Cytotoxicity of titanium dioxide nanoparticles differs in four liver cells from human and rat

Titanium dioxide (TiO₂) nanoparticles (NPs) are the important nanoscale components of composites. Although TiO₂ NPs and their related nanocomposites have been widely used in industrial and medical applications, the adverse effects of TiO₂ nanomaterials have not been well studied. Here, we investigated the cytotoxicity of TiO₂ NPs in vitro using four liver cell lines: human hepatocellular carcinoma cell line (SMMC-7721), human liver cell line (HL-7702), rat hepatocarcinoma cell line (CBRH-7919) and rat liver cell line (BRL-3A). We checked cell viability, cell morphology, and the levels of reactive oxygen species (ROS) and glutathione (GSH) after TiO₂ exposure at varying concentrations (0.1–100 μg/mL) and different exposure periods of time (12–48 h). Compared to the NP-free control, all four cell lines exposed to TiO₂ NPs showed cytotoxicity in a dosage-dependent and time-dependent manner, which was associated with the changes of cell viability and cell morphology, increased intercellular ROS levels, and decreased intracellular GSH levels. Further, we observed that carcinomatous liver cells and human liver cells exhibited more tolerance to TiO₂ NPs exposure for 24 h, compared to normal liver cells and rat liver cells, respectively. The results indicate that the in vitro cytotoxicity induced by NPs should be assessed with great caution before the use of nanocomposites and that there is a need to standardize the cytotoxicity testing procedure of nanoscale components in composites when using different cell lines.     

PEGylated TiO2 nanoparticles mediated inhibition of cell migration via integrin beta 1

Nanoparticles (NPs) elicit various physiological responses in cellular environment, and the effect of NPs on cell migration is of high interest. In this work, the effects of NPs on cell migration and their possible mechanisms were studied. Here, we showed that after exposure to pegylated titanium dioxide nanoparticles (TiO₂-PEG NPs, where PEG stands for the polyethylene glycol), NCI-H292 cells exhibited slower migration than control cells. Furthermore, larger NPs inhibited cell migration much stronger than smaller NPs. Following NP exposure, the cells showed decreased expression of integrin beta 1 and phosphorylated focal adhesion kinase (pFAK), and disrupted F-actin structures. We demonstrated that a possible mechanism involved NP-mediated promotion of the lysosomal degradation of integrin beta 1, thus leading to reduced expression of pFAK and cytoskeletal disruption and inhibited cell migration. Therefore, our results showed that inhibition of NCI-H292 cell migration by NPs is mediated through integrin beta 1, which provides useful information for the application of NPs in cancer therapy and related fields.     

Quantitative Proteomics Study Reveals Changes in the Molecular Landscape of Human Embryonic Stem Cells with Impaired Stem Cell Differentiation upon Exposure to Titanium Dioxide Nanoparticles

The increasing number of nanoparticles (NPs) being used in various industries has led to growing concerns of potential hazards that NP exposure can incur on human health. However, its global effects on humans and the underlying mechanisms are not systemically studied. Human embryonic stem cells (hESCs), with the ability to differentiate to any cell types, provide a unique system to assess cellular, developmental, and functional toxicity in vitro within a single system highly relevant to human physiology. Here, the quantitative proteomics approach is adopted to evaluate the molecular consequences of titanium dioxide NPs (TiO₂ NPs) exposure in hESCs. The study identifies ≈328 unique proteins significantly affected by TiO₂ NPs exposure. Proteomics analysis highlights that TiO₂ NPs can induce DNA damage, elevated oxidative stress, apoptotic responses, and cellular differentiation. Furthermore, in vivo analysis demonstrates remarkable reduction in the ability of hESCs in teratoma formation after TiO₂ NPs exposure, suggesting impaired pluripotency. Subsequently, it is found that TiO₂ NPs can disrupt hESC mesoderm differentiation into cardiomyocytes. The study unveils comprehensive changes in the molecular landscape of hESCs by TiO₂ NPs and identifies the impact which TiO₂ NPs can have on the pluripotency and differentiation properties of human stem cells.     

