NLS公司
核定位序列
内化
转染
壳聚糖
基因传递
化学
肽
核运输
生物物理学
内生
天然化学连接
细胞生物学
基因
生物化学
生物
细胞核
细胞
酶
半胱氨酸
作者
Diogo B. Bitoque,Joana Morais,Ana V. Oliveira,Raquel L. Sequeira,Sofia M. Calado,Tiago M. Fortunato,Sónia Simão,Ana M. Rosa da Costa,Gabriela A. Silva
摘要
Nuclear import is considered as one of the major limitations for non-viral gene delivery systems and the incorporation of nuclear localization signals (NLS) that mediate nuclear intake can be used as a strategy to enhance internalization of exogenous DNA. In this work, human-derived endogenous NLS peptides based on insulin growth factor binding proteins (IGFBP), namely IGFBP-3 and IGFBP-5, were tested for their ability to improve nuclear translocation of genetic material by non-viral vectors. Several strategies were tested to determine their effect on chitosan mediated transfection efficiency: co-administration with polyplexes, co-complexation at the time of polyplex formation, and covalent ligation to chitosan. Our results show that co-complexation and covalent ligation of the NLS peptide derived from IGFBP-3 to chitosan polyplexes yields a 2-fold increase in transfection efficiency, which was not observed for NLS peptide derived from IGFBP-5. These results indicate that the integration of IGFBP-NLS-3 peptides into polyplexes has potential as a strategy to enhance the efficiency of non-viral vectors.
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