Peptide-Drug Conjugate with Statistically Designed Transcellular Peptide for Psoriasis-Like Inflammation

  • Do Hyun Bae
  • , Hayeon Bae
  • , Hyung Seok Yu
  • , Banzragch Dorjsembe
  • , Young Hyun No
  • , Taejung Kim
  • , Nam Hyeong Kim
  • , Jin Woo Kim
  • , Jiyool Kim
  • , Bok Soo Lee
  • , Ye Ji Kim
  • , Seongchan Park
  • , Zinah Hilal Khaleel
  • , Deok Hyang Sa
  • , Eui Chul Lee
  • , Jaecheol Lee
  • , Jungyeob Ham
  • , Jin Chul Kim
  • , Yong Ho Kim

Research output: Contribution to journalArticlepeer-review

Abstract

Peptide-drug conjugates (PDCs) are a promising class of drug delivery systems that utilize covalently conjugated carrier peptides with therapeutic agents. PDCs offer several advantages over traditional drug delivery systems including enhanced target engagement, improved bioavailability, and increased cell permeability. However, the development of efficient transcellular peptides capable of effectively transporting drugs across biological barriers remains an unmet need. In this study, physicochemical criteria based on cell-penetrating peptides are employed to design transcellular peptides derived from an antimicrobial peptides library. Among the statistically designed transcellular peptides (SDTs), SDT7 exhibits higher skin permeability, faster kinetics, and improved cell permeability in human keratinocyte cells compared to the control peptide. Subsequently, it is found that 6-Paradol (PAR) exhibits inhibitory activity against phosphodiesterase 4, which can be utilized for an anti-inflammatory PDC. The transcellular PDC (SDT7-conjugated with PAR, named TM5) is evaluated in mouse models of psoriasis, exhibiting superior therapeutic efficacy compared to PAR alone. These findings highlight the potential of transcellular PDCs (TDCs) as a promising approach for the treatment of inflammatory skin disorders.

Original languageEnglish
Article number2303480
JournalAdvanced Healthcare Materials
Volume13
Issue number15
DOIs
StatePublished - 13 Jun 2024

Keywords

  • anti-inflammation
  • ginger-driven compounds
  • peptide-drug conjugates
  • skin barrier
  • transcellular peptide

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