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通过全身给药的可穿透血脑屏障和作用于外周的局部麻醉药对神经损伤诱导的热和触觉超敏反应进行差异性阻断。

Differential blockade of nerve injury-induced thermal and tactile hypersensitivity by systemically administered brain-penetrating and peripherally restricted local anesthetics.

作者信息

Chen Qingmin, King Tamara, Vanderah Todd W, Ossipov Michael H, Malan T Philip, Lai Josephine, Porreca Frank

机构信息

Department of Pharmacology, College of Medicine, University of Arizona, Tucson, AZ 85724, USA.

出版信息

J Pain. 2004 Jun;5(5):281-9. doi: 10.1016/j.jpain.2004.05.002.

Abstract

UNLABELLED

Systemic administration of local anesthetics has been shown to transiently reverse thermal and tactile hypersensitivity induced by peripheral nerve injury, effects that have been taken as suggesting direct actions on the peripheral nerves. The present study sought to determine whether a central site of action could contribute to, or account for, the effects of lidocaine on nerve injury-induced thermal and tactile hypersensitivity. Systemic lidocaine and its peripherally restricted analogues, QX-314 or QX-222, effectively reversed thermal hypersensitivity after spinal nerve ligation injury. Nerve injury-induced tactile hypersensitivity, however, was reversed by systemic lidocaine but not QX-314 or QX-222. Microinjection of either lidocaine or QX-314 into the rostral ventromedial medulla fully reversed spinal nerve ligation-induced thermal and tactile hypersensitivity. The data strongly suggest that nerve injury-induced thermal and tactile hypersensitivity are mediated through different mechanisms. In addition, the present study supports a prominent contribution of the central nervous system in the activity of systemically given lidocaine against nerve injury-induced tactile and thermal hypersensitivity. Thus, lidocaine might reverse tactile hypersensitivity mainly through its actions within the central nervous system, whereas its reversal of thermal hypersensitivity might occur through either central or peripheral sites.

PERSPECTIVE

Nerve injury-induced neuropathic pain has proved remarkably difficult to treat. Systemic administration of ion channel blockers such as lidocaine has been explored for the management of chronic pain. This work indicates that systemic rather than local administration of lidocaine would be more effective in treating tactile allodynia.

摘要

未标记

已表明局部麻醉药的全身给药可短暂逆转由周围神经损伤引起的热和触觉超敏反应,这些作用被认为提示对周围神经有直接作用。本研究旨在确定作用于中枢部位是否有助于或解释利多卡因对神经损伤诱导的热和触觉超敏反应的影响。全身给予利多卡因及其外周受限类似物QX - 314或QX - 222,可有效逆转脊神经结扎损伤后的热超敏反应。然而,神经损伤诱导的触觉超敏反应可被全身给予的利多卡因逆转,但不能被QX - 314或QX - 222逆转。向延髓头端腹内侧微量注射利多卡因或QX - 314可完全逆转脊神经结扎诱导的热和触觉超敏反应。数据强烈表明,神经损伤诱导的热和触觉超敏反应是通过不同机制介导的。此外,本研究支持中枢神经系统在全身给予利多卡因对抗神经损伤诱导的触觉和热超敏反应的活性中起重要作用。因此,利多卡因可能主要通过其在中枢神经系统内的作用逆转触觉超敏反应,而其对热超敏反应的逆转可能通过中枢或外周部位发生。

观点

事实证明,神经损伤引起的神经性疼痛极难治疗。已探索全身给予离子通道阻滞剂如利多卡因来管理慢性疼痛。这项工作表明,全身而非局部给予利多卡因在治疗触觉异常性疼痛方面会更有效。

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