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Electroacupuncture lowers high blood pressureDong, Siwei 08 April 2016 (has links)
OBJECTIVE: To determine if applying electroacupuncture at ST 36-37 will lower the systolic, diastolic, and mean blood pressures of chronic hypertensive rats.
DESIGN: A 12 week study on the effect of electroacupuncture was conducted from September 2014 to December 2014. The total number of rats used in the study was 16 (n=16). The rats were divided into four groups: Electroacupuncture, Sham-EA, Hypertensive control, and Normotensive control. All of the rats, expect for those in the Normotensive group, were housed in the cold room to induce chronic hypertension. After 8 weeks in the cold room, the rats in the Electroacupuncture group received electrical stimulation twice a week for 30 min. Needles were also inserted into the rats in the Sham-EA group, but there was no electric current. The blood pressures of all of the rats were measured once a week for 12 weeks. Lastly, the data was analyzed using SigmaStat to perform One Way ANOVA and T-tests.
RESULT: The initial blood pressures between the 4 groups were similar with a difference of less than 5 mmHg. The groups placed in cold rooms showed a significant difference of more than 20 mmHg compared to their initial blood pressures (P≤0.05) at week 7. Finally, the blood pressures of the Sham-EA and Hypertensive control group did not lower at 12 weeks compared to week 7. However, the systolic, mean, and diastolic blood pressures in the EA group lowered with a significant difference of greater than 20 mmHg at week 12 compared to week 7. There was no significant change between the initial and final blood pressures for those in the Normotensive group.
CONCLUSION: The data showed that systolic, diastolic, and mean blood pressures in the Electroacupuncture group lowered significantly at week 12 or after 5 weeks of treatment. Thus, we can conclude that electroacupuncture does have a beneficial effect in lowering blood pressure in chronically hypertensive rats.
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Chronic Hypertension and Pregnancy : Epidemiological Aspects on Maternal and Perinatal ComplicationsZetterström, Karin January 2007 (has links)
<p>These studies were undertaken to investigate risks of maternal and perinatal complications in pregnant women with chronic hypertensive disease, and to investigate future risk of preeclampsia in women born small for gestational age (SGA). Population based cohort studies using the Swedish Medical Birth Register from different years were performed.</p><p>The maternal complications mild and severe preeclampsia, gestational diabetes and abruptio placenta were studied in a population of 681 515 women, with a prevalence of 0,5% for chronic hypertension. Risk estimates were adjusted for differences in maternal characteristics as age, parity, BMI, ethnicity and smoking habits. Chronic hypertensive women wore found to have significantly increased risks of all complications. </p><p>The perinatal complication SGA was studied in a population of 560 188, with a prevalence of 0,5% for chronic hypertension. Risk estimates were adjusted for differences in maternal characteristics and for the secondary complications mild and severe preeclampsia. Chronic hypertensive women were found to suffer a significantly increased risk of giving birth to an offspring that is SGA. </p><p>The perinatal complication fetal/infant mortality was studied in a population of 1 222 952 with a prevalence of 0,6% for chronic hypertension. Risk estimates were adjusted for differences in maternal characteristics and for the complications mild and severe preeclampsia, gestational diabetes, abruptio placenta and offspring being SGA In the analysis an effect modification by gender was included. Chronic hypertensive women were found to have a significantly increased risk for stillbirth and neonatal death in male, but not in female, offspring. Thus a clear gender difference in mortality was revealed. The risk of mortality of offspring was mediated by severe preeclampsia, abruptio placenta and offspring being SGA. Mild preeclampsia and gestational diabetes did not affect the risk. No increased risk of post neonatal mortality was found.</p><p>A generation study was performed in 118 634 girls of which 5.8% were born SGA. Their future risk for mild and severe preeclampsia in first pregnancy was analysed. Risk estimates were adjusted for age, smoking, BMI and for preeclampsia in the mothers while pregnant with the study population. Women who were born SGA were shown to have a significantly increased risk for severe preeclampsia, but not for mild preeclampsia. </p>
