齐口裂腹鱼Hsp60 cDNA克隆及其在无乳链球菌感染中的mRNA表达
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Q 785;S 941.42

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四川省重点科研项目(2018NZ0007);四川省淡水鱼产业技术体系创新团队建设项目(SCCXTD-15);雅安市市校合作项目(21SXHZ0016)


Cloning and mRNA expression analysis of Schizothorax prenanti Hsp60 in Streptococcus agalactiae infection
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Key Research Projects of Sichuan (2018NZ0007); Sichuan Freshwater Fish Industry Techno-logy System Innovation Team Construction Project (SCCXTD-15)

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    摘要:

    为探究齐口裂腹鱼热休克蛋白60基因(SpHsp60) cDNA序列的分子特征和在细菌感染中的响应情况,实验利用RACE技术克隆获得了2 277 bp的SpHsp60 cDNA序列,预测编码575个氨基酸,其与脊椎动物具有较高的保守性。齐口裂腹鱼的组织表达模式分析显示,SpHsp60在肝胰脏中表达量最高,血液次之,而在皮肤、肌肉和肠道中表达量低。无乳链球菌感染过程中,血液、肝胰脏、中肾和脾脏的SpHsp60 mRNA表达量在感染后6 h发生显著变化,提示组织中SpHsp60能快速响应感染。肝胰脏和中肾在感染后6~72 h表达量变化均显著高于对照组,而脾脏则显著低于对照组。研究表明,SpHsp60可能通过快速响应参与齐口裂腹鱼对抗细菌感染的过程,研究为肝胰脏和中肾组织中Hsp60 mRNA表达量作为齐口裂腹鱼感染无乳链球菌的危险信号分子提供基础数据。

    Abstract:

    Heat shock protein (HSP) is a ubiquitous and highly conserved stress protein, and its expression changes are associated with the health status of fish. Hsp60 is a member of the heat shock protein family with a molecular weight of about 60 ku, which is mainly distributed in mitochondria of eukaryotic cells. Hsp60 was up-regulated during stress or cell injury and recognized by pattern recognition receptors as a danger signaling molecule. Previous studies showed that cytoplasmic Hsp60 could interact with caspase-3 to increase stress tolerance and maintain cell homeostasis. However, excessive accumulation of Hsp60 can also accelerate the activation of caspase-3, induce the release of cytochrome C and promote cell apoptosis. Hsp60 can refold and repair damaged proteins under stress by ATP binding and hydrolysis. Therefore, it is very important to study the function of Hsp60 in fish during bacterial infection. Fish in natural water are threatened by environmental pollution, natural toxins and microbial infection, and bacterial infection was a common disease. Schizothorax prenanti is a unique sub-cold-water economic fish in China and an essential variety of proliferation and release in the Yangtze River’s upper reaches. S. prenanti is a special economic animal with high content of umami amino acids and good content and ratio of amino acids and fatty acids. In recent years, the techniques of artificial domestication and breeding have been relatively mature, but the specific immune system is poor. Streptococcus agalactiae is an important pathogen that harms S. prenanti and the typical clinical symptoms of infection are exophthalmic protrusion and subcutaneous abscess on the body surface. However, the early infection of S. agalactiae is not easy to detect. As an important pathogen, S. agalactiae can spread to the whole body through blood and eventually cause pathological manifestations of edema and sepsis. After entering the blood circulation, S. agalactiae can bind with serum complement C3b through polysaccharide, transforming the activated C3b into an inhibited state to avoid non-specific immune clearance of the host. Besides, S. agalactiae can also avoid phagocytosis and clearance of macrophages through polysaccharide in the capsule, thus causing damage to the visceral tissues and organs. In this study, the molecular characteristics and response to bacterial infection were investigated to explore S. prenanti Heat shock protein 60 (SpHsp60). The 2 277 bp SpHsp60 cDNA sequence was cloned using RACE technology, which encoded 575 amino acids and had relatively conserved spatial conformation with vertebrates. Then, the analysis of tissue expression pattern showed that the expression level of SpHsp60 was the highest in hepatopancreas, followed by blood, and the lowest in skin, muscle, and intestines. Furthermore, the mRNA expression of SpHsp60 in blood, hepatopancreas, trunk kidney and spleen had significant differences in 6 h after S. agalactiae infection. Compared with the control group, the mRNA expression of SpHsp60 in hepatopancreas and trunk kidney expression significantly increased from 6 h to 72 h post-infection, while those in the spleen were significantly decreased. Our results suggested that SpHsp60 could play an early warning role in bacterial infection, providing primary data for Hsp60 mRNA expression in hepatopancreas and trunk kidney as a warning signal for S. agalactiae infection in S. prenanti.

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陈德芳,芦路,蒲云丹,瞿炼石,刘博,黄小丽,欧阳萍,李志琼,耿毅.齐口裂腹鱼Hsp60 cDNA克隆及其在无乳链球菌感染中的mRNA表达[J].水产学报,2022,46(9):1680~1688

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  • 收稿日期:2021-02-19
  • 最后修改日期:2021-04-13
  • 录用日期:2021-05-28
  • 在线发布日期: 2022-09-01
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