Introduction Department Genetics of Model Diseases

Genetics of Model Diseases

Metabolic syndrome is a cluster of several risk factors for type 2 diabetes and cardiovascular disease, including obesity, hypertension, insulin resistance, and dyslipidemia. These pathological conditions are determined multifactorially by many genes and their interactions with environmental effects. Genome wide association studies (GWAS) in humans which are based on the “common variants – common diseases“ hypothesis identified only a minor proportion of the total heritability of complex traits so far.

Statistically significant variants (SNPs – single nucleotide polymorphisms) are typically associated with a miniscule phenotypic variability without meaningful clinical effects. Studies in animal models of human complex diseases can provide a useful alternative. Experiments with rat models can control for both genetic background and environmental effects as well as enable genetic manipulation of experimental animals. The spontaneously hypertensive rat (SHR) is the most widely used animal model of essential hypertension and associated metabolic disturbances typical for metabolic syndrome. Although it cannot be expected that the individual predisposing genes themselves might be conserved between rats and humans, it is likely that the networks and pathways of genes leading to disease susceptibility will be conserved across species. Therefore, identification of the networks and pathways of genes underlying the cellular pathology of disease phenotypes in the rat could provide insight into the pathogenesis and treatment of the corresponding human diseases.

Our research is focused on these projects:

Identification of genes that regulate hemodynamic and metabolic traits in the SHR.
Identification of new genes coding for mitochondrial proteins and their role in the pathogenesis of metabolic syndrome.
Derivation of new animal models using highly effective methods for transgenesis and gene targeting.
Study of the role of inflammatory processes and oxidative stress in the pathogenesis of metabolic syndrome and possibility of pharmacologic interventions.

Current grant support.

Projects

Development of new efficient methods for transgenesis and gene targeting in the rat

Recently, new highly efficient techniques become available for derivation of transgenic or knockout rats for in vivo functional studies of candidate genes for QTL, for analyses of genes with unknown function or for derivation of new rat models of human diseases. More

Linkage and correlation analyses of intermediary phenotypes in the SHR for identification of candidate genes regulating pathophysiological traits

For genetic dissection of complex pathophysiological traits in recombinant inbred (RI) strains, it is possible to take the advantage of accumulated genotypes and intermediary phenotypes. Intermediate phenotypes have simpler genetic architectures and can be used for connecting variabilty at the DNA level with complex pathophysiological traits. Abundance of mRNA (transcriptome), proteins (proteome), metabolites (metabolome), etc. are the most widely used intermediary phenotypes. More

In vivo functional analyses of candidate genes for hemodynamic and metabolic traits

Candidate genes for pathophysiological traits, identified by linkage and correlation analyses with intermediary phenotypes and by their sequencing, are tested by in vivo functional analysis in transgenic rescue or knockout experiments with the aim to identify quantitative trait loci at the molecular level and analyze responsible pathophysiological mechanisms. More

Genetic and correlation analyses of mitochondrial proteome

We plan to identify genetic determinants of the mitochondrial proteome in relation to important complex disease traits in the rat and thereby improve understanding of the pathogenetic role of mitochondria in common clinical disorders. More

Publications

Šilhavý, Jan - Mlejnek, Petr - Šimáková, Miroslava - Vaněčková, Ivana - Behuliak, Michal - Kuda, Ondřej - Sticová, E. - Jirsa, M. - Pravenec, Michal . Acute toxic effects of telmisartan in spontaneously hypertensive rats fed a high fructose diet . Physiological Research 2018, 67(6), 851-856 . IF = 1.324 [ASEP]

Šilhavý, Jan - Krijt, J. - Sokolová, J. - Zídek, Václav - Mlejnek, Petr - Šimáková, Miroslava - Škop, V. - Trnovská, J. - Oliyarnyk, O. - Marková, I. - Hüttl, M. - Malínská, H. - Kazdová, L. - Liška, F. - Kožich, V. - Pravenec, Michal . Dissecting the role of Folr1 and Folh1 genes in the pathogenesis of metabolic syndrome in spontaneously hypertensive rats . Physiological Research 2018, 67(4), 657-662 . IF = 1.324 [ASEP]

