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Mechanisms linking exposure to preeclampsia in utero and the risk for cardiovascular disease

Part of: DOHaD ANZ Conference 2018: Genes, Environment and Evolution

Published online by Cambridge University Press:  19 February 2020

Prabha H. Andraweera Open the ORCID record for Prabha H. Andraweera [Opens in a new window] ,
Kathryn L. Gatford Open the ORCID record for Kathryn L. Gatford [Opens in a new window] ,
Alison S. Care ,
Tina Bianco-Miotto ,
Zohra S. Lassi ,
Gus A. Dekker ,
Margaret Arstall  and
Claire T. Roberts
Prabha H. Andraweera*
Affiliation:
Adelaide Medical School, The University of Adelaide, Adelaide, Australia Robinson Research Institute, The University of Adelaide, Adelaide, Australia
Kathryn L. Gatford
Affiliation:
Adelaide Medical School, The University of Adelaide, Adelaide, Australia Robinson Research Institute, The University of Adelaide, Adelaide, Australia
Alison S. Care
Affiliation:
Adelaide Medical School, The University of Adelaide, Adelaide, Australia Robinson Research Institute, The University of Adelaide, Adelaide, Australia
Tina Bianco-Miotto
Affiliation:
Robinson Research Institute, The University of Adelaide, Adelaide, Australia School of Agriculture, Food and Wine, The University of Adelaide, Adelaide, Australia
Zohra S. Lassi
Affiliation:
Adelaide Medical School, The University of Adelaide, Adelaide, Australia Robinson Research Institute, The University of Adelaide, Adelaide, Australia
Gus A. Dekker
Affiliation:
Adelaide Medical School, The University of Adelaide, Adelaide, Australia Robinson Research Institute, The University of Adelaide, Adelaide, Australia Division of Women’s Health, Lyell McEwin Hospital, Elizabeth Vale, Australia
Margaret Arstall
Affiliation:
Adelaide Medical School, The University of Adelaide, Adelaide, Australia Department of Cardiology, Lyell McEwin Hospital, Elizabeth Vale, Australia
Claire T. Roberts
Affiliation:
Adelaide Medical School, The University of Adelaide, Adelaide, Australia Robinson Research Institute, The University of Adelaide, Adelaide, Australia
*
Address for correspondence: Prabha Andraweera, Adelaide Medical School, The Robinson Research Institute, The University of Adelaide, Adelaide, Australia. Email: prabha.andraweera@adelaide.edu.au
Rights & Permissions [Opens in a new window]

Abstract

Preeclampsia (PE) is now recognised as a cardiovascular risk factor for women. Emerging evidence suggests that children exposed to PE in utero may also be at increased risk of cardiovascular disease (CVD) in later life. Individuals exposed to PE in utero have higher systolic and diastolic blood pressure and higher body mass index (BMI) compared to those not exposed to PE in utero. The aim of this review is to discuss the potential mechanisms driving the relationship between PE and offspring CVD. Exposure to an adverse intrauterine environment as a consequence of the pathophysiological changes that occur during a pregnancy complicated by PE is proposed as one mechanism that programs the fetus for future CVD risk. Consistent with this hypothesis, animal models of PE where progeny have been studied demonstrate causality for programming of offspring cardiovascular health by the preeclamptic environment. Shared alleles between mother and offspring, and shared lifestyle factors between mother and offspring provide alternate pathways explaining associations between PE and offspring CVD risk. In addition, adverse lifestyle habits can also act as second hits for those programmed for increased CVD risk. PE and CVD are both multifactorial diseases and, hence, identifying the relative contribution of PE to offspring risk for CVD is a very complex task. However, considering the emerging strong association between PE and CVD, those exposed to PE in utero may benefit from targeted primary CVD preventive strategies.

Keywords

Preeclampsiacardiovascular diseaseoffspringprogeny
Type
Review
Information
Journal of Developmental Origins of Health and Disease , Volume 11 , Issue 3 , June 2020 , pp. 235 - 242
Copyright
© The Author(s) 2020. Published by Cambridge University Press and the International Society for Developmental Origins of Health and Disease

Introduction

Preeclampsia (PE) is a pregnancy-specific disorder that complicates 2%–5% of all pregnancies and is a leading cause of maternal morbidity and mortality worldwide.Reference Duley1 PE was traditionally diagnosed when a pregnant woman presented with increased blood pressure and proteinuria. According to the current International Society for the Study of Hypertension in Pregnancy guidelines, PE is defined as an onset of hypertension (systolic blood pressure higher than 140 mmHg or diastolic blood pressure higher than 90 mmHg on two occasions that are 4–6 h apart) after 20 weeks gestation and the coexistence of one or more of the following new-onset conditions: (1) proteinuria (spot urine protein/creatinine >30 mg/mmol [0.3 mg/mg] or >300 mg/day or at least 1 g/l [‘2 + ’] on dipstick testing), (2) organ dysfunction (such as renal insufficiency [creatinine >90 umol/l; 1.02 mg/dl], liver involvement (elevated transaminases – at least twice upper limit of normal ± right upper quadrant or epigastric abdominal pain), neurological complications (examples include eclampsia, altered mental status, blindness, stroke or more commonly hyperreflexia when accompanied by clonus, severe headaches when accompanied by hyperreflexia, persistent visual scotomata), haematological complications (thrombocytopenia – platelet count below 150,000/dl, DIC, haemolysis) and (3) uteroplacental dysfunction evidenced by fetal growth restriction.Reference Tranquilli, Dekker and Magee2 Although the hypertension and proteinuria resolve after pregnancy, women who develop PE are at increased risk of vascular diseases in later life. Previous systematic reviews and meta-analyses have shown that women who develop PE are at more than two-fold increased risk of developing coronary artery disease (CAD) compared to women who have non-preeclamptic pregnancies.Reference Bellamy, Casas, Hingorani and Williams3-Reference Heida, Bots and de Groot5 Early onset PE (<34 weeks gestation) is associated with nearly eight-fold increased risk of subsequent CAD for the woman compared to late onset disease and severe PE (blood pressure >160/110 mmHg plus proteinuria >0.3 g/24 h or diastolic blood pressure >110 mmHg plus proteinuria >5 g/24 h) is associated with a higher risk of CAD compared to mild PE.Reference Heida, Bots and de Groot5,Reference Tranquilli, Brown, Zeeman, Dekker and Sibai6 Women who develop PE are at increased risk of other vascular diseases including hypertension, thromboembolic disorders, cerebrovascular events and diabetes compared to women who do not experience PE.Reference Bellamy, Casas, Hingorani and Williams3-Reference Heida, Bots and de Groot5 The evidence linking PE with cardiovascular disease (CVD) has resulted in PE being recognised by the American Heart Association as a female-specific, cardiovascular risk factor.Reference Mosca, Benjamin and Berra7

