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Patogeneze klíšťové encefalitidy a její ovlivnění genetickým pozadím hostitele / The role of genetic background of the host on the pathogenesis of tick-borne encephalitisPALUS, Martin January 2011 (has links)
We examined the influence of the host genetic background on the pathogenesis of tick-borne encephalitis. We determined virus titers in organs and serum in different time intervals post-infection for different ways of inoculation. We also stated mean survival times and antibody production in different strains of mice infected with tick-borne encephalitis virus. Moreover, differences in expression of immunologicaly important genes in brains of infected mice were compared.
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O efeito da infecção por Toxoplasma gondii em camundongos gestantes CB10-H2 (H-2b) e C57BL/KsJ (H-2d)Coutinho, Loyane Bertagnolli 29 February 2016 (has links)
Successful pregnancy is related to Th2 immune response profile, including molecules encoded by the major histocompatibility complex (MHC); however, Toxoplasma gondii infection induces Th1 immune response that is associated with adverse pregnancy outcome. To investigate the influence of MHC haplotype in pregnancy outcome in T. gondii-infected animals, congenic mice, C57BL/KsJ and CB10-H2 females, were orally infected with ME-49 strain on the first day of pregnancy and sacrificed on 8 and 18 days post-infection. C57BL/KsJ showed higher number of parasites in the lungs at 8dI, irrespective of pregnancy, compared with CB10-H2; and both CB10-H2 and C57BL/KsJ showed high number of parasites in the brain at 18dI, irrespective of pregnancy. Parasites were not found in the uterus/placenta in both lineages of mice irrespective of the day of infection and there was no difference in abortion rate of infected mice, although CB10-H2 mice presented higher histological damage compared with C57BL/KsJ at 8 and 18 days of pregnancy and infection. Infection of non-pregnant C57BL/KsJ increased mast cell infiltration in the uterus, and gestation decreased this cell numbers. Furthermore, C57BL/KsJ presented higher IFN-γ levels systemically on 8dI; and TNF and IL-6 on 8 and 18dI compared with CB10-H2, despite gestation or not. Additionally, in the uterus/placenta of CB10-H2, pregnancy increased FOXP3 and under infection IL-10, IL-13 and IL-17 expression levels. Our data suggest that both genetic background and MHC haplotypes are essential to protect against reabsorption rate and abortion in congenital toxoplasmosis. / O sucesso da gestação está relacionado com um perfil de resposta imunológica tipo Th2 e envolvimento de vários mecanismos para manutenção da tolerância materno-fetal, incluindo as moléculas codificadas pelo complexo principal de histocompatibilidade (MHC). Entretanto, a infecção por Toxoplasma gondii induz um perfil de resposta tipo Th1 que é associada aos resultados prejudiciais da gestação. Para investigar a influência do haplotipo do MHC na toxoplasmose congênita, fêmeas de camundongos congênicos, C57BL/KsJ (H-2d) e CB10-H2 (H-2b) foram oralmente infectadas com 5 cistos da cepa ME-49 no primeiro dia de gestação e sacrificadas aos 8 e 18 dias após a infecção. As fêmeas C57BL/KsJ apresentaram alto número de parasitos nos pulmões aos 8dI, comparadas às fêmeas CB10-H2 e ambas as linhagens apresentaram alto número de parasitos no cérebro aos 18dI, independentemente da gestação. Não foram encontrados parasitos no útero/placenta em nenhuma das linhagens, independente do tempo de infecção e não houve diferença no índice de aborto dentre as fêmeas infectadas, apesar da linhagem CB10-H2 ter apresentado maiores danos histológicos comparada à C57BL/KsJ aos 8 e 18 dias de gestação e infecção. A infecção nas fêmeas C57BL/KsJ não-gestantes provocou aumento na migração de mastócitos para o útero enquanto que a gestação diminui tal migração. Além disso, camundongos C57BL/KsJ apresentaram altos níveis sistêmicos de IFN-γ aos 8dI e TNF e IL-6 aos 8 e 18dI comparados aos CB10-H2 gestantes e não-gestantes. Ainda, no útero/placenta das fêmeas CB10-H2 a gestação aumentou os níveis de expressão de FOXP3 e, sob a infecção, houve aumento no nível de expressão de IL-10, IL-13 e IL-17. Nossos resultados sugerem que, tanto o background genético como o haplotipo do MHC sejam essenciais na proteção contra os índices de reabsorção fetal e aborto nos casos de toxoplasmose congênita. / Doutor em Imunologia e Parasitologia Aplicadas
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Mapping and CRISPR/Cas9 Gene Editing for Identifying Novel Genomic Factors Influencing Blood PressureWaghulde, Harshal B. January 2016 (has links)
No description available.
