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基因治疗相关性葡萄膜炎的特征:玻璃体内注射腺相关病毒在小鼠模型中的研究。

Characterization of Gene Therapy Associated Uveitis Following Intravitreal Adeno-Associated Virus Injection in Mice.

机构信息

University of Washington, Department of Ophthalmology, Seattle, Washington, United States.

出版信息

Invest Ophthalmol Vis Sci. 2021 Feb 1;62(2):41. doi: 10.1167/iovs.62.2.41.

Abstract

PURPOSE

To characterize the intraocular immune cell infiltrate induced by intravitreal adeno-associated virus (AAV) gene therapy.

METHODS

AAV vectors carrying plasmids expressing green fluorescent protein under the control of PR2.1 were injected intravitreally into AAV naive and AAV primed C57Bl/6 mice. Clinical inflammation was assessed using optical coherence tomography. Intraocular immune cell populations were identified and quantified by flow cytometry on days 1, 7, and 29 after intravitreal injection and compared with sham and fellow eye controls.

RESULTS

Optical coherence tomography inflammation score and total CD45+ cell number were significantly higher in AAV injected eyes compared to uninjected fellow eye and sham injected controls. Clinically apparent inflammation (vitritis on optical coherence tomography) and cellular inflammation (CD45+ cell number) was significantly increased in AAV injected eyes and peaked around day 7. Vitritis resolved by day 29, but cellular inflammation persisted through day 29. On day 1, neutrophils and activated monocytes were the dominant cell populations in all AAV injected eyes. On day 7, eyes of AAV exposed animals had significantly more dendritic cells and T cells than eyes of AAV naive animals. By day 29, CD8- T cells were the dominant CD45+ cell population in AAV injected eyes.

CONCLUSIONS

Intravitreal AAV injection in mice generates clinically evident inflammation that is mild and seems to resolve spontaneously. However, the total number of intraocular CD45+ cells, particularly T cells, remain elevated. Both innate and adaptive immune cells respond to intravitreal AAV regardless of prior immune status, but the adaptive response is delayed in AAV naive eyes.

摘要

目的

描述玻璃体内腺相关病毒(AAV)基因治疗引起的眼内免疫细胞浸润。

方法

将表达绿色荧光蛋白的质粒载体通过 AAV 注射到 AAV 未处理和 AAV 预处理的 C57Bl/6 小鼠的玻璃体内。使用光学相干断层扫描评估临床炎症。通过流式细胞术在玻璃体内注射后第 1、7 和 29 天识别和定量眼内免疫细胞群,并与假手术和对侧眼对照进行比较。

结果

与未注射的对侧眼和假手术对照组相比,AAV 注射眼的光学相干断层扫描炎症评分和总 CD45+细胞数显著升高。AAV 注射眼的临床明显炎症(光学相干断层扫描上的虹膜炎)和细胞炎症(CD45+细胞数)显著增加,并在第 7 天达到高峰。虹膜炎在第 29 天消退,但细胞炎症持续至第 29 天。在第 1 天,所有 AAV 注射眼的主要细胞群是中性粒细胞和活化的单核细胞。在第 7 天,暴露于 AAV 的动物的眼内有明显更多的树突状细胞和 T 细胞,而 AAV 未处理的动物的眼内则没有。到第 29 天,CD8-T 细胞是 AAV 注射眼内的主要 CD45+细胞群。

结论

在小鼠中玻璃体内注射 AAV 会引起明显的临床炎症,这种炎症是轻度的,似乎可以自发消退。然而,眼内总 CD45+细胞数量,特别是 T 细胞,仍然升高。无论先前的免疫状态如何,固有和适应性免疫细胞都会对玻璃体内 AAV 产生反应,但在 AAV 未处理的眼中,适应性反应会延迟。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/dd7e/7910624/054c0df22461/iovs-62-2-41-f001.jpg

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