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Chronic Hypertension and Pregnancy : Epidemiological Aspects on Maternal and Perinatal ComplicationsZetterström, Karin January 2007 (has links)
These studies were undertaken to investigate risks of maternal and perinatal complications in pregnant women with chronic hypertensive disease, and to investigate future risk of preeclampsia in women born small for gestational age (SGA). Population based cohort studies using the Swedish Medical Birth Register from different years were performed. The maternal complications mild and severe preeclampsia, gestational diabetes and abruptio placenta were studied in a population of 681 515 women, with a prevalence of 0,5% for chronic hypertension. Risk estimates were adjusted for differences in maternal characteristics as age, parity, BMI, ethnicity and smoking habits. Chronic hypertensive women wore found to have significantly increased risks of all complications. The perinatal complication SGA was studied in a population of 560 188, with a prevalence of 0,5% for chronic hypertension. Risk estimates were adjusted for differences in maternal characteristics and for the secondary complications mild and severe preeclampsia. Chronic hypertensive women were found to suffer a significantly increased risk of giving birth to an offspring that is SGA. The perinatal complication fetal/infant mortality was studied in a population of 1 222 952 with a prevalence of 0,6% for chronic hypertension. Risk estimates were adjusted for differences in maternal characteristics and for the complications mild and severe preeclampsia, gestational diabetes, abruptio placenta and offspring being SGA In the analysis an effect modification by gender was included. Chronic hypertensive women were found to have a significantly increased risk for stillbirth and neonatal death in male, but not in female, offspring. Thus a clear gender difference in mortality was revealed. The risk of mortality of offspring was mediated by severe preeclampsia, abruptio placenta and offspring being SGA. Mild preeclampsia and gestational diabetes did not affect the risk. No increased risk of post neonatal mortality was found. A generation study was performed in 118 634 girls of which 5.8% were born SGA. Their future risk for mild and severe preeclampsia in first pregnancy was analysed. Risk estimates were adjusted for age, smoking, BMI and for preeclampsia in the mothers while pregnant with the study population. Women who were born SGA were shown to have a significantly increased risk for severe preeclampsia, but not for mild preeclampsia.
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Effect of exercise training on preeclampsia superimposed on chronic hypertension in a mouse modelGenest, Suzanne Dominique 08 1900 (has links)
Preeclampsia is among the leading causes of perinatal mortality and morbidity, affecting 2-7% of pregnancies. Its incidence increases to 10-25% in already hypertensive women. To date, no treatment, aside from delivery, is known. Interestingly, several studies have reported that exercise training (ExT) can reduce preeclampsia prevalence although the available studies are considered insufficient. Therefore, the aim of this study is to determine the impact of ExT when practiced before and during gestation on pregnancy outcome in a mouse model of preeclampsia superimposed on chronic hypertension (SPE).
To do so, mice overexpressing both human angiotensinogen and renin (R+A+)
were used because they are hypertensive at baseline and they develop many hallmark features of SPE. Mice were trained by placing them in a cage with access to a running wheel 4 weeks before and during gestation.
ExT in this study prevented the rise in blood pressure at term observed in the sedentary transgenic mothers. This may be realized through an increased activity of the angiotensin-(1-7) axis in the aorta. In addition, ExT prevented the increase in albumin/creatinine ratio. Moreover, placental alterations were prevented with training in transgenic mice, leading to improvements in placental and fetal development. Placental mRNA and circulating levels of sFlt-1 were normalized with training. Additionally, the increase in angiotensin II type I receptor and the decrease in Mas receptor protein were reversed with training.
