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A region-confined PROTAC nanoplatform for spatiotemporally tunable protein degradation and enhanced cancer therapy

  • Jing Gao
  • , Xingyu Jiang
  • , Shumin Lei
  • , Wenhao Cheng
  • , Yi Lai
  • , Min Li
  • , Lei Yang
  • , Peifeng Liu
  • , Xiao Hua Chen
  • , Min Huang
  • , Haijun Yu*
  • , Huixiong Xu*
  • , Zhiai Xu*
  • *此作品的通讯作者
  • CAS - Shanghai Institute of Materia Medica
  • Fudan University
  • Tongji University
  • East China Normal University
  • Nanjing University of Chinese Medicine
  • Shanghai Jiao Tong University

科研成果: 期刊稿件文章同行评审

摘要

The antitumor performance of PROteolysis-TArgeting Chimeras (PROTACs) is limited by its insufficient tumor specificity and poor pharmacokinetics. These disadvantages are further compounded by tumor heterogeneity, especially the presence of cancer stem-like cells, which drive tumor growth and relapse. Herein, we design a region-confined PROTAC nanoplatform that integrates both reactive oxygen species (ROS)-activatable and hypoxia-responsive PROTAC prodrugs for the precise manipulation of bromodomain and extraterminal protein 4 expression and tumor eradication. These PROTAC nanoparticles selectively accumulate within and penetrate deep into tumors via response to matrix metalloproteinase-2. Photoactivity is then reactivated in response to the acidic intracellular milieu and the PROTAC is discharged due to the ROS generated via photodynamic therapy specifically within the normoxic microenvironment. Moreover, the latent hypoxia-responsive PROTAC prodrug is restored in hypoxic cancer stem-like cells overexpressing nitroreductase. Here, we show the ability of region-confined PROTAC nanoplatform to effectively degrade BRD4 in both normoxic and hypoxic environments, markedly hindering tumor progression in breast and head-neck tumor models.

源语言英语
文章编号6608
期刊Nature Communications
15
1
DOI
出版状态已出版 - 12月 2024

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