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Carfilzomib Delivery by Quinic Acid-Conjugated Nanoparticles: Discrepancy Between Tumoral Drug Accumulation and Anticancer Efficacy in a Murine 4T1 Orthotopic Breast Cancer Model

Cited 3 time in Web of Science Cited 3 time in Scopus
Authors

Jun, Yearin; Xu, Jun; Kim, Hyungjun; Park, Ji Eun; Jeong, Yoo-Seong; Min, Jee Sun; Yoon, Naeun; Choi, Ji Yoon; Yoo, Jisu; Kyung, Soo; Chung, Suk-Jae; Yeo, Yoon; Lee, Wooin

Issue Date
2020-04
Publisher
Elsevier Inc.
Citation
Journal of Pharmaceutical Sciences, Vol.109 No.4, pp.1615-1622
Abstract
Despite being a major breakthrough in multiple myeloma therapy, carfilzomib (CFZ, a second-generation proteasome inhibitor drug) has been largely ineffective against solid cancer, possibly due to its pharmacokinetic drawbacks including metabolic instability. Recently, quinic acid (QA, a low-affinity ligand of selectins upregulated in peritumoral vasculature) was successfully utilized as a surface modifier for nanoparticles containing paclitaxel. Here, we designed QA-conjugated nanoparticles containing CFZ (CFZ@QANP; the surface of poly(lactic-co-glycolic acid) nanoparticles modified by conjugation with a QA derivative). Compared to the clinically used cyclodextrin-based formulation (CFZ-CD), CFZ@QANP enhanced the metabolic stability and in vivo exposure of CFZ in mice. CFZ@QANP, however, showed little improvement in suppressing tumor growth over CFZ-CD against the murine 4T1 orthotopic breast cancer model. CFZ@QANP yielded no enhancement in proteasomal inhibition in excised tumors despite having a higher level of remaining CFZ than CFZ-CD. These results likely arise from delayed, incomplete CFZ release from CFZ@QANP as observed using biorelevant media in vitro. These results suggest that the applicability of QANP may not be predicted by physicochemical parameters commonly used for formulation design. Our current results highlight the importance of considering drug release kinetics in designing effective CFZ formulations for solid cancer therapy. (C) 2020 American Pharmacists Association (R). Published by Elsevier Inc. All rights reserved.
ISSN
0022-3549
URI
https://hdl.handle.net/10371/190090
DOI
https://doi.org/10.1016/j.xphs.2020.01.008
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