177 results on '"Claire T. Roberts"'
Search Results
2. The association of breast feeding for at least six months with hemodynamic and metabolic health of women and their children aged three years: an observational cohort study
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Maleesa M. Pathirana, Prabha H. Andraweera, Emily Aldridge, Madeline Harrison, Jade Harrison, Shalem Leemaqz, Margaret A. Arstall, Gustaaf A. Dekker, and Claire T. Roberts
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Breastfeeding ,Pregnancy complications ,Maternal and child health ,Pediatrics ,RJ1-570 ,Public aspects of medicine ,RA1-1270 - Abstract
Abstract Background Breastfeeding is important for both mother and child in reducing risk of future cardiovascular disease. Therefore, it may be an effective method to improve cardio-metabolic health, particularly those who are exposed to pregnancy complications which increase later CVD risk for both mother and child. The aim of this study is to assess differences in cardiometabolic health at three years postpartum in mothers who breastfed for at least six months and their children compared to those who did not. Methods Women and children from the Screening Tests to Predict Poor Outcomes of Pregnancy (STOP) study (2015–2017) were invited to attend a health check-up at three years postpartum. Women’s breastfeeding status at least six months postpartum was ascertained through their child health record. Anthropometric and hemodynamic measurements were taken from women and their children. A fasting blood sample was taken from women to measure blood glucose and lipids. Results A total of 160 woman-child dyads were assessed in this study. Women who breastfed for at least six months had significantly lower maternal BMI, systolic blood pressure, diastolic blood pressure, mean arterial pressure, central systolic blood pressure, and central diastolic blood pressure than those who did not and this did not change after adjusting for BMI and socioeconomic index in early pregnancy, prenatal smoking and maternal age in early pregnancy. Subgroup analysis on women who had one or more pregnancy complications during the index pregnancy (i.e. preeclampsia, gestational hypertension, delivery of a small for gestational age infant, delivery of a preterm infant, and/or gestational diabetes mellitus) demonstrated that women who breastfed for at least six months had significantly lower maternal systolic and diastolic blood pressures, serum insulin and triglycerides, and higher HDL cholesterol. There were no differences in child anthropometric or hemodynamic variables at three years of age between those children who had been breastfed for at least six months and those who had not. Conclusion Breastfeeding for at least six months may reduce some maternal; cardiovascular risk factors in women at three years postpartum, in particular, in those who have experienced a complication of pregnancy. Trial registration ACTRN12614000985684 (12/09/2014).
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- 2023
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3. Asymmetric growth-limiting development of the female conceptus
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Consuelo Amor S. Estrella, Kathryn L. Gatford, Ruidong Xiang, Ali Javadmanesh, Mani Ghanipoor-Samami, Greg S. Nattrass, Entesar Shuaib, Milton M. McAllister, Ian Beckman, Dana A. Thomsen, Vicki L. Clifton, Julie A. Owens, Claire T. Roberts, Stefan Hiendleder, and Karen L. Kind
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conceptus ,uncomplicated pregnancy ,sex differences ,asymmetric growth ,IGF system ,histomorphology ,Diseases of the endocrine glands. Clinical endocrinology ,RC648-665 - Abstract
IntroductionSex differences in prenatal growth may contribute to sex-dependent programming effects on postnatal phenotype. MethodsWe integrated for the first time phenotypic, histomorphological, clinico-chemical, endocrine and gene expression analyses in a single species, the bovine conceptus at mid-gestation. ResultsWe demonstrate that by mid-gestation, before the onset of accelerated growth, the female conceptus displays asymmetric lower growth compared to males. Female fetuses were smaller with lower ponderal index and organ weights than males. However, their brain:body weight, brain:liver weight and heart:body weight ratios were higher than in males, indicating brain and heart ‘sparing’. The female placenta weighed less and had lower volumes of trophoblast and fetal connective tissue than the male placenta. Female umbilical cord vessel diameters were smaller, and female-specific relationships of body weight and brain:liver weight ratios with cord vessel diameters indicated that the umbilico-placental vascular system creates a growth-limiting environment where blood flow is redistributed to protect brain and heart growth. Clinico-chemical indicators of liver perfusion support this female-specific growth-limiting phenotype, while lower insulin-like growth factor 2 (IGF2) gene expression in brain and heart, and lower circulating IGF2, implicate female-specific modulation of key endocrine mediators by nutrient supply. ConclusionThis mode of female development may increase resilience to environmental perturbations in utero and contribute to sex-bias in programming outcomes including susceptibility to non-communicable diseases.
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- 2024
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4. A prospective registry analysis of psychosocial and metabolic health between women with and without metabolic syndrome after a complicated pregnancy
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Emily Aldridge, K. Oliver Schubert, Maleesa Pathirana, Susan Sierp, Shalem Y. Leemaqz, Claire T. Roberts, Gustaaf A. Dekker, and Margaret A. Arstall
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Maternal health ,Metabolic syndrome ,Pregnancy complications ,Maternal mental health ,Gynecology and obstetrics ,RG1-991 ,Public aspects of medicine ,RA1-1270 - Abstract
Abstract Purpose Pregnancy complications affect over one quarter of Australian pregnancies, and this group of mothers is vulnerable and more likely to experience adverse cardiometabolic health outcomes in the postpartum period. Metabolic syndrome is common in this population and may be associated with postpartum mental health issues. However, this relationship remains poorly understood. To compare the differences in psychosocial parameters and mental health outcomes between women with metabolic syndrome and women without metabolic syndrome 6 months after a complicated pregnancy. Methods This study is prospective registry analysis of women attending a postpartum healthy lifestyle clinic 6 months following a complicated pregnancy. Mental health measures included 9-item Patient Health Questionnaire (PHQ-9), 7-item Generalised Anxiety Disorder questionnaire (GAD-7), self-reported diagnosed history of depression, anxiety and/or other psychiatric condition, and current psychotropic medication use. Results Women with metabolic syndrome reported significantly more subjective mental health concerns, were more likely to have a history of depression and other psychiatric diagnoses and were more likely prescribed psychotropic medications. However, there were no significant differences in PHQ-9 and GAD-7 scores. Conclusion Amongst new mothers who experienced complications of pregnancy, those with metabolic syndrome represent a particularly vulnerable group with regards to psychosocial disadvantage and mental health outcomes. These vulnerabilities may not be apparent when using common standardised cross-sectional mental health screening tools such as PHQ-9 and GAD-7.
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- 2022
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5. Effectiveness of a nurse practitioner-led cardiovascular prevention clinic at reduction of metabolic syndrome following maternal complications of pregnancy: a preliminary analysis
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Emily Aldridge, Maleesa Pathirana, Melanie Wittwer, Susan Sierp, Shalem Y. Leemaqz, Claire T. Roberts, Gustaaf A. Dekker, and Margaret A. Arstall
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Metabolic syndrome ,Cardiovascular disease prevention ,Pregnancy complications ,Maternal health ,Nutritional diseases. Deficiency diseases ,RC620-627 - Abstract
Abstract Aim Maternal complications of pregnancy, including hypertensive disorders of pregnancy, gestational diabetes mellitus, intrauterine growth restriction, preterm labour, and placental abruption, are associated with increased risk of future cardiometabolic disease. Lifestyle interventions that focus on preventative strategies for this young, high-risk population of women may assist in cardiometabolic disease risk reduction. The aim of this preliminary registry analysis was to observe the change in maternal metabolic syndrome status after receiving a nurse practitioner-led lifestyle intervention delivered soon after a complicated pregnancy. Method This preliminary analysis included 64 eligible women who had attended both baseline (approximately 6 months postpartum) and review (approximately eighteen months postpartum) appointments at the postpartum lifestyle clinic after an index pregnancy complicated by at least one maternal complication of pregnancy. Metabolic syndrome status at both appointments was assessed. Results At the baseline appointment, 22 (34.4%) women met the criteria for metabolic syndrome. This number reduced at the review appointment to 19 (29.7%). This difference was not statistically significant. There were some modest improvements in the individual cardiometabolic risk factors, as well as marked improvements in the women who had recovered from metabolic syndrome over twelve months. Conclusion There was a high percentage of metabolic syndrome present early in the postpartum period. The results of this preliminary analysis highlight the importance of continuing preventative care and ongoing research for this group of high-risk women.
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- 2022
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6. ‘Fetal side’ of the placenta: anatomical mis-annotation of carbon particle ‘transfer’ across the human placenta
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Beth Holder, John D. Aplin, Nardhy Gomez-Lopez, Alexander E. P. Heazell, Joanna L. James, Carolyn J. P. Jones, Helen Jones, Rohan M. Lewis, Gil Mor, Claire T. Roberts, Sarah A. Robertson, and Ana C. Zenclussen
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Science - Published
- 2021
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7. Prevalence of Metabolic Syndrome in Women After Maternal Complications of Pregnancy: An Observational Cohort Analysis
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Emily Aldridge, Maleesa Pathirana, Melanie Wittwer, Susan Sierp, Shalem Y. Leemaqz, Claire T. Roberts, Gustaaf A. Dekker, and Margaret A. Arstall
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metabolic syndrome ,pregnancy complications ,cardiovascular disease ,cardiovascular disease prevention ,women ,Diseases of the circulatory (Cardiovascular) system ,RC666-701 - Abstract
IntroductionCertain complications of pregnancy, including hypertensive disorders of pregnancy, gestational diabetes mellitus, intrauterine growth restriction, spontaneous preterm birth, and placental abruption, are established independent risk factors for premature cardiovascular disease in women. Metabolic syndrome, which is associated with an increased risk of cardiovascular disease, may be a suitable alternative to traditional cardiovascular risk calculators that underestimate risk in young women. This study aimed to investigate the prevalence of metabolic syndrome in women who experienced a complicated pregnancy 6 months earlier.MethodsThis observational study investigated the prevalence of metabolic syndrome as defined by the International Diabetes Federation in all eligible participants (n = 247) attending a postpartum lifestyle intervention clinic from August 2018 to June 2021 at the Lyell McEwin Hospital in Adelaide, South Australia.ResultsA total of 89 (36%) participants met the criteria for metabolic syndrome at a mean follow up time of 7 months postpartum. Almost 90% of the cohort were abdominally obese, and over two thirds of the total cohort met at least two of the criteria for metabolic syndrome.ConclusionsWomen with a prior history of one of the common major pregnancy complications are at high risk of future cardiovascular and metabolic disease, with many showing either metabolic syndrome or multiple risk factors at only 7 months postpartum. The results indicate that follow-up within 1 year postpartum is an appropriate time to commence preventative strategies, as many women are already showing early signs of disease.
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- 2022
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8. Placental Inflammasome mRNA Levels Differ by Mode of Delivery and Fetal Sex
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Anya L. Arthurs, Melanie D. Smith, Mhyles D. Hintural, James Breen, Dylan McCullough, Francesca I. Thornton, Shalem Y. Leemaqz, Gustaaf A. Dekker, Tanja Jankovic-Karasoulos, and Claire T. Roberts
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placenta ,inflammation ,pregnancy ,labour ,parturition ,inflammasome ,Immunologic diseases. Allergy ,RC581-607 - Abstract
Parturition signals the end of immune tolerance in pregnancy. Term labour is usually a sterile inflammatory process triggered by damage associated molecular patterns (DAMPs) as a consequence of functional progesterone withdrawal. Activation of DAMPs recruits leukocytes and inflammatory cytokine responses in the myometrium, decidua, cervix and fetal membranes. Emerging evidence shows components of the inflammasome are detectable in both maternal decidua and placenta. However, the activation of the placental inflammasome with respect to mode of delivery has not been profiled. Placental chorionic villus samples from women delivering at term via unassisted vaginal (UV) birth, labouring lower segment caesarean section (LLSCS, emergency caesarean section) and prelabour lower segment caesarean section (PLSCS, elective caesarean section) underwent high throughput RNA sequencing (NextSeq Illumina) and bioinformatic analyses to identify differentially expressed inflammatory (DE) genes. DE genes (IL1RL1, STAT1, STAT2, IL2RB, IL17RE, IL18BP, TNFAIP2, TNFSF10 and TNFRSF8), as well as common inflammasome genes (IL1B, IL1R1, IL1R2, IL6, IL18, IL18R1, IL18R1, IL10, and IL33), were targets for further qPCR analyses and Western blotting to quantify protein expression. There was no specific sensor molecule-activated inflammasome which dominated expression when stratified by mode of delivery, implying that multiple inflammasomes may function synergistically during parturition. Whilst placentae from women who had UV births overall expressed pro-inflammatory mediators, placentae from LLSCS births demonstrated a much greater pro-inflammatory response, with additional interplay of pro- and anti-inflammatory mediators. As expected, inflammasome activation was very low in placentae from women who had PLSCS births. Sex-specific differences were also detected. Placentae from male-bearing pregnancies displayed higher inflammasome activation in LLSCS compared with PLSCS, and placentae from female-bearing pregnancies displayed higher inflammasome activation in LLSCS compared with UV. In conclusion, placental inflammasome activation differs with respect to mode of delivery and neonatal sex. Its assessment may identify babies who have been exposed to aberrant inflammation at birth that may compromise their development and long-term health and wellbeing.
