Stimuli-responsive clustered nanoparticles for improved tumor penetration and therapeutic efficacy

Li, Hong Jun; Du, Jin Zhi; Du, Xiao; Xu, Cong; Sun, Chun; Wang, Hongxia; Cao, Zhi Ting; Yang, Xianzhu; Zhu, Yahui; Nie, Shuming; Wang, Jun

doi:10.1073/pnas.1522080113

Cited by 647 publications

(412 citation statements)

References 49 publications

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“…These NPs undergo particle size change [34] , surface charge status switching [35] , or a hydrophobic to hydrophilic transition [36] by responding to the pH drop in the weakly acidic microenvironment of tumor or cancer cells. For instance, Wang et al recently reported a novel set of intelligent cluster (iCluster) NPs to improve the tumor penetration and distribution of the poly(amidoamine) (PAMAM) prodrug [37] . The NPs were composed of two distinct components.…”

Section: Overcoming Extracellular Barriers Using Nanomedicinementioning

confidence: 99%

“…The PAMAM prodrug penetrated deeply into the tumor, owing to the small particle size (~5 nm). Subsequently, the prodrug performed its antitumor function by being converted to cisplatin in the reducing environment of the cytosol ( Figure 1B) [37] . In a multilayer spheroidal cancer (MSC) model derived from BxPC-3 human pancreatic cancer cells, the hydrophobic PCL core (with red fluorescence labeling) of the iCluster NPs was observed to attach to the periphery of MCSs without a noticeable distribution in the internal area, after a 24 h incubation at a pH of 6.8.…”

Section: Overcoming Extracellular Barriers Using Nanomedicinementioning

confidence: 99%

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Smart nanoparticles improve therapy for drug-resistant tumors by overcoming pathophysiological barriers

Liu

Wang

et al. 2016

Acta Pharmacol Sin

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The therapeutic outcome of chemotherapy is severely limited by intrinsic or acquired drug resistance, the most common causes of chemotherapy failure. In the past few decades, advancements in nanotechnology have provided alternative strategies for combating tumor drug resistance. Drug-loaded nanoparticles (NPs) have several advantages over the free drug forms, including reduced cytotoxicity, prolonged circulation in the blood and increased accumulation in tumors. Currently, however, nanoparticulate drugs have only marginally improved the overall survival rate in clinical trials because of the various pathophysiological barriers that exist in the tumor microenvironment, such as intratumoral distribution, penetration and intracellular trafficking, etc. Smart NPs with stimulusadaptable physico-chemical properties have been extensively developed to improve the therapeutic efficacy of nanomedicine. In this review, we summarize the recent advances of employing smart NPs to treat the drug-resistant tumors by overcoming the pathophysiological barriers in the tumor microenvironment.

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Section: Overcoming Extracellular Barriers Using Nanomedicinementioning

confidence: 99%

Section: Overcoming Extracellular Barriers Using Nanomedicinementioning

confidence: 99%

Smart nanoparticles improve therapy for drug-resistant tumors by overcoming pathophysiological barriers

Liu

Wang

et al. 2016

Acta Pharmacol Sin

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“…In principle, this transition would make DNPs inclined to aggregate and thus slow down reentry into the blood stream because of its inherently hydrophobic nature, which consequently leads to a locally long‐term entrapment of drug‐vehicle system within neighboring tumor cells. And, the photothermal effect of PDA can trigger the release of small DNPs (≈5 nm) that enable deep and uniform penetration into more cancer cells, ultimately enhancing the chemotherapy of the DOX 34, 35. Attractively, the structure alteration will simultaneously induce a selectively fast drug release, favoring the enhanced drug efficacy inside tumor cells and finally realizing the chemo‐/photothermal synergistic therapy of cancer.…”