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Identificação e análise estrutural e funcional de genes candidatos do cromossomo 4 de ratos SHR que possam influenciar a hipertensão essencial / Identification and structural and functional analysis of candidate genes on chromosome 4 in SHR that may influence essential hypertensionTeixeira, Samantha Kuwada 10 December 2013 (has links)
O emprego de \"Total Genome Scan\" em modelos genéticos de doenças complexas tem sido fundamental para seleção de regiões cromossômicas envolvidas com traços complexos. Em nosso laboratório, identificamos cinco regiões cromossômicas associadas ao traço quantitativo pressão arterial (BP-QTL) que explicam 43% da variação da pressão arterial numa progênie obtida a partir de animais espontaneamente hipertensos (SHR) e \"Brown Norway\" (BN). Os BP-QTLs foram, então, validados por desenvolvimento de linhagens congênicas, incluindo uma para o cromossomo 4 (SHR.BN4) cuja substituição das sequências SHR pelo do animal BN levou a redução da pressão arterial sistólica basal (~14 mm Hg). O objetivo deste trabalho foi identificar as variantes genéticas candidatas neste intervalo cromossômico com base em diferenças no padrão de expressão gênica e na presença de alterações genéticas não sinônimas \"missense\" ou em regiões regulatórias conservadas que possam estar envolvidas na gênese da hipertensão. Identificamos 533 genes com expressão renal, dentre os 682 do intervalo, sendo que 28 apresentaram padrão de expressão diferente entre amostras de animais adultos (congênico vs. SHR) e seis apresentaram alterações não sinônimas \"missense\". É importante salientar que dos genes diferentemente expressos, encontramos alterações estruturais em regiões conservadas com potencial de participar na regulação em 11. Em conjunto, utilizamos uma plataforma integrada para selecionar 34 genes candidatos no cromossomo 4, dos quais 17 genes serão priorizados, para ser investigados quanto sua contribuição na hipertensão arterial do SHR e na hipertensão primária humana / Total genome scan in genetic models of complex diseases have been instrumental to select candidate genes underlying complex traits. We previously mapped 5 blood pressure related quantitative trait loci (BP-QTLs) that explain about 43% of the BP variance in a progeny derived from Spontaneous Hypertensive Rat (SHR) and Brown Norway (BN) rats. The BP-QTLs were then validated by derivation of congenic strains, including one for chromosome 4 (SHR.BN4) in which a segment from BN replaced the SHR sequences reducing basal systolic BP (~14 mm Hg). The aim of this project is to identify the candidate genetic variants within the chromosome interval based on differences in renal gene expression patterns and structural changes in both non-synonymous missense or within adjacent regulatory sequences that may contribute to hypertension. We identified 533 genes with renal expression, out of 682 in the interval, in which 28 presented differences in expression pattern in adult samples (congenic vs. SHR) and six presented non-synonymous missense alterations. In addition, 11 out of 28 differentially expressed genes showed structural alterations in adjacent conserved regions that potentially contribute to gene regulation. Taken together, using the proposed combination of strategies, we selected 34 hypertensive candidate genes in chromosome 4, in which 17 will be prioritized, to be further explored to assess their contribution to hypertension in the SHR and to essential hypertension in humans
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Identificação e análise estrutural e funcional de genes candidatos do cromossomo 4 de ratos SHR que possam influenciar a hipertensão essencial / Identification and structural and functional analysis of candidate genes on chromosome 4 in SHR that may influence essential hypertensionSamantha Kuwada Teixeira 10 December 2013 (has links)
O emprego de \"Total Genome Scan\" em modelos genéticos de doenças complexas tem sido fundamental para seleção de regiões cromossômicas envolvidas com traços complexos. Em nosso laboratório, identificamos cinco regiões cromossômicas associadas ao traço quantitativo pressão arterial (BP-QTL) que explicam 43% da variação da pressão arterial numa progênie obtida a partir de animais espontaneamente hipertensos (SHR) e \"Brown Norway\" (BN). Os BP-QTLs foram, então, validados por desenvolvimento de linhagens congênicas, incluindo uma para o cromossomo 4 (SHR.BN4) cuja substituição das sequências SHR pelo do animal BN levou a redução da pressão arterial sistólica basal (~14 mm Hg). O objetivo deste trabalho foi identificar as variantes genéticas candidatas neste intervalo cromossômico com base em diferenças no padrão de expressão gênica e na presença de alterações genéticas não sinônimas \"missense\" ou em regiões regulatórias conservadas que possam estar envolvidas na gênese da hipertensão. Identificamos 533 genes com expressão renal, dentre os 682 do intervalo, sendo que 28 apresentaram padrão de expressão diferente entre amostras de animais adultos (congênico vs. SHR) e