Targeting Human Endothelial Cells with Glutathione and Alanine Increases the Crossing of a Polypeptide Nanocarrier through a Blood-Brain Barrier Model and Entry to Human Brain Organoids

Mária Mészáros; Thi Ha My Phan; Judit P Vigh; Gergő Porkoláb; Anna Kocsis; Emese K Páli; Tamás F Polgár; Fruzsina R Walter; Silvia Bolognin; Jens C Schwamborn; Jeng-Shiung Jan; Mária A Deli; Szilvia Veszelka

doi:10.3390/cells12030503

Targeting Human Endothelial Cells with Glutathione and Alanine Increases the Crossing of a Polypeptide Nanocarrier through a Blood-Brain Barrier Model and Entry to Human Brain Organoids

Cells. 2023 Feb 3;12(3):503. doi: 10.3390/cells12030503.

Authors

Affiliations

¹ Institute of Biophysics, Biological Research Centre, Eötvös Loránd Research Network, H-6726 Szeged, Hungary.
² Department of Chemical Engineering, National Cheng Kung University, Tainan 70101, Taiwan.
³ Doctoral School of Biology, University of Szeged, H-6720 Szeged, Hungary.
⁴ Theoretical Medicine Doctoral School, University of Szeged, H-6722 Szeged, Hungary.
⁵ Luxembourg Centre for Systems Biomedicine (LCSB), Developmental and Cellular Biology, University of Luxembourg, 4365 Belvaux, Luxembourg.

Abstract

Nanoparticles (NPs) are the focus of research efforts that aim to develop successful drug delivery systems for the brain. Polypeptide nanocarriers are versatile platforms and combine high functionality with good biocompatibility and biodegradability. The key to the efficient brain delivery of NPs is the specific targeting of cerebral endothelial cells that form the blood-brain barrier (BBB). We have previously discovered that the combination of two different ligands of BBB nutrient transporters, alanine and glutathione, increases the permeability of vesicular NPs across the BBB. Our aim here was to investigate whether the combination of these molecules can also promote the efficient transfer of 3-armed poly(l-glutamic acid) NPs across a human endothelial cell and brain pericyte BBB co-culture model. Alanine and glutathione dual-targeted polypeptide NPs showed good cytocompatibility and elevated cellular uptake in a time-dependent and active manner. Targeted NPs had a higher permeability across the BBB model and could subsequently enter midbrain-like organoids derived from healthy and Parkinson's disease patient-specific stem cells. These results indicate that poly(l-glutamic acid) NPs can be used as nanocarriers for nervous system application and that the right combination of molecules that target cerebral endothelial cells, in this case alanine and glutathione, can facilitate drug delivery to the brain.

Keywords: 3-armed polypeptides; alanine; blood–brain barrier; brain endothelial cells; brain organoid; dual-targeting; glutathione; peptide nanocarriers.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Alanine
Blood-Brain Barrier*
Brain
Endothelial Cells*
Glutamic Acid
Glutathione
Humans
Organoids
Peptides / chemistry
Peptides / pharmacology

Substances

Alanine
Glutamic Acid
Peptides
Glutathione

Grants and funding

This work was funded by the National Research, Development and Innovation Office of Hungary, grant numbers NNE-29617 (M-ERA.NET2 nanoPD). S.V. was supported by the Premium Postdoctoral Research Program (Premium-2019–469) of the Hungarian Academy of Sciences and the OTKA Young Researcher Excellence Program (OTKA-FK 143233) by National Research, Development and Innovation Office of Hungary. M.M. was supported by the research grant (PD 138930) of the National Research, Development and Innovation Office, Budapest, Hungary, the Gedeon Richter Plc. Centenarial Foundation (H-1103 Budapest, Gyömrői str. 19–21. Hungary) and the “National Talent Program” with the financial aid of the Ministry of Human Resources (NTP-NFTÖ-21-B-0228 and NTP-NFTÖ-22-B-0150). G.P. was supported by the National Academy of Scientist Education Program of the National Biomedical Foundation under the sponsorship of the Hungarian Ministry of Culture and Innovation, the Stephen W. Kuffler Research Foundation, the Gedeon Richter Plc. Centenarial Foundation, as well as by the ÚNKP-22-3-SZTE-446 New National Excellence Program of the Ministry for Innovation and Technology from the source of the National Research, Development and Innovation. E.K.P. was supported by the National Academy of Scientist Education Program of the National Biomedical Foundation under the sponsorship of the Hungarian Ministry of Culture and Innovation and the Gedeon Richter Plc. Centenarial Foundation. (T.F.P.) was supported by the “National Talent Program” with the financial aid of the Ministry of Human Resources (NTP-NFTÖ-22-C-0023). The project was supported by the Secretariat of Lorand Eotvos Research Network, SA-111/2021, granted for F.R.W., J.C.S and S.B. were supported by the Fonds National de la Recherche (FNR) Luxembourg (INTER/MERA/17/11760144). J.S.J. was supported by the National Science Technology Council, Taiwan: NSTC107-2923-M-006-002-MY3.