Your search keyword '"Jixing Ye"' showing total 48 results

1. Effect of antibiotic monensin on cell proliferation and IGF1R signaling pathway in human colorectal cancer cells

Author

Youping Zhou, Youlin Deng, Jing Wang, Zhengjian Yan, Qiang Wei, Jixing Ye, Junhui Zhang, Tong-Chuan He, and Min Qiao

Subjects

Colorectal cancer, monensin, cell proliferation, IGF signaling, cancer therapy, Medicine

Abstract

AbstractBackground/Aims Colorectal cancer is the third leading cause of death in patients with cancers in America. Monensin has represented anti-cancer effect on various human cancer cells. We seek to investigate the effect of monensin on proliferation of human colorectal cancer cells and explore whether IGF1R signaling pathway is involved in anti-cancer mechanism of monensin.Methods Cell proliferation and migration were assessed by crystal violet staining and cell wounding assay respectively. Cell apoptosis was analyzed by Hoechst 33258 staining and flow cytometry. Cell cycle progression was detected with the use of flow cytometry. Cancer-associated pathways were assessed with the use of pathway-specific reporters. Gene expression was detected by touchdown-quantitative real-time PCR. Inhibition of IGF1R was tested by immunofluorescence staining. Inhibition of IGF1R signaling was accomplished by adenovirus-mediated expression of IGF1.Results We found that monensin not only effectively inhibited cell proliferation, cell migration as well as cell cycle progression, but also induced apoptosis and G1 arrest in human colorectal cancer cells. Monensin was shown to target multiple cancer-related signaling pathways such as Elk1, AP1, as well as Myc/max, and suppressed IGF1R expression via increasing IGF1 in colorectal cancer cells.Conclusion Monensin could suppressed IGF1R expression via increasing IGF1 in colorectal cancer cells. It has the potential to be repurposed as an anti-colorectal cancer agent, but further studies are still required to investigate the detailed mechanisms of monensin underlying its anti-cancer motion.Key MessagesMonensin inhibits the cell proliferation and the migration, induces apoptosis and inhibits cell cycle progression in human colorectal cancer cells.Monensin may exert anti-cancer activity by targeting multiple signaling pathways, including the IGF1R signaling pathway.Monensin has the potential to be repurposed as an anti-colorectal cancer agent.

Published

2023

2. Silicon Radiation Detector Technologies: From Planar to 3D

Author

Gian-Franco Dalla Betta and Jixing Ye

Subjects

silicon radiation detectors, fabrication technology, planar detectors, 3D detectors, Electronic computers. Computer science, QA75.5-76.95, Electric apparatus and materials. Electric circuits. Electric networks, TK452-454.4

Abstract

Silicon radiation detectors, a special type of microelectronic sensor which plays a crucial role in many applications, are reviewed in this paper, focusing on fabrication aspects. After addressing the basic concepts and the main requirements, the evolution of detector technologies is discussed, which has been mainly driven by the ever-increasing demands for frontier scientific experiments.

Published

2023

3. TCAD Analysis of Leakage Current and Breakdown Voltage in Small Pitch 3D Pixel Sensors

Author

Jixing Ye, Abderrezak Boughedda, D M S Sultan, and Gian-Franco Dalla Betta

Subjects

3D pixel sensors, TCAD simulation, breakdown voltage, Chemical technology, TP1-1185

Abstract

Small-pitch 3D pixel sensors have been developed to equip the innermost layers of the ATLAS and CMS tracker upgrades at the High Luminosity LHC. They feature 50 × 50 and 25 × 100 μm2 geometries and are fabricated on p-type Si–Si Direct Wafer Bonded substrates of 150 μm active thickness with a single-sided process. Due to the short inter-electrode distance, charge trapping effects are strongly mitigated, making these sensors extremely radiation hard. Results from beam test measurements of 3D pixel modules irradiated at large fluences (1016neq/cm2) indeed demonstrated high efficiency at maximum bias voltages of the order of 150 V. However, the downscaled sensor structure also lends itself to high electric fields as the bias voltage is increased, meaning that premature electrical breakdown due to impact ionization is a concern. In this study, TCAD simulations incorporating advanced surface and bulk damage models are used to investigate the leakage current and breakdown behavior of these sensors. Simulations are compared with measured characteristics of 3D diodes irradiated with neutrons at fluences up to 1.5 × 1016neq/cm2. The dependence of the breakdown voltage on geometrical parameters (e.g., the n+ column radius and the gap between the n+ column tip and the highly doped p++ handle wafer) is also discussed for optimization purposes.

Published

2023

4. Correction: Adenovirus-Mediated Efficient Gene Transfer into Cultured Three-Dimensional Organoids

Author

Ning Wang, Hongyu Zhang, Bing-Qiang Zhang, Wei Liu, Zhonglin Zhang, Min Qiao, Hongmei Zhang, Fang Deng, Ningning Wu, Xian Chen, Sheng Wen, Junhui Zhang, Zhan Liao, Qian Zhang, Zhengjian Yan, Liangjun Yin, Jixing Ye, Youlin Deng, Hue H. Luu, Rex C. Haydon, Houjie Liang, and Tong-Chuan He

Subjects

Medicine, Science

Published

2021

5. The Calcium-Binding Protein S100A6 Accelerates Human Osteosarcoma Growth by Promoting Cell Proliferation and Inhibiting Osteogenic Differentiation

Author

Yasha Li, Eric R. Wagner, Zhengjian Yan, Zhonliang Wang, Gaurav Luther, Wei Jiang, Jixing Ye, Qiang Wei, Jing Wang, Lianggong Zhao, Shun Lu, Xin Wang, Maryam K. Mohammed, Shengli Tang, Hao Liu, Jiaming Fan, Fugui Zhang, Yulong Zou, Dongzhe Song, Junyi Liao, Rex C. Haydon, Hue H. Luu, and Tong-Chuan He

Subjects

Bone tumor, S100A6, Apoptosis, S100 proteins, BMP9, Osteoblastic differentiation, Mesenchymal stem cells, Osteosarcoma, Physiology, QP1-981, Biochemistry, QD415-436

Abstract

Background/Aims: Although osteosarcoma (OS) is the most common primary malignancy of bone, its molecular pathogenesis remains to be fully understood. We previously found the calcium-binding protein S100A6 was expressed in ∼80% of the analyzed OS primary and/or metastatic tumor samples. Here, we investigate the role of S100A6 in OS growth and progression. Methods: S100A6 expression was assessed by qPCR and Western blotting. Overexpression or knockdown of S100A6 was carried out to determine S100A6's effect on proliferation, cell cycle, apoptosis, tumor growth, and osteogenic differentiation. Results: S100A6 expression was readily detected in human OS cell lines. Exogenous S100A6 expression promoted cell proliferation in vitro and tumor growth in an orthotopic xenograft model of human OS. S100A6 overexpression reduced the numbers of OS cells in G1 phase and increased viable cells under serum starvation condition. Conversely, silencing S100A6 expression induced the production of cleaved caspase 3, and increased early stage apoptosis. S100A6 knockdown increased osteogenic differentiation activity of mesenchymal stem cells, while S100A6 overexpression inhibited osteogenic differentiation. BMP9-induced bone formation was augmented by S100A6 knockdown. Conclusion: Our findings strongly suggest that S100A6 may promote OS cell proliferation and OS tumor growth at least in part by facilitating cell cycle progression, preventing apoptosis, and inhibiting osteogenic differentiation. Thus, it is conceivable that targeting S100A6 may be exploited as a novel anti-OS therapy.

Published

2015

6. Low Magnitude of Compression Enhances Biosynthesis of Mesenchymal Stem Cells towards Nucleus Pulposus Cells via the TRPV4-Dependent Pathway

Author

Yibo Gan, Bing Tu, Pei Li, Jixing Ye, Chen Zhao, Lei Luo, Chengmin Zhang, Zetong Zhang, Linyong Zhu, and Qiang Zhou

Subjects

Internal medicine, RC31-1245

Abstract

Mesenchymal stem cell- (MSC-) based therapy is regarded as a promising tissue engineering strategy to achieve nucleus pulposus (NP) regeneration for the treatment of intervertebral disc degeneration (IDD). However, it is still a challenge to promote the biosynthesis of MSC to meet the requirement of NP regeneration. The purpose of this study was to optimize the compressive magnitude to enhance the extracellular matrix (ECM) deposition towards discogenesis of MSCs. Thus, we constructed a 3D culture model for MSCs to bear different magnitudes of compression for 7 days (5%, 10%, and 20% at the frequency of 1.0 Hz for 8 hours/day) using an intelligent and mechanically active bioreactor. Then, the underlying mechanotransduction mechanism of transient receptor potential vanilloid 4 (TRPV4) was further explored. The MSC-encapsulated hybrids were evaluated by Live/Dead staining, biochemical content assay, real-time PCR, Western blot, histological, and immunohistochemical analysis. The results showed that low-magnitude compression promoted anabolic response where high-magnitude compression induced the catabolic response for the 3D-cultured MSCs. The anabolic effect of low-magnitude compression could be inhibited by inhibiting TRPV4. Meanwhile, the activation of TRPV4 enhanced the biosynthesis analogous to low-magnitude compression. These findings demonstrate that low-magnitude compression promoted the anabolic response of ECM deposition towards discogenesis for the 3D-cultured MSCs and the TRPV4 channel plays a key role on mechanical signal transduction for low-magnitude compressive loading. Further understanding of this mechanism may provide insights into the development of new therapies for MSC-based NP regeneration.

Published

2018

7. Repair of critical sized cranial defects with BMP9-transduced calvarial cells delivered in a thermoresponsive scaffold.

Author

Zari P Dumanian, Viktor Tollemar, Jixing Ye, Minpeng Lu, Yunxiao Zhu, Junyi Liao, Guillermo A Ameer, Tong-Chuan He, and Russell R Reid

Subjects

Medicine, Science

Abstract

Large skeletal defects caused by trauma, congenital malformations, and post-oncologic resections of the calvarium present major challenges to the reconstructive surgeon. We previously identified BMP-9 as the most osteogenic BMP in vitro and in vivo. Here we sought to investigate the bone regenerative capacity of murine-derived calvarial mesenchymal progenitor cells (iCALs) transduced by BMP-9 in the context of healing critical-sized calvarial defects. To accomplish this, the transduced cells were delivered to the defect site within a thermoresponsive biodegradable scaffold consisting of poly(polyethylene glycol citrate-co-N-isopropylacrylamide mixed with gelatin (PPCN-g). A total of three treatment arms were evaluated: PPCN-g alone, PPCN-g seeded with iCALs expressing GFP, and PPCN-g seeded with iCALs expressing BMP-9. Defects treated only with PPCN-g scaffold did not statistically change in size when evaluated at eight weeks postoperatively (p = 0.72). Conversely, both animal groups treated with iCALs showed significant reductions in defect size after 12 weeks of follow-up (BMP9-treated: p = 0.0025; GFP-treated: p = 0.0042). However, H&E and trichrome staining revealed more complete osseointegration and mature bone formation only in the BMP9-treated group. These results suggest that BMP9-transduced iCALs seeded in a PPCN-g thermoresponsive scaffold is capable of inducing bone formation in vivo and is an effective means of creating tissue engineered bone for critical sized defects.

Published

2017

8. Reversibly Immortalized Mouse Articular Chondrocytes Acquire Long-Term Proliferative Capability While Retaining Chondrogenic Phenotype

Author

Joseph D. Lamplot, Bo Liu, Liangjun Yin, Wenwen Zhang, Zhongliang Wang, Gaurav Luther, Eric Wagner, Ruidong Li, Guoxin Nan, Wei Shui, Zhengjian Yan, Richard Rames, Fang Deng, Hongmei Zhang, Zhan Liao, Wei Liu, Junhui Zhang, Zhonglin Zhang, Qian Zhang, Jixing Ye, Youlin Deng, Min Qiao, Rex C. Haydon, Hue H. Luu, Jovito Angeles, Lewis L. Shi, Tong-Chuan He M.D., Ph.D., and Sherwin H. Ho M.D.

Subjects

Medicine

Abstract

Cartilage tissue engineering holds great promise for treating cartilaginous pathologies including degenerative disorders and traumatic injuries. Effective cartilage regeneration requires an optimal combination of biomaterial scaffolds, chondrogenic seed cells, and biofactors. Obtaining sufficient chondrocytes remains a major challenge due to the limited proliferative capability of primary chondrocytes. Here we investigate if reversibly immortalized mouse articular chondrocytes (iMACs) acquire long-term proliferative capability while retaining the chondrogenic phenotype. Primary mouse articular chondrocytes (MACs) can be efficiently immortalized with a retroviral vector-expressing SV40 large T antigen flanked with Cre/loxP sites. iMACs exhibit long-term proliferation in culture, although the immortalization phenotype can be reversed by Cre recombinase. iMACs express the chondrocyte markers Col2a1 and aggrecan and produce chondroid matrix in micromass culture. iMACs form subcutaneous cartilaginous masses in athymic mice. Histologic analysis and chondroid matrix staining demonstrate that iMACs can survive, proliferate, and produce chondroid matrix. The chondrogenic growth factor BMP2 promotes iMACs to produce more mature chondroid matrix resembling mature articular cartilage. Taken together, our results demonstrate that iMACs acquire long-term proliferative capability without losing the intrinsic chondrogenic features of MACs. Thus, iMACs provide a valuable cellular platform to optimize biomaterial scaffolds for cartilage regeneration, to identify biofactors that promote the proliferation and differentiation of chondrogenic progenitors, and to elucidate the molecular mechanisms underlying chondrogenesis.

