Vang-Dings - Center for Integrative Nanotechnology Sciences - ÌÇÐÄVlog´«Ã½ Little Rock /nanotechnology/category/vang-dings/ ÌÇÐÄVlog´«Ã½ Little Rock Wed, 30 Oct 2024 13:32:47 +0000 en-US hourly 1 https://wordpress.org/?v=6.9.4 Dendritic cell biocompatibility of ether-based urethane films /nanotechnology/2021/03/01/dendritic-cell-biocompatibility-of-ether-based-urethane-films/ Mon, 01 Mar 2021 22:32:09 +0000 https://ualrprd.wpengine.com/nanotechnology/?p=2727 Authors: Ingrid Safina, Karrer M Alghazali, Luke Childress, Christopher Griffin, Ahmed Hashoosh, Ganesh Kannarpady, Fumiya Watanabe, Shawn E Bourdo, Ruud P M Dings, Alexandru S Biris, Kieng Bao Vang  Publication: J Appl Toxicol. 2021 Jan 8. doi: 10.1002/jat.4136. Epub ahead of ... Dendritic cell biocompatibility of ether-based urethane films

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Authors: Ingrid SafinaKarrer M AlghazaliLuke ChildressChristopher GriffinAhmed HashooshGanesh KannarpadyFumiya WatanabeShawn E BourdoRuud P M DingsAlexandru S BirisKieng Bao Vang 

Publication: J Appl Toxicol. 2021 Jan 8. doi: 10.1002/jat.4136. Epub ahead of print. PMID: 33417269.

Abstract: The use of synthetic materials for biomedical applications is ever expanding. One of the major requirements for these materials is biocompatibility, which includes prevention of immune system responses. Due to the inherent complexity of their structural composition, the polyurethane (PU) family of polymers is being used in a variety of medical applications, from soft and hard tissue scaffolds to intricate coatings on implantable devices. Herein, we investigated whether two polymer materials, D3 and D7, induced an immune response, measured by their effects on a dendritic cell (DC) line, JAWS II. Using a lactate dehydrogenase cytotoxicity assay and Annexin V/PI staining, we found that the PU materials did not induce cytotoxicity in DC cells. Using confocal microscopy, we also showed that the materials did not induce activation or maturation, as compared to positive controls. This was confirmed by looking at various markers, CD80, CD86, MHC class I, and MHC class II, via flow cytometry. Overall, the results indicated that the investigated PU films are biocompatible in terms of immunotoxicology and immunogenicity and show great promise for use in regenerative medicine.

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Graphene-based 2D constructs for enhanced fibroblast support /nanotechnology/2020/05/18/graphene-based-2d-constructs-for-enhanced-fibroblast-support/ Mon, 18 May 2020 18:54:44 +0000 https://ualrprd.wpengine.com/nanotechnology/?p=2702 Authors: Ingrid Safina, Shawn E. Bourdo, Karrer M. Algazali, Ganesh Kannarpady, Fumiya Watanabe, Kieng Bao Vang, Alexandru S. Biris Publication: PLoS One. 2020;15(5):e0232670. Published 2020 May 18. doi:10.1371/journal.pone.0232670 Abstract: Complex skin ... Graphene-based 2D constructs for enhanced fibroblast support

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Authors: Ingrid Safina, Shawn E. Bourdo, Karrer M. Algazali, Ganesh Kannarpady, Fumiya Watanabe, Kieng Bao Vang, Alexandru S. Biris

Publication: PLoS One. 2020;15(5):e0232670. Published 2020 May 18. doi:10.1371/journal.pone.0232670

Abstract: Complex skin wounds have always been a significant health and economic problem worldwide due to their elusive and sometimes poor or non-healing conditions. If not well-treated,
such wounds may lead to amputation, infections, cancer, or even death. Thus, there is a need to efficiently generate multifunctional skin grafts that address a wide range of skin conditions, including non-healing wounds, and enable the regeneration of new skin tissue. Here, we propose studying pristine graphene and two of its oxygen-functionalized derivatives—high and low-oxygen graphene films—as potential substrates for skin cell proliferation and differentiation. Using BJ cells (human foreskin-derived fibroblasts) to represent basic skin cells, we show that the changes in surface properties of pristine graphene due to oxygen functionalization do not seem to statistically impact the normal proliferation and maturation of skin cells. Our results indicate that the pristine and oxidized graphenes presented relatively low cytotoxicity to BJ fibroblasts and, in fact, support their growth and bioactivity. Therefore, these graphene films could potentially be integrated into more complex skin regenerative systems to support skin regeneration. Because graphene’s surface can be relatively easily functionalized with various chemical groups, this finding presents a major opportunity for the development of various composite materials that can act as active components in regenerative applications such as skin regeneration.

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Identification of Cellular Sources of IL-2 Needed for Regulatory T Cell Development and Homeostasis /nanotechnology/2018/06/15/identification-of-cellular-sources-of-il-2-needed-for-regulatory-t-cell-development-and-homeostasis/ Fri, 15 Jun 2018 17:54:28 +0000 https://ualrprd.wpengine.com/nanotechnology/?p=2638 Authors: David L. Owen, Shawn A. Mahmud, Kieng B. Vang, Ryan M. Kelly, Bruce R. Blazar, Kendall A. Smith and Michael A. Farrar Publication: J Immunol June 15, 2018, 200 (12) 3926-3933 Abstract: The cytokine IL-2 is critical for promoting the ... Identification of Cellular Sources of IL-2 Needed for Regulatory T Cell Development and Homeostasis

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Authors: David L. OwenShawn A. MahmudKieng B. VangRyan M. KellyBruce R. BlazarKendall A. Smith and Michael A. Farrar

Publication:

Abstract: The cytokine IL-2 is critical for promoting the development, homeostasis, and function of regulatory T (Treg) cells. The cellular sources of IL-2 that promote these processes remain unclear. T cells, B cells, and dendritic cells (DCs) are known to make IL-2 in peripheral tissues. We found that T cells and DCs in the thymus also make IL-2. To identify cellular sources of IL-2 in Treg cell development and homeostasis, we used Il2FL/FL mice to selectively delete Il2 in T cells, B cells, and DCs. Because IL-15 can partially substitute for IL-2 in Treg cell development, we carried out the majority of these studies on an Il15−/− background. Deletion of Il2 in B cells, DCs, or both these subsets had no effect on Treg cell development, either in wild-type (WT) or Il15−/− mice. Deletion of Il2 in T cells had minimal effects in WT mice but virtually eliminated developing Treg cells in Il15−/− mice. In the spleen and most peripheral lymphoid organs, deletion of Il2 in B cells, DCs, or both subsets had no effect on Treg cell homeostasis. In contrast, deletion of Il2 in T cells led to a significant decrease in Treg cells in either WT or Il15−/− mice. The one exception was the mesenteric lymph nodes where significantly fewer Treg cells were observed when Il2 was deleted in both T cells and DCs. Thus, T cells are the sole source of IL-2 needed for Treg cell development, but DCs can contribute to Treg cell homeostasis in select organs.

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