Differential Blood–Brain Barrier Transport and Cell Uptake of Cyclic Peptides In Vivo and In Vitro

Author:

Melander Erik1,Eriksson Camilla2,Wellens Sara3,Hosseini Kimia2,Fredriksson Robert2,Gosselet Fabien3ORCID,Culot Maxime3,Göransson Ulf2,Hammarlund-Udenaes Margareta1,Loryan Irena1ORCID

Affiliation:

1. Department of Pharmacy, Uppsala University, 75123 Uppsala, Sweden

2. Department of Pharmaceutical Biosciences, Uppsala University, 75123 Uppsala, Sweden

3. Laboratoire de la Barrière Hémato-Encéphalique (LBHE), Faculté des Sciences Jean Perrin, University of Artois, UR 2465, Rue Jean Souvraz SP18, F-62300 Lens, France

Abstract

The blood–brain barrier (BBB) poses major challenges to drug delivery to the CNS. SFTI-1 and kalata B1 are cyclic cell-penetrating peptides (cCPPs) with high potential to be used as scaffolds for drug delivery. We here studied their transport across the BBB and distribution within the brain to gauge the potential of these two cCPPs as scaffolds for CNS drugs. In a rat model, SFTI-1 exhibited, for a peptide, high extent of BBB transport with a partitioning of unbound SFTI-1 across the BBB, Kp,uu,brain, of 13%, while only 0.5% of kalata B1 equilibrated across the BBB. By contrast, kalata B1, but not SFTI-1, readily entered neural cells. SFTI-1, but not kalata B1, could be a potential CNS delivery scaffold for drugs directed to extracellular targets. These findings indicate that differences between the BBB transport and cellular uptake abilities of CPPs are crucial in the development of peptide scaffolds.

Funder

Swedish Research Council

Marie Sklodowska-Curie Action—Innovative Training Network project in 3

Innovative Medicines Initiative 2 Joint Undertaking projects IM2PACT

Publisher

MDPI AG

Subject

Pharmaceutical Science

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