摘要
转基因表达的免疫应答继续妨碍基因治疗的发展。已翻译的外源蛋白胞内定位一般难以接近免疫系统,但是他们可以通过MHC I 类和II类分子途径出现在免疫系统中。随着远交小鼠质粒DNA的肌内投递,当外源蛋白荧光素酶表达时,其表达时间下降到4周。通过表达质粒和荧光素酶转基因的修饰,我们检测了远离抗原递呈细胞 (APCs)靶向抑制表达和骨骼肌及甘氨酰胺核苷酸(GAr) 融合的靶向表达的作用,他们会阻止MHC I 类分子出现在荧光霉素表达的持续时间。来自APCs的miR142-3p 3’端非翻译区荧光素酶靶序列的靶向抑制表达可以减少内源基因和表达时间未延长的GAr短序列修饰的荧光素酶的体液免疫应答。当骨骼肌的特异启动子与miR靶序列结合时,体液免疫应答受到抑制并且萤光素酶以更持久更高水平的状态表达。有趣的是,萤光素酶与较长的Gar序列结合会促进降低萤光素酶的表达,增加萤光素酶体液免疫应答。这些研究表明表达因素和转基因修饰可以改变转基因表达的持续时间,但是在骨骼肌的外源转基因表达前需要克服,其它因素处于免疫静默状态。
关键词: 基因治疗,荧光素酶,microRNA,质粒DNA,骨骼肌,组织特异启动子,转基因致免疫性
Call for Papers in Thematic Issues
Programmed Cell Death Genes in Oncology: Pioneering Therapeutic and Diagnostic Frontiers (BMS-CGT-2024-HT-45)
Programmed Cell Death (PCD) is recognized as a pivotal biological mechanism with far-reaching effects in the realm of cancer therapy. This complex process encompasses a variety of cell death modalities, including apoptosis, autophagic cell death, pyroptosis, and ferroptosis, each of which contributes to the intricate landscape of cancer development and ...read more
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