In situ albumin-binding and esterase-specifically cleaved BRD4-degrading PROTAC for targeted cancer therapy

Authors
Cho, HanheeJeon, Seong IkShim, Man KyuAhn, Cheol-HeeKim, Kwangmeyung
Issue Date
2023-04
Publisher
Pergamon Press Ltd.
Citation
Biomaterials, v.295
Abstract
Proteolysis-targeting chimeras (PROTACs) have recently been of great interest in cancer therapy. However, the bioavailability of PROTACs is considerably restricted due to their high hydrophobicity, poor cell permeability, and thereby low tumor targeting ability. Herein, esterase-cleavable maleimide linker (ECMal)-conjugated bromodomain 4 (BRD4)-degrading PROTAC (ECMal-PROTAC) is newly synthesized to exploit plasma albumin as an 'innate drug carrier' that can be accumulated in targeted tumor tissues. The BRD4-degrading ECMal-PROTAC is spontaneously bound to albumins via the thiol-maleimide click chemistry and its esterase-specific cleavage of ECMal-PROTAC is characterized in physiological conditions. The albumin-bound ECMal-PROTACs (Alb-ECMalPROTACs) have an average size of 6.99 +/- 1.38 nm, which is similar to that of free albumins without denaturation or aggregation. When Alb-ECMal-PROTACs are treated to 4T1 tumor cells, they are actively endocytosed and reach their highest intracellular level within 12 h. Furthermore, the maleimide linkers of Alb-ECMal-PROTACs are cleaved by the esterase to release free BRD-4 degrading PROTACs and the cell-internalized PROTACs successfully catalyze the selective degradation of BRD4 proteins, resulting in BRD4 deficiency-related apoptosis. When ECMal-PROTACs are intravenously injected into tumor-bearing mice, they exhibit a 16.3-fold higher tumor accumulation than free BRD4-PROTAC, due to the shuttling effect of albumin for tumor targeting. Finally, ECMal-PROTACs show 5.3-fold enhanced antitumor efficacy compared to free BRD4-PROTAC, without provoking any severe systemic toxicity. The expression of Bcl-2 and c-Myc, the downstream oncogenic proteins of BRD4, are also effectively suppressed. In summary, the in situ albumin binding of ECMal-PROTAC is proven as a promising strategy that effectively modulates its pharmacokinetics and therapeutic performance with high applicability to other types of PROTACs.
Keywords
PROTEIN-DEGRADATION; PROLIFERATION; PRODRUG; DESIGN; BRD4; PROTACs; BRD4 degradation; Esterase-cleavable maleimide linker; Albumin-binding; Shuttling effect; Targeted cancer therapy
ISSN
0142-9612
URI
https://pubs.kist.re.kr/handle/201004/113821
DOI
10.1016/j.biomaterials.2023.122038
Appears in Collections:
KIST Article > 2023
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