Your search keyword '"Jia-Huei Zheng"' showing total 19 results

1. Structure-based virtual screening and biological evaluation of novel small-molecule BTK inhibitors

Author

Tony Eight Lin, Li-Chin Sung, Min-Wu Chao, Min Li, Jia-Huei Zheng, Tzu-Ying Sung, Jui-Hua Hsieh, Chia-Ron Yang, Hsueh-Yun Lee, Er-Chieh Cho, and Kai-Cheng Hsu

Subjects

virtual screening, kinase inhibitor, btk, solid tumours, small-molecule inhibitors, Therapeutics. Pharmacology, RM1-950

Abstract

Bruton tyrosine kinase (BTK) is linked to multiple signalling pathways that regulate cellular survival, activation, and proliferation. A covalent BTK inhibitor has shown favourable outcomes for treating B cell malignant leukaemia. However, covalent inhibitors require a high reactive warhead that may contribute to unexpected toxicity, poor selectivity, or reduced effectiveness in solid tumours. Herein, we report the identification of a novel noncovalent BTK inhibitor. The binding interactions (i.e. interactions from known BTK inhibitors) for the BTK binding site were identified and incorporated into a structure-based virtual screening (SBVS). Top-rank compounds were selected and testing revealed a BTK inhibitor with >50% inhibition at 10 µM concentration. Examining analogues revealed further BTK inhibitors. When tested across solid tumour cell lines, one inhibitor showed favourable inhibitory activity, suggesting its potential for targeting BTK malignant tumours. This inhibitor could serve as a basis for developing an effective BTK inhibitor targeting solid cancers.

Published

2022

2. Application of Drug Testing Platforms in Circulating Tumor Cells and Validation of a Patient-Derived Xenograft Mouse Model in Patient with Primary Intracranial Ependymomas with Extraneural Metastases

Author

Muh-Lii Liang, Ting-Chi Yeh, Man-Hsu Huang, Pao-Shu Wu, Shih-Pei Wu, Chun-Chao Huang, Tsung-Yu Yen, Wei-Hsin Ting, Jen-Yin Hou, Jia-Yun Huang, Yi-Huei Ding, Jia-Huei Zheng, Hsi-Che Liu, Che-Sheng Ho, Shiu-Jau Chen, and Tsung-Han Hsieh

Subjects

ependymoma, extraneural metastasis, circulating tumor cells, patient-derived xenograft, drug screening, Medicine (General), R5-920

Abstract

Primary intracranial ependymoma is a challenging tumor to treat despite the availability of multidisciplinary therapeutic modalities, including surgical resection, radiotherapy, and adjuvant chemotherapy. After the completion of initial treatment, when resistant tumor cells recur, salvage therapy needs to be carried out with a more precise strategy. Circulating tumor cells (CTCs) have specifically been detected and validated for patients with primary or recurrent diffused glioma. The CTC drug screening platform can be used to perform a mini-invasive liquid biopsy for potential drug selection. The validation of potential drugs in a patient-derived xenograft (PDX) mouse model based on the same patient can serve as a preclinical testing platform. Here, we present the application of a drug testing model in a six-year-old girl with primary ependymoma on the posterior fossa, type A (EPN-PFA). She suffered from tumor recurrence with intracranial and spinal seeding at 2 years after her first operation and extraneural metastases in the pleura, lung, mediastinum, and distant femoral bone at 4 years after initial treatment. The CTC screening platform results showed that everolimus and entrectinib could be used to decrease CTC viability. The therapeutic efficacy of these two therapeutic agents has also been validated in a PDX mouse model from the same patient, and the results showed that these two therapeutic agents significantly decreased tumor growth. After precise drug screening and the combination of focal radiation on the femoral bone with everolimus chemotherapy, the whole-body bone scan showed significant shrinkage of the metastatic tumor on the right femoral bone. This novel approach can combine liquid biopsy, CTC drug testing platforms, and PDX model validation to achieve precision medicine in rare and challenging tumors with extraneural metastases.

