单细胞分析血脑屏障对周细胞缺失的反应。
Single-Cell Analysis of Blood-Brain Barrier Response to Pericyte Loss.
机构信息
Department of Immunology, Genetics, and Pathology, Rudbeck Laboratory, Uppsala University, Sweden (M.A.M., L.H., S.N., E.V.-L., K.N., B.J., B.L., M.J., M.V., C.B.).
Neurosurgery, Tianjin Medical University General Hospital, Tianjin Neurological Institute, Key Laboratory of Post-Neuroinjury Neuro-Repair and Regeneration in Central Nervous System, Ministry of Education and Tianjin City, China (L.H.).
出版信息
Circ Res. 2021 Feb 19;128(4):e46-e62. doi: 10.1161/CIRCRESAHA.120.317473. Epub 2020 Dec 30.
RATIONALE
Pericytes are capillary mural cells playing a role in stabilizing newly formed blood vessels during development and tissue repair. Loss of pericytes has been described in several brain disorders, and genetically induced pericyte deficiency in the brain leads to increased macromolecular leakage across the blood-brain barrier (BBB). However, the molecular details of the endothelial response to pericyte deficiency remain elusive.
OBJECTIVE
To map the transcriptional changes in brain endothelial cells resulting from lack of pericyte contact at single-cell level and to correlate them with regional heterogeneities in BBB function and vascular phenotype.
METHODS AND RESULTS
We reveal transcriptional, morphological, and functional consequences of pericyte absence for brain endothelial cells using a combination of methodologies, including single-cell RNA sequencing, tracer analyses, and immunofluorescent detection of protein expression in pericyte-deficient adult mice. We find that endothelial cells without pericyte contact retain a general BBB-specific gene expression profile, however, they acquire a venous-shifted molecular pattern and become transformed regarding the expression of numerous growth factors and regulatory proteins. Adult brains display ongoing angiogenic sprouting without concomitant cell proliferation providing unique insights into the endothelial tip cell transcriptome. We also reveal heterogeneous modes of pericyte-deficient BBB impairment, where hotspot leakage sites display arteriolar-shifted identity and pinpoint putative BBB regulators. By testing the causal involvement of some of these using reverse genetics, we uncover a reinforcing role for angiopoietin 2 at the BBB.
CONCLUSIONS
By elucidating the complexity of endothelial response to pericyte deficiency at cellular resolution, our study provides insight into the importance of brain pericytes for endothelial arterio-venous zonation, angiogenic quiescence, and a limited set of BBB functions. The BBB-reinforcing role of ANGPT2 (angiopoietin 2) is paradoxical given its wider role as TIE2 (TEK receptor tyrosine kinase) receptor antagonist and may suggest a unique and context-dependent function of ANGPT2 in the brain.
背景
周细胞是毛细血管壁细胞,在发育和组织修复过程中对稳定新形成的血管起作用。在几种脑部疾病中已描述了周细胞的丢失,并且在大脑中遗传诱导的周细胞缺乏会导致血脑屏障(BBB)的大分子通透性增加。然而,内皮细胞对周细胞缺乏的分子反应细节仍不清楚。
目的
在单细胞水平上绘制因缺乏周细胞接触而导致的脑内皮细胞的转录变化,并将其与 BBB 功能和血管表型的区域异质性相关联。
方法和结果
我们使用包括单细胞 RNA 测序、示踪分析和周细胞缺失的成年小鼠中蛋白质表达的免疫荧光检测在内的多种方法,揭示了周细胞缺失对脑内皮细胞的转录、形态和功能后果。我们发现,没有周细胞接触的内皮细胞保留了一般的 BBB 特异性基因表达谱,但是它们获得了静脉移位的分子模式,并在许多生长因子和调节蛋白的表达方面发生了转化。成年 大脑显示出持续的血管生成发芽,而没有伴随的细胞增殖,这为内皮尖端细胞转录组提供了独特的见解。我们还揭示了周细胞缺失 BBB 损伤的异质模式,其中热点渗漏部位显示出小动脉移位的特征,并确定了潜在的 BBB 调节剂。通过使用反向遗传学测试其中一些的因果关系,我们揭示了血管生成素 2 在 BBB 中的增强作用。
结论
通过阐明内皮细胞对周细胞缺乏的反应在细胞分辨率下的复杂性,我们的研究深入了解了脑周细胞对内皮细胞动静脉分带、血管生成静止和一组有限的 BBB 功能的重要性。ANGPT2(血管生成素 2)的 BBB 增强作用是矛盾的,因为它作为 TIE2(TEK 受体酪氨酸激酶)受体拮抗剂的作用更广泛,这可能表明 ANGPT2 在大脑中具有独特和依赖于上下文的功能。
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