Published

2015

9. TqPCR: A Touchdown qPCR Assay with Significantly Improved Detection Sensitivity and Amplification Efficiency of SYBR Green qPCR.

Author

Qian Zhang, Jing Wang, Fang Deng, Zhengjian Yan, Yinglin Xia, Zhongliang Wang, Jixing Ye, Youlin Deng, Zhonglin Zhang, Min Qiao, Ruifang Li, Sahitya K Denduluri, Qiang Wei, Lianggong Zhao, Shun Lu, Xin Wang, Shengli Tang, Hao Liu, Hue H Luu, Rex C Haydon, Tong-Chuan He, and Li Jiang

Subjects

Medicine, Science

Abstract

The advent of fluorescence-based quantitative real-time PCR (qPCR) has revolutionized the quantification of gene expression analysis in many fields, including life sciences, agriculture, forensic science, molecular diagnostics, and medicine. While SYBR Green-based qPCR is the most commonly-used platform due to its inexpensive nature and robust chemistry, quantifying the expression of genes with low abundance or RNA samples extracted from highly restricted or limited sources can be challenging because the detection sensitivity of SYBR Green-based qPCR is limited. Here, we develop a novel and effective touchdown qPCR (TqPCR) protocol by incorporating a 4-cycle touchdown stage prior to the quantification amplification stage. Using the same cDNA templates, we find that TqPCR can reduce the average Cq values for Gapdh, Rps13, and Hprt1 reference genes by 4.45, 5.47, and 4.94 cycles, respectively, when compared with conventional qPCR; the overall average Cq value reduction for the three reference genes together is 4.95. We further find that TqPCR can improve PCR amplification efficiency and thus increase detection sensitivity. When the quantification of Wnt3A-induced target gene expression in mesenchymal stem cells is analyzed, we find that, while both conventional qPCR and TqPCR can detect the up-regulation of the relatively abundant target Axin2, only TqPCR can detect the up-regulation of the lowly-expressed targets Oct4 and Gbx2. Finally, we demonstrate that the MRQ2 and MRQ3 primer pairs derived from mouse reference gene Tbp can be used to validate the RNA/cDNA integrity of qPCR samples. Taken together, our results strongly suggest that TqPCR may increase detection sensitivity and PCR amplification efficiency. Overall, TqPCR should be advantageous over conventional qPCR in expression quantification, especially when the transcripts of interest are lowly expressed, and/or the availability of total RNA is highly restricted or limited.

Published

2015

10. Characterization of constitutive promoters for piggyBac transposon-mediated stable transgene expression in mesenchymal stem cells (MSCs).

Author

Sheng Wen, Hongmei Zhang, Yasha Li, Ning Wang, Wenwen Zhang, Ke Yang, Ningning Wu, Xian Chen, Fang Deng, Zhan Liao, Junhui Zhang, Qian Zhang, Zhengjian Yan, Wei Liu, Zhonglin Zhang, Jixing Ye, Youlin Deng, Guolin Zhou, Hue H Luu, Rex C Haydon, Lewis L Shi, Tong-Chuan He, and Guanghui Wei

Subjects

Medicine, Science

Abstract

Multipotent mesenchymal stem cells (MSCs) can undergo self-renewal and give rise to multi-lineages under given differentiation cues. It is frequently desirable to achieve a stable and high level of transgene expression in MSCs in order to elucidate possible molecular mechanisms through which MSC self-renewal and lineage commitment are regulated. Retroviral or lentiviral vector-mediated gene expression in MSCs usually decreases over time. Here, we choose to use the piggyBac transposon system and conduct a systematic comparison of six commonly-used constitutive promoters for their abilities to drive RFP or firefly luciferase expression in somatic HEK-293 cells and MSC iMEF cells. The analyzed promoters include three viral promoters (CMV, CMV-IVS, and SV40), one housekeeping gene promoter (UbC), and two composite promoters of viral and housekeeping gene promoters (hEFH and CAG-hEFH). CMV-derived promoters are shown to drive the highest transgene expression in HEK-293 cells, which is however significantly reduced in MSCs. Conversely, the composite promoter hEFH exhibits the highest transgene expression in MSCs whereas its promoter activity is modest in HEK-293 cells. The reduced transgene expression driven by CMV promoters in MSCs may be at least in part caused by DNA methylation, or to a lesser extent histone deacetlyation. However, the hEFH promoter is not significantly affected by these epigenetic modifications. Taken together, our results demonstrate that the hEFH composite promoter may be an ideal promoter to drive long-term and high level transgene expression using the piggyBac transposon vector in progenitor cells such as MSCs.

Published

2014

11. Adenovirus-mediated efficient gene transfer into cultured three-dimensional organoids.

Author

Ning Wang, Hongyu Zhang, Bing-Qiang Zhang, Wei Liu, Zhonglin Zhang, Min Qiao, Hongmei Zhang, Fang Deng, Ningning Wu, Xian Chen, Sheng Wen, Junhui Zhang, Zhan Liao, Qian Zhang, Zhengjian Yan, Liangjun Yin, Jixing Ye, Youlin Deng, Hue H Luu, Rex C Haydon, Houjie Liang, and Tong-Chuan He

Subjects

Medicine, Science

Abstract

Three-dimensional organoids have been recently established from various tissue-specific progenitors (such as intestinal stem cells), induced pluripotent stem cells, or embryonic stem cells. These cultured self-sustaining stem cell-based organoids may become valuable systems to study the roles of tissue-specific stem cells in tissue genesis and disease development. It is thus conceivable that effective genetic manipulations in such organoids may allow us to reconstruct disease processes and/or develop novel therapeutics. Recombinant adenoviruses are one of the most commonly used viral vectors for in vitro and in vivo gene deliveries. In this study, we investigate if adenoviruses can be used to effectively deliver transgenes into the cultured "mini-gut" organoids derived from intestinal stem cells. Using adenoviral vectors that express fluorescent proteins, we demonstrate that adenoviruses can effectively deliver transgenes into the cultured 3-D "mini-gut" organoids. The transgene expression can last at least 10 days in the cultured organoids. As a proof-of-principle experiment, we demonstrate that adenovirus-mediated noggin expression effectively support the survival and self-renewal of mini-gut organoids, while adenovirus-mediated expression of BMP4 inhibits the self-sustainability and proliferation of the organoids. Thus, our results strongly suggest that adenovirus vectors can be explored as effective gene delivery vehicles to introduce genetic manipulations in 3-D organoids.

Published

2014

12. A simplified and versatile system for the simultaneous expression of multiple siRNAs in mammalian cells using Gibson DNA Assembly.

Author

Fang Deng, Xiang Chen, Zhan Liao, Zhengjian Yan, Zhongliang Wang, Youlin Deng, Qian Zhang, Zhonglin Zhang, Jixing Ye, Min Qiao, Ruifang Li, Sahitya Denduluri, Jing Wang, Qiang Wei, Melissa Li, Nisha Geng, Lianggong Zhao, Guolin Zhou, Penghui Zhang, Hue H Luu, Rex C Haydon, Russell R Reid, Tian Yang, and Tong-Chuan He

Subjects

Medicine, Science

Abstract

RNA interference (RNAi) denotes sequence-specific mRNA degradation induced by short interfering double-stranded RNA (siRNA) and has become a revolutionary tool for functional annotation of mammalian genes, as well as for development of novel therapeutics. The practical applications of RNAi are usually achieved by expressing short hairpin RNAs (shRNAs) or siRNAs in cells. However, a major technical challenge is to simultaneously express multiple siRNAs to silence one or more genes. We previously developed pSOS system, in which siRNA duplexes are made from oligo templates driven by opposing U6 and H1 promoters. While effective, it is not equipped to express multiple siRNAs in a single vector. Gibson DNA Assembly (GDA) is an in vitro recombination system that has the capacity to assemble multiple overlapping DNA molecules in a single isothermal step. Here, we developed a GDA-based pSOK assembly system for constructing single vectors that express multiple siRNA sites. The assembly fragments were generated by PCR amplifications from the U6-H1 template vector pB2B. GDA assembly specificity was conferred by the overlapping unique siRNA sequences of insert fragments. To prove the technical feasibility, we constructed pSOK vectors that contain four siRNA sites and three siRNA sites targeting human and mouse β-catenin, respectively. The assembly reactions were efficient, and candidate clones were readily identified by PCR screening. Multiple β-catenin siRNAs effectively silenced endogenous β-catenin expression, inhibited Wnt3A-induced β-catenin/Tcf4 reporter activity and expression of Wnt/β-catenin downstream genes. Silencing β-catenin in mesenchymal stem cells inhibited Wnt3A-induced early osteogenic differentiation and significantly diminished synergistic osteogenic activity between BMP9 and Wnt3A in vitro and in vivo. These findings demonstrate that the GDA-based pSOK system has been proven simplistic, effective and versatile for simultaneous expression of multiple siRNAs. Thus, the reported pSOK system should be a valuable tool for gene function studies and development of novel therapeutics.

Published

2014

13. Adenovirus-mediated gene transfer in mesenchymal stem cells can be significantly enhanced by the cationic polymer polybrene.

Author

Chen Zhao, Ningning Wu, Fang Deng, Hongmei Zhang, Ning Wang, Wenwen Zhang, Xian Chen, Sheng Wen, Junhui Zhang, Liangjun Yin, Zhan Liao, Zhonglin Zhang, Qian Zhang, Zhengjian Yan, Wei Liu, Di Wu, Jixing Ye, Youlin Deng, Guolin Zhou, Hue H Luu, Rex C Haydon, Weike Si, and Tong-Chuan He

Subjects

Medicine, Science

Abstract

Mesenchymal stem cells (MSCs) are multipotent progenitors, which can undergo self-renewal and give rise to multi-lineages. A great deal of attentions have been paid to their potential use in regenerative medicine as potential therapeutic genes can be introduced into MSCs. Genetic manipulations in MSCs requires effective gene deliveries. Recombinant adenoviruses are widely used gene transfer vectors. We have found that although MSCs can be infected in vitro by adenoviruses, high virus titers are needed to achieve high efficiency. Here, we investigate if the commonly-used cationic polymer Polybrene can potentiate adenovirus-mediated transgene delivery into MSCs, such as C2C12 cells and iMEFs. Using the AdRFP adenovirus, we find that AdRFP transduction efficiency is significantly increased by Polybrene in a dose-dependent fashion peaking at 8 μg/ml in C2C12 and iMEFs cells. Quantitative luciferase assay reveals that Polybrene significantly enhances AdFLuc-mediated luciferase activity in C2C12 and iMEFs at as low as 4 μg/ml and 2 μg/ml, respectively. FACS analysis indicates that Polybrene (at 4 μg/ml) increases the percentage of RFP-positive cells by approximately 430 folds in AdRFP-transduced iMEFs, suggesting Polybrene may increase adenovirus infection efficiency. Furthermore, Polybrene can enhance AdBMP9-induced osteogenic differentiation of MSCs as early osteogenic marker alkaline phosphatase activity can be increased more than 73 folds by Polybrene (4 μg/ml) in AdBMP9-transduced iMEFs. No cytotoxicity was observed in C2C12 and iMEFs at Polybrene up to 40 μg/ml, which is about 10-fold higher than the effective concentration required to enhance adenovirus transduction in MSCs. Taken together, our results demonstrate that Polybrene should be routinely used as a safe, effective and inexpensive augmenting agent for adenovirus-mediated gene transfer in MSCs, as well as other types of mammalian cells.

Published

2014

14. The piggyBac transposon-mediated expression of SV40 T antigen efficiently immortalizes mouse embryonic fibroblasts (MEFs).

