Development of bionic invasion membrane for the study of multiple sclerosis

Chia Yi Lee; Kin Fong Lei; Cheng Lung Ku; Chia Hao Huang

doi:10.1109/NEMS.2016.7758270

Development of bionic invasion membrane for the study of multiple sclerosis

Chia Yi Lee, Kin Fong Lei, Cheng Lung Ku, Chia Hao Huang

Chang Gung University

Research output: Chapter in Book/Report/Conference proceeding › Conference contribution › peer-review

Abstract

Multiple sclerosis (MS) is an autoimmune disease and leads to many inflammations. Cause of this disease is autoreactive T cells invade the blood-brain-barrier and attack the myelin sheath. Because MS infringes upon young human and has gradual loss of bodily functions, the disease has a burden on society and economy. Traditional treatment is to use immune-suppressant, but it has many side effects. Currently, the most effective treatment of MS is to use Natalizumab. Target molecule of this agent is α4-integrin of T cells. The mechanism is to prevent invasion of activated lymphocytes across the blood-brain-barrier. However, this agent affects the overall immune response and easily generates side effects of progressive multifocal leukoencephalopathy (PML). Transwall systems are often used to investigate cell invasion, but there is no specific protein immobilizing on the isolation membrane of these systems. In this work, we have successfully developed a bionic invasion membrane for the study of MS. Different chemokines were applied to the system for the demonstration of drug screening application. The bionic invasion membrane was a PP/PTEE membrane coated with VCAM-1 protein. Jurkat T cell was used to evaluate the feasibility of using the membrane for the study of MS. Results indicated that the invasion ability of T cells was reduced by VCAM-1 protein. The current work provides bionic invasion membrane for the study of MS in vitro.

Original language	English
Title of host publication	2016 IEEE 11th Annual International Conference on Nano/Micro Engineered and Molecular Systems, NEMS 2016
Publisher	Institute of Electrical and Electronics Engineers Inc.
Pages	370-374
Number of pages	5
ISBN (Electronic)	9781509019472
DOIs	https://doi.org/10.1109/NEMS.2016.7758270
State	Published - 28 11 2016
Event	11th IEEE Annual International Conference on Nano/Micro Engineered and Molecular Systems, NEMS 2016 - Sendai, Japan Duration: 17 04 2016 → 20 04 2016

Publication series

Name	2016 IEEE 11th Annual International Conference on Nano/Micro Engineered and Molecular Systems, NEMS 2016

Conference

Conference	11th IEEE Annual International Conference on Nano/Micro Engineered and Molecular Systems, NEMS 2016
Country/Territory	Japan
City	Sendai
Period	17/04/16 → 20/04/16

Bibliographical note

Publisher Copyright:
© 2016 IEEE.

Keywords

Biochip
Jurkat T cell
Multiple sclerosis
Transwell
blood-brain-barrier

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

Access to Document

10.1109/NEMS.2016.7758270

Cite this

Lee, C. Y., Lei, K. F., Ku, C. L., & Huang, C. H. (2016). Development of bionic invasion membrane for the study of multiple sclerosis. In 2016 IEEE 11th Annual International Conference on Nano/Micro Engineered and Molecular Systems, NEMS 2016 (pp. 370-374). Article 7758270 (2016 IEEE 11th Annual International Conference on Nano/Micro Engineered and Molecular Systems, NEMS 2016). Institute of Electrical and Electronics Engineers Inc.. https://doi.org/10.1109/NEMS.2016.7758270

Lee, Chia Yi ; Lei, Kin Fong ; Ku, Cheng Lung et al. / Development of bionic invasion membrane for the study of multiple sclerosis. 2016 IEEE 11th Annual International Conference on Nano/Micro Engineered and Molecular Systems, NEMS 2016. Institute of Electrical and Electronics Engineers Inc., 2016. pp. 370-374 (2016 IEEE 11th Annual International Conference on Nano/Micro Engineered and Molecular Systems, NEMS 2016).

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abstract = "Multiple sclerosis (MS) is an autoimmune disease and leads to many inflammations. Cause of this disease is autoreactive T cells invade the blood-brain-barrier and attack the myelin sheath. Because MS infringes upon young human and has gradual loss of bodily functions, the disease has a burden on society and economy. Traditional treatment is to use immune-suppressant, but it has many side effects. Currently, the most effective treatment of MS is to use Natalizumab. Target molecule of this agent is α4-integrin of T cells. The mechanism is to prevent invasion of activated lymphocytes across the blood-brain-barrier. However, this agent affects the overall immune response and easily generates side effects of progressive multifocal leukoencephalopathy (PML). Transwall systems are often used to investigate cell invasion, but there is no specific protein immobilizing on the isolation membrane of these systems. In this work, we have successfully developed a bionic invasion membrane for the study of MS. Different chemokines were applied to the system for the demonstration of drug screening application. The bionic invasion membrane was a PP/PTEE membrane coated with VCAM-1 protein. Jurkat T cell was used to evaluate the feasibility of using the membrane for the study of MS. Results indicated that the invasion ability of T cells was reduced by VCAM-1 protein. The current work provides bionic invasion membrane for the study of MS in vitro.",

