Zhou Lan, Lin Dongyue, Xu Guihua, Wang Xiaoyi, Chen Zilin, Wang Dingding, Fan Huiya
Ophthalmological Center of Huizhou Central People's Hospital, Huizhou, Guangdong, China.
State Key Laboratory of Ophthalmology, Zhongshan Ophthalmic Center, Sun Yat-sen University, Guangzhou, Guangdong, China.
Front Neurol. 2023 Mar 22;14:1091697. doi: 10.3389/fneur.2023.1091697. eCollection 2023.
Retinal ganglion cells (RGCs) axon loss at the site of optic nerve head (ONH) is long believed as the common pathology in glaucoma since different types of glaucoma possessing different characteristic of intraocular pressure, and this damage was only detected at the later stage.
To address these disputes and detect early initiating events underlying RGCs, we firstly detected somatic or axonal change and compared their difference in acute and chronic phase of primary angle-closed glaucoma (PACG) patient using optical coherence tomography (OCT), then an axonal-enriched cytoskeletal protein neurofilament heavy chain and its phosphoforms (NF-H, pNF-H) were utilized to reveal spatio-temporal undetectable damage insulted by acute and chronic ocular hypertension (AOH, COH) in two well characterized glaucoma mice models.
In clinic, we detected nonhomogeneous changes such as ONH and soma of RGCs presenting edema in acute phase but atrophy in chronic one by OCT. In AOH animal models, an increase expression of NF-H especially its phosphorylation modification was observed as early as 4 h before RGCs loss, which presented as somatic accumulation in the peripheral retina and at the sites of ONH. In contrast, in microbeads induced COH model, NF-H and pNF-H reduced significantly, these changes firstly occurred as NF-H or pNF-H disconnection at ONH and optic nerve after 2 weeks when the intraocular pressure reaching the peak; Meanwhile, we detected aqueous humor pNF-H elevation after AOH and slight reduction in the COH.
Together, our data supports that early alteration of NF-H and its phosphoforms would reveal undetectable subcellular damage consisting of peripheral somatic neurofilament compaction, impaired axonal transport and distal axonal disorganization of cytoskeleton beyond the ONH, and identifies two distinct axonal degeneration which were Wallerian combination with retrograde degeneration in acute PACG and retrograde degeneration in the chronic one.
长期以来,人们一直认为视网膜神经节细胞(RGCs)在视神经乳头(ONH)部位的轴突丢失是青光眼的常见病理特征,因为不同类型的青光眼具有不同的眼压特征,而这种损伤仅在疾病后期才能检测到。
为了解决这些争议并检测RGCs早期起始事件,我们首先使用光学相干断层扫描(OCT)检测原发性闭角型青光眼(PACG)患者急性期和慢性期RGCs的体细胞或轴突变化,并比较两者差异。然后,利用轴突富集的细胞骨架蛋白神经丝重链及其磷酸化形式(NF-H,pNF-H),揭示两种特征明确的青光眼小鼠模型中急性和慢性高眼压(AOH,COH)引起的时空不可检测的损伤。
在临床研究中,我们通过OCT检测到RGCs的ONH和体细胞存在非均匀变化,急性期表现为水肿,慢性期则表现为萎缩。在AOH动物模型中,早在RGCs丢失前4小时就观察到NF-H表达增加,尤其是其磷酸化修饰增加,表现为外周视网膜和ONH部位的体细胞积聚。相比之下,在微珠诱导的COH模型中,NF-H和pNF-H显著降低,这些变化在眼压达到峰值2周后首先表现为ONH和视神经处的NF-H或pNF-H断开连接;同时,我们检测到AOH后房水pNF-H升高,COH后则略有降低。
总之,我们的数据支持,NF-H及其磷酸化形式的早期改变将揭示不可检测的亚细胞损伤,包括外周体细胞神经丝压缩、轴突运输受损以及ONH以外的远端轴突细胞骨架紊乱,并确定了两种不同的轴突变性,即急性PACG中的华勒氏合并逆行变性和慢性PACG中的逆行变性。
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