Kidins220-deficient hydrocephalus mice exhibit altered glial phenotypes and AQP4 differential regulation in the retina and optic nerve, with preserved retinal ganglion cell survival.

IF 6.2 1区医学 Q1 NEUROSCIENCES

Fluids and Barriers of the CNS Pub Date : 2025-02-12 DOI:10.1186/s12987-025-00626-z

Jose A Fernández-Albarral, Ana Simón-García, Elena Salobrar-García, Juan J Salazar, Celia López-Menéndez, Luis S M Pajuelo, Jose A Matamoros, Rosa de Hoz, Inés López-Cuenca, Lorena Elvira-Hurtado, Lidia Sanchez-Puebla, Marina P Sánchez-Carralero, Marina Sanz, José M Ramírez, Teresa Iglesias, Ana I Ramírez

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引用次数: 0

Abstract

Hydrocephalus, characterized by ventriculomegaly due to cerebrospinal fluid accumulation in the cerebral ventricles, is a co-morbidity factor in several neurodevelopmental, psychiatric and neurodegenerative diseases. Aquaporin-4 (AQP4) is crucial for brain water homeostasis, with Aqp4 knockout mice showing sporadic ventriculomegaly and increased brain water content. Kinase D interacting substrate of 220 kDa (Kidins220), a transmembrane protein involved in neuronal survival, synaptic activity and neurogenesis, controls AQP4 levels in ependymocytes and brain astrocytes. Indeed, Kidins220 deficiency in mice leads to hydrocephalus by downregulating VPS35, a key component of the retromer complex, and targeting AQP4 to lysosomal degradation. Importantly, the ependymal barrier of idiopathic normal pressure hydrocephalus patients shows a similar downregulation of KIDINS220 and AQP4. In addition, pathogenic variants in the KIDINS220 gene are linked to SINO syndrome, a rare disorder characterized by spastic paraplegia, intellectual disability, nystagmus, and obesity associated with hydrocephalus and ventriculomegaly. Given the retina's structural and functional similarities to the brain, we hypothesized that Kidins220 deficiency would affect retinal water regulation. However, the diminished expression of Kidins220 and VPS35 in the retina of Kidins220-deficient hydrocephalus mice, did not cause edema or downregulate AQP4 in Müller cells. Surprisingly, there was an increase in AQP4 levels within this glial cell population. Conversely, AQP4 expression in the optic nerve astrocytes was reduced, as observed in brain astrocytes, suggesting a distinctive adaptive response to hydrocephalus in Müller glia within the Kidins220-deficient retina. Furthermore, we observed phenotypic modifications in retinal glia in Kidins220-deficient hydrocephalus mice. However, we did not find any signs of neuronal damage in the retina. Future studies using OCT and OCTA in SINO syndrome patients with ventriculomegaly will be essential in elucidating the relationship between KIDINS220 pathogenic variants, retinal alterations, papilledema, and visual function.

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kidins220缺陷脑积水小鼠在视网膜和视神经中表现出神经胶质表型改变和AQP4差异调节，视网膜神经节细胞存活保留。

脑积水的特点是脑室内脑脊液积聚导致脑室肿大，是几种神经发育、精神和神经退行性疾病的合并症因素。水通道蛋白-4 （AQP4）对脑水稳态至关重要，AQP4敲除小鼠表现出散发性脑室增大和脑含水量增加。220 kDa的激酶D相互作用底物（Kidins220）是一种参与神经元存活、突触活性和神经发生的跨膜蛋白，控制室管膜细胞和脑星形胶质细胞中的AQP4水平。事实上，小鼠的Kidins220缺乏通过下调VPS35（逆转录物复合体的关键成分）和靶向AQP4溶酶体降解导致脑积水。重要的是，特发性常压脑积水患者的室管膜屏障显示类似的KIDINS220和AQP4下调。此外，KIDINS220基因的致病变异与SINO综合征有关，SINO综合征是一种罕见的疾病，以痉挛性截瘫、智力残疾、眼球震颤和脑积水和脑室肿大相关的肥胖为特征。鉴于视网膜的结构和功能与大脑相似，我们假设Kidins220缺乏会影响视网膜的水分调节。然而，在缺乏Kidins220的脑积水小鼠视网膜中，Kidins220和VPS35的表达减少并未引起水肿或降低 ller细胞中的AQP4。令人惊讶的是，在这个神经胶质细胞群中AQP4水平增加。相反，视神经星形胶质细胞中的AQP4表达降低，正如在脑星形胶质细胞中观察到的那样，这表明在kidins220缺失的视网膜中，神经胶质细胞对脑积水有独特的适应性反应。此外，我们在kidins220缺陷脑积水小鼠中观察到视网膜胶质细胞的表型改变。然而，我们没有在视网膜上发现任何神经元损伤的迹象。未来在脑室肿大的SINO综合征患者中使用OCT和OCTA的研究对于阐明KIDINS220致病变异、视网膜改变、乳头水肿和视觉功能之间的关系至关重要。

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来源期刊

Fluids and Barriers of the CNS Neuroscience-Developmental Neuroscience

CiteScore

10.70

自引率

8.20%

发文量

审稿时长

14 weeks

期刊介绍： "Fluids and Barriers of the CNS" is a scholarly open access journal that specializes in the intricate world of the central nervous system's fluids and barriers, which are pivotal for the health and well-being of the human body. This journal is a peer-reviewed platform that welcomes research manuscripts exploring the full spectrum of CNS fluids and barriers, with a particular focus on their roles in both health and disease. At the heart of this journal's interest is the cerebrospinal fluid (CSF), a vital fluid that circulates within the brain and spinal cord, playing a multifaceted role in the normal functioning of the brain and in various neurological conditions. The journal delves into the composition, circulation, and absorption of CSF, as well as its relationship with the parenchymal interstitial fluid and the neurovascular unit at the blood-brain barrier (BBB).