Development of potent class II transactivator gene delivery systems capable of inducing de novo MHC II expression in human cells, in vitro and ex vivo

被引:0
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作者
M L Palma
P Duangkhae
B Douradinha
I F T Viana
P O Rigato
R Dhalia
R B Mailliard
S M Barratt-Boyes
E J M Nascimento
T M Oshiro
A J da Silva Duarte
E T A Marques
机构
[1] University of Pittsburgh Center for Vaccine Research,Virology and Experimental Virology Department
[2] Laboratory of Dermatology and Immunodeficiencies,Department of Infectious Diseases and Microbiology
[3] School of Medicine from University of São Paulo,undefined
[4] Fondazione Ri.MED,undefined
[5] Center of Immunology,undefined
[6] Institute Adolfo Lutz,undefined
[7] Secretary of Health of São Paulo,undefined
[8] São Paulo,undefined
[9] Brazil,undefined
[10] Aggeu Magalhães Research Center,undefined
[11] Fiocruz,undefined
[12] University of Pittsburgh,undefined
来源
Gene Therapy | 2017年 / 24卷
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摘要
Class II transactivator (CIITA) induces transcription of major histocompatibility complex (MHC) II genes and can potentially be used to improve genetic immunotherapies by converting non-immune cells into cells capable of presenting antigens to CD4+ T cells. However, CIITA expression is tightly controlled and it remains unclear whether distinct non-immune cells differ in this transactivator regulation. Here we describe the development of gene delivery systems capable of promoting the efficient CIITA expression in non-immune cell lines and in primary human cells of an ex vivo skin explant model. Different human cell types undergoing CIITA overexpression presented high-level de novo expression of MHC II, validating the delivery systems as suitable tools for the CIITA evaluation as a molecular adjuvant for gene therapies.
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页码:342 / 352
页数:10
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