Co-delivery of doxorubicin and curcumin by pH-sensitive prodrug nanoparticle for combination therapy of cancer

Zhang, Yumin; Yang, Cuihong; Wang, Weiwei; Liu, Jinjian; Liu, Qiang; Huang, Fan; Chu, Liping; Gao, Honglin; Li, Chen; Kong, Deling; Liu, Qian; Liu, Jianfeng

doi:10.1038/srep21225

Cited by 197 publications

(142 citation statements)

References 46 publications

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“…The nanoformulation of curcumin is versatile. Free curcumin, polymeric, liposomal and other types of formulations of curcumin can be co/concurrently-delivered with chemotherapy, such as camptothecin (CPT) [86], etoposide [45, 87], platinum [88], PTX [48, 89] and DOX [90, 91] to induce synergy. One study utilized flaxseed oil nanoemulsion to effectively encapsulate PTX and curcumin to enhance the cytotoxicity against both wild-type and resistant ovarian tumor cell line SKOV3[48].…”

Section: Rationales and Significance Of Traditional Combination Thmentioning

confidence: 99%

“…Single or multiple drug-conjugated polymers exhibiting amphiphilic properties were also used to encapsulate small-molecule drugs for combination therapy based on the supramolecular interaction between drug-conjugated polymer carriers and the other drugs [90, 107–110]. For example, the platinum (IV) prodrug is conjugated to a PLA backbone via an ester bond to form the PLA-Pt(IV) conjugate [108, 109].…”

Section: Nanoformulation-mediated Co-delivery Of Small-molecule Chmentioning

confidence: 99%

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Nanoformulations for combination or cascade anticancer therapy

Miao

Guo

Lin

et al. 2017

Advanced Drug Delivery Reviews

148

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Nanoparticle drug formulations have been extensively investigated, developed, and in some cases, approved by the Food and Drug Administration (FDA). Synergistic combinations of drugs having distinct tumor-inhibiting mechanisms and non-overlapping toxicity can circumvent the issue of treatment resistance and may be essential for effective anti-cancer therapy. At the same time, co-delivery of a combined regimen by a single nanocarrier presents a challenge due to differences in solubility, molecular weight, functional groups and encapsulation conditions between the two drugs. This review discusses cellular and microenvironment mechanisms behind treatment resistance and nanotechnology-based solutions for effective anti-cancer therapy. Co-loading or cascade delivery of multiple drugs using of polymeric nanoparticles, polymer-drug conjugates and lipid nanoparticles will be discussed along with lipid-coated drug nanoparticles developed by our lab and perspectives on combination therapy.

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Section: Rationales and Significance Of Traditional Combination Thmentioning

confidence: 99%

Section: Nanoformulation-mediated Co-delivery Of Small-molecule Chmentioning

confidence: 99%

Nanoformulations for combination or cascade anticancer therapy

Miao

Guo

Lin

et al. 2017

Advanced Drug Delivery Reviews

148

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“…13 Zhang et al reported that co-delivery NPs of DOX and curcumin could simultaneously release the drugs in the acidic microenvironment of cancer cells. 23 However, even if these drugs are transported to the cytoplasm, they still face the difficulty of escaping the fate of efflux associated with P-gp. Therefore, the intracellular precision release of NDDS-loaded P-gp substrates is still a demanding issue.…”

Section: Introductionmentioning

confidence: 99%

Co-delivery nanoparticles with characteristics of intracellular precision release drugs for overcoming multidrug resistance

