Abstract
The development of cancer nanotherapeutics has attracted great interest in the recent decade. Cancer nanotherapeutics have overcome several limitations of conventional therapies, such as nonspecific biodistribution, poor water solubility, and limited bioavailability. Nanoparticles with tuned size and surface characteristics are the key components of nanotherapeutics, and are designed to passively or actively deliver anti-cancer drugs to tumor cells. We provide an overview of nanoparticle-based drug delivery methods and cancer therapies based on tumor-targeting delivery strategies that have been developed in recent years.
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Introduction
Nanomedicine involves the development and application of nanometer-scaled materials in the diagnosis, treatment, and prevention of diseases. Its indications range from the medical applications of nanomaterials and biological devices to nanometer-scaled electronic biosensors. Nanoparticles are the key components of nanomedicine and have received extensive interest as promising drug-delivery systems for cancer diagnosis and treatment.1-3 Nanoparticles applied as drug delivery systems are submicron-sized (100–1,000 nm) particles, devices, or systems synthesized from various materials, including polymers (e.g., polymeric nanoparticles, micelles, vesicles, or dendrimers),4 lipids (liposomes),5 viruses (viral nanoparticles),6 and even inorganics.7,8 By using either passive or active targeting strategies, nanoparticles can increase the intracellular concentration of drugs in cancer cells while preventing toxicity to normal cells. Nanoparticles are usually enveloped by endosomes via receptor-mediated endocytosis after entering tumor cells, therefore escaping P-glycoprotein recognition,9 one of the main mechanisms of drug resistance.
However, although nanoparticles are promising drug carrier systems, their poor oral bioavailability, instability in circulation, inadequate tissue distribution, and toxicity are some limitations to practical application that remain unresolved. In 2016, Wilhelm et al.10 surveyed the literature from the past 10 years on nanoparticle-based drug carriers; their review showed that only 0.7% (median) of the administered nanoparticle dose was delivered to a solid tumor. This low delivery efficiency negatively affects the translation of nanotechnology to clinical applications.
To overcome these concerns and to satisfy safety, regulatory, and ethical requirements, researchers have continued to develop nanomedicine with improved characteristics. A more recent review by a group of pioneers in nanomedicine has provided a comprehensive overview of developments and current challenges in the field. The review also highlighted the upcoming opportunities in the field and clinical applications11 of nanomedicine for in vivo diagnosis, in vitro diagnosis, in vivo therapeutics, and implantable materials.
Despite of all the problems associated with nanomedicine, nanoparticle-based drug delivery systems remain as a potential strategy for cancer therapy. Some nanoparticle formulations for cancer treatment have been already approved by regulatory agencies. These formulations exert fewer adverse effects than unmodified or bare drugs. Considerable effort has been expended to develop systems with precisely controlled functions and material properties. In this review, we will focus on the recent progress in the development of novel responsive nanoparticle systems with high sensitivity to tumor microenvironments for improved cancer diagnosis and treatment, as well as on combined nanoparticle-assisted cancer therapies.
Tumor targeting by nanoparticles
The basis of tumor-targeting drug delivery systems is the ability of nanoparticles to passively or actively accumulate in the desired tissues or cells. In passive targeting, nanoparticles are designed for transport through leaky vessels and the unique intra-organ pressures of tumors. In active targeting, nanoparticles are designed to adhere to specific biological structures in tumors via the molecular recognition of surface-bound ligands. The nanoparticles and loaded drugs thus escape immune clearance, avoid nonspecific cell uptake, and specifically accumulate in the targeted tumor cells and tissues.
Enhanced permeability and retention (EPR) effect
EPR effect is the property by which molecules of certain sizes (normally 100–1,000 nm) preferentially accumulate in tumor tissues instead of in normal tissues. Given their vigorous activity, tumor cells require more nutrients than normal cells, thus leading to the secretion of vascular endothelial growth factor and other growth factors that promote angiogenesis in tumors. Compared with that of normal vessels, the endothelial gap of new blood vessels is larger, thus facilitating the transport of macromolecular substances through blood vessels to tumor tissue. In addition, the lack of lymphatic vessels causes lymph circumfluence to suffocate. Under these double circumstances, macromolecular substances, or nanoparticles, accumulate in tumor tissues. EPR-passive targeting is the basis of tumor drug delivery. By stimulating tumor vasodilation, reducing lymphocytes, and extending circulation time, we can maximize the EPR effect of tumor-targeting delivery systems.
Park et al.12 developed a new type of porous silicon nanoparticle to decrease the metabolic rate and increase the circulation time of loaded drugs in the body. To allow the nanomaterials to accumulate in the tumor site, the group used silicon and silicon dioxide as the core of the nanoparticles and packed dextran outside of the nanoparticles after drug loading. After loading on the formed luminescent porous silicon nanoparticles (LPSiNPs), the circulation time of the drugs in the body was extended. The fluorescence emitted by the LPSiNPs under near-infrared (NIR) excitation can be used to trace the metabolism of the drug in the body. Low toxicity metabolism, extended circulation time, and fluorescence tracing make LPSiNPs a unique nanomaterial with broad prospective applications.