seis apresentaram alterações não sinônimas \"missense\". É importante salientar que dos genes diferentemente expressos, encontramos alterações estruturais em regiões conservadas com potencial de participar na regulação em 11. Em conjunto, utilizamos uma plataforma integrada para selecionar 34 genes candidatos no cromossomo 4, dos quais 17 genes serão priorizados, para ser investigados quanto sua contribuição na hipertensão arterial do SHR e na hipertensão primária humana / Total genome scan in genetic models of complex diseases have been instrumental to select candidate genes underlying complex traits. We previously mapped 5 blood pressure related quantitative trait loci (BP-QTLs) that explain about 43% of the BP variance in a progeny derived from Spontaneous Hypertensive Rat (SHR) and Brown Norway (BN) rats. The BP-QTLs were then validated by derivation of congenic strains, including one for chromosome 4 (SHR.BN4) in which a segment from BN replaced the SHR sequences reducing basal systolic BP (~14 mm Hg). The aim of this project is to identify the candidate genetic variants within the chromosome interval based on differences in renal gene expression patterns and structural changes in both non-synonymous missense or within adjacent regulatory sequences that may contribute to hypertension. We identified 533 genes with renal expression, out of 682 in the interval, in which 28 presented differences in expression pattern in adult samples (congenic vs. SHR) and six presented non-synonymous missense alterations. In addition, 11 out of 28 differentially expressed genes showed structural alterations in adjacent conserved regions that potentially contribute to gene regulation. Taken together, using the proposed combination of strategies, we selected 34 hypertensive candidate genes in chromosome 4, in which 17 will be prioritized, to be further explored to assess their contribution to hypertension in the SHR and to essential hypertension in humans
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Funkčně genomická a farmakogenomická analýza aspektů metabolického syndromu / Functional genomic and pharmacogenomic analysis of metabolic syndrome aspectsKrupková, Michaela January 2014 (has links)
Metabolic syndrome is a prevalent disease characterized by concurrent manifestation of insulin resistance, obesity, dyslipidemia, hypertension and other hemodynamic and metabolic disorders. It has multifactorial type of inheritance and its resultant phenotype is determined by both environmental and genetic factors as well as their interactions. That is the main reason why comprehensive analysis of the genetic component of this syndrome is complicated in human population. Genetically designed experimental animal models are significant tools for analysis of genetic architecture of human complex conditions including the metabolic syndrome. The aim of this Thesis is utilization of functional and comparative genomic tools to uncover pathogenesis of metabolic syndrome aspects and their genetic determinants. We also studied pharmacogenetic interactions of these genetic determinants with drugs affecting particular components of the metabolic syndrome. Establishing and utilizing several genetically designed congenic rat strains, we undertook four different research projects focusing on pharmacogenetic interaction of all-trans retinoic acid and ondansetron with differential segment of rat chromosome 8, pharmacogenetic interaction of differential segment of rat chromosome 4 and dexamethasone, determining Plzf...
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Funkčně genomická a farmakogenomická analýza aspektů metabolického syndromu / Functional genomic and pharmacogenomic analysis of metabolic syndrome aspectsKrupková, Michaela January 2014 (has links)
Metabolic syndrome is a prevalent disease characterized by concurrent manifestation of insulin resistance, obesity, dyslipidemia, hypertension and other hemodynamic and metabolic disorders. It has multifactorial type of inheritance and its resultant phenotype is determined by both environmental and genetic factors as well as their interactions. That is the main reason why comprehensive analysis of the genetic component of this syndrome is complicated in human population. Genetically designed experimental animal models are significant tools for analysis of genetic architecture of human complex conditions including the metabolic syndrome. The aim of this Thesis is utilization of functional and comparative genomic tools to uncover pathogenesis of metabolic syndrome aspects and their genetic determinants. We also studied pharmacogenetic interactions of these genetic determinants with drugs affecting particular components of the metabolic syndrome. Establishing and utilizing several genetically designed congenic rat strains, we undertook four different research projects focusing on pharmacogenetic interaction of all-trans retinoic acid and ondansetron with differential segment of rat chromosome 8, pharmacogenetic interaction of differential segment of rat chromosome 4 and dexamethasone, determining Plzf...