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- 2022
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9. Sex- and growth-specific characteristics of small for gestational age infants: a prospective cohort study
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Eva R. van der Vlugt, Petra E. Verburg, Shalem Y. Leemaqz, Lesley M. E. McCowan, Lucilla Poston, Louise C. Kenny, Jenny Myers, James J. Walker, Gustaaf A. Dekker, Claire T. Roberts, and on behalf of the SCOPE Consortium
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Small for gestational age ,Sexual dimorphism ,Risk factor ,Asymmetric growth ,Symmetric growth ,Medicine ,Physiology ,QP1-981 - Abstract
Abstract Background Asymmetric fetal growth and male sex are both associated with adverse neonatal outcome. However, less is known about the influence of asymmetric growth and fetal sex within SGA neonates, a group of infants already at increased risk for adverse neonatal outcomes. The aim of the present study was to provide insight into variance in risk factors for SGA in a fetal sex- and growth symmetry-specific way. Methods For this prospective, multicenter cohort study, data from the Screening for Pregnancy Endpoints (SCOPE) study were used with 5628 nulliparous participants, of which 633 (11.3%) pregnancies were complicated with SGA and 3376 (60.0%) women had uncomplicated pregnancies. Association between risk factors for SGA, SGA subgroups, and uncomplicated pregnancies were assessed with multivariable analyses. Results Prevalence of asymmetric growth varied from 45.8% of SGA infants to 5.5% of infants with a customized birthweight > 90th percentile (p < 0.001). Significantly more SGA males had asymmetric growth compared to SGA female infants (51.2% vs 40.4%, p = 0.009). Maternal pre-pregnancy diet and BMI < 20 and ≥ 30 were significantly associated with symmetric SGA but not with asymmetric SGA. Asymmetric SGA infants had not only lower customized birthweight percentile (4.4 (SD 2.8) vs 5.0 (SD 3.0), p < 0.001), but also lower rates of stillbirth (p = 0.041) and less often Apgar scores < 7 (p = 0.060). Conclusions Among SGA infants, low customized birthweight percentiles and male sex are associated with asymmetric growth. Only symmetric SGA is significantly associated with maternal risk factors in early pregnancy. There is a substantial variance in risk factors and neonatal outcomes for SGA based on growth symmetry, implying a different pathogenesis. Trial registration ACTRN12607000551493
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- 2020
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10. Characterization of 5-methylcytosine and 5-hydroxymethylcytosine in human placenta cell types across gestation
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Rebecca L. Wilson, Maxime François, Tanja Jankovic-Karasoulos, Dale McAninch, Dylan McCullough, Wayne R. Leifert, Claire T. Roberts, and Tina Bianco-Miotto
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placenta ,5-methylcytosine ,5-hydroxymethylcytosine ,preeclampsia ,cytotrophoblast ,syncytiotrophoblast ,Genetics ,QH426-470 - Abstract
The placenta is an important organ in pregnancy, however, very little is understood about placental development at a molecular level. This includes the role of epigenetic mechanisms and how they change throughout gestation. DNA methylation studies in this organ are complicated by the different cell types that make up the placenta, each with their own unique transcriptome and epigenome. Placental dysfunction is often associated with pregnancy complications such as preeclampsia (PE). Aberrant DNA methylation in the placenta has been identified in pregnancy complications. We used immunohistochemistry (IHC) and immunofluorescence (IF) to localize 5-methylcytosine (5-mC) and 5-hydroxymethylcytosine (5-hmC) in placenta tissue from first and second trimester as well as uncomplicated term and PE samples. IHC analysis of whole placental tissues showed 5-mC increased across gestation. When cytotrophoblasts (CTB) and syncytiotrophoblasts (STB) were isolated and assessed using IF, both 5-mC and 5-hmC increased in term CTBs compared to first/second-trimester samples. Staining intensity of 5-hmC was higher in first/second trimester STBs compared to CTBs (P = 0.0011). Finally, IHC staining of term tissue from PE and uncomplicated pregnancies revealed higher 5-mC staining intensity in placentas from PE pregnancies (P = 0.028). Our study has shown increased 5-mC and 5-hmC staining intensities across gestation and differed between two trophoblast populations. Differences in DNA methylation profiles between placental cell types may be indicative of different functions and requires further study to elucidate what changes accompany placental pathologies.
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- 2019
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11. Safety and protective effects of maternal influenza vaccination on pregnancy and birth outcomes: A prospective cohort study
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Hassen Mohammed, Claire T. Roberts, Luke E. Grzeskowiak, Lynne C. Giles, Gustaaf A. Dekker, and Helen S. Marshall
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Medicine (General) ,R5-920 - Abstract
Background: Our study aimed to assess the safety and protective effect of maternal influenza vaccination on pregnancy and birth outcomes. Methods: The study population comprised 1253 healthy nulliparous pregnant women in South Australia between 2015 and 2018. Participants were followed prospectively, with vaccination status (confirmed by medical records), pregnancy, and birth outcome data collected by midwives. Adjusted relative risks (aRRs) and adjusted hazard ratios (aHRs) were estimated accounting for time-varying vaccine exposure and temporal nature of each outcome. Findings: Maternal influenza vaccination (48%, 603 of 1253) reduced the risk for pre-delivery hospitalisation with influenza like illness (aHR 0•61; 95% CI 0•39, 0•97). Maternal influenza vaccination was not associated with spontaneous abortion (aHR 0•42, 95% CI 0•12, 1•45), chorioamnionitis (aRR 0•78, 95% CI, 0•32, 1•88), gestational hypertension (aHR 0•78, 95% CI 0•47, 1•29), pre-eclampsia (aHR 0.84, 95% CI 0•54, 1•27), gestational diabetes (aHR 1•16, 95% CI 0•82, 1•66) nor preterm birth (aHR 0•94, 95% CI 0•59, 1•49). No associations between antenatal influenza vaccination and congenital anomalies, admission to the neonatal care unit, low Apgar scores, and mechanical ventilation were observed. Results were not materially changed after adjustment for pertussis vaccination. We observed a protective effect of maternal influenza vaccination on low birth weight (aHR 0•46, 95% CI 0•23, 0•94) and a marginal protective effect on small for gestational age births (aHR 0•65, 95% CI 0•40, 1•04) during periods of high influenza activity. Interpretation: These results support the safety of maternal influenza vaccination and suggest a protective effect in reducing the rates of low birthweight and small for gestational age births. Funding: There was no funding for this study.
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- 2020
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12. A Protocol for Nurse-Practitioner Led Cardiovascular Follow-Up After Pregnancy Complications in a Socioeconomically Disadvantaged Population
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Emily Aldridge, Petra E. Verburg, Susan Sierp, Prabha Andraweera, Gustaaf A. Dekker, Claire T. Roberts, and Margaret A. Arstall
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cardiovascular disease ,pregnancy complications ,postpartum follow-up ,lifestyle intervention ,prevention ,women ,Diseases of the circulatory (Cardiovascular) system ,RC666-701 - Abstract
Background: Women who experience pregnancy complications have an increased risk of future cardiovascular disease when compared to their healthy counterparts. Despite recommendations, there is no standardized cardiovascular follow-up in the postpartum period for these women, and the Australian follow-up protocols that have been previously described are research-based. This study proposes a new model of care for a nurse practitioner-led postpartum intervention clinic for women who experience severe hypertensive disorders of pregnancy, gestational diabetes mellitus requiring medication, severe intrauterine growth restriction, idiopathic preterm delivery, or placental abruption, in a socioeconomically disadvantaged population.Methods: All women receiving antenatal care or who deliver at the Lyell McEwin Hospital, a tertiary acute care facility located in the northern Adelaide metropolitan area, following a severe complication of pregnancy are referred to the intervention clinic for review at 6 months postpartum. A comprehensive assessment is conducted from demographics, medical history, diet and exercise habits, psychosocial information, health literacy, pathology results, and physical measurements. Subsequently, patient-specific education and clinical counseling are provided by a specialized nurse practitioner. Clinic appointments are repeated at 18 months and 5 years postpartum. All data is also collated into a registry, which aims to assess the efficacy of the intervention at improving modifiable cardiovascular risk factors and reducing cardiovascular risk.Discussion: There is limited information on the efficacy of postpartum intervention clinics in reducing cardiovascular risk in women who have experienced pregnancy complications. Analyses of the data collected in the registry will provide essential information about how best to reduce cardiovascular risk in women in socioeconomically disadvantaged and disease-burdened populations.
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- 2020
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13. Vitamin D levels in an Australian and New Zealand cohort and the association with pregnancy outcome
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Rebecca L. Wilson, Alison J. Leviton, Shalem Y. Leemaqz, Paul H. Anderson, Jessica A. Grieger, Luke E. Grzeskowiak, Petra E. Verburg, Lesley McCowan, Gustaaf A. Dekker, Tina Bianco-Miotto, and Claire T. Roberts
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Vitamin D ,Pregnancy ,Pregnancy outcome ,Gestational diabetes mellitus ,Fetal sex ,Gynecology and obstetrics ,RG1-991 - Abstract
Abstract Background Pregnant women are at increased susceptibility to vitamin D deficiency. Hence, there is continuing interest in determining how vitamin D influences pregnancy health. We aimed to compare vitamin D status in two distinct populations of pregnant women in Australia and New Zealand and to investigate the relationship between vitamin D status and pregnancy outcome. This included evaluating possible effect measure modifications according to fetal sex. Methods Serum 25-hydroxy vitamin D (25(OH)D) was measured at 15 ± 1 weeks’ gestation in 2800 women from Adelaide and Auckland who participated in the multi-centre, prospective cohort SCreening fOr Pregnancy Endpoints (SCOPE) study. Results Mean serum 25(OH)D in all women was 68.1 ± 27.1 nmol/L and 28% (n = 772) were considered vitamin D deficient ( 81 nmol/L) “standardised” vitamin D status when compared to moderate-high (63–81 nmol/L, aRR, 0.47; 95% CI: 0.23, 0.96). Marginal sex-specific differences occurred between vitamin D status and GDM: women carrying a female fetus had a 56% decreased risk for GDM in those with low-moderate levels of standardised vitamin D (44–63 nmol/L) compared to moderate-high levels (aRR: 0.44; 95% CI: 0.20, 0.97), whilst in women carrying a male fetus, a 55% decreased risk of GDM was found with high standardised vitamin D when compared to moderately-high vitamin D, but this was not statistically significant (aRR: 0.45; 95% CI: 0.15, 1.38). Conclusions High serum 25(OH)D at 15 ± 1 weeks’ gestation was shown to be protective against the development of GDM. A possible association between fetal sex, vitamin D status and GDM provides further questions and encourages continual research and discussion into the role of vitamin D in pregnancy, particularly in vitamin D replete populations.