Author

Ning Wang, Wenwen Zhang, Jing Cui, Hongmei Zhang, Xiang Chen, Ruidong Li, Ningning Wu, Xian Chen, Sheng Wen, Junhui Zhang, Liangjun Yin, Fang Deng, Zhan Liao, Zhonglin Zhang, Qian Zhang, Zhengjian Yan, Wei Liu, Jixing Ye, Youlin Deng, Zhongliang Wang, Min Qiao, Hue H Luu, Rex C Haydon, Lewis L Shi, Houjie Liang, and Tong-Chuan He

Subjects

Medicine, Science

Abstract

Mouse embryonic fibroblasts (MEFs) are mesenchymal stem cell (MSC)-like multipotent progenitor cells and can undergo self-renewal and differentiate into to multiple lineages, including bone, cartilage and adipose. Primary MEFs have limited life span in culture, which thus hampers MEFs' basic research and translational applications. To overcome this challenge, we investigate if piggyBac transposon-mediated expression of SV40 T antigen can effectively immortalize mouse MEFs and that the immortalized MEFs can maintain long-term cell proliferation without compromising their multipotency. Using the piggyBac vector MPH86 which expresses SV40 T antigen flanked with flippase (FLP) recognition target (FRT) sites, we demonstrate that mouse embryonic fibroblasts (MEFs) can be efficiently immortalized. The immortalized MEFs (piMEFs) exhibit an enhanced proliferative activity and maintain long-term cell proliferation, which can be reversed by FLP recombinase. The piMEFs express most MEF markers and retain multipotency as they can differentiate into osteogenic, chondrogenic and adipogenic lineages upon BMP9 stimulation in vitro. Stem cell implantation studies indicate that piMEFs can form bone, cartilage and adipose tissues upon BMP9 stimulation, whereas FLP-mediated removal of SV40 T antigen diminishes the ability of piMEFs to differentiate into these lineages, possibly due to the reduced expansion of progenitor populations. Our results demonstrate that piggyBac transposon-mediated expression of SV40 T can effectively immortalize MEFs and that the reversibly immortalized piMEFs not only maintain long-term cell proliferation but also retain their multipotency. Thus, the high transposition efficiency and the potential footprint-free natures may render piggyBac transposition an effective and safe strategy to immortalize progenitor cells isolated from limited tissue supplies, which is essential for basic and translational studies.

Published

2014

15. Injectable, Hierarchically Degraded Bioactive Scaffold for Bone Regeneration

Author

Jixing Ye, Ningyuan Liu, Zongxin Li, Liehua Liu, Ming Zheng, Xueping Wen, Nan Wang, Yanqin Xu, Biemin Sun, and Qiang Zhou

Subjects

General Materials Science

Published

2023

16. Optimization of rapid-repair material ratio and performance analysis based on orthogonal test

Author

Jixing, Ye, primary, Zhu, Pan, additional, and Junhui, Luo, additional

Published

2023

17. SIRT1 alleviates high-magnitude compression-induced senescence in nucleus pulposus cells via PINK1-dependent mitophagy

Author

Lei Luo, Haoming Wang, Pei Li, Yunyun Zhuo, Qiang Zhou, Zetong Zhang, Yanzhu Hu, Yiyang Wang, Chen Zhao, Jixing Ye, and Liehua Liu

Subjects

Adult, Male, Senescence, Aging, Nucleus Pulposus, senescence, Cell, Regulator, PINK1, Intervertebral Disc Degeneration, Pathogenesis, Bioreactors, SIRT1, Sirtuin 1, Mitophagy, Pressure, medicine, Humans, Cells, Cultured, Cellular Senescence, Cell phenotype, Chemistry, Cell Biology, Middle Aged, compression, Mitochondria, Cell biology, Oxidative Stress, medicine.anatomical_structure, Female, Stress, Mechanical, Protein Kinases, Nucleus, Signal Transduction, Research Paper

Abstract

Mechanical overloading-induced nucleus pulposus (NP) cells senescence plays an important role in the pathogenesis of intervertebral disc degeneration (IVDD). The silent mating type information regulator 2 homolog-1 (SIRT1)-mediated pathway preserves the normal NP cell phenotype and mitochondrial homeostasis under multiple stresses. We aimed to investigate the role of SIRT1 in IVDD by assessing the effects of SIRT1 overexpression on high-magnitude compression-induced senescence in NP cells. High-magnitude compression induced cellular senescence and mitochondrial dysfunction in human NP cells. Moreover, SIRT1 overexpression tended to alleviate NP cell senescence and mitochondrial dysfunction under compressive stress. Given the mitophagy-inducing property of SIRT1, activity of mitophagy was evaluated in NP cells to further demonstrate the underlying mechanism. The results showed that SIRT1-overexpression attenuated senescence and mitochondrial injury in NP cells subjected to high-magnitude compression. However, depletion of PINK1, a key mitophagic regulator, impaired mitophagy and blocked the protective role of SIRT1 against compression induced senescence in NP cells. In summary, these results suggest that SIRT1 plays a protective role in alleviating NP cell senescence and mitochondrial dysfunction under high-magnitude compression, the mechanism of which is associated with the regulation of PINK1-dependent mitophagy. Our findings may provide a potential therapeutic approach for IVDD treatment.

Published

2020

18. Correction: Adenovirus-Mediated Efficient Gene Transfer into Cultured Three-Dimensional Organoids

Author

Rex C. Haydon, Sheng Wen, Ning Wang, Xian Chen, Hongmei Zhang, Min Qiao, Youlin Deng, Wei Liu, Zhan Liao, Tong-Chuan He, Zhengjian Yan, Liangjun Yin, Bing-Qiang Zhang, Jixing Ye, Qian Zhang, Hongyu Zhang, Junhui Zhang, Fang Deng, Houjie Liang, Zhonglin Zhang, Ningning Wu, and Hue H. Luu

Subjects

Multidisciplinary, Chemistry, Science, Organoid, Medicine, Gene transfer, Cell biology

Abstract

[This corrects the article DOI: 10.1371/journal.pone.0093608.].

Published

2021

19. BMP9 induces osteogenesis and adipogenesis in the immortalized human cranial suture progenitors from the patent sutures of craniosynostosis patients

Author

Qiang Wei, Michael J. Lee, Xingye Wu, Shujuan Yan, Chao Ma, Yulong Zou, Wenwen Zhang, Xue Hu, Chen Zhao, Junyi Liao, Yichun Yu, Xiangyang Qu, Russell R. Reid, Yasha Li, Tong-Chuan He, Dongzhe Song, Zongyue Zeng, Yi Shu, Fugui Zhang, Li Li, Xinyi Yu, Tingting Wu, Jiaming Fan, Jia Wang, Dingming Huang, Zhicai Zhang, Jixing Ye, Liqun Chen, Jiayan Lei, Ruyi Zhang, and Jennifer Moriatis Wolf

Subjects

0301 basic medicine, Male, Mesenchyme, osteogenic differentiation, Gene Expression, Simian virus 40, Biology, BMP9, Craniosynostosis, adipogenesis, 03 medical and health sciences, Craniosynostoses, Transformation, Genetic, Tissue engineering, Suture (anatomy), cell immortalization, Osteogenesis, medicine, Adipocytes, Growth Differentiation Factor 2, Humans, Progenitor cell, Cell Line, Transformed, Cell Proliferation, suture‐derived stem cells, Osteoblasts, Mesenchymal stem cell, Infant, Cell Differentiation, Mesenchymal Stem Cells, Cell Biology, Anatomy, Original Articles, Cranial Sutures, medicine.disease, Founder Effect, Cell biology, Growth Differentiation Factors, craniosynostosis, 030104 developmental biology, medicine.anatomical_structure, Intramembranous ossification, Molecular Medicine, Original Article, Bone marrow, cranial suture

Abstract

The cranial suture complex is a heterogeneous tissue consisting of osteogenic progenitor cells and mesenchymal stem cells (MSCs) from bone marrow and suture mesenchyme. The fusion of cranial sutures is a highly coordinated and tightly regulated process during development. Craniosynostosis is a congenital malformation caused by premature fusion of cranial sutures. While the progenitor cells derived from the cranial suture complex should prove valuable for studying the molecular mechanisms underlying suture development and pathogenic premature suture fusion, primary human cranial suture progenitors (SuPs) have limited life span and gradually lose osteoblastic ability over passages. To overcome technical challenges in maintaining sufficient and long‐term culture of SuPs for suture biology studies, we establish and characterize the reversibly immortalized human cranial suture progenitors (iSuPs). Using a reversible immortalization system expressing SV40 T flanked with FRT sites, we demonstrate that primary human suture progenitor cells derived from the patent sutures of craniosynostosis patients can be efficiently immortalized. The iSuPs maintain long‐term proliferative activity, express most of the consensus MSC markers and can differentiate into osteogenic and adipogenic lineages upon BMP9 stimulation in vitro and in vivo. The removal of SV40 T antigen by FLP recombinase results in a decrease in cell proliferation and an increase in the endogenous osteogenic and adipogenic capability in the iSuPs. Therefore, the iSuPs should be a valuable resource to study suture development, intramembranous ossification and the pathogenesis of craniosynostosis, as well as to explore cranial bone tissue engineering.

Published

2017

20. The Prodomain-Containing BMP9 Produced from a Stable Line Effectively Regulates the Differentiation of Mesenchymal Stem Cells

Author

Minpeng Lu, Ruifang Li, Fugui Zhang, Shengli Tang, Zhonglin Zhang, Feng Liu, Jiaming Fan, Tong-Chuan He, Michael J Lee, Junyi Liao, Dongzhe Song, Jixing Ye, Lianggong Zhao, Yulong Zou, Zhengjian Yan, Qiang Wei, Aravind Athiviraham, Shun Lu, Jing Wang, Lewis L. Shi, Xin Wang, He Huang, and Zhongliang Wang

Subjects

0301 basic medicine, Signal peptide, Cellular differentiation, GDF2, osteogenic differentiation, SMAD, Biology, Bioinformatics, BMP9, recombinant proteins, 03 medical and health sciences, Mice, stem cells, Osteogenesis, Growth Differentiation Factor 2, Animals, Humans, HEK 293 cells, Mesenchymal stem cell, Cell Differentiation, Mesenchymal Stem Cells, General Medicine, In vitro, Cell biology, 030104 developmental biology, conditioned medium, HEK293 Cells, Culture Media, Conditioned, Stem cell, Research Paper

Abstract

Background: BMPs play important roles in regulating stem cell proliferation and differentiation. Using adenovirus-mediated expression of the 14 types of BMPs we demonstrated that BMP9 is one of the most potent BMPs in inducing osteogenic differentiation of mesenchymal stem cells (MSCs), which was undetected in the early studies using recombinant BMP9 proteins. Endogenous BMPs are expressed as a precursor protein that contains an N-terminal signal peptide, a prodomain and a C-terminal mature peptide. Most commercially available recombinant BMP9 proteins are purified from the cells expressing the mature peptide. It is unclear how effectively these recombinant BMP9 proteins functionally recapitulate endogenous BMP9. Methods: A stable cell line expressing the full coding region of mouse BMP9 was established in HEK-293 cells by using the piggyBac transposon system. The biological activities and stability of the conditioned medium generated from the stable line were analyzed. Results: The stable HEK-293 line expresses a high level of mouse BMP9. BMP9 conditioned medium (BMP9-cm) was shown to effectively induce osteogenic differentiation of MSCs, to activate BMP-R specific Smad signaling, and to up-regulate downstream target genes in MSCs. The biological activity of BMP9-cm is at least comparable with that induced by AdBMP9 in vitro. Furthermore, BMP9-cm exhibits an excellent stability profile as its biological activity is not affected by long-term storage at -80oC, repeated thawing cycles, and extended storage at 4oC. Conclusions: We have established a producer line that stably expresses a high level of active BMP9 protein. Such producer line should be a valuable resource for generating biologically active BMP9 protein for studying BMP9 signaling mechanism and functions.

Published

2016

21. Multifaceted signaling regulators of chondrogenesis: Implications in cartilage regeneration and tissue engineering

Author

Tong-Chuan He, Hue H. Luu, Viktor Tollemar, Rex C. Haydon, Liangjun Yin, Lewis L. Shi, Maryam K. Mohammed, Mark C. Dougherty, Jixing Ye, Aravind Athiviraham, Michael J Lee, Richard W. Kang, Zhengjian Yan, Jordan D. Green, Zachary J Collier, and Sherwin H. Ho

Subjects

Cell signaling, Pathology, medicine.medical_specialty, BMPs, Biology, Fibroblast growth factor, Biochemistry, Article, Wnt, TGFβ, 03 medical and health sciences, 0302 clinical medicine, Tissue engineering, medicine, FGF, Molecular Biology, Genetics (clinical), 030304 developmental biology, 0303 health sciences, Hyaline cartilage, Regeneration (biology), Cartilage, Wnt signaling pathway, Cell Biology, Chondrogenesis, Cell biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Regenerative medicine, Hedgehog, Sox9

Abstract

Defects of articular cartilage present a unique clinical challenge due to its poor self-healing capacity and avascular nature. Current surgical treatment options do not ensure consistent regeneration of hyaline cartilage in favor of fibrous tissue. Here, we review the current understanding of the most important biological regulators of chondrogenesis and their interactions, to provide insight into potential applications for cartilage tissue engineering. These include various signaling pathways, including fibroblast growth factors (FGFs), transforming growth factor β (TGF-β)/bone morphogenic proteins (BMPs), Wnt/β-catenin, Hedgehog, Notch, hypoxia, and angiogenic signaling pathways. Transcriptional and epigenetic regulation of chondrogenesis will also be discussed. Advances in our understanding of these signaling pathways have led to promising advances in cartilage regeneration and tissue engineering.