Published

2023

3. Clerodane Diterpene Ameliorates Inflammatory Bowel Disease and Potentiates Cell Apoptosis of Colorectal Cancer

Author

Jia-Huei Zheng, Shian-Ren Lin, Feng-Jen Tseng, May-Jywan Tsai, Sheng-I Lue, Yi-Chen Chia, Mindar Woon, Yaw-Syan Fu, and Ching-Feng Weng

Subjects

colorectal cancer, diterpenes, inflammatory bowel diseases, polyalthia longifolia, herbal medicine., Microbiology, QR1-502

Abstract

Inflammatory bowel disease (IBD) is general term for ulcerative colitis and Crohn’s disease, which is chronic intestinal and colorectal inflammation caused by microbial infiltration or immunocyte attack. IBD is not curable, and is highly susceptible to develop into colorectal cancer. Finding agents to alleviate these symptoms, as well as any progression of IBD, is a critical effort. This study evaluates the anti-inflammation and anti-tumor activity of 16-hydroxycleroda-3,13-dien-15,16-olide (HCD) in in vivo and in vitro assays. The result of an IBD mouse model induced using intraperitoneal chemical azoxymethane (AOM)/dextran sodium sulfate (DSS) injection showed that intraperitoneal HCD adminstration could ameliorate the inflammatory symptoms of IBD mice. In the in vitro assay, cytotoxic characteristics and retained signaling pathways of HCD treatment were analyzed by MTT assay, cell cycle analysis, and Western blotting. From cell viability determination, the IC50 of HCD in Caco-2 was significantly lower in 2.30 μM at 48 h when compared to 5-fluorouracil (5-FU) (66.79 μM). By cell cycle and Western blotting analysis, the cell death characteristics of HCD treatment in Caco-2 exhibited the involvement of extrinsic and intrinsic pathways in cell death, for which intrinsic apoptosis was predominantly activated via the reduction in growth factor signaling. These potential treatments against colon cancer demonstrate that HCD could provide a promising adjuvant as an alternative medicine in combating colorectal cancer and IBD.

Published

2019

4. Mitochondrial Factor C20orf7 Facilitates the EMT-Mediated Cancer Cell Migration and the Proliferation of Colon Cancer In Vitro and In Vivo

Author

Hou-Hsien Liu, Chia-Hwa Lee, Yi-Chen Hsieh, Jia-Huei Zheng, Yun-Ru Liu, Chia-Hsuan Chang, and Er-Chieh Cho

Subjects

mitochondrial factor, C20orf7, epithelial–mesenchymal transition (EMT), 5-fluorouracil (5FU), colon cancer progression, therapeutic target, Mice, Disease Models, Animal, Epithelial-Mesenchymal Transition, Cell Movement, Colonic Neoplasms, Genetics, Humans, Animals, Fluorouracil, Genetics (clinical), Mitochondria, Cell Proliferation

Abstract

Colon cancer is a major malignant neoplasm with a low survival rate for late-stage patients. Therefore, the investigation of molecules regulating colon cancer progression and the discovery of novel therapeutic targets is critical. Mitochondria play a vital role in maintaining the homeostasis of cells. Abnormal mitochondrial metabolism alterations and the induction of glycolysis can facilitate tumor growth; therefore, targeting mitochondrial molecules is suggested to be a promising strategy for cancer treatment. In this study, we investigated the role of this largely unknown mitochondrial factor, chromosome 20 open reading frame 7 (C20orf7), in colon cancer progression. Clustered regularly interspaced short palindromic repeats (CRISPR) technology was utilized for C20orf7 depletion, and functional assays were performed to examine the regulation of C20orf7 in colon cancer cells. We demonstrated that C20orf7 facilitates epithelial–mesenchymal transition (EMT)-mediated cell migration and promotes the proliferation of colon cancer. The anti-cancer drug 5-fluorouracil (5FU) was also applied, and C20orf7 was targeted with a combination of 5FU treatment, which could further enhance the anti-cancer effect in the colon cancer cell line and the xenograft mice model. In summary, this study demonstrated, for the first time, that C20orf7 plays a promotional role in cancer tumorigenesis and could be a promising therapeutic target in colon cancer treatment.

Published

2022

5. GFP Plasmid and Chemoreagent Conjugated with Graphene Quantum Dots as a Novel Gene Delivery Platform for Colon Cancer Inhibition In Vitro and In Vivo

Author

Kuen Chan Lee, Er Chieh Cho, Jen Hsien Huang, Jia Huei Zheng, Guang Yu Lee, and Pei Ying Lo

Subjects

Chemistry, Colorectal cancer, Biochemistry (medical), Biomedical Engineering, General Chemistry, Gene delivery, Conjugated system, medicine.disease, In vitro, Green fluorescent protein, Cell biology, Biomaterials, Plasmid, In vivo, medicine, Gene

