2017
DOI: 10.1016/j.jconrel.2017.08.026
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Protease-activatable cell-penetrating peptide possessing ROS-triggered phase transition for enhanced cancer therapy

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Cited by 91 publications
(89 citation statements)
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“…Liposomes [139][140][141][142][143][144][145] Quantum dots (QDs) [157] Polymersomes [158] Magnetic nanoparticles [159] Micelles [146][147][148][149][150][151][152][153][154][155][156] [ 160,161] External Light Liposomes [163] MSN [164] Micelles [168] [ 63,[165][166][167]169]…”
Section: Glutathione (Gsh) (4-80 µM) Disulfidementioning
confidence: 99%
“…Liposomes [139][140][141][142][143][144][145] Quantum dots (QDs) [157] Polymersomes [158] Magnetic nanoparticles [159] Micelles [146][147][148][149][150][151][152][153][154][155][156] [ 160,161] External Light Liposomes [163] MSN [164] Micelles [168] [ 63,[165][166][167]169]…”
Section: Glutathione (Gsh) (4-80 µM) Disulfidementioning
confidence: 99%
“…The destruction of the micelle structures was determined with DLS and two peaks containing a large aggregated form were observed, indicating the high sensitivity of the micellar system to ROS. The underlying mechanism was that thioether groups in methionine segments were changed to hydrophilic sulfoxide groups by ROS and then were induced the disassembly of micelle [20,29] . In this work, the preparation and drug release behavior of PPT/D(DMA)@DOX was used illustrated in Figure 2a.…”
Section: Resultsmentioning
confidence: 99%
“…Secondly, TOS, an analogue of vitamin E, rapidly generates ROS in cells after interacting with mitochondrial respiratory complex II and interfering the electron transportation chain in mitochondria [13] . Thioether groups in polymethionine segments are changed to hydrophilic sulfoxide groups in cancer cells due to an inundation of ROS [11,12,20] . We hypothesized that ROS concentration under pathological conditions can induce the less decomposition of the polymeric drug by the phase transitions and then exposed TOS segment interacted with mitochondria in tumor cells to generate additional ROS.…”
Section: Introductionmentioning
confidence: 99%
“…89 Cancer The findings of this study suggesting that dual-stimuli-based delivery systems have great potential in cancer therapy. 90 Although MMP-based ACPPs are known to target tumors effectively in vivo, ACPP substrates are not perfectly selective for MMPs, and MMP is not exclusively expressed in tumors. Therefore, in order to improve the targeting potential of ACPPs, Whitney et al explored other classes of proteases and substrates that might offer better specificity and flexibility than MMP-based approaches by using phage display.…”
Section: Enzyme-activated Cppsmentioning
confidence: 99%