Section: Introductionmentioning

confidence: 99%

NIR‐Activated Polydopamine‐Coated Carrier‐Free “Nanobomb” for In Situ On‐Demand Drug Release

et al. 2018

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Carrier‐free nanoparticles with high drug loading have attracted increasing attention; however, in situ on‐demand drug release remains a challenge. Here, a novel near‐infrared (NIR) laser‐induced blasting carrier‐free nanodrug delivery system is designed and fabricated by coating doxorubicin (DOX) nanoparticles (DNPs) with a polydopamine film (PDA) that would prolong the blood circulation time of DNPs and avoid the preleakage of the DOX during blood circulation. Meanwhile, the NH4HCO3 is introduced to trigger in situ “bomb‐like” release of DOX for the production of carbon dioxide (CO2) and ammonia (NH3) gases driven by NIR irradiated photothermal effect of PDA. Both in vitro and in vivo studies demonstrate that the carrier‐free nanovectors with high drug loading efficiency (85.8%) prolong tumor accumulation, enhance chemotherapy, achieve the synergistic treatment of chemotherapy and photothermal treatment, and do not induce any foreign‐body reaction over a three‐week implantation. Hence, the delicate design opens a self‐assembly path to develop PDA‐based NIR‐responsive multifunctional carrier‐free nanoparticles for tumor therapy.

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“…In particular, positively charged oligoarginines have raised special interest, which possess several advantages including cell penetrating, nucleic acids binding capability, synthetic versatility, accessibility for tagging/labeling, and the easy design of various stimuli‐responsive sequences 29, 30, 31. At present, various stimuli‐responsive “smart” nanostructures have been developed according to the heterogeneity of extra‐ and intratumoral microenvironments, such as low pH, altered redox potential, hypoxia, and dysregulated enzymes, which allow spatially controlled release of the therapeutics only in the sites of interest to improve therapeutic efficiency 32, 33, 34, 35. For instance, the concentration of glutathione (GSH) is remarkably higher in tumor cells (10 × 10 −3 m ) compared to that in the blood plasma whose concentration is about 2 × 10 −6 to 10 × 10 −6 m 36.…”

Section: Introductionmentioning

confidence: 99%

In Situ Monitoring of MicroRNA Replacement Efficacy and Accurate Imaging‐Guided Cancer Therapy through Light‐Up Inter‐Polyelectrolyte Nanocomplexes

Deng

Yin

et al. 2018

Advanced Science

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Replacement of downregulated tumor‐suppressive microRNA (Ts‐miRNA) is recognized as an alternative approach for tumor gene therapy. However, in situ monitoring of miRNA replacement efficacy in a real‐time manner via noninvasive imaging is continually challenging. Here, glutathione (GSH)‐activated light‐up peptide‐polysaccharide‐inter‐polyelectrolyte nanocomplexes are established through self‐assembly of carboxymethyl dextran with disulfide‐bridged (“S—S”) oligoarginine peptide (S‐Arg4), in which microRNA‐34a (miR‐34a) and indocyanine green (ICG) are simultaneously embedded and the nanocomplexes are subsequently stabilized by intermolecular cross‐linking. Upon confinement within the robust nanocomplexes, the near‐infrared fluorescence (NIRF) of ICG is considerably quenched (“off”) due to the aggregation‐caused quenching effect. However, after intracellular delivery, the disulfide bond in S‐Arg4 can be cleaved by intracellular GSH, which leads to the dissociation of nanocomplexes and triggers the simultaneous release of miR‐34a and ICG. The NIRF of ICG is concomitantly activated through dequenching of the aggregated ICG. Very interestingly, a good correlation between time‐dependent increase in NIRF intensity and miR‐34a replacement efficacy is found in nanocomplexes‐treated tumor cells and tumor tissues through either intratumoral or intravenous injections. Systemic nanocomplexes‐mediated miR‐34a replacement significantly suppresses the growth of HepG‐2‐ and MDA‐MB‐231‐derived tumor xenografts, and provides a pronounced survival benefit in these animal models.

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Stimuli-responsive clustered nanoparticles for improved tumor penetration and therapeutic efficacy

Cited by 647 publications

References 49 publications

Smart nanoparticles improve therapy for drug-resistant tumors by overcoming pathophysiological barriers

Smart nanoparticles improve therapy for drug-resistant tumors by overcoming pathophysiological barriers

NIR‐Activated Polydopamine‐Coated Carrier‐Free “Nanobomb” for In Situ On‐Demand Drug Release

In Situ Monitoring of MicroRNA Replacement Efficacy and Accurate Imaging‐Guided Cancer Therapy through Light‐Up Inter‐Polyelectrolyte Nanocomplexes

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