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- 2018
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14. Increased methylation and decreased expression of homeobox genes TLX1, HOXA10 and DLX5 in human placenta are associated with trophoblast differentiation
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Boris Novakovic, Thierry Fournier, Lynda K. Harris, Joanna James, Claire T. Roberts, Hannah E. J. Yong, Bill Kalionis, Danièle Evain-Brion, Peter R. Ebeling, Euan M. Wallace, Richard Saffery, and Padma Murthi
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Medicine ,Science - Abstract
Abstract Homeobox genes regulate embryonic and placental development, and are widely expressed in the human placenta, but their regulatory control by DNA methylation is unclear. DNA methylation analysis was performed on human placentae from first, second and third trimesters to determine methylation patterns of homeobox gene promoters across gestation. Most homeobox genes were hypo-methylated throughout gestation, suggesting that DNA methylation is not the primary mechanism involved in regulating HOX genes expression in the placenta. Nevertheless, several genes showed variable methylation patterns across gestation, with a general trend towards an increase in methylation over gestation. Three genes (TLX1, HOXA10 and DLX5) showed inverse gains of methylation with decreasing mRNA expression throughout pregnancy, supporting a role for DNA methylation in their regulation. Proteins encoded by these genes were primarily localised to the syncytiotrophoblast layer, and showed decreased expression later in gestation. siRNA mediated downregulation of DLX5, TLX1 and HOXA10 in primary term villous cytotrophoblast resulted in decreased proliferation and increased expression of differentiation markers, including ERVW-1. Our data suggest that loss of DLX5, TLX1 and HOXA10 expression in late gestation is required for proper placental differentiation and function.
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- 2017
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15. Viperin is an important host restriction factor in control of Zika virus infection
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Kylie H. Van der Hoek, Nicholas S. Eyre, Byron Shue, Onruedee Khantisitthiporn, Kittirat Glab-Ampi, Jillian M. Carr, Matthew J. Gartner, Lachlan A. Jolly, Paul Q. Thomas, Fatwa Adikusuma, Tanja Jankovic-Karasoulos, Claire T. Roberts, Karla J. Helbig, and Michael R. Beard
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Medicine ,Science - Abstract
Abstract Zika virus (ZIKV) infection has emerged as a global health threat and infection of pregnant women causes intrauterine growth restriction, spontaneous abortion and microcephaly in newborns. Here we show using biologically relevant cells of neural and placental origin that following ZIKV infection, there is attenuation of the cellular innate response characterised by reduced expression of IFN-β and associated interferon stimulated genes (ISGs). One such ISG is viperin that has well documented antiviral activity against a wide range of viruses. Expression of viperin in cultured cells resulted in significant impairment of ZIKV replication, while MEFs derived from CRISPR/Cas9 derived viperin−/− mice replicated ZIKV to higher titers compared to their WT counterparts. These results suggest that ZIKV can attenuate ISG expression to avoid the cellular antiviral innate response, thus allowing the virus to replicate unchecked. Moreover, we have identified that the ISG viperin has significant anti-ZIKV activity. Further understanding of how ZIKV perturbs the ISG response and the molecular mechanisms utilised by viperin to suppress ZIKV replication will aid in our understanding of ZIKV biology, pathogenesis and possible design of novel antiviral strategies.
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- 2017
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16. The effect of Vdr gene ablation on global gene expression in the mouse placenta
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Sam Buckberry, Fleur Spronk, Rebecca L. Wilson, Jessica A. Laurence, Tina Bianco-Miotto, Shalem Leemaqz, Sean O'Leary, Paul H. Anderson, and Claire T. Roberts
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Vitamin D ,Placenta ,Gene expression ,VDR ,Genetics ,QH426-470 - Abstract
The effects of vitamin D are mediated through the vitamin D receptor (VDR), a predominantly nuclear receptor, expressed in numerous tissues including the placenta. VDR and the retinoid X receptor (RXR) form a dimer complex which binds to genomic vitamin D responsive elements located primarily in promoter regions and recruit cell-specific transcription factor complexes which regulate the expression of numerous genes. To investigate the role of VDR on regulating placental gene expression, mice heterozygous (+/−) for an ablated Vdr allele (C57Bl6 strain B6.129S4-VDRtm1Mbd/J, Jackson Laboratory) were mated to generate Vdr+/+, Vdr+/− and Vdr −/− fetuses and placental samples were collected at day 18.5 of pregnancy. RNA was isolated from placental tissue with global gene expression measured using Affymetrix Mouse Gene 2.1 ST Arrays to assess the effects of VDR on global gene expression in the placenta. All raw array data are deposited in Gene Expression Omnibus (GEO) under accession GSE61583.
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- 2015
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17. Bioengineered Microphysiological Placental Models: Towards Improving Understanding of Pregnancy Health and Disease
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Claire T. Roberts, Tanja Jankovic-Karasoulos, Marnie Winter, Tina Bianco-Miotto, Benjamin Thierry, Winter, Marnie, Jankovic-Karasoulos, Tanja, Roberts, Claire T, Bianco-Miotto, Tina, and Thierry, Benjamin
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0301 basic medicine ,Pregnancy ,microphysiological systems ,business.industry ,Placenta ,microfluidics ,Bioengineering ,Human placenta ,02 engineering and technology ,Disease ,021001 nanoscience & nanotechnology ,medicine.disease ,03 medical and health sciences ,030104 developmental biology ,medicine.anatomical_structure ,medicine ,Humans ,Female ,0210 nano-technology ,business ,in vitro placental models ,Neuroscience ,Biotechnology - Abstract
Driven by a lack of appropriate human placenta models, recent years have seen the introduction of bioengineered in vitro models to better understand placental health and disease. Thus far, the focus has been on the maternal–foetal barrier. However, there are many other physiologically and pathologically significant aspects of the placenta that would benefit from state-of-the-art bioengineered models, in particular, integrating advanced culture systems with contemporary biological concepts such as organoids. This critical review defines and discusses the key parameters required for the development of physiologically relevant in vitro models of the placenta. Specifically, it highlights the importance of cell type, mechanical forces, and culture microenvironment towards the use of physiologically relevant models to improve the understanding of human placental function and dysfunction. Refereed/Peer-reviewed
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- 2021
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18. Relative importance of metabolic syndrome components for developing gestational diabetes
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Claire T. Roberts, Jessica A. Grieger, Lesley M. E. McCowan, Gustaaf A. Dekker, Emma Knight, Shalem Leemaqz, and Luke E. Grzeskowiak
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medicine.medical_specialty ,Pregnancy ,Waist ,endocrine system diseases ,Obstetrics ,business.industry ,nutritional and metabolic diseases ,Obstetrics and Gynecology ,General Medicine ,medicine.disease ,Logistic regression ,female genital diseases and pregnancy complications ,Gestational diabetes ,Blood pressure ,medicine ,Gestation ,Metabolic syndrome ,Risk factor ,business - Abstract
To assess the independent and joint contribution of the individual components of metabolic syndrome, and known risk factors for gestational diabetes (GDM), on risk of GDM. Two thousand nine hundred and fifteen women from Australia and New Zealand, who participated in The Screening for Pregnancy Endpoints Study (SCOPE), were included. Using the SCOPE clinical data set and biomarkers obtained at 14–16 weeks’ gestation, a logistic regression model was fitted to the binary outcome GDM, with individual metabolic syndrome components (waist circumference, blood pressure, glucose, HDL-C, triglycerides), recruitment site, and other established factors associated with GDM. Hierarchical partitioning was used to assess the relative contribution of each variable. Of the 2915 women, 103 women (3.5%) developed GDM. The deviance explained by the logistic regression model containing all variables was 18.65% and the AUC was 0.809. Seventy percent of the independent effect was accounted for by metabolic syndrome components. The highest independent relative contribution to GDM was circulating triglycerides (17 ± 3%), followed by waist circumference (13 ± 3%). Glucose and maternal BMI contributed 12 ± 2% and 12 ± 3%, respectively. The remaining factors had an independent relative contribution of
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- 2021
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19. Large-scale transcriptome-wide profiling of microRNAs in human placenta and maternal plasma at early to mid gestation
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Dale McAninch, Claire T. Roberts, Tanja Jankovic-Karasoulos, Katherine A. Pillman, Melanie D. Smith, Tina Bianco-Miotto, K. Justinian Bogias, James Breen, Qianhui Wan, Dylan McCullough, Smith, Melanie D, Pillman, Katherine, Jankovic-Karasoulos, Tanja, McAninch, Dale, Wan, Qianhui, Bogias, K Justinian, McCullough, Dylan, Bianco-Miotto, Tina, Breen, James, and Roberts, Claire T
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Male ,placenta ,Gestational Age ,Biology ,Bioinformatics ,Andrology ,Transcriptome ,Pregnancy ,Placenta ,parasitic diseases ,microRNA ,medicine ,Humans ,DLK1-DI03 ,Maternal-Fetal Exchange ,Molecular Biology ,miRNA ,C14MC ,Mid gestation ,Early gestation ,Infant, Newborn ,Gestational age ,Gene Expression Regulation, Developmental ,Human placenta ,Cell Biology ,medicine.disease ,C19MC ,MicroRNAs ,medicine.anatomical_structure ,embryonic structures ,Chorionic villi ,Gestation ,Biomarker (medicine) ,miR-17~92 ,Female ,pregnancy ,Research Article ,Research Paper - Abstract
BackgroundMicroRNAs (miRNAs) are increasingly seen as important regulators of placental development and opportunistic biomarker targets. Given the difficulty in obtaining samples from early gestation and subsequent paucity of the same, investigation of the role of miRNAs in early gestation human placenta has been limited. To address this, we generated miRNA profiles using 96 placentas from presumed normal pregnancies, across early gestation, in combination with matched profiles from maternal plasma. Placenta samples range from 6–23 weeks’ gestation, a time period that includes placenta from the early, relatively low but physiological (6–10 weeks’ gestation) oxygen environment, and later, physiologically normal oxygen environment (11–23 weeks’ gestation).ResultsWe identified 637 miRNAs with expression in 86 samples (after removing poor quality samples), showing a clear gestational age gradient from 6–23 weeks’ gestation. We identified 374 differentially expressed (DE) miRNAs between placentas from 6–10 weeks’ versus 11–23 weeks’ gestation. We see a clear gestational age group bias in miRNA clusters C19MC, C14MC, miR-17∼92 and paralogs, regions that also include many DE miRNAs. Proportional change in expression of placenta-specific miRNA clusters was reflected in maternal plasma.ConclusionThe presumed introduction of oxygenated maternal blood into the placenta (between ∼10–12 weeks’ gestation) changes the miRNA profile of the chorionic villus, particularly in placenta-specific miRNA clusters. Data presented here comprise a clinically important reference set for studying early placenta development and may underpin the generation of minimally invasive methods for monitoring placental health.
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- 2021
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20. High Folate, Perturbed One-Carbon Metabolism and Gestational Diabetes Mellitus
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Jessica M. Williamson, Anya L. Arthurs, Melanie D. Smith, Claire T. Roberts, and Tanja Jankovic-Karasoulos
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Nutrition and Dietetics ,Thymidylate Synthase ,5-Methyltetrahydrofolate-Homocysteine S-Methyltransferase ,Carbon ,Choline ,Betaine ,Diabetes, Gestational ,Vitamin B 12 ,Folic Acid ,Pregnancy ,Animals ,Humans ,Female ,Micronutrients ,Neural Tube Defects ,Homocysteine ,Methylenetetrahydrofolate Reductase (NADPH2) ,Food Science - Abstract
Folate is a dietary micronutrient essential to one-carbon metabolism. The World Health Organisation recommends folic acid (FA) supplementation pre-conception and in early pregnancy to reduce the risk of fetal neural tube defects (NTDs). Subsequently, many countries (~92) have mandatory FA fortification policies, as well as recommendations for periconceptional FA supplementation. Mandatory fortification initiatives have been largely successful in reducing the incidence of NTDs. However, humans have limited capacity to incorporate FA into the one-carbon metabolic pathway, resulting in the increasingly ubiquitous presence of circulating unmetabolised folic acid (uFA). Excess FA intake has emerged as a risk factor in gestational diabetes mellitus (GDM). Several other one-carbon metabolism components (vitamin B12, homocysteine and choline-derived betaine) are also closely entwined with GDM risk, suggesting a role for one-carbon metabolism in GDM pathogenesis. There is growing evidence from in vitro and animal studies suggesting a role for excess FA in dysregulation of one-carbon metabolism. Specifically, high levels of FA reduce methylenetetrahydrofolate reductase (MTHFR) activity, dysregulate the balance of thymidylate synthase (TS) and methionine synthase (MTR) activity, and elevate homocysteine. High homocysteine is associated with increased oxidative stress and trophoblast apoptosis and reduced human chorionic gonadotrophin (hCG) secretion and pancreatic β-cell function. While the relationship between high FA, perturbed one-carbon metabolism and GDM pathogenesis is not yet fully understood, here we summarise the current state of knowledge. Given rising rates of GDM, now estimated to be 14% globally, and widespread FA food fortification, further research is urgently needed to elucidate the mechanisms which underpin GDM pathogenesis.
