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囊性纤维化的基因治疗:改进的递送技术和溶血磷脂酰胆碱预处理可增强慢病毒在小鼠肺气道中的基因转移。

Gene therapy for Cystic Fibrosis: Improved delivery techniques and conditioning with lysophosphatidylcholine enhance lentiviral gene transfer in mouse lung airways.

作者信息

Cmielewski Patricia, Farrow Nigel, Devereux Sharnna, Parsons David, Donnelley Martin

机构信息

a Department of Respiratory and Sleep Medicine , Women's and Children's Hospital Network , North Adelaide , SA , Australia.

b Robinson Research Institute, University of Adelaide , Adelaide , SA , Australia.

出版信息

Exp Lung Res. 2017 Nov-Dec;43(9-10):426-433. doi: 10.1080/01902148.2017.1395931. Epub 2017 Dec 13.

Abstract

UNLABELLED

Purpose/Aim: Cystic fibrosis (CF) is the most common, fatal recessive genetic disease among the Caucasian population. Gene therapy has the potential to treat CF long term, however physiological barriers can prevent VSV-G pseudotyped lentiviral (LV) vectors from efficiently accessing the relevant receptors on the basolateral membrane of airway epithelial cells. The aims of this experiment were to use our new dose delivery techniques to determine whether conditioning the mouse lung conducting airways with lysophosphatidylcholine (LPC) improves the level of airway gene expression.

MATERIALS AND METHODS

Anaesthetised normal C57Bl/6 mice were intubated with an endotracheal cannula to non-invasively facilitate airway access. The airways were conditioned with 0.1% LPC, 0.3% LPC, or PBS (control) instilled via the ET tube. One hour later a VSV-G pseudotyped LV vector carrying the LacZ transgene was delivered. LacZ expression was measured by X-gal staining of the excised lungs 3 months after gene delivery.

RESULTS

Endotracheal intubation enabled precise dose delivery to the trachea and conducting airways. The cartilaginous airways of the groups conditioned with 0.1% and 0.3% LPC contained significantly larger numbers of LacZ positive cells compared to the PBS control group. In the LPC conditioned groups the majority of cell transduction was in ciliated epithelial cells.

CONCLUSION

LPC conditioning prior to LV vector delivery, substantially enhanced the level of conducting airway gene expression after a single gene vector delivery. These results extend the previously established effectiveness of this protocol for producing gene expression in the nasal airways to the lung airways, the primary site of deleterious pathophysiology in CF individuals.

摘要

未标记

目的/目标:囊性纤维化(CF)是白种人群中最常见的致命隐性遗传病。基因治疗有潜力长期治疗CF,然而生理屏障可阻止水泡性口炎病毒糖蛋白(VSV-G)假型慢病毒(LV)载体有效进入气道上皮细胞基底外侧膜上的相关受体。本实验的目的是使用我们新的剂量递送技术,确定用溶血磷脂酰胆碱(LPC)预处理小鼠肺传导气道是否能提高气道基因表达水平。

材料与方法

将麻醉的正常C57Bl/6小鼠经气管插管进行气管内插管,以无创方式便于气道进入。通过气管内导管向气道内注入0.1% LPC、0.3% LPC或PBS(对照)进行预处理。1小时后,递送携带LacZ转基因的VSV-G假型LV载体。基因递送3个月后,通过对切除的肺进行X-gal染色来测量LacZ表达。

结果

气管内插管能够将精确剂量递送至气管和传导气道。与PBS对照组相比,用0.1%和0.3% LPC预处理的组的软骨气道中LacZ阳性细胞数量明显更多。在LPC预处理组中,大多数细胞转导发生在纤毛上皮细胞中。

结论

在LV载体递送前用LPC预处理,在单次基因载体递送后显著提高了传导气道基因表达水平。这些结果将先前确立的该方案在鼻气道产生基因表达的有效性扩展到了肺气道,而肺气道是CF患者有害病理生理学的主要部位。

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