Litcius/Paper detail

Structure–Activity Relationship of pH-Sensitive Doxorubicin-Fatty Acid Prodrug Albumin Nanoparticles

Yinxian Yang, Xiuhong Li, Jiaxuan Song, Lingxiao Li, Qing Ye, Shiyi Zuo, Tian Liu, Fudan Dong, Xiaohong Liu, Zhonggui He, Bingjun Sun, Jin Sun

2023Nano Letters38 citationsDOI

Abstract

Albumin has emerged as a versatile drug carrier. To harness albumin as a carrier for doxorubicin (DOX), we synthesized three acid-labile DOX prodrugs using stearic acid (SA), oleic acid (OA), and linoleic acid (LA) as the albumin-binding motif, respectively. Different from conventional albumin nanodrugs (such as Abraxane, with a drug loading of 10%), the DOX prodrugs assembled albumin nanoparticles (NPs) have an ultrahigh drug loading (>35%). Noteworthy, we demonstrated that the saturation of fatty acids exerted great influence on colloidal stability of prodrug NPs, thus affecting their in vivo pharmacokinetics, tumor accumulation and antitumor efficacy. Furthermore, the hydrazone bond-bridged DOX prodrugs could remain intact in the bloodstream but allow DOX to be released in the acidic tumor environment, resulting in improved antitumor efficacy and safety. Our work gives novel insights into the structure-to-efficacy relationship of albumin-bound fatty acid prodrugs and provides a simple strategy for advanced albumin-bound nanomedicines.

Topics & Concepts

ProdrugAlbuminChemistryDoxorubicinOleic acidFatty acidHuman serum albuminSerum albuminIn vivoBiochemistryMedicineBiologyBiotechnologyChemotherapySurgeryNanoparticle-Based Drug DeliveryProtein Interaction Studies and Fluorescence AnalysisLung Cancer Research Studies