Published

2015

22. Whole-Proteome Analysis of Human Craniosynostotic Tissue Suggests a Link between Inflammatory Signaling and Osteoclast Activation in Human Cranial Suture Patency

Author

Russell R. Reid, David M. Frim, Sarah Lyon, M. Rose Rogers, Michael Januszyk, Tong-Chuan He, Dongzhe Song, Ashley Ralston, Jixing Ye, and Anoop Mayampurath

Subjects

0301 basic medicine, Proteomics, Adolescent, Proteome, Osteoclasts, Collagen Type VI, Bioinformatics, Real-Time Polymerase Chain Reaction, Craniosynostosis, 03 medical and health sciences, Craniosynostoses, 0302 clinical medicine, Downregulation and upregulation, Osteoclast, Tandem Mass Spectrometry, medicine, Humans, RNA, Messenger, Child, Chromatography, High Pressure Liquid, Fibrous joint, Extracellular Matrix Proteins, business.industry, Cranial Sutures, medicine.disease, Immunohistochemistry, Pathophysiology, Up-Regulation, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Child, Preschool, Surgery, Proteoglycans, Signal transduction, business, Signal Transduction

Abstract

The pathophysiology of nonsyndromic craniosynostosis remains poorly understood. The authors seek to understand the cause of this condition with a specific focus on how osteoclasts may contribute to craniosynostosis. Here, the authors characterize proteins differentially expressed in patent and fused cranial sutures by comparing their respective proteomes.Fused and patent suture samples were obtained from craniosynostotic patients undergoing surgery at a single academic medical center. Extracted protein from samples was interrogated using mass spectrometry. Differential protein expression was determined using maximum likelihood-based G-test with a q-value cutoffs of 0.5 after correction for multiple hypothesis testing. Immunolocalization of lead protein candidates was performed to validate proteomic findings. In addition, quantitative polymerase chain reaction analysis of corresponding gene expression of proteins of interest was performed.Proteins differentially expressed in patent versus fused sutures included collagen 6A1 (Col6A1), fibromodulin, periostin, aggrecan, adipocyte enhancer-binding protein 1, and osteomodulin (OMD). Maximum likelihood-based G-test suggested that Col6A1, fibromodulin, and adipocyte enhancer-binding protein 1 are highly expressed in patent sutures compared with fused sutures, whereas OMD is up-regulated in fused sutures compared with patent sutures. These results were corroborated by immunohistochemistry. Quantitative polymerase chain reaction data point to an inverse relationship in proteins of interest to RNA transcript levels, in prematurely fused and patent sutures that potentially describes a feedback loop mechanism.Proteome analysis validated by immunohistochemistry may provide insight into the mechanism of cranial suture patency and disease from an osteoclast perspective. The authors results suggest a role of inflammatory mediators in nonsyndromic craniosynostosis. Col6A1 may aid in the regulation of suture patency, and OMD may be involved in premature fusion. Additional validation studies are required.

Published

2018

23. The Anthelmintic Drug Niclosamide Inhibits the Proliferative Activity of Human Osteosarcoma Cells by Targeting Multiple Signal Pathways

Author

Zhongliang Wang, Guoxin Nan, Hue H. Luu, Jixing Ye, Jing Wang, Zhonglin Zhang, Guolin Zhou, Ruifang Li, Zhan Liao, Shun Lu, Min Qiao, Zhengjian Yan, Nisha Geng, Tong-Chuan He, Rex C. Haydon, Liyi Zeng, Qiang Wei, Youlin Deng, Xin Wang, Sahitya K. Denduluri, and Lianggong Zhao

Subjects

Cancer Research, Cell Survival, Notch signaling pathway, Mice, Nude, Antineoplastic Agents, Bone Neoplasms, Biology, Pharmacology, Mice, Drug Delivery Systems, Cell Movement, Cell Line, Tumor, Drug Discovery, Biomarkers, Tumor, medicine, Animals, Humans, Niclosamide, Cell Proliferation, Anthelmintics, Osteosarcoma, Cell growth, Wnt signaling pathway, NFAT, Cell migration, medicine.disease, Xenograft Model Antitumor Assays, Oncology, Apoptosis, Female, Signal Transduction, medicine.drug

Abstract

Osteosarcoma (OS) is the most common primary malignant tumor of bone with a high propensity for lung metastasis. Despite significant advances in surgical techniques and chemotherapeutic regimens over the past few decades, there has been minimal improvement in OS patient survival. There is an urgent need to identify novel antitumor agents to treat human OS. Repurposing the clinically-used drugs represents a rapid and effective approach to the development of new anticancer agents. The anthelmintic drug niclosamide has recently been identified as a potential anticancer agent in human cancers. Here, we investigate if niclosamide can be developed as an anti-OS drug. We find that niclosamide can effectively inhibit OS cell proliferation and survival at low micromolar concentrations. Cell migration and wounding closure are significantly inhibited by niclosamide. Niclosamide induces cell apoptosis and inhibits cell cycle progression in OS cells. Analysis of niclosamide's effect on 11 cancer-related signal pathway reporters reveals that three of them, the E2F1, AP1, and c-Myc-responsive reporters, are significantly inhibited. To a lesser extent, the HIF1α, TCF/LEF, CREB, NFκB, Smad/TGFβ, and Rbpj/Notch pathway reporters are also inhibited, while the NFAT and Wnt/β-catenin reporters are not significantly affected by niclosamide treatment. We demonstrate that the expression of c-Fos, c-Jun. E2F1, and c-Myc in OS cells is effectively inhibited by niclosamide. Furthermore, niclosamide is shown to effectively inhibit tumor growth in a mouse xenograft tumor model of human osteosarcoma cells. Taken together, these results strongly suggest that niclosamide may exert its anticancer activity in OS cells by targeting multiple signaling pathways. Future investigations should be directed to exploring the antitumor activity in clinically relevant OS models and ultimately in clinical trials.

Published

2015

24. Insulin-like growth factor (IGF) signaling in tumorigenesis and the development of cancer drug resistance

Author

Qiang Wei, Zhengjian Yan, Jixing Ye, Sahitya K. Denduluri, Zhan Liao, Jing Jing Wang, Maryam K. Mohammed, Hue H. Luu, Olumuyiwa Idowu, Zhongliang Wang, and Lianggong Zhao

Subjects

Drug, Basic science, medicine.medical_treatment, media_common.quotation_subject, Resistance, Drug resistance, medicine.disease_cause, Bioinformatics, Biochemistry, Article, Insulin-like growth factor, medicine, Molecular Biology, Genetics (clinical), Sensitization, Cancer, media_common, business.industry, Growth factor, Cell Biology, medicine.disease, 3. Good health, medicine.anatomical_structure, Tumorigenesis, Therapy, business, Carcinogenesis

Abstract

One of the greatest obstacles to current cancer treatment efforts is the development of drug resistance by tumors. Despite recent advances in diagnostic practices and surgical interventions, many neoplasms demonstrate poor response to adjuvant or neoadjuvant radiation and chemotherapy. As a result, the prognosis for many patients afflicted with these aggressive cancers remains bleak. The insulin-like growth factor (IGF) signaling axis has been shown to play critical role in the development and progression of various tumors. Many basic science and translational studies have shown that IGF pathway modulators can have promising effects when used to treat various malignancies. There also exists a substantial body of recent evidence implicating IGF signaling dysregulation in the dwindling response of tumors to current standard-of-care therapy. By better understanding both the IGF-dependent and -independent mechanisms by which pathway members can influence drug sensitivity, we can eventually aim to use modulators of IGF signaling to augment the effects of current therapy. This review summarizes and synthesizes numerous recent investigations looking at the role of the IGF pathway in drug resistance. We offer a brief overview of IGF signaling and its general role in neoplasia, and then delve into detail about the many types of human cancer that have been shown to have IGF pathway involvement in resistance and/or sensitization to therapy. Ultimately, our hope is that such a compilation of evidence will compel investigators to carry out much needed studies looking at combination treatment with IGF signaling modulators to overcome current therapy resistance.

Published

2015

25. Canonical Wnt signaling acts synergistically on BMP9-induced osteo/odontoblastic differentiation of stem cells of dental apical papilla (SCAPs)

Author

Feng Deng, Zhonglin Zhang, Zhongliang Wang, Tong-Chuan He, Hue H. Luu, Rex C. Haydon, Zhengjian Yan, Jinhua Wang, Fang Deng, Qian Zhang, Jing Wang, Enyi Huang, Min Qiao, Qiang Wei, Youlin Deng, Hongmei Zhang, Jixing Ye, Ruifang Li, and Guolin Zhou

Subjects

Male, Cellular differentiation, Mice, 0302 clinical medicine, Osteopontin, Mice, Inbred BALB C, 0303 health sciences, biology, Stem Cells, Wnt signaling pathway, Growth differentiation factor, Cell Differentiation, Drug Synergism, Cell biology, Growth Differentiation Factors, Stem cells of apical papilla, Mechanics of Materials, 030220 oncology & carcinogenesis, embryonic structures, Osteocalcin, Odontogenesis, Female, Stem cell, Signal Transduction, medicine.medical_specialty, BMP signaling, Biophysics, Mice, Nude, Odontoblastic differentiation, Bioengineering, Dontogenesis, Article, Cell Line, Biomaterials, 03 medical and health sciences, stomatognathic system, Internal medicine, medicine, Animals, Humans, Dental papilla, Dental Papilla, 030304 developmental biology, Gossypol, Rats, Wnt Proteins, Endocrinology, Dental stem cells, Ceramics and Composites, biology.protein, WNT3A, HeLa Cells, Wnt/β-catenin signaling

Abstract

Dental pulp/dentin regeneration using dental stem cells combined with odontogenic factors may offer great promise to treat and/or prevent premature tooth loss. Here, we investigate if BMP9 and Wnt/β-catenin act synergistically on odontogenic differentiation. Using the immortalized SCAPs (iSCAPs) isolated from mouse apical papilla tissue, we demonstrate that Wnt3A effectively induces early osteogenic marker alkaline phosphatase (ALP) in iSCAPs, which is reduced by β-catenin knockdown. While Wnt3A and BMP9 enhance each other's ability to induce ALP activity in iSCAPs, silencing β-catenin significantly diminishes BMP9-induced osteo/odontogenic differentiation. Furthermore, silencing β-catenin reduces BMP9-induced expression of osteocalcin and osteopontin and in vitro matrix mineralization of iSCAPs. In vivo stem cell implantation assay reveals that while BMP9-transduced iSCAPs induce robust ectopic bone formation, iSCAPs stimulated with both BMP9 and Wnt3A exhibit more mature and highly mineralized trabecular bone formation. However, knockdown of β-catenin in iSCAPs significantly diminishes BMP9 or BMP9/Wnt3A-induced ectopic bone formation in vivo. Thus, our results strongly suggest that β-catenin may play an important role in BMP9-induced osteo/ondontogenic signaling and that BMP9 and Wnt3A may act synergistically to induce osteo/odontoblastic differentiation of iSCAPs. It's conceivable that BMP9 and/or Wnt3A may be explored as efficacious biofactors for odontogenic regeneration and tooth engineering.