Mundra et al.13 covalently conjugated indocyanine green (ICG)-NH2 to the pendant carboxyl groups of poly (ethylene glycol)-block-poly(2-methyl-2-carboxyl-propylene carbonate) copolymer via carbodiimide coupling. The system self-assembles into micelles with a particle size of 30–50 nm and high ICG loading. In vivo NIR imaging demonstrated that ICG-conjugated micelles have prolonged circulation time and increased tumor accumulation through the EPR effect. Compared with the control ICG solution, the NIR-irradiated ICG-conjugated micelles have improved therapeutic efficacy with complete tumor regression in an A375 human melanoma tumor model in athymic nude mice.
pH response
The abnormal metabolism and protein regulation of tumor tissues form an acidic microenvironment that favors the proliferation of tumor cells. This pH abnormality is widely exploited in tumor-targeted delivery. In the acidic microenvironment of tumors, nanocarrier structures can be changed by chemical bond dissociation or charge reversal for specific drug release.
To overcome the resistance of breast cancer to doxorubicin (DOX), which is currently the most widely used anti-cancer drug, Yu et al.14 constructed pH-sensitive microspheres that encapsulate DOX. The microspheres are formed by the self-assembly of polyethylene glycol (PEG)-block-poly[2-(diisopropylamino)ethyl methacrylate (PEG-b-PDPA)], and D-a-tocopheryl PEG 1000 succinate (TPGS). DOX is encapsulated in the cores of the microspheres. The microspheres are stable under the normal pH level of 7.4 but are degraded after cellular absorption. The early endosome and dissolved enzyme in tumor cells provide an acidic environment, which transforms the protonated PDPA/TPGS@DOX microspheres into micelles and releases DOX in the cells. At the same time, TPGS greatly reduces the toxicity of mitochondria, thus leading to the synergistic effect of the treatment.
Lee et al.15 designed pH-responsive intelligent microspheres Doxorubicin (DOX) loaded P(Asp-g-Im)-PEG micelles (DPHAIM, Figure 1) for the weakly acidic tumor microenvironment. With aspartic acid imidazole as the hydrophobic group and ethylene glycol as the hydrophilic group, the formed copolymer P(Aspg-Im)-PEG can load up to 28% DOX. In the pH<7 acid conditions of the tumor microenvironment, the microspheres are protonated and dissolved, thus releasing DOX and achieving the goal of targeted DOX delivery with reduced toxicity.
Schematic for the proposed in vivo behavior of DPHAIM. Reproduced with permission from Ref. 15.
Talelli et al.16 developed a multi-layer package for the targeted delivery of DOX and to overcome its serious side effects. DOX derivatives are introduced into the core of the polymer micelles by covalent coupling. Under weak acidic conditions, such as the tumor microenvironment and the endosome, covalent bonds are broken and free DOX derivatives are released. Experiments showed that only approximately 5% of the drug is released under pH 7.4 but is fully released within the same duration at pH 5 and 37°C. This result indicated the good characteristics of targeted drug delivery and reduced damage to normal tissues.
Numerous pH-responsive, intelligent nanoparticle delivery examples have been developed. A double-strand pH-sensitive DNA has been developed to release DOX to the tumor17. Jia et al.18 also designed a nanovehicle with hydrophilic methoxy poly(ethylene glycol) (mPEG)-PBA and hydrophobic HEHDO, which has a pH-labile profile. Torres et al.19 developed a pH-sensitive liposome system that accelerates cytosolic release at pH values of 5.5–6.0. Seib et al.20 synthesized silk nanoparticles with pH-dependent release (pH 4.5>6.0>7.4). Battogtokh et al.21 reported an acid-cleavable nanocarrier with enhanced cellular delivery at pH 6.5 compared with that at pH 7.4; by contrast, the cellular delivery of drugs by noncleavable nanocarriers showed no difference at pH 5.5 and pH 7.4. Tail vein injections enhance the intracellular uptake of the acid-cleavable nanocarrier relative to the noncleavable nanocarrier into the tumor cells of tumor-bearing mice, although total tumor accumulation is not significantly different. Van Butsele et al.22 reported the preparation and the aqueous solution properties of hybrid polymeric micelles that consist of a hydrophobic poly (ε-caprolactone) (PCL) core and a mixed shell of hydrophilic poly(ethylene oxide) and pH-sensitive poly (2-vinylpyridine).
Temperature response
The temperature of tumor tissues is slightly higher than that of surrounding normal tissues. This temperature difference can be applied in temperature-responsive drug delivery to tumors. Lv et al.23 developed a novel polymer system for intelligent drug release; the developed system is based on molecular recognition and phase transition temperature response (Figure 2). In their nanoparticle drug delivery system, magnetic Fe3O4 colloidal nanocrystal clusters (MCNCs) are used as the core, and poly (N-isopropylacrylamide) is used as a communication bridge between MCNCs and β-cyclodextrin (β-CD). β-CD can incorporate a number of hydrophobic groups and can easily load hydrophobic 8-anilino-1-naphthalenesulfonic acid ammonium salt (ANS) drugs. The conformation of MCNCs changes with the change in external magnetic field and temperature, thus decreasing the drug loadings of the whole system and consequently releasing ANS. The release rate of ANS from a drug nanoparticle system is easily controlled by simply adjusting external temperature. These nanoparticles have great potential for targeted delivery.
