Chon Helena, Bluyssen Hans A R, Holstege Frank C P, Koomans Hein A, Joles Jaap A, Braam Branko
Department of Nephrology and Hypertension, University Medical Center, GA Utrecht, Netherlands.
Eur J Pharmacol. 2005 Apr 18;513(1-2):21-33. doi: 10.1016/j.ejphar.2005.01.054. Epub 2005 Apr 22.
Hypertension demands cardiac synthetic and metabolic adaptations to increased afterload. We studied gene expression in two models of mild hypertension without overt left ventricular hypertrophy using the NO synthase inhibitor nitro-L-arginine (L-NNA) and the glutathione depletor buthionine-S,R-sulfoximine (BSO). Mice were administered L-NNA, BSO, or water for 8 weeks. RNA of left ventricles was pooled per group, reverse transcribed, Cy3 and Cy5 labeled, and hybridized to cDNA microarrays. Normalized log(2) Cy3/Cy5 ratios of > or =0.7 or < or =-0.7 were considered significant. L-NNA and BSO both caused hypertension. Gene expression was regulated in cytoskeletal components in both models, protein synthesis in L-NNA-treated mice, and energy metabolism in BSO-treated mice. Energy metabolism genes shared several common transcription factor-binding sites such as Coup-Tf2, of which gene expression was increased in BSO-treated mice, and COMP-1. Characterization of the left ventricular adaptations as assessed with gene expression profiles reveals differential expression in energy and protein metabolism related to the pathogenetic background of the hypertension.
高血压需要心脏进行合成和代谢适应以应对增加的后负荷。我们使用一氧化氮合酶抑制剂硝基-L-精氨酸(L-NNA)和谷胱甘肽消耗剂丁硫氨酸-S,R-亚砜亚胺(BSO),在两种无明显左心室肥厚的轻度高血压模型中研究基因表达。给小鼠连续8周给予L-NNA、BSO或水。每组收集左心室的RNA,进行逆转录,用Cy3和Cy5标记,并与cDNA微阵列杂交。标准化的log(2) Cy3/Cy5比值≥0.7或≤-0.7被认为具有显著性。L-NNA和BSO均导致高血压。在两种模型中,细胞骨架成分的基因表达均受到调节,L-NNA处理的小鼠中蛋白质合成相关基因表达受到调节,BSO处理的小鼠中能量代谢相关基因表达受到调节。能量代谢基因共享几个常见的转录因子结合位点,如Coup-Tf2,其在BSO处理的小鼠中基因表达增加,还有COMP-1。通过基因表达谱评估左心室适应情况的特征揭示了与高血压发病背景相关的能量和蛋白质代谢中的差异表达。
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