Key Laboratory of Aquatic Nutrition and Feed Science of Jiangsu Province, College of Animal Science and Technology, Nanjing Agricultural University, No.1 Weigang Road, Nanjing, 210095, People's Republic of China.
National Laboratory of Animal Science, Nanjing Agricultural University, No.1 Weigang Road, Nanjing, 210095, People's Republic of China.
Fish Physiol Biochem. 2024 Feb;50(1):183-196. doi: 10.1007/s10695-023-01205-5. Epub 2023 Jun 9.
Hypoxia is the most significant factor that threatens the health and even survival of freshwater and marine fish. Priority should be given to the investigation of hypoxia adaptation mechanisms and their subsequent modulation. Acute and chronic studies were designed for the current study. Acute hypoxia comprised of normoxia dissolved oxygen (DO) 7.0 ± 0.5 mg/mL (N0), low-oxygen 5.0 ± 0.5 mg/mL(L0), and hypoxia 1.0 ± 0.1 mg/mL (H0) and 300 mg/L Vc for hypoxia regulation (N300, L300, H300). Chronic hypoxia comprised of normoxia (DO 7.0 ± 0.5 mg/mL) with 50 mg/kg Vc in the diet (N50) and low oxygen (5.0 ± 0.5 mg/mL) with 50, 250, 500 mg/kg Vc in the diet (L50, L250, L500) to assess the effect of Vc in hypoxia. The growth, behavior, hematological parameters, metabolism, antioxidants, and related inflammatory factors of channel catfish were investigated, and it was found that channel catfish have a variety of adaptive mechanisms in response to acute and chronic hypoxia. Under acute 5 mg/mL DO, the body color lightened (P < 0.05) and reverted to normal with 300 mg/mL Vc. PLT was significantly elevated after 300 mg/L Vc (P < 0.05), indicating that Vc can effectively restore hemostasis following oxygen-induced tissue damage. Under acute hypoxia, the significantly increased of cortisol, blood glucose, the gene of pyruvate kinase (pk), and phosphofructokinase (pfk), together with the decreased expression of fructose1,6-bisphosphatase (fbp) and the reduction in myoglycogen, suggested that Vc might enhance the glycolytic ability of the channel catfish. And the enzyme activities of superoxide dismutase (SOD) and catalase (CAT) and the gene expression of sod rose significantly, showing that Vc might improve the antioxidant capacity of the channel catfish. The significant up-regulation of tumor necrosis factor-alpha (tnf-α), interleukin-1β (il-1β), and cd68 under acute hypoxia implies that hypoxia may generate inflammation in channel catfish, whereas the addition of Vc and down-regulation of these genes suggests that Vc suppresses inflammation under acute hypoxia. We found that the final weight, WGR, FCR, and FI of channel catfish were significantly reduced under chronic hypoxia, and that feeding 250 mg/kg of Vc in the diet was effective in alleviating the growth retardation caused by hypoxia. The significant increase in cortisol, blood glucose, myoglycogen, and the expression of tnf-α, il-1β, and cd68 (P < 0.05) and the significant decrease in lactate (P < 0.05) under chronic hypoxia indicated that the channel catfish had gradually adapted to the survival threat posed by hypoxia and no longer relied on carbohydrates as their primary source of energy. While the addition of Vc did not appear to increase the energy supply of the fish under hypoxia in terms of glucose metabolism, but the significantly decreased expression of tnf-α, il-1β, and cd68 (P < 0.05) also were found, indicating that chronic hypoxia, similar acute hypoxia, may increase inflammation in the channel catfish. This study indicates that under acute stress, channel catfish withstand stress by raising energy supply through glycolysis, and acute hypoxic stress significantly promotes inflammation in channel catfish, but Vc assists the channel catfish resist stress by raising glycolysis, antioxidant capacity, and decreasing the production of inflammatory markers. Under chronic hypoxia, the channel catfish no longer utilize carbohydrates as their primary energy source, and Vc may still effectively reduce inflammation in the channel catfish under hypoxia.
缺氧是威胁淡水和海水鱼类健康甚至生存的最重要因素。应该优先研究缺氧适应机制及其随后的调节。本研究设计了急性和慢性研究。急性缺氧包括正常氧溶解氧 (DO) 7.0 ± 0.5 mg/mL (N0)、低氧 5.0 ± 0.5 mg/mL (L0) 和缺氧 1.0 ± 0.1 mg/mL (H0) 和 300 mg/L 抗坏血酸用于缺氧调节 (N300、L300、H300)。慢性缺氧包括正常氧 (DO 7.0 ± 0.5 mg/mL) 和饮食中 50 mg/kg 抗坏血酸 (N50) 和低氧 (5.0 ± 0.5 mg/mL) 和饮食中 50、250、500 mg/kg 抗坏血酸 (L50、L250、L500) 以评估抗坏血酸在缺氧中的作用。研究了斑点叉尾鮰的生长、行为、血液学参数、代谢、抗氧化剂和相关炎症因子,发现斑点叉尾鮰对急性和慢性缺氧有多种适应机制。在急性 5 mg/mL DO 下,体色变浅 (P < 0.05),并在 300 mg/L 抗坏血酸下恢复正常。添加 300 mg/L 抗坏血酸后 PLT 显著升高 (P < 0.05),表明抗坏血酸可以有效恢复氧诱导的组织损伤后的止血功能。在急性缺氧下,皮质醇、血糖、丙酮酸激酶 (pk) 和磷酸果糖激酶 (pfk) 的基因显著增加,果糖 1,6-二磷酸酶 (fbp) 的表达降低,肌糖原减少,表明抗坏血酸可能增强斑点叉尾鮰的糖酵解能力。超氧化物歧化酶 (SOD) 和过氧化氢酶 (CAT) 的酶活性以及 sod 基因的表达显著升高,表明抗坏血酸可能提高斑点叉尾鮰的抗氧化能力。急性缺氧下肿瘤坏死因子-α (tnf-α)、白细胞介素-1β (il-1β) 和 cd68 的显著上调表明缺氧可能导致斑点叉尾鮰产生炎症,而添加抗坏血酸和下调这些基因表明抗坏血酸在急性缺氧下抑制炎症。我们发现,慢性缺氧下斑点叉尾鮰的最终体重、WGR、FCR 和 FI 显著降低,饮食中添加 250 mg/kg 抗坏血酸可有效缓解缺氧引起的生长迟缓。慢性缺氧下皮质醇、血糖、肌糖原和 tnf-α、il-1β 和 cd68 的表达显著增加 (P < 0.05) 以及乳酸的显著减少 (P < 0.05) 表明,斑点叉尾鮰已逐渐适应缺氧对生存的威胁,不再依赖碳水化合物作为其主要能量来源。虽然在缺氧条件下添加抗坏血酸似乎没有增加葡萄糖代谢中鱼类的能量供应,但发现 tnf-α、il-1β 和 cd68 的表达显著降低 (P < 0.05),表明慢性缺氧与急性缺氧一样,可能会增加斑点叉尾鮰的炎症。本研究表明,在急性应激下,斑点叉尾鮰通过提高糖酵解的能量供应来承受应激,急性缺氧应激会显著促进斑点叉尾鮰的炎症,但抗坏血酸通过提高糖酵解、抗氧化能力和降低炎症标志物的产生来帮助斑点叉尾鮰抵抗应激。在慢性缺氧下,斑点叉尾鮰不再将碳水化合物作为其主要能量来源,而抗坏血酸可能仍能有效降低缺氧下斑点叉尾鮰的炎症。