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- 2022
21. The interaction between metabolic syndrome and physical activity, and risk for gestational diabetes mellitus
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Jessica A. Grieger, Gus Dekker, Ashleigh K Schneider, Claire T. Roberts, Ben W.J. Mol, Shalem Leemaqz, Petra E. Verburg, and J. Dalton
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medicine.medical_specialty ,Pregnancy ,business.industry ,Obstetrics ,Endocrinology, Diabetes and Metabolism ,030209 endocrinology & metabolism ,General Medicine ,030204 cardiovascular system & hematology ,medicine.disease ,Disease cluster ,Gestational diabetes ,03 medical and health sciences ,0302 clinical medicine ,Endocrinology ,Diabetes mellitus ,Epidemiology ,Internal Medicine ,Medicine ,Gestation ,Metabolic syndrome ,business ,Prospective cohort study - Abstract
Metabolic syndrome (MetS) is a cluster of risk factors which increases risk of cardiometabolic diseases in the adult population and increases risk for pregnancy complications such as gestational diabetes mellitus (GDM). Epidemiological data indicate that moderate-to-high levels of physical activity reduces the risk for GDM. The study aims to determine whether the association between MetS and GDM is affected by physical activity. We performed a prospective cohort study among 1373 pregnant nulliparous women in Adelaide, South Australia. At 9–16 weeks’ gestation, demographic, lifestyle and self-reported frequencies of physical activity were obtained, and a non-fasting blood sample was taken for assessment of MetS, defined using the International Diabetes Federation criteria. GDM was diagnosed at 24–28 weeks’ gestation using the World Health Organization classification. 1158 pregnant women were included: 107 (9%) women had MetS in early pregnancy, and 184 (16%) developed GDM. Having MetS increased the risk of developing GDM (37.4% vs. 13.7%, adjusted RR 2.5; 95% CI 1.7, 3.6). The interaction effect (RR; (95% CI) between MetS and physical activity was not significant (vigorous physical activity: 2.60; 0.46, 14.71) for ≥ 4 times per week; less vigorous activity; 0.77; 0.15, 4.02 for ≥ 4 times per week; stair climbing ≥ once day (1.16; 0.54, 2.51), all compared to no physical activity). Physical activity was not an effect modifier in the association between GDM and MetS. Information collected about the nature and extent of physical activity needs to be more detailed and granular to determine whether physical activity really has an effect.
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- 2021
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22. Elevated Maternal Folate Status and Changes in Maternal Prolactin, Placental Lactogen and Placental Growth Hormone Following Folic Acid Food Fortification: Evidence from Two Prospective Pregnancy Cohorts
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Tanja Jankovic-Karasoulos, Melanie D. Smith, Shalem Leemaqz, Jessica Williamson, Dylan McCullough, Anya L. Arthurs, Lauren A. Jones, Konstantinos Justin Bogias, Ben W. Mol, Julia Dalton, Gustaaf A. Dekker, and Claire T. Roberts
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folic acid ,prolactin ,human placental lactogen ,placental growth hormone ,pregnancy ,obesity ,gestational diabetes mellitus ,Nutrition and Dietetics ,Food Science - Abstract
Folic acid (FA) food fortification in Australia has resulted in a higher-than-expected intake of FA during pregnancy. High FA intake is associated with increased insulin resistance and gestational diabetes. We aimed to establish whether maternal one-carbon metabolism and hormones that regulate glucose homeostasis change in healthy pregnancies post-FA food fortification. Circulating folate, B12, homocysteine, prolactin (PRL), human placental lactogen (hPL) and placental growth hormone (GH2) were measured in early pregnancy maternal blood in women with uncomplicated pregnancies prior to (SCOPE: N = 604) and post (STOP: N = 711)-FA food fortification. FA food fortification resulted in 63% higher maternal folate. STOP women had lower hPL (33%) and GH2 (43%) after 10 weeks of gestation, but they had higher PRL (29%) and hPL (28%) after 16 weeks. FA supplementation during pregnancy increased maternal folate and reduced homocysteine but only in the SCOPE group, and it was associated with 54% higher PRL in SCOPE but 28% lower PRL in STOP. FA food fortification increased maternal folate status, but supplements no longer had an effect, thereby calling into question their utility. An altered secretion of hormones that regulate glucose homeostasis in pregnancy could place women post-fortification at an increased risk of insulin resistance and gestational diabetes, particularly for older women and those with obesity.
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- 2023
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23. A sexually dimorphic murine model of IUGR induced by embryo transfer
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Alison S. Care, Kathryn L. Gatford, Beverly S. Muhlhausler, Paul Q. Thomas, Sandra Piltz, Claire T. Roberts, Rebecca L. Wilson, and Harleen Kaur
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Male ,Litter (animal) ,Embryology ,Litter Size ,Placenta ,Intrauterine growth restriction ,Biology ,Andrology ,Mice ,Endocrinology ,Pregnancy ,medicine ,Animals ,reproductive and urinary physiology ,Fetus ,Fetal Growth Retardation ,Obstetrics and Gynecology ,Embryo ,Cell Biology ,Embryo Transfer ,medicine.disease ,Embryo transfer ,Sexual dimorphism ,Disease Models, Animal ,Fetal Weight ,Reproductive Medicine ,In utero ,embryonic structures ,Gestation ,Female - Abstract
Animal models are needed to develop interventions to prevent or treat intrauterine growth restriction (IUGR). Foetal growth rates and effects of in utero exposures differ between sexes, but little is known about sex-specific effects of increasing litter size. We established a murine IUGR model using pregnancies generated by multiple embryo transfers, and evaluated sex-specific responses to increasing litter size. CBAF1 embryos were collected at gestation day 0.5 (GD0.5) and 6, 8, 10 or 12 embryos were transferred into each uterine horn of pseudopregnant female CD1 mice (n = 32). Foetal and placental outcomes were measured at GD18.5. In the main experiment, foetuses were genotyped (Sry) for analysis of sex-specific outcomes. The number of implantation sites (P = 0.033) and litter size (number of foetuses, P = 0.008) correlated positively with the number of embryos transferred, while placental weight correlated negatively with litter size (both P < 0.01). The relationship between viable litter size and foetal weight differed between sexes (interaction P = 0.002), such that foetal weights of males (P = 0.002), but not females (P = 0.233), correlated negatively with litter size. Placental weight decreased with increasing litter size (P < 0.001) and was lower in females than males (P = 0.020). Our results suggest that male foetuses grow as fast as permitted by nutrient supply, whereas the female maintains placental reserve capacity. This strategy reflecting sex-specific gene expression is likely to place the male foetus at greater risk of death in the event of a ‘second hit’.
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- 2021
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24. Safety of maternal pertussis vaccination on pregnancy and birth outcomes: A prospective cohort study
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Gustaaf A. Dekker, Claire T. Roberts, Luke E. Grzeskowiak, Hassen Mohammed, Helen Marshall, Lynne C. Giles, and Petra E. Verburg
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Gestational hypertension ,medicine.medical_specialty ,Whooping Cough ,Diphtheria-Tetanus-acellular Pertussis Vaccines ,03 medical and health sciences ,0302 clinical medicine ,Pregnancy ,030225 pediatrics ,South Australia ,Humans ,Medicine ,Prospective Studies ,030212 general & internal medicine ,Prospective cohort study ,General Veterinary ,General Immunology and Microbiology ,business.industry ,Obstetrics ,Vaccination ,Infant, Newborn ,Public Health, Environmental and Occupational Health ,Infant ,medicine.disease ,Low birth weight ,Infectious Diseases ,Relative risk ,Premature Birth ,Molecular Medicine ,Gestation ,Small for gestational age ,Female ,medicine.symptom ,business - Abstract
Objective To evaluate the safety of maternal pertussis vaccination on pregnancy and birth outcomes. Methods The study population comprised 1272 healthy nulliparous pregnant women who participated in Screening Tests to identify poor Outcomes in Pregnancy (STOP) study at two obstetric hospitals in South Australia between 2015 and 2018. Participants were followed prospectively, with vaccination (confirmed by medical records), extensive amounts of pregnancy and birth outcome data collected by research midwives. Adjusted relative risks (aRRs) and hazard ratios (aHRs) were estimated accounting for time-varying vaccine exposure and the temporal nature of each outcome. Results Of the 1272 women included in this study, 80.1% (n = 1019) received maternal pertussis vaccination. Vaccinated women had an average 0.22 weeks (95% CI 0.001, 0.44) longer gestation at delivery compared to unvaccinated women. Maternal pertussis vaccination was not associated with chorioamnionitis (aRR 0.71, 95% CI 0.27,1.82), gestational hypertension (aHR 1.24, 95% CI, 0.66, 2.30), preeclampsia (aHR 0.75, 95% CI 0.47, 1.18) nor preterm birth (aHR 0.99, 95% CI 0.47, 2.07). Neither risk of low birth weight (aHR 0.72, 95% CI 0.41, 1.27) nor small for gestational age infants (aHR 0.67,95% CI 0.29, 1.55) were increased following maternal pertussis vaccination. No associations between pertussis vaccination during pregnancy and adverse birth outcomes including admission to the neonatal care unit, low Apgar scores, and mechanical ventilation were observed. Results were not materially changed after adjustment for maternal influenza vaccination. Conclusion Our study provides reassuring evidence of the safety of maternal pertussis vaccination with no increased risk of adverse pregnancy and birth outcomes. These findings support recommendations for pertussis vaccination during pregnancy to prevent morbidity and mortality associated with early-infant pertussis disease.
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- 2021
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25. Haemolysis detection in microRNA-seq from clinical plasma samples
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Melanie D. Smith, Shalem Y. Leemaqz, Tanja Jankovic-Karasoulos, Dale McAninch, Dylan McCullough, James Breen, Claire T. Roberts, Katherine A. Pillman, Smith, Melanie D, Leemaqz, Shalem Y, Jankovic-Karasoulos, Tanja, McAninch, Dale, McCullough, Dylan, Breen, James, Roberts, Claire T, and Pillman, Katherine A
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Male ,microRNA ,High-Throughput Nucleotide Sequencing ,bioinformatics ,prediction ,Hemolysis ,MicroRNAs ,plasma ,biomarker ,haemolysis ,Genetics ,Humans ,Female ,Circulating MicroRNA ,Biomarkers ,Genetics (clinical) - Abstract
The abundance of cell-free microRNA (miRNA) has been measured in many body fluids, including blood plasma, which has been proposed as a source with novel, minimally invasive biomarker potential for several diseases. Despite improvements in quantification methods for plasma miRNAs, there is no consensus on optimal reference miRNAs or to what extent haemolysis may affect plasma miRNA content. Here we propose a new method for the detection of haemolysis in miRNA high-throughput sequencing (HTS) data from libraries prepared using human plasma. To establish a miRNA haemolysis signature in plasma we first identified differentially expressed miRNAs between samples with known haemolysis status and selected miRNA with statistically significant higher abundance in our haemolysed group. Given there may be both technical and biological reasons for differential abundance of signature miRNA, and to ensure the method developed here was relevant outside of our specific context, that is women of reproductive age, we tested for significant differences between pregnant and non-pregnant groups. Here we report a novel 20 miRNA signature (miR-106b-3p, miR-140-3p, miR-142-5p, miR-532-5p, miR-17-5p, miR-19b-3p, miR-30c-5p, miR-324-5p, miR-192-5p, miR-660-5p, miR-186-5p, miR-425-5p, miR-25-3p, miR-363-3p, miR-183-5p, miR-451a, miR-182-5p, miR-191-5p, miR-194-5p, miR-20b-5p) that can be used to identify the presence of haemolysis, in silico, in high throughput miRNA sequencing data. Given the potential for haemolysis contamination, we recommend that assay for haemolysis detection become standard pre-analytical practice and provide here a simple method for haemolysis detection.