ExT appears to prevent many SPE-like features that develop in this animal model and may be of use in the prevention of preeclampsia in women. / La prééclampsie est l’une des causes primaires de mortalité et morbidité périnatales, touchant 2-7% des grossesses. Sa prévalence augmente à 10-25% chez les femmes hypertendues. Jusqu’à maintenant, aucun traitement, mis à part l’accouchement précoce, n’est connu. Néanmoins, plusieurs études épidémiologiques suggèrent une diminution de l’incidence de la prééclampsie chez les femmes entraînées quoique, ces études sont considérées insuffisantes. Ainsi, le but de cette étude est de déterminer si l’entraînement avant et pendant la grossesse prévient la maladie dans un modèle animal de prééclampsie superposée à de l’hypertension chronique (SPE).
Nous avons utilisé des souris double transgéniques, surexpirmant la rénine et l’angiotensinogène humaines (R+A+), puisqu'elles sont hypertensives à la base, et développent plusieurs symptômes de la prééclampsie. Pour l'entraînement, les souris ont été mises dans des cages d’exercice 4 semaines avant leur grossesse et y sont restées jusqu’au sacrifice.
L'entraînement physique a prévenu la hausse de pression artérielle en fin de gestation présente chez les souris R+A+ sédentaires, possiblement via l’axe de l’angiotensine-(1-7). Le rapport entre l’albumine: créatinine a également été réduit avec l’entraînement. Les altérations placentaires ont été prévenues chez les souris entraînées, améliorant le développement placentaire et fœtal. Ceci était accompagné d'une normalisation de sFlt-1 circulant et placentaire. De plus, l’augmentation du récepteur à l’angiotensine II de type 1 et la diminution du récepteur Mas dans le placenta étaient renversées.
L’entraînement semble prévenir plusieurs symptômes de la SPE dans un modèle animal suggérant qu'il pourrait être d'une grande utilité dans la prévention de la maladie chez la femme.
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Effect of exercise training on preeclampsia superimposed on chronic hypertension in a mouse modelGenest, Suzanne Dominique 08 1900 (has links)
Preeclampsia is among the leading causes of perinatal mortality and morbidity, affecting 2-7% of pregnancies. Its incidence increases to 10-25% in already hypertensive women. To date, no treatment, aside from delivery, is known. Interestingly, several studies have reported that exercise training (ExT) can reduce preeclampsia prevalence although the available studies are considered insufficient. Therefore, the aim of this study is to determine the impact of ExT when practiced before and during gestation on pregnancy outcome in a mouse model of preeclampsia superimposed on chronic hypertension (SPE).
To do so, mice overexpressing both human angiotensinogen and renin (R+A+)
were used because they are hypertensive at baseline and they develop many hallmark features of SPE. Mice were trained by placing them in a cage with access to a running wheel 4 weeks before and during gestation.
ExT in this study prevented the rise in blood pressure at term observed in the sedentary transgenic mothers. This may be realized through an increased activity of the angiotensin-(1-7) axis in the aorta. In addition, ExT prevented the increase in albumin/creatinine ratio. Moreover, placental alterations were prevented with training in transgenic mice, leading to improvements in placental and fetal development. Placental mRNA and circulating levels of sFlt-1 were normalized with training. Additionally, the increase in angiotensin II type I receptor and the decrease in Mas receptor protein were reversed with training.
ExT appears to prevent many SPE-like features that develop in this animal model and may be of use in the prevention of preeclampsia in women. / La prééclampsie est l’une des causes primaires de mortalité et morbidité périnatales, touchant 2-7% des grossesses. Sa prévalence augmente à 10-25% chez les femmes hypertendues. Jusqu’à maintenant, aucun traitement, mis à part l’accouchement précoce, n’est connu. Néanmoins, plusieurs études épidémiologiques suggèrent une diminution de l’incidence de la prééclampsie chez les femmes entraînées quoique, ces études sont considérées insuffisantes. Ainsi, le but de cette étude est de déterminer si l’entraînement avant et pendant la grossesse prévient la maladie dans un modèle animal de prééclampsie superposée à de l’hypertension chronique (SPE).