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Defining Mutation-Specific NRAS Functions that Drive MelanomagenesisMurphy, Brandon M. January 2021 (has links)
No description available.
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L’impact du locus Idd2 dans la susceptibilité au diabète auto-immunCaron, Laurence 02 1900 (has links)
Le diabète de type 1 (DT1) est une maladie auto-immune caractérisée par la destruction des cellules β pancréatiques par les cellules immunitaires, ce qui entraîne une insuffisance en insuline. L’étude des souris Non-Obese Diabetic (NOD), qui développent spontanément le diabète auto-immun, a permis l'identification de plusieurs loci de susceptibilité associés au diabète, appelés Idds. D’ailleurs, Idd1 est lié au locus du CMH. L’utilisation de souris congéniques NOD.B6-Idd1 et B6.NOD-Idd1 a démontré qu’Idd1 est nécessaire mais insuffisant pour la progression du diabète auto-immun. Précédemment, nous avons démontré que les allèles de résistance au locus Idd2 offrent une protection significative contre l’apparition du diabète auto-immun, semblable à Idd1. Pour identifier les facteurs génétiques minimaux requis pour l'apparition du DT1, nous avons introduit les loci NOD Idd1 et Idd2 chez des souris B6, générant des souris doubles congéniques B6.Idd1.Idd2. Bien que la combinaison de Idd1 et Idd2 n’est pas suffisante pour induire l’apparition du diabète, nous avons observé une infiltration immunitaire dans le pancréas exocrine des souches congéniques B6 Idd2. De plus, nous avons observé d'importantes différences phénotypiques dans les sous-populations de lymphocytes T chez les souris B6.Idd1.Idd2 par rapport aux souris simple congéniques, suggérant une interaction épistatique entre Idd1 et Idd2 dans la modulation des fonctions des lymphocytes T. De plus, des augmentations de neutrophiles et de la fibrose spécifiques à Idd2 ont été découvertes, suggérant qu’Idd2 est impliqué dans le processus cellulaire inflammatoire du diabète auto-immun. Dans l’ensemble, ces données montrent que la combinaison des allèles de susceptibilité Idd1 et Idd2 ne mène pas à la progression du diabète auto-immun. Des facteurs génétiques ou environnementaux supplémentaires sont donc nécessaires pour provoquer le diabète auto-immun chez la souris. Néanmoins, nous constatons que les allèles NOD au niveau des locus Idd2 coopèrent pour induire une inflammation et une infiltration immunitaire dans le pancréas. / Type 1 diabetes (T1D) is an autoimmune disease characterized by the destruction of pancreatic β cells by immune cells, leading to an insulin deficiency. Non-Obese Diabetic (NOD) mice, which spontaneously develop autoimmune diabetes, have enabled the identification of several loci associated with diabetes susceptibility, termed Idds. Notably, Idd1 is linked to the MHC locus and resistance alleles at this locus provide full protection from diabetes onset. Conversely, C57BL/6 (B6) mice bearing NOD Idd1 alleles exhibit immune infiltration in the pancreas without causing overt diabetes. These results show that NOD Idd1 alleles are necessary but not sufficient for autoimmune diabetes progression. In a previous study, we demonstrated that diabetes resistance alleles at the Idd2 locus provide significant protection from autoimmune diabetes onset, second to Idd1. To identify the minimal genetic factors required for T1D onset, we introduced the NOD Idd1 and Idd2 loci in B6 mice, generating B6.Idd1.Idd2 double congenic mice. Although the introduction of susceptibility alleles at both Idd1 and Idd2 was not sufficient to induce diabetes onset, we observed immune infiltration in the exocrine pancreas of B6 Idd2 congenic strains. In addition, we observed important phenotypic differences in T cell subsets in B6.Idd1.Idd2 mice relative to single congenic mice, suggesting epistatic interaction between Idd1 and Idd2 in modulating T cell functions. Moreover, Idd2-specific increases in neutrophils and fibrosis were discovered, suggesting that Idd2 is involved in the inflammatory cellular process of autoimmune diabetes. Altogether, these data show that susceptibility alleles at Idd1 and Idd2 together are not sufficient to autoimmune diabetes progression. Additional genetic factors or environmental triggers are therefore required to cause autoimmune diabetes in mice. Still, we find that NOD alleles at the Idd2 loci cooperate to induce inflammation and immune infiltration in the pancreas.
