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转录组和网络分析揭示贻贝中内分泌干扰的机制相关生物标志物

Transcriptomic and Network Analyses Reveal Mechanistic-Based Biomarkers of Endocrine Disruption in the Marine Mussel, Mytilus edulis.

机构信息

School for the Environment , University of Massachusetts Boston , Boston , Massachusetts 02125 United States.

Center for Environmental and Human Toxicology , University of Florida , Gainesville , Florida 32611 United States.

出版信息

Environ Sci Technol. 2018 Aug 21;52(16):9419-9430. doi: 10.1021/acs.est.8b01604. Epub 2018 Jun 28.

DOI:10.1021/acs.est.8b01604
PMID:29953215
Abstract

Transcriptomics, high-throughput assays, and adverse outcome pathways (AOP) are promising approaches applied to toxicity monitoring in the 21st century, but development of these methods is challenging for nonmodel organisms and emerging contaminants. For example, Endocrine Disrupting Compounds (EDCs) may cause reproductive impairments and feminization of male bivalves; however, the mechanism linked to this adverse outcome is unknown. To develop mechanism-based biomarkers that may be linked through an AOP, we exposed Mytilus edulis to 17-alpha-ethinylestradiol (5 and 50 ng/L) and 4-nonylphenol (1 and 100 μg/L) for 32 and 39 days. When mussels were exposed to these EDCs, we found elevated female specific transcripts and significant female-skewed sex ratios using a RT-qPCR assay. We performed gene expression analysis on digestive gland tissue using an M. edulis microarray and through network and targeted analyses identified the nongenomic estrogen signaling pathway and steroidogenesis pathway as the likely mechanisms of action for a putative AOP. We also identified several homologues to genes within the vertebrate steroidogenesis pathway including the cholesterol side chain cleavage complex. From this AOP, we designed the Coastal Biosensor for Endocrine Disruption (C-BED) assay which was confirmed in the laboratory and tested in the field.

摘要

转录组学、高通量检测和不良结局途径(AOP)是 21 世纪应用于毒性监测的有前途的方法,但这些方法的开发对于非模式生物和新兴污染物具有挑战性。例如,内分泌干扰化合物(EDCs)可能导致贝类雄性生殖损伤和雌性化;然而,与这种不良结局相关的机制尚不清楚。为了开发可能通过 AOP 联系起来的基于机制的生物标志物,我们用 17-α-乙炔基雌二醇(5 和 50ng/L)和 4-壬基酚(1 和 100μg/L)处理贻贝 32 和 39 天。当贻贝暴露于这些 EDCs 时,我们发现使用 RT-qPCR 检测到雌性特异性转录本升高和显著的雌性偏性性别比。我们使用贻贝微阵列对消化腺组织进行了基因表达分析,并通过网络和靶向分析鉴定了非基因组雌激素信号通路和类固醇生成途径作为潜在 AOP 的作用机制。我们还鉴定了几个与脊椎动物类固醇生成途径中的基因同源的基因,包括胆固醇侧链裂解复合物。从这个 AOP 中,我们设计了海岸生物传感器内分泌干扰(C-BED)检测,该检测在实验室中得到了验证,并在现场进行了测试。

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