Schematic of the temperature-switched Fe3O4@PNG-CD nanosystem for controlled drug release. Reproduced with permission from Ref. 23.
Talelli et al.24 developed biodegradable thermosensitive polymeric micelles for the stable encapsulation of hydrophobic oleic-acid-coated superparamagnetic iron oxide nanoparticles (diameter 5-10 nm). The micelles are composed of amphiphilic, thermosensitive, and biodegradable block copolymers of poly (ethylene glycol)-b-poly[N-(2-hydroxypropyl) methacrylamide dilactate] [mPEGb-p(HPMAm-Lac2)]. Liu et al.25 developed a precision cancer nanomedicine based on Bi2S3 nanorods (NRs) designed specifically for multispectral optoacoustic tomography (MSOT)/X-ray computed tomography (CT). The as-prepared Bi2S3 NRs exhibit an ideal photothermal effect and contrast enhancement in MSOT/CT bimodal imaging.
Enzymatic response
Some enzymes are only present or are highly concentrated in tumor cells. Their specific binding with enzyme substrates can be employed to achieve the intelligent response of targeting drugs. Mi et al.26 constructed a multistage complex targeted drug delivery nanosystem enzyme-stimulated multistage vector (ESMSV) based on the special recognition between the enzyme and the appropriate substrate. A metalloproteinases-2 (MMP-2) enzyme substrate is modified on a polymer poly (lactic-co-glycolic acid) (PLGA)-PEG nanoparticle surface, followed by loading onto porous silicon. When ESMSV accumulates in pulmonary tumor tissues because of MMP2 enzymatic activity, the connecting structure between polymeric nanoparticles and porous silicon nanoparticles (SiNP) is destroyed, thus releasing poly nanoparticles from porous silicon. These processes have been validated both in vivo and in vitro. The results indicated that ESMSV showed noticeable efficacy in the treatment of metastatic lung melanoma.
Tang et al.27 reported a general strategy for the direct delivery of functional proteins to the cytosol by nanoparticle-stabilized capsules (NPSCs). The effectiveness of these NPSCs as therapeutic protein carriers has been demonstrated through the delivery of fully functionalized caspase-3 to HeLa cells with concomitant apoptosis. The similar delivery of green fluorescent protein confirmed the cytosolic delivery and intracellular targeting of the delivered protein, thus demonstrating the utility of the system for both therapeutic and imaging applications.
Barve et al.28 developed an enzyme-responsive peptide drug conjugate for TGX-D1, a promising PI3K inhibitor for prostate cancer. In this system, the LNCaP-specific KYL peptide is used as the targeting ligand and the prostate-specific antigen (PSA)-cleavable peptide (SSKYQSL) is used as the enzyme-responsive linker. Ruan et al.29 experimentally proved that pre-incubating G-AuNP-DOX-PEG with MMP-2 can significantly enhance the penetrating efficiency of the drug. Yu et al.30 developed surface-engineering nanoparticles with programmable extended circulation and targeting ability. The nanoparticles, which are structured with a targeting middle layer and a hydrophobic internal core, are constructed by mixing matrix metalloproteinase MMP2, MMP9-sensitive copolymers (mPEG-Pep-PCL), and folate receptor targeted copolymers (FA-PEG-PCL). The results showed the successful combination between enzymatic stimulus and surface-engineered technology for tumor targeting.
Antigen response
Similar to enzymes, the special identification and connection between antigens and antibodies can be exploited for the design of active targeting drug delivery. Ding et al.31 utilized the specific binding between a receptor and a ligand to realize targeted drug delivery. The authors combined immune nanoparticles containing the death receptor 5 monoclonal antibody (DR5 mAb) and nanoparticles carrying kappa oxazine (DTIC) to form the composite nanoparticle DTIC NP-DR5 mAb. The drug-loading nanoparticles accumulate in tumor cells due to the specificity of the monoclonal antibody and DR5 recognition effect in the body. This system is also a good example of the combined therapy of immune therapy and chemotherapy. The authors demonstrated that DTIC-PLA-DR5 mAb nanoparticles are an active targeting drug delivery system that can specifically target DR5-overexpressing malignant melanoma cells and can be efficiently internalized. Most strikingly, compared with conventional DTIC-NPs, DTIC-NP-DR5 mAb showed significantly enhanced cytotoxicity and increased cell apoptosis in DR5-positive malignant melanoma cells.
Saraf et al.32 synthesized cyclic Arg-Gly-Asp (RGD) micelles, which exhibit better targeting efficacy than linear RGD micelles as drug delivery vehicles. This improved targeting efficacy is attributed to the low drug solubilization and kinetic stability of the micelles. The results from the study proved the effectiveness of self-assembling low-molecular-weight RGD amphiphiles as carriers for the targeted delivery of paclitaxel (PTX).