Abstract

Scientists have studied intensively the gene delivery carriers for treating genetic diseases. However, there are challenges that impede the application of naked gene-based therapy at the clinical level, such as quick elimination of the circulation, lack of membrane penetrability, and poor endosome trapping. Herein, we develop graphene quantum dots (GQDs)-derivative nanocarriers and introduce polyethylenimine (PEI) to equip the system with enhanced biocompatibility and abundant functional groups for modification. In addition to carrying green fluorescent protein (GFP) as an example of gene delivery, this system covalently binds colon cancer cells targeted antibody and epidermal growth factor receptor (EGFR) to enhance cell membrane penetrability and cell uptake of nanocarriers. To achieve multistrategy cancer therapy, the anticancer drug doxorubicin (Dox) is noncovalently encapsulated to achieve pH-induced drug release at tumor sites and leaves space for further functional gene modification. This nanoparticle serves as a multifunctional gene delivery system, which facilitates improved cytotoxicity and longer-sustained inhibition capacity compared to free Dox treatments in colon cancer cells. Moreover, our GQD composites display compatible tumor suppression ability compared with the free Dox treatment group in xenograft mice experiment with significantly less toxicity. This GQD nanoplatform was demonstrated as a multifunctional gene delivery system that could contribute to treating other genetic diseases in the future.

Published

2022

6. Combining an Autophagy Inhibitor, MPT0L145, with Abemaciclib Is a New Therapeutic Strategy in GBM Treatment

Author

Tsung-Han Hsieh, Muh-Lii Liang, Jia-Huei Zheng, Yu-Chen Lin, Yu-Chen Yang, Thanh-Hoa Vo, Jing-Ping Liou, Yun Yen, and Chun-Han Chen

Subjects

Cancer Research, glioblastoma multiforme, MPT0L145, Oncology, abemaciclib, synergism, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282, Article

Abstract

Simple Summary Glioblastoma multiforme is a common and lethal malignant brain tumor, and occurrence of therapeutic resistance in GBM often causes relapse. Therefore, this study aimed to find a new therapeutic strategy to treat these malignant tumors. In the current study, combined abemaciclib with an autophagy inhibitor, MPT0L145, significantly reduced cell proliferation and elevated intracellular reactive oxygen species (ROS) level. A blood–brain barrier permeability assay also showed that MPT0L145 could penetrate endothelial cells and has a penetration ability similar to that of TMZ. Therefore, this work represents a potential therapeutic strategy for treating the GBM in the future. Abstract Glioblastoma multiforme (GBM) is the most malignant brain tumor in the world, only 25% of GBM patients were alive one year after diagnosis. Although Temozolamide combined with radiation therapy more effectively prolonged the survival rate than radiation alone, the overall survival rate is still dismal. Therefore, a new therapeutic strategy is urgently needed. CDK4/6 inhibitors are newly FDA-approved agents to treat HR-positive, HER2-negative advanced, and metastatic breast cancers, and preclinical results showed that CDK4/6 inhibitors significantly reduced cell proliferation and tumor growth. However, several studies have suggested that CDK4/6 inhibitor-induced non-genetic changes caused treatment failure, including autophagy activation. Therefore, this study aimed to combine an autophagy inhibitor, MPT0L145, with abemaciclib to improve therapeutic efficiency. The use of abemaciclib effectively inhibited cell proliferation via suppression of RB phosphorylation and induced autophagy activation in GBM cancer cells. MPT0L145 treatment alone not only blocked autophagy activation, but also induced generation of ROS and DNA damage in a concentration-dependent manner. Importantly, MPT0L145 had a comparable penetration ability to TMZ in our blood brain barrier permeability assay. Combined MPT0L145 with abemaciclib significantly reduced cell proliferation, suppressed RB phosphorylation, and increased ROS production. In conclusion, the data suggested that blocking autophagy by MPT0L145 synergistically sensitized GBM cancer cells to abemaciclib and represents a potential therapeutic strategy for treating GBM in the future.

Published

2021

7. Structure-based virtual screening and biological evaluation of novel small-molecule BTK inhibitors.

Author

Lin, Tony Eight, Li-Chin Sung, Min-Wu Chao, Min Li, Jia-Huei Zheng, Tzu-Ying Sung, Jui-Hua Hsieh, Chia-Ron Yang, Hsueh-Yun Lee, Er-Chieh Cho, and Kai-Cheng Hsu