Nous avons utilisé des souris double transgéniques, surexpirmant la rénine et l’angiotensinogène humaines (R+A+), puisqu'elles sont hypertensives à la base, et développent plusieurs symptômes de la prééclampsie. Pour l'entraînement, les souris ont été mises dans des cages d’exercice 4 semaines avant leur grossesse et y sont restées jusqu’au sacrifice.
L'entraînement physique a prévenu la hausse de pression artérielle en fin de gestation présente chez les souris R+A+ sédentaires, possiblement via l’axe de l’angiotensine-(1-7). Le rapport entre l’albumine: créatinine a également été réduit avec l’entraînement. Les altérations placentaires ont été prévenues chez les souris entraînées, améliorant le développement placentaire et fœtal. Ceci était accompagné d'une normalisation de sFlt-1 circulant et placentaire. De plus, l’augmentation du récepteur à l’angiotensine II de type 1 et la diminution du récepteur Mas dans le placenta étaient renversées.
L’entraînement semble prévenir plusieurs symptômes de la SPE dans un modèle animal suggérant qu'il pourrait être d'une grande utilité dans la prévention de la maladie chez la femme.
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Caractérisation et modulation pharmacologique de la fonction ventriculaire gauche et du couplage contraction-relaxation par la mesure de la torsion et de la détorsion au cours de l’hypertension artérielle chronique / Characterization and pharmacological modulation of the left ventricular function and contraction-relaxation coupling by measuring twist and untwist during chronic arterial hypertensionJozwiak, Mathieu 21 December 2017 (has links)
L’hypertension artérielle chronique induit une hypertrophie ventriculaire gauche, à l’origine d’une dysfonction diastolique caractérisée par des troubles de la relaxation, de la compliance et du remplissage ventriculaires gauches, le tout aggravé par toute augmentation de la fréquence cardiaque. Le couplage contraction-relaxation physiologique implique, en cas de préservation dans ce contexte d’hypertrophie ventriculaire gauche, que cette dysfonction diastolique s’accompagne d’une dysfonction systolique. Ainsi, ce travail de thèse s’est attaché (1) à caractériser la fonction ventriculaire gauche et le couplage contraction-relaxation à l’aide de la mesure de la torsion et la détorsion, (2) à étudier les mécanismes cellulaires impliqués dans le couplage contraction-relaxation et (3) à explorer les effets d’une stratégie thérapeutique visant à réduire la fréquence cardiaque sur la torsion et la détorsion du ventricule gauche dans un modèle d’hypertension artérielle chronique et d’hypertrophie ventriculaire induites chez le porc chroniquement instrumenté par la perfusion continue d’angiotensine II pendant 28 jours. A J28, la torsion et la détorsion étaient diminuées et la détorsion également retardée au sein du cycle cardiaque, alors que la fraction d’éjection ventriculaire gauche était préservée. Le couplage contraction-relaxation était préservé, tant au niveau du ventricule gauche qu’à l’échelon cardiomyocytaire, suggérant que toute dysfonction diastolique devrait faire rechercher une dysfonction systolique. A J28, ces anomalies fonctionnelles s’accompagnaient d’une diminution de l’expression de la SERCA2a et de sa protéine régulatrice le phospholamban. Des anomalies du récepteur de la ryanodine de type 2 étaient aussi observées avec son hyperphosphorylation et la dissociation de sa protéine régulatrice calstabine 2, à l’origine de fuites calciques systoliques et diastoliques. Ce dernier pourrait ainsi jouer un rôle clé dans la préservation du couplage contraction-relaxation et représenter l’intégrateur entre les anomalies ventriculaire gauche systolique et diastolique observées. Enfin, la réduction pharmacologique de la fréquence cardiaque à J28 par l’ivabradine, un inhibiteur sélectif des canaux If, permettait d’améliorer, en partie par des effets fréquence-indépendants dont les mécanismes cellulaires restent à élucider, tant les anomalies ventriculaire gauche diastolique que systolique, avec une amélioration des temps de contraction et de relaxation isovolumiques, de la torsion et de la détorsion ainsi