Nanoparticle-based cancer therapy
Magnetic therapy
Tissues rarely absorb magnetic waves, which penetrate deeper than visible light and infrared without side effects. Therefore, magnetic nanomaterials are good candidates for disease treatment. Magnetic nanoparticles, which mainly contain iron oxide, can be used for localized heating when triggered by a magnetic field. Carregal-Romero et al.33 synthesized multilayer-assembled polyelectrolyte microcapsules with diameters of 4.6 µm. The walls of the microcapsules are integrated with 18 nm-diameter iron oxide nanotubes to supply a magnetic trigger for the release of molecules with low absorption and deep permeability. An organic fluorescent polymer (Cascade-Blue-labeled dextran) is then loaded onto the microcapsules as a model molecular cargo. Under an alternating magnetic field, the magnetic nanotubes can heat their surroundings and destroy the walls of the microcapsules, thus releasing the embedded cargo into the surrounding solution. The use of magnetic nanoparticles with high heating properties allows the release of the magnetic properties of the encapsulated material; moreover, this use provides the possibility of applying new and exciting materials in the body.
Fang et al.34 employed core-shell magnetoresponsive virus-mimetic nanocapsules (VNs) anchored with iron oxide nanoparticles for rapid and simultaneous drug release. The VNs produce a strong heating effect under an external high frequency magnetic field. Furthermore, the VNs can subsequently infect adjacent cancer cells and deliver sufficient therapeutic agents to the next target. Kuo et al.35 used Fe3O4 nanoparticles to encapsulate anticancer drugs and to immobilize the antibody-targeting peptide AP-1 (MPVA-AP1) to form multifunctional magnetic nanovehicles. The magnetic nanovehicles can be stably stored and exert thermotherapeutic (i.e., hyperthermia) and chemotherapeutic (i.e., anti-cancer drug) effects on tumor tissues under a high-frequency magnetic field. Lee et al.36 used magnetoretic-responsive DOX-encapsulated supramolecular magnetic nanoparticles (DOX-SMNPs) as a unique one-demand drug release system to enhance therapeutic effects and attenuate systematic toxicity to the tumor. The SMNPs self-assemble from four different molecular building blocks: Ad-grafted polyamidoamine dendrimers, β-CD-grafted branched polyethylenimine, Ad-PEG, and 6-nm Ad-grafted Zn0.4Fe2.6O4 superparamagnetic nanoparticles. Li and coworkers37 designed a magnetothermally responsive nanocarrier, in which NIPAAm and HMAAm are composed of thermosensitive copolymers and Mn-Zn ferrite nanoparticles are embedded in the polymer matrix. Under an alternating magnetic field, this system demonstrated efficient therapeutic effects and good biocompatibility.
Photodynamic therapy (PDT)
PDT can kill tumor cells through the transformation of tumor oxygen into cytotoxic reactive singlet oxygen (1O2) under light irradiation. PDT is a safe and selective treatment method for various cancer types. However, the efficacy of PDT in tumor therapy is limited due to the hypoxic microenvironment of tumors and oxygen consumption during PDT. To overcome this problem, Cheng et al.38 developed a novel oxygen self-enriched photodynamic therapy system by loading IR780 on perfluorohexane (PFH) nanodroplets. PFH can maintain a high oxygen content and extend1O2 lifetime because of its high oxygen capacity. The photosensitizer IR780 is dispersed in a lipid monolayer composed of lecithin, cholesterol, and DSPE-PEG2000. Under irradiation by a NIR 808-nm laser, IR780 transfers energy to the oxygen enriched in the PFH, thus producing singlet oxygen and exerting a cytotoxic effect, which significantly improves the photodynamic effect. After intratumoral injection into tumors, tumor growth is inhibited in Oxy-PDT-treated mice. Later, Gong et al.39 used PEGylated chlorine e6 (Ce6)-coupled poly (maleic anhydridealt-1-octadecene) to form Ce6-containing nanomicelles in an aqueous solution (Figure 3) and discovered that hyaluronidase resolves hyaluronan, a major component of extracellular matrix in tumors. The complex enhances the efficacy of nanoparticle-based PDT for in vivo cancer treatment.
Scheme showing the effects of HAase on the modulation of the tumor microenvironment. By improving tumor oxygenation and promoting the EPR effect, HAase enhances the efficacy of in vivo PDT cancer treatment. Reproduced with permission from Ref. 39.
Hou et al.40 developed a nanodumbbell model, which consists of a hydrophobic upconversion nanoparticle (UCN) core and a hydrophilic polymersome shell. UCN NaYF4:Yb:Er nanocrystals, which were synthesized via the thermal decomposition method, can be used as transducers to convert NIR light to visible light to activate the photosensitizers zinc (II) phthalocyanine (ZnPc) in photodynamic therapy. The polymersome lipid shell is used to load ZnPc and to avoid non-specific absorbance or corrosion during transportation. In addition, folic acid may combine with hybrid Fe3O4-ZnO (FZ-SFA) nanoparticles in therapeutic applications associated with PDT41. The photo-killing effect and photo-induced toxicity are significantly enhanced under UV irradiation. To increase the production of reactive oxygen species (ROS) under normoxic and hypoxic conditions, Usacheva et al.42 used a polymer-surfactant nanoparticle system to load the photosensitizer methylene blue. Nanoparticles loaded with methylene blue can remove cancer stem cells under hypoxic conditions, therefore providing a novel route for cancer treatment.
Photothermal therapy (PTT)
In PTT, cancer tissues are irradiated with electromagnetic radiation, which elevates temperature to kill targeted cells. In this method, the careful selection of laser parameters and illumination can enable local light penetration for specific targeting.