Subjects

BRUTON tyrosine kinase, MEDICAL screening, B cells

Abstract

Bruton tyrosine kinase (BTK) is linked to multiple signalling pathways that regulate cellular survival, activation, and proliferation. A covalent BTK inhibitor has shown favourable outcomes for treating B cell malignant leukaemia. However, covalent inhibitors require a high reactive warhead that may contribute to unexpected toxicity, poor selectivity, or reduced effectiveness in solid tumours. Herein, we report the identification of a novel noncovalent BTK inhibitor. The binding interactions (i.e. interactions from known BTK inhibitors) for the BTK binding site were identified and incorporated into a structure-based virtual screening (SBVS). Top-rank compounds were selected and testing revealed a BTK inhibitor with >50% inhibition at 10 mM concentration. Examining analogues revealed further BTK inhibitors. When tested across solid tumour cell lines, one inhibitor showed favourable inhibitory activity, suggesting its potential for targeting BTK malignant tumours. This inhibitor could serve as a basis for developing an effective BTK inhibitor targeting solid cancers. [ABSTRACT FROM AUTHOR]

Published

2022

8. Simultaneous formation of Bi

Author

Guang-Yu, Lee, Er-Chieh, Cho, Pei-Ying, Lo, Jia-Huei, Zheng, Jen-Hsien, Huang, Yi-Lun, Chen, and Kuen-Chan, Lee

Subjects

Nitrates, Light, Bismuth, Catalysis, Environmental Restoration and Remediation, Microspheres

Abstract

As a two-dimensional nanomaterial, bismuth oxybromide (BiOBr) have attracted tremendous interest in the area of visible-light photocatalysis since it can provide the internal electric field (IEF) through z-axis through its unique electronic band structure. However, the insufficient active sites and rapid recombination rate of charged carriers hamper the efficiency of the photocatalysis. To address these two major obstacles, an enticing strategy of constructing heterojunction was established by introducing Bi

Published

2020

9. Integration of PEG and PEI with graphene quantum dots to fabricate pH-responsive nanostars for colon cancer suppression in vitro and in vivo

Author

Guang-Yu Lee, Er-Chieh Cho, Pei-Ying Lo, Kuen Chan Lee, Jen Hsien Huang, Min Li, and Jia-Huei Zheng

Subjects

Materials science, Tertiary amine, Cell growth, Surfaces, Coatings and Films, Electronic, Optical and Magnetic Materials, Green fluorescent protein, In vivo, Cancer cell, Drug delivery, Materials Chemistry, Ceramics and Composites, medicine, Biophysics, Doxorubicin, Drug carrier, medicine.drug

Abstract

There has been great improvement in nanomaterial fields, and the biomedical potential of nanomaterials as drug delivery system is under intensive studies. Among them, graphene quantum dots (GQDs) are considered to be the next generation of carbon-based nanomaterial for biomedical applications. In this study, we utilized green fluorescent protein (GFP) nucleic acid, DNA-targeting chemoreagent doxorubicin (DOX), and branched polyethyleneimine (PEI) conjugated GQDs, to form pH-responsive nanostar drug carrier for colon cancer suppression investigation. GFP expression plasmid was applied to examine the delivery capacity of our drug carrier. DOX was encapsulated by intrinsic π-π interaction to form GQDs-polymer-DOX conjugates (GECD) as drug carrier. We proposed that once GECD enters the tumor lesion, the acidic tumor microenvironment protonated the tertiary amine of GECD from neutral to mild positive, possessed higher affinity to negatively charged cell membrane, triggered the drug release, and then cancer cells would be inhibited. The anti-cancer ability of our drug carrier system, GECD, was demonstrated in cancer cells by cell proliferation assay. Moreover, GECD exhibited its powerful anti-tumor capacity in the mice xenograft model. The in vivo and in vitro results indicate that our GECD with high cancer suppression capacity could be adopted for future cancer therapy.

Published

2022

10. Microwave-assisted synthesis of TiO2/WS2 heterojunctions with enhanced photocatalytic activity

Author

Cai Wan Chang-Jian, Bo Cheng Ho, Jia Huei Zheng, Yu-Sheng Hsiao, Er Chieh Cho, Kuen Chan Lee, and Jen Hsien Huang

Subjects

Materials science, Absorption spectroscopy, General Chemical Engineering, Heterojunction, 02 engineering and technology, General Chemistry, 010402 general chemistry, 021001 nanoscience & nanotechnology, Photochemistry, 01 natural sciences, Hydrothermal circulation, 0104 chemical sciences, Photocatalysis, Degradation (geology), Irradiation, 0210 nano-technology, Absorption (electromagnetic radiation), Ultraviolet photoelectron spectroscopy

Abstract

In this study, visible light-responsive photocatalysts based on TiO2/WS2 were prepared through a microwave-assisted hydrothermal process. These TiO2/WS2 composites featured a larger surface area and a wider range of optical absorption when compared with those of pure TiO2. Ultraviolet photoelectron spectroscopy revealed that the energy band levels of the heterojunction between the TiO2 and WS2 components were compatible for charge transfer. Compared with pristine TiO2, the photocatalytic activity of the TiO2/WS2 composites was enhanced significantly—the result of expanding the optical absorption spectrum into the visible region as well as decreasing the rate of recombination of the photogenerated electron/hole pairs. The visible photocatalytic activity of the as-prepared photocatalysts was evaluated through the degradation of methylene blue, using a white light emitting diode (LED) as the irradiation source. For the degradation under LED irradiation, the optimal content of WS2 was 3.0 wt%. An examination of the TiO2/WS2 composites in human cells indicated that they were highly biocompatible; they did not affect the cellular proliferation or morphology, suggesting future applications in a biomedical capacity.