In addition to the maternal risk, emerging evidence suggests that children born to women who experience PE may also be at increased risk of CVD in adulthood. A recent population-based cohort study of 231,298 deliveries demonstrated a significant linear association between PE (no PE, mild PE, severe PE and eclampsia) and rates of CVD in the offspring (0.24% vs. 0.33% vs. 0.51% vs. 2.73%, respectively, p < 0.001).Reference Nahum Sacks, Friger and Shoham-Vardi8 Furthermore, compared to children of normotensive pregnancies, those exposed to PE in utero (mild, severe and eclampsia) had significantly higher rates of hypertension (0.06% vs. 0.11% vs. 0.14% vs. 1.37%, respectively, p < 0.001), arrhythmias (0.13% vs. 0.18% vs. 0.18% vs. 1.37%, respectively, p = 0.016) and heart failure (0.04% vs. 0.03% vs. 0.18% vs. 0.00%, respectively, p = 0.004)Reference Nahum Sacks, Friger and Shoham-Vardi8. Over the last decade, many studies have also reported a greater prevalence of conventional CVD risk factors in children exposed to PE in utero compared to children not exposed to PE in utero. We recently conducted a systematic review and meta-analysis of prospective and retrospective studies that had compared CVD risk factors among those exposed to PE in utero compared to those not exposed to PE in utero.Reference Andraweera and Lassi9 This pooled evidence from 36 studies and over 53,000 participants found that systolic blood pressure, diastolic blood pressure and body mass index (BMI) were significantly higher among those exposed to PE in utero compared to those not exposed to PE in utero.Reference Andraweera and Lassi9 The link between maternal PE and offspring CVD is likely to be due to abnormalities in vascular function. This is supported by the finding of impaired vascular responses in some offspring animal models that mimic PEReference Anderson, Lopez, Zimmer and Benoit10 as well as the majority of human studies of those exposed to PE in utero.Reference Davis, Newton and Lewandowski11 Endothelial dysfunction, a hallmark of PE and an early biological marker of CVD, is evident in children and adolescents exposed to PE in utero.Reference Kvehaugen, Dechend, Ramstad, Troisi, Fugelseth and Staff12,Reference Jayet, Rimoldi and Stuber13 Endothelium-dependent differences in microvascular function have also been reported in children born to women who experienced PE as early as in the neonatal period.Reference Touwslager, Houben and Gielen14 Furthermore, carotid intima-media thickness is increased among young adults in their 20s exposed to PE in utero.Reference Lazdam, de la Horra and Pitcher15 A study that compared aortic intima-media thickness (aIMT) and cord blood lipid profiles of neonates born to women with PE with those of neonates born of healthy pregnancies showed significantly increased aIMT and cord blood triglyceride and decreased cord blood high density lipoprotein cholesterol levels in neonates of preeclamptic pregnancies compared to the control group.Reference Akcakus, Altunay, Yikilmaz, Yazici and Koklu16 These findings suggest the possibility that an early atherogenic phenotype independent of blood pressure may contribute to the link between exposure to PE in utero and later life CVD.

The above evidence demonstrates a clear association between PE and later life CVD for both women and their children. CVD is a major global health burden that results in the greatest number of deaths worldwide. The World Health Organization estimates that 17.6 million people died from CVD in 2012 accounting for 31.43% of global mortality.Reference McAloon, Boylan and Hamborg17 In the context of an increasing global obesity epidemic, this calls for an urgent need to develop potential primary preventive strategies for at-risk populations. The association between maternal PE and offspring CVD is well known. However, the mechanisms underlying this link are poorly understood. This review outlines the evidence for developmental programming, epigenetics and shared genetics as potential mechanisms driving the relationship between PE and offspring CVD.

Developmental programming of CVD risk by in utero exposure to PE

Developmental programming of chronic diseases is now an established paradigm. The link between early life environmental factors and later life disease susceptibility was initially proposed by David Barker who in early 1990s showed that restricted growth in fetal life was associated with mortality from CVD.Reference Barker18,Reference Barker19 This concept that exposure to unfavourable conditions in utero at times of critical organ development may lead to later life disease risk was originally called the Barker Hypothesis/fetal origins of disease hypothesis and now the Developmental Origins of Health and Disease hypothesis.Reference Barker20 While most of the initial work on this topic linked intrauterine undernutrition with later life CVD and metabolic disease risk, subsequent epidemiological studies have shown that numerous intrauterine exposures including major pregnancy complications (PE, intrauterine growth restriction [IUGR], spontaneous preterm birth and gestational diabetes mellitus), maternal obesity and smoking during pregnancy and exposure to environmental chemicals can each trigger propensity for a myriad of cardiovascular, metabolic, immunological, reproductive and neurodevelopmental disorders in the offspring.Reference Murphy, Cohn and Loria21

Depending on the severity of the insult during critical periods of rapid growth and development, permanent tissue adjustments can occur which lead to long-term functional changes in vital organs. Although PE is a multifactorial disorder, several pathophysiological mechanisms including angiogenic imbalance, excessive inflammation, ischaemia/perfusion and imbalances in the renin angiotensin system are all implicated in its pathogenesis.Reference Andraweera, Dekker and Roberts22,Reference Stojanovska, Scherjon and Plosch23 During a pregnancy complicated by PE, the placenta releases circulating factors, including sFlt and sEng,Reference Staff24,Reference Redman and Sargent25 into the maternal circulation as a result of syncytiotrophoblast stress due to a variety of insults including placental ischemia/hypoxia, contributing to excessive inflammation and generation of reactive oxygen species.Reference Brennan, Morton and Davidge26-Reference Kao, Morton, Quon, Reyes, Lopez-Jaramillo and Davidge29 Consistent with a causal role for these placental factors in programming of progeny CVD, overexpression of sFlt in a mouse model of PE mimicking the placenta of a pregnancy affected by PE results in elevated systolic and diastolic blood pressure in male offspring.Reference Lu, Bytautiene and Tamayo30 Higher than normal levels of these placental circulating factors lead to placental oxidative stress, inflammation and lipid peroxidationReference Aouache, Biquard, Vaiman and Miralles31,Reference Myatt, Rosenfield, Eis, Brockman, Greer and Lyall32 which can have permanent effects on the susceptibility of that fetus to CVD later in life. Increased oxidative stress and placental oxidative DNA damage are associated with fetal growth restriction in offspring from pregnancies complicated by PE,Reference Fujimaki, Watanabe, Mori, Kimura, Shinohara and Wakatsuki33 and there is evidence of oxidative stress and DNA damage in cord blood from offspring of PE-affected pregnancies.Reference Hilali, Kocyigit and Demir34 Exposure to hypoxia in a rat model of PE leads to impaired placental function, and offspring exhibit inflammation and atherosclerosis.Reference Wang, Huang, Lu, Lin and Ferrari35-Reference Zhang, Zhu and Chen37

The impact of perinatal exposure to inflammation also has various impacts on the fetus, including changes to the fetal immune systemReference Santner-Nanan, Straubinger and Hsu38,Reference Hu, Eviston and Hsu39 (e.g. lower abundance of regulatory T [Treg] cells) which persist into early childhood.Reference Hu, Eviston and Hsu39 Exposure to intrauterine inflammation as a result of placental dysfunction may lead to increased inflammation and reduced capacity to dampen inflammation due to a deficiency in Treg cells in later life. Such immune programming may contribute to progeny CVD, since inflammation is central in the pathogenesis of atherosclerosis and CVD.Reference Hu, Eviston and Hsu39,Reference Nguyen Maria, Wallace Megan, Pepe, Menheniott, Moss Timothy and Burgner40