Growth of ZnO nanorods on TiO2 nanoparticles films and their application to the electrode of dye-sensitized solar cells

A ZnO nanorods (NRs)/TiO₂ nanoparticles (NPs) film has been prepared by electrochemical deposition of ZnO NRs growth on P25 TiO₂ NPs film surfaces. It was found that ZnO NRs/TiO₂ NPs could significantly improve the efficiency of dye-sensitized solar cells owing to its relatively enhanced light-scattering capability and efficient charge transport efficiency. The overall energy-conversion efficiency (η) of 3.48 % was achieved by the formation of ZnO NRs/TiO₂ NPs film, which is 33 % higher than that formed by TiO₂ NPs alone (η = 2.62 %). The charge recombination behavior of cells was investigated by electrochemical impedance spectra, and the results showed that ZnO NRs/TiO₂ NPs film has the longer electron lifetime than TiO₂ NPs alone, which could facilitate the reduction of recombination processes and thus would promote the photocatalysis and solar cell performance.     

Effect of particle size on in vitro cytotoxicity of titania and alumina nanoparticles

Aluminium oxide (Al₂O₃) and titanium dioxide (TiO₂) nanoparticles (NPs) have been widely used in nanotechnology-based products. Recently, researchers and the public have raised concerns about the adverse effects of these NPs in biological systems, particularly in humans. The aim of this study was to investigate the possible adverse effects of these two common metal oxide NPs on human lung epithelium cells (A549) and to investigate NP size-dependent effects on these cells, considering both the primary and hydrodynamic particle size. NPs were found to inhibit cell viability and proliferation at the highest concentration level (10?mg/mL) included in this study, as measured by a clonogenic assay. Moreover, cell viability, proliferation and metabolism were impaired to a greater extent by the smaller NPs (5?nm TiO₂ and 10?nm Al₂O₃) relative to the larger particles (200?nm TiO₂ and 50?nm Al₂O₃) included in this study, as measured by cell proliferation and metabolism. Notably, the observed cytotoxic effects correlated to the primary size, rather than the hydrodynamic size. Similarly, NP cytotoxicity was found to be correlated with the NP surface area. These findings highlight the importance of including primary size and surface area information in NP characterisation in cytotoxicity studies.     

Toxicological Aspects of Long‐Term Treatment of Keratinocytes with ZnO and TiO2 Nanoparticles

Sunscreens containing ZnO and TiO₂ nanoparticles (NPs) are increasingly applied to skin over long time periods to reduce the risk of skin cancer. However, long‐term toxicological studies of NPs are very sparse. The in vitro toxicity of ZnO and TiO₂ NPs on keratinocytes over short‐ and long‐term applications is reported. The effects studied are intracellular formation of radicals, alterations in cell morphology, mitochondrial activity, and cell‐cycle distribution. Cellular response depends on the type of NP, concentration, and exposure time. ZnO NPs have more pronounced adverse effects on keratinocytes than TiO₂. TiO₂ has no effect on cell viability up to 100 μg mL^?1, whereas ZnO reduces viability above 15 μg mL^?1 after short‐term exposure. Prolonged exposure to ZnO NPs at 10 μg mL^?1 results in decreased mitochondrial activity, loss of normal cell morphology, and disturbances in cell‐cycle distribution. From this point of view TiO₂ has no harmful effect. More nanotubular intercellular structures are observed in keratinocytes exposed to either type of NP than in untreated cells. This observation may indicate cellular transformation from normal to tumor cells due to NP treatment. Transmission electron microscopy images show NPs in vesicles within the cell cytoplasm, particularly in early and late endosomes and amphisomes. Contrary to insoluble TiO₂, partially soluble ZnO stimulates generation of reactive oxygen species to swamp the cell redox defense system thus initiating the death processes, seen also in cell‐cycle distribution and fluorescence imaging. Long‐term exposure to NPs has adverse effects on human keratinocytes in vitro, which indicates a potential health risk.     

Role of toll-like receptors 3, 4 and 7 in cellular uptake and response to titanium dioxide nanoparticles

Innate immune response is believed to be among the earliest provisional cellular responses, and mediates the interactions between microbes and cells. Toll-like receptors (TLRs) are critical to these interactions. We hypothesize that TLRs also play an important role in interactions between nanoparticles (NPs) and cells, although little information has been reported concerning such an interaction. In this study, we investigated the role of TLR3, TLR4 and TLR7 in cellular uptake of titanium dioxide NP (TiO₂ NP) agglomerates and the resulting inflammatory responses to these NPs. Our data indicate that TLR4 is involved in the uptake of TiO₂ NPs and promotes the associated inflammatory responses. The data also suggest that TLR3, which has a subcellular location distinct from that of TLR4, inhibits the denaturation of cellular protein caused by TiO₂ NPs. In contrast, the unique cellular localization of TLR7 has middle-ground functional roles in cellular response after TiO₂ NP exposure. These findings are important for understanding the molecular interaction mechanisms between NPs and cells.     