One of the most promising directions for PTT is the use of plasma nanostructures, particularly gold nanostructures, such as gold nanoparticles (AuNPs) and gold nanoshells, to take the advantage of localized surface plasmon resonance. In addition, visible light with a longer wavelength or NIR can be used in PTT since they have a deep tissue permeation and low energy, which causes limited damage to other cells and tissues.
Chen et al.43 combined NaYF4:Yb3+/Er3+ nanoparticles with AuNPs and gold NRs (GNRs) coated with silica shells. The surfaces of the nanocomposites were then decorated with folic acid through multiple steps to form UCP@SiO2-NP-FA and UCP@SiO2-NR-FA (Figure 4). NaYF4:Yb3+/Er3+ nanoparticles act as light converters and emit green and red light under 980 nm laser excitation. The silica shell increases biocompatibility and connects the nanoparticles and Au nanomaterials. This system exhibits significantly enhanced therapeutic efficacy.
Schematic of the synthetic process of UCP@SiO2-NPs and UCP@SiO2-NRs and application in the PTT of oral cancer. Reproduced with permission from Ref. 43.
Many other nanomaterials have been applied in PPT. Yang et al.44 developed a double-shelled hollow sphere structure with luminescent Y2O3:Yb, Er as the inner shell and mesoporous silica as the outer shell. The surface of Y2O3:Yb, Er@mSiO2 was then decorated with ultra small CuxS (semiconductor) nanoparticles (photothermal agents) and DOX to form a DOX-DSHS-CuxS composite. When irradiated with 980 nm NIR light, the composite showed high anti-cancer efficacy and biocompatibility in vitro and in vivo. AuNPs may also specifically conjugate with a thermally sensitive elastin-like polypeptide (ELP) to form ELP-AuNPs45. The ELP-AuNPs, which contain short-necked gold nanostructures formed in situ at high temperatures by AuNP assemblies, exhibit strong NIR absorption and high light-heat effect, therefore enhancing therapeutic effect. Prussian blue nanoparticles are utilized as PTT agents in combination with MEK inhibitor and PD-032590146. This combined system inhibits tumor growth and increases survival rate by blocking MEK activity under NIR irradiation.
Radiotherapy (RT)
RT is a popular remote cancer treatment method that induces DNA damage or free radical damage in tumor sites. However, it causes severe side effects in patients. Protecting normal tissue adjacent to the tumor site from radiation damage remains challenging. Many approaches have been recently developed to improve the effect of RT and to decrease its side effects.
Yu and coworkers[47] used MPEG-PCL to prepare PTX-NPs via the solid dispersion method. Although PTX is one of the most common antineoplastic drugs, its therapeutic effect is limited because of its short circulation half-life, poor water solubility, and serious side effects. With the rapid development of nanotechnology, nanoscale drug delivery systems now offer an alternative solution for drug transport to tumor tissues. Yu et al.47 demonstrated that PTX-NPs inhibit tumor growth by acting on Ki-67 and inhibit angiogenesis in tumor tissues through RT. PTX-NPs combined with RT exhibit higher efficiency in cancer therapy than PTX-NPs or RT alone. Satterlee et al.48 used lipid-calcium-phosphate nanoparticles in combination with177Lutetium (177Lu) for RT. Combretastatin A-4 phosphate was loaded onto nanoparticles to increase the enrichment of nanoparticles. Through the beta decay of 177Lu, the combined system exerts significant inhibitory effects on tumor cell growth, as well as increases tumor EPR effect and nanoparticle uptake.
Zhang et al.49 developed dual functional mesoporous silica nanoparticles (MSNs), by dissolving MSNs in valproic acid sodium salt solution to form VPA-MSNs. The developed VPA-MSNs enhance tumor cell death and decrease damage to healthy adjacent tissues by targeting cancer cells with overexpressed folic acid and by conditionally releasing VPA in an acidic turmeric microenvironment. Song et al.50 developed epidermal growth factor (EGF)-AuNPs that consist of AuNPs as radiosensitizers and EGF. EGF was modified with diethylenetriaminepentaacetic dianhydride (DTPA) to form DTPA-EGF, which was further labeled with 111In. 111In-EGF-Au NPs specifically target EGFR-positive cancer cells and enhance cell death by increasing radiotoxicity with a high111In payload. Song et al.51 prepared PEG-stabilized perfluorocarbon (PFC) nanodroplets decorated with TaOx nanoparticles as a multifunctional RT sensitizer. The complex improved in vivo RT treatment by concentrating radiation energy and improving tumor oxygenation.
