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骨髓基质细胞在持续性疼痛的大鼠模型中产生长期的疼痛缓解。

Bone marrow stromal cells produce long-term pain relief in rat models of persistent pain.

机构信息

Department of Neural and Pain Sciences, Dental School, University of Maryland, Baltimore, Maryland 21201-1586, USA.

出版信息

Stem Cells. 2011 Aug;29(8):1294-303. doi: 10.1002/stem.667.

Abstract

Chronic pain conditions are difficult to treat and are major health problems. Bone marrow stromal cells (BMSCs) have generated considerable interest as a candidate for cell-based therapy. BMSCs are readily accessible and are easy to isolate and expand ex vivo. Clinical studies show that direct injection of BMSCs does not produce unwanted side effects and is well tolerated and safe. Here, we show that a single systemic (intravenous) or local injection (into the lesion site) of rat primary BMSCs reversed pain hypersensitivity in rats after injury and that the effect lasted until the conclusion of the study at 22 weeks. The pain hypersensitivity was rekindled by naloxone hydrochloride, an opioid receptor antagonist that acts peripherally and centrally, when tested at 1-5 weeks after BMSC infusion. In contrast, naloxone methiodide, a peripherally acting opioid receptor antagonist, only rekindled hyperalgesia in the first 3 weeks of BMSC treatment. Focal downregulation of brainstem mu opioid receptors by RNA interference (RNAi) reversed the effect of BMSCs, when RNAi was introduced at 5- but not 1-week after BMSC transplantation. Thus, BMSCs produced long-term relief of pain and this effect involved activation of peripheral and central opioid receptors in distinct time domains. The findings prompt studies to elucidate the cellular mechanisms of the BMSC-induced pain relieving effect and translate these observations into clinical settings.

摘要

慢性疼痛是一种难以治疗的疾病,也是主要的健康问题。骨髓基质细胞(BMSCs)作为细胞治疗的候选者引起了相当大的兴趣。BMSCs 易于获取,并且易于体外分离和扩增。临床研究表明,BMSCs 的直接注射不会产生不良的副作用,并且耐受性和安全性良好。在这里,我们表明,单次系统(静脉内)或局部注射(到病变部位)大鼠原代 BMSCs 可逆转损伤后大鼠的疼痛敏感性,并且该效果持续到 22 周的研究结束。当在 BMSC 输注后 1-5 周进行测试时,阿片受体拮抗剂盐酸纳洛酮重新引发了疼痛超敏反应,阿片受体拮抗剂盐酸纳洛酮仅在 BMSC 治疗的前 3 周重新引发痛觉过敏。通过 RNA 干扰(RNAi)对脑干 μ 阿片受体进行局部下调,当在 BMSC 移植后 5-但不是 1 周时引入 RNAi 时,逆转了 BMSCs 的作用。因此,BMSCs 产生了长期的疼痛缓解作用,这种作用涉及到外周和中枢阿片受体在不同时间域的激活。这些发现促使研究阐明 BMSC 诱导的疼痛缓解作用的细胞机制,并将这些观察结果转化为临床环境。

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