视神经病变相关蛋白基因突变对 Parkin 依赖性线粒体自噬的影响有限。

Glaucoma-Associated Mutations in the Optineurin Gene Have Limited Impact on Parkin-Dependent Mitophagy.

机构信息

Department of Cellular Physiology, Niigata University Graduate School of Medical and Dental Sciences, Niigata, Japan.

Department of Ophthalmology, Niigata University Graduate School of Medical and Dental Sciences, Niigata, Japan.

出版信息

Invest Ophthalmol Vis Sci. 2019 Aug 1;60(10):3625-3635. doi: 10.1167/iovs.19-27184.

DOI:10.1167/iovs.19-27184

PMID:31469402

Abstract

PURPOSE

Glaucoma results in progressive degeneration of the optic nerve and irreversible vision loss. Several mutations in the gene encoding optineurin (OPTN), the receptor for Parkin-dependent mitochondrial autophagy (mitophagy), are associated with glaucoma and amyotrophic lateral sclerosis (ALS). ALS mutations in the ubiquitin-binding domain of OPTN impair Parkin-dependent mitophagy. However, the effects of glaucoma mutations in this region remain unknown. We examined the impact of glaucoma-associated OPTN mutations on Parkin-dependent mitophagy.

METHODS

The mitochondria-localized, pH-sensitive fluorescent protein mito-Keima was used to monitor mitophagy. HeLa cells expressing Parkin were treated with carbonyl cyanide 3-chlorophenylhydrazone (CCCP) or oligomycin/antimycin A (O/A) to induce Parkin-dependent mitophagy. Two complementary mitophagy receptors, OPTN and NDP52, were deleted in HeLa cells expressing mito-Keima and Parkin (DKO_HeLa). The mutant OPTN genes were re-introduced into DKO_HeLa cells using retroviruses or through transfection. Mitophagy activity and OPTN localization were evaluated via microscopic analyses. OPTN binding to ubiquitin was examined using an immunoprecipitation assay.

RESULTS

Parkin-dependent mitophagy was inhibited in DKO_HeLa cells. Introduction of two glaucoma mutations in the ubiquitin-interacting region of OPTN restored mitophagy in CCCP-treated DKO_HeLa cells, whereas the two ALS mutations failed to replicate this effect. Under treatment with CCCP, the two glaucoma-mutant OPTN proteins normally translocated to mitochondria and bound to ubiquitinated proteins. Furthermore, five additional glaucoma-mutant OPTN proteins restored CCCP-induced mitophagy. Moreover, treatment with O/A exhibited similar results.

CONCLUSIONS

Glaucoma-mutant OPTN proteins retain their normal properties as mitophagy receptors, suggesting that mutations in the OPTN gene cause glaucoma through a mechanism independent of mitophagy defects.

摘要

目的

青光眼导致视神经进行性退化和不可逆转的视力丧失。几种编码 optineurin（OPTN）的基因突变与青光眼和肌萎缩侧索硬化症（ALS）有关，OPTN 是 Parkin 依赖性线粒体自噬（mitophagy）的受体。OPTN 泛素结合结构域中的 ALS 突变会损害 Parkin 依赖性的线粒体自噬。然而，该区域的青光眼突变的影响仍不清楚。我们研究了青光眼相关 OPTN 突变对 Parkin 依赖性线粒体自噬的影响。

方法

使用定位于线粒体的、pH 敏感的荧光蛋白 mito-Keima 监测线粒体自噬。用羰基氰化物 3-氯苯腙（CCCP）或寡霉素/抗霉素 A（O/A）处理表达 Parkin 的 HeLa 细胞，诱导 Parkin 依赖性线粒体自噬。在表达 mito-Keima 和 Parkin 的 HeLa 细胞（DKO_HeLa）中，两种互补的线粒体自噬受体 OPTN 和 NDP52 被删除。使用逆转录病毒或转染将突变 OPTN 基因重新引入 DKO_HeLa 细胞。通过显微镜分析评估线粒体自噬活性和 OPTN 定位。使用免疫沉淀测定检查 OPTN 与泛素的结合。

结果

Parkin 依赖性线粒体自噬在 DKO_HeLa 细胞中受到抑制。在 OPTN 的泛素相互作用区域引入两种青光眼突变可恢复 CCCP 处理的 DKO_HeLa 细胞中的线粒体自噬，而两种 ALS 突变则未能复制这种效果。在 CCCP 处理下，两种青光眼突变 OPTN 蛋白正常转位到线粒体并与泛素化蛋白结合。此外，另外五种青光眼突变 OPTN 蛋白恢复了 CCCP 诱导的线粒体自噬。此外，O/A 处理也得到了类似的结果。