Studies on interfacial interactions of TiO2 nanoparticles with bacterial cells under light and dark conditions

The probable underlying mechanism(s) of bacterial cell–TiO₂ nanoparticles (TiO₂ NPs) interaction in the absence of photo-irradiation has been less studied since most of the prior cytotoxicity studies focused on irradiated TiO₂. The present study draws attention to the possible role of cell surface–TiO₂ NP interactions under dark conditions, through an array of spectroscopic and microscopic investigations. A dominant freshwater bacterial isolate, Bacillus licheniformis, which interacted with environmentally relevant concentrations of TiO₂ NPs (1 μg/mL), was analysed and compared under both light and dark conditions. Aggregation of cells upon NP interaction and adsorption of NPs onto the cell membrane was evident from the scanning electron micrographs under both light and dark conditions. The FT–IR and FT–Raman spectra suggested stress response of bacterial cells by elevated protein and polysaccharide content in the cell–NP interaction. The Xray photoelectron spectroscopic data substantiated the reduction of titanium from Ti(IV) to Ti(III) species which might have contributed to the redox interactions on the cell surface under light as well as dark conditions. The internalization of NPs in the cytoplasm were obvious from the transmission electron micrographs. The consequent cell death/damage was confirmed through fluorescence spectroscopy and microscopy. To conclude, the current study established the substantial role of interfacial interactions in cytotoxicity of the TiO₂ NPs irrespective of the irradiation conditions.     

Label‐free and dynamic monitoring of cytotoxicity to the blood–brain barrier cells treated with nanometre copper oxide

A cytotoxicity study was conducted with a primary culture of the nervous system cells, including brain microvascular endothelial cells (BMECs) and astrocytes, which are important components of the blood–brain barrier. The real‐time cell analysis (RTCA) was used to determine the cytotoxicity of copper‐oxide nanoparticles (CuO NPs). The IC₅₀ values of CuO NPs in astrocytes and BMECs were determined by the RTCA at different exposure times and were used as base values for further research. DNA damage after exposure to CuO NPs for 3 and 24 h was assessed using comet assay at the IC₅₀ obtained from RTCA. The onset time of cytotoxicity induced by CuO NPs was 2 and 2–4 h post‐exposure in BMECs and astrocytes, respectively. Furthermore, the degree of cytotoxicity induced by exposure to CuO NPs for 24–48 h in the BMECs and astrocytes was similar. Treatment with CuO NPs at 1/2*IC₅₀ and 1/5*IC₅₀ for 3 h induced genotoxicity in both cells as assessed by a measurement of DNA damage, although no cytotoxicity was observed. However, significant DNA damage was observed at all concentrations of CuO NPs used in this study, when the treatment time was 24 h.Inspec keywords: biochemistry, blood, brain, cellular biophysics, copper compounds, DNA, molecular biophysics, nanoparticles, toxicologyOther keywords: label‐free cytotoxicity monitoring, dynamic cytotoxicity monitoring, blood‐brain barrier cells, nervous system cells, brain microvascular endothelial cells, astrocytes, real‐time cell analysis, copper‐oxide nanoparticles, comet assay, genotoxicity, DNA damage measurement, time 24 h to 48 h, time 2 h to 4 h, CuO     

Analysis of the cytotoxicity of differentially sized titanium dioxide nanoparticles in murine MC3T3-E1 preosteoblasts

There is an increased use of nanophase titanium dioxide (TiO₂) in bone implants and scaffolds. However, nano-debris is generated at the bone-biomaterial interface. Therefore, TiO₂ nanoparticles (NPs) of many sizes were investigated for cytotoxic effects on murine MC3T3-E1 preosteoblasts. These TiO₂ NPs induced a time- and dose-dependent decrease in cell viability. There was a significant increase in lactate dehydrogenase (LDH) release, apoptosis and mitochondrial membrane permeability following short-term exposure of the cells to TiO₂ NPs. These NPs also increased granulocyte-macrophage colony stimulating factor (GM-CSF) and granulocyte colony-stimulating factor (G-CSF) gene expression. Compared with the 32 nm TiO₂ NPs, 5 nm TiO₂ NPs were more toxic, induced more apoptosis, increased mitochondrial membrane permeability and stimulated more GM-CSF expression at a high concentration (≥100 μg/ml). The results implied that the differential toxicity was associated with variations in size, so more attention should be given to the toxicity of small NPs for the design of future materials for implantation.     

