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在预防达尔盐敏感性高血压方面,肾脏基因组和生物学途径的动态汇聚和发散。

Dynamic convergence and divergence of renal genomic and biological pathways in protection from Dahl salt-sensitive hypertension.

机构信息

Department of Physiology, Medical College of Wisconsin, Milwaukee, WI 53226, USA.

出版信息

Physiol Genomics. 2010 Mar 3;41(1):63-70. doi: 10.1152/physiolgenomics.00170.2009. Epub 2009 Dec 15.

Abstract

Chromosome 13 consomic and congenic rat strains were analyzed to investigate the pattern of genomic pathway utilization involved in protection against salt-sensitive hypertension and renal injury. Introgression of the entire Brown-Norway chromosome 13 (consomic SS-13(BN)) or nonoverlapping segments of this chromosome (congenic strains, 16 Mbp in D13Rat151-D13Rat197 or 14 Mbp in D13Rat111-D13Got22) into the genome of the Dahl salt-sensitive rat attenuated salt-induced hypertension and proteinuria. mRNA abundance profiles in the renal cortex and the renal medulla from rats receiving 0.4% or 8% NaCl diets revealed two important features of pathway recruitment in these rat strains. First, the two congenic strains shared alterations in several pathways compared with Dahl salt-sensitive rats, despite the fact that the genomic segments introgressed in the two congenic strains did not overlap. Second, even though the genomic segment introgressed in each congenic strain was a part of the chromosome introgressed in the consomic strain, pathways altered in each congenic strain were not simply a subset of those altered in the consomic. Supporting the relevance of the mRNA data, differential expression of oxidative stress-related genes among the four strains of rats was associated with differences in urinary excretion of lipid peroxidation products. The findings suggest that different genetic alterations might converge to influence shared pathways in protection from hypertension, and that, depending on the genomic context, the same genetic alteration might diverge to affect different pathways.

摘要

通过分析 13 号染色体同源和同基因大鼠品系,研究了参与保护盐敏感型高血压和肾脏损伤的基因组途径利用模式。将整个布朗-挪威 13 号染色体(同源 SS-13(BN))或该染色体的非重叠片段(同基因品系,16 Mbp 在 D13Rat151-D13Rat197 或 14 Mbp 在 D13Rat111-D13Got22)导入 Dahl 盐敏感大鼠基因组,可减轻盐诱导的高血压和蛋白尿。接受 0.4%或 8%NaCl 饮食的大鼠肾皮质和肾髓质 mRNA 丰度谱揭示了这些大鼠品系中途径募集的两个重要特征。首先,尽管两种同基因品系中导入的基因组片段不重叠,但与 Dahl 盐敏感大鼠相比,它们共享几个途径的改变。其次,尽管每个同基因品系导入的基因组片段是导入同源品系的染色体的一部分,但每个同基因品系中改变的途径并不是同源品系中改变的途径的子集。支持 mRNA 数据的相关性,四种大鼠品系之间与氧化应激相关的基因的差异表达与尿液中脂质过氧化产物排泄的差异有关。研究结果表明,不同的遗传改变可能趋同于影响高血压保护中的共享途径,并且取决于基因组背景,相同的遗传改变可能发散以影响不同的途径。

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