Pravenec, Michal - Saba, L. M. - Zídek, Václav - Landa, Vladimír - Mlejnek, Petr - Šilhavý, Jan - Šimáková, Miroslava - Strnad, Hynek - Trnovská, J. - Škop, V. - Hüttl, M. - Marková, I. - Oliyarnyk, O. - Malínská, H. - Kazdová, L. - Smith, H. - Tabakoff, B. Systems genetic analysis of brown adipose tissue function . Physiological Genomics 2018, roč. 50, 1, p. 52-66 . IF = 2.782 [ASEP] [ doi ]

Pravenec, Michal - Leung, K.-Y. - Zídek, Václav - Mlejnek, Petr - Šimáková, Miroslava - Šilhavý, Jan - Kožich, V. - Greene, N. D. E. Genetically Determined Folate Deficiency Is Associated With Abnormal Hepatic Folate Profiles in the Spontaneously Hypertensive Rat . Physiological Research 2018, roč. 67, 3, p. 417-422 . IF = 1.324 [ASEP]

Nedvědová, I. - Kolář, D. - Elsnicová, B. - Horníková, D. - Novotný, J. - Kalous, M. - Pravenec, Michal - Neckář, Jan - Kolář, František - Žurmanová, J.M. Mitochondrial genome modulates myocardial Akt/Glut/HK salvage pathway in spontaneously hypertensive rats adapted to chronic hypoxia . Physiological Genomics 2018, roč. 50, 7, p. 532-541 . IF = 2.782 [ASEP] [ doi ]

Manakov, D. - Kolář, D. - Žurmanová, J. - Pravenec, Michal - Novotný, J. Changes in the activity of some metabolic enzymes in the heart of SHR rat incurred by transgenic expression of CD36 . Journal of Physiology and Biochemistry 2018, roč. 74, 3, p. 479-489 . IF = 2.736 [ASEP] [ doi ]

Lusk, R. - Saba, L. M. - Vanderlinden, L. A. - Zídek, Václav - Šilhavý, Jan - Pravenec, Michal - Hoffman, P.L. - Tabakoff, B. Unsupervised, Statistically Based Systems Biology Approach for Unraveling the Genetics of Complex Traits: A Demonstration with Ethanol Metabolism . Alcoholism-Clinical and Experimental Research 2018, roč. 42, 7, p. 1177-1191 . IF = 3.183 [ASEP] [ doi ]

Kurtz, T. W. - DiCarlo, S. E. - Pravenec, Michal - Morris, R. C. Functional foods for augmenting nitric oxide activity and reducing the risk for salt-induced hypertension and cardiovascular disease in Japan . Journal of Cardiology 2018, roč. 72, 1, p. 42-49 . IF = 2.918 [ASEP] [ doi ]

Kurtz, T. W. - DiCarlo, S. E. - Pravenec, Michal - Morris Jr., R. C. Mechanisms of salt sensitivity of blood pressure: an unbiased approach to skinning a cat Reply . Journal of Hypertension 2018, roč. 36, 3, p. 703-704 . IF = 4.092 [ASEP] [ doi ]

Kurtz, T. W. - DiCarlo, S. E. - Pravenec, Michal - Morris Jr., R. C. The pivotal role of renal vasodysfunction in salt sensitivity and the initiation of salt-induced hypertension . Current Opinion in Nephrology and Hypertension 2018, roč. 27, 2, p. 83-92 . IF = 3.370 [ASEP] [ doi ]

Contacts

Institute of Physiology AS CR, v.v.i.
Department of Genetics of Model Diseases
Vídeňská 1083
14220 Prague 4

Czech Republic

tel.	+420 241 062 297
fax.	+420 241 062 488

pravenec@fgu.cas.cz

People

	Ing. Michal Pravenec, DrSc. head of the department
	Ing. Jan Šilhavý, PhD. deputy head of the department
	Ing. Václav Zídek, CSc. senior researcher
	Ing. Miroslava Šimáková, PhD. senior researcher
	Ing. Petr Mlejnek, PhD. senior researcher
	doc. MUDr. František Liška, PhD. senior researcher
	Ing. Magdalena Melčová PhD student
	Alena Musilová technician