Published

2015

26. Bone morphogenetic protein 2 inhibits the proliferation and growth of human colorectal cancer cells

Author

Ning Wang, Liangjun Yin, Bing-Qiang Zhang, Zhonglin Zhang, Fang Deng, Rex C. Haydon, Xian Chen, Zhongliang Wang, Lan Zhou, Hue H. Luu, Wei Liu, Hongyu Zhang, Qian Zhang, Min Qiao, Liyi Zeng, Tong-Chuan He, Zhan Liao, Junhui Zhang, Jixing Ye, Zhengjian Ya, Youlin Deng, and Yunyuan Zhang

Subjects

Cancer Research, Colorectal cancer, Bone Morphogenetic Protein 2, Apoptosis, Mice, 0302 clinical medicine, Cell Movement, Medicine, 0303 health sciences, Wnt signaling pathway, Combination chemotherapy, Articles, General Medicine, Dependovirus, Cell cycle, 3. Good health, Oncology, 030220 oncology & carcinogenesis, embryonic structures, intestinal epithelial cells, Colorectal Neoplasms, BMP signaling, animal structures, proliferation, Genetic Vectors, BMP2, Mice, Nude, colorectal cancer, Bone morphogenetic protein, Bone morphogenetic protein 2, 03 medical and health sciences, Animals, Humans, Neoplasm Invasiveness, neoplasms, Cell Proliferation, 030304 developmental biology, Oncogene, business.industry, Cancer, Genetic Therapy, HCT116 Cells, medicine.disease, digestive system diseases, tumorigenesis, HEK293 Cells, Immunology, Cancer research, business, Neoplasm Transplantation

Abstract

Colorectal cancer (CRC) is one of the most deadly cancers worldwide. Significant progress has been made in understanding the molecular pathogenesis of CRC, which has led to successful early diagnosis, surgical intervention and combination chemotherapy. However, limited therapeutic options are available for metastatic and/or drug-resistant CRC. While the aberrantly activated Wnt/β-catenin pathway plays a critical initiating role in CRC development, disruption of the bone morphogenetic protein (BMP) pathway causes juvenile polyposis syndrome, suggesting that BMP signaling may play a role in CRC development. However, conflicting results have been reported concerning the possible roles of BMP signaling in sporadic colon cancer. Here, we investigated the effect of BMP2 on the proliferation, migration, invasiveness and tumor growth capability of human CRC cells. Using an adenovirus vector that overexpresses BMP2 and the piggyBac transposon-mediated stable BMP2 overexpression CRC line, we found that exogenous BMP2 effectively inhibited HCT116 cell proliferation and colony formation. BMP2 was shown to suppress colon cancer cell migration and invasiveness. Under a low serum culture condition, forced expression of BMP2 induced a significantly increased level of apoptosis in HCT116 cells. Using a xenograft tumor model, we found that forced expression of BMP2 in HCT116 cells suppressed tumor growth, accompanied by decreased cell proliferation activity. Taken together, our results strongly suggest that BMP2 plays an important inhibitory role in governing the proliferation and aggressive features of human CRC cells.

Published

2014

27. Targeting BMP9-Promoted Human Osteosarcoma Growth by Inactivation of Notch Signaling

Author

Wei Liu, Rex C. Haydon, Wenwen Zhang, Hongyu Zhang, Junhui Zhang, Guoxin Nan, Tong-Chuan He, Qian Zhang, Zhan Liao, Hue H. Luu, Liangjun Yin, Yang Wang, Jing Cui, Zhengjian Yan, Fang Deng, Ruidong Li, Wei Shui, Youlin Deng, Zhonglin Zhang, Ningning Wu, Sheng Wen, Ning Wang, Xian Chen, Hongmei Zhang, Guolin Zhou, Zhong-Liang Deng, and Jixing Ye

Subjects

Pharmacology, JAG2, Osteosarcoma, Cancer Research, JAG1, Cell growth, Notch signaling pathway, Cell cycle, Biology, medicine.disease_cause, medicine.disease, Metastasis, Oncology, Cell Line, Tumor, Drug Discovery, Immunology, Growth Differentiation Factor 2, medicine, Cancer research, Humans, Carcinogenesis, Cell Division

Abstract

Osteosarcoma (OS) is the most common primary malignancy of bone and is usually associated with poor prognosis due to its high incidence of metastasis and chemoresistance. Molecular pathogenesis of OS is poorly understood. We previously showed that OS cells are refractory to BMP9-induced osteogenesis and respond favorably to proliferation and tumor growth. Here we investigate if Notch signaling mediates the BMP9-promoted cell proliferation and tumor growth of human osteosarcoma (OS). We find that the expression of Notch1, Notch2, Notch3, DLL1, JAG1 and JAG2 is readily detected in most of the tested OS cell lines. BMP9-promoted OS cell proliferation, migration, and cell cycle S/G2 progression are effectively inhibited by a dominant-negative mutant of Notch1 (dnNotch1) or the γ-secretase inhibitor Compound E (ComE). Furthermore, BMP9-promoted tumor growth and osteolytic lesions in vivo are significantly inhibited by dnNotch1. BMP9 up-regulates the expression of Notch1, Notch3, DLL1, and JAG1 in OS cells. Accordingly, BMP9 stimulation induces a nuclear accumulation of NICD, which is blocked by ComE. Our results demonstrate that BMP9-promoted OS proliferation and tumor growth is at least in part mediated by Notch signaling, suggesting that osteogenic BMPs may function as upstream regulators of Notch signaling in OS tumorigenesis. Thus, pharmacologic intervention of Notch signaling may be explored as a new therapeutic strategy for human OS tumors.

Published

2014

28. Insider information: Testing cancer drug sensitivity for personalized therapy

Author

Hue H. Luu, Qiang Wei, Rex C. Haydon, Xin Xin Wang, Tong-Chuan He, Maryam K. Mohammed, Jing Wang, Sahitya K. Denduluri, and Jixing Ye

Subjects

medicine.medical_specialty, Cancer drugs, Alternative medicine, Drug resistance, Pharmacology, Biochemistry, Article, Insider, 03 medical and health sciences, 0302 clinical medicine, Chemotherapy, Medicine, Personalized therapy, Intensive care medicine, Molecular Biology, Genetics (clinical), Cancer, 030304 developmental biology, 0303 health sciences, Drug discovery, business.industry, Cell Biology, medicine.disease, Personalized medicine, 3. Good health, Drug screening, 030220 oncology & carcinogenesis, business

Abstract

Cancer death is usually caused by incurable drug-resistant and metastatic cancers. Although tremendous progress has been made in anticancer drug development during the past two decades, cancer medicine still faces unprecedented challenges associated with choosing effective treatments for individual patients. Three recent reports have offered encouraging approaches towards potentially personalized cancer drug selection.

Published

2015

29. Adenovirus-Mediated Wnt5a Expression Inhibits the Telogen-To-Anagen Transition of Hair Follicles in Mice

Author

Tian Yang, Xiaohua Lian, Long He, Ke Yang, Fang Deng, Haiying Guo, Yuhong Li, Yizhan Xing, Ruimin Wang, and Jixing Ye

Subjects

Cell type, Hair growth, In situ hybridization, Biology, Real-Time Polymerase Chain Reaction, Wnt-5a Protein, Adenoviridae, Wnt signaling pathway, Mice, Hair cycle, medicine, Animals, Oligonucleotide Array Sequence Analysis, integumentary system, Gene Expression Profiling, General Medicine, Wnt5a, Hair follicle, Molecular biology, WNT5A, body regions, Mice, Inbred C57BL, Wnt Proteins, Dermal papillae, medicine.anatomical_structure, embryonic structures, Microscopy, Electron, Scanning, Hair cell, sense organs, Research Paper, Hair

Abstract

The canonical Wnt/β-catenin pathway plays an important role in hair cycle induction. Wnt5a is a non-canonical Wnt family member that generally antagonizes canonical Wnt signaling in other systems. In hair follicles, Wnt5a and canonical Wnt are both expressed in cells in the telogen stage. Wnt5a has been shown to be critical for controlling hair cell fate. However, the role that Wnt5a plays in the transition from the telogen to anagen stage is unknown. In this study, using whole-mount in situ hybridization, we show that Wnt5a is produced by several other cell types, excluding dermal papilla cells, throughout the hair cycle. For example, Wnt5a is expressed in bulge and secondary hair germ cells in the telogen stage. Our studies focused on the depilated 8-week-old mouse as a synchronized model of hair growth. Interestingly, overexpression of adenovirus Wnt5a in the dorsal skin of mice led to the elongation of the telogen stage and inhibition of the initiation of the anagen stage. However, following an extended period of time, four pelage hair types grew from hairless skin that was induced by Wnt5a, and the structure of these new hair shafts was normal. Using microarray analysis and quantitative arrays, we showed that the expression of β-catenin and some target genes of canonical Wnt signaling decreased after Wnt5a treatment. These data demonstrate that Wnt5a may inhibit the telogen stage to maintain a quiescent state of the hair follicle.

Published

2013

30. Immortalized Mouse Achilles Tenocytes Demonstrate Long-Term Proliferative Capacity While Retaining Tenogenic Properties

Author

Jixing Ye, Jing Wang, Sherwin H. Ho, Maryam K. Mohammed, Tong-Chuan He, Joseph D. Lamplot, Rex C. Haydon, Richard W. Kang, Aravind Athiviraham, Liangjun Yin, Zhongliang Wang, Zhengjian Yan, Lewis L. Shi, Qiang Wei, Bryan Scott, and Sahitya K. Denduluri

Subjects

0301 basic medicine, Piggybac transposon, SV40 large T antigen, Cell Survival, FLP-FRT recombination, Antigens, Polyomavirus Transforming, Biomedical Engineering, Medicine (miscellaneous), Bioengineering, Biology, Real-Time Polymerase Chain Reaction, Achilles Tendon, Article, 03 medical and health sciences, Mice, 0302 clinical medicine, Animals, Humans, Tendon healing, Cell Shape, Cell Line, Transformed, Cell Proliferation, Mechanism (biology), Proliferative capacity, In vitro, Cell biology, Tenocytes, 030104 developmental biology, HEK293 Cells, Target site, 030220 oncology & carcinogenesis, Bone Morphogenetic Proteins, DNA Nucleotidyltransferases, NIH 3T3 Cells, Biomarkers, Biomedical engineering

Abstract

Investigating the cellular processes underlying tendon healing can allow researchers to improve long-term outcomes after injury. However, conducting meaningful studies to uncover the injury healing mechanism at cellular and molecular levels remains challenging. This is due to the inherent difficulty in isolating, culturing, and expanding sufficient primary tenocytes, due to their limited proliferative capacity and short lifespan. In this study, we sought to establish a novel line of immortalized mouse Achilles tenocytes (iMATs) with primary tenocyte properties, but increased proliferative capacity suitable for extensive in vitro experimentation. We show that isolated primary mouse Achilles tenocytes (pMATs) can be effectively immortalized using a piggyBac transposon expressing SV40 large T antigen flanked by FLP recombination target site (FRT). The resulting iMATs exhibit markedly greater proliferation and survival, which can be reversed with FLP recombinase. Furthermore, iMATs express the same set of tendon-specific markers as that of primary cells, although in lower levels, and respond similarly to exogenous stimulation with bone morphogenetic protein 13 (BMP13) as has been previously reported with pMATs. Taken together, our results suggest that iMATs acquire long-term proliferative capacity while maintaining tenogenic properties. We believe that iMATs are a suitable model for studying not only the native cellular processes involved in injury and healing, but also potential therapeutic agents that may augment the stability of tendon repair.

Published

2016

31. Wnt3a promotes melanin synthesis of mouse hair follicle melanocytes

Author

Tian Yang, Yizhan Xing, Yuhong Li, Xiaohua Lian, Ke Yang, Fang Deng, Haiying Guo, and Jixing Ye

Subjects

Genetically modified mouse, animal structures, Tyrosinase, Biophysics, Mice, Transgenic, Melanocyte, Biology, Biochemistry, Cell Line, Wnt3 Protein, Mice, Downregulation and upregulation, Hair cycle, medicine, Animals, Molecular Biology, Melanins, integumentary system, Stem Cells, Cell Biology, beta-Galactosidase, Microphthalmia-associated transcription factor, Hair follicle, body regions, medicine.anatomical_structure, embryonic structures, Cancer research, Melanocytes, Hair Follicle, WNT3A

Abstract

Although the importance of Wnt3a in melanocyte development has been well recognized, the effect of Wnt3a in normal HF melanocytes has not been clearly elucidated yet. Thus, we sought to examine the presence and location of Wnt3a in HF during hair cycle. By using melanocyte-targeted Dct-LacZ transgenic mice, we found that Wnt3a signaling is activated in mouse HF melanocytes during anagen of hair cycle. To further explore the potential functions of Wnt3a in mouse melanocytes, we infected melan-a cells with AdWnt3a to serve as the production source of Wnt3a protein. We demonstrated that Wnt3a promoted melanogenesis through upregulation of MITF and its downstream genes, tyrosinase and TRP1, in melanocytes. In vivo, AdWnt3a rescued the effects of AdsimMITF on HF melanocytes and promoted melanin synthesis. Our results suggest that Wnt3a plays an important role in mouse HF melanocytes homeostasis.

