiency for CD44 expressing LFs-derived from BOS and CTD-ILD patients.

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