Published

2018

11. Robust multifunctional superhydrophobic coatings with enhanced water/oil separation, self-cleaning, anti-corrosion, and anti-biological adhesion

Author

Kao Shuh Chuang, Cai Wan Chang-Jian, Jen Hsien Huang, Er Chieh Cho, Hsin Chou Chen, Kuen Chan Lee, Yu-Sheng Hsiao, and Jia Huei Zheng

Subjects

Nanocomposite, Materials science, Biological adhesion, General Chemical Engineering, Composite number, Anti-corrosion, Nanoparticle, Nanotechnology, 02 engineering and technology, General Chemistry, 010402 general chemistry, 021001 nanoscience & nanotechnology, 01 natural sciences, Industrial and Manufacturing Engineering, Superhydrophobic coating, 0104 chemical sciences, Contact angle, chemistry.chemical_compound, chemistry, Siloxane, Environmental Chemistry, 0210 nano-technology

Abstract

In this study, superhydrophobic and transparent siloxane-based nanocomposites have been synthesized. The as-synthesized superhydrophobic nanoparticles reveal uniform particle size distribution and high dispersibility in alcohol solvents which can be easily integrated into solution-process. Further improvement of superhydrophobicity of this composite is achieved by the chemical modification with fluorosilane. The cast hybrid surface reveals superhydrophobic (water contact angle (WCA) = 168°), non-stick and transparent properties (90% at 550 nm) on a variety of substrates. As a result, the as-prepared superhydrophobic coating shows outstanding water/oil separation, self-cleaning, anti-corrosion and anti-adhesion of bacteria and algae. Moreover, the superhydrophobic coating can remain its extreme water repellency without obvious decay of WCA after weathering resistance test for 90 days. It is believed that the facile and low-cost method offers an effective strategy and promising industrial applications for fabricating superhydrophobic surfaces.

Published

2017

12. Clerodane Diterpene Ameliorates Inflammatory Bowel Disease and Potentiates Cell Apoptosis of Colorectal Cancer

Author

Sheng-I Lue, Yi-Chen Chia, Mindar Woon, Feng-Jen Tseng, Ching-Feng Weng, May-Jywan Tsai, Shian-Ren Lin, Jia-Huei Zheng, and Yaw-Syan Fu

Subjects

Male, Colorectal cancer, lcsh:QR1-502, Apoptosis, Biochemistry, Inflammatory bowel disease, lcsh:Microbiology, chemistry.chemical_compound, 0302 clinical medicine, 0303 health sciences, Cell Cycle, Dextran Sulfate, digestive, oral, and skin physiology, diterpenes, Cell cycle, Ulcerative colitis, Intestines, 030220 oncology & carcinogenesis, herbal medicine, Fluorouracil, Colorectal Neoplasms, HT29 Cells, Cell Survival, Azoxymethane, colorectal cancer, digestive system, inflammatory bowel diseases, Article, Diterpenes, Clerodane, Polyalthia longifolia, 03 medical and health sciences, medicine, Biomarkers, Tumor, Animals, Humans, Viability assay, Molecular Biology, 030304 developmental biology, Cell Proliferation, Inflammation, business.industry, Intrinsic apoptosis, medicine.disease, digestive system diseases, Mice, Inbred C57BL, chemistry, Cancer research, Caco-2 Cells, business

