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Peptides as Pharmacological Carriers to the Brain: Promises, Shortcomings and Challenges

Journal

MOLECULAR PHARMACEUTICS
Volume 19, Issue 11, Pages 3700-3729

Publisher

AMER CHEMICAL SOC
DOI: 10.1021/acs.molpharmaceut.2c00523

Keywords

peptides; blood-brain-barrier; receptor-mediated transcytosis; cell-penetrating peptides; drug delivery

Funding

  1. AIRC [20286, 26584]
  2. CNR InterOmics project (GLIOMICS)

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Central nervous system diseases are difficult to treat due to the blood-brain barrier (BBB), which prevents most drugs from reaching the brain. Peptides show promise in helping drugs cross the BBB and target the brain. However, there are challenges such as potential toxic effects, short in vivo lifespan, and inadequate drug levels in the brain.
Central nervous system (CNS) diseases are among the most difficult to treat, mainly because the vast majority of the drugs fail to cross the blood-brain barrier (BBB) or to reach the brain at concentrations adequate to exert a pharmacological activity. The obstacle posed by the BBB has led to the in-depth study of strategies allowing the brain delivery of CNS-active drugs. Among the most promising strategies is the use of peptides addressed to the BBB. Peptides are versatile molecules that can be used to decorate nanoparticles or can be conjugated to drugs, with either a stable link or as pro-drugs. They have been used to deliver to the brain both small molecules and proteins, with applications in diverse therapeutic areas such as brain cancers, neurodegenerative diseases and imaging. Peptides can be generally classified as receptor-targeted, recognizing membrane proteins expressed by the BBB microvessels (e.g., Angiopep2, CDX, and iRGD), cell-penetrating peptides (CPPs; e.g. TAT(47-57), SynB1/3, and Penetratin), undergoing transcytosis through unspecific mechanisms, or those exploiting a mixed approach. The advantages of peptides have been extensively pointed out, but so far few studies have focused on the potential negative aspects. Indeed, despite having a generally good safety profile, some peptide conjugates may display toxicological characteristics distinct from those of the peptide itself, causing for instance antigenicity, cardiovascular alterations or hemolysis. Other shortcomings are the often brief lifetime in vivo, caused by the presence of peptidases, the vulnerability to endosomal/lysosomal degradation, and the frequently still insufficient attainable increase of brain drug levels, which remain below the therapeutically useful concentrations. The aim of this review is to analyze not only the successful and promising aspects of the use of peptides in brain targeting but also the problems posed by this strategy for drug delivery.

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