Toxicological impact of TiO2 nanoparticles on Eudrilus euginiae

The concern regarding the toxicological effects of nanoparticles (NPs) on the terrestrial environment is increasing. To avoid risks of exposure to these NPs in the environment, it is essential to develop an understanding of their reactivity, toxicity, and persistency. Due to the increased usage of nano‐titanium dioxide (TiO₂) in various industrial products, an exponential increase in exposure is expected, which would exacerbate concerns about its ecological risks. The present study is conducted to evaluate the size‐dependent effects of TiO₂ NPs on the soil, especially on earthworm (Eudrilus euginiae). To date, many studies have been reported on the impact of TiO₂ NPs on ecotoxicology. However, histotoxicology studies are sparse. This study serves to be the first report on the size‐dependent histotoxicological impact of nano‐TiO₂ on earthworms particularly, E. euginiae. This report presents an intensive overall view of the longer time ecotoxicological impact of TiO₂ nanomaterials on various biological parameters of earthworms at cellular levels. The results show that the survival and growth of adult earthworms are severely affected by the TiO₂ NPs in the soil, which substantiates the adverse effects of TiO₂ NPs on earthworms.Inspec keywords: nanobiotechnology, nanoparticles, titanium compounds, semiconductor materials, toxicology, zoology, soil, cellular biophysics, particle sizeOther keywords: toxicological impact, nanoparticles, Eudrilus euginiae, terrestrial environment, soil, earthworm, ecotoxicology, size‐dependent histotoxicological impact, nanomaterials, biological parameters, cellular levels, TiO₂      

Mechanistic Investigation of the Biological Effects of SiO2, TiO2, and ZnO Nanoparticles on Intestinal Cells

Silicon dioxide (SiO₂), titanium dioxide (TiO₂), and zinc oxide (ZnO) are currently among the most widely used nanoparticles (NPs) in the food industry. This could potentially lead to unintended exposure of the gastrointestinal tract to these NPs. This study aims to investigate the potential side‐effects of these food‐borne NPs on intestinal cells and to mechanistically understand the observed biological responses. Among the panel of tested NPs, ZnO NPs are the most toxic. Consistently in all three tested intestinal cell models, ZnO NPs invoke the most inflammatory responses from the cells and induce the highest intracellular production of reactive oxygen species (ROS). The elevated ROS levels induce significant damage to the DNA of the cells, resulting in cell‐cycle arrest and subsequently cell death. In contrast, both SiO₂ and TiO₂ NPs elicit minimum biological responses from the intestinal cells. Overall, the study showcases the varying capability of the food‐borne NPs to induce a cellular response in the intestinal cells. In addition to physicochemical differences in the NPs, the genetic landscape of the intestinal cell models governs the toxicology profile of these food‐borne NPs.     

Diverse biotechnological applications of multifunctional titanium dioxide nanoparticles: An up‐to‐date review

Titanium dioxide (TiO₂) nanoparticles (NPs) are one of the topmost widely used metallic oxide nanoparticles. Whether present in naked form or doped with metals or polymers, TiO₂ NPs perform immensely important functions. However, the alteration in size and shape by doping results in improving the physical, chemical, and biological behaviour of TiO₂ NPs. Hence, the differential effects of various TiO₂ nanostructures including nanoflakes, nanoflowers, and nanotubes in various domains of biotechnology have been elucidated by researchers. Recently, the exponential growth of research activities regarding TiO₂ NPs has been observed owing to their chemical stability, low toxicity, and multifaceted properties. Because of their enormous abundance, plants, humans, and environment are inevitably exposed to TiO₂ NPs. These NPs play a significant role in improving agricultural attributes, removing environmental pollution, and upgrading the domain of nanomedicine. Therefore, the currently ongoing studies about the employment of TiO₂ NPs in enhancement of different aspects of agriculture, environment, and medicine have been extensively discussed in this review.     