Abstract

Inflammatory bowel disease (IBD) is general term for ulcerative colitis and Crohn&rsquo, s disease, which is chronic intestinal and colorectal inflammation caused by microbial infiltration or immunocyte attack. IBD is not curable, and is highly susceptible to develop into colorectal cancer. Finding agents to alleviate these symptoms, as well as any progression of IBD, is a critical effort. This study evaluates the anti-inflammation and anti-tumor activity of 16-hydroxycleroda-3,13-dien-15,16-olide (HCD) in in vivo and in vitro assays. The result of an IBD mouse model induced using intraperitoneal chemical azoxymethane (AOM)/dextran sodium sulfate (DSS) injection showed that intraperitoneal HCD adminstration could ameliorate the inflammatory symptoms of IBD mice. In the in vitro assay, cytotoxic characteristics and retained signaling pathways of HCD treatment were analyzed by MTT assay, cell cycle analysis, and Western blotting. From cell viability determination, the IC50 of HCD in Caco-2 was significantly lower in 2.30 &mu, M at 48 h when compared to 5-fluorouracil (5-FU) (66.79 &mu, M). By cell cycle and Western blotting analysis, the cell death characteristics of HCD treatment in Caco-2 exhibited the involvement of extrinsic and intrinsic pathways in cell death, for which intrinsic apoptosis was predominantly activated via the reduction in growth factor signaling. These potential treatments against colon cancer demonstrate that HCD could provide a promising adjuvant as an alternative medicine in combating colorectal cancer and IBD.

Published

2019

13. Intercalating pyrene with polypeptide as a novel self-assembly nano-carrier for colon cancer suppression in vitro and in vivo

Author

Guang Yu Lee, Pei Ying Lo, Jen Hsien Huang, Er Chieh Cho, Jia Huei Zheng, and Kuen Chan Lee

Subjects

Drug, Nanostructure, Materials science, media_common.quotation_subject, Lysine, Nanoparticle, Mice, Nude, Bioengineering, 02 engineering and technology, 010402 general chemistry, 01 natural sciences, Biomaterials, Mice, In vivo, Animals, Humans, Polylysine, media_common, Drug Carriers, Pyrenes, Hydrogen-Ion Concentration, 021001 nanoscience & nanotechnology, HCT116 Cells, Xenograft Model Antitumor Assays, In vitro, Intercalating Agents, 0104 chemical sciences, Mechanics of Materials, Doxorubicin, Delayed-Action Preparations, Colonic Neoplasms, Biophysics, Nanoparticles, Self-assembly, Nanocarriers, 0210 nano-technology

Abstract

Giving patients right dosage is an essential concept of precision medicine. Most of nanocarriers lack of flexible drug capacity and structural stability to be customized for specific treatment, resulting in low therapeutic efficacy and unexpected side effects. Thus, a growing need emerges for fast and rigorous approaches to develop nanoparticles with properties of adjustable dosage and controllable particle size. Poly- l -Lysine is known for its enhanced bioadhesivity and pH-triggered structural swelling effect, which is utilized as the main agent to activate the multistage drug releasing. Inspired by natural bio-assembly system, we report a simple method to self-assemble Poly- l -Lysine-based nanoparticles via supramolecular recognitions of cross-linked pyrenes, which provides noncovalent force to flexibly encapsulate Doxorubincin and to construct robust nanostructures. Pyrene-modified polypeptide self-assemblies are able to adjust drug payload from 1: 10 to 2:1 (drug: polypeptide) without changing its uniform nano-spherical morphology. This nanostructure remained the as-made morphology even after experiencing the long-term (~ 10 weeks) storage at room temperature. Also, the nanoparticles displayed multi-step drug release behaviours and exhibited great in vitro and in vivo cytotoxicity towards colon cancer cells. The as-mentioned nanoparticles provide a novel perspective to compensate the clinical needs of specific drug feedings and scalable synthesis with advantages of simple-synthesis, size-adaptivity, and morphology reversibility.

Published

2019

14. [Untitled]

Author

Mei-Hsiang, Lin, Juo-Shan, Wang, Yi-Chen, Hsieh, Jia-Huei, Zheng, and Er-Chieh, Cho

Subjects

Proto-Oncogene Proteins p21(ras), Cell Movement, Coumarins, Cell Line, Tumor, Colonic Neoplasms, Mutation, Nitrogen Dioxide, Humans, Apoptosis, Drug Screening Assays, Antitumor, Cell Proliferation

Abstract

Colon cancer is one of the most lethal cancers worldwide even with the significant progress made in screening techniques and therapeutic agents. Genetic mutations in tumors complicated the treatments, and the survival rate remains low for patients at late or metastatic stages. KRAS gene mutation which leads to failure of the EGFR targeted therapies stands for an example of the challenges in clinical sites. Therefore, development of novel agents for colon cancer treatment is in need. Natural and synthetic coumarin derivatives have been suggested with various biological activities with pharmacologic potential including anti-cancer capacity. Here in this study, five coumarin derivatives, include trifluoromethyl-, dimethoxy-, and/or nitro-substitutions at different positions, were synthesized. Their cancer inhibition potential was investigated in various cancer cell lines. Our data demonstrated that one nitro-coumarin derivate, 5,7-Dimethoxy-4-methyl-6-nitro-chromen-2-one, exhibits cytotoxicity specifically towards colon cancer cells under competitive EC