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Évaluation neurobiologique des souris spontanément hypertendues : Du vieillissement à la génomique comparativeThifault, Stéphane 12 1900 (has links)
Le but de cette thèse est premièrement d’évaluer l’effet du vieillissement sur les fonctions psychomotrices des souches de souris sélectionnées génétiquement en fonction de leur tension artérielle (TA); deuxièmement, de localiser les déterminants génétiques des phénotypes psychophysiologiques à partir de souches recombinantes congéniques (RCS). Ces travaux ont mené à la publication de 4 articles. Le premier article décrit l’évaluation des fonctions psychomotrices des souches avec une tension artérielle élevée (HBP), basse (LBP) et normale (NBP). La performance aux épreuves d’exploration, d’habiletés motrices et d’apprentissage spatial, a été mesurée sur deux cohortes âgées respectivement de 12 mois et de trois mois. Indépendamment de l’âge, les HBPs sont hyperactives dans l’open-field (OF), mais pas dans le test d’exploration de trous. Inversement, les LBP explorent moins d’espaces que les NBP et, à trois mois seulement, sont hypoactives dans l’OF. Par ailleurs, les HBPs et les LBP présentent des déficits précoces de coordination motrice et des fonctions visuo-motrices. Le second article concerne l’évaluation longitudinale de la coordination motrice, de l’anxiété et de l’apprentissage spatial des souches HBP, LBP et NBP, à l’âge de deux mois et de 12 mois. Le vieillissement accentue l’hyperactivité des HBPs dans l’OF. Par contre, l’hypoactivité des souris LBP est détectable seulement à l’âge de deux mois. Indépendamment de l’âge, les souris HBP et LBP montrent une perception réduite du danger dans l’épreuve d’anxiété et des dysfonctions visuo-motrices au labyrinthe aquatique. Enfin, des déficits précoces de coordination motrice se manifestent seulement chez les HBPs. Il reste à déterminer si les déficits observés sont liés à des déterminants génétiques indépendants ou secondaires aux altérations de la tension artérielle. Le troisième article présente la comparaison entre les souches consanguines A/J et C57Bl/6J (B6) aux épreuves de l’OF, de la planche à trous, du labyrinthe aquatique et du cintre (coordination motrice). Les B6 explore d’avantage l’OF et la planche à trous. Les B6 sont moins rapides sur le cintre, mais supérieurs aux A/J dans le labyrinthe aquatique, avec une plate-forme invisible ou visible. Ces résultats démontrent l’implication de déterminants génétiques.
Cette thèse se termine par un quatrième article sur la localisation des déterminants génétiques de la susceptibilité au stress dans les RCS, dérivées de A/J et B6, et présentant un agencement spécifique de 12.5% du génome. La réactivité émotionnelle est évaluée dans l’OF et le plus-maze; la réponse de stress est mesurée par radio télémétrie de la température interne pendant le stress d’immobilisation (SI) sous diète régulière et riche en sel; l’excrétion des électrolytes urinaires est dosée après 24 heures de diète salée. Les loci les plus significatifs sont situés dans les régions suivantes: de l’émotionalité dans l’OF (Emo1) sur le chr. 1 (LOD=4.6) correspondant à la région homologue impliquée dans la cohorte d’hypertension familiale du Saguenay; de la dopa décarboxylase (ddc) sur le chr. 11 pour l’émergence du plus-maze (LOD=4.7); de la protéine liant l’endotoxine (lbp) sur le chr. 2 pour l’hypothermie initiale en réponse au SI (LOD=4); et de HSP90 sur le chr. 12 pour l’excrétion de Ca++ (LOD=4.6). Des banques de données sont ensuite interrogées pour recenser les polymorphismes des régions régulatrices ou codantes des gènes candidats chez les souches ancestrales A/J et B6, dont les séquences sont disponibles pour le génome entier. Des utilitaires web permettent de dévoiler les changements dans la structure secondaire de l’ARNm, l’interférence avec des microARN ou avec d’autres motifs de liaison. Plusieurs SNPs fonctionnels ont été identifiés pour le QTL du chr. 1, particulièrement dans les éléments de régulation; ceux-ci impliquant des gènes reliés avec les réponses inflammatoire/immunitaire ou avec le système cardiovasculaire. La quantification par la PCR confirme une régulation à la baisse d’atp1a2 dans le cœur et le cerveau des souches susceptibles à l’anxiété. Ces résultats confirment l’intrication des