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61 results on '"Carolyn A. Meyers"'

51. miRNA-214 Inhibits Cellular Proliferation and Migration in Glioma Cells Targeting Caspase 1 Involved in Pyroptosis

Author

Jianhang Chen, Jia Shen, Minwei Zhu, Yufang Zhao, Zhiyan Li, Chuncheng Xie, Guizhen Ma, Panpan Xu, Hong Shen, Zhiguo Lin, Hongge Ma, Wang Zhang, Lifen Yao, Shupei Qiao, Zhenfeng Jiang, Haiyang Wang, Qi Dong, Carolyn A. Meyers, Li Liu, Hongbo Bao, and Mian Guo

Subjects
0301 basic medicine, Cancer Research, Programmed cell death, Caspase 1, Biology, miR-214, Article, 03 medical and health sciences, 0302 clinical medicine, Cell Movement, Glioma, Cell Line, Tumor, microRNA, medicine, Pyroptosis, Humans, neoplasms, Cell Proliferation, Regulation of gene expression, Cell growth, Brain Neoplasms, General Medicine, medicine.disease, Cell biology, nervous system diseases, Gene Expression Regulation, Neoplastic, MicroRNAs, 030104 developmental biology, Oncology, Cell culture, 030220 oncology & carcinogenesis, Cancer research
Abstract

Pyroptosis is a type of proinflammatory programmed cell death mediated by caspase 1 activity and occurs in several types of eukaryotic tumor cells, including gliomas. MicroRNAs (miRNAs), small endogenous noncoding RNAs, have been demonstrated to be advantageous in glioma therapy. However, the question of whether miRNAs regulate pyroptosis in glioma remains unknown. The current study found that caspase 1 expression was substantially increased in both glioma tissues and glioma cell lines, U87 and T98G, while miR-214 expression was significantly downregulated. Luciferase reporter assay recognized caspase 1 as a target gene of miR-214. These findings demonstrate that miR-214 could inhibit cell proliferation and migration through the regulation of pyroptosis intermediated by caspase 1 in glioma U87 and T98G cells and may suggest a novel therapeutic for the intervention of glioma.

Published
2017

52. Calvarial Defect Healing Induced by Small Molecule Smoothened Agonist

Author

Greg Asatrian, Min Lee, Soonchul Lee, Aaron W. James, Alan Nguyen, Kang Ting, Jia Shen, Carolyn A. Meyers, Swati Shrestha, Hsin Chuan Pan, Chia Soo, and Vi Nguyen

Subjects
0301 basic medicine, Agonist, Male, Pathology, medicine.medical_specialty, medicine.drug_class, small molecule, Biomedical Engineering, Bioengineering, Bone healing, Thiophenes, Biochemistry, osteogenesis, vasculogenesis, Biomaterials, Parietal Bone, 03 medical and health sciences, Mice, Drug Delivery Systems, Tissue engineering, parasitic diseases, medicine, Animals, Dental/Oral and Craniofacial Disease, Endochondral ossification, Fracture Healing, Cyclohexylamines, Tissue Scaffolds, Chemistry, Histology, Materials Engineering, Original Articles, hedgehog signaling, Hedgehog signaling pathway, 030104 developmental biology, Intramembranous ossification, Biochemistry and Cell Biology, bone healing, smoothened agonist, Smoothened, Biomedical engineering
Abstract

Hedgehog (Hh) signaling positively regulates both endochondral and intramembranous ossification. Use of small molecules for tissue engineering applications poses several advantages. In this study, we examined whether use of an acellular scaffold treated with the small molecule Smoothened agonist (SAG) could aid in critical-size mouse calvarial defect repair. First, we verified the pro-osteogenic effect of SAG in vitro, using primary neonatal mouse calvarial cells (NMCCs). Next, a 4 mm nonhealing defect was created in the mid-parietal bone of 10-week-old CD-1 mice. The scaffold consisted of a custom-fabricated poly(lactic-co-glycolic acid) disc with hydroxyapatite coating (measuring 4 mm diameter × 0.5 mm thickness). Treatment groups included dimethylsulfoxide control (n = 6), 0.5 mM SAG (n = 7) or 1.0 mM SAG (n = 7). Evaluation was performed at 4 and 8 weeks postoperative, by a combination of high-resolution microcomputed tomography, histology (H & E, Masson's Trichrome), histomorphometry, and immunohistochemistry (BSP, OCN, VEGF). In vivo results showed that SAG treatment induced a significant and dose-dependent increase in calvarial bone healing by all radiographic parameters. Histomorphometric analysis showed an increase in all parameters of bone formation with SAG treatment, but also an increase in blood vessel number and density. In summary, SAG is a pro-osteogenic, provasculogenic stimulus when applied locally in a bone defect environment.

Published
2016

53. Pericytic mimicry (extravascular migratory metastasis) in neoplasia-reply

Author

Jia Shen, Carolyn A. Meyers, and Aaron W. James

Subjects
0301 basic medicine, business.industry, medicine.disease, Pathology and Forensic Medicine, Metastasis, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, 030220 oncology & carcinogenesis, Cancer research, Mimicry, Medicine, Humans, Neoplasm Metastasis, business, Pericytes, Melanoma
Published
2016

56. Texture and microstructure contributions to anisotropy in wrought aluminium alloys

Author

Carolyn W. Meyers and T. S. Srivatsan

Subjects
Mechanical property, Precipitation hardening, Materials science, chemistry, Aluminium, Metallurgy, chemistry.chemical_element, General Materials Science, Texture (crystalline), Microstructure, Anisotropy
Abstract

Revue des facteurs microstructuraux et de la texture influant sur les variations des proprietes mecaniques des alliages d'aluminium 2020, 6061, 7075 durcis par precipitation

Published
1987
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57. THE INFLUENCE OF MICROSTRUCTURE ON FRACTURE TOUGHNESS LEVELS IN A357 ALUMINUM ALLOY

Author

Carolyn W. Meyers

Subjects
Materials science, Metallurgy, Alloy, Sem analysis, chemistry.chemical_element, engineering.material, Microstructure, Fracture toughness, chemistry, Aluminium, engineering, sense organs, Composite material, skin and connective tissue diseases, Eutectic system
Abstract

Cast aluminum alloy A357 is used in structural applications when treated to the T6 temper. The first part of the protocol, the solution heat treatment, produces measurable changes in the silicon-rich eutectic microconstituent. This is a study of how these changes affect fracture toughness levels. The fracture toughness levels, determined using the chevron-notched short bar specimen, for a range of solution heat treatments reflect the morphological changes in the silicon-rich microconstituent. Through SEM analysis, mechanistic explanations are proposed.

Published
1988
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58. Book Reviews

Author

Carolyn W. Meyers, T. S. Srivatsan, and R. M. German

Subjects
General Engineering, General Materials Science
Published
1987
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59. Lysosomal protein surface expression discriminates fat- from bone-forming human mesenchymal precursor cells

Author

Jiajia Xu, Yiyun Wang, Ching-Yun Hsu, Stefano Negri, Robert J Tower, Yongxing Gao, Ye Tian, Takashi Sono, Carolyn A Meyers, Winters R Hardy, Leslie Chang, Shuaishuai Hu, Nusrat Kahn, Kristen Broderick, Bruno Péault, and Aaron W James

Subjects
perivascular stem cell, mesenchymal stem cell, osteogenesis, adipogenesis, CD107a/LAMP1, exocytosis, Medicine, Science, Biology (General), QH301-705.5
Abstract

