龙腾通络方利用血清基因组学对肺癌疼痛患者进行精准治疗的试点研究。

W U Ruixin, Fang Qingliang, Guan Sisi, Wei Xianglong, Shan Mengjun, Mao Zhujun, Gong Yabin, X U Ling, Zhou Di, Dong Changsheng
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引用次数: 0

摘要

研究目的探讨龙藤通络汤联合三阶梯镇痛治疗肺癌疼痛的疗效,以及龙藤通络汤治疗前后血清miRNA表达的变化及其与肺癌疼痛的相关性。研究还探讨了LTL治疗肺癌疼痛的可能机制:试验研究于2018年3月至2019年10月期间在岳阳医院和龙华医院肿瘤科病房进行。对24例确诊为肺癌的癌痛患者进行LTL或安慰剂联合三阶梯镇痛治疗的前瞻性、单盲、安慰剂对照、随机临床试验。镇痛效果是主要研究结果。等效吗啡消耗量和数字评分量表(NRS)评分作为次要结果。在本研究中,我们利用深度测序技术比较了肺癌疼痛治疗组(LTL + 三步镇痛法)和对照组(安慰剂 + 三步镇痛法)两组血清样本中不同的 miRNA 表达。接下来,我们利用靶标预测数据库研究了 miRNA 差异表达的靶基因,并利用基因本体(GO)分析和京都基因组百科全书(KEGG)通路富集分析分别研究了与差异表达靶基因相关的作用和主要生化及信号通路:结果:与治疗前相比,LTL治疗可明显降低NRS评分(P = 0.021),与对照组相比,总吗啡当量消耗量(P = 0.007)和平均每日吗啡当量消耗量(P = 0.003)也明显降低。两组患者中 31 种 miRNA 的表达差异很大(上调或下调≥ 2 倍):LTL对减轻肺癌疼痛有明显作用,其作用机制可能与下调has-miR-2110和has-miR-7d-3p的表达有关。这项试验研究为进一步探索 LTTL 在肺癌疼痛患者中的应用提供了支持。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
A pilot study of precision treatment for patients with lung cancer pain by Longteng Tongluo recipe using serum genomics.

Objective: To investigate the efficacy of Longteng Tongluo recipe (, LTTL) combined with three-step analgesia for the treatment of lung cancer pain, and the changes in serum miRNA expressions before- and after treatment with LTTL and its correlation with lung cancer pain. The possible mechanism underlying LTTL effects on the treatment of lung cancer pain was conducted.

Methods: The pilot study was conducted at the oncology ward of the Yueyang Hospital and the Longhua Hospital between March 2018 and October 2019. A prospective, single-blind, placebo controlled, randomized clinical trial of LTTL or placebo combined with three-step analgesia treatments were administered to 24 cancer pain patients diagnosed with lung cancer. Analgesic efficacy was investigated as the primary outcome. Equivalent morphine consumption and numerical rating scale (NRS) scores were used as the secondary outcome. In the present study, we utilized deep sequencing techniques to compare the differential miRNA expressions in serum samples obtained from two groups: the lung cancer pain treatment group (LTTL + three-step analgesia) and the control group (placebo + three-step analgesia). Next, we employed the target prediction database to investigate the target genes for differential miRNA expressions and Gene Ontology (GO) analysis along with Kyoto Encyclopedia of Genes and Genomes (KEGG) pathway enrichment analysis to examine the roles and the major biochemical and signaling pathways related to the differentially expressed target genes, respectively.

Results: LTTL treatment significantly reduces the NRS score (P = 0.021) as compared to those before treatment, along with significant reductions in the total morphine equivalent consumption (P = 0.007) and the average daily equivalent morphine consumption (P = 0.003) as opposed to the control group. The expressions of 31 miRNAs differed considerably between the two groups of patients (≥ 2 times up-modulated or down-regulated between these groups, P<0.05). For instance, the miRNAs expression levels for patients before treatment (has-miR-2110 and has-miR-7d-3p) were significantly enhanced as compared to the healthy people, after LTTL treatment, the expressions of miR-2110 and miR-7d-3p in patients with lung cancer pain reduced significantly. Studies show that the above two miRNAs were significantly associated with lung cancer pain, which could mediate lung cancer pain. Furthermore, we identified 355 genes as potential targets of the 31 differentially expressed miRNAs. Pathway enrichment analyses using KEGG and GO analysis indicated that these target genes may play a crucial role in the development and modulation of lung cancer pain.

Conclusion: LTTL demonstrated a discernible impact on alleviating lung cancer pain and its mechanism of action may be related to the downregulation of has-miR-2110 and has-miR-7d-3p expressions. This pilot study provides support for further exploration of LTTL in patients with lung cancer pain.

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