Ocular surface changes in mice with streptozotocin-induced diabetes and diabetic polyneuropathy

IF 5.9 1区 医学 Q1 OPHTHALMOLOGY Ocular Surface Pub Date : 2024-01-01 DOI:10.1016/j.jtos.2023.12.006
Martin Schicht , Jessica Farger , Saskia Wedel , Marco Sisignano , Klaus Scholich , Gerd Geisslinger , Natarajan Perumal , Franz H. Grus , Swati Singh , Afsun Sahin , Friedrich Paulsen , Elke Lütjen-Drecoll
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Abstract

Purpose

Diabetes mellitus (DM) is a leading risk factor for corneal neuropathy and dry eye disease (DED). Another common consequence of DM is diabetic peripheral polyneuropathy (DPN). Both complications affect around 50 % of the DM patients but the relationship between DM, DED and DPN remains unclear.

Methods

In this study, we examined mice with early onset of DM and PN after streptozotocin (STZ)-induced diabetes (DPN). We compared the early morphological changes of the sciatic nerve, dorsal root and trigeminal ganglia with the changes in the ocular surface, including tear proteomic and we also investigated respective changes in the gene expressions and morphological alterations in the eye tissues involved in tear production.

Results

The lacrimal gland, conjunctival goblet cells and cornea showed morphological changes along with alterations in tear proteins without any obvious signs of ocular surface inflammation. The gene expression for respectively altered tear proteins i.e., of Clusterin in cornea, Car6, Adh3a1, and Eef1a1 in eyelids, and Pigr in the lacrimal gland also showed significant changes compared to control mice. In the trigeminal ganglia like in the dorsal root ganglia neuronal cells showed swollen mitochondria and, in the latter, there was a significant increase of NADPH oxidases and MMP9 suggestive of oxidative and neuronal stress. In the dorsal root ganglia and the sciatic nerve, there was an upregulation of a number of pro-inflammatory cytokines and pain-mediating chemokines.

Conclusion

The early ocular changes in DM Mice only affect the lacrimal gland. Which, is reflected in the tear film composition of DPN mice. Due to the high protein concentration in tear fluid in humans, proteomic analysis in addition to noninvasive investigation of goblet cells and cornea can serve as a tools for the early diagnosis of DPN, DED in clinical practice. Early treatment could delay or even prevent the ocular complications of DM such as DED and PN.

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链脲佐菌素诱发糖尿病和糖尿病多发性神经病变小鼠眼表的变化
目的糖尿病(DM)是角膜神经病变和干眼症(DED)的主要危险因素。糖尿病的另一个常见后果是糖尿病周围多发性神经病变(DPN)。这两种并发症影响了约 50% 的 DM 患者,但 DM、DED 和 DPN 之间的关系仍不清楚。方法在这项研究中,我们观察了链脲佐菌素(STZ)诱导糖尿病(DPN)后早期发病的 DM 和 PN 小鼠。我们将坐骨神经、背根和三叉神经节的早期形态学变化与眼表的变化(包括泪液蛋白组)进行了比较,并研究了参与泪液生成的眼部组织的基因表达和形态学变化。与对照组小鼠相比,泪液蛋白改变的基因表达,即角膜中的 Clusterin、眼睑中的 Car6、Adh3a1 和 Eef1a1 以及泪腺中的 Pigr 也发生了显著变化。三叉神经节和背根神经节的神经细胞一样,线粒体肿胀,后者的 NADPH 氧化酶和 MMP9 显著增加,表明存在氧化和神经元应激反应。在背根神经节和坐骨神经中,一些促炎细胞因子和介导疼痛的趋化因子上调。DPN小鼠的泪膜成分反映了这一点。由于人类泪液中蛋白质浓度较高,蛋白质组分析以及对腺泡细胞和角膜的无创检查可作为临床实践中早期诊断 DPN 和 DED 的工具。早期治疗可以延缓甚至预防DM的眼部并发症,如DED和PN。
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来源期刊
Ocular Surface
Ocular Surface 医学-眼科学
CiteScore
11.60
自引率
14.10%
发文量
97
审稿时长
39 days
期刊介绍: The Ocular Surface, a quarterly, a peer-reviewed journal, is an authoritative resource that integrates and interprets major findings in diverse fields related to the ocular surface, including ophthalmology, optometry, genetics, molecular biology, pharmacology, immunology, infectious disease, and epidemiology. Its critical review articles cover the most current knowledge on medical and surgical management of ocular surface pathology, new understandings of ocular surface physiology, the meaning of recent discoveries on how the ocular surface responds to injury and disease, and updates on drug and device development. The journal also publishes select original research reports and articles describing cutting-edge techniques and technology in the field. Benefits to authors We also provide many author benefits, such as free PDFs, a liberal copyright policy, special discounts on Elsevier publications and much more. Please click here for more information on our author services. Please see our Guide for Authors for information on article submission. If you require any further information or help, please visit our Support Center
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