Animal studies provide mechanistic evidence that each of these exposures programs offspring blood pressure. The strength of most of the animal models is that they avoid the confounding factors of shared genetics and shared lifestyles and focus specifically on in utero exposure. The models of PE in which programming of progeny cardiometabolic outcomes has been most extensively characterised are in rodents. These include the surgically induced reduced uterine perfusion pressure (RUPP) rat, and PE induced by maternal treatment during pregnancy with hypoxia, the nitric oxide synthase (NOS) inhibitor L-NAME or angiotensin II autoantibodies. Postnatal outcomes have also been well characterised in progeny of mice where elevated sFlt1 was achieved by adenoviral transfection of dams during pregnancy. In each of these models, progeny are lighter at birth but catch up in body weight to that of controls during or before adulthood.Reference Zhang, Zhu and Chen37,Reference Alexander41-Reference McDonnold, Tamayo and Kechichian51 Development of obesity is variable, with obesity reported in adult female, but not male, RUPP rats with ageing,Reference Intapad, Tull and Brown52,Reference Intapad, Dasinger, Fahling, Backstrom and Alexander53 but normal body and central fat abundance in adult progeny of sFlt1-transduced mice of both sexes.Reference Bytautiene, Tamayo and Kechichian54 Likewise, effects of in utero exposure to a preeclamptic phenotype on postnatal glucose tolerance are sex- and age-dependent in the RUPP rat,Reference Intapad, Dasinger, Fahling, Backstrom and Alexander53,Reference Intapad, Dasinger, Brown, Fahling, Esters and Alexander55 L-NAME-treated ratReference Butruille, Mayeur and Moitrot56 and sFlt1-transduced miceReference McDonnold, Tamayo and Kechichian51 models of PE. Progeny cardiac dysfunction is common to all of these models, although with some variation in phenotype and different sets of outcomes studied in each model. Hypertension at baseline and/or in response to stress or adrenaline has been reported in progeny of the RUPP rat,Reference Anderson, Lopez, Zimmer and Benoit10,Reference Alexander41-Reference Dasinger, Intapad, Backstrom, Carter and Alexander45,Reference Intapad, Tull and Brown52,Reference Payne, Alexander and Khalil57 hypoxic ratReference Tang, Zhu and Xia47,Reference Liu, Liu and Shi48,Reference Peyronnet, Dalmaz and Ehrstrom58,Reference Wang, Li, Huang and Wang59 and in males but not females in the sFlt1-transduced mice model of PE.Reference Lu, Bytautiene and Tamayo30,Reference Bytautiene, Tamayo and Kechichian54 Interestingly, progeny of the L-NAME-treated rat are normotensive as young and mature adults.Reference Herraiz, Pellicer and Serra50,Reference Witlin, Gangula, Thompson and Yallampalli60 Greater arterial vasoconstriction in response to stimuli, greater renal sympathetic nerve activity, contributions from circulating sex steroids and impaired vasodilation are all implicated as mechanisms for hypertension in progeny of the RUPP rat.Reference Anderson, Lopez, Zimmer and Benoit10,Reference Alexander, Hendon, Ferril and Dwyer42,Reference Ojeda, Grigore and Yanes43,Reference Intapad, Tull and Brown52,Reference Payne, Alexander and Khalil57 Similarly, in progeny of hypoxic rat dams, phenylephrine-induced vasoconstriction is greater, and both endothelium-dependent and endothelium-independent vasodilatation are reduced compared to control progeny.Reference Giussani, Camm and Niu36,Reference Tang, Zhu and Xia47,Reference Liu, Liu and Shi48,Reference Allison, Kaandorp and Kane61,Reference Tang, Li and Chen62

Progeny heart structure and function are also impaired in several of these models. For example, cardiac and cardiomyocyte size are normal at 3 months of age in young male adults whose mothers were exposed to intermittent hypoxia from early pregnancy (10% O2 for 3 h/day from GD7 to 21)Reference Wang, Li, Huang and Wang59. At 5 months of age, hypertensive adult male progeny from these dams exhibit cardiac hypertrophy, with normal cardiomyocyte size but greater left ventricular collagen expression of collagen I and III.Reference Wang, Li, Huang and Wang59 Furthermore, lesions suggestive of developing atherosclerosis are present in the aortas of adult male progeny at 5 months of age of dams housed continuously in 10.5% O2 from GD5-delivery,Reference Zhang, Zhu and Chen37 and in aged adult male and female progeny at 16 months of age who were exposed to hypoxia in utero 10% O2 for 3 h/day from GD7 to 21.Reference Wang, Huang, Lu, Lin and Ferrari35 Although their relative heart weights are normal, male progeny of dams treated with angiotensin-II-like auto-antibodies (which bind and activate the angiotensin II-type I receptor) have enlarged cardiomyocytes, with areas of disorganisation, necrotis and apoptosis evident in their left ventricles as young adults at 5 months postnatal age.Reference Jin, Zhang and Yang49 The function of isolated hearts from these progeny in a Langendorff apparatus is normal under basal conditions, but they have impaired recovery and larger infarcts following ischaemia-reperfusion.Reference Jin, Zhang and Yang49 Cardiac hypertrophy is also evident throughout the first month of postnatal life in progeny of rats treated with L-NAME before and throughout pregnancy.Reference Martini and Mandarim-de-Lacerda63

The fact that hypertension and impaired metabolism occur in progeny in these models of induced PE provides direct evidence of causality for the exposure. Nevertheless, these models lack the initiating processes that lead to spontaneous PE in humans. Interpretation of the programming mechanisms in progeny exposed to PE in utero and evaluation of potential maternal or postnatal interventions also need to consider the stage of cardiovascular development when in utero exposure occurs. For example, the switch from cardiomyocyte proliferation to hypertrophy occurs postnatally in rodents but before birth in other species including humans.Reference Lock, Tellam and Botting64 A recent report that progeny of preeclamptic baboons exhibit elevated systolic blood pressure during a dietary salt loading challengeReference Yeung, Sunderland and Lind65 provides direct evidence of cardiovascular programming by in utero exposure to PE in species that are more mature at birth, although studies with greater animal numbers are needed to assess any sex differences.

When combined with epidemiological evidence from human studies, these suggest several plausible mechanisms for the hypertensive phenotype seen in offspring of preeclamptic pregnancies.Reference Davis, Newton and Lewandowski11 Several studies have shown reduced numbers of nephrons and cardiomyocytes in offspring born with low birthweight or born preterm, two pregnancy complications that often co-exist with PE.Reference Luyckx, Bertram and Brenner66 A reduction in the number of nephrons contributes to a reduction in the rate of renal ultrafiltration that affects the circulating blood volume leading to increased blood pressure.Reference Keller, Zimmer, Mall, Ritz and Amann67 Altered nephron number is associated with glomerular hypertrophy and reduced renal vascular dilation contributing to risk of hypertension.Reference Richter, Briffa, Moritz, Wlodek and Hryciw68,Reference Marchand and Langley-Evans69 Alterations in the renin–angiotensin–aldosterone system (RAAS) including upregulation or downregulation of specific receptors within the kidney, blood vessels and the placenta have also been implicated in the development of renal dysfunction.Reference Moritz, Cuffe and Wilson70 Emerging evidence suggests that epigenetic processes which are strongly influenced by the environment may play a key role in developmental programming of adult CVD.