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- 2022
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26. DraculR: A web based application for in silico haemolysis detection in high throughput small RNA sequencing data
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Melanie D. Smith, Shalem Y. Leemaqz, Tanja Jankovic-Karasoulos, Dylan McCullough, Dale McAninch, James Breen, Claire T. Roberts, and Katherine A. Pillman
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MotivationThe search for novel microRNA (miRNA) biomarkers in plasma is hampered by haemolysis, the lysis and subsequent release of red blood cell (RBC) contents, including miRNAs, into surrounding fluid. The biomarker potential of miRNAs comes in part from their multi-compartment origin, and the long-lived nature of miRNA transcripts in plasma, giving researchers a functional window for tissues that are otherwise difficult or disadvantageous to sample. The inclusion of RBC derived miRNA transcripts in downstream analysis introduces a source of error that is difficult to identify post hoc and may lead to spurious results. Where access to a physical specimen is not possible, our tool will provide an in silico approach to haemolysis prediction.ResultsWe present DraculR, an interactive Shiny/R application that enables a user to upload microRNA expression data from short read sequencing of human plasma as a raw read counts table and interactively calculate a metric that indicates the degree of haemolysis contamination.Availability and implementationDraculR and its tutorial are freely available from (https://mxhp75.shinyapps.io/shinyVamp/). Code is available from (https://github.com/mxhp75/shinyVamp.git).
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- 2022
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27. Circular RNAs in Pregnancy and the Placenta
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Anya L. Arthurs, Tanja Jankovic-Karasoulos, Melanie D. Smith, and Claire T. Roberts
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Placenta ,Organic Chemistry ,General Medicine ,RNA, Circular ,Catalysis ,Computer Science Applications ,Inorganic Chemistry ,MicroRNAs ,Pregnancy ,Humans ,Female ,Physical and Theoretical Chemistry ,Molecular Biology ,Spectroscopy ,Signal Transduction - Abstract
The emerging field of circular RNAs (circRNAs) has identified their novel roles in the development and function of many cancers and inspired the interest of many researchers. circRNAs are also found throughout the healthy body, as well as in other pathological states, but while research into the function and abundance of circRNAs has progressed, our overall understanding of these molecules remains primitive. Importantly, recent studies are elucidating new roles for circRNAs in pregnancy, particularly in the placenta. Given that many of the genes responsible for circRNA production in cancer are also highly expressed in the placenta, it is likely that the same genes act in the production of circRNAs in the placenta. Furthermore, placental development can be referred to as ‘controlled cancer’, as it shares many key signalling pathways and hallmarks with tumour growth and metastasis. Hence, the roles of circRNAs in this field are important to study with respect to pregnancy success but also may provide novel insights for cancer progression. This review illuminates the known roles of circRNAs in pregnancy and the placenta, as well as demonstrating differential placental expressions of circRNAs between complicated and uncomplicated pregnancies.
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- 2022
28. Gestational diabetes mellitus and cardio-metabolic risk factors in women and children at 3 years postpartum
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Maleesa M. Pathirana, Prabha H. Andraweera, Emily Aldridge, Shalem Y. Leemaqz, Madeline Harrison, Jade Harrison, Petra E. Verburg, Margaret A. Arstall, Gustaaf A. Dekker, and Claire T. Roberts
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Blood Glucose ,Metabolic Syndrome ,Endocrinology, Diabetes and Metabolism ,Postpartum Period ,General Medicine ,Body Mass Index ,Diabetes, Gestational ,Endocrinology ,Pregnancy ,Risk Factors ,Child, Preschool ,Internal Medicine ,Humans ,Female ,Triglycerides - Abstract
IntroductionGestational diabetes mellitus (GDM) is thought to be associated with cardio-metabolic risk factor development in women and their children during the early postpartum period and early childhood. We hypothesized that these women and their children would exhibit increased abnormal cardio-metabolic risk factors three years after pregnancy.MethodsWomen from the Screening Tests to Predict Poor Outcomes of Pregnancy study were invited to attend a follow-up with the child from their index pregnancy at 3 years postpartum. Women and children were assessed for anthropometric measures and haemodynamic function. Fasting blood samples were obtained from women to assess lipid and glucose status.ResultsA total of 281 woman-child dyads participated in the 3-year follow-up, with 40 women developing GDM during their index pregnancy. Fasting serum insulin was higher in women with GDM in index pregnancy compared to those with an uncomplicated pregnancy. However, this association was mediated by early pregnancy BMI and socioeconomic index (SEI). The rate of metabolic syndrome was higher in the GDM group than the uncomplicated pregnancy group. Maternal GDM was associated with elevated maternal fasting serum triglycerides at 3 years after adjustment for early pregnancy BMI and SEI. Children exposed to GDM in utero had higher waist circumference compared to children born after an uncomplicated pregnancy, but this is mediated the above covariates.ConclusionExposure to GDM is associated with elevated serum triglycerides in women at 3 years postpartum but other cardiometabolic outcomes in women and children appear to be mediated by early pregnancy BMI and SEI.
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- 2022
29. Placental transcription profiling in 6-23 weeks’ gestation reveals differential transcript usage in early development
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Konstantinos J. Bogias, Stephen M. Pederson, Shalem Leemaqz, Melanie D. Smith, Dale McAninch, Tanja Jankovic-Karasoulos, Dylan McCullough, Qianhui Wan, Tina Bianco-Miotto, James Breen, and Claire T. Roberts
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Gene Expression Profiling ,Placenta ,Organic Chemistry ,Gestational Age ,General Medicine ,Placentation ,Catalysis ,Computer Science Applications ,Inorganic Chemistry ,Pregnancy ,Humans ,Female ,Chorionic Villi ,Physical and Theoretical Chemistry ,RNA-seq ,human ,placenta ,development ,transcriptome ,Molecular Biology ,Spectroscopy - Abstract
The human placenta is a rapidly developing transient organ that is key to pregnancy success. Early development of the conceptus occurs in a low oxygen environment before oxygenated maternal blood begins to flow into the placenta at ∼10-12 weeks’ gestation. This process is likely to substantially affect overall placental gene expression. Transcript variability underlying gene expression has yet to be profiled. In this study, accurate transcript expression profiles were identified for 84 human placental chorionic villus tissue samples collected across 6-23 weeks’ gestation. Differential gene expression (DGE), differential transcript expression (DTE) and differential transcript usage (DTU) between 6-10 weeks’ and 11-23 weeks’ gestation groups were assessed. In total, 229 genes had significant DTE yet no significant DGE. Integration of DGE and DTE analyses found that differential expression patterns of individual transcripts were commonly masked upon aggregation to the gene-level. Of the 611 genes that exhibited DTU, 534 had no significant DGE or DTE. The four most significant DTU genes ADAM10, VMP1, GPR126, and ASAH1, were associated with hypoxia-responsive pathways. Transcript usage is a likely regulatory mechanism in early placentation. Identification of functional roles will facilitate new insight in understanding the origins of pregnancy complications.
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- 2022
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30. Cardiovascular risk factors in women with previous gestational diabetes mellitus: A systematic review and meta-analysis
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Margaret Arstall, Maleesa M. Pathirana, Anna Ali, Claire T. Roberts, Prabha H. Andraweera, and Zohra S Lassi
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medicine.medical_specialty ,Glucose tolerance test ,medicine.diagnostic_test ,Cholesterol ,business.industry ,Endocrinology, Diabetes and Metabolism ,030209 endocrinology & metabolism ,medicine.disease ,Gestational diabetes ,03 medical and health sciences ,chemistry.chemical_compound ,0302 clinical medicine ,Endocrinology ,Blood pressure ,Insulin resistance ,chemistry ,Meta-analysis ,Internal medicine ,Diabetes mellitus ,Medicine ,Metabolic syndrome ,business - Abstract
This systematic review and meta-analysis aimed to synthesize evidence on conventional cardiovascular disease (CVD) risk factors among women with previous Gestational Diabetes Mellitus (GDM). The review protocol is registered with PROSPERO (CRD42019118149). PubMed, CINAHL, SCOPUS, and EMBASE databases were searched. Studies reporting on CVD risk factors in women with previous GDM compared to women without previous GDM were selected. A total of 139 studies were eligible, of which 93 were included in the meta-analysis. Women with previous GDM have significantly higher systolic blood pressure (2.47 mmHg 95% CI 1.74 to 3.40, n = 48, 50,118 participants) diastolic blood pressure (1.89 mmHg 95% CI 1.32 to 2.46, n = 48, 49,495 participants), BMI (1.54 kg/m2 95% CI 1.32 to 2.46, n = 78, 255,308 participants), total cholesterol (0.26 SMD 95% CI 0.15 to 0.37, n = 48, 38,561 participants), LDL cholesterol (0.19 SMD 95% CI 0.08 to 0.30, n = 44, 16,980 participants), triglycerides (0.56 SMD 95% CI 0.42 to 0.70, n = 46, 13,175 participants), glucose (0.69 SMD 95% CI 0.56 to 0.81, n = 55, 127,900 participants), insulin (0.41 SMD 95% CI 0.23 to 0.59, n = 32, 8881 participants) and significantly lower HDL cholesterol (-0.28 SMD 95% CI -0.39 to -0.16, n = 56, 35,882 participants), compared to women without previous GDM. The increased blood pressure, total cholesterol, triglycerides and glucose are seen as early as
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- 2020
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31. Hypertensive disorders of pregnancy and later cardiovascular disease risk in mothers and children
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Margaret Arstall, Gustaaf A. Dekker, Emily Aldridge, Amy J. Garrett, Melanie R. Wittwer, Claire T. Roberts, Michelle D. Plummer, Shalem Leemaqz, and Prabha H. Andraweera
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Adult ,Male ,Gestational hypertension ,medicine.medical_specialty ,Offspring ,Medicine (miscellaneous) ,Blood Pressure ,Disease ,030204 cardiovascular system & hematology ,Preeclampsia ,03 medical and health sciences ,0302 clinical medicine ,Pregnancy ,medicine ,Humans ,030212 general & internal medicine ,Child ,Sex Characteristics ,Obstetrics ,business.industry ,Hypertension, Pregnancy-Induced ,Middle Aged ,medicine.disease ,Pulse pressure ,Heart Disease Risk Factors ,In utero ,Prenatal Exposure Delayed Effects ,Cohort ,Female ,business ,Follow-Up Studies - Abstract
Preeclampsia (PE) and gestational hypertension (GH) are pregnancy-specific diseases that occur in around 10% of pregnancies worldwide. Increasing evidence suggests that women whose pregnancies were complicated by PE or GH, and their offspring, are at increased risk of cardiovascular disease (CVD) later in life. We hypothesised that PE and GH would associate with CVD risk factors 8–10 years after the first pregnancy in the mother and child and that differences in cardiovascular risk profile would be seen between 8- and 10-year-old male and female children. This is a follow-up study of the Adelaide SCOPE pregnancy cohort where 1164 nulliparous women and their babies were recruited between 2005 and 2008. Haemodynamic function was assessed using non-invasive USCOMBP+ and USCOM1A devices. Microvascular function was assessed by post-occlusive reactive hyperaemia. Of the 273 mother–child pairs followed up, 38 women had PE and 20 had GH during pregnancy. Augmentation index (Aix) and suprasystolic pulse pressure (ssPP) were increased, whereas measures of microvascular function were decreased in children who were born to PE compared to uncomplicated pregnancies. Female children had decreased Aix and ssPP compared to male children after in utero exposure to PE. Women who developed GH during their first pregnancy had increased systolic, diastolic and mean arterial pressures compared to women who had uncomplicated pregnancy. Our data suggest that GH is associated with increased cardiovascular risk in women 8–10 years after first pregnancy and PE is associated with increased offspring risk at 8–10 years of age, highlighting differences between these two hypertensive disorders of pregnancy.
