眨眼睛。

C. Karson
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引用次数: 17

摘要

自发眨眼频率受起源于PPRF的一个可定义的神经系统控制,该神经系统受SN和上丘的促进调节和小脑和枕皮质的抑制调节。丘脑也可能参与其中,但其影响的结果尚不清楚。当自发眨眼频率增加时,反射性眨眼往往会减少,反之亦然。反射的解剖学控制主要在脑桥被尾侧和中脑吻侧的结构中。然而,SN和小脑等调节眨眼频率的结构也调节反射性眨眼。神经药理实验确定的神经化学控制是由脑干的多巴胺能、胆碱能和gaba能系统发挥作用的。多巴胺活性与眨眼频率直接相关,而其他两种相关神经递质系统的激动作用可能抑制眨眼频率。中枢神经系统疾病的临床应用目前仅限于帕金森病、精神分裂症和自闭症。在前一种疾病中,眨眼次数减少意味着疾病的恶化,而在接受多巴胺激动剂治疗的患者中,眨眼次数的显著增加可能是激动剂诱发的运动障碍的前兆。在精神分裂症患者中,眨眼频率的增加,即使是在未接受药物治疗的受试者中,也可能表明调节眨眼的结构受到了影响。这一点很重要,因为这些结构很少被认为是精神分裂症的潜在病理生理输入位点。类似的考虑也适用于自闭症,除了频繁眨眼更明显地将这种疾病与其他形式的发育迟缓区分开来。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Blinking.
Spontaneous blink rates are controlled by a definable neural system originating in PPRF with facilitatory modulation from SN and superior colliculus and inhibitory modulation provided by cerebellum and occipital cortex. The thalamus may also be involved but the result of its influence is not clear. Reflex blinking is often reduced when spontaneous blink rate is increased and the reverse applies as well. The anatomic control of reflex is primarily in structures in the caudal half of pontine tegmentum and rostral midbrain. However, SN and cerebellum and other structures that regulate blink rate also modulate reflex blinking. Neurochemical control as determined by neuropharmacological experiments is exerted by dopaminergic, cholinergic and GABAergic systems of brain stem. Dopamine activity correlates directly with blink rate whereas agonism of the other two relevant neurotransmitter systems may inhibit blink rate. Clinical implications in central nervous system disease are currently restricted to Parkinson's disease, schizophrenia and autism. In the former illness, reduced blink rate signifies a worsening of the illness and a significant increase in blink rate in patients treated with dopamine agonist may be a harbinger of agonist-induced dyskinesia. In schizophrenia, increased blink rate, even in medication-naive subjects, may signify involvement of the structures that regulate blinking. This is important because these structures are rarely invoked as sites of potential pathophysiological import in schizophrenia. Similar considerations apply to autism except that increased blinking more clearly differentiates this disorder from other forms of retardation.
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