Enhanced Mesenteric Arterial Responsiveness to Angiotensin II Is Androgen Receptor-Dependent in Prenatally Protein-Restricted Adult Female Rat Offspring1

Sathishkumar, K.; Balakrishnan, Meena; Yallampalli, Chandra

doi:10.1095/biolreprod.114.126482

Cited by 12 publications

(16 citation statements)

References 40 publications

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“…Sathishkumar et al. () discovered an enhanced response to Angiotensin II (potent vasoconstrictor) in the mesenteric artery of 6‐month‐old females following a maternal protein restriction diet, however, these same arteries had no change in sensitivity to PE. Others have also shown an age‐specific difference (Hemmings et al.…”

Section: Discussionmentioning

confidence: 99%

The effect of intrauterine growth restriction on Ca²⁺-activated force and contractile protein expression in the mesenteric artery of adult (6-month-old) male and female Wistar-Kyoto rats

et al. 2018

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Intrauterine growth restriction (IUGR) is known to alter vascular smooth muscle reactivity, but it is currently unknown whether these changes are driven by downstream events that lead to force development, specifically, Ca2+‐regulated activation of the contractile apparatus or a shift in contractile protein content. This study investigated the effects of IUGR on Ca2+‐activated force production, contractile protein expression, and a potential phenotypic switch in the resistance mesenteric artery of both male and female Wistar‐Kyoto (WKY) rats following two different growth restriction models. Pregnant female WKY rats were randomly assigned to either a control (C; N = 9) or food restriction diet (FR; 40% of control; N = 11) at gestational day‐15 or underwent a bilateral uterine vessel ligation surgery restriction (SR; N = 10) or a sham surgery control model (SC; N = 12) on day‐18 of gestation. At 6‐months of age, vascular responsiveness of intact mesenteric arteries was studied, before chemically permeabilization using 50 μmol/L β‐escin to investigate Ca2+‐activated force. Peak responsiveness to a K+‐induced depolarization was decreased (P ≤ 0.05) due to a reduction in maximum Ca2+‐activated force (P ≤ 0.05) in both male growth restricted experimental groups. Vascular responsiveness was unchanged between female experimental groups. Segments of mesenteric artery were analyzed using Western blotting revealed IUGR reduced the relative abundance of important receptor and contractile proteins in male growth restricted rats (P ≤ 0.05), suggesting a potential phenotypic switch, whilst no changes were observed in females. Results from this study suggest that IUGR alters the mesenteric artery reactivity due to a decrease in maximum Ca2+‐activated force, and likely contributed to by a reduction in contractile protein and receptor/channel content in 6‐month‐old male rats, while female WKY rats appear to be protected.

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Section: Discussionmentioning

confidence: 99%

The effect of intrauterine growth restriction on Ca²⁺-activated force and contractile protein expression in the mesenteric artery of adult (6-month-old) male and female Wistar-Kyoto rats

et al. 2018

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“…Numerous adverse prenatal environments alter postnatal growth, but the specific effect is dependent on the timing and severity of the insult, as well as on the quality of the postnatal environment to which the offspring is exposed. Prenatal perturbations, such as calorie restriction (10–35%; Kind et al, 1999 , 2002 , 2003 ; Vickers et al, 2000 ; Riviere et al, 2005 ; Breton et al, 2009 ; Camm et al, 2011 ; Lukaszewski et al, 2011 , 2013 ), low-protein diet (6%; Sathishkumar et al, 2009 , 2012 , 2015 ), iron restriction (Crowe et al, 1995 ; Lewis et al, 2001c , 2002 ) and uterine artery ligation (e.g., Wlodek et al, 2007 , 2008 ; Siebel et al, 2008 ) in rats and guinea pigs reduce birth weight. Furthermore, offspring remain smaller through to adulthood, irrespective of the stage at which the manipulation occurs prenatally.…”

Section: Effects Of Maternal Environment On Offspring Growthmentioning

confidence: 99%

The Programming Power of the Placenta

2016

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Size at birth is a critical determinant of life expectancy, and is dependent primarily on the placental supply of nutrients. However, the placenta is not just a passive organ for the materno-fetal transfer of nutrients and oxygen. Studies show that the placenta can adapt morphologically and functionally to optimize substrate supply, and thus fetal growth, under adverse intrauterine conditions. These adaptations help meet the fetal drive for growth, and their effectiveness will determine the amount and relative proportions of specific metabolic substrates supplied to the fetus at different stages of development. This flow of nutrients will ultimately program physiological systems at the gene, cell, tissue, organ, and system levels, and inadequacies can cause permanent structural and functional changes that lead to overt disease, particularly with increasing age. This review examines the environmental regulation of the placental phenotype with particular emphasis on the impact of maternal nutritional challenges and oxygen scarcity in mice, rats and guinea pigs. It also focuses on the effects of such conditions on fetal growth and the developmental programming of disease postnatally. A challenge for future research is to link placental structure and function with clinical phenotypes in the offspring.