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- 2020
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32. Maternal diet and offspring telomere length: a systematic review
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Claire T. Roberts, Yan Yin Phoi, Tina Bianco-Miotto, Nahal Habibi, Jessica A. Grieger, Tanja Jankovic-Karasoulos, Habibi, Nahal, Bianco-Miotto, Tina, Phoi, Yan Yin, Jankovic-Karasoulos, Tanja, Roberts, Claire T, and Grieger, Jessica A
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Adult ,Offspring ,Nutritional Status ,Medicine (miscellaneous) ,Physiology ,vitamin D ,Context (language use) ,folate ,Eating ,Young Adult ,Folic Acid ,Pregnancy ,Caffeine ,Fatty Acids, Omega-3 ,telomere length ,medicine ,Vitamin D and neurology ,Humans ,maternal diet ,Child ,Prospective cohort study ,Calcifediol ,chemistry.chemical_classification ,Nutrition and Dietetics ,offspring ,maternal nutritional status ,business.industry ,Telomere Homeostasis ,Maternal Nutritional Physiological Phenomena ,Vitamins ,Telomere ,Fetal Blood ,medicine.disease ,Diet ,chemistry ,Child, Preschool ,Cord blood ,Leukocytes, Mononuclear ,cord blood ,Biomarker (medicine) ,Female ,pregnancy ,business ,Polyunsaturated fatty acid - Abstract
ContextMany studies assert a negative influence of inappropriate maternal diet and nutritional status during pregnancy on offspring, not only in utero but throughout life, because of the role in the programing of noncommunicable diseases. Telomere length is a biomarker of aging, and shorter telomeres are associated with chronic disease later in life. Maternal nutrition and nutritional status may be an important determinant of offspring telomere length.ObjectiveA systematic review was conducted to determine the effect of maternal nutrition and nutritional status in pregnancy on offspring telomere length.Data SourcesThis systematic review was conducted according to PRISMA guidelines. Database searches of PubMed, CINAHL, Scopus, Medline, and Web of Science were performed.Study SelectionIncluded studies assessed the association between maternal nutrition (dietary intake and nutritional status) during pregnancy and offspring telomere length measured in cord blood, serum, plasma, and peripheral blood mononuclear cells.Data ExtractionThree authors screened and determined the quality of the articles; disagreements were resolved by a fourth author. All authors compared the compiled data.ResultsSeven studies were extracted and evaluated. Studies comprised a double-blind placebo-controlled trial (n = 1), prospective cohort studies (n = 5), and a cross-sectional study (n = 1). Higher circulating maternal folate and 25-hydroxyvitamin D3 concentrations, along with higher maternal dietary caffeine intakes, were associated with longer offspring telomere length, whereas higher dietary intake of carbohydrate, folate, n-3 polyunsaturated fatty acids, vitamin C, or sodium was not.ConclusionThe limited but suggestive evidence highlights the need for further research to be conducted in this area, particularly longitudinal studies involving larger cohorts of pregnant women.Systematic review registrationPROSPERO registration no. CRD42019136506
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- 2020
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33. Association between metabolic syndrome and gestational diabetes mellitus in women and their children: a systematic review and meta-analysis
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Margaret Arstall, Maleesa M. Pathirana, Claire T. Roberts, Anna Ali, Prabha H. Andraweera, and Zohra S Lassi
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Pregnancy ,medicine.medical_specialty ,endocrine system diseases ,business.industry ,Offspring ,Obstetrics ,Endocrinology, Diabetes and Metabolism ,nutritional and metabolic diseases ,030209 endocrinology & metabolism ,Subgroup analysis ,medicine.disease ,female genital diseases and pregnancy complications ,Childhood obesity ,Gestational diabetes ,03 medical and health sciences ,0302 clinical medicine ,Endocrinology ,030220 oncology & carcinogenesis ,Meta-analysis ,Diabetes mellitus ,medicine ,Metabolic syndrome ,business - Abstract
The primary aim of this systematic review and meta-analysis was to determine the association between gestational diabetes mellitus (GDM) and metabolic syndrome (MetS) in women and children. Our secondary aim was to assess the development of MetS with respect to the elapsed time postpartum at which MetS was diagnosed. This review is registered with PROSPERO (CRD42020173319). PubMed, CINHAL, SCOPUS, and EMBASE databases were searched. Studies reporting on the rate of MetS in pregnant women with GDM, the rate of MetS in women with a history of GDM, and the rate of MetS in offspring exposed to GDM in utero compared to healthy controls were selected. We identified 588 articles from the literature search. Fifty-one studies were included in the review and of those 35 were included in the meta-analysis. Quantitative summary measures showed that women with a history of GDM had an increased risk of developing MetS compared to those without a history of GDM (RR 2.36, 95% CI 1.77–3.14, 29 studies, 13,390 participants; heterogeneity: χ2 p
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- 2020
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34. The metabolic syndrome in pregnancy and its association with child telomere length
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Claire T. Roberts, Dale McAninch, Prabha H. Andraweera, Tina Bianco-Miotto, Gus Dekker, Michelle D. Plummer, Amy J. Garrett, K.L. Gatford, Lisa G. Smithers, Shalem Leemaqz, and Jessica A. Grieger
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Adult ,Male ,0301 basic medicine ,medicine.medical_specialty ,Endocrinology, Diabetes and Metabolism ,030209 endocrinology & metabolism ,Body Mass Index ,Cohort Studies ,Young Adult ,03 medical and health sciences ,0302 clinical medicine ,Pregnancy ,Internal Medicine ,Humans ,Medicine ,Prospective Studies ,Child ,Prospective cohort study ,Telomere Shortening ,Metabolic Syndrome ,business.industry ,Obstetrics ,Australia ,Telomere ,Anthropometry ,medicine.disease ,Obesity ,United Kingdom ,Pregnancy Complications ,030104 developmental biology ,Prenatal Exposure Delayed Effects ,Cohort ,Biomarker (medicine) ,Gestation ,Female ,Metabolic syndrome ,business ,Ireland ,New Zealand - Abstract
The aim of this study was to determine whether presence of the metabolic syndrome in pregnancy associates with child telomere length or child anthropometry (weight, BMI) and BP, measured at 10 years of age. The Screening for Pregnancy Endpoints study (SCOPE) was a multicentre, international prospective cohort of nulliparous pregnant women recruited from Australia, New Zealand, Ireland and the UK (N = 5628). The current analysis is a 10 year follow-up of SCOPE pregnant women and their children, from the Australian cohort. Clinical data collected at 14–16 weeks’ gestation during the SCOPE study were used to diagnose the metabolic syndrome using IDF criteria. Telomere length, a biomarker of ageing, was assessed by quantitative PCR from children’s saliva collected at 10 years of age. In women who completed follow-up (n = 255), 20% had the metabolic syndrome in pregnancy. After adjusting for a range of confounders, children of mothers who had the metabolic syndrome in pregnancy had 14% shorter telomeres than children of mothers without the metabolic syndrome in pregnancy (mean difference −0.36 [95% CI −0.74, 0.01]). Height- and weight-for-age, and BMI z scores were similar in children of mothers who did and did not have the metabolic syndrome during pregnancy. Children of mothers who had the metabolic syndrome in pregnancy have shorter telomeres, a biomarker of accelerated ageing. These findings warrant further studies in larger cohorts of children, as well as investigations into whether telomere length measured in cord blood associates with telomere length in childhood.
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- 2020
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35. Animal Models of Preeclampsia
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Claire T. Roberts, Kathryn L. Gatford, Prabha H. Andraweera, and Alison S. Care
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0301 basic medicine ,medicine.medical_specialty ,Psychological intervention ,030204 cardiovascular system & hematology ,Preeclampsia ,03 medical and health sciences ,0302 clinical medicine ,Pre-Eclampsia ,Pregnancy ,Internal Medicine ,medicine ,Animals ,Maternal hypertension ,Intensive care medicine ,reproductive and urinary physiology ,Fetus ,Aspirin ,Proteinuria ,business.industry ,Organ dysfunction ,medicine.disease ,female genital diseases and pregnancy complications ,Disease Models, Animal ,030104 developmental biology ,embryonic structures ,Female ,medicine.symptom ,business ,medicine.drug - Abstract
Preeclampsia is a common pregnancy complication, affecting 2% to 8% of pregnancies worldwide, and is an important cause of both maternal and fetal morbidity and mortality. Importantly, although aspirin and calcium are able to prevent preeclampsia in some women, there is no cure apart from delivery of the placenta and fetus, often necessitating iatrogenic preterm birth. Preclinical models of preeclampsia are widely used to investigate the causes and consequences of preeclampsia and to evaluate safety and efficacy of potential preventative and therapeutic interventions. In this review, we provide a summary of the published preclinical models of preeclampsia that meet human diagnostic criteria, including the development of maternal hypertension, together with new-onset proteinuria, maternal organ dysfunction, and uteroplacental dysfunction. We then discuss evidence from preclinical models for multiple causal factors of preeclampsia, including those implicated in early-onset and late-onset preeclampsia. Next, we discuss the impact of exposure to a preeclampsia-like environment for later maternal and progeny health. The presence of long-term impairment, particularly cardiovascular outcomes, in mothers and progeny after an experimentally induced preeclampsia-like pregnancy, implies that later onset or reduced severity of preeclampsia will improve later maternal and progeny health. Finally, we summarize published intervention studies in preclinical models and identify gaps in knowledge that we consider should be targets for future research.
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- 2020
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36. Pregnancy, but not dietary octanoic acid supplementation, stimulates the ghrelin-pituitary growth hormone axis in mice
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Georgia S Clarke, Lili Huang, Amanda J. Page, Kathryn L. Gatford, Beverly S. Muhlhausler, Pamela S-l Sim, Claire T. Roberts, Johannes D. Veldhuis, Hui Li, Rebecca L. Wilson, Chen Chen, Maria Nunez-Salces, and Harleen Kaur
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medicine.medical_specialty ,Acylation ,Placenta ,Endocrinology, Diabetes and Metabolism ,Mice ,Endocrinology ,Pregnancy ,Internal medicine ,medicine ,Animals ,RNA, Messenger ,Receptor ,Chemistry ,Stomach ,digestive, oral, and skin physiology ,Trophoblast ,medicine.disease ,Ghrelin ,Growth hormone secretion ,Mice, Inbred C57BL ,medicine.anatomical_structure ,Gastric Mucosa ,Growth Hormone ,Dietary Supplements ,Female ,Secretagogue ,Caprylates - Abstract
Circulating growth hormone (GH) concentrations increase during pregnancy in mice and remain pituitary-derived. Whether abundance or activation of the GH secretagogue ghrelin increase during pregnancy, or in response to dietary octanoic acid supplementation, is unclear. We therefore measured circulating GH profiles in late pregnant C57BL/6J mice and in aged-matched non-pregnant females fed with standard laboratory chow supplemented with 5% octanoic or palmitic (control) acid (n = 4–13/group). Serum total and acyl-ghrelin concentrations, stomach and placenta ghrelin mRNA and protein expression, Pcsk1 (encoding prohormone convertase 1/3) and Mboat4 (membrane bound O-acyl transferase 4) mRNA were determined at zeitgeber (ZT) 13 and ZT23. Total and basal GH secretion were higher in late pregnant than non-pregnant mice (P P = 0.004), but not acyl-ghrelin, and the density of ghrelin-positive cells in the gastric antrum (P = 0.019) were higher, and gastric Mboat4 and Pcsk1 mRNA expression were lower in pregnant than non-pregnant mice at ZT23. In the placenta, ghrelin protein was localised mostly to labyrinthine trophoblast cells. Serum acyl-, but not total, ghrelin was lower at mid-pregnancy than in non-pregnant mice, but not different at early or late pregnancy. In conclusion, dietary supplementation with 5% octanoic acid did not increase activation of ghrelin in female mice. Our results further suggest that increases in maternal GH secretion throughout murine pregnancy are not due to circulating acyl-ghrelin acting at the pituitary. Nevertheless, time-dependent increased circulating total ghrelin could potentially increase ghrelin action in tissues that express the acylating enzyme and receptor.
