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脉络丛细胞外囊泡将血液中胰岛素样生长因子1转运至未成熟大脑的海马体。

Choroid plexus extracellular vesicle transport of blood-borne insulin-like growth factor 1 to the hippocampus of the immature brain.

作者信息

Ortenlöf Niklas, Vallius Suvi, Karlsson Helena, Ekström Claes, Kristiansson Amanda, Holmqvist Bo, Pankratova Stanislava, Barton Norman, Ley David, Gram Magnus

机构信息

Department of Clinical Sciences Lund, Pediatrics, Lund University, 22184 Lund, Sweden.

Department of Neonatology, Skåne University Hospital, 22184 Lund, Sweden.

出版信息

PNAS Nexus. 2024 Nov 12;3(12):pgae496. doi: 10.1093/pnasnexus/pgae496. eCollection 2024 Dec.

Abstract

Reduced serum level of insulin-like growth factor 1 (IGF-1), a major regulator of perinatal development, in extremely preterm infants has been shown to be associated with neurodevelopmental impairment. To clarify the mechanism of IGF-1 transport at the blood-cerebrospinal fluid (CSF) barrier of the immature brain, we combined studies of in vivo preterm piglet and rabbit models with an in vitro transwell cell culture model of neonatal primary murine choroid plexus epithelial (ChPE) cells. We identified IGF-1-positive intracellular vesicles in ChPE cells and provided data indicating a directional transport of IGF-1 from the basolateral to the apical media in extracellular vesicles (EVs). Exposure of the ChPE cells to human IGF-1 on the basolateral side increased the secretion of IGF-1-positive EVs in the apical media. Mass spectrometry analysis displayed similarities in protein content between EVs derived from preterm piglet CSF-derived and ChPE cell-derived EVs. Furthermore, exposure of ChPE cells to human IGF-1 caused an enrichment of human IGF-1 and transmembrane p24 trafficking protein 2, proteins important for perinatal development, in apical media-derived EVs. Moreover, intraventricular injections of ChPE cell-derived EVs in preterm rabbit pups resulted in an uptake of EVs in the brain, displaying penetration through the ependymal lining and deep into the hippocampus. Finally, exposure of rat hippocampus neurons to ChPE cell-derived EVs resulted in internalization of the EVs in hippocampal soma and neurites. In summary, we describe a transport pathway for blood-borne IGF-1 in EVs through the blood-CSF barrier to the hippocampus in the immature brain.

摘要

胰岛素样生长因子1(IGF-1)是围产期发育的主要调节因子,极低出生体重儿血清中IGF-1水平降低与神经发育障碍有关。为了阐明未成熟脑血脑屏障(CSF)处IGF-1的转运机制,我们将体内早产仔猪和家兔模型的研究与新生小鼠原代脉络丛上皮(ChPE)细胞的体外Transwell细胞培养模型相结合。我们在ChPE细胞中鉴定出IGF-1阳性细胞内囊泡,并提供数据表明IGF-1在细胞外囊泡(EVs)中从基底外侧向顶侧培养基定向转运。将ChPE细胞基底外侧暴露于人IGF-1可增加顶侧培养基中IGF-1阳性EVs的分泌。质谱分析显示,早产仔猪脑脊液来源的EVs和ChPE细胞来源的EVs在蛋白质含量上具有相似性。此外,将ChPE细胞暴露于人IGF-1会导致顶侧培养基来源的EVs中富含人IGF-1和跨膜p24转运蛋白2,这两种蛋白对围产期发育很重要。此外,向早产家兔幼崽脑室内注射ChPE细胞来源的EVs会导致脑内EVs的摄取,显示其穿过室管膜内衬并深入海马体。最后,将大鼠海马神经元暴露于ChPE细胞来源的EVs会导致EVs在海马体细胞体和神经突内化。总之,我们描述了一种血源性IGF-1通过血脑屏障在EVs中转运至未成熟脑海马体的途径。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a319/11630522/654e5335608b/pgae496f1.jpg

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