The role of epigenetics in the relationship between PE and increased risk of CVD in offspring

Epigenetics refers to modifications that result in gene expression changes, often through chromatin remodelling, without altering the underlying DNA sequenceReference Berdasco and Esteller71 These modifications include DNA methylation, histone modifications, non-coding RNA (ncRNA) and other modifications that can result in altered gene expression.Reference Berdasco and Esteller71 Epigenetic changes have been widely studied in developmental processes, especially their role in determining cell lineages, and also in disease states as they can mediate aberrant gene expression.Reference Berdasco and Esteller71 In addition, epigenetic modifications are routinely used for diagnostic and prognostic biomarkers of adverse outcomes. Epigenetic modifications are also altered in response to environmental exposures and can potentially indicate whether an adverse exposure early in life is associated with future chronic disease risk.Reference Berdasco and Esteller71

The most widely studied epigenetic alteration is DNA methylation which is the addition of a methyl group to a cytosine catalysed by enzymes known as DNA methyltransferases. DNA methylation is involved in development, imprinting and X chromosome inactivation, as well as numerous other processes.Reference Berdasco and Esteller71 Hypermethylation at gene regulatory regions or promoter associated CpG islands is often associated with gene repression. Histone modifications refer to changes to the histone tails including acetylation, methylation or phosphorylation and together with DNA methylation impact chromatin packing and hence accessibility of transcription factors to the regulatory DNA sequences controlling gene expression. ncRNAs consist of short ncRNAs like microRNAs, piwiRNAs, snoRNAs or long non-coding RNAs (lncRNA) and can inhibit transcription and translation or alter protein trafficking and folding to name just a few of their actions.Reference Karlsson and Baccarelli72

Epigenetic changes are considered likely mechanisms that link maternal PE with offspring CVD with the possibility of passing on the risk to subsequent generations, by germ-line inheritance of epigenetic marks.Reference Heindel73,Reference Hanson and Skinner74 Animal models, which allow for tight regulation and control of the adverse exposure, have repeatedly shown that adverse events in utero are associated with increased risk of chronic disease in offspring.Reference Heindel73,Reference Goyal, Limesand and Goyal75,Reference Hanson76 Similar studies in humans are difficult, not only due to the lack of control of ‘other’ life-time environmental exposures but also due to genetic predispositions and additionally access to the appropriate tissue for assessment. However, epidemiological studies do show evidence for changes in DNA methylation as potential mediators or biomarkers of in utero exposure to PE when assessed in the placentaReference Apicella, Ruano, Mehats, Miralles and Vaiman77,Reference Bianco-Miotto, Mayne, Buckberry, Breen, Rodriguez Lopez and Roberts78 and cord blood.Reference Kazmi, Sharp and Reese79 Whether these epigenetic changes are associated with an increased risk of CVD in the offspring later in life is unknown as no studies have yet reported epigenetic alterations in the adult offspring born to women who experience PE. This is not surprising due to the length of follow-up required for these studies and also access to the right tissue sample for the epigenetic analyses. However, there are a few studies that demonstrate an association between PE exposure and epigenetic changes in offspring. In a 2015 study by Julian et al., DNA methylation in blood from young adult men born following hypertensive pregnancies (n = 5) compared to controls (n = 19) showed differential methylation in the genes SMOC2, ARID1B and CTRHC1.Reference Julian, Pedersen and Salmon80 Murray et al. reported that DNA methylation in cord blood leukocytes of ANRIL predicted pulse wave velocity and heart rate in the child at 9 years of age.Reference Murray, Bryant and Titcombe81 Therefore, with the appropriate longitudinal cohorts, in future, we may be able to determine whether epigenetic change induced by in utero exposure to PE underlies increased risk of future CVD risk in the offspring.

The placenta may mediate this future CVD risk in the offspring as several studies have shown altered DNA methylation in placentas from women who experience PE compared to healthy pregnancies (reviewed in ref.Reference Apicella, Ruano, Mehats, Miralles and Vaiman77). The genes shown to have aberrant DNA methylation include those with a role in trophoblast proliferation, differentiation and invasion, as well as genes involved in vascular function and immunological processes.Reference Apicella, Ruano, Mehats, Miralles and Vaiman77 Epigenetic alterations in these critical genes may impact the function of the placenta during pregnancy resulting in an adverse environment for the fetus.Reference Tarrade, Panchenko, Junien and Gabory82 The fetus adapts to this adverse environment, resulting in epigenetic alterations that mediate future CVD risk. More work is required to define how PE impacts the intrauterine environment, what epigenetic alterations this induces in the fetus and if these epigenetic alterations are still evident in adult offspring. Dissecting out the epigenetic mechanism is made difficult in humans by the need for longitudinal cohorts as well as determining which tissue to assess.

The role of shared genetics in the relationship between PE and increased risk of CVD in offspring

The link between PE and CVD in offspring could also be explained by shared genetic factors that predispose individuals to vascular diseases that manifest at different time points during the life course.Reference Andraweera, Dekker, Arstall, Bianco-Miotto and Roberts83 The incidence of PE is higher among women who were born of a pregnancy complicated by PE,Reference Lie, Rasmussen, Brunborg, Gjessing, Lie-Nielsen and Irgens84 while the risk of fathering a pregnancy complicated by PE is also higher among men who previously fathered a pregnancy complicated by PE with a different partnerReference Lie, Rasmussen, Brunborg, Gjessing, Lie-Nielsen and Irgens84 and among men who were themselves the product of a pregnancy complicated by PE,Reference Esplin, Fausett and Fraser85 all suggesting that PE is at least in part heritable. Further evidence for a genetic mechanism is provided by studies that show that genetic variants that are known risk factors for CVD are more prevalent among women who experience PE, men who father pregnancies complicated by PE and among infants born of pregnancies complicated by PE compared to unaffected populations.Reference Andraweera, Dekker, Thompson and Roberts86-Reference Andraweera, Dekker, Thompson, North, McCowan and Roberts89 Genetics, therefore, may act as a confounding factor in the association between maternal PE and offspring CVD. The underlying mechanism for some offspring who experience CVD in adult life after exposure to PE in utero may not be the effect of PE but genetic susceptibility to CVD, and these individuals may experience CVD even if they had not been exposed to PE in utero. This theory is supported by the findings of genetic variants that are common in both PE and CVD from a study on genetic dissection of the 2q22 PE susceptibility locus.Reference Sitras, Fenton and Acharya90 This study identified four independent single nucleotide polymorphisms (SNPs) within four genes that were associated with PE in an Australian family cohort: lactase (LCT, rs2322659), low-density lipoprotein receptor-related protein 1B (LRP1B, rs35821928), rho family GTPase 3 (RND3, rs115015150) and grancalcin (GCA, rs17783344).Reference Johnson, Fitzpatrick and Dyer91 These four SNPs were also associated with cardiovascular risk factors in an independent cohort of Mexican American families.Reference Johnson, Fitzpatrick and Dyer91 An attempt to confirm the above findings in an independent Australian population-based cohort of mothers and their adolescents showed nominal associations with cardiovascular risk factors (weight, blood glucose and triglycerides) for all four SNPs.Reference Loset, Johnson and Melton92 These findings suggest the possibility that certain genetic variants may predispose individuals to different vascular diseases, with some women developing PE during pregnancy, some men fathering pregnancies complicated by PE and some developing CVD.

The role of shared environment and lifestyle in the relationship between PE and increased risk of CVD in offspring

Similar to shared alleles, shared lifestyle factors between mother and offspring may also confound the association between maternal PE and offspring CVD. It is well known that suboptimal environmental and lifestyle conditions including unhealthy diets, lack of exercise, low socioeconomic status and low educational levels are all associated with both PE and CVD. Since these factors are very likely to be shared between mothers and their children, they may underlie the association between maternal PE and CVD in offspring in a manner similar to the potential role of similar genes. These unfavourable lifestyle factors are also proposed to act as ‘second hits’ for some individuals. Some who are ‘programmed’ for increased disease risk only develop disease when exposed to a ‘second hit’Reference Cheong, Wlodek, Moritz and Cuffe93 at a later stage in life. These ‘second hits’ are often adverse lifestyle factors including smoking, unhealthy diets and sedentary lifestyles,Reference Cheong, Wlodek, Moritz and Cuffe93 so shared adverse environment may contribute to CVD risk both directly and by providing a ‘second hit’ exposure to individuals who are susceptible as a consequence of their intrauterine exposures.