Published

2019

15. Simultaneous formation of Bi2O2(OH)(NO3)/BiOBr ultrathin hierarchical microspheres for effectively promoting visible-light-driven photocatalytic activity in environmental remediation

Author

Yi Lun Chen, Jia Huei Zheng, Jen Hsien Huang, Kuen Chan Lee, Pei Ying Lo, Er Chieh Cho, and Guang Yu Lee

Subjects

Environmental Engineering, Materials science, Health, Toxicology and Mutagenesis, 0208 environmental biotechnology, Public Health, Environmental and Occupational Health, chemistry.chemical_element, Heterojunction, 02 engineering and technology, General Medicine, General Chemistry, 010501 environmental sciences, 01 natural sciences, Pollution, 020801 environmental engineering, Nanomaterials, Bismuth, Chemical engineering, chemistry, Specific surface area, Photocatalysis, Environmental Chemistry, Hydrothermal synthesis, Hydrate, 0105 earth and related environmental sciences, Visible spectrum

Abstract

As a two-dimensional nanomaterial, bismuth oxybromide (BiOBr) have attracted tremendous interest in the area of visible-light photocatalysis since it can provide the internal electric field (IEF) through z-axis through its unique electronic band structure. However, the insufficient active sites and rapid recombination rate of charged carriers hamper the efficiency of the photocatalysis. To address these two major obstacles, an enticing strategy of constructing heterojunction was established by introducing Bi2O2(OH)(NO3) (BiON) in BiOBr with the same precursor. Through a facile one-pot hydrothermal synthesis, two Sillen-type layered photocatalysts, with intimately constructed ultrathin heterostructure, was synthesized by the co-precipitation method. In this work, the formation of Bismuth-based heterojunction for charge separation is established by the excessive bismuth nitrate, which subsequently participates with the in situ growth of ultrathin hierarchical microspheres. By attenuating the thickness of BiOBr from 20 nm to 8 nm with the aid of BiON, the photogenerated charges could migrate to the active sites through shorter charge diffusion pathway. Also, the BiOBr and BiON act as an active bridge to promote the separation of electron-hole pairs, which also brings out more active sites due to its increased specific surface area. BiON/BiOBr ultrathin hierarchical microspheres exhibited enhanced visible-light photocatalytic activity for decontaminating several types of pollutants. Besides, the activity of as-prepared BiON/BiOBr was further evaluated by inhibiting the growth of kanamycin-resistant bacteria strains. This study presents a novel strategy to incorporate the crystalline bismuth hydrate nitrate into BiOBr to form ultrathin hierarchical microspheres with high surface area for environmental remediation.

Published

2020

16. Carboxylated carbon nanomaterials in cell cycle and apoptotic cell death regulation

Author

Jia Huei Zheng, Er Chieh Cho, Guang Yu Lee, Pei Ying Lo, and Kuen Chan Lee

Subjects

0106 biological sciences, 0301 basic medicine, Biocompatibility, Cell Survival, Surface Properties, Bioengineering, Apoptosis, Carbon nanotube, 01 natural sciences, Applied Microbiology and Biotechnology, law.invention, Nanomaterials, 03 medical and health sciences, law, 010608 biotechnology, Cell Line, Tumor, Materials Testing, Humans, Carbon nanomaterials, Chemistry, Graphene, Nanotubes, Carbon, Cell Cycle, General Medicine, Cell cycle, Nanostructures, G2 Phase Cell Cycle Checkpoints, 030104 developmental biology, Gene Expression Regulation, Biophysics, Cell Cycle Profile, Graphite, Biotechnology

Abstract

Carbon nanomaterials, include carbon nanotubes and graphene nanosheets, have drawn an increasing amount of attention because of their potential applications in daily life or in providing novel therapeutic possibilities for treating diseases. However, the overall biocompatibility, the potential toxic effects of carbon nanomaterials toward human cells, and their modulations in cellular mechanism, are not fully understood. Herein, four types of carbon nanomaterials, include long and short carbon nanotubes and graphene nanosheets, at low and high concentrations, were functionalized and dispersed in the biocompatible buffer for assessment. The surface structure, the morphology, and chemical composition of carbon nanomaterials were characterized. Also, biological assays investigating cellular viability, vitality, cell cycle, and apoptotic cell death were applied on cells co-incubated with nanomaterials, to evaluate the biocompatibility of these nanomaterials in human cells. Our data suggested that even though co-incubation of nanomaterials did not seem to affect the viability of cells notably, high concentrations (50 ug/ml) of SW could lead to unhealthy cells, and we observed dramatic G2 arrest effect mediated by p21 induction in high SW incubated cells. Other nanomaterials at high concentration may also alter cell cycle profile of the cells. In summary, our data demonstrated that these nanomaterials could regulate cell cycle and lead to apoptosis at high concentrations, and the underling molecular mechanisms have been addressed. Caution should be taken on their concentration when nanomaterials are in used in future medical applications.