Published

2012

32. Antibiotic monensin synergizes with EGFR inhibitors and oxaliplatin to suppress the proliferation of human ovarian cancer cells

Author

Hue H. Luu, Yulong Zou, Maryam K. Mohammed, Jiaming Fan, Shun Lu, Junyi Liao, Zhongliang Wang, Jing Wang, Junhui Zhang, Xin Wang, Tong-Chuan He, Zhengjian Yan, Rex C. Haydon, Lianggong Zhao, Hongbo Qi, Hao Liu, Fugui Zhang, Min Qiao, Qiang Wei, Youlin Deng, Shengli Tang, Liangdan Tang, and Jixing Ye

Subjects

Organoplatinum Compounds, Antineoplastic Agents, Apoptosis, Pharmacology, Article, Receptor, IGF Type 1, chemistry.chemical_compound, Cell Movement, Cell Line, Tumor, medicine, Humans, Monensin, Protein Kinase Inhibitors, EGFR inhibitors, Cell Proliferation, Ovarian Neoplasms, Wound Healing, Multidisciplinary, Cell growth, business.industry, Cell Cycle, Cancer, Drug Synergism, Cell cycle, medicine.disease, Xenograft Model Antitumor Assays, 3. Good health, Oxaliplatin, Anti-Bacterial Agents, ErbB Receptors, HEK293 Cells, chemistry, Female, Ovarian cancer, business, medicine.drug, Signal Transduction

Abstract

Ovarian cancer is the most lethal gynecologic malignancy with an overall cure rate of merely 30%. Most patients experience recurrence within 12–24 months of cure and die of progressively chemotherapy-resistant disease. Thus, more effective anti-ovarian cancer therapies are needed. Here, we investigate the possibility of repurposing antibiotic monensin as an anti-ovarian cancer agent. We demonstrate that monensin effectively inhibits cell proliferation, migration and cell cycle progression and induces apoptosis of human ovarian cancer cells. Monensin suppresses multiple cancer-related pathways including Elk1/SRF, AP1, NFκB and STAT and reduces EGFR expression in ovarian cancer cells. Monensin acts synergistically with EGFR inhibitors and oxaliplatin to inhibit cell proliferation and induce apoptosis of ovarian cancer cells. Xenograft studies confirm that monensin effectively inhibits tumor growth by suppressing cell proliferation through targeting EGFR signaling. Our results suggest monensin may be repurposed as an anti-ovarian cancer agent although further preclinical and clinical studies are needed.

Published

2015

33. A Novel Organ Culture Model of Mouse Intervertebral Disc Tissues

Author

Sahitya K. Denduluri, Tong-Chuan He, Shun Lu, Xin Wang, Shengli Tang, Liangjun Yin, Qiang Wei, Zhongliang Wang, Lewis L. Shi, Zhengjian Yan, Zhonglin Zhang, Michael J. Lee, Jing Wang, Ruifang Li, Jixing Ye, Lianggong Zhao, and Zhong Liang Deng

Subjects

0301 basic medicine, musculoskeletal diseases, Male, Pathology, medicine.medical_specialty, Histology, Intervertebral Disc Degeneration, Organ culture, medicine.disease_cause, Article, Adenoviridae, Cell Line, 03 medical and health sciences, Mice, Lumbar, Organ Culture Techniques, Tissue engineering, Transduction, Genetic, Proliferating Cell Nuclear Antigen, medicine, Animals, Humans, Intervertebral Disc, Cell Proliferation, business.industry, Lumbosacral Region, Intervertebral disc, Anatomy, musculoskeletal system, In vitro, 030104 developmental biology, medicine.anatomical_structure, HEK293 Cells, Cell culture, business, Fetal bovine serum

Abstract

The intervertebral disc (IVD) is a fibrocartilaginous joint between two vertebral bodies. An IVD unit consists of a gelatinous central nucleus pulposus, encased by the annulus fibrosus, which is sandwiched between cartilaginous endplates (EP). The IVD homeostasis can be disrupted by injuries, ageing, and/or genetic predispositions, leading to degenerative disc disorders and subsequent low back pain. The complex structure and distinct characteristics of the IVDs warrant the establishment of robust in vitro IVD organ culture for studying the etiology and treatment of disc degeneration. Here, we isolate mouse lumbar IVDs and culture the minimal IVD units in submersion or suspension medium supplemented with 2% bovine serum or 10% fetal bovine serum (FBS). We find the minimal IVD units remain healthy up to 14 days when cultured in submersion culture supplemented with 10% FBS. New bone formation in the EPs of the cultured IVDs can be assessed with calcein labeling. Furthermore, the cultured IVDs can be effectively transduced by recombinant adenovirus, and transgene expression lasts for two weeks. Thus, our findings demonstrate that the optimized intervertebral disc organ culture system can be used to study intervertebral disc biology and screen for biological factors that may prevent, alleviate, and/or treat disc degeneration.

Published

2015

34. Reversibly Immortalized Mouse Articular Chondrocytes Acquire Long-Term Proliferative Capability While Retaining Chondrogenic Phenotype

Author

Guoxin Nan, Eric R. Wagner, Zhonglin Zhang, Zhan Liao, Fang Deng, Joseph D. Lamplot, Richard Rames, Wenwen Zhang, Sherwin H. Ho, Qian Zhang, Junhui Zhang, Lewis L. Shi, Zhongliang Wang, Jixing Ye, Liangjun Yin, Jovito Angeles, Min Qiao, Tong-Chuan He, Zhengjian Yan, Rex C. Haydon, Wei Liu, Hue H. Luu, Ruidong Li, Wei Shui, Youlin Deng, Gaurav Luther, Hongmei Zhang, and Bo Liu

Subjects

Cartilage, Articular, Time Factors, Cell Survival, Biomedical Engineering, lcsh:Medicine, Cell Separation, Biology, Bone morphogenetic protein 2, Chondrocyte, Mice, Chondrocytes, Subcutaneous Tissue, Tissue engineering, medicine, Animals, Humans, Antigens, Viral, Tumor, Aggrecan, Cell Aggregation, Cell Line, Transformed, Cell Proliferation, Transplantation, Integrases, Regeneration (biology), Cartilage, lcsh:R, Mesenchymal Stem Cells, Cell Biology, Chondrogenesis, Cell aggregation, Cell biology, Extracellular Matrix, medicine.anatomical_structure, HEK293 Cells, Phenotype, Immunology, Biomarkers

Abstract

Cartilage tissue engineering holds great promise for treating cartilaginous pathologies including degenerative disorders and traumatic injuries. Effective cartilage regeneration requires an optimal combination of biomaterial scaffolds, chondrogenic seed cells, and biofactors. Obtaining sufficient chondrocytes remains a major challenge due to the limited proliferative capability of primary chondrocytes. Here we investigate if reversibly immortalized mouse articular chondrocytes (iMACs) acquire long-term proliferative capability while retaining the chondrogenic phenotype. Primary mouse articular chondrocytes (MACs) can be efficiently immortalized with a retroviral vector-expressing SV40 large T antigen flanked with Cre/loxP sites. iMACs exhibit long-term proliferation in culture, although the immortalization phenotype can be reversed by Cre recombinase. iMACs express the chondrocyte markers Col2a1 and aggrecan and produce chondroid matrix in micromass culture. iMACs form subcutaneous cartilaginous masses in athymic mice. Histologic analysis and chondroid matrix staining demonstrate that iMACs can survive, proliferate, and produce chondroid matrix. The chondrogenic growth factor BMP2 promotes iMACs to produce more mature chondroid matrix resembling mature articular cartilage. Taken together, our results demonstrate that iMACs acquire long-term proliferative capability without losing the intrinsic chondrogenic features of MACs. Thus, iMACs provide a valuable cellular platform to optimize biomaterial scaffolds for cartilage regeneration, to identify biofactors that promote the proliferation and differentiation of chondrogenic progenitors, and to elucidate the molecular mechanisms underlying chondrogenesis.

Published

2015

35. TqPCR: A Touchdown qPCR Assay with Significantly Improved Detection Sensitivity and Amplification Efficiency of SYBR Green qPCR

Author

Tong-Chuan He, Min Qiao, Hao Liu, Ruifang Li, Qian Zhang, Shun Lu, Xin Wang, Hue H. Luu, Sahitya K. Denduluri, Li Jiang, Qiang Wei, Youlin Deng, Zhengjian Yan, Fang Deng, Zhonglin Zhang, Jing Wang, Jixing Ye, Zhongliang Wang, Shengli Tang, Yinglin Xia, Rex C. Haydon, and Lianggong Zhao

Subjects

Ribosomal Proteins, Hypoxanthine Phosphoribosyltransferase, DNA, Complementary, lcsh:Medicine, Biology, Real-Time Polymerase Chain Reaction, law.invention, Cell Line, Mice, law, Complementary DNA, Reference genes, Wnt3A Protein, Gene expression, Animals, Humans, lcsh:Science, Gene, Polymerase chain reaction, Fluorescent Dyes, Multidisciplinary, lcsh:R, Glyceraldehyde-3-Phosphate Dehydrogenases, Mesenchymal Stem Cells, Molecular diagnostics, Molecular biology, 3. Good health, Up-Regulation, HEK293 Cells, lcsh:Q, RNA extraction, Primer (molecular biology), Research Article

Abstract

The advent of fluorescence-based quantitative real-time PCR (qPCR) has revolutionized the quantification of gene expression analysis in many fields, including life sciences, agriculture, forensic science, molecular diagnostics, and medicine. While SYBR Green-based qPCR is the most commonly-used platform due to its inexpensive nature and robust chemistry, quantifying the expression of genes with low abundance or RNA samples extracted from highly restricted or limited sources can be challenging because the detection sensitivity of SYBR Green-based qPCR is limited. Here, we develop a novel and effective touchdown qPCR (TqPCR) protocol by incorporating a 4-cycle touchdown stage prior to the quantification amplification stage. Using the same cDNA templates, we find that TqPCR can reduce the average Cq values for Gapdh, Rps13, and Hprt1 reference genes by 4.45, 5.47, and 4.94 cycles, respectively, when compared with conventional qPCR; the overall average Cq value reduction for the three reference genes together is 4.95. We further find that TqPCR can improve PCR amplification efficiency and thus increase detection sensitivity. When the quantification of Wnt3A-induced target gene expression in mesenchymal stem cells is analyzed, we find that, while both conventional qPCR and TqPCR can detect the up-regulation of the relatively abundant target Axin2, only TqPCR can detect the up-regulation of the lowly-expressed targets Oct4 and Gbx2. Finally, we demonstrate that the MRQ2 and MRQ3 primer pairs derived from mouse reference gene Tbp can be used to validate the RNA/cDNA integrity of qPCR samples. Taken together, our results strongly suggest that TqPCR may increase detection sensitivity and PCR amplification efficiency. Overall, TqPCR should be advantageous over conventional qPCR in expression quantification, especially when the transcripts of interest are lowly expressed, and/or the availability of total RNA is highly restricted or limited.

Published

2015

36. Wnt

Author

Zhongliang, Wang, Jixing, Ye, Youlin, Deng, Zhengjian, Yan, Sahitya, Denduluri, and Tong-Chuan, He

Subjects

body regions, Wnt/β-catenin, animal structures, Proteasome degradation, Hippo, fungi, Destruction complex, YAP/TAZ, Signal transduction, Article, β-TrCP

Abstract

The Hippo signaling pathway was first discovered in Drosophila as a conserved regulator of organ size. Genetic inactivation in mice demonstrates that the Hippo pathway functions as a fundamental inhibitor of organ growth during development, and as a critical tumor suppressor in epithelial tissues.

Published

2015

37. Repair of critical sized cranial defects with BMP9-transduced calvarial cells delivered in a thermoresponsive scaffold

Author

Junyi Liao, Viktor Tollemar, Minpeng Lu, Yunxiao Zhu, Russell R. Reid, Tong-Chuan He, Jixing Ye, Guillermo A. Ameer, and Zari P. Dumanian

Subjects

0301 basic medicine, Pathology, Scaffold, Physiology, Organogenesis, lcsh:Medicine, Ossification, Polyethylene Glycols, Diagnostic Radiology, Mice, Transduction, Genetic, Animal Cells, Animal Products, Growth Differentiation Factor 2, Medicine and Health Sciences, lcsh:Science, Fracture Healing, Multidisciplinary, Tissue Scaffolds, Chemistry, Stem Cells, Radiology and Imaging, Agriculture, Bone Imaging, Growth Differentiation Factors, Bone Remodeling, Anatomy, Cellular Types, Stem cell, Research Article, Cell Physiology, medicine.medical_specialty, Histology, Mature Bone, Imaging Techniques, Context (language use), Research and Analysis Methods, Osseointegration, Cell Line, 03 medical and health sciences, Diagnostic Medicine, In vivo, Tissue Repair, medicine, Animals, Humans, Progenitor cell, Bone Development, lcsh:R, Skull, Mesenchymal stem cell, Biology and Life Sciences, Mesenchymal Stem Cells, Cell Biology, Surgery, 030104 developmental biology, Gelatin, lcsh:Q, Cell Immortalization, Physiological Processes, Organism Development, Developmental Biology

Abstract

Large skeletal defects caused by trauma, congenital malformations, and post-oncologic resections of the calvarium present major challenges to the reconstructive surgeon. We previously identified BMP-9 as the most osteogenic BMP in vitro and in vivo. Here we sought to investigate the bone regenerative capacity of murine-derived calvarial mesenchymal progenitor cells (iCALs) transduced by BMP-9 in the context of healing critical-sized calvarial defects. To accomplish this, the transduced cells were delivered to the defect site within a thermoresponsive biodegradable scaffold consisting of poly(polyethylene glycol citrate-co-N-isopropylacrylamide mixed with gelatin (PPCN-g). A total of three treatment arms were evaluated: PPCN-g alone, PPCN-g seeded with iCALs expressing GFP, and PPCN-g seeded with iCALs expressing BMP-9. Defects treated only with PPCN-g scaffold did not statistically change in size when evaluated at eight weeks postoperatively (p = 0.72). Conversely, both animal groups treated with iCALs showed significant reductions in defect size after 12 weeks of follow-up (BMP9-treated: p = 0.0025; GFP-treated: p = 0.0042). However, H&E and trichrome staining revealed more complete osseointegration and mature bone formation only in the BMP9-treated group. These results suggest that BMP9-transduced iCALs seeded in a PPCN-g thermoresponsive scaffold is capable of inducing bone formation in vivo and is an effective means of creating tissue engineered bone for critical sized defects.