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- 2020
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37. Psychosocial determinants of pertussis and influenza vaccine uptake in pregnant women: A prospective study
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Claire T. Roberts, J. Dalton, Hassen Mohammed, Helen Marshall, Shalem Leemaqz, Lynne C. Giles, Luke E. Grzeskowiak, and Gustaaf A. Dekker
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medicine.medical_specialty ,Whooping Cough ,Influenza vaccine ,030231 tropical medicine ,03 medical and health sciences ,0302 clinical medicine ,Pregnancy ,Internal medicine ,Influenza, Human ,South Australia ,medicine ,Humans ,Prospective Studies ,030212 general & internal medicine ,Pregnancy Complications, Infectious ,Immunization during pregnancy ,Prospective cohort study ,Pertussis Vaccine ,Depressive Disorder, Major ,General Veterinary ,General Immunology and Microbiology ,business.industry ,Vaccination ,Public Health, Environmental and Occupational Health ,medicine.disease ,Cross-Sectional Studies ,Infectious Diseases ,Influenza Vaccines ,Molecular Medicine ,Gestation ,Pertussis vaccine ,Female ,Pregnant Women ,business ,Psychosocial ,medicine.drug - Abstract
Objective To identify the psychosocial factors influencing women’s uptake and willingness to receive pertussis and influenza vaccine during pregnancy. Methods The study population comprised 1364 healthy nulliparous pregnant women who participated in a prospective cohort study at two obstetric hospitals in South Australia between 2015 and 2017. Information on women's vaccination status, sociodemographic, lifestyle and psychological state were collected at 9–16 weeks’ gestation and medical case notes were checked post-delivery to verify the reported vaccination status. Poisson regression models were used to estimate the crude and adjusted prevalence ratios (aPRs) to identify psychosocial factors influencing uptake of vaccination during pregnancy. Results Willingness to receive the recommended maternal vaccines was high (90%). Overall, 79% and 48% received maternal pertussis and influenza vaccines respectively. There was no evidence to support the influence of psychosocial factors on women’s willingness to receive immunization during pregnancy. High levels of anxiety (aPR 0.98, 95% CI: 0.87–1.09) was not associated with uptake of maternal pertussis vaccine. However, elevated depressive symptoms (aPR 1.14, 95% CI: 1.00–1.30) and very high-perceived stress during pregnancy were significantly associated with receipt of pertussis vaccination (aPR 0.87; 95% CI 0.76–0.99). Women with mild depressive symptoms (aPR 1.21, 95% CI 1.00–1.44) and mild anxiety symptoms (aPR 1.21, 95% CI: 0.99–1.48) were more likely to receive influenza vaccine during pregnancy (aPR 1.27, 95% CI: 1.08–1.49). A history of major depressive disorder was independently associated with receipt of pertussis (aPR 1.16, 95% CI 1.06–1.26) and influenza vaccination during pregnancy (aPR 1.32; 95% CI 1.14–1.58). Conclusion Regardless of psychosocial factors, most women reported a positive willingness to receive the recommended vaccinations during pregnancy. However, psychosocial factors influenced the uptake of pertussis and influenza vaccines during pregnancy. Psychosocial factors should be taken into consideration in designing interventions and implementation of maternal pertussis and influenza immunization programs.
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- 2020
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38. Mechanisms linking exposure to preeclampsia in utero and the risk for cardiovascular disease
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Alison S. Care, Kathryn L. Gatford, Claire T. Roberts, Prabha H. Andraweera, Gus Dekker, Margaret Arstall, Zohra S Lassi, and Tina Bianco-Miotto
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0301 basic medicine ,medicine.medical_specialty ,Pregnancy ,Obstetrics ,business.industry ,Mechanism (biology) ,Offspring ,Medicine (miscellaneous) ,Disease ,030204 cardiovascular system & hematology ,medicine.disease ,Preeclampsia ,03 medical and health sciences ,030104 developmental biology ,0302 clinical medicine ,Blood pressure ,medicine ,Risk factor ,business ,Body mass index - 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.
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- 2020
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39. Reduced Dietary Calcium and Vitamin D Results in Preterm Birth and Altered Placental Morphogenesis in Mice During Pregnancy
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Rebecca L. Wilson, Claire T. Roberts, Dale McAninch, Zona Goh, Tina Bianco-Miotto, Paul H. Anderson, Jessica A. Phillips, Wilson, Rebecca L, Phillips, Jessica A, Bianco-Miotto, Tina, McAninch, Dale, Goh, Zona, Anderson, Paul H, and Roberts, Claire T
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0301 basic medicine ,medicine.medical_specialty ,placenta ,Placenta ,chemistry.chemical_element ,vitamin D ,Calcium ,vitamin D deficiency ,Fetal Development ,Mice ,03 medical and health sciences ,0302 clinical medicine ,Pregnancy ,Internal medicine ,medicine ,Vitamin D and neurology ,Animals ,Vitamin D ,mouse ,calcium ,030219 obstetrics & reproductive medicine ,business.industry ,Pregnancy Outcome ,Obstetrics and Gynecology ,Gestational age ,Vitamin D Deficiency ,medicine.disease ,Micronutrient ,Calcium, Dietary ,Pregnancy Complications ,Disease Models, Animal ,Pregnancy rate ,030104 developmental biology ,Endocrinology ,chemistry ,Premature Birth ,Gestation ,Female ,pregnancy ,business - Abstract
Vitamin D and calcium are essential micronutrients for reproductive success. Vitamin D deficiency during pregnancy is associated with increased risk of pregnancy complications including pre-eclampsia and preterm birth (PTB). However, inconsistencies in the literature reflect uncertainties regarding the true biological importance of vitamin D but may be explained by maternal calcium intakes. We aimed to determine whether low dietary consumption of calcium along with vitamin D deficiency had an additive effect on adverse pregnancy outcome by investigating placental morphogenesis and foetal growth in a mouse model.Female mice were randomly assigned to one of four diets: control-fed (+Ca+VD), reduced vitamin D only (+Ca−VD), reduced calcium only (−Ca+VD) and reduced calcium and vitamin D (−Ca−VD), and sacrificed at gestational day (GD) 18.5. Maternal serum 25-hydroxy vitamin D (25(OH)D3) levels were lower in each reduced diet group when compared with levels in +Ca+VD fed mice. While the pregnancy rate did not differ between groups, in the −Ca−VD-fed group, 55% (5 out of 9 pregnant of known gestational age) gave birth preterm (
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- 2020
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40. Women's awareness of cardiovascular disease risk after complications of pregnancy
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Emily Aldridge, Maleesa Pathirana, Melanie Wittwer, Susan Sierp, Claire T. Roberts, Gustaaf A. Dekker, and Margaret Arstall
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Maternity and Midwifery ,Obstetrics and Gynecology - Abstract
Certain maternal complications of pregnancy, including hypertensive disorders of pregnancy, gestational diabetes mellitus, birth of a growth restricted infant, idiopathic preterm labour, and placental abruption, are associated with a significantly increased risk of future maternal cardiovascular disease. In Australia, it is relatively unknown how many women with a history of complicated pregnancies are aware of their future cardiovascular disease risk.The aim of this study was to determine what percentage of women attending a cardiovascular disease prevention clinic in South Australia soon after a complicated pregnancy were aware of their increased risk of cardiovascular disease.This prospective observational study included 188 women attending a postpartum prevention clinic between 7th August 2018 and 10th February 2021. These women had experienced a serious maternal complication of pregnancy approximately seven months earlier. Women completed a self-administered health awareness survey immediately prior to their first clinic appointment to assess their awareness of their increased cardiovascular risk.Over two-thirds (69.1 %) of the women were unaware of the association between pregnancy complications and cardiovascular disease, and 6.4 % of the cohort did not realise they had experienced a complicated pregnancy. Almost 10 % of the cohort did not correctly identify the complication/s they had been diagnosed with during pregnancy.Awareness of the association between complications of pregnancy and future cardiovascular disease was low in our cohort of women who had experienced a complication of pregnancy only seven months earlier. This emphasises the need for improved education for and communication with women to assist in implementing preventative care strategies.
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- 2022
41. Effects of race and ethnicity on perinatal outcomes in high-income and upper-middle-income countries: an individual participant data meta-analysis of 2 198 655 pregnancies
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Jameela Sheikh, John Allotey, Tania Kew, Borja M Fernández-Félix, Javier Zamora, Asma Khalil, Shakila Thangaratinam, Mali Abdollahain, Ary I. Savitri, Kjell Åsmund Salvesen, Sohinee Bhattacharya, Cuno S.P.M. Uiterwaal, Annetine C. Staff, Louise Bjoerkholt Andersen, Elisa Llurba Olive, George Daskalakis, Maureen Macleod, Baskaran Thilaganathan, Javier Arenas Ramírez, Jacques Massé, Francois Audibert, Per Minor Magnus, Line Sletner, Ahmet Baschat, Akihide Ohkuchi, Fionnuala M. McAuliffe, Jane West, Lisa M. Askie, Fionnuala Mone, Diane Farrar, Peter A. Zimmerman, Luc J.M. Smits, Catherine Riddell, John C. Kingdom, Joris van de Post, Sebastián E. Illanes, Claudia Holzman, Sander M.J. van Kuijk, Lionel Carbillon, Pia M. Villa, Anne Eskild, Lucy Chappell, Federico Prefumo, Luxmi Velauthar, Paul Seed, Miriam van Oostwaard, Stefan Verlohren, Lucilla Poston, Enrico Ferrazzi, Christina A. Vinter, Chie Nagata, Mark, Brown, Karlijn C. Vollebregt, Satoru Takeda, Josje Langenveld, Mariana Widmer, Shigeru Saito, Camilla Haavaldsen, Guillermo Carroli, Jørn Olsen, Hans Wolf, Nelly Zavaleta, Inge Eisensee, Patrizia Vergani, Pisake Lumbiganon, Maria Makrides, Fabio Facchinetti, Evan Sequeira, Robert Gibson, Sergio Ferrazzani, Tiziana Frusca, Ernesto A. Figueiró-Filho, Olav Lapaire, Hannele Laivuori, Jacob A. Lykke, Agustin Conde-Agudelo, Alberto Galindo, Alfred Mbah, Ana Pilar Betran, Ignacio Herraiz, Lill Trogstad, Gordon G.S. Smith, Eric A.P. Steegers, Read Salim, Tianhua Huang, Annemarijne Adank, Jun Zhang, Wendy S. Meschino, Joyce L. Browne, Rebecca E. Allen, Fabricio Da Silva Costa, Kerstin Klipstein-Grobusch, Jan Stener Jørgensen, Jean-Claude Forest, Alice R. Rumbold, Ben W. Mol, Yves Giguère, Wessel Ganzevoort, Anthony O. Odibo, Jenny Myers, SeonAe Yeo, Helena J. Teede, Francois Goffinet, Lesley McCowan, Eva Pajkrt, Bassam G. Haddad, Gustaaf Dekker, Emily C. Kleinrouweler, Édouard LeCarpentier, Claire T. Roberts, Henk Groen, Ragnhild Bergene Skråstad, Seppo Heinonen, Kajantie Eero, Louise C. Kenny, Dewi Anggraini, Athena Souka, Jose Cecatti, Ilza Monterio, Arri Coomarasamy, Melanie Smuk, Athanasios Pillalis, Francesca Crovetto, Renato Souza, Lee Ann Hawkins, Rinat Gabbay- Benziv, Richard Riley, Kym Snell, Lucinda Archer, Francesc Figuera, Marleen van Gelder, Graduate School, Obstetrics and Gynaecology, APH - Quality of Care, ARD - Amsterdam Reproduction and Development, APH - Personalized Medicine, and APH - Digital Health
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General Medicine - Abstract
Background: Existing evidence on the effects of race and ethnicity on pregnancy outcomes is restricted to individual studies done within specific countries and health systems. We aimed to assess the impact of race and ethnicity on perinatal outcomes in high-income and upper-middle-income countries, and to ascertain whether the magnitude of disparities, if any, varied across geographical regions. Methods: For this individual participant data (IPD) meta-analysis we used data from the International Prediction of Pregnancy Complications (IPPIC) Network of studies on pregnancy complications; the full dataset comprised 94 studies, 53 countries, and 4 539 640 pregnancies. We included studies that reported perinatal outcomes (neonatal death, stillbirth, preterm birth, and small-for-gestational-age babies) in at least two racial or ethnic groups (White, Black, south Asian, Hispanic, or other). For our two-step random-effects IPD meta-analysis, we did multiple imputations for confounder variables (maternal age, BMI, parity, and level of maternal education) selected with a directed acyclic graph. The primary outcomes were neonatal mortality and stillbirth. Secondary outcomes were preterm birth and a small-for-gestational-age baby. We estimated the association of race and ethnicity with perinatal outcomes using a multivariate logistic regression model and reported this association with odds ratios (ORs) and 95% CIs. We also did a subgroup analysis of studies by geographical region. Findings: 51 studies from 20 high-income and upper-middle-income countries, comprising 2 198 655 pregnancies, were eligible for inclusion in this IPD meta-analysis. Neonatal death was twice as likely in babies born to Black women than in babies born to White women (OR 2·00, 95% CI 1·44–2·78), as was stillbirth (2·16, 1·46–3·19), and babies born to Black women were at increased risk of preterm birth (1·65, 1·46–1·88) and being small for gestational age (1·39, 1·13–1·72). Babies of women categorised as Hispanic had a three-times increased risk of neonatal death (OR 3·34, 95% CI 2·77–4·02) than did those born to White women, and those born to south Asian women were at increased risk of preterm birth (OR 1·26, 95% CI 1·07–1·48) and being small for gestational age (1·61, 1·32–1·95). The effects of race and ethnicity on preterm birth and small-for-gestational-age babies did not vary across regions. Interpretation: Globally, among underserved groups, babies born to Black women had consistently poorer perinatal outcomes than White women after adjusting for maternal characteristics, although the risks varied for other groups. The effects of race and ethnicity on adverse perinatal outcomes did not vary by region. Funding: National Institute for Health and Care Research, Wellbeing of Women.