Tissue resident mesenchymal stem/stromal cells (MSCs) occupy perivascular spaces. Profiling human adipose perivascular mesenchyme with antibody arrays identified 16 novel surface antigens, including endolysosomal protein CD107a. Surface CD107a expression segregates MSCs into functionally distinct subsets. In culture, CD107alow cells demonstrate high colony formation, osteoprogenitor cell frequency, and osteogenic potential. Conversely, CD107ahigh cells include almost exclusively adipocyte progenitor cells. Accordingly, human CD107alow cells drove dramatic bone formation after intramuscular transplantation in mice, and induced spine fusion in rats, whereas CD107ahigh cells did not. CD107a protein trafficking to the cell surface is associated with exocytosis during early adipogenic differentiation. RNA sequencing also suggested that CD107alow cells are precursors of CD107ahigh cells. These results document the molecular and functional diversity of perivascular regenerative cells, and show that relocation to cell surface of a lysosomal protein marks the transition from osteo- to adipogenic potential in native human MSCs, a population of substantial therapeutic interest.

Published
2020
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60. Human perivascular stem cell-derived extracellular vesicles mediate bone repair

Author

Jiajia Xu, Yiyun Wang, Ching-Yun Hsu, Yongxing Gao, Carolyn Ann Meyers, Leslie Chang, Leititia Zhang, Kristen Broderick, Catherine Ding, Bruno Peault, Kenneth Witwer, and Aaron Watkins James

Subjects
pericyte, mesenchymal stem cell, exosome, osteogenesis, bone tissue engineering, bone repair, Medicine, Science, Biology (General), QH301-705.5
Abstract

The vascular wall is a source of progenitor cells that are able to induce skeletal repair, primarily by paracrine mechanisms. Here, the paracrine role of extracellular vesicles (EVs) in bone healing was investigated. First, purified human perivascular stem cells (PSCs) were observed to induce mitogenic, pro-migratory, and pro-osteogenic effects on osteoprogenitor cells while in non-contact co-culture via elaboration of EVs. PSC-derived EVs shared mitogenic, pro-migratory, and pro-osteogenic properties of their parent cell. PSC-EV effects were dependent on surface-associated tetraspanins, as demonstrated by EV trypsinization, or neutralizing antibodies for CD9 or CD81. Moreover, shRNA knockdown in recipient cells demonstrated requirement for the CD9/CD81 binding partners IGSF8 and PTGFRN for EV bioactivity. Finally, PSC-EVs stimulated bone repair, and did so via stimulation of skeletal cell proliferation, migration, and osteodifferentiation. In sum, PSC-EVs mediate the same tissue repair effects of perivascular stem cells, and represent an ‘off-the-shelf’ alternative for bone tissue regeneration.

Published
2019
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61. Isolation and characterization of canine perivascular stem/stromal cells for bone tissue engineering.

Author

Aaron W James, Xinli Zhang, Mihaela Crisan, Winters R Hardy, Pei Liang, Carolyn A Meyers, Sonja Lobo, Venu Lagishetty, Martin K Childers, Greg Asatrian, Catherine Ding, Yu-Hsin Yen, Erin Zou, Kang Ting, Bruno Peault, and Chia Soo

Subjects
Medicine, Science
Abstract

For over 15 years, human subcutaneous adipose tissue has been recognized as a rich source of tissue resident mesenchymal stem/stromal cells (MSC). The isolation of perivascular progenitor cells from human adipose tissue by a cell sorting strategy was first published in 2008. Since this time, the interest in using pericytes and related perivascular stem/stromal cell (PSC) populations for tissue engineering has significantly increased. Here, we describe a set of experiments identifying, isolating and characterizing PSC from canine tissue (N = 12 canine adipose tissue samples). Results showed that the same antibodies used for human PSC identification and isolation are cross-reactive with canine tissue (CD45, CD146, CD34). Like their human correlate, canine PSC demonstrate characteristics of MSC including cell surface marker expression, colony forming unit-fibroblast (CFU-F) inclusion, and osteogenic differentiation potential. As well, canine PSC respond to osteoinductive signals in a similar fashion as do human PSC, such as the secreted differentiation factor NEL-Like Molecule-1 (NELL-1). Nevertheless, important differences exist between human and canine PSC, including differences in baseline osteogenic potential. In summary, canine PSC represent a multipotent mesenchymogenic cell source for future translational efforts in tissue engineering.

Published
2017
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