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大脑和咽反应与老年患者口咽吞咽困难的药物治疗相关。

Brain and Pharyngeal Responses Associated with Pharmacological Treatments for Oropharyngeal Dysphagia in Older Patients.

机构信息

Gastrointestinal Physiology Laboratory, Hospital de Mataró, Consorci Sanitari del Maresme, Mataró, Spain.

Centro de Investigación Biomédica en Red de Enfermedades Hepáticas y Digestivas (CIBERehd), Madrid, Spain.

出版信息

Dysphagia. 2023 Dec;38(6):1449-1466. doi: 10.1007/s00455-023-10578-x. Epub 2023 May 5.

Abstract

Impaired pharyngo-laryngeal sensory function is a critical mechanism for oropharyngeal dysphagia (OD). Discovery of the TRP family in sensory nerves opens a window for new active treatments for OD. To summarize our experience of the action mechanism and therapeutic effects of pharyngeal sensory stimulation by TRPV1, TRPA1 and TRPM8 agonists in older patients with OD. Summary of our studies on location and expression of TRP in the human oropharynx and larynx, and clinical trials with acute and after 2 weeks of treatment with TRP agonists in older patients with OD. (1) TRP receptors are widely expressed in the human oropharynx and larynx: TRPV1 was localized in epithelial cells and TRPV1, TRPA1 and TRPM8 in sensory fibers mainly below the basal lamina. (2) Older people present a decline in pharyngeal sensory function, more severe in patients with OD associated with delayed swallow response, impaired airway protection and reduced spontaneous swallowing frequency. (3) Acute stimulation with TRP agonists improved the biomechanics and neurophysiology of swallowing in older patients with OD TRPV1 = TRPA1 > TRPM8. (4) After 2 weeks of treatment, TRPV1 agonists induced cortical changes that correlated with improvements in swallowing biomechanics. TRP agonists are well tolerated and do not induce any major adverse events. TRP receptors are widely expressed in the human oropharynx and larynx with specific patterns. Acute oropharyngeal sensory stimulation with TRP agonists improved neurophysiology, biomechanics of swallow response, and safety of swallowing. Subacute stimulation promotes brain plasticity further improving swallow function in older people with OD.

摘要

咽-喉感觉功能障碍是口咽吞咽障碍(OD)的一个关键机制。感觉神经中 TRP 家族的发现为 OD 的新主动治疗开辟了一扇窗。总结我们在 OD 老年患者中使用 TRPV1、TRPA1 和 TRPM8 激动剂刺激咽感觉的作用机制和治疗效果的经验。总结我们在人类口咽和喉中 TRP 位置和表达的研究,以及在 OD 老年患者中进行的急性和治疗 2 周后使用 TRP 激动剂的临床试验。(1)TRP 受体在人类口咽和喉中广泛表达:TRPV1 定位于上皮细胞,TRPV1、TRPA1 和 TRPM8 定位于基底膜以下的感觉纤维中。(2)老年人咽感觉功能下降,OD 患者下降更明显,与吞咽反应延迟、气道保护受损和自发吞咽频率降低有关。(3)TRP 激动剂急性刺激改善 OD 老年患者的吞咽生物力学和神经生理学:TRPV1=TRPA1>TRPM8。(4)治疗 2 周后,TRPV1 激动剂诱导的皮质变化与吞咽生物力学的改善相关。TRP 激动剂耐受性良好,不会引起任何重大不良事件。TRP 受体在人类口咽和喉中广泛表达,具有特定的模式。TRP 激动剂急性刺激咽感觉可改善神经生理学、吞咽反应的生物力学和吞咽安全性。亚急性刺激促进大脑可塑性,进一步改善 OD 老年患者的吞咽功能。

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