Ultrasound (US)
US is a conventional method for cancer diagnosis and treatment. It can form cavitation bubbles, heat local tissues, and produce radiation force, which are used to release drugs from nanocomposites, to purify drugs and/or nanoparticles from blood vessels in tumors, and to improve drug penetration to the tumor. Wang et al.52 developed an efficient strategy to overcome multi-drug resistance (MDR) by combining negatively charged nanoparticles with US. In their study, cells are exposed to US with microbubbles prior to treatment with negatively charged Heparin-Folate-Tat-Taxol nanoparticles. This work reported that the optimal reversal of the MDR effect occurs through the enhancement of cell membrane permeability, the inhibition of cell proliferation rate, and the downregulation of the genes and proteins associated with MDR. Furthermore, US enhances the accumulation of nanoparticles by indirectly inducing the endosomal escape of negatively charged nanoparticles. The combined strategy can potentially overcome the MDR problem in cancer therapy. Sviridov et al.53 prepared SiNPs by mechanically grinding luminescent porous silicon decorated with dextran. They found that dextran-coated SiNPs could significantly decrease cytotoxicity. After SiNP uptake, cells were treated with therapeutic US for 5–20 min. The living cells decreased whereas the total cells was almost unchanged, indicating the potential of the system as a mild cancer therapy. Brazzale et al.54 used folic acid to decorate AuNPs surface-coated with PEG to stabilize the colloid and prevent opsonization in vivo. The nanoparticles, as US sensitizers, can specifically act on KB and HCT-116 cells and inhibit cell growth by generating reactive oxygen and increasing cell necrosis.
Combined cancer therapy
Although nanoparticle-based cancer therapies have already demonstrated intriguing therapeutic efficacies, researchers continue to pursue an ideal synergistic effect by combining two or more treatment methods. Significantly enhanced anti-tumor efficacy has been achieved by combined treatment strategies.
PTT and PDT combined therapy
Qiu et al.55 devised a GNR-activated, cell-penetrating peptide-protoporphyrin (GNR-ACPP-PpIX) nanoplatform that can be applied for dual imaging and combined activatable PDT/PTT therapy (Figure 5A). In GNR-ACPI, GNRs are conjugated with a protoporphyrin (PpIX, a PDT agent) combined with ACPP. The ACPP comprises a matrix of the MMP-2-sensitive peptide sequence GPLGLAG. First, the special “U-type” structure of ACPP facilitates close contact between PpIX and GNR. As tumor cells can overexpress MMP-2, the GPLGLAG sequence is hydrolyzed by MMP-2 as soon as it arrives at the tumor site, leading to the release of residual CPP bound to PpIX (CPP-PpIX) and the recovery of the optical activity of PpIX. Moreover, with the help of CPP, the cellular uptake of PpIX by tumor cells can be more efficient, greatly enhancing PDT efficacy. GNR can also be used for photothermal imaging and PTT in the treatment of tumors. Experimental results show that the combination of PTT and PDT can greatly enhance the anti-tumor effect with negligible systemic toxicity.
(A) Construction of the GNR-ACPI nanoplatform. (B) Dual-mode imaging and combined PTT/PDT therapy in vivo after the intravenous injection of GNR-ACPI. (B1) Accumulation of GNR-ACPI in the tumor site through the EPR effect. (B2) Enhanced internalization of activated CPP-PpIX by tumor cells via the help of CPP and triggered by the combination of PTT/PDT therapy upon laser irradiation. Reproduced with permission from Ref. 55.
Other PDT/PTT combined cancer therapy strategies and applied nanoparticle systems include: cyanine dye-integrated micelles loaded on photosensitizers as potential theranostic micelles56; Cit/CuS@Fe3O4-based nanoparticles for PDT/PTT therapy with magnetic-targeting capability57; collagen-gold hybrid hydrogels58; Au NR-capped and Ce6-doped mesoporous silica NRs; and Au NR-capped and Ce6-doped mesoporous silica nanorods59.
Chemotherapy and PTT combined therapy
In malignant glioma, treatment effect and patient compliance are unsatisfactory due to low efficiency and systemic side effects of treatment methods. Wang et al.60 combined the chemo-photothermal targeted therapy of glioma with a novel multifunctional drug delivery system. A targeting peptide-modified graphene nanosheet coated with mesoporous silica (GSPI) was successfully synthesized. The developed DOX-loaded GSPI system (GSPID) showed good heat-stimulative, pH-responsive, and sustained release properties. Based on the results of cytotoxicity experiments, glioma cells treated with the combined therapy showed higher mortality rates than those treated with single chemotherapy or PTT alone. In addition, peptide modification significantly enhanced GSPID accumulation in glioma cells. GSPID demonstrated advanced chemo-photothermal synergistic targeted therapy and good drug release properties, providing an excellent drug delivery system for the combined therapy of glioma. In addition, this therapy can effectively avoid frequent and invasive dosing and improve patient compliance.