Maternal PE and offspring CVD: developmental programming, shared genes or shared lifestyle?

If the association between maternal PE and offspring CVD was solely due to developmental programming, adverse cardiovascular profiles would only be seen among those exposed to PE in utero and siblings born of normotensive pregnancies will be unaffected. On the other hand, if the association between maternal PE and offspring CVD is due to shared genetics and/or lifestyles, then offspring of the same parents from pregnancies unaffected by PE would demonstrate similar CVD risk to that of offspring of pregnancies complicated by PE. The HUNT study comprising three large population-based surveys (HUNT 1, n = 77,212; HUNT2, n = 65,215; HUNT 3, n = 50,807) conducted in Norway explored these questions by comparing CVD risk factors among siblings discordant for the exposure to hypertensive disease in pregnancy (n = 472 participants within 210 sibships).Reference Alsnes, Vatten and Fraser94 In this large study, offspring exposed in utero to maternal hypertension including PE and their siblings born after a normotensive pregnancy had similar adverse CVD risk profiles, suggesting that shared genes or lifestyle may account for the association, rather than an intrauterine effect. However, other studies suggest that the increased CVD risk in the offspring could be a long-term consequence of fetal exposure to PE. In support of this theory, offspring who were born after a pregnancy complicated by PE display marked vascular dysfunction (higher pulmonary artery pressure and lower flow-mediated dilation), but their siblings born after a normotensive pregnancy display normal vascular function.Reference Jayet, Rimoldi and Stuber13 In this study, the birthweight of offspring exposed to PE in utero was approximately 400 g lower than the control group. This suggests the possibility of an alternative explanation. Birthweight correlates linearly with nephron number in adults and children, with nephron number increasing by 257,426 per kg increase in birthweightReference Hughson, Farris, Douglas-Denton, Hoy and Bertram95 and low nephron number being associated with higher blood pressure (reviewed in ref.Reference Luyckx, Bertram and Brenner66). Effects of PE exposure in utero on postnatal blood pressure may therefore be in part mediated by effects of fetal growth restriction on renal function. Interpretation of associations between exposure to PE in utero and later life CVD becomes more complicated by the fact that offspring of pregnancies complicated by PE can also be born with low birthweight and prematurity. Low birthweight and prematurity are both associated with a congenital reduction in nephron number, raised blood pressure, proteinuria and chronic kidney disease in adulthood.Reference Luyckx, Bertram and Brenner66 Therefore, developmental programming as a consequence of these conditions may confound the associations between PE and offspring CVD risk. Low birthweight and prematurity both suggest exposure to a more severe placental disease and are mostly seen in early onset PE. Due to the interactions between genes, environment and potentially programming mechanisms, understanding the relative contribution of each of these mechanisms to the link between PE and CVD is complex and a combination of all three mechanisms appears the most plausible explanation.

Conclusion

Considering the current evidence, PE appears to have a long-term impact on the cardiovascular health of the offspring. Epidemiological evidence from long-term follow-up studies on humans shows that those exposed to PE in utero have higher blood pressure and higher BMI compared to those not exposed to PE in utero. The possible link between exposure to PE in utero and offspring risk for CVD is shown in Fig. 1. Three main mechanisms could explain the association between maternal PE and offspring CVD, and these are not mutually exclusive. Firstly, shared non-genetic (environmental and lifestyle exposures) risk factors may account for the association. Secondly, contributions from shared genetic variants to both PE and CVD risk are a plausible explanation. Thirdly, developmental programming due to exposure to the preeclamptic intrauterine environment can result in long-lasting effects on the cardiovascular health of the offspring. Animal models provide important insights into possible mechanistic pathways as they avoid confounding factors of shared lifestyle factors and can address specific in utero exposures. The different phenotypes of PE including early vs. late, severe vs. non-severe also make the interpretation of findings from different studies harder as each phenotype has different confounding factors.

Fig. 1. Potential mechanistic link between exposure to PE in utero and offspring risk for CVD.

In conclusion, there is strong evidence to demonstrate an association between maternal PE and offspring CVD. However, the mechanistic pathways leading to the risk for CVD after intrauterine exposure to PE are not yet clear. It is very likely that there is an overlap among all three mechanisms explored in this review and that dissecting the relative contribution of each pathway is impossible. Considering the risk for CVD among offspring exposed to PE in utero, primary preventive strategies are warranted in this target population.

Financial Support

ASC was supported by a Future Leader Fellowship (101998) from the National Heart Foundation of Australia. ZSL was supported by the NHMRC Australia Public Health Early Career Fellowship (GNT1141382). CTR was supported by the Lloyd Cox Professorial Research Fellowship from the University of Adelaide.

Conflicts of interest

The authors declare no conflicts of interest.

