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Rag1 immunodeficiency‐induced early aging and senescence in zebrafish are dependent on chronic inflammation and oxidative stress

机译:Rag1免疫缺陷引起的斑马鱼的早期衰老和衰老取决于慢性炎症和氧化应激

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摘要

In mammals, recombination activating gene 1 (RAG1) plays a crucial role in adaptive immunity, generating a vast range of immunoglobulins. Rag1 −/− zebrafish (Danio rerio) are viable and reach adulthood without obvious signs of infectious disease in standard nonsterile conditions, suggesting that innate immunity could be enhanced to compensate for the lack of adaptive immunity. By using microarray analysis, we confirmed that the expression of immunity‐ and apoptosis‐related genes was increased in the rag1 −/− fish. This tool also allows us to notice alterations of the DNA repair and cell cycle mechanisms in rag1 −/− zebrafish. Several senescence and aging markers were analyzed. In addition to the lower lifespan of rag1 −/− zebrafish compared to their wild‐type (wt) siblings, rag1 −/− showed a higher incidence of cell cycle arrest and apoptosis, a greater amount of phosphorylated histone H2AX, oxidative stress and decline of the antioxidant mechanisms, an upregulated expression and activity of senescence‐related genes and senescence‐associated β‐galactosidase, respectively, diminished telomere length, and abnormal self‐renewal and repair capacities in the retina and liver. Metabolomic analysis also demonstrated clear differences between wt and rag1 −/− fish, as was the deficiency of the antioxidant metabolite l‐acetylcarnitine (ALCAR) in rag1 −/− fish. Therefore, Rag1 activity does not seem to be limited to V(D)J recombination but is also involved in senescence and aging. Furthermore, we confirmed the senolytic effect of ABT‐263, a known senolytic compound and, for the first time, the potential in vivo senolytic activity of the antioxidant agent ALCAR, suggesting that this metabolite is essential to avoid premature aging.
机译:在哺乳动物中,重组激活基因1(RAG1)在适应性免疫中起着至关重要的作用,产生了广泛的免疫球蛋白。 Rag1 -/-斑马鱼(Danio rerio)在标准非无菌条件下可存活并成年,而没有明显的传染病迹象,这表明可以增强先天免疫力以弥补缺乏适应性免疫力的不足。通过使用微阵列分析,我们证实了rag1 -/-鱼中免疫相关和凋亡相关基因的表达增加。该工具还使我们能够注意到rag1 -/-斑马鱼中DNA修复和细胞周期机制的改变。分析了几种衰老和衰老标记。除了rag1 -/-斑马鱼的寿命比野生型(wt)兄弟姐妹低之外,rag1 -/-的斑马鱼还表现出更高的细胞周期停滞和凋亡,大量的磷酸化组蛋白H2AX,氧化应激和抗氧化机制的下降,衰老相关基因和衰老相关的β-半乳糖苷酶的表达和活性分别升高,端粒长度减少,异常的自我更新和修复视网膜和肝脏的能力。代谢组学分析还表明wt和rag1 -/-鱼之间存在明显差异,rag1 -/-鱼中抗氧化剂代谢物l-乙酰肉碱(ALCAR)的缺乏也是如此。因此,Rag1活性似乎不仅限于V(D)J重组,而且还涉及衰老和衰老。此外,我们证实了一种已知的衰老化合物ABT-263的衰老作用,并且首次证实了抗氧化剂ALCAR在体内的潜在衰老作用,这表明该代谢产物对于避免过早衰老至关重要。

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