Published

2018

17. Fullerene C 70 decorated TiO 2 nanowires for visible-light-responsive photocatalyst

Author

Jen Hsien Huang, Jing-Hao Ciou, Job Pan, Kuen Chan Lee, Yu-Sheng Hsiao, Er Chieh Cho, and Jia Huei Zheng

Subjects

Materials science, Fullerene, business.industry, Nanowire, General Physics and Astronomy, Surfaces and Interfaces, General Chemistry, Photoelectrochemical cell, Condensed Matter Physics, medicine.disease_cause, Photochemistry, Surfaces, Coatings and Films, Chemical bond, medicine, Photocatalysis, Optoelectronics, Irradiation, business, Ultraviolet, Visible spectrum

Abstract

In this study, we have synthesized C 60 and C 70 -modified TiO 2 nanowire (NW) through interfacial chemical bonding. The results indicate that the fullerenes (C 60 and C 70 derivatives) can act as sinks for photogenerated electrons in TiO 2 , while the fullerene/TiO 2 is illuminated under ultraviolet (UV) light. Therefore, in comparison to the pure TiO 2 NWs, the modified TiO 2 NWs display a higher photocatalytic activity under UV irradiation. Moreover, the fullerenes also can function as a sensitizer to TiO 2 which expand the utilization of solar light from UV to visible light. The results reveal that the C 70 /TiO 2 NWs show a significant photocatalytic activity for degradation of methylene blue (MB) in visible light region. To better understand the mechanism responsible for the effect of fullerenes on the photocatalytic properties of TiO 2 , the electron only devices and photoelectrochemical cells based on fullerenes/TiO 2 are also fabricated and evaluated.

Published

2015

18. NO2 functionalized coumarin derivatives suppress cancer progression and facilitate apoptotic cell death in KRAS mutant colon cancer

Author

Jia Huei Zheng, Juo Shan Wang, Er Chieh Cho, Yi Chen Hsieh, and Mei Hsiang Lin

Subjects

0301 basic medicine, business.industry, Colorectal cancer, Wild type, Cancer, General Medicine, Toxicology, medicine.disease_cause, medicine.disease, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, KRAS Gene Mutation, Apoptosis, 030220 oncology & carcinogenesis, Cancer cell, Cancer research, Medicine, KRAS, business, Cytotoxicity

Abstract

Colon cancer is one of the most lethal cancers worldwide even with the significant progress made in screening techniques and therapeutic agents. Genetic mutations in tumors complicated the treatments, and the survival rate remains low for patients at late or metastatic stages. KRAS gene mutation which leads to failure of the EGFR targeted therapies stands for an example of the challenges in clinical sites. Therefore, development of novel agents for colon cancer treatment is in need. Natural and synthetic coumarin derivatives have been suggested with various biological activities with pharmacologic potential including anti-cancer capacity. Here in this study, five coumarin derivatives, include trifluoromethyl-, dimethoxy-, and/or nitro-substitutions at different positions, were synthesized. Their cancer inhibition potential was investigated in various cancer cell lines. Our data demonstrated that one nitro-coumarin derivate, 5,7-Dimethoxy-4-methyl-6-nitro-chromen-2-one, exhibits cytotoxicity specifically towards colon cancer cells under competitive EC50. Our results showed that this compound can effectively suppress colon cancer cells harboring either wild type or mutant KRAS genes, and that it could inhibit short-term proliferation, long term proliferation, and migration capacities of cancer cells. Finally, we demonstrated that this coumarin derivate facilitates cancer cell death through activation of apoptosis pathway. Our results suggest that this coumarin derivate is a promising lead drug worth further investigation and development for future cancer treatment.

Published

2019

19. GFP Plasmid and Chemoreagent Conjugated with Graphene Quantum Dots as a Novel Gene Delivery Platform for Colon Cancer Inhibition In Vitro and In Vivo.

Author

Pei-Ying Lo, Guang-Yu Lee, Jia-Huei Zheng, Jen-Hsien Huang, Er-Chieh Cho, and Kuen-Chan Lee

Published

2020