References

Duley, L.The global impact of pre-eclampsia and eclampsia. Semin. Perinatol. 2009; 33, 130137.CrossRefGoogle ScholarPubMed
Tranquilli, AL, Dekker, G, Magee, L, et al.The classification, diagnosis and management of the hypertensive disorders of pregnancy: a revised statement from the ISSHP. Pregnancy Hypertens. 2014; 4, 97104.Google ScholarPubMed
Bellamy, L, Casas, JP, Hingorani, AD, Williams, DJ.Pre-eclampsia and risk of cardiovascular disease and cancer in later life: systematic review and meta-analysis. BMJ (Clinical Research Edition) 2007; 335, 974.CrossRefGoogle ScholarPubMed
Brown, MC, Best, KE, Pearce, MS, Waugh, J, Robson, SC, Bell, R.Cardiovascular disease risk in women with pre-eclampsia: systematic review and meta-analysis. Eur J Epidemiol. 2013; 28, 119.CrossRefGoogle ScholarPubMed
Heida, KY, Bots, ML, de Groot, CJ, et al.Cardiovascular risk management after reproductive and pregnancy-related disorders: a Dutch multidisciplinary evidence-based guideline. Eur J Prevent Cardiol. 2016; 23, 18631879.CrossRefGoogle ScholarPubMed
Tranquilli, AL, Brown, MA, Zeeman, GG, Dekker, G, Sibai, BM.The definition of severe and early-onset preeclampsia. Statements from the International Society for the Study of Hypertension in Pregnancy (ISSHP). Pregnancy Hypertens. 2013; 3, 4447.CrossRefGoogle Scholar
Mosca, L, Benjamin, EJ, Berra, K, et al.Effectiveness-based guidelines for the prevention of cardiovascular disease in women–2011 update: a guideline from the american heart association. Circulation. 2011; 123, 12431262.CrossRefGoogle Scholar
Nahum Sacks, K, Friger, M, Shoham-Vardi, I, et al.Prenatal exposure to preeclampsia as an independent risk factor for long-term cardiovascular morbidity of the offspring. Pregnancy Hypertens. 2018; 13, 181186.CrossRefGoogle ScholarPubMed
Andraweera, PH, Lassi, ZS.Cardiovascular risk factors in offspring of preeclamptic pregnancies-systematic review and meta-analysis. J Pediatr. 2019; 208, 104113.e6.CrossRefGoogle ScholarPubMed
Anderson, CM, Lopez, F, Zimmer, A, Benoit, JN.Placental insufficiency leads to developmental hypertension and mesenteric artery dysfunction in two generations of Sprague-Dawley rat offspring. Biol Reprod. 2006; 74, 538544.Google ScholarPubMed
Davis, EF, Newton, L, Lewandowski, AJ, et al.Pre-eclampsia and offspring cardiovascular health: mechanistic insights from experimental studies. Clin Sci. (London, England : 1979) 2012; 123, 5372.CrossRefGoogle ScholarPubMed
Kvehaugen, AS, Dechend, R, Ramstad, HB, Troisi, R, Fugelseth, D, Staff, AC.Endothelial function and circulating biomarkers are disturbed in women and children after preeclampsia. Hypertension. 2011; 58, 6369.CrossRefGoogle ScholarPubMed
Jayet, PY, Rimoldi, SF, Stuber, T, et al.Pulmonary and systemic vascular dysfunction in young offspring of mothers with preeclampsia. Circulation. 2010; 122, 488494.CrossRefGoogle ScholarPubMed
Touwslager, RN, Houben, AJ, Gielen, M, et al.Endothelial vasodilatation in newborns is related to body size and maternal hypertension. J Hypertens. 2012; 30, 124131.CrossRefGoogle ScholarPubMed
Lazdam, M, de la Horra, A, Pitcher, A, et al.Elevated blood pressure in offspring born premature to hypertensive pregnancy: is endothelial dysfunction the underlying vascular mechanism? Hypertension. 2010; 56, 159165.CrossRefGoogle ScholarPubMed
Akcakus, M, Altunay, L, Yikilmaz, A, Yazici, C, Koklu, E.The relationship between abdominal aortic intima-media thickness and lipid profile in neonates born to mothers with preeclampsia. J Pediatr Endocrinol Metabol (JPEM). 2010; 23, 11431149.Google ScholarPubMed
McAloon, CJ, Boylan, LM, Hamborg, T, et al.The changing face of cardiovascular disease 2000–2012: An analysis of the world health organisation global health estimates data. Int J Cardiol. 2016; 224, 256264.CrossRefGoogle ScholarPubMed
Barker, DJ.Fetal growth and adult disease. Br J Obstet Gynaecol. 1992; 99, 275276.CrossRefGoogle ScholarPubMed
Barker, DJ.The effect of nutrition of the fetus and neonate on cardiovascular disease in adult life. Proc Nutr Soc. 1992; 51, 135144.CrossRefGoogle ScholarPubMed
Barker, DJ.The developmental origins of chronic adult disease. Acta Paediatr Suppl. 2004; 93, 2633.CrossRefGoogle ScholarPubMed
Murphy, MO, Cohn, DM, Loria, AS.Developmental origins of cardiovascular disease: impact of early life stress in humans and rodents. Neurosci Biobehav Rev. 2017; 74, 453465.CrossRefGoogle ScholarPubMed
Andraweera, PH, Dekker, GA, Roberts, CT.The vascular endothelial growth factor family in adverse pregnancy outcomes. Human Reprod Update. 2012; 18, 436457.CrossRefGoogle ScholarPubMed
Stojanovska, V, Scherjon, SA, Plosch, T.Preeclampsia as modulator of offspring health. Biol Reprod. 2016; 94, 53.Google ScholarPubMed
Staff, AC.The two-stage placental model of preeclampsia: an update. J Reprod Immunol. 2019; 134–135, 110.CrossRefGoogle ScholarPubMed
Redman, CWG, Sargent, IL.Placental stress and pre-eclampsia: a revised view. Placenta. 2009; 30, 3842.CrossRefGoogle ScholarPubMed
Brennan, LJ, Morton, JS, Davidge, ST.Vascular dysfunction in preeclampsia. Microcirculation. 2014; 21, 414.CrossRefGoogle ScholarPubMed
Roberts, JM, Taylor, RN, Goldfien, A.Clinical and biochemical evidence of endothelial cell dysfunction in the pregnancy syndrome preeclampsia. Am J Hypertens. 1991; 4, 700708.CrossRefGoogle ScholarPubMed
Myers, J, Mires, G, Macleod, M, Baker, P.In preeclampsia, the circulating factors capable of altering in vitro endothelial function precede clinical disease. Hypertension. 2005; 45, 258263.CrossRefGoogle ScholarPubMed
Kao, CK, Morton, JS, Quon, AL, Reyes, LM, Lopez-Jaramillo, P, Davidge, ST.Mechanism of vascular dysfunction due to circulating factors in women with pre-eclampsia. Clin Sci (Lond). 2016; 130, 539549.CrossRefGoogle ScholarPubMed
Lu, F, Bytautiene, E, Tamayo, E, et al.Gender-specific effect of overexpression of sFlt-1 in pregnant mice on fetal programming of blood pressure in the offspring later in life. Am J Obstetr Gynecol. 2007; 197, 418.e1418.e5.CrossRefGoogle ScholarPubMed
Aouache, R, Biquard, L, Vaiman, D, Miralles, F.Oxidative stress in preeclampsia and placental diseases. Int J Mol Sci. 2018; 19, pii: E1496.CrossRefGoogle ScholarPubMed
Myatt, L, Rosenfield, RB, Eis, AL, Brockman, DE, Greer, I, Lyall, F.Nitrotyrosine residues in placenta. Evidence of peroxynitrite formation and action. Hypertension. 1996; 28, 488493.CrossRefGoogle ScholarPubMed
Fujimaki, A, Watanabe, K, Mori, T, Kimura, C, Shinohara, K, Wakatsuki, A.Placental oxidative DNA damage and its repair in preeclamptic women with fetal growth restriction. Placenta. 2011; 32, 367372.Google ScholarPubMed
