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四坏素对长角血蜱血食消化的毒性作用机制。

Mechanism of the toxic effects of tetracycline on blood meal digestion in Haemaphysalis longicornis.

机构信息

Hebei Key Laboratory of Animal Physiology, Biochemistry and Molecular Biology, College of Life Sciences, Hebei Normal University, Shijiazhuang, 050024, Hebei, China.

Hebei Key Laboratory of Wetland Ecology and Conservation, Hengshui University, Hengshui, 053000, Hebei, China.

出版信息

Exp Appl Acarol. 2023 Dec;91(4):681-695. doi: 10.1007/s10493-023-00858-4. Epub 2023 Nov 21.

Abstract

The extensive utilization of antibiotics in the field of animal husbandry gives rise to various concerns pertaining to the environment and human health. Here, we demonstrate that the administration of tetracycline impedes blood meal digestion in the tick Haemaphysalis longicornis. Tissue sectioning, 16S rRNA high-throughput sequencing, and transcriptome sequencing of the midgut were employed to elucidate the mechanism underlying tetracycline toxicity. The treatment group consisted of engorged female ticks that were subjected to tetracycline microinjections (75 µg per tick), whereas the control group received sterile water injections. On days 2 and 4 following the injections, the tick body weight changes were assessed and the midguts were dissected and processed. Change in tick body weight in tetracycline-treated group was less than in the control group. In tetracycline-treated ticks, midgut epithelial cells were loosely connected and blood meal digestion was impaired compared to the control group. There was no significant change in midgut bacterial diversity after tetracycline treatment. On day 2 following treatment, the relative abundance of Escherichia-Shigella was significantly decreased, whereas the relative abundance of Allorhizobium was significantly increased compared to the control group. On day 4 following treatment, the relative abundance of Escherichia-Shigella, Allorhizobium, Ochrobactrum, and Acidibacter decreased significantly, whereas the relative abundance of Paraburkholderia and Pelomonas increased significantly. Tetracycline treatment also affected midgut gene expression, producing a cumulative effect wherein the differentially expressed genes (DEGs) were mostly down-regulated. KEGG enrichment pathway analysis revealed that on day 2 the up-regulated DEGs were significantly enriched in 21 pathways, including apoptosis and phagosome. Comparatively, the down-regulated DEGs were significantly enriched in 26 pathways, including N-glycan biosynthesis, lysosome, and autophagy. In contrast, on day 4 the up-regulated DEGs were significantly enriched in 10 pathways including aminoacyl-tRNA biosynthesis, ribosome biogenesis, RNA transport, and DNA replication, whereas the down-regulated differential genes were significantly enriched in 11 pathways including lysosome, peroxisome, N-glycan biosynthesis, and fatty acid synthesis. This indicates that tetracycline injection inhibited blood meal digestion by affecting midgut digestive cells, gut flora diversity, and gene expression. These findings could contribute to tick control by inhibiting blood meal digestion.

摘要

抗生素在畜牧业中的广泛应用引起了人们对环境和人类健康的各种关注。在这里,我们证明了四环素的给药会阻碍 tick Haemaphysalis longicornis 的血餐消化。通过组织切片、16S rRNA 高通量测序和中肠转录组测序,阐明了四环素毒性的作用机制。实验组由接受四环素微注射(每只 tick 75μg)的饱血雌性 tick 组成,而对照组接受无菌水注射。在注射后的第 2 天和第 4 天,评估 tick 体重变化并解剖和处理中肠。与对照组相比,四环素处理组的 tick 体重变化较小。在四环素处理的 tick 中,与对照组相比,中肠上皮细胞连接松散,血餐消化受损。四环素处理后中肠细菌多样性没有显著变化。在处理后的第 2 天,与对照组相比,Escherichia-Shigella 的相对丰度显著降低,而 Allorhizobium 的相对丰度显著增加。在处理后的第 4 天,Escherichia-Shigella、Allorhizobium、Ochrobactrum 和 Acidibacter 的相对丰度显著降低,而 Paraburkholderia 和 Pelomonas 的相对丰度显著增加。四环素处理还影响了中肠基因表达,产生累积效应,差异表达基因(DEGs)主要下调。KEGG 富集途径分析表明,在第 2 天,上调的 DEGs 显著富集在 21 条途径中,包括凋亡和吞噬体。相比之下,下调的 DEGs 显著富集在 26 条途径中,包括 N-聚糖生物合成、溶酶体和自噬。相反,在第 4 天,上调的 DEGs 显著富集在 10 条途径中,包括氨酰-tRNA 生物合成、核糖体生物发生、RNA 转运和 DNA 复制,而下调的差异基因显著富集在 11 条途径中,包括溶酶体、过氧化物酶体、N-聚糖生物合成和脂肪酸合成。这表明四环素注射通过影响中肠消化细胞、肠道菌群多样性和基因表达来抑制血餐消化。这些发现可能有助于通过抑制血餐消化来控制 tick。

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