Published

2017

38. The piggyBac Transposon-Mediated Expression of SV40 T Antigen Efficiently Immortalizes Mouse Embryonic Fibroblasts (MEFs)

Author

Min Qiao, Fang Deng, Xiang Chen, Zhonglin Zhang, Houjie Liang, Ningning Wu, Zhengjian Yan, Jing Cui, Jixing Ye, Rex C. Haydon, Lewis L. Shi, Hue H. Luu, Liangjun Yin, Qian Zhang, Ning Wang, Junhui Zhang, Tong-Chuan He, Wenwen Zhang, Ruidong Li, Wei Liu, Youlin Deng, Sheng Wen, Zhongliang Wang, Zhan Liao, Xian Chen, and Hongmei Zhang

Subjects

Cellular differentiation, Antigens, Polyomavirus Transforming, lcsh:Medicine, Gene Expression, Simian virus 40, Cell Fate Determination, Mice, 0302 clinical medicine, Cell Signaling, Animal Cells, Molecular Cell Biology, lcsh:Science, Musculoskeletal System, Cell Line, Transformed, 0303 health sciences, Multidisciplinary, Stem Cells, Cell Differentiation, Cell biology, Adult Stem Cells, Connective Tissue, 030220 oncology & carcinogenesis, Stem cell, Anatomy, Cellular Types, Research Article, Signal Transduction, Cell Potency, Biology, 03 medical and health sciences, Animals, Humans, Progenitor cell, Bone, 030304 developmental biology, Cell growth, Multipotent Stem Cells, lcsh:R, HEK 293 cells, Mesenchymal stem cell, fungi, Biology and Life Sciences, Mesenchymal Stem Cells, Cell Biology, Molecular Development, Fibroblasts, Embryo, Mammalian, Embryonic stem cell, Molecular biology, Biological Tissue, HEK293 Cells, Cell culture, DNA Transposable Elements, lcsh:Q, Developmental Biology

Abstract

Mouse embryonic fibroblasts (MEFs) are mesenchymal stem cell (MSC)-like multipotent progenitor cells and can undergo self-renewal and differentiate into to multiple lineages, including bone, cartilage and adipose. Primary MEFs have limited life span in culture, which thus hampers MEFs' basic research and translational applications. To overcome this challenge, we investigate if piggyBac transposon-mediated expression of SV40 T antigen can effectively immortalize mouse MEFs and that the immortalized MEFs can maintain long-term cell proliferation without compromising their multipotency. Using the piggyBac vector MPH86 which expresses SV40 T antigen flanked with flippase (FLP) recognition target (FRT) sites, we demonstrate that mouse embryonic fibroblasts (MEFs) can be efficiently immortalized. The immortalized MEFs (piMEFs) exhibit an enhanced proliferative activity and maintain long-term cell proliferation, which can be reversed by FLP recombinase. The piMEFs express most MEF markers and retain multipotency as they can differentiate into osteogenic, chondrogenic and adipogenic lineages upon BMP9 stimulation in vitro. Stem cell implantation studies indicate that piMEFs can form bone, cartilage and adipose tissues upon BMP9 stimulation, whereas FLP-mediated removal of SV40 T antigen diminishes the ability of piMEFs to differentiate into these lineages, possibly due to the reduced expansion of progenitor populations. Our results demonstrate that piggyBac transposon-mediated expression of SV40 T can effectively immortalize MEFs and that the reversibly immortalized piMEFs not only maintain long-term cell proliferation but also retain their multipotency. Thus, the high transposition efficiency and the potential footprint-free natures may render piggyBac transposition an effective and safe strategy to immortalize progenitor cells isolated from limited tissue supplies, which is essential for basic and translational studies.

Published

2014

39. Adenovirus-mediated efficient gene transfer into cultured three-dimensional organoids

Author

Hongyu Zhang, Zhan Liao, Zhonglin Zhang, Ningning Wu, Sheng Wen, Qian Zhang, Xian Chen, Hongmei Zhang, Tong-Chuan He, Liangjun Yin, Bing-Qiang Zhang, Fang Deng, Junhui Zhang, Youlin Deng, Hue H. Luu, Min Qiao, Jixing Ye, Ning Wang, Wei Liu, Houjie Liang, Rex C. Haydon, and Zhengjian Yan

Subjects

medicine.medical_treatment, lcsh:Medicine, Mice, 0302 clinical medicine, Animal Cells, Molecular Cell Biology, Gastrointestinal Cancers, Medicine and Health Sciences, Induced pluripotent stem cell, lcsh:Science, 0303 health sciences, Multidisciplinary, Stem Cells, Gene Transfer Techniques, Stem-cell therapy, Gene Therapy, 3. Good health, Cell biology, Intestines, Adult Stem Cells, 030220 oncology & carcinogenesis, Small Intestine, Stem cell, Anatomy, Cellular Types, Viral Vectors, Research Article, Genetic Vectors, Gastroenterology and Hepatology, Gene delivery, Biology, Microbiology, Viral vector, Adenoviridae, 03 medical and health sciences, Virology, Organoid, medicine, Genetics, Animals, Humans, Progenitor cell, Molecular Biology Techniques, Molecular Biology, 030304 developmental biology, lcsh:R, Correction, Biology and Life Sciences, Human Genetics, Cell Biology, Embryonic stem cell, Molecular biology, Gastrointestinal Tract, HEK293 Cells, Culture Media, Conditioned, lcsh:Q, Digestive System, Viral Transmission and Infection

Abstract

Three-dimensional organoids have been recently established from various tissue-specific progenitors (such as intestinal stem cells), induced pluripotent stem cells, or embryonic stem cells. These cultured self-sustaining stem cell–based organoids may become valuable systems to study the roles of tissue-specific stem cells in tissue genesis and disease development. It is thus conceivable that effective genetic manipulations in such organoids may allow us to reconstruct disease processes and/or develop novel therapeutics. Recombinant adenoviruses are one of the most commonly used viral vectors for in vitro and in vivo gene deliveries. In this study, we investigate if adenoviruses can be used to effectively deliver transgenes into the cultured “mini-gut” organoids derived from intestinal stem cells. Using adenoviral vectors that express fluorescent proteins, we demonstrate that adenoviruses can effectively deliver transgenes into the cultured 3-D “mini-gut” organoids. The transgene expression can last at least 10 days in the cultured organoids. As a proof-of-principle experiment, we demonstrate that adenovirus-mediated noggin expression effectively support the survival and self-renewal of mini-gut organoids, while adenovirus-mediated expression of BMP4 inhibits the self-sustainability and proliferation of the organoids. Thus, our results strongly suggest that adenovirus vectors can be explored as effective gene delivery vehicles to introduce genetic manipulations in 3-D organoids.

Published

2014

40. Bone Morphogenetic Protein-9 Effectively Induces Osteo/Odontoblastic Differentiation of the Reversibly Immortalized Stem Cells of Dental Apical Papilla

Author

Hue H. Luu, Wei Liu, Tong-Chuan He, Jinhua Wang, Jixing Ye, Feng Deng, Wenwen Zhang, Zhengjian Yan, Enyi Huang, Liangjun Yin, Rex C. Haydon, Sheng Wen, Junhui Zhang, Ning Wang, Xian Chen, Hongmei Zhang, Youlin Deng, Zhonglin Zhang, Ningning Wu, Zhan Liao, Qian Zhang, and Fang Deng

Subjects

Cellular differentiation, GDF2, Cre recombinase, Biology, Mice, stomatognathic system, Original Research Reports, Growth Differentiation Factor 2, Animals, Regeneration, Dental papilla, Dental Papilla, Cell Proliferation, Odontoblasts, Stem Cells, Mesenchymal stem cell, Gene Expression Regulation, Developmental, Cell Differentiation, Cell Biology, Hematology, Anatomy, Cell biology, RUNX2, Odontoblast, Odontogenesis, Stem cell, Developmental Biology

Abstract

Dental pulp/dentin regeneration using dental stem cells combined with odontogenic factors may offer great promise to treat and/or prevent premature tooth loss. We previously demonstrated that bone morphogenetic protein 9 (BMP9) is one of the most potent factors in inducing bone formation. Here, we investigate whether BMP9 can effectively induce odontogenic differentiation of the stem cells from mouse apical papilla (SCAPs). Using a reversible immortalization system expressing SV40 T flanked with Cre/loxP sites, we demonstrate that the SCAPs can be immortalized, resulting in immortalized SCAPs (iSCAPs) that express mesenchymal stem cell markers. BMP9 upregulates Runx2, Sox9, and PPARγ2 and odontoblastic markers, and induces alkaline phosphatase activity and matrix mineralization in the iSCAPs. Cre-mediated removal of SV40 T antigen decreases iSCAP proliferation. The in vivo stem cell implantation studies indicate that iSCAPs can differentiate into bone, cartilage, and, to lesser extent, adipocytes upon BMP9 stimulation. Our results demonstrate that the conditionally iSCAPs not only maintain long-term cell proliferation but also retain the ability to differentiate into multiple lineages, including osteo/odontoblastic differentiation. Thus, the reversibly iSCAPs may serve as an important tool to study SCAP biology and SCAP translational use in tooth engineering. Further, BMP9 may be explored as a novel and efficacious factor for odontogenic regeneration.

Published

2014

41. Adenovirus-mediated gene transfer in mesenchymal stem cells can be significantly enhanced by the cationic polymer polybrene

Author

Youlin Deng, Liangjun Yin, Sheng Wen, Jixing Ye, Xian Chen, Hongmei Zhang, Tong-Chuan He, Qian Zhang, Chen Zhao, Wei Liu, Di Wu, Wenwen Zhang, Guolin Zhou, Weike Si, Zhan Liao, Ning Wang, Fang Deng, Hue H. Luu, Zhonglin Zhang, Ningning Wu, Junhui Zhang, Zhengjian Yan, and Rex C. Haydon

Subjects

Epidemiology, Cellular differentiation, Cancer Treatment, Gene Expression, lcsh:Medicine, Disease Vectors, medicine.disease_cause, Mice, chemistry.chemical_compound, Animal Cells, Genes, Reporter, Transduction, Genetic, Molecular Cell Biology, Medicine and Health Sciences, Transgenes, lcsh:Science, Hexadimethrine bromide, Multidisciplinary, Stem Cells, Gene Transfer Techniques, Genomics, Gene Therapy, Flow Cytometry, Oncology, Cellular Types, Viral Vectors, Stem cell, Research Article, Genetic Vectors, Biology, Microbiology, Vector Biology, Adenoviridae, Cell Line, Genomic Medicine, Virology, Genetics, medicine, Animals, Humans, Adenovirus infection, Progenitor cell, Molecular Biology Techniques, Molecular Biology, Hexadimethrine Bromide, Dose-Response Relationship, Drug, Mesenchymal stem cell, lcsh:R, Biology and Life Sciences, Mesenchymal Stem Cells, Human Genetics, Cell Biology, medicine.disease, Molecular biology, chemistry, Cell culture, lcsh:Q, Viral Transmission and Infection, Developmental Biology

Abstract

Mesenchymal stem cells (MSCs) are multipotent progenitors, which can undergo self-renewal and give rise to multi-lineages. A great deal of attentions have been paid to their potential use in regenerative medicine as potential therapeutic genes can be introduced into MSCs. Genetic manipulations in MSCs requires effective gene deliveries. Recombinant adenoviruses are widely used gene transfer vectors. We have found that although MSCs can be infected in vitro by adenoviruses, high virus titers are needed to achieve high efficiency. Here, we investigate if the commonly-used cationic polymer Polybrene can potentiate adenovirus-mediated transgene delivery into MSCs, such as C2C12 cells and iMEFs. Using the AdRFP adenovirus, we find that AdRFP transduction efficiency is significantly increased by Polybrene in a dose-dependent fashion peaking at 8 μg/ml in C2C12 and iMEFs cells. Quantitative luciferase assay reveals that Polybrene significantly enhances AdFLuc-mediated luciferase activity in C2C12 and iMEFs at as low as 4 μg/ml and 2 μg/ml, respectively. FACS analysis indicates that Polybrene (at 4 μg/ml) increases the percentage of RFP-positive cells by approximately 430 folds in AdRFP-transduced iMEFs, suggesting Polybrene may increase adenovirus infection efficiency. Furthermore, Polybrene can enhance AdBMP9-induced osteogenic differentiation of MSCs as early osteogenic marker alkaline phosphatase activity can be increased more than 73 folds by Polybrene (4 μg/ml) in AdBMP9-transduced iMEFs. No cytotoxicity was observed in C2C12 and iMEFs at Polybrene up to 40 μg/ml, which is about 10-fold higher than the effective concentration required to enhance adenovirus transduction in MSCs. Taken together, our results demonstrate that Polybrene should be routinely used as a safe, effective and inexpensive augmenting agent for adenovirus-mediated gene transfer in MSCs, as well as other types of mammalian cells.