Hilali, N, Kocyigit, A, Demir, M, et al.DNA damage and oxidative stress in patients with mild preeclampsia and offspring. Eur J Obstet Gynecol Reprod Biol. 2013; 170, 377380.CrossRefGoogle ScholarPubMed
Wang, Z, Huang, Z, Lu, G, Lin, L, Ferrari, M.Hypoxia during pregnancy in rats leads to early morphological changes of atherosclerosis in adult offspring. Am J Physiol Heart Circ Physiol. 2009; 296, H1321H1328.CrossRefGoogle ScholarPubMed
Giussani, DA, Camm, EJ, Niu, Y, et al.Developmental programming of cardiovascular dysfunction by prenatal hypoxia and oxidative stress. PloS One. 2012; 7, e31017.CrossRefGoogle ScholarPubMed
Zhang, P, Zhu, D, Chen, X, et al.Prenatal hypoxia promotes atherosclerosis via vascular inflammation in the offspring rats. Atherosclerosis. 2016; 245, 2834.CrossRefGoogle ScholarPubMed
Santner-Nanan, B, Straubinger, K, Hsu, P, et al.Fetal–maternal alignment of regulatory T cells correlates with IL-10 and Bcl-2 upregulation in pregnancy. J Immunol. 2013; 191, 145.CrossRefGoogle ScholarPubMed
Hu, M, Eviston, D, Hsu, P, et al.Decreased maternal serum acetate and impaired fetal thymic and regulatory T cell development in preeclampsia. Nat Commun. 2019; 10, 3031.CrossRefGoogle ScholarPubMed
Nguyen Maria, U, Wallace Megan, J, Pepe, S, Menheniott, TR, Moss Timothy, J, Burgner, D.Perinatal inflammation: a common factor in the early origins of cardiovascular disease? Clin Sci. 2015; 129: 769784.CrossRefGoogle Scholar
Alexander, BT.Placental insufficiency leads to development of hypertension in growth-restricted offspring. Hypertension. 2003; 41: 457462.CrossRefGoogle ScholarPubMed
Alexander, BT, Hendon, AE, Ferril, G, Dwyer, TM.Renal denervation abolishes hypertension in low-birth-weight offspring from pregnant rats with reduced uterine perfusion. Hypertension. 2005; 45, 754758.CrossRefGoogle ScholarPubMed
Ojeda, NB, Grigore, D, Yanes, LL, et al.Testosterone contributes to marked elevations in mean arterial pressure in adult male intrauterine growth restricted offspring. Am J Physiol Regul Integr Comp Physiol. 2007; 292, R758R763.CrossRefGoogle ScholarPubMed
Heltemes, A, Gingery, A, Soldner, EL, et al.Chronic placental ischemia alters amniotic fluid milieu and results in impaired glucose tolerance, insulin resistance and hyperleptinemia in young rats. Exp Biol Med (Maywood). 2010; 235, 892899.CrossRefGoogle ScholarPubMed
Dasinger, JH, Intapad, S, Backstrom, MA, Carter, AJ, Alexander, BT.Intrauterine growth restriction programs an accelerated age-related increase in cardiovascular risk in male offspring. Am J Physiol Renal Physiol. 2016; 311, F312F319.CrossRefGoogle ScholarPubMed
Peyronnet, J, Roux, JC, Geloen, A, et al.Prenatal hypoxia impairs the postnatal development of neural and functional chemoafferent pathway in rat. J Physiol. 2000; 524(Pt 2), 525537.CrossRefGoogle ScholarPubMed
Tang, J, Zhu, Z, Xia, S, et al.Chronic hypoxia in pregnancy affected vascular tone of renal interlobar arteries in the offspring. Sci Rep. 2015; 5, 9723.CrossRefGoogle ScholarPubMed
Liu, B, Liu, Y, Shi, R, et al.Chronic prenatal hypoxia down-regulated BK channel beta1 subunits in mesenteric artery smooth muscle cells of the offspring. Cell Physiol Biochem. 2018; 45, 16031616.CrossRefGoogle ScholarPubMed
Jin, Z, Zhang, W, Yang, H, et al.Maternal treatment with agonistic autoantibodies against type-1 angiotensin II receptor in late pregnancy increases apoptosis of myocardial cells and myocardial susceptibility to ischemia-reperfusion injury in offspring rats. PloS One. 2013; 8, e80709.CrossRefGoogle ScholarPubMed
Herraiz, S, Pellicer, B, Serra, V, et al.Sildenafil citrate improves perinatal outcome in fetuses from pre-eclamptic rats. BJOG. 2012; 119, 13941402.CrossRefGoogle ScholarPubMed
McDonnold, M, Tamayo, E, Kechichian, T, et al.The effect of prenatal pravastatin treatment on altered fetal programming of postnatal growth and metabolic function in a preeclampsia-like murine model. Am J Obstet Gynecol. 2014; 210, 542 e1542 e7.CrossRefGoogle Scholar
Intapad, S, Tull, FL, Brown, AD, et al.Renal denervation abolishes the age-dependent increase in blood pressure in female intrauterine growth-restricted rats at 12 months of age. Hypertension. 2013; 61, 828834.CrossRefGoogle ScholarPubMed
Intapad, S, Dasinger, JH, Fahling, JM, Backstrom, MA, Alexander, BT.Testosterone is protective against impaired glucose metabolism in male intrauterine growth-restricted offspring. PloS One. 2017; 12, e0187843.CrossRefGoogle ScholarPubMed
Bytautiene, E, Tamayo, E, Kechichian, T, et al.Prepregnancy obesity and sFlt1-induced preeclampsia in mice: developmental programming model of metabolic syndrome. Am J Obstet Gynecol. 2011; 204, 398 e1398 e8.CrossRefGoogle ScholarPubMed
Intapad, S, Dasinger, JH, Brown, AD, Fahling, JM, Esters, J, Alexander, BT.Glucose intolerance develops prior to increased adiposity and accelerated cessation of estrous cyclicity in female growth-restricted rats. Pediatr Res. 2016; 79, 962970.CrossRefGoogle ScholarPubMed
Butruille, L, Mayeur, S, Moitrot, E, et al.Maternal hypertension induced by NO blockade does not program adult metabolic diseases in growth-restricted rat fetuses. Metabolism. 2013; 62, 442445.CrossRefGoogle Scholar
Payne, JA, Alexander, BT, Khalil, RA.Reduced endothelial vascular relaxation in growth-restricted offspring of pregnant rats with reduced uterine perfusion. Hypertension. 2003; 42, 768774.CrossRefGoogle ScholarPubMed
Peyronnet, J, Dalmaz, Y, Ehrstrom, M, et al.Long-lasting adverse effects of prenatal hypoxia on developing autonomic nervous system and cardiovascular parameters in rats. Pflugers Arch. 2002, 443, 858865.CrossRefGoogle ScholarPubMed
Wang, L, Li, M, Huang, Z, Wang, Z.The influence of hypoxia during different pregnancy stages on cardiac collagen accumulation in the adult offspring. Biomed Res Int. 2014; 2014, 419805.Google ScholarPubMed
Witlin, AG, Gangula, PR, Thompson, ML, Yallampalli, C.Growth and fertility rates in the offspring of pregnant rats treated with L-omega nitro-L-arginine methyl ester (L-NAME), a nitric oxide inhibitor. Am J Obstet Gynecol. 2002; 186, 8993.CrossRefGoogle Scholar
Allison, BJ, Kaandorp, JJ, Kane, AD, et al.Divergence of mechanistic pathways mediating cardiovascular aging and developmental programming of cardiovascular disease. FASEB J. 2016; 30, 19681975.CrossRefGoogle ScholarPubMed
Tang, J, Li, N, Chen, X, et al.Prenatal hypoxia induced dysfunction in cerebral arteries of offspring rats. J Am Heart Assoc. 2017; 6, pii: e006630.CrossRefGoogle ScholarPubMed
Martini, VC, Mandarim-de-Lacerda, CA. Offspring myocardium alteration from dams submitted to nitric oxide synthesis inhibition during pregnancy. Int J Cardiol. 2005; 100, 377382.CrossRefGoogle ScholarPubMed
