Literature DB >> 30756483

Conjugate of Doxorubicin to Albumin-Binding Peptide Outperforms Aldoxorubicin.

Parisa Yousefpour1, Lucie Ahn1, Joel Tewksbury1, Soumen Saha1, Simone A Costa1, Joseph J Bellucci1, Xinghai Li1, Ashutosh Chilkoti1.   

Abstract

Short circulation time and off-target toxicity are the main challenges faced by small-molecule chemotherapeutics. To overcome these shortcomings, an albumin-binding peptide conjugate of chemotherapeutics is developed that binds specifically to endogenous albumin and harnesses its favorable pharmacokinetics and pharmacodynamics for drug delivery to tumors. A protein-G-derived albumin-binding domain (ABD) is conjugated with doxorubicin (Dox) via a pH-sensitive linker. One to two Dox molecules are conjugated to ABD without loss of aqueous solubility. The albumin-binding ABD-Dox conjugate exhibits nanomolar affinity for human and mouse albumin, and upon administration in mice, shows a plasma half-life of 29.4 h, which is close to that of mouse albumin. Additionally, 2 h after administration, ABD-Dox exhibits an approximately 4-fold higher concentration in the tumor than free Dox. Free Dox clears quickly from the tumor, while ABD-Dox maintains a steady concentration in the tumor for at least 72 h, so that its relative accumulation at 72 h is ≈120-fold greater than that of free Dox. The improved pharmacokinetics and biodistribution of ABD-Dox result in enhanced therapeutic efficacy in syngeneic C26 colon carcinoma and MIA PaCa-2 pancreatic tumor xenografts, compared with free Dox and aldoxorubicin, an albumin-reactive Dox prodrug currently in clinical development.
© 2019 WILEY-VCH Verlag GmbH & Co. KGaA, Weinheim.

Entities:  

Keywords:  albumin binding; cancer; doxorubicin; drug delivery; peptides

Mesh:

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Year:  2019        PMID: 30756483      PMCID: PMC8114561          DOI: 10.1002/smll.201804452

Source DB:  PubMed          Journal:  Small        ISSN: 1613-6810            Impact factor:   13.281


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