Published

2014

42. A simplified and versatile system for the simultaneous expression of multiple siRNAs in mammalian cells using Gibson DNA Assembly

Author

Ruifang Li, Qiang Wei, Youlin Deng, Tong-Chuan He, Zhongliang Wang, Xiang Chen, Zhan Liao, Melissa Li, Zhengjian Yan, Jixing Ye, Min Qiao, Sahitya K. Denduluri, Nisha Geng, Rex C. Haydon, Lianggong Zhao, Fang Deng, Zhonglin Zhang, Jing Wang, Penghui Zhang, Russell R. Reid, Tian Yang, Qian Zhang, Hue H. Luu, and Guolin Zhou

Subjects

Small interfering RNA, lcsh:Medicine, Mice, Cell Signaling, Osteogenesis, Animal Cells, RNA interference, Molecular Cell Biology, Growth Differentiation Factor 2, Medicine and Health Sciences, RNA, Small Interfering, lcsh:Science, beta Catenin, WNT Signaling Cascade, Multidisciplinary, Stem Cells, Gene targeting, Cell Differentiation, Transfection, Signaling Cascades, Cell biology, Growth Differentiation Factors, Oncology, RNA Interference, Cellular Types, Research Article, Signal Transduction, Adhesion Molecules, Genetic Vectors, Trans-acting siRNA, Biology, Cell Line, Tumor, Wnt3A Protein, Animals, Humans, Gene silencing, Molecular Biology, Base Sequence, lcsh:R, Biology and Life Sciences, RNA, Mesenchymal Stem Cells, DNA, Cell Biology, Molecular Development, Molecular biology, HEK293 Cells, lcsh:Q, In vitro recombination, Developmental Biology

Abstract

RNA interference (RNAi) denotes sequence-specific mRNA degradation induced by short interfering double-stranded RNA (siRNA) and has become a revolutionary tool for functional annotation of mammalian genes, as well as for development of novel therapeutics. The practical applications of RNAi are usually achieved by expressing short hairpin RNAs (shRNAs) or siRNAs in cells. However, a major technical challenge is to simultaneously express multiple siRNAs to silence one or more genes. We previously developed pSOS system, in which siRNA duplexes are made from oligo templates driven by opposing U6 and H1 promoters. While effective, it is not equipped to express multiple siRNAs in a single vector. Gibson DNA Assembly (GDA) is an in vitro recombination system that has the capacity to assemble multiple overlapping DNA molecules in a single isothermal step. Here, we developed a GDA-based pSOK assembly system for constructing single vectors that express multiple siRNA sites. The assembly fragments were generated by PCR amplifications from the U6-H1 template vector pB2B. GDA assembly specificity was conferred by the overlapping unique siRNA sequences of insert fragments. To prove the technical feasibility, we constructed pSOK vectors that contain four siRNA sites and three siRNA sites targeting human and mouse β-catenin, respectively. The assembly reactions were efficient, and candidate clones were readily identified by PCR screening. Multiple β-catenin siRNAs effectively silenced endogenous β-catenin expression, inhibited Wnt3A-induced β-catenin/Tcf4 reporter activity and expression of Wnt/β-catenin downstream genes. Silencing β-catenin in mesenchymal stem cells inhibited Wnt3A-induced early osteogenic differentiation and significantly diminished synergistic osteogenic activity between BMP9 and Wnt3A in vitro and in vivo. These findings demonstrate that the GDA-based pSOK system has been proven simplistic, effective and versatile for simultaneous expression of multiple siRNAs. Thus, the reported pSOK system should be a valuable tool for gene function studies and development of novel therapeutics.

Published

2014

43. Wnt versus Hippo: A balanced act or dynamic duo?

Author

Tong-Chuan He, Zhongliang Wang, Jixing Ye, Sahitya K. Denduluri, Youlin Deng, and Zhengjian Yan

Subjects

animal structures, Regulator, Biology, Signal transduction, Bioinformatics, Biochemistry, β-TrCP, law.invention, 03 medical and health sciences, 0302 clinical medicine, Proteasome degradation, Hippo, law, Destruction complex, YAP/TAZ, Molecular Biology, Genetics (clinical), 030304 developmental biology, 0303 health sciences, Hippo signaling pathway, Wnt/β-catenin, fungi, Wnt signaling pathway, Cell Biology, Organ Size, Cell biology, body regions, 030220 oncology & carcinogenesis, Suppressor

Abstract

The Hippo signaling pathway was first discovered in Drosophila as a conserved regulator of organ size. Genetic inactivation in mice demonstrates that the Hippo pathway functions as a fundamental inhibitor of organ growth during development, and as a critical tumor suppressor in epithelial tissues.

Published

2014

44. Whole-Proteome Analysis of Human Craniosynostotic Tissue Suggests a Link between Inflammatory Signaling and Osteoclast Activation in Human Cranial Suture Patency.

Author

Lyon, Sarah M., Mayampurath, Anoop, Dongzhe Song, Jixing Ye, Januszyk, Michael, Rogers, M. Rose, Ralston, Ashley, Frim, David M., Tong-Chuan He, and Reid, Russell R.

Published

2018

45. A thermoresponsive polydiolcitrate-gelatin scaffold and delivery system mediates effective bone formation from BMP9-transduced mesenchymal stem cells

Author

Jianxiang Liu, Dongzhe Song, Li Yang, Feng Liu, Jiaming Fan, Guillermo A. Ameer, Yulong Zou, Minpeng Lu, Jian Yang, Fugui Zhang, Yunxiao Zhu, Maryam K. Mohammed, Evan M. Farina, Chao Ma, Junyi Liao, Dan Guo, Rex C. Haydon, Jixing Ye, Michael J Lee, Xue Hu, Xin Wang, Jing Wang, Russell R. Reid, Shengli Tang, Qiang Wei, Tong-Chuan He, Li Li, Jiayi Huang, and Hao Liu

Subjects

0301 basic medicine, Materials science, Cell Survival, Cellular differentiation, Acrylic Resins, Melanoma, Experimental, Biomedical Engineering, Mice, Nude, GDF2, Biocompatible Materials, Bioengineering, Polyethylene Glycols, Biomaterials, Mice, 03 medical and health sciences, Tissue engineering, Osteogenesis, Transduction, Genetic, Materials Testing, Cell Adhesion, Growth Differentiation Factor 2, medicine, Animals, Humans, Citrates, Progenitor cell, Cell adhesion, Tissue Engineering, Tissue Scaffolds, Mesenchymal stem cell, Temperature, Cell Differentiation, Mesenchymal Stem Cells, Osteoblast, Embryonic stem cell, Cell biology, Growth Differentiation Factors, HEK293 Cells, 030104 developmental biology, medicine.anatomical_structure, Gelatin, Female, Biomedical engineering

Abstract

Successful bone tissue engineering requires at the minimum sufficient osteoblast progenitors, efficient osteoinductive factors, and biocompatible scaffolding materials. We previously demonstrated that bone morphogenetic protein 9 (BMP9) is one of the most potent factors in inducing osteogenic differentiation of mesenchymal stem cells (MSCs). Here, we investigated the potential use of a biodegradable citrate-based thermosensitive macromolecule, poly(polyethyleneglycol citrate-co-N-isopropylacrylamide) (PPCN) mixed with gelatin (PPCNG) as a scaffold for the delivery of BMP9-stimulated MSCs to promote localized bone formation. The addition of gelatin to PPCN effectively enhanced the cell adhesion and survival properties of MSCs entrapped within the gel in 3D culture. Using the BMP9-transduced MSC line immortalized mouse embryonic fibroblasts (iMEFs), we found that PPCNG facilitated BMP9-induced osteogenic differentiation of iMEFs in vivo and promoted the formation of well-ossified and vascularized trabecular bone-like structures in a mouse model of ectopic bone formation. Histologic evaluation revealed that vascularization of the bony masses retrieved from the iMEFs + PPCNG group was significantly more pronounced than that of the direct cell injection group. Accordingly, vascular endothelial growth factor (VEGF) expression was shown to be significantly higher in the bony masses recovered from the iMEFs + PPCNG group. Taken together, our results suggest that PPCNG may serve as a novel biodegradable and injectable scaffold and carrier for gene and cell-based bone tissue engineering.

Published

2016

46. Characterization of Constitutive Promoters for piggyBac Transposon-Mediated Stable Transgene Expression in Mesenchymal Stem Cells (MSCs)

Author

Wei Liu, Sheng Wen, Xian Chen, Hongmei Zhang, Guang-Hui Wei, Ning Wang, Jixing Ye, Youlin Deng, Ke Yang, Zhan Liao, Zhengjian Yan, Junhui Zhang, Yasha Li, Rex C. Haydon, Wenwen Zhang, Zhonglin Zhang, Ningning Wu, Tong-Chuan He, Qian Zhang, Fang Deng, Guolin Zhou, Lewis L. Shi, and Hue H. Luu

Subjects

Transgene, Genetic Vectors, Gene Expression, lcsh:Medicine, Biology, Cell Line, Histones, Animal Cells, Genes, Reporter, Molecular Cell Biology, Gene expression, Genetics, Humans, Gene Silencing, Transgenes, Epigenetics, Homologous Recombination, Promoter Regions, Genetic, lcsh:Science, Multidisciplinary, Stem Cells, lcsh:R, Mesenchymal stem cell, Gene Transfer Techniques, Biology and Life Sciences, Mesenchymal Stem Cells, Acetylation, Promoter, Cell Biology, DNA Methylation, Molecular biology, HEK293 Cells, PiggyBac Transposon System, DNA methylation, DNA Transposable Elements, lcsh:Q, Cellular Types, Stem cell, Research Article, Developmental Biology

Abstract

Multipotent mesenchymal stem cells (MSCs) can undergo self-renewal and give rise to multi-lineages under given differentiation cues. It is frequently desirable to achieve a stable and high level of transgene expression in MSCs in order to elucidate possible molecular mechanisms through which MSC self-renewal and lineage commitment are regulated. Retroviral or lentiviral vector-mediated gene expression in MSCs usually decreases over time. Here, we choose to use the piggyBac transposon system and conduct a systematic comparison of six commonly-used constitutive promoters for their abilities to drive RFP or firefly luciferase expression in somatic HEK-293 cells and MSC iMEF cells. The analyzed promoters include three viral promoters (CMV, CMV-IVS, and SV40), one housekeeping gene promoter (UbC), and two composite promoters of viral and housekeeping gene promoters (hEFH and CAG-hEFH). CMV-derived promoters are shown to drive the highest transgene expression in HEK-293 cells, which is however significantly reduced in MSCs. Conversely, the composite promoter hEFH exhibits the highest transgene expression in MSCs whereas its promoter activity is modest in HEK-293 cells. The reduced transgene expression driven by CMV promoters in MSCs may be at least in part caused by DNA methylation, or to a lesser extent histone deacetlyation. However, the hEFH promoter is not significantly affected by these epigenetic modifications. Taken together, our results demonstrate that the hEFH composite promoter may be an ideal promoter to drive long-term and high level transgene expression using the piggyBac transposon vector in progenitor cells such as MSCs.

Published

2014

47. Bone morphogenetic protein 2 inhibits the proliferation and growth of human colorectal cancer cells.

Author

YUNYUAN ZHANG, XIAN CHEN, MIN QIAO, BING-QIANG ZHANG, NING WANG, ZHONGLIN ZHANG, ZHAN LIAO, LIYI ZENG, YOULIN DENG, FANG DENG, JUNHUI ZHANG, LIANGJUN YIN, WEI LIU, QIAN ZHANG, ZHENGJIAN YAN, JIXING YE, ZHONGLIANG WANG, LAN ZHOU, LUU, HUE H., and HAYDON, REX C.

Published

2014

48. A thermoresponsive polydiolcitrate-gelatin scaffold and delivery system mediates effective bone formation from BMP9-transduced mesenchymal stem cells.

Author

Jixing Ye, Jing Wang, Yunxiao Zhu, Qiang Wei, Xin Wang, Jian Yang, Shengli Tang, Hao Liu, Jiaming Fan, Fugui Zhang, Evan M Farina, Maryam K Mohammed, Yulong Zou, Dongzhe Song, Junyi Liao, Jiayi Huang, Dan Guo, Minpeng Lu, Feng Liu, and Jianxiang Liu

Published

2016