摘要
Background Low-intensity focused ultrasound stimulation(LIFUS)has been developed to enhance neurological repair and remodelling during the late acute stage of ischaemic stroke in rodents.However,the cellular and molecular mechanisms of neurological repair and remodelling after LIFUS in ischaemic stroke are unclear.Methods Ultrasound stimulation was treated in adult male mice 7 days after transient middle cerebral artery occlusion.Angiogenesis was measured by laser speckle imaging and histological analyses.Electromyography and fibre photometry records were used for synaptogenesis.Brain atrophy volume and neurobehaviour were assessed 0–14 days after ischaemia.iTRAQ proteomic analysis was performed to explore the differentially expressed protein.scRNA-seq was used for subcluster analysis of astrocytes.Fluorescence in situ hybridisation and Western blot detected the expression of HMGB1 and CAMK2N1.Results Optimal ultrasound stimulation increased cerebral blood flow,and improved neurobehavioural outcomes in ischaemic mice(p<0.05).iTRAQ proteomic analysis revealed that the expression of HMGB1 increased and CAMK2N1 decreased in the ipsilateral hemisphere of the brain at 14 days after focal cerebral ischaemia with ultrasound treatment(p<0.05).scRNA-seq revealed that this expression pattern belonged to a subcluster of astrocytes after LIFUS in the ischaemic brain.LIFUS upregulated HMGB1 expression,accompanied by VEGFA elevation compared with the control group(p<0.05).Inhibition of HMGB1 expression in astrocytes decreased microvessels counts and cerebral blood flow(p<0.05).LIFUS reduced CAMK2N1 expression level,accompanied by increased extracellular calcium ions and glutamatergic synapses(p<0.05).CAMK2N1 overexpression in astrocytes decreased dendritic spines,and aggravated neurobehavioural outcomes(p<0.05).Conclusion Our results demonstrated that LIFUS promoted angiogenesis and synaptogenesis after focal cerebral ischaemia by upregulating HMGB1 and downregulating CAMK2N1 in a subcluster of astrocytes,suggesting that LIFUS activated specific astrocyte subcluster could be a key target for ischaemic brain therapy.
基金
Scientific Research and Innovation Program of Shanghai Education Commission 2019-01-07-00-02-E00064(G-YY)
National Natural Science Foundation of China 82271320(ZZ),82172529(WJ),81974179(ZZ),82071284(YT)
Scientific and Technological Innovation Act Program of Shanghai Science and Technology Commission,20JC1411900(G-YY)
National Key R&D Program of China 2022YFA1603604(ZZ),2019YFA0112000(YT),2018YFA0701400(WQ)and 2021ZD0200401(WQ)
Shenzhen Foundation Grant JCYJ20200109114237902(WQ),SGDX2020110309400200(WQ).