Shao et al.61 constructed a polydopamine-functionalized reduced graphene oxide (pRGO) with mesoporous silica (MS) coating. pRGO was further modified with hyaluronic acid (HA) to form pRGO@MS (DOX)-HA nanocomposites, a multimodal therapy system and a multifunctional drug delivery system. These nanoparticles exhibit efficient synergistic targeted chemo-PTT. With mussel-inspired dopamine as the reducing reagent, the functionalized biomolecule was prepared as biocompatible biopolymer-coated RGO nanosheets in one step. Mesoporous silica (MS) was then coated with pRGO to enhance DOX loading and to provide an active interface for modification with HA, the targeting moiety. The pRGO@MS (DOX)-HA showed excellent photothermal properties and good dispersibility under NIR laser irradiation. Gao et al.62 developed a thermal/pH dual-sensitive nanocarrier for the treatment of bladder cancer. Their results revealed that chemo/photothermal targeted therapy might be more advantageous than conventional therapeutics for bladder cancer. Meng et al.63 designed and synthesized a “smart” MEO2MA@MEO2MA-co-OEGMA-CuS-DOX composite (abbreviated as G-CuS-DOX). The nanoparticles consisted of thermosensitive MEO2MA@MEO2MA-co-OEGMA nanogels, with a low critical solution temperature of 42°C, CuS as the photothermal component, and DOX as the anticancer drug. Upon the injection of the nanocapsule solution into tumors in mice, DOX is released and temperature elevation in the tumor can be switched on/off by an ex vivo NIR laser, thus exhibiting an efficient synergistic photothermal/chemotherapy for tumors. Shen et al.64 studied the in vivo and in vitro ablation of the tumor via combined chemotherapy and PTT with DOX-loaded GNRs@mSiO2. Feng et al.65 designed a magnetic tumor-targeting and NIR-responsive drug delivery system. This nanoplatform can generate improved photothermal transduction efficiency in a short time, and DOX is spontaneously released due to photohyperthermia with the spatiotemporal control of NIR irradiation.
Chemo-photodynamic combined therapy
Advanced colorectal cancer is one of the deadliest cancers. Traditional treatments, such as the inhibition of the PD-1/PD-L1 axis by antibodies, remain the most promising immunotherapies, but the sustained response rate of these therapies is very low. He et al.66 developed nanoscale coordination polymer (NCP) core-shell nanoparticles, which carry oxaliplatin in the core and the photosensitizer pyropheophorbide-lipid conjugate (pyrolipid) in the shell (NCP@pyrolipid), for PDT, chemotherapy, and PD-L1 checkpoint blockade cancer therapy. NCP@pyrolipid has high drug loading and long circulation. It can also avoid being salvaged in the body; hence, it can be enriched in the tumor site. Research showed that upon subcutaneous injection in CT26 and HT29 mouse models, the PDT effect of NCP@pyrolipid effectively inhibits tumor growth. Moreover, the combination of oxaliplatin and PDT creates an immune microenvironment in the tumor site, significantly increasing the efficacy of the PD-L1 checkpoint blockade therapy. This strategy greatly increases the curative effect of tumor treatment strategies.
Dong et al.67 introduced UCNs that were surface modified with bovine serum albumin-poly (ε-caprolactone) BSA-PCL, and achieved a combined system of tumor cell imaging, photodynamic therapy, and chemotherapy. The UCN core comprises a protein-polymer bioconjugate-coated multifunctional upconversion nanosystem. The antitumor drugs DOX and ZnPc are co-loaded in the tailored amphiphilic protein-polymer bioconjugate shell. In this structure, the UCN core converts NIR light to visible light, thus allowing for cell fluorescence imaging, whereas activated ZnPc generates cytotoxic ROS to achieve photodynamic therapy. The BSA-PCL system exhibits good stability, water solubility, and low cytotoxicity. Similarly, Ai et al.68 assembled biocompatible core-shell-shell UCNs (NaGdF4:Yb/Nd@NaGdF4:Yb/Er@NaGdF4) loaded with photosensitizers and Pt (IV) prodrugs for simultaneous PDT and Pt chemotherapy. Chen et al.69 developed a type of theranostic micelle based on multifunctional UCN, which combines chemotherapy and PDT for NIR-controlled and neuroendocrine tumor targeting. Feng et al.70 prepared a nanovehicle that can co-deliver the photosensitizer pyropheophorbide-a (PPa) and the drug PTX through the synthesis of PPa-conjugated amphiphilic copolymer PPa-PLA-PEG-PLA-PPa. The nanovehicle has a high drug-loading capacity for both drugs. Decorating the obtained nanoparticles with the tumor-targeting and penetrating peptide F3 achieved tumor-targeting therapy.
Immunotherapy and photothermal combined therapy
The immunotherapy and PTT bined therapeutic strategy can inhibit tumor metastasis and eliminate primary tumors through the combination of adjuvant nanoparticle-based PTT with checkpoint-blockade immunotherapy. Chen et al.71 developed a class of PLGA-ICG-R837 nanoparticles, in which PLGA co-encapsulated imiquimod (R837) serves as a Toll-like-receptor-7 agonist and ICG serves as a photothermal agent. When excited by NIR light, the nanoparticles can generate a photothermal effect to eliminate the main tumor, and the contained R837 produces tumor-associated antigens and behaves as a vaccine. Anti-cytotoxic T-lymphocyte antigen-4 has been used as the checkpoint-blockade, which produces an immune response in mice to eliminate remaining tumor cells and to inhibit metastases. Moreover, this strategy is suitable for various kinds of tumor models and has the advantage of immune memory (Figure 6).
Mechanism of anti-tumor immune responses induced by PLGA-ICG-R837-based PTT in combination with checkpoint-blockade. Reproduced with permission from Ref. 71.
Whole tumor cell lysate (TCL) has been used as a tumor antigen for the development of cancer vaccines. Shi et al.72 designed chitosan nanoparticles (CTS NPs) with surface mannose (Man) moieties (Man-CTS NPs) for the specific targeting of dendritic cells. The Man-CTS NPs were then loaded with TCL generated from B16 melanoma cells (Man-CTS-TCL NPs). TCL improves the efficacy of TCL-based vaccines as a result of the effective activation of humoral and cellular immunity. The traditional anti-fibroblast-activation protein (FAP) treatment is associated with numerous side effects. Studies have shown that FAP is excessively expressed on the surface of carcinoma-associated fibroblasts (CAFs); therefore, FAP can be used as a target antigen in tumor cells. Zhen et al.73 reported a photoimmunotherapy (PIT) approach based on nanoparticles. The author applied ferritin, a compact nanoparticle protein cage, as the photosensitizer carrier connected with a FAP-specificity single-variable region (scFv). Under photoirradiation, nanoPIT can effectively eliminate CAFs in tumors but not harm healthy tissues due to localized targeting. The nanoPIT effectively suppresses tumor growth by inhibiting the secretion of C-X-C motif chemokine ligand (CXCL12), thus enhancing T cell infiltration and in turn decreasing the number of tumor cells. Cano-Mejia et al.74 combined Prussian-blue-nanoparticle-based PTT and anti-CTLA-4 checkpoint inhibition for neuroblastoma treatment. The strategy can lead to an immune response and decrease tumor burden. Huo et al.75 proposed a PLGA-PEG-MBA micelle system for the implementation of the tumor-targeted delivery of a low dose of sunitinib. The therapy can decrease the number of MCSCs and Tregs in the tumor microenvironment, increase T-cell infiltration in the tumor site, and eliminate immunosuppression in the tumor site.
Diagnosis and PTT
The early detection or diagnosis of disease and the precise monitoring of therapeutic effects on lesions after treatment are critical to improve the effectiveness of cancer treatment. Combined diagnosis and treatment has become an important cancer therapy strategy. Liu et al.76 prepared ultrasmall Cu3BiS3 nanodots (NDs), single-phased ternary bimetal sulfide nanomaterials that are powerful, degradable, and safe nanomedicine for PTT-guided MSOT and X-ray CT. The authors demonstrated that Cu3BiS3 NDs could be quickly degraded through renal clearance. The metabolic behavior of NDs, which have low toxicity, from biological and chemical aspects was monitored through CT and X-ray absorption near-edge spectroscopy. Moon et al.77 reported a system of reduced graphene oxide-coated gold nanorods (r-GO-AuNRs) which has a strongly amplified photoacoustic (PA) performance provided by the excellent NIR light absorption and photothermal stability of the reduced graphene oxide layer. Chen et al.78 proposed a nanosystem composed of human serum albumin (HSA), PTX, and ICG; this system can self-assemble into stable nanoparticles. ICG acts as a photothermal agent and a fluorescence imaging probe. The obtained HSA-ICG-PTX nanoparticles have good stability and long circulation. The heat generated by ICG under NIR laser irradiation promotes the uptake of HSA-ICG-PTX nanoparticles and tumor cell death.
Wang et al.79 designed a Gd-hybridized plasmonic Au-nanocomposite system, where citrate-Gd complexes and DOX are co-loaded on mesoporous silica-coated AuNR. Under NIR laser irradiation, the mild heat produced by nanoparticles enhances circulation and targets drug delivery to the tumor site. The nanocomposite materials promote five imaging or analysis techniques: tumor diagnosis by CT and MRI, therapeutic responses by PA imaging, synchrotron radiation (SR), X-ray fluorescence mapping, and SR scanning-transmission X-ray microscopy imaging. Yang et al.80 developed a polymer micelle system for dual NIR fluorescence imaging and the PTT of tumors. The copolymers, which consist of monomethoxy poly (ethylene glycol) and alkylamine-grafted poly (L-aspartic acid), form theranostic micelles by assembly with carbocyanine dyes. Given their small size, high loading capacity, good stability, and sustained release, the micelles can enhance the cellular uptake of micelles and achieve better biological distribution and the long-term retention of cyanine dye in the tumor site, thus enhancing NIR fluorescence imaging. In addition, the stability of subcellular organelles is destroyed under photoirradiation, resulting in severe photothermal damage to cancer cells.
Conclusions and perspectives
More and more nanoparticles tuned for diverse nanomedicine applications have emerged, thus suggesting the potential development of multifunctional “smart” nanoparticle drug delivery systems that may facilitate individualized cancer therapy. Various types of nanoparticles have been evaluated for their suitability for simultaneous in vivo imaging and the treatment of cancers with improved efficacy.
Although nanoparticles have raised exciting expectations for cancer diagnosis and treatment, challenges continue to exist and arise, especially in achieving practical application in living organisms. Nevertheless, current research studies are closer than ever to solving these issues and achieving practical nanotherapy for cancer. Prospective directions for the development in this field include the specific accumulation of nanoparticles solely in malignant cells; the real-time imaging and monitoring of treatment effects in vivo; and killing the cancer cells with minimal side effects by sparing normal cells.
Footnotes
Conflict of interest statement No potential conflicts of interest are disclosed.
- Received April 29, 2017.
- Accepted May 24, 2017.
- Copyright: © 2017, Cancer Biology & Medicine
This is an open access article distributed under the terms of the Creative Commons Attribution License (CC BY) 4.0, which permits unrestricted use, distribution and reproduction in any medium, provided the original author and source are credited.
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