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Lee, CY, Lei, KF , Ku, CL & Huang, CH 2016, Development of bionic invasion membrane for the study of multiple sclerosis. in 2016 IEEE 11th Annual International Conference on Nano/Micro Engineered and Molecular Systems, NEMS 2016., 7758270, 2016 IEEE 11th Annual International Conference on Nano/Micro Engineered and Molecular Systems, NEMS 2016, Institute of Electrical and Electronics Engineers Inc., pp. 370-374, 11th IEEE Annual International Conference on Nano/Micro Engineered and Molecular Systems, NEMS 2016, Sendai, Japan, 17/04/16. https://doi.org/10.1109/NEMS.2016.7758270

Development of bionic invasion membrane for the study of multiple sclerosis. / Lee, Chia Yi; Lei, Kin Fong ; Ku, Cheng Lung et al.
2016 IEEE 11th Annual International Conference on Nano/Micro Engineered and Molecular Systems, NEMS 2016. Institute of Electrical and Electronics Engineers Inc., 2016. p. 370-374 7758270 (2016 IEEE 11th Annual International Conference on Nano/Micro Engineered and Molecular Systems, NEMS 2016).

Research output: Chapter in Book/Report/Conference proceeding › Conference contribution › peer-review

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AU - Lei, Kin Fong

AU - Ku, Cheng Lung

AU - Huang, Chia Hao

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N2 - Multiple sclerosis (MS) is an autoimmune disease and leads to many inflammations. Cause of this disease is autoreactive T cells invade the blood-brain-barrier and attack the myelin sheath. Because MS infringes upon young human and has gradual loss of bodily functions, the disease has a burden on society and economy. Traditional treatment is to use immune-suppressant, but it has many side effects. Currently, the most effective treatment of MS is to use Natalizumab. Target molecule of this agent is α4-integrin of T cells. The mechanism is to prevent invasion of activated lymphocytes across the blood-brain-barrier. However, this agent affects the overall immune response and easily generates side effects of progressive multifocal leukoencephalopathy (PML). Transwall systems are often used to investigate cell invasion, but there is no specific protein immobilizing on the isolation membrane of these systems. In this work, we have successfully developed a bionic invasion membrane for the study of MS. Different chemokines were applied to the system for the demonstration of drug screening application. The bionic invasion membrane was a PP/PTEE membrane coated with VCAM-1 protein. Jurkat T cell was used to evaluate the feasibility of using the membrane for the study of MS. Results indicated that the invasion ability of T cells was reduced by VCAM-1 protein. The current work provides bionic invasion membrane for the study of MS in vitro.

AB - Multiple sclerosis (MS) is an autoimmune disease and leads to many inflammations. Cause of this disease is autoreactive T cells invade the blood-brain-barrier and attack the myelin sheath. Because MS infringes upon young human and has gradual loss of bodily functions, the disease has a burden on society and economy. Traditional treatment is to use immune-suppressant, but it has many side effects. Currently, the most effective treatment of MS is to use Natalizumab. Target molecule of this agent is α4-integrin of T cells. The mechanism is to prevent invasion of activated lymphocytes across the blood-brain-barrier. However, this agent affects the overall immune response and easily generates side effects of progressive multifocal leukoencephalopathy (PML). Transwall systems are often used to investigate cell invasion, but there is no specific protein immobilizing on the isolation membrane of these systems. In this work, we have successfully developed a bionic invasion membrane for the study of MS. Different chemokines were applied to the system for the demonstration of drug screening application. The bionic invasion membrane was a PP/PTEE membrane coated with VCAM-1 protein. Jurkat T cell was used to evaluate the feasibility of using the membrane for the study of MS. Results indicated that the invasion ability of T cells was reduced by VCAM-1 protein. The current work provides bionic invasion membrane for the study of MS in vitro.

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Lee CY, Lei KF , Ku CL, Huang CH. Development of bionic invasion membrane for the study of multiple sclerosis. In 2016 IEEE 11th Annual International Conference on Nano/Micro Engineered and Molecular Systems, NEMS 2016. Institute of Electrical and Electronics Engineers Inc. 2016. p. 370-374. 7758270. (2016 IEEE 11th Annual International Conference on Nano/Micro Engineered and Molecular Systems, NEMS 2016). doi: 10.1109/NEMS.2016.7758270

Development of bionic invasion membrane for the study of multiple sclerosis

Abstract

Publication series

Conference

Bibliographical note

Keywords

UN SDGs

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