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- 2022
42. DraculR: A Web-Based Application for In Silico Haemolysis Detection in High-Throughput microRNA Sequencing Data
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Melanie D. Smith, Shalem Y. Leemaqz, Tanja Jankovic-Karasoulos, Dylan McCullough, Dale McAninch, Anya L. Arthurs, James Breen, Claire T. Roberts, Katherine A. Pillman, Smith, Melanie D, Leemaqz, Shalem Y, Jankovic-Karasoulos, Tanja, McCullough, Dylan, McAninch, Dale, Arthurs, Anya L, Breen, James, Roberts, Claire T, and Pillman, Katherine A
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microRNA ,Genetics ,biomarker ,haemolysis ,prediction ,bioinformatics ,plasma ,Genetics (clinical) - Abstract
Refereed/Peer-reviewed The search for novel microRNA (miRNA) biomarkers in plasma is hampered by haemolysis, the lysis and subsequent release of red blood cell contents, including miRNAs, into surrounding fluid. The biomarker potential of miRNAs comes in part from their multicompartment origin and the long-lived nature of miRNA transcripts in plasma, giving researchers a functional window for tissues that are otherwise difficult or disadvantageous to sample. The inclusion of red-blood-cell-derived miRNA transcripts in downstream analysis introduces a source of error that is difficult to identify posthoc and may lead to spurious results. Where access to a physical specimen is not possible, our tool will provide an in silico approach to haemolysis prediction. We present DraculR, an interactive Shiny/R application that enables a user to upload miRNA expression data from a short-read sequencing of human plasma as a raw read counts table and interactively calculate a metric that indicates the degree of haemolysis contamination. The code, DraculR web tool and its tutorial are freely available as detailed herein.
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- 2023
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43. Early pregnancy cardio metabolic risk factors and the prevalence of metabolic syndrome 10 years after the first pregnancy
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Prabha H. Andraweera, Michelle D. Plummer, Amy Garrett, Shalem Leemaqz, Melanie R. Wittwer, Emily Aldridge, Maleesa M. Pathirana, Gus A. Dekker, Claire T. Roberts, and Margaret A. Arstall
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Multidisciplinary - Abstract
Background We aimed to compare risk factors for CVD 10 years postpartum among women who had ≥ 1 compared to no cardio metabolic risk factor in early first pregnancy. Methods Women of the SCOPE (Screening fOr Pregnancy Endpoints) study from Adelaide, South Australia were invited to participate in a cardiovascular risk assessment 10 years after the delivery of the first child. Data from 141 women who completed all the assessments are included in the analyses. Result Compared to women who did not have any cardio metabolic risk factor at 15 ± 1 weeks’ gestation during the first pregnancy, those who had ≥ 1 risk factor were 5.5 times more likely to have metabolic syndrome 10 years postpartum (aOR = 5.5, 95% CI 1.8–17.3, p = 0.004). Women who had ≥ 1cardio metabolic risk factor during the first pregnancy were more likely to be obese (p = 0.001), have high total cholesterol levels (p Conclusion Cardio metabolic risk factors at the booking visit in the first pregnancy may be useful in identifying young women at risk of future CVD.
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- 2023
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44. Do raised two-hour pre-pregnancy insulin levels confer the same risks of developing GDM, as raised fasting levels, in recurrent miscarriage patients?
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Claire T. Roberts, Shalem Leemaqz, Gustaaf A. Dekker, Catherine McCormack, and Denise Furness
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Adult ,Abortion, Habitual ,medicine.medical_specialty ,medicine.medical_treatment ,Miscarriage ,03 medical and health sciences ,0302 clinical medicine ,Insulin resistance ,Pregnancy ,Risk Factors ,Hyperinsulinism ,Recurrent miscarriage ,Humans ,Insulin ,Medicine ,Prospective Studies ,Oral glucose tolerance ,030219 obstetrics & reproductive medicine ,business.industry ,Obstetrics ,Pre pregnancy ,Obstetrics and Gynecology ,Fasting ,Glucose Tolerance Test ,medicine.disease ,Diabetes, Gestational ,030220 oncology & carcinogenesis ,Female ,Insulin Resistance ,business - Abstract
This study questioned whether raised pre-pregnancy two-hour (2 h) insulin levels, measured in recurrent embryonic miscarriage (RM) patients via a 75 g Oral Glucose Tolerance Test (OGTT), are associated with an increased risk of gestational diabetes mellitus (GDM) in a subsequent pregnancy. Patients had a 75 g OGTT and insulin levels evaluated (
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- 2019
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45. Placental Inflammasome mRNA Levels Differ by Mode of Delivery and Fetal Sex
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Anya L. Arthurs, Melanie D. Smith, Mhyles D. Hintural, James Breen, Dylan McCullough, Francesca I. Thornton, Shalem Y. Leemaqz, Gustaaf A. Dekker, Tanja Jankovic-Karasoulos, and Claire T. Roberts
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Male ,Cesarean Section ,Inflammasomes ,Pregnancy ,Placenta ,Immunology ,Infant, Newborn ,Parturition ,Immunology and Allergy ,Humans ,Infant ,Female ,RNA, Messenger - Abstract
Parturition signals the end of immune tolerance in pregnancy. Term labour is usually a sterile inflammatory process triggered by damage associated molecular patterns (DAMPs) as a consequence of functional progesterone withdrawal. Activation of DAMPs recruits leukocytes and inflammatory cytokine responses in the myometrium, decidua, cervix and fetal membranes. Emerging evidence shows components of the inflammasome are detectable in both maternal decidua and placenta. However, the activation of the placental inflammasome with respect to mode of delivery has not been profiled. Placental chorionic villus samples from women delivering at termviaunassisted vaginal (UV) birth, labouring lower segment caesarean section (LLSCS, emergency caesarean section) and prelabour lower segment caesarean section (PLSCS, elective caesarean section) underwent high throughput RNA sequencing (NextSeq Illumina) and bioinformatic analyses to identify differentially expressed inflammatory (DE) genes. DE genes (IL1RL1,STAT1,STAT2,IL2RB,IL17RE,IL18BP,TNFAIP2,TNFSF10andTNFRSF8), as well as common inflammasome genes (IL1B,IL1R1,IL1R2,IL6,IL18,IL18R1,IL18R1,IL10, andIL33), were targets for further qPCR analyses and Western blotting to quantify protein expression. There was no specific sensor molecule-activated inflammasome which dominated expression when stratified by mode of delivery, implying that multiple inflammasomes may function synergistically during parturition. Whilst placentae from women who had UV births overall expressed pro-inflammatory mediators, placentae from LLSCS births demonstrated a much greater pro-inflammatory response, with additional interplay of pro- and anti-inflammatory mediators. As expected, inflammasome activation was very low in placentae from women who had PLSCS births. Sex-specific differences were also detected. Placentae from male-bearing pregnancies displayed higher inflammasome activation in LLSCS compared with PLSCS, and placentae from female-bearing pregnancies displayed higher inflammasome activation in LLSCS compared with UV. In conclusion, placental inflammasome activation differs with respect to mode of delivery and neonatal sex. Its assessment may identify babies who have been exposed to aberrant inflammation at birth that may compromise their development and long-term health and wellbeing.
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- 2021
46. Protective Influence of Breastfeeding on Cardiovascular Risk Factors in Women With Previous Gestational Diabetes Mellitus and Their Children: A Systematic Review and Meta-Analysis
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Prabha H. Andraweera, Anna Ali, Margaret Arstall, Maleesa M. Pathirana, Zohra S Lassi, and Claire T. Roberts
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medicine.medical_specialty ,business.industry ,Obstetrics ,Cardiovascular risk factors ,Breastfeeding ,Obstetrics and Gynecology ,medicine.disease ,Gestational diabetes ,Diabetes, Gestational ,Breast Feeding ,Diabetes Mellitus, Type 2 ,Cardiovascular Diseases ,Heart Disease Risk Factors ,Pregnancy ,Risk Factors ,Meta-analysis ,Medicine ,Humans ,Maternal health ,Female ,business ,Child - Abstract
Background: There is evidence that breastfeeding may provide protection against cardiovascular risk factors in mothers with a history of gestational diabetes mellitus and their children who were exposed in utero. Research Aim: To perform a systematic review and meta-analysis of observational studies to ascertain the effects of breastfeeding on cardiovascular risk factors in women with previous gestational diabetes mellitus and their children exposed in utero. Methods: Studies assessing conventional cardiovascular risk factors in women with previous gestational diabetes mellitus and children exposed in utero stratified by breastfeeding/no breastfeeding or breastfed/not breastfed were included. Gestational diabetes mellitus was defined based on the International Association of Diabetes in Pregnancy Study Group definition or previous accepted definitions. Breastfeeding was defined as reported in each study. Results: The literature search yielded 260 titles, of which 17 studies were selected to be in the review. Women with previous gestational diabetes mellitus who did not breastfeed had higher blood glucose ( SMD: 0.32, 95% CI [0.12, 0.53]) and a greater risk of developing Type 2 diabetes mellitus ( RR: 2.08 95% CI [1.44, 3.00]) compared to women with no history. There were not enough studies to conduct a meta-analysis on the effects of breastfeeding on risk factors for cardiovascular disease among children exposed to gestational diabetes mellitus in utero. Conclusion: Breastfeeding appears to be protective against cardiovascular risk factors among women who experience gestational diabetes mellitus.
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- 2021
47. Effectiveness of birthing kits for clean childbirth: a systematic review
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Prabha H. Andraweera, Zohra S Lassi, Alexandra Cummins, Zeshi Fisher, and Claire T. Roberts
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medicine.medical_specialty ,Health (social science) ,clean birth kits ,Review ,childbirth ,CINAHL ,Cochrane Library ,03 medical and health sciences ,0302 clinical medicine ,Pregnancy ,Sepsis ,birth kits ,medicine ,Humans ,Infection control ,Childbirth ,030212 general & internal medicine ,Randomized Controlled Trials as Topic ,030219 obstetrics & reproductive medicine ,business.industry ,Infant, Newborn ,Parturition ,Public Health, Environmental and Occupational Health ,General Medicine ,Delivery, Obstetric ,medicine.disease ,infection ,Infant mortality ,Neonatal tetanus ,Family medicine ,Female ,business ,Qualitative research - Abstract
Poor infection control practices during childbirth are recognised as a critical factor leading to life-threatening maternal and newborn sepsis. Therefore, this paper assesses the effectiveness of clean birth kits (CBKs) to ensure a safe birthing environment. We searched PubMed, Cochrane Library and CINAHL, as well as Google Scholar, to identify both qualitative and quantitative studies on CBKs published in English up to November 2018. Studies were included if the pregnant women or women giving birth intended to use or used a CBK. The methodological quality of included papers was assessed. A total of 37 studies, 26 quantitative and 11 qualitative studies, were included. Quantitative studies showed a positive impact of CBKs on reducing the incidence of puerperal sepsis and neonatal tetanus. The review also identified CBK use to be associated with a reduction in perinatal, neonatal and young infant mortality. Qualitative studies suggested that a lack of awareness of the importance of CBKs and clean delivery practices, unavailability of CBKs and financial constraints to purchase CBKs were the potential barriers. CBKs appear to be a promising strategy to reduce maternal and neonatal morbidity and mortality. However, the current evidence is limited and further large-scale trials are required.
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- 2019
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48. Low Serum Levels of HtrA3 at 15 Weeks of Gestation Are Associated with Late-Onset Preeclampsia Development and Small for Gestational Age Birth
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Claire T. Roberts, Shalem Leemaqz, Yao Wang, Guiying Nie, Sonia Soo Yee Teoh, Gus Dekker, and Ying Li
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Adult ,Gestational hypertension ,Embryology ