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阿片类药物暴露停止后斑马鱼胚胎中持续的转录组改变。

Persistent Transcriptome Alterations in Zebrafish Embryos After Discontinued Opioid Exposure.

作者信息

North Ryan J, Cooper Gwendolyn, Mears Lucas, Bothner Brian, Dlakić Mensur, Merzdorf Christa S

机构信息

Department of Microbiology and Cell Biology, Montana State University, Bozeman, MT 59717, USA.

Department of Chemistry and Biochemistry, Montana State University, Bozeman, MT 59717, USA.

出版信息

Int J Mol Sci. 2025 May 19;26(10):4840. doi: 10.3390/ijms26104840.

Abstract

Much attention has been paid to the public health crisis that has resulted from the opioid epidemic. Given the high number of opioid users that are of childbearing age, the impact of utero exposure is a serious concern. Unfortunately, there is little knowledge regarding the consequences of opioid exposure during early development. While neurobehavioral effects of opioid exposure are well-documented, effects of exposure on embryogenesis remain largely unexplored. To address this gap in knowledge, we investigated the effects of oxycodone and fentanyl exposure on gene expression in zebrafish () embryos using whole embryo RNA sequencing. Embryos were exposed to environmentally relevant (oxycodone HCl 10.6 ng/L and fentanyl citrate 0.629 ng/L) and therapeutically relevant doses (oxycodone HCl 35.14 μg/L and fentanyl citrate 3.14 μg/L) from 2 to 24 h post-fertilization (hpf), followed by another 24 h of opioid-free development. mRNA profiling at 48 hpf revealed dose- and drug-specific gene expression changes. Lower doses of oxycodone and fentanyl both induced more differentially expressed transcripts (DETs) than higher doses, potentially indicative of opioid receptor desensitization occurring at higher concentrations. In total, 892 DETs (corresponding to 866 genes) were identified across all conditions suggesting continued differential gene expression well after cessation of opioid exposure. Gene ontology analysis revealed changes in gene expression relating to extracellular matrix (ECM) organization, cell adhesion, and visual and nervous system formation. Key pathways include those involved in axon guidance, synapse formation, and ECM biosynthesis/remodeling, all of which have potential implications on neural connectivity and sensory development. These findings demonstrate that very early developmental exposure to opioids induces persistent transcriptomic changes which may have lasting implications for vertebrate cellular functions. Overall, these data provide insights into the molecular mechanisms of opioid-induced alterations during development.

摘要

阿片类药物流行引发的公共卫生危机已受到广泛关注。鉴于育龄阿片类药物使用者数量众多,子宫内接触阿片类药物的影响令人严重担忧。不幸的是,关于早期发育过程中接触阿片类药物的后果知之甚少。虽然阿片类药物接触的神经行为影响已有充分记录,但对胚胎发生的影响仍 largely 未被探索。为填补这一知识空白,我们使用全胚胎 RNA 测序研究了羟考酮和芬太尼接触对斑马鱼胚胎基因表达的影响。在受精后 2 至 24 小时(hpf),胚胎暴露于环境相关剂量(盐酸羟考酮 10.6 ng/L 和枸橼酸芬太尼 0.629 ng/L)和治疗相关剂量(盐酸羟考酮 35.14 μg/L 和枸橼酸芬太尼 3.14 μg/L),随后进行 24 小时无阿片类药物的发育。48 hpf 时的 mRNA 谱分析揭示了剂量和药物特异性的基因表达变化。较低剂量的羟考酮和芬太尼诱导的差异表达转录本(DETs)均多于较高剂量,这可能表明在较高浓度下发生了阿片类受体脱敏。在所有条件下共鉴定出 892 个 DETs(对应 866 个基因),表明在阿片类药物暴露停止后很长时间内基因表达仍持续存在差异。基因本体分析揭示了与细胞外基质(ECM)组织、细胞粘附以及视觉和神经系统形成相关的基因表达变化。关键途径包括那些参与轴突导向、突触形成和 ECM 生物合成/重塑的途径,所有这些都对神经连接和感觉发育具有潜在影响。这些发现表明,在发育早期接触阿片类药物会诱导持续的转录组变化,这可能对脊椎动物细胞功能产生持久影响。总体而言,这些数据为发育过程中阿片类药物诱导改变的分子机制提供了见解。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b9e4/12111994/a450263a402a/ijms-26-04840-g001.jpg

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