Lock, MC, Tellam, RL, Botting, KJ, et al.The role of miRNA regulation in fetal cardiomyocytes, cardiac maturation and the risk of heart disease in adults. J Physiol. 2018; 596, 56255640.Google ScholarPubMed
Yeung, KR, Sunderland, N, Lind, JM, et al.Increased salt sensitivity in offspring of pregnancies complicated by experimental preeclampsia. Clin Exp Pharmacol Physiol. 2018; 45, 13021308.CrossRefGoogle ScholarPubMed
Luyckx, VA, Bertram, JF, Brenner, BM, et al.Effect of fetal and child health on kidney development and long-term risk of hypertension and kidney disease. Lancet. 2013; 382, 273283.CrossRefGoogle ScholarPubMed
Keller, G, Zimmer, G, Mall, G, Ritz, E, Amann, K.Nephron number in patients with primary hypertension. New Engl J Med. 2003; 348, 101108.CrossRefGoogle ScholarPubMed
Richter, VF, Briffa, JF, Moritz, KM, Wlodek, ME, Hryciw, DH.The role of maternal nutrition, metabolic function and the placenta in developmental programming of renal dysfunction. Clin Exp Pharmacol Physiol. 2016; 43, 135141.CrossRefGoogle ScholarPubMed
Marchand, MC, Langley-Evans, SC.Intrauterine programming of nephron number: the fetal flaw revisited. J Nephrol. 2001; 14, 327331.Google ScholarPubMed
Moritz, KM, Cuffe, JS, Wilson, LB, et al.Review: sex specific programming: a critical role for the renal renin-angiotensin system. Placenta. 2010; 31(Suppl), S40S46.CrossRefGoogle ScholarPubMed
Berdasco, M, Esteller, M.Clinical epigenetics: seizing opportunities for translation. Nat Rev Genet. 2019; 20, 109127.CrossRefGoogle ScholarPubMed
Karlsson, O, Baccarelli, AA.Environmental health and long non-coding RNAs. Curr Environ Health Rep. 2016; 3, 178187.CrossRefGoogle ScholarPubMed
Heindel, JJ. The developmental basis of disease: update on environmental exposures and animal models. Basic Clin Pharmacol Toxicol. 2019; 125(Suppl 3), 513.Google Scholar
Hanson, MA, Skinner, MK.Developmental origins of epigenetic transgenerational inheritance. Environ Epigenet. 2016; 2, pii: dvw002.CrossRefGoogle ScholarPubMed
Goyal, D, Limesand, SW, Goyal, R.Epigenetic responses and the developmental origins of health and disease. J Endocrinol. 2019; 242, T105T119.CrossRefGoogle ScholarPubMed
Hanson, M.The Inheritance Of Cardiovascular Disease Risk. Acta Paediatrica (Oslo, Norway : 1992). 2019; 108, 17471756.CrossRefGoogle ScholarPubMed
Apicella, C, Ruano, CSM, Mehats, C, Miralles, F, Vaiman, D.The role of epigenetics in placental development and the etiology of preeclampsia. Int J Molecul Sci. 2019; 20, pii: E2837.CrossRefGoogle ScholarPubMed
Bianco-Miotto, T, Mayne, BT, Buckberry, S, Breen, J, Rodriguez Lopez, CM, Roberts, CT.Recent progress towards understanding the role of DNA methylation in human placental development. Reproduction (Cambridge, England). 2016; 152, R23R30.CrossRefGoogle ScholarPubMed
Kazmi, N, Sharp, GC, Reese, SE, et al.Hypertensive disorders of pregnancy and DNA methylation in newborns. Hypertension. 2019; 74, 375383.CrossRefGoogle ScholarPubMed
Julian, CG, Pedersen, BS, Salmon, CS, et al.Unique DNA methylation patterns in offspring of hypertensive pregnancy. Clin Transl Sci. 2015; 8, 740745.CrossRefGoogle ScholarPubMed
Murray, R, Bryant, J, Titcombe, P, et al.DNA methylation at birth within the promoter of ANRIL predicts markers of cardiovascular risk at 9 years. Clin Epigenet. 2016; 8, 90.CrossRefGoogle ScholarPubMed
Tarrade, A, Panchenko, P, Junien, C, Gabory, A.Placental contribution to nutritional programming of health and diseases: epigenetics and sexual dimorphism. J Experiment Biol. 2015; 218, 5058.CrossRefGoogle ScholarPubMed
Andraweera, PH, Dekker, GA, Arstall, M, Bianco-Miotto, T, Roberts, CT.Complications of Pregnancy and Future Cardiovascular Risk. Encycl Cardiovasc Res Med. 2018; 1, 643650.CrossRefGoogle Scholar
Lie, RT, Rasmussen, S, Brunborg, H, Gjessing, HK, Lie-Nielsen, E, Irgens, LM.Fetal and maternal contributions to risk of pre-eclampsia: population based study. BMJ (Clinical Research Edition). 1998; 316, 13431347.CrossRefGoogle ScholarPubMed
Esplin, MS, Fausett, MB, Fraser, A, et al.Paternal and maternal components of the predisposition to preeclampsia. New Engl J Med. 2001; 344, 867872.CrossRefGoogle ScholarPubMed
Andraweera, PH, Dekker, GA, Thompson, SD, Roberts, CT.Single-nucleotide polymorphisms in the KDR gene in pregnancies complicated by gestational hypertensive disorders and small-for-gestational-age infants. Reprod Sci. 2012; 19, 547554.CrossRefGoogle ScholarPubMed
Andraweera, PH, Gatford, KL, Dekker, GA, et al.The INSR rs2059806 single nucleotide polymorphism, a genetic risk factor for vascular and metabolic disease, associates with pre-eclampsia. Reprod Biomed Online. 2017; 34, 392398.CrossRefGoogle ScholarPubMed
Andraweera, PH, Dekker, GA, Thompson, SD, Dissanayake, VH, Jayasekara, RW, Roberts, CT.Hypoxia-inducible factor-1alpha gene polymorphisms in early and late onset preeclampsia in Sinhalese women. Placenta. 2014; 35, 491495.CrossRefGoogle ScholarPubMed
Andraweera, PH, Dekker, GA, Thompson, SD, North, RA, McCowan, LM, Roberts, CT.A functional variant in ANGPT1 and the risk of pregnancies with hypertensive disorders and small-for-gestational-age infants. Mol Hum Reprod. 2012; 18, 325332.CrossRefGoogle ScholarPubMed
Sitras, V, Fenton, C, Acharya, G.Gene expression profile in cardiovascular disease and preeclampsia: a meta-analysis of the transcriptome based on raw data from human studies deposited in Gene Expression Omnibus. Placenta. 2015; 36, 170178.CrossRefGoogle ScholarPubMed
Johnson, MP, Fitzpatrick, E, Dyer, TD, et al.Identification of two novel quantitative trait loci for pre-eclampsia susceptibility on chromosomes 5q and 13q using a variance components-based linkage approach. Mol Hum Reprod. 2007; 13, 6167.CrossRefGoogle ScholarPubMed
Loset, M, Johnson, MP, Melton, PE, et al.Preeclampsia and cardiovascular disease share genetic risk factors on chromosome 2q22. Pregnancy Hypertens. 2014; 4, 178185.CrossRefGoogle ScholarPubMed
Cheong, JN, Wlodek, ME, Moritz, KM, Cuffe, JS.Programming of maternal and offspring disease: impact of growth restriction, fetal sex and transmission across generations. J Physiol. 2016; 594, 47274740.CrossRefGoogle Scholar
Alsnes, IV, Vatten, LJ, Fraser, A, et al.Hypertension in pregnancy and offspring cardiovascular risk in young adulthood: prospective and sibling studies in the HUNT Study (Nord-Trondelag Health Study) in Norway. Hypertension. 2017; 69, 591598.CrossRefGoogle Scholar
Hughson, M, Farris, AB, 3rd, Douglas-Denton, R, Hoy, WE, Bertram, JF.Glomerular number and size in autopsy kidneys: the relationship to birth weight. Kidney Int. 2003; 63, 21132122.CrossRefGoogle ScholarPubMed
Figure 0

Fig. 1. Potential mechanistic link between exposure to PE in utero and offspring risk for CVD.