altérations de la susceptibilité au stress et de la régulation de la TA. / Our studies in this thesis, which led to 4 publications, are divided in two parts. The first part describes the neuropsychological effects of aging in strains of mice genetically selected for high (HBP), low (LBP) or normal blood pressure (NBP). The second part focuses on the genetic determinants of these neuropsychological phenotypes in recombinant congenic strains (RCS) of mice. The first manuscript compares HBP or LBP mice to normotensive controls in tests of exploration, motor coordination, and spatial learning at two age levels: 3 and 12 months. At either age, HBPs were hyperactive in an open field (OF) but not in terms of hole-poking responses. On the contrary, LBPs were hypoactive in the OF and in the hole-board, with the effect on the former measure being limited to the younger cohort. In either cohort, HBP and LBP mice were deficient in subtle aspects of motor coordination, and visuomotor function. These strains may serve as experimental models for the evaluation of beneficial early antihypertensive or antihypotensive treatments on brain function. The second study uses a longitudinal design to compare either HBP or LBP mice to normotensive controls at 2 and 12 months of age for motor coordination, anxiety, and spatial learning. Hyperactivity of HBPs in the OF increased with aging; whereas LBP mice were hypoactive only at 2 months of age. At both age, HBP and LBP mice displayed reduced levels of anxiety in the elevated plus-maze (EPM), abnormal coordination and visuomotor guidance. It remains to determine if these strain-, age-, and test-specific abnormalities are genetically related or secondary to uncontrolled hypertension or hypotension. The following article compares the C57BL/6J (B6) to the A/J inbred mouse strain in exploration of the OF and the hole-board, in the coat-hanger coordination test, and in spatial learning of a water maze. B6 mice displayed a higher number of segment crossings in the open-field and of hole-poking responses than A/J mice. By contrast to their hypo activity, A/J strain were faster in the coat-hanger motor test, but deficient in the submerged but also in the visible platform version of the water maze. These results indicate the considerable potential of genetic models derived from B6 and A/J mice for discerning the determinants of several behavioural phenotypes.
In the last manuscript, the genomic loci bearing stress-related phenotypes were dissected by genome wide analysis of linkage in the recombinant congenic strains (RCS), resulting from a cross of B6 and A/J progenitors, each strain bearing 12.5% of specific parts of one progenitor on the background of the other. Adult male mice from 14 A/J and 22 B6 background lines were evaluated for emotional reactivity in the OF and the EPM. Core temperature was monitored by radio-telemetry during immobilization (IM), under standard and salt-enriched diets. In addition, urinary electrolytes were measured. The highest LOD scores strengthen the evidence for a previously reported locus for emotionality in the open-field on Chr 1 (LOD=4.6), in the Ddc region encoding dopa decarboxylase, on Chr 11 in the EPM (LOD=4.7), near Lbp (lipopolysaccharide binding protein), on Chr 2 for initial hypothermia during IM (LOD=4), as well as in the region of Hspca, encoding heat shock protein 1 alpha (48.0 cM) on Chr 12 for Ca++ excretion after a 24 hr-salt load (LOD=4.6). RCS stress QTL overlapped with several candidate loci for cardiovascular disease. In silico evidence of functional polymorphisms by comparative sequence analysis of progenitor strains assisted to ascertain this convergence, then further tested using quantitative PCR for releant genes mRNA. The anxious BcA70 strain showed down regulation of the Atp1a2 gene expression in the heart (P < 0.001) and brain (P < 0.05) compared to its parental B6 strain, compatible with the enhanced emotionality described in knock out animals for this gene, also involved in the salt-sensitive component of hypertension. Functional polymorphisms in regulatory elements of candidate genes of the cardiovascular / inflammatory / immune systems support the hypothesis of genetically-altered environmental susceptibility in cardiovascular disease development.
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