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迈向共学互学的未来:当前隔代学习研究的知识图景 被引量:7
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作者 程豪 吕珂漪 李家成 《中国远程教育》 CSSCI 2022年第10期48-57,共10页
为应对人口老龄化带来的严峻挑战,加快终身学习的时代步伐,促进青少年的健康发展,世界各国逐渐将隔代学习提上日程。本文基于国内外隔代学习研究的动态,试图呈现隔代学习的发生与发展机制。积极老龄化的愿景、隔代关系的疏离与冲突以及... 为应对人口老龄化带来的严峻挑战,加快终身学习的时代步伐,促进青少年的健康发展,世界各国逐渐将隔代学习提上日程。本文基于国内外隔代学习研究的动态,试图呈现隔代学习的发生与发展机制。积极老龄化的愿景、隔代关系的疏离与冲突以及隔代学习的功能,催生了隔代学习,其具体表现为知识传递、交往方式和日常生活三种内涵。从目标指向来看,隔代学习聚焦于老年人的丰富生活、青少年的健康发展和隔代关系的积极建构。在隔代学习场域、方式和内容的交互作用下,隔代学习助力隔代主体的互惠共生、促进家庭和谐和社区可持续发展、实现积极老龄化和和谐社会的建设。 展开更多
关键词 学习型社会 隔代学习 终身学习 老年学习 老年大学 隔代关系 人口老龄化 积极老龄化
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Actin polymerization inhibition by targeting ARPC2 affects intestinal stem cell homeostasis 被引量:1
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作者 Ruzhen Zhang Sheng Chen +9 位作者 Zhifan Yang Ning Zhang Kenan Guo keyi lv Zimo Zhou Meijiao Gao Xiancheng Hu Yongping Su Jianming He Fengchao Wang 《Burns & Trauma》 SCIE 2023年第1期709-721,共13页
Background:The rapid turnover of the intestinal epithelium is driven by the proliferation and differentiation of intestinal stem cells(ISCs).The dynamics of the F-actin cytoskeleton are critical for maintaining interc... Background:The rapid turnover of the intestinal epithelium is driven by the proliferation and differentiation of intestinal stem cells(ISCs).The dynamics of the F-actin cytoskeleton are critical for maintaining intercellular force and the signal transduction network.However,it remains unclear how direct interference with actin polymerization impacts ISC homeostasis.This study aims to reveal the regulatory effects of the F-actin cytoskeleton on the homeostasis of intestinal epithelium,as well as the potential risks of benproperine(BPP)as an anti-tumor drug.Methods:Phalloidin fluorescence staining was utilized to test F-actin polymerization.Flow cytom-etry and IHC staining were employed to discriminate different types of intestinal epithelial cells.Cell proliferation was assessed through bromo-deoxyuridine(BrdU)and 5-ethynyl-2-deoxyuridine(EdU)incorporation assays.The proliferation and differentiation of intestinal stem cells were replicated in vitro through organoid culture.Epithelial migrationwas evaluated through BrdU pulse labeling and chasing in mice.Results:The F-actin content was observed to significantly increase as crypt cells migrated into the villus region.Additionally,actin polymerization in secretory cells,especially in Paneth cells(PCs),was much higher than that in neighboring ISCs.Treatment with the newly identified actin-related protein 2/3 complex subunit 2(ARPC2)inhibitor BPP led to a dose-dependent increase or inhibition of intestinal organoid growth in vitro and crypt cell proliferation in vivo.Compared with the vehicle group,BPP treatment decreased the expression of Lgr5 ISC feature genes in vivo and in organoid culture.Meanwhile,PC differentiation derived from ISCs and progenitors was decreased by inhibition of F-actin polymerization.Mechanistically,BPP-induced actin polymerization inhibition may activate the Yes1-associated transcriptional regulator pathway,which affects ISC proliferation and differentiation.Accordingly,BPP treatment affected intestinal epithelial cell migration in a dose-dependent manner.Conclusion:Our findings indicate that the regulation of cytoskeleton reorganization can affect ISC homeostasis.In addition,inhibiting ARPC2 with the Food and Drug Administration-approved drug BPP represents a novel approach to influencing the turnover of intestinal epithelial cells. 展开更多
关键词 F-ACTIN BENPROPERINE ARPC2 Intestinal stem cell YAP
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