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硼替佐米相关性化学感觉神经病患者的随访精神物理学研究。

Follow-up psychophysical studies in bortezomib-related chemoneuropathy patients.

机构信息

Department of Anesthesia and Pain Medicine, The University of Texas MD Anderson Cancer Center, Houston, Texas, USA.

出版信息

J Pain. 2011 Sep;12(9):1017-24. doi: 10.1016/j.jpain.2011.04.008. Epub 2011 Jun 24.

Abstract

UNLABELLED

Many frontline chemotherapeutic agents produce robust neuropathy as a dose-limiting side effect; however, the persistence of chemotherapy-related sensory disturbances and pain are not well documented. We have previously investigated the qualities of bortezomib-induced pain, and now seek to determine the ongoing nature of this pain. Twenty-six control subjects and 11 patients who had previously been treated with bortezomib and who were experiencing ongoing pain consented to recurring quantitative sensory testing. A pilot immunohistochemistry study of skin innervation was also performed on patient-obtained biopsies. Psychophysical testing in patients revealed persistent changes including decreased skin temperature in the area of pain, diminished touch and sharpness detection, increased pegboard completion times, and decreased sensitivity to skin heating. Additionally, the intensity of pain, as captured by the use of a visual analog scale and pain descriptors, was reported by patients to be unchanged during the retest despite similar morphine equivalent daily doses. The patient skin biopsies displayed a marked decrease in the density of epidermal nerve fibers and Meissner's corpuscles. These results signify a persistent and severe impairment of Aβ, Aδ, and C fibers in patients with chronic bortezomib-induced chemoneuropathy. Further, this study reports a loss of both epidermal nerve fibers and Meissner's corpuscles.

PERSPECTIVE

The results of this article indicate a persistent, painful peripheral neuropathy in patients treated with bortezomib. Pilot data indicates a loss of nerve fibers innervating the area of pain. This is the first paper to address the persistence, and potential contributing factors, of bortezomib chemoneuropathy.

摘要

未标记

许多一线化疗药物会产生强烈的神经病变,作为剂量限制的副作用;然而,化疗相关的感觉障碍和疼痛的持续存在并没有得到很好的记录。我们之前研究了硼替佐米引起的疼痛的性质,现在试图确定这种疼痛的持续性质。26 名对照受试者和 11 名曾接受硼替佐米治疗且正在经历持续疼痛的患者同意进行反复的定量感觉测试。还对患者获得的活检进行了皮肤神经支配的初步免疫组织化学研究。患者的心理物理测试显示持续存在变化,包括疼痛区域皮肤温度降低、触觉和锐度检测降低、穿孔板完成时间增加以及对皮肤加热的敏感性降低。此外,患者使用视觉模拟量表和疼痛描述符报告的疼痛强度在复测时保持不变,尽管每日等效吗啡剂量相似。患者的皮肤活检显示表皮神经纤维和迈斯纳小体的密度明显降低。这些结果表明,慢性硼替佐米诱导的化学神经病变患者的 Aβ、Aδ 和 C 纤维持续严重受损。此外,本研究报告了表皮神经纤维和迈斯纳小体的丧失。

观点

本文的结果表明,接受硼替佐米治疗的患者存在持续的、疼痛的周围神经病变。初步数据表明,疼痛区域的神经纤维丧失。这是第一篇探讨硼替佐米化学神经病变的持续性及其潜在促成因素的论文。

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