首页> 外文期刊>Molecular therapy: the journal of the American Society of Gene Therapy >Design of tissue-specific regulatory cassettes for high-level rAAV-mediated expression in skeletal and cardiac muscle.
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Design of tissue-specific regulatory cassettes for high-level rAAV-mediated expression in skeletal and cardiac muscle.

机译:组织特异性调节盒的设计,用于在骨骼肌和心肌中进行高水平的rAAV介导的表达。

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Systemic delivery of recombinant adeno-associated virus (rAAV) 6 vectors mediates efficient transduction of the entire striated musculature, making this an attractive strategy for muscle gene therapy. However, owing to widespread transduction of non-muscle tissues, optimization of this method would benefit from the use of muscle-specific promoters. Most such promoters either lack high-level expression in certain muscle types or are too large for inclusion in rAAV vectors encoding microdystrophin. Here, we describe novel regulatory cassettes based on enhancer/promoter regions of murine muscle creatine kinase (CK) and alpha-myosin heavy-chain genes. The strongest cassette, MHCK7 (770 bp), directs high-level expression comparable to cytomegalovirus and Rous sarcoma virus promoters in fast and slow skeletal and cardiac muscle, and low expression in the liver, lung, and spleen following systemic rAAV6 delivery in mice. Compared with CK6, our previous best cassette, MHCK7 activity is approximately 400-, approximately 50-, and approximately 10-fold higher in cardiac, diaphragm, and soleus muscles, respectively. MHCK7 also directs strong microdystrophin expression in mdx muscles. While further study of immune responses to MHCK7-regulated microdystrophin expression is needed, this cassette is not active in dendritic cell lines. MHCK7 is thus a highly improved regulatory cassette for experimental studies of rAAV-mediated transduction of striated muscle.
机译:重组腺相关病毒(rAAV)6载体的系统递送介导了整个横纹肌组织的有效转导,这使其成为肌肉基因治疗的诱人策略。但是,由于非肌肉组织的广泛转导,该方法的优化将受益于使用肌肉特异性启动子。大多数此类启动子在某些肌肉类型中缺乏高水平表达,或者太大而无法包含在编码微肌营养蛋白的rAAV载体中。在这里,我们描述了基于鼠肌肉肌酸激酶(CK)和α-肌球蛋白重链基因的增强子/启动子区域的新型调控盒。最强的盒体MHCK7(770 bp)指导快速和慢速骨骼肌和心肌中与巨细胞病毒和Rous肉瘤病毒启动子相当的高水平表达,并在小鼠全身性rAAV6递送后在肝,肺和脾中低表达。与我们以前最好的盒式磁带CK6相比,MHCK7在心肌,diaphragm肌和比目鱼肌中的活性分别高约400倍,约50倍和约10倍。 MHCK7还指导mdx肌肉中强烈的抗肌营养不良蛋白表达。虽然需要进一步研究对MHCK7调节的微肌营养不良蛋白表达的免疫反应,但该盒在树突状细胞系中不活跃。因此,MHCK7是高度改良的调控盒,用于rAAV介导的横纹肌转导的实验研究。

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