Genetic background in apolipoprotein A-I and cystathionine beta-synthase deficiency.

Front Biosci

Departamento de Bioquimica y Biologia Molecular y Celular, Facultad de Veterinaria, Universidad de Zaragoza, Spain.

Published: May 2008

AI Article Synopsis

  • Double heterozygous mice lacking alleles of Cbs and Apoa1 exhibit hyperhomocysteinemia and moderate hypertension, with differences in severity based on genetic background.
  • In the study, C57BL/6J mice displayed milder hypertension compared to those in a mixed genetic background (C57BL/6J x 129), showing less increase in blood pressure and different nitric oxide levels.
  • Hepatic profiling revealed significant differences in contractile protein expression between the two groups, indicating that hypertension severity is linked to a range of biological processes involving vascular health and liver function.

Article Abstract

Double heterozygous mice lacking one allele of Cbs and Apoa1 develop hyperhomocysteinemia and hypoalphalipoproteinemia together with moderate hypertension. To study the influence of the genetic background into this specific phenotype, four groups of male mice were established: control and double heterozygous groups in C57BL/6J and in C57BL/6J x 129 backgrounds, respectively. Nitric oxide levels, systolic blood pressure, plasma lipid parameters, arylesterase activity and aorta histology were analyzed as well as oligonucleotide array hybridization of liver RNA. Results demonstrated that double heterozygous mice in C57BL/6J substrate had a milder phenotype showing lower increase in blood pressure compared to double heterozygous group in hybrid background. The severity of the phenotype in the latter group was associated with lower nitric oxide and arylesterase activity levels, and hyperplasia of the vascular media layer. Hepatic profiling of both genetic substrates showed profound differences in expression of contractile proteins that could explain these pathological findings. In summary, the phenotypic presentation of hypertension is associated with multiple processes from vascular bedside to liver as evidenced by nitric oxide production or paraoxonase levels.

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Source
http://dx.doi.org/10.2741/3071DOI Listing

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