Your search keyword '"Michael G. Sun"' showing total 5 results

1. Silk films with nanotopography and extracellular proteins enhance corneal epithelial wound healing

Author

Yuncin Luo, Kai B. Kang, Rachel Sartaj, Michael G. Sun, Qiang Zhou, Victor H. Guaiquil, and Mark I. Rosenblatt

Subjects

Medicine, Science

Abstract

Abstract Corneal wound healing depends on extracellular matrix (ECM) and topographical cues that modulate migration and proliferation of regenerating cells. In our study, silk films with either flat or nanotopography patterned parallel ridge widths of 2000, 1000, 800 nm surfaces were combined with ECMs which include collagen type I (collagen I), fibronectin, laminin, and Poly-d-Lysine to accelerate corneal wound healing. Silk films with 800 nm ridge width provided better cell spreading and wound recovery than other size topographies. Coating 800 nm patterned silk films with collagen I proves to optimally further increased mouse and rabbit corneal epithelial cells growth and wound recovery. This enhanced cellular response correlated with redistribution and increase in size and total amount of focal adhesion. Transcriptomics and signaling pathway analysis suggested that silk topography regulates cell behaviors via actin nucleation ARP-WASP complex pathway, which regulate filopodia formation. This mechanism was further explored and inhibition of Cdc42, a key protein in this pathway, delayed wound healing and decreased the length, density, and alignment of filopodia. Inhibition of Cdc42 in vivo resulted in delayed re-epithelization of injured corneas. We conclude that silk film nanotopography in combination with collagen I constitutes a better substrate for corneal wound repair than either nanotopography or ECM alone.

Published

2021

2. VEGF receptor heterodimers and homodimers are differentially expressed in neuronal and endothelial cell types.

Author

Joy Sarkar, Yuncin Luo, Qiang Zhou, Evguenia Ivakhnitskaia, Daniel Lara, Eitan Katz, Michael G Sun, Victor Guaiquil, and Mark Rosenblatt

Subjects

Medicine, Science

Abstract

PurposeWe have previously reported that VEGF-B is more potent than VEGF-A in mediating corneal nerve growth in vitro and in vivo, and this stimulation of nerve growth appears to be different from stimulation of angiogenesis by these same ligands, at least in part due to differences in VEGF receptor activation. VEGF signaling may be modulated by a number of factors including receptor number or the formation of receptor hetero- vs. homodimers. In endothelial cells, VEGF receptor heterodimer (VEGR1/R2) activation after ligand binding and subsequent phosphorylation alters the activation of downstream signaling cascades. However, our understanding of these processes in neuronal cell types remains unclear. The purpose of this study was to identify the presence and distribution of VEGF Receptor-Ligand interactions in neuronal cells as compared to endothelial cells.MethodsPC12 (rat neuronal cell line), MAEC (mouse aortic endothelial cell line), MVEC (mouse venous endothelial cell line) and HUVEC (human umbilical venous endothelial cell line; control group) were used. Cells were acutely stimulated either with VEGF-A (50 ng/μL) or VEGF-B (50 ng/μL) or "vehicle" (PBS; control group). We also isolated mouse trigeminal ganglion cells from thy1-YFP neurofluorescent mice. After treatment, cells were used as follows: (i) One group was fixed in 4% paraformaldehyde and processed for VEGFR1 and VEGFR2 immunostaining and visualized using confocal fluorescence microscopy and Total Internal Reflection (TIRF) microscopy; (ii) the second group was harvested in cell lysis buffer (containing anti-protease / anti-phosphatase cocktail), lysed and processed for immunoprecipitation (IP; Thermo Fisher IP kit) and immunoblotting (IB; LI-COR® Systems). Immunoprecipitated proteins were probed either with anti-VEGFR1 or anti-VEGFR2 IgG antibodies to evaluate VEGFR1-R2-heterodimerization; (iii) a third group of cells was also processed for Duolink Proximity Ligation Assay (PLA; Sigma) to assess the presence and distribution of VEGF-receptor homo- and heterodimers in neuronal and endothelial cells.ResultsTIRF and fluorescence confocal microscopy revealed the presence of VEGFR1 co-localized with VEGFR2 in endothelial and PC12 neuronal cells. Cell lysates immunoprecipitated with anti-VEGFR1 further validated the existence of VEGFR1-R2 heterodimers in PC12 neuronal cells. Neuronal cells showed higher levels of VEGFR1-R2 heterodimers as compared to endothelial cells whereas endothelial cells showed higher VEGFR2-R2 homodimers compared to neuronal cells as demonstrated by Duolink PLA. Levels of VEGFR1-R1 homodimers were very low in neuronal and endothelial cells.ConclusionsDifferences in VEGF Receptor homo- and heterodimer distribution may explain the differential role of VEGF ligands in neuronal versus endothelial cell types. This may in turn influence VEGF activity and regulation of neuronal cell homeostasis.

