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视网膜神经血管单元的层特异性解剖学和生理学特征。

Layer-specific anatomical and physiological features of the retina's neurovascular unit.

作者信息

Grimes William N, Berson David M, Sabnis Adit, Hoon Mrinalini, Sinha Raunak, Tian Hua, Diamond Jeffrey S

机构信息

Synaptic Physiology Section, National Institute of Neurological Disorder and Stroke, National Institutes of Health, Bethesda, MD 20814, USA.

Department of Neuroscience, Brown University, Providence, RI 02912, USA.

出版信息

Curr Biol. 2025 Jan 6;35(1):109-120.e4. doi: 10.1016/j.cub.2024.11.023. Epub 2024 Dec 16.

Abstract

The neurovascular unit (NVU), comprising vascular, glial, and neural elements, supports the energetic demands of neural computation, but this aspect of the retina's trilaminar vessel network is poorly understood. Only the innermost vessel layer-the superficial vascular plexus (SVP)-is associated with astrocytes, like brain capillaries, whereas radial Müller glia interact with vessels in the other layers. Using serial electron microscopic reconstructions from mouse and primate retina, we find that Müller processes cover capillaries in a tessellating pattern, mirroring the wrapping of brain capillaries by tiled astrocytic endfeet. Gaps in the Müller sheath, found mainly in the intermediate vascular plexus (IVP), permit diverse neuron types to contact pericytes and the endothelial cells directly. Pericyte somata are a favored target, often at spine-like structures with reduced or absent vascular basement lamina. Focal application of ATP to the vitreal surface evoked Ca signals in Müller sheaths in all three vascular layers. Pharmacological experiments confirmed that Müller sheaths express purinergic receptors that, when activated, trigger intracellular Ca signals that are amplified by inositol triphosphate (IP)-controlled intracellular Ca stores. When rod photoreceptors die in a mouse model of retinitis pigmentosa (rd10), Müller sheaths dissociate from the deep vascular plexus (DVP) but are largely unchanged within the IVP or SVP. Thus, Müller glia interact with retinal vessels in a laminar, compartmentalized manner: glial sheaths are virtually complete in the SVP but fenestrated in the IVP, permitting direct neurovascular contacts. In the DVP, the glial sheath is only modestly fenestrated and is vulnerable to photoreceptor degeneration.

摘要

神经血管单元(NVU)由血管、神经胶质和神经成分组成,支持神经计算的能量需求,但视网膜三层血管网络的这一方面却鲜为人知。只有最内层的血管层——浅表血管丛(SVP)——与星形胶质细胞相关联,就像脑毛细血管一样,而放射状的米勒胶质细胞与其他层的血管相互作用。通过对小鼠和灵长类动物视网膜进行连续电子显微镜重建,我们发现米勒细胞的突起以镶嵌模式覆盖毛细血管,这与星形胶质细胞终足平铺包裹脑毛细血管的方式相似。米勒胶质鞘中的间隙主要存在于中间血管丛(IVP)中,允许不同类型的神经元直接接触周细胞和内皮细胞。周细胞胞体是一个受青睐的靶点,通常位于血管基底膜减少或缺失的棘状结构处。将ATP局部应用于玻璃体表面可在所有三个血管层的米勒胶质鞘中诱发钙信号。药理学实验证实,米勒胶质鞘表达嘌呤能受体,当这些受体被激活时,会触发细胞内钙信号,这些信号会被三磷酸肌醇(IP)控制的细胞内钙库放大。在视网膜色素变性(rd10)小鼠模型中,当视杆光感受器死亡时,米勒胶质鞘会与深层血管丛(DVP)分离,但在IVP或SVP内基本保持不变。因此,米勒胶质细胞以分层、分区的方式与视网膜血管相互作用:胶质鞘在SVP中几乎是完整的,但在IVP中有窗孔,允许直接的神经血管接触。在DVP中,胶质鞘只有适度的窗孔,并且容易受到光感受器变性的影响。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5420/11867051/cf6261705f33/nihms-2041803-f0001.jpg

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