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六氟环氧丙烷二聚酸在秀丽隐杆线虫发育过程中的生理和转录组效应。

Physiological and transcriptomic effects of hexafluoropropylene oxide dimer acid in Caenorhabditis elegans during development.

机构信息

Boz Life Science Research and Teaching Institute, 3030 Bunker Hill Street, San Diego, CA, USA; School of Public Health, San Diego State University, 5500 Campanile Drive, San Diego, CA, USA.

Boz Life Science Research and Teaching Institute, 3030 Bunker Hill Street, San Diego, CA, USA; Division of Extended Studies, University of California San Diego, 9600N. Torrey Pines Road, La Jolla, CA, USA.

出版信息

Ecotoxicol Environ Saf. 2022 Oct 1;244:114047. doi: 10.1016/j.ecoenv.2022.114047. Epub 2022 Sep 5.

Abstract

Per- and polyfluoroalkyl substances (PFAS) are chemicals resistant to degradation. While such a feature is desirable in consumer and industrial products, some PFAS, including perfluorooctanoic acid (PFOA), are toxic and bioaccumulate. Hexafluoropropylene oxide dimer acid (HFPO-DA), an emerging PFAS developed to replace PFOA, has not been extensively studied. To evaluate the potential toxicity of HFPO-DA with a cost- and time-efficient approach, we exposed C. elegans larvae for 48 h to 4 × 10-4 g/L HFPO-DA in liquid media and measured developmental, behavioral, locomotor, and transcriptional effects at various exposure levels. Worms exposed to 1.5-4 g/L HFPO-DA were developmentally delayed, and progeny production was significantly delayed (p < 0.05) in worms exposed to 2-4 g/L HFPO-DA. Statistically significant differential gene expression was identified in all fourteen HFPO-DA exposure groups ranging from 1.25 × 10 to 4 g/L, except for 6.25 × 10 g/L. Among 10298 analyzed genes, 2624 differentially expressed genes (DEGs) were identified in the developmentally delayed 4 g/L group only, and 78 genes were differentially expressed in at least one of the thirteen groups testing 1.25 × 10-2 g/L HFPO-DA exposures. Genes encoding for detoxification enzymes including cytochrome P450 and UDP glucuronosyltransferases were upregulated in 0.25-4 g/L acute exposure groups. DEGs were also identified in lower exposure level groups, though they did not share biological functions except for six ribosomal protein-coding genes. While our transcriptional data is inconclusive to infer mechanisms of toxicity, the significant gene expression differences at 1.25 × 10 g/L, the lowest concentration tested for transcriptional changes, calls for further targeted analyses of low-dose HFPO-DA exposure effects.

摘要

全氟和多氟烷基物质(PFAS)是抗降解的化学物质。虽然这种特性在消费和工业产品中是理想的,但一些 PFAS,包括全氟辛酸(PFOA),是有毒的,会生物积累。六氟丙烯氧化物二聚酸(HFPO-DA)是为替代 PFOA 而开发的一种新兴 PFAS,尚未得到广泛研究。为了以经济高效的方式评估 HFPO-DA 的潜在毒性,我们将 C. elegans 幼虫在液体培养基中暴露于 4 × 10-4 g/L HFPO-DA 中 48 小时,并在不同暴露水平下测量发育、行为、运动和转录效应。暴露于 1.5-4 g/L HFPO-DA 的蠕虫发育延迟,暴露于 2-4 g/L HFPO-DA 的蠕虫的后代产生明显延迟(p < 0.05)。在所有 14 个 HFPO-DA 暴露组中,除了 6.25 × 10 g/L 外,都鉴定出了统计学上显著的差异基因表达,范围从 1.25 × 10 到 4 g/L。在分析的 10298 个基因中,仅在发育延迟的 4 g/L 组中鉴定出 2624 个差异表达基因(DEGs),在至少一个测试 1.25 × 10-2 g/L HFPO-DA 暴露的 13 个组中,有 78 个基因差异表达。细胞色素 P450 和 UDP 葡萄糖醛酸转移酶等解毒酶的编码基因在 0.25-4 g/L 急性暴露组中上调。在较低的暴露水平组中也鉴定出 DEGs,尽管它们除了六个核糖体蛋白编码基因外没有共同的生物学功能。虽然我们的转录数据不足以推断毒性机制,但在测试的最低浓度 1.25 × 10 g/L 时,显著的基因表达差异表明需要进一步分析低剂量 HFPO-DA 暴露的影响。

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