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Neuronal guidance signaling in neurodegenerative diseases:Key regulators that function at neuron-glia and neuroimmune interfaces

摘要The nervous system processes a vast amount of information,performing computations that underlie perception,cognition,and behavior.During development,neuronal guidance genes,which encode extracellular cues,their receptors,and downstream signal transducers,organize neural wiring to generate the complex architecture of the nervous system.It is now evident that many of these neuroguidance cues and their receptors are active during development and are also expressed in the adult nervous system.This suggests that neuronal guidance pathways are critical not only for neural wiring but also for ongoing function and maintenance of the mature nervous system.Supporting this view,these pathways continue to regulate synaptic connectivity,plasticity,and remodeling,and overall brain homeostasis throughout adulthood.Genetic and transcriptomic analyses have further revealed many neuronal guidance genes to be associated with a wide range of neurodegenerative and neuropsychiatric disorders.Although the precise mechanisms by which aberrant neuronal guidance signaling drives the pathogenesis of these diseases remain to be clarified,emerging evidence points to several common themes,including dysfunction in neurons,microglia,astrocytes,and endothelial cells,along with dysregulation of neuron-microglia-astrocyte,neuroimmune,and neurovascular interactions.In this review,we explore recent advances in understanding the molecular and cellular mechanisms by which aberrant neuronal guidance signaling contributes to disease pathogenesis through altered cell-cell interactions.For instance,recent studies have unveiled two distinct semaphorin-plexin signaling pathways that affect microglial activation and neuroinflammation.We discuss the challenges ahead,along with the therapeutic potentials of targeting neuronal guidance pathways for treating neurodegenerative diseases.Particular focus is placed on how neuronal guidance mechanisms control neuron-glia and neuroimmune interactions and modulate microglial function under physiological and pathological conditions.Specifically,we examine the crosstalk between neuronal guidance signaling and TREM2,a master regulator of microglial function,in the context of pathogenic protein aggregates.It is well-established that age is a major risk factor for neurodegeneration.Future research should address how aging and neuronal guidance signaling interact to influence an individual's susceptibility to various late-onset neurological diseases and how the progression of these diseases could be therapeutically blocked by targeting neuronal guidance pathways.

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作者 Junichi Yuasa-Kawada [1] Mariko Kinoshita-Kawada [1] Masaki Hiramoto [2] Satoru Yamagishi [3] Takayasu Mishima [4] Shin'ichiro Yasunaga [5] Yoshio Tsuboi [1] Nobutaka Hattori [1] Jane Y.Wu [6] 学术成果认领
作者单位 Department of Neurology,Juntendo University Faculty of Medicine,Tokyo,Japan [1] The Scripps Research Institute,La Jolla,CA,USA [2] Department of Optical Neuroanatomy,Institute of Photonics Medicine,Hamamatsu University School of Medicine,Hamamatsu,Japan [3] Division of Neurology,Department of Internal Medicine,Sakura Medical Center,Toho University,Sakura,Japan [4] Department of Biochemistry,Fukuoka University Faculty of Medicine,Fukuoka,Japan [5] Department of Neurology,Center for Genetic Medicine,Lurie Cancer Center,Northwestern University Feinberg School of Medicine,Chicago,IL,USA [6]
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DOI 10.4103/NRR.NRR-D-24-01330
发布时间 2025-12-09(万方平台首次上网日期,不代表论文的发表时间)
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中国神经再生研究(英文版)

中国神经再生研究(英文版)

2026年21卷2期

612-635页

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