晚期癌症和重症疼痛的新型药物治疗:关注神经性疼痛和化疗引起的周围神经病变。

IF 2.7 Q2 HEALTH CARE SCIENCES & SERVICES
Palliative Care and Social Practice Pub Date : 2024-07-31 eCollection Date: 2024-01-01 DOI:10.1177/26323524241266603
Mellar P Davis
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引用次数: 0

摘要

应将市售但作用机制新颖的药物作为镇痛药进行研究。本综述将讨论氟哌啶醇、米拉卡巴林、棕榈酰乙醇酰胺(PEA)和氯尼丁作为辅助镇痛剂或镇痛药的问题。氟哌啶醇是一种σ-1受体拮抗剂。在压力和神经病理性损伤的情况下,sigma-1 受体作为一种伴侣蛋白,会降低阿片受体的活性,并打开多个离子通道。在临床上,仅有少量证据表明氟哌啶醇与吗啡、美沙酮或曲马多合用可改善癌症、纤维化引起的疼痛、放射性坏死或神经性疼痛患者的疼痛。米拉格巴林是一种加巴喷丁类药物,自 2019 年起在日本获准用于治疗神经病理性疼痛。在随机试验中,糖尿病神经病变患者对米拉加巴林产生了反应。它与钙通道亚基的结合半衰期较长,与其他加巴喷丁类药物相比可能更具优势。PEA 属于一类被称为 ALIAmides(自体局部损伤拮抗剂酰胺)的内源性生物活性脂质,在调节多种生物过程,特别是神经病理性损伤和全身炎症的非神经元神经炎症反应方面具有重要作用。多项随机试验和荟萃分析表明,PEA 能有效减轻不同疼痛表型引起的疼痛严重程度。氯尼丁是α2肾上腺素受体激动剂和咪唑啉2受体激动剂,已被美国联邦药品管理局批准用于治疗儿童注意缺陷多动障碍、抽动秽语综合征、癌症相关疼痛的辅助治疗和高血压。氯尼地定激活α2肾上腺素受体会导致抑制性G蛋白(Gi/Go)的下游激活,从而抑制环磷酸腺苷(AMP)的产生并使神经元膜超极化,从而减轻异动症。静脉注射氯硝安定已被用于症状控制不佳,尤其是疼痛和躁动的临终病人。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Novel drug treatments for pain in advanced cancer and serious illness: a focus on neuropathic pain and chemotherapy-induced peripheral neuropathy.

Drugs that are commercially available but have novel mechanisms of action should be explored as analgesics. This review will discuss haloperidol, miragabalin, palmitoylethanolamide (PEA), and clonidine as adjuvant analgesics or analgesics. Haloperidol is a sigma-1 receptor antagonist. Under stress and neuropathic injury, sigma-1 receptors act as a chaperone protein, which downmodulates opioid receptor activities and opens several ion channels. Clinically, there is only low-grade evidence that haloperidol improves pain when combined with morphine, methadone, or tramadol in patients who have cancer, pain from fibrosis, radiation necrosis, or neuropathic pain. Miragabalin is a gabapentinoid approved for the treatment of neuropathic pain in Japan since 2019. In randomized trials, patients with diabetic neuropathy have responded to miragabalin. Its long binding half-life on the calcium channel subunit may provide an advantage over other gabapentinoids. PEA belongs to a group of endogenous bioactive lipids called ALIAmides (autocoid local injury antagonist amides), which have a sense role in modulating numerous biological processes in particular non-neuronal neuroinflammatory responses to neuropathic injury and systemic inflammation. Multiple randomized trials and meta-analyses have demonstrated PEA's effectiveness in reducing pain severity arising from diverse pain phenotypes. Clonidine is an alpha2 adrenoceptor agonist and an imidazoline2 receptor agonist, which is U.S. Federal Drug Administration approved for attention deficit hyperactivity disorder in children, Tourette's syndrome, adjunctive therapy for cancer-related pain, and hypertension. Clonidine activation at alpha2 adrenoceptors causes downstream activation of inhibitory G-proteins (Gi/Go), which inhibits cyclic Adenosine monophosphate (AMP) production and hyperpolarizes neuron membranes, thus reducing allodynia. Intravenous clonidine has been used in terminally ill patients with poorly controlled symptoms, in particular pain and agitation.

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来源期刊
Palliative Care and Social Practice
Palliative Care and Social Practice Nursing-Advanced and Specialized Nursing
CiteScore
2.90
自引率
0.00%
发文量
37
审稿时长
9 weeks
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