Published

2022

3. VEGF receptor heterodimers and homodimers are differentially expressed in neuronal and endothelial cell types

Author

Joy Sarkar, Yuncin Luo, Qiang Zhou, Evguenia Ivakhnitskaia, Daniel Lara, Eitan Katz, Michael G. Sun, Victor Guaiquil, and Mark Rosenblatt

Subjects

Vascular Endothelial Growth Factor A, Mice, Vascular Endothelial Growth Factor B, Multidisciplinary, Receptors, Vascular Endothelial Growth Factor, Vascular Endothelial Growth Factor Receptor-1, Human Umbilical Vein Endothelial Cells, Animals, Humans, Ligands, Vascular Endothelial Growth Factor Receptor-2, Rats

Abstract

Purpose We have previously reported that VEGF-B is more potent than VEGF-A in mediating corneal nerve growth in vitro and in vivo, and this stimulation of nerve growth appears to be different from stimulation of angiogenesis by these same ligands, at least in part due to differences in VEGF receptor activation. VEGF signaling may be modulated by a number of factors including receptor number or the formation of receptor hetero- vs. homodimers. In endothelial cells, VEGF receptor heterodimer (VEGR1/R2) activation after ligand binding and subsequent phosphorylation alters the activation of downstream signaling cascades. However, our understanding of these processes in neuronal cell types remains unclear. The purpose of this study was to identify the presence and distribution of VEGF Receptor-Ligand interactions in neuronal cells as compared to endothelial cells. Methods PC12 (rat neuronal cell line), MAEC (mouse aortic endothelial cell line), MVEC (mouse venous endothelial cell line) and HUVEC (human umbilical venous endothelial cell line; control group) were used. Cells were acutely stimulated either with VEGF-A (50 ng/μL) or VEGF-B (50 ng/μL) or “vehicle” (PBS; control group). We also isolated mouse trigeminal ganglion cells from thy1-YFP neurofluorescent mice. After treatment, cells were used as follows: (i) One group was fixed in 4% paraformaldehyde and processed for VEGFR1 and VEGFR2 immunostaining and visualized using confocal fluorescence microscopy and Total Internal Reflection (TIRF) microscopy; (ii) the second group was harvested in cell lysis buffer (containing anti-protease / anti-phosphatase cocktail), lysed and processed for immunoprecipitation (IP; Thermo Fisher IP kit) and immunoblotting (IB; LI-COR® Systems). Immunoprecipitated proteins were probed either with anti-VEGFR1 or anti-VEGFR2 IgG antibodies to evaluate VEGFR1-R2-heterodimerization; (iii) a third group of cells was also processed for Duolink Proximity Ligation Assay (PLA; Sigma) to assess the presence and distribution of VEGF-receptor homo- and heterodimers in neuronal and endothelial cells. Results TIRF and fluorescence confocal microscopy revealed the presence of VEGFR1 co-localized with VEGFR2 in endothelial and PC12 neuronal cells. Cell lysates immunoprecipitated with anti-VEGFR1 further validated the existence of VEGFR1-R2 heterodimers in PC12 neuronal cells. Neuronal cells showed higher levels of VEGFR1-R2 heterodimers as compared to endothelial cells whereas endothelial cells showed higher VEGFR2-R2 homodimers compared to neuronal cells as demonstrated by Duolink PLA. Levels of VEGFR1-R1 homodimers were very low in neuronal and endothelial cells. Conclusions Differences in VEGF Receptor homo- and heterodimer distribution may explain the differential role of VEGF ligands in neuronal versus endothelial cell types. This may in turn influence VEGF activity and regulation of neuronal cell homeostasis.