Zhang

Kong

Jie

et al. 2017

IJN

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Combination chemotherapy in clinical practice has been generally accepted as a feasible strategy for overcoming multidrug resistance (MDR). Here, we designed and successfully prepared a co-delivery system named S-D1@L-D2 NPs, where denoted some smaller nanoparticles (NPs) carrying a drug doxorubicin (DOX) were loaded into a larger NP containing another drug (vincristine [VCR]) via water-in-oil-in-water double-emulsion solvent diffusion-evaporation method. Chitosan-alginate nanoparticles carrying DOX (CS-ALG-DOX NPs) with a smaller diameter of about 20 nm formed S-D1 NPs; vitamin E D-α-tocopheryl polyethylene glycol 1000 succinate-modified poly(lactic-co-glycolic acid) nanoparticles carrying VCR (TPGS-PLGA-VCR NPs) with a larger diameter of about 200 nm constituted L-D2 NPs. Some CS-ALG-DOX NPs loaded into TPGS-PLGA-VCR NPs formed CS-ALG-DOX@TPGS-PLGA-VCR NPs. Under the acidic environment of cytosol and endosome or lysosome in MDR cell, CS-ALG-DOX@TPGS-PLGA-VCR NPs released VCR and CS-ALG-DOX NPs. VCR could arrest cell cycles at metaphase by inhibiting microtubule polymerization in the cytoplasm. After CS-ALG-DOX NPs escaped from endosome, they entered the nucleus through the nuclear pore and released DOX in the intra-nuclear alkaline environment, which interacted with DNA to stop the replication of MDR cells. These results indicated that S-D1@L-D2 NPs was a co-delivery system of intracellular precision release loaded drugs with pH-sensitive characteristics. S-D1@L-D2 NPs could obviously enhance the in vitro cytotoxicity and the in vivo anticancer efficiency of co-delivery drugs, while reducing their adverse effects. Overall, S-D1@L-D2 NPs can be considered an innovative platform for the co-delivery drugs of clinical combination chemotherapy for the treatment of MDR tumor.

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“…When an intracellular pH-triggered drug release carrier is incorporated with a tumour-targeting ligand, this multifunctional nanocarrier can recognize tumour cells and release the encapsulated drug at tumour sites in a controlled manner12. A variety of nanomaterials responding to pH stimuli, such as liposomes, micelles, polymeric and prodrug nanoparticles, have been synthesised and developed as effective drug delivery systems3456. However, not much effort has gone toward developing a pH-responsive drug delivery system based on virus-like nanoparticles (VLNPs).…”

mentioning

confidence: 99%

pH-responsive Virus-like Nanoparticles with Enhanced Tumour-targeting Ligands for Cancer Drug Delivery

Biabanikhankahdani

Alitheen

et al. 2016

Sci Rep

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Multifunctional nanocarriers harbouring specific targeting moieties and with pH-responsive properties offer great potential for targeted cancer therapy. Several synthetic drug carriers have been studied extensively as drug delivery systems but not much information is available on the application of virus-like nanoparticles (VLNPs) as multifunctional nanocarriers. Here, we describe the development of pH-responsive VLNPs, based on truncated hepatitis B virus core antigen (tHBcAg), displaying folic acid (FA) for controlled drug delivery. FA was conjugated to a pentadecapeptide containing nanoglue bound on tHBcAg nanoparticles to increase the specificity and efficacy of the drug delivery system. The tHBcAg nanoparticles loaded with doxorubicin (DOX) and polyacrylic acid (PAA) demonstrated a sustained drug release profile in vitro under tumour tissue conditions in a controlled manner and improved the uptake of DOX in colorectal cancer cells, leading to enhanced antitumour effects. This study demonstrated that DOX-PAA can be packaged into VLNPs without any modification of the DOX molecules, preserving the pharmacological activity of the loaded DOX. The nanoglue can easily be used to display a tumour-targeting molecule on the exterior surface of VLNPs and can bypass the laborious and time-consuming genetic engineering approaches.

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Co-delivery of doxorubicin and curcumin by pH-sensitive prodrug nanoparticle for combination therapy of cancer

Cited by 197 publications

References 46 publications

Nanoformulations for combination or cascade anticancer therapy

Nanoformulations for combination or cascade anticancer therapy

Co-delivery nanoparticles with characteristics of intracellular precision release drugs for overcoming multidrug resistance

pH-responsive Virus-like Nanoparticles with Enhanced Tumour-targeting Ligands for Cancer Drug Delivery

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