首页> 美国卫生研究院文献>Journal of Pain Research >Multivariate proteomic analysis of the cerebrospinal fluid of patients with peripheral neuropathic pain and healthy controls – a hypothesis-generating pilot study
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Multivariate proteomic analysis of the cerebrospinal fluid of patients with peripheral neuropathic pain and healthy controls – a hypothesis-generating pilot study

机译:周围神经性疼痛和健康对照患者脑脊液的多变量蛋白质组学分析-一项假设产生的先导研究

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摘要

Pain medicine lacks objective biomarkers to guide diagnosis and treatment. Combining two-dimensional gel proteomics with multivariate data analysis by projection, we exploratively analyzed the cerebrospinal fluid of eleven patients with severe peripheral neuropathic pain due to trauma and/or surgery refractory to conventional treatment and eleven healthy controls. Using orthogonal partial least squares discriminant analysis, we identified a panel of 36 proteins highly discriminating between the two groups. Due to a possible confounding effect of age, a new model with age as outcome variable was computed for patients (n=11), and four out of 36 protein spots were excluded due to a probable influence of age. Of the 32 remaining proteins, the following seven had the highest discriminatory power between the two groups: an isoform of angiotensinogen (upregulated in patients), two isoforms of alpha-1-antitrypsin (downregulated in patients), three isoforms of haptoglobin (upregulated in patients), and one isoform of pigment epithelium-derived factor (downregulated in patients). It has recently been hypothesized that the renin–angiotensin system may play a role in the pathophysiology of neuropathic pain, and a clinical trial of an angiotensin II receptor antagonist was recently published. It is noteworthy that when searching for neuropathic pain biomarkers with a purely explorative methodology, it was indeed a renin–angiotensin system protein that had the highest discriminatory power between patients and controls in the present study. The results from this hypothesis-generating pilot study have to be confirmed in larger, hypothesis-driven studies with age-matched controls, but the present study illustrates the fruitfulness of combining proteomics with multivariate data analysis in hypothesis-generating pain biomarker studies in humans.
机译:止痛药缺乏客观的生物标志物来指导诊断和治疗。结合二维凝胶蛋白质组学和投影数据分析,我们探索性地分析了11例因常规治疗难以治疗的创伤和/或手术导致的重度周围神经性疼痛的患者的脑脊液。使用正交偏最小二乘判别分析,我们确定了一组高度区分两组的36种蛋白质。由于年龄可能造成的混淆影响,针对患者(n = 11)计算了一个以年龄为结果变量的新模型,并且由于年龄的可能影响,排除了36个蛋白质斑点中的四个。在剩余的32种蛋白质中,以下7种在两组之间具有最高的鉴别能力:血管紧张素原亚型(患者中上调),两种α-1-抗胰蛋白酶亚型(患者中下调),三种触珠蛋白亚型(在患者中上调)。患者)和色素上皮衍生因子的一种同工型(在患者中被下调)。最近有人假设,肾素-血管紧张素系统可能在神经性疼痛的病理生理中起作用,并且最近发表了血管紧张素II受体拮抗剂的临床试验。值得注意的是,当以纯粹的探索性方法搜索神经性疼痛生物标志物时,在本研究中,确实是肾素-血管紧张素系统蛋白在患者和对照组之间具有最高的辨别力。这项假设产生的先导研究的结果必须在更大的,假设驱动的,年龄匹配的对照研究中得到证实,但是本研究说明了蛋白质组学与多元数据分析相结合在人类产生假设的疼痛生物标志物研究中的成果。

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