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13号染色体对里昂高血压大鼠高血压及相关疾病的影响。

Implication of chromosome 13 on hypertension and associated disorders in Lyon hypertensive rats.

作者信息

Gilibert Sophie, Bataillard Alain, Nussberger Juerg, Sassard Jean, Kwitek Anne E

机构信息

Université de Lyon, Université Lyon1, Département de Physiologie et Pharmacologie Clinique, Faculté de Pharmacie, Lyon, France.

出版信息

J Hypertens. 2009 Jun;27(6):1186-93. doi: 10.1097/hjh.0b013e328329e4c0.

Abstract

BACKGROUND

Hypertension and associated disorders are major risk factors for cardiovascular disease. The Lyon hypertensive rat (LH) is a genetically hypertensive strain that exhibits spontaneous and salt-sensitive hypertension, exaggerated proteinuria, high body weight, hyperlipidemia, and elevated insulin-to-glucose ratio. Previous genetic mapping identified quantitative trait loci (QTLs) influencing blood pressure (BP) on rat chromosome 13 (RNO13) in several models of hypertension.

METHODS

To study the effects of a single chromosome on the mapped traits, we generated consomic strains by substituting LH RNO13 with that of the normotensive Brown Norway (BN) strain (LH-13BN) and reciprocal consomics by substituting a BN RNO13 with that of LH (BN-13LH). These reciprocal consomic strains, as well as the two parental strains were characterized for BP, metabolic and morphological parameters.

RESULTS

Compared with LH parents, LH-13BN rats showed decreased mean BP (up to -24 mmHg on 2% NaCl in the drinking water), urine proteins and lipids, and increased body weight. Differences between BN-13LH and BN rats were much smaller than those observed between LH-13BN and LH rats, demonstrating the effects of the highly resistant BN genome background. Plasma renin activity was not affected by the substitution of RNO13, despite the significant BP differences.

CONCLUSION

The present work demonstrates that RNO13 is a determinant of BP, proteinuria, and plasma lipids in the LH rat. The distinct phenotypic differences between the consomic LH-13BN and the LH make it a powerful model to determine genes and pathways leading to these risk factors for cardiovascular and renal disease.

摘要

背景

高血压及相关疾病是心血管疾病的主要危险因素。里昂高血压大鼠(LH)是一种遗传性高血压品系,表现出自发性和盐敏感性高血压、蛋白尿增加、体重增加、高脂血症以及胰岛素与葡萄糖比值升高。先前的基因定位在几种高血压模型中确定了大鼠13号染色体(RNO13)上影响血压(BP)的数量性状基因座(QTL)。

方法

为了研究单条染色体对定位性状的影响,我们通过用正常血压的褐家鼠(BN)品系的RNO13替换LH的RNO13(LH-13BN)来生成代换系,并通过用LH的RNO13替换BN的RNO13来生成 reciprocal 代换系(BN-13LH)。对这些 reciprocal 代换系以及两个亲本系的血压、代谢和形态学参数进行了表征。

结果

与LH亲本相比,LH-13BN大鼠的平均血压降低(饮用水中含2%氯化钠时高达-24 mmHg)、尿蛋白和脂质减少,体重增加。BN-13LH与BN大鼠之间的差异远小于LH-13BN与LH大鼠之间的差异,这表明了高度抗性的BN基因组背景的影响。尽管血压存在显著差异,但RNO13的替换对血浆肾素活性没有影响。

结论

目前的研究表明,RNO13是LH大鼠血压、蛋白尿和血脂的决定因素。代换系LH-13BN与LH之间明显的表型差异使其成为确定导致心血管和肾脏疾病这些危险因素的基因和途径的有力模型。

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