Published

2021

4. Optical coherence elastography for assessing the influence of intraocular pressure on elastic wave dispersion in the cornea

Author

Michael G. Sun, Taeyoon Son, Joseph Crutison, Victor Guaiquil, Shujun Lin, Lara Nammari, Dieter Klatt, Xincheng Yao, Mark I. Rosenblatt, and Thomas J. Royston

Subjects

Cornea, Biomaterials, Tonometry, Ocular, Sound, Swine, Mechanics of Materials, Biomedical Engineering, Animals, Elasticity Imaging Techniques, Intraocular Pressure, Article

Abstract

The cornea is a highly specialized organ that relies on its mechanical stiffness to maintain its aspheric geometry and refractive power, and corneal diseases such as keratoconus have been linked to abnormal tissue stiffness and biomechanics. Dynamic optical coherence elastography (OCE) is a clinically promising non-contact and non-destructive imaging technique that can provide measurements of corneal tissue stiffness directly in vivo. The method relies on the concepts of elastography where shear waves are generated and imaged within a tissue to obtain mechanical properties such as tissue stiffness. The accuracy of OCE-based measurements is ultimately dependent on the mathematical theories used to model wave behavior in the tissue of interest. In the cornea, elastic waves propagate as guided wave modes which are highly dispersive and can be mathematically complex to model. While recent groups have developed detailed theories for estimating corneal tissue properties from guided wave behavior, the effects of intraocular pressure (IOP)-induced prestress have not yet been considered. It is known that prestress alone can strongly influence wave behavior, in addition to the associated non-linear changes in tissue properties. This present study shows that failure to account for the effects of prestress may result in overestimations of the corneal shear moduli, particularly at high IOPs. We first examined the potential effects of IOP and IOP-induced prestress using a combination of approximate mathematical theories describing wave behavior in thin plates with observations made from data published in the OCE literature. Through wave dispersion analysis, we deduce that IOP introduces a tensile hoop stress and may also influence an elastic foundational effect that were observable in the low-frequency components of the dispersion curves. These effects were incorporated into recently developed models of wave behavior in nearly incompressible, transversely isotropic (NITI) materials. Fitting of the modified NITI model with ex vivo porcine corneal data demonstrated that incorporation of the effects of IOP resulted in reduced estimates of corneal shear moduli. We believe this demonstrates that overestimation of corneal stiffness occurs if IOP is not taken into consideration. Our work may be helpful in separating inherent corneal stiffness properties that are independent of IOP; changes in these properties and in IOP are distinct, clinically relevant issues that affect the cornea health.

Published

2022

5. Climate and Spring Phenology Effects on Autumn Phenology in the Greater Khingan Mountains, Northeastern China

Author

Yuanyuan Fu, Hong S. He, Jianjun Zhao, David R. Larsen, Hongyan Zhang, Michael G. Sunde, and Shengwu Duan

Subjects

autumn phenology, Greater Khingan Mountains, ecogeographical region, GIMMS NDVI3g, climate change, spring phenology, Science

Abstract

Vegetation phenology plays a key role in terrestrial ecosystem nutrient and carbon cycles and is sensitive to global climate change. Compared with spring phenology, which has been well studied, autumn phenology is still poorly understood. In this study, we estimated the date of the end of the growing season (EOS) across the Greater Khingan Mountains, China, from 1982 to 2015 based on the Global Inventory Modeling and Mapping Studies (GIMMS) normalized difference vegetation index third-generation (NDVI3g) dataset. The temporal correlations between EOS and climatic factors (e.g., preseason temperature, preseason precipitation), as well as the correlation between autumn and spring phenology, were investigated using partial correlation analysis. Results showed that more than 94% of the pixels in the Greater Khingan Mountains exhibited a delayed EOS trend, with an average rate of 0.23 days/y. Increased preseason temperature resulted in earlier EOS in most of our study area, except for the semi-arid grassland region in the south, where preseason warming generally delayed EOS. Similarly, EOS in most of the mountain deciduous coniferous forest, forest grassland, and mountain grassland forest regions was earlier associated with increased preseason precipitation, but for the semi-arid grassland region, increased precipitation during the preseason mainly led to delayed EOS. However, the effect of preseason precipitation on EOS in most of the Greater Khingan Mountains was stronger than that of preseason temperature. In addition to the climatic effects on EOS, we also found an influence of spring phenology on EOS. An earlier SOS led to a delayed EOS in most of the study area, while in the southern of mountain deciduous coniferous forest region and northern of semi-arid grassland region, an earlier SOS was often followed by an earlier EOS. These findings suggest that both climatic factors and spring phenology should be incorporated into autumn phenology models in order to improve prediction accuracy under present and future climate change scenarios.

Published

2018