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“…In a model of maternal nutrient restriction in sheep, female adult offspring (6 yr of age) were demonstrated to have reduced steroidogenic enzyme expression and subsequently reduced circulating and luteal progesterone levels (228). In the female offspring of protein-restricted rats, plasma testosterone levels were increased along with increased blood pressure (359). In this study, treatment of the offspring with the androgen receptor antagonist flutamide (10 mg·kg Ϫ1 ·day Ϫ1 sc, for 10 days) ameliorated the hypertensive phenotype and reversed the enhanced mesenteric artery responses to ANG II, suggesting that the alterations in RAS might be androgen-dependent.…”

Section: F Sex Differencesmentioning

confidence: 99%

In Utero Origins of Hypertension: Mechanisms and Targets for Therapy

Morton

Cooke

Davidge³

2016

Physiological Reviews

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The developmental origins of health and disease theory is based on evidence that a suboptimal environment during fetal and neonatal development can significantly impact the evolution of adult-onset disease. Abundant evidence exists that a compromised prenatal (and early postnatal) environment leads to an increased risk of hypertension later in life. Hypertension is a silent, chronic, and progressive disease defined by elevated blood pressure (>140/90 mmHg) and is strongly correlated with cardiovascular morbidity/mortality. The pathophysiological mechanisms, however, are complex and poorly understood, and hypertension continues to be one of the most resilient health problems in modern society. Research into the programming of hypertension has proposed pharmacological treatment strategies to reverse and/or prevent disease. In addition, modifications to the lifestyle of pregnant women might impart far-reaching benefits to the health of their children. As more information is discovered, more successful management of hypertension can be expected to follow; however, while pregnancy complications such as fetal growth restriction, preeclampsia, preterm birth, etc., continue to occur, their offspring will be at increased risk for hypertension. This article reviews the current knowledge surrounding the developmental origins of hypertension, with a focus on mechanistic pathways and targets for therapeutic and pharmacologic interventions.

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Enhanced Mesenteric Arterial Responsiveness to Angiotensin II Is Androgen Receptor-Dependent in Prenatally Protein-Restricted Adult Female Rat Offspring1

Cited by 12 publications

References 40 publications

The effect of intrauterine growth restriction on Ca²⁺-activated force and contractile protein expression in the mesenteric artery of adult (6-month-old) male and female Wistar-Kyoto rats

The effect of intrauterine growth restriction on Ca²⁺-activated force and contractile protein expression in the mesenteric artery of adult (6-month-old) male and female Wistar-Kyoto rats

The Programming Power of the Placenta

In Utero Origins of Hypertension: Mechanisms and Targets for Therapy

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Enhanced Mesenteric Arterial Responsiveness to Angiotensin II Is Androgen Receptor-Dependent in Prenatally Protein-Restricted Adult Female Rat Offspring1

Cited by 12 publications

References 40 publications

The effect of intrauterine growth restriction on Ca2+-activated force and contractile protein expression in the mesenteric artery of adult (6-month-old) male and female Wistar-Kyoto rats

The effect of intrauterine growth restriction on Ca2+-activated force and contractile protein expression in the mesenteric artery of adult (6-month-old) male and female Wistar-Kyoto rats

The Programming Power of the Placenta

In Utero Origins of Hypertension: Mechanisms and Targets for Therapy

Contact Info

Product

Resources

About

The effect of intrauterine growth restriction on Ca²⁺-activated force and contractile protein expression in the mesenteric artery of adult (6-month-old) male and female Wistar-Kyoto rats

The effect of intrauterine growth restriction on Ca²⁺-activated force and contractile protein expression in the mesenteric artery of adult (6-month-old) male and female Wistar-Kyoto rats