que du remplissage du ventricule gauche. En l’absence d’hypertrophie ventriculaire gauche, la réduction de la fréquence cardiaque à des valeurs inférieures à 60 batt/min s’accompagnait d’un effet délétère fréquence-dépendant, à l’origine d’une altération isolée de la fonction diastolique caractérisée par une diminution de la détorsion du ventricule gauche et une augmentation de la pression télédiastolique ventriculaire gauche. La caractérisation de la fonction ventriculaire gauche et l’étude du couplage contraction-relaxation par la mesure de la torsion et de la détorsion en cas de décompensation cardiaque restent à déterminer. / Chronic hypertension induces left ventricular (LV) hypertrophy, resulting in abnormalities in LV relaxation, passive stiffness and filling. The higher the heart rate, the more pronounced the LV diastolic dysfunction. Moreover, in the normal heart, there is a tight coupling between LV contraction and relaxation, implying that in case of preserved contraction-relaxation coupling during LV hypertrophy, there is no diastolic dysfunction without systolic dysfunction. Thus, the three main objectives of this thesis were to investigate 1) the LV function and contraction-relaxation coupling with LV twist and untwist, which represent LV myocardial deformation during systole and diastole, 2) the cellular mechanisms of the LV contraction-relaxation coupling and 3) the effects effects of heart rate reduction on LV twist and untwist in the context of chronic hypertension and LV hypertrophy. All experiments were conducted in a pig model of chronic hypertension and LV hypertrophy induced by four weeks of continuous angiotensin II infusion. Chronic angiotensin II infusion decreased LV twist and untwist but also delayed LV untwist in the cardiac cycle, whereas the LV ejection fraction was preserved. The contraction-relaxation coupling was preserved as illustrated by the strong relationship between LV twist and untwist. The contraction-relaxation coupling was also preserved at the level of cardiomyocytes. This implies that LV hypertrophy is associated with concomitant LV diastolic and systolic dysfunction despite preserved LV ejection fraction. Thus, LV diastolic dysfunction is always accompanied by LV systolic dysfunction, i.e., the discovery of LV diastolic dysfunction with preserved ejection fraction might imply the track of LV systolic dysfunction. At the cellular level, LV systolic and diastolic dysfunctions were associated to aberrant calcium handling with a remodelling of the type 2 ryanodine receptor calcium release channel (RyR2), i.e., PKA-hyperphosphorylation and depletion of calstabin 2 (FKBP12.6). RyR2 were leaky and hypersensitive to cytosolic calcium, during both the contraction and the relaxation phases. Since both LV systolic and diastolic dysfunctions were associated to leaky and hypersensitive RyR2 channels, it might suggest considering RyR2 as an integrator contributing to control contraction-relaxation coupling during chronic hypertension and LV hypertrophy. Finally, we investigated the effects of heart rate reduction induced by ivabradine, an If-channel blocker, which does not modify atrioventricular or LV conduction and is devoid of any intrinsic negative inotropic or lusitropic effects. In the context of chronic hypertension and LV hypertrophy, ivabradine improved both LV systolic and diastolic functions, as attested by the improvement in contraction and relaxation times, LV twist and untwist as well as LV filling. Heart-rate independent effects of ivabradine, i.e., pleiotropic effects, participate to its beneficial effect. However, the cellular mechanisms of these beneficial effects of ivabradine were not elucidated and require further investigations. In normal heart, when heart rate was reduced to a low level (approximately <60 beats/min) with ivabradine, LV twist was not affected but LV diastolic function was altered as suggested by decreased LV untwist parameters and increased LV end-diastolic pressure. Investigation of contraction-relaxation coupling during decompensation from stable LV hypertrophy remains a goal to achieve.
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