Electrospun nylon-6 spider-net like nanofiber mat containing TiO2 nanoparticles: A multifunctional nanocomposite textile material

In this study, electrospun nylon-6 spider-net like nanofiber mats containing TiO₂ nanoparticles (TiO₂ NPs) were successfully prepared. The nanofiber mats containing TiO₂ NPs were characterized by SEM, FE-SEM, TEM, XRD, TGA and EDX analyses. The results revealed that fibers in two distinct sizes (nano and subnano scale) were obtained with the addition of a small amount of TiO₂ NPs. In low TiO₂ content nanocomposite mats, these nanofiber weaves were found uniformly loaded with TiO₂ NPs on their wall. The presence of a small amount of TiO₂ NPs in nylon-6 solution was found to improve the hydrophilicity (antifouling effect), mechanical strength, antimicrobial and UV protecting ability of electrospun mats. The resultant nylon-6/TiO₂ antimicrobial spider-net like composite mat with antifouling effect may be a potential candidate for future water filter applications, and its improved mechanical strength and UV blocking ability will also make it a potential candidate for protective clothing.     

Dye sensitized solar cell of TiO2 nanoparticle/nanorod composites prepared via low-temperature synthesis in oleic acid

Titania (TiO₂) nanorods (NRs) and nanoparticles (NPs) were synthesized using oleic acid as a surfactant and employed as photoanodes for dye sensitized solar cell (DSSC) fabrication. The synthesized NRs and NPs were characterized using transmission electron microscopy and X-ray diffraction. The photovoltaic performances were compared between NRs, NPs, and their composites. The results showed that the power conversion efficiencies (η) of the composites depend on the relative compositions of NRs and NPs in photoanodes, reaching the greatest at 10% NR content. η of the pure NRs DSSC was lower than that of the NPs DSSC. Electrochemical impedance spectroscopy revealed that the highest η at 10% NRs is mainly due to reduced charge transport resistance at the TiO₂/dye/electrolyte interface and electrolyte diffusion resistance, overcoming the reduction of the number of adsorbed dye molecules.     

RGD-conjugated titanium dioxide nanoparticles: targeted near-infrared photothermal therapy for α<Subscript>v</Subscript>β<Subscript>3</Subscript> integrin overexpressed cancer cells

Photothermal agents, which can convert near-infrared light into heat with a minimal attenuation of the energy and prevent undesirable thermal damage to healthy tissue, provided an opportunity for accurate heat delivery to desired sites. Herein, we designed cyclo(Arg-Gly-Asp-D-Tyr-Lys) peptide c(RGDyK)-conjugated TiO₂ nanoparticles (TiO₂-RGD NPs) with an ideal biocompatibility and targeting property. TiO₂-RGD NPs exhibited intense absorbance in near-infrared region, a high stability in physiological conditions, and the photothermal conversion efficiency of ~38.5%. Due to the specific affinity between c(RGDyK) and α_vβ₃ integrin, TiO₂-RGD NPs showed the high targeting property for U87-MG cells with overexpression of α_vβ₃ integrin. After incubation with TiO₂-RGD NPs (100 µg/mL) and under 808 nm near-infrared laser irradiation (1 W/cm²), the viability of MCF-7 cells by deficient expression of α_vβ₃ integrin was ~71%, while the viability of U87-MG decreased to ~31%, which have been demonstrated as an effective targeting photothermal therapy agent.     

Penetration,distribution and brain toxicity of titanium nanoparticles in rodents' body: a review

Titanium dioxide (TiO₂) has been vastly used commercially, especially as white pigment in paints, colorants, plastics, coatings, cosmetics. Certain industrial uses TiO₂ in diameter <100 nm. There are three common exposure routes for TiO₂ : (i) inhalation exposure, (ii) exposure via gastrointestinal tract, (iii) dermal exposure. Inhalation and gastrointestinal exposure appear to be the most probable ways of exposure, although nanoparticle (NP) penetration is limited. However, the penetration rate may increase substantially when the tissue is impaired. When TiO₂ NPs migrate into the circulatory system, they can be distributed into all tissues including brain. In brain, TiO₂ lead to oxidative stress mediated by the microglia phagocytic cells which respond to TiO₂ NPs by the production and release of superoxide radicals that convert to multiple reactive oxygen species (ROS). The ROS production may also cause the damage of blood–brain barrier which then becomes more permeable for NPs. Moreover, several studies have showed neuron degradation and the impairment of spatial recognition memory and learning abilities in laboratory rodent exposed to TiO₂ NPs.Inspec keywords: nanoparticles, permeability, health hazards, molecular biophysics, biochemistry, biological tissues, toxicology, oxidation, brain, neurophysiology, blood, reviews, cosmetics, cellular biophysics, titanium compoundsOther keywords: rodents, white pigment, gastrointestinal tract, dermal exposure, gastrointestinal exposure, nanoparticle penetration, penetration rate, blood–brain barrier, titanium nanoparticles, brain toxicity, size 100.0 nm, TiO₂      

