Enhancing infection affinity of therapeutic recombinant viral vectors to targeted cells in regenerative nanomedicine

Enhancing infection affinity of therapeutic recombinant viral vectors to targeted cells in regenerative nanomedicine

Hyaline articular cartilage trauma and degeneration are major causes of suffering and pose great threat to the life quality of human beings worldwide. In cell-based therapy, TGF-β3 could be dosed to synovium-derived mesenchymal stem cells to induce differentiation into chondrocytes. However, type I...

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Main Authors: Zhang, Feng, Su, Kai, Fang, Yu, Wang, Dong-An
Other Authors: School of Chemical and Biomedical Engineering
Format: Article
Language:English
Published: 2014
Subjects:
DRNTU::Science::Chemistry::Biochemistry
Online Access:https://hdl.handle.net/10356/100873
http://hdl.handle.net/10220/18980
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Institution: Nanyang Technological University
Language: English
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spelling sg-ntu-dr.10356-1008732020-03-07T11:40:20Z Enhancing infection affinity of therapeutic recombinant viral vectors to targeted cells in regenerative nanomedicine Zhang, Feng Su, Kai Fang, Yu Wang, Dong-An School of Chemical and Biomedical Engineering DRNTU::Science::Chemistry::Biochemistry Hyaline articular cartilage trauma and degeneration are major causes of suffering and pose great threat to the life quality of human beings worldwide. In cell-based therapy, TGF-β3 could be dosed to synovium-derived mesenchymal stem cells to induce differentiation into chondrocytes. However, type I collagen is intrinsically expressed and upregulated during monolayer culture by the introduction of TGF-β3, which would result in the formation of fibrous cartilage. Therefore, RNA interference strategy was adopted to suppress the expression of type I collagen by degrading its mRNA in a posttranscriptional pathway. In our study, we constructed a dual-functioning lentiviral vector that can express TGF-β3 and inhibit type I collagen expression. Based on this lentiviral vector, protocols for lentiviral titration, transduction and TGF-β3 quantification in the active form with modified ELISA would be specifically formulated and provided. Optimal medium would also be selected for the culture of transduced cells. Particularly, as the lentiviral nanoparticles are encapsulated in negative-charged envelope, there would be electrical repulsion between the lentiviral nanoparticles and the cells during viral transduction. Therefore, positive-charged polybrene has been added to mitigate the repulsion and facilitate lentiviral transduction. In our study, we tried several polybrene concentrations and determined the optimal one for lentiviral transduction. 2014-03-26T08:44:41Z 2019-12-06T20:29:34Z 2014-03-26T08:44:41Z 2019-12-06T20:29:34Z 2013 2013 Journal Article Zhang, F., Su, K., Fang, Y., & Wang, D.-A. (2013). Enhancing Infection Affinity of Therapeutic Recombinant Viral Vectors to Targeted Cells in Regenerative Nanomedicine. Nanoscience and Nanotechnology Letters, 5(2), 167-173. https://hdl.handle.net/10356/100873 http://hdl.handle.net/10220/18980 10.1166/nnl.2013.1493 en Nanoscience and nanotechnology letters © 2013 American Scientific Publishers.
institution Nanyang Technological University
building NTU Library
country Singapore
collection DR-NTU
language English
topic DRNTU::Science::Chemistry::Biochemistry
spellingShingle DRNTU::Science::Chemistry::Biochemistry
Zhang, Feng
Su, Kai
Fang, Yu
Wang, Dong-An
Enhancing infection affinity of therapeutic recombinant viral vectors to targeted cells in regenerative nanomedicine
description Hyaline articular cartilage trauma and degeneration are major causes of suffering and pose great threat to the life quality of human beings worldwide. In cell-based therapy, TGF-β3 could be dosed to synovium-derived mesenchymal stem cells to induce differentiation into chondrocytes. However, type I collagen is intrinsically expressed and upregulated during monolayer culture by the introduction of TGF-β3, which would result in the formation of fibrous cartilage. Therefore, RNA interference strategy was adopted to suppress the expression of type I collagen by degrading its mRNA in a posttranscriptional pathway. In our study, we constructed a dual-functioning lentiviral vector that can express TGF-β3 and inhibit type I collagen expression. Based on this lentiviral vector, protocols for lentiviral titration, transduction and TGF-β3 quantification in the active form with modified ELISA would be specifically formulated and provided. Optimal medium would also be selected for the culture of transduced cells. Particularly, as the lentiviral nanoparticles are encapsulated in negative-charged envelope, there would be electrical repulsion between the lentiviral nanoparticles and the cells during viral transduction. Therefore, positive-charged polybrene has been added to mitigate the repulsion and facilitate lentiviral transduction. In our study, we tried several polybrene concentrations and determined the optimal one for lentiviral transduction.
author2 School of Chemical and Biomedical Engineering
author_facet School of Chemical and Biomedical Engineering
Zhang, Feng
Su, Kai
Fang, Yu
Wang, Dong-An
format Article
author Zhang, Feng
Su, Kai
Fang, Yu
Wang, Dong-An
author_sort Zhang, Feng
title Enhancing infection affinity of therapeutic recombinant viral vectors to targeted cells in regenerative nanomedicine
title_short Enhancing infection affinity of therapeutic recombinant viral vectors to targeted cells in regenerative nanomedicine
title_full Enhancing infection affinity of therapeutic recombinant viral vectors to targeted cells in regenerative nanomedicine
title_fullStr Enhancing infection affinity of therapeutic recombinant viral vectors to targeted cells in regenerative nanomedicine
title_full_unstemmed Enhancing infection affinity of therapeutic recombinant viral vectors to targeted cells in regenerative nanomedicine
title_sort enhancing infection affinity of therapeutic recombinant viral vectors to targeted cells in regenerative nanomedicine
publishDate 2014
url https://hdl.handle.net/10356/100873
http://hdl.handle.net/10220/18980
_version_ 1681039508655570944

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