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辅助依赖性犬腺病毒载体介导的神经退行性溶酶体贮积病中的转基因表达。

Helper-dependent canine adenovirus vector-mediated transgene expression in a neurodegenerative lysosomal storage disorder.

机构信息

Lysosomal Diseases Research Unit, SA Pathology at the Women's and Children's Hospital, Australia.

出版信息

Gene. 2012 Jan 1;491(1):53-7. doi: 10.1016/j.gene.2011.09.004. Epub 2011 Sep 22.

Abstract

Mucopolysaccharidosis type IIIA (MPS-IIIA) is a severe neurodegenerative lysosomal storage disorder caused by a deficiency of N-sulfoglucosamine sulfohydrolase (SGSH) activity with subsequent accumulation of partially-degraded heparan sulfate and other glycolipids. In this study, we have evaluated a gene therapy approach using a helper-dependent canine adenovirus vector that expresses human SGSH as a means of delivering sustained transgene expression to the brain. Initial testing in a mixed neural cell culture model demonstrated that the vector could significantly increase SGSH activity in transduced cells, resulting in near-normalization of heparan sulfate-derived fragments. While administration of vector by direct injection into the brain of adult MPS-IIIA mice enabled transgene expression for at least 8.5 months post-treatment, it was only in discrete areas of brain. Heparan sulfate storage was reduced in some regions following treatment, however there was no improvement in secondary neuropathological changes. These data demonstrate that helper-dependent canine adenovirus vectors are capable of neural transduction and mediate long-term transgene expression, but increased SGSH expression throughout the brain is likely to be required in order to effectively treat all aspects of the MPS-IIIA phenotype.

摘要

黏多糖贮积症 IIIA 型(MPS-IIIA)是一种严重的神经退行性溶酶体贮积病,由 N-磺基葡萄糖胺磺基水解酶(SGSH)活性缺乏引起,随后会积累部分降解的肝素硫酸和其他糖脂。在这项研究中,我们评估了一种使用辅助依赖性犬腺病毒载体的基因治疗方法,该载体表达人 SGSH,作为向大脑提供持续转基因表达的手段。在混合神经细胞培养模型中的初步测试表明,该载体可以显著增加转导细胞中的 SGSH 活性,导致肝素硫酸衍生片段接近正常化。虽然将载体直接注射到成年 MPS-IIIA 小鼠的大脑中可以使转基因表达至少在治疗后 8.5 个月,但仅在大脑的离散区域中。治疗后,一些区域的肝素硫酸储存减少,但继发性神经病理学变化没有改善。这些数据表明,辅助依赖性犬腺病毒载体能够进行神经转导并介导长期转基因表达,但为了有效治疗 MPS-IIIA 表型的所有方面,可能需要在整个大脑中增加 SGSH 表达。

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