Evaluation of in vitro cytotoxicity,biocompatibility, and changes in the expression of apoptosis regulatory proteins induced by cerium oxide nanocrystals

Abstract

Cerium oxide nanocrystals (CeO₂-NCs) exhibit superoxide dismutase and catalase mimetic activities. Based on these catalytic activities, CeO₂-NCs have been suggested to have the potential to treat various diseases. The crystalline size of these materials is an important factor that influences the performance of CeO₂-NCs. Previous reports have shown that several metal-based nanocrystals, including CeO₂-NCs, can induce cytotoxicity in cancer cells. However, the underlying mechanisms have remained unclear. To characterize the anticancer activities of CeO₂-NCs, several assays related to the mechanism of cytotoxicity and induction of apoptosis has been performed. Here, we have carried out a systematic study to characterize CeO₂-NCs phase purity (X-ray diffraction), morphology (electron microscopy), and optical features (optical absorption, Raman scattering, and photoluminescence) to better establish their potential as anticancer drugs. Our study revealed anticancer effects of CeO₂-NCs in HT29 and SW620 colorectal cancer cell lines with half-maximal inhibitory concentration (IC₅₀) values of 2.26 and 121.18 μg ml^–1, respectively. Reductions in cell viability indicated the cytotoxic potential of CeO₂-NCs in HT29 cells based on inverted and florescence microscopy assessments. The mechanism of cytotoxicity confirmed by estimating possible changes in the expression levels of Bcl2, BclxL, Bax, PARP, cytochrome c, and β-actin (control) proteins in HT29 cells. Down-regulation of Bcl2 and BclxL and up-regulation of Bax, PARP, and cytochrome c proteins suggested the significant involvement of CeO₂-NCs exposure in the induction of apoptosis. Furthermore, biocompatibility assay showed minimum effect of CeO₂-NCs on human red blood cells.     

Facile synthesis of copper oxide nanotubes decorated by TiO2 nanoparticles,optical and photocatalytic activity in water

Copper oxide nanotubes decorated by TiO₂ nanoparticles (CNTNs) were fabricated by simple three-step method. First, deposition of copper onto cellulose fibres, then thermal oxidation of copper and cellulose fibres and last simply mixing copper oxide nanotubes and TiO₂ nanoparticles (NPs). Scanning electron microscopy, transmission electron microscopy and X-ray diffraction showed that the synthesised nanotubes were monoclinic-structured polycrystalline CuO with diameter and wall thickness of approximately 50～100 nm and 20～25 nm, respectively. Moreover, the diameter of the TiO₂ NPs is about 20～30 nm. Optical properties of the solutions containing copper oxide nanotubes decorated by TiO₂ NPs were studied. Discrete dipole approximation was used for the calculation of absorption, scattering and extinction cross sections of the deposited CNTNs on a glass substrate. Our simulation results show that there are good agreements between the experimental date and the simulation results. Moreover, the photocatalytic tests were done by methyl orange under visible light (λ = 633 nm) irradiation for prepared samples.     

Preparation of ultrathin TiO2 single-crystal nanowires for high performance dye sensitized solar cells

Ultrathin TiO₂ anatase nanowires (NWs) were successfully prepared via a rapid and facile hydrothermal route. Consequently, the TiO₂ NWs and TiO₂ nanoparticles (NPs) composites electrodes were prepared with different weight ratios (25, 50 and 100 %) for a dye sensitized solar cell, and the photoelectrical performance has been systematically studied. It is observed that although the amount of absorption dye decreases, the composite solar cells exhibit a higher power conversion efficiency compared to either pure TiO₂ NP or NW solar cells by rationally tuning the weight ratios. The behavior was attributed to a combination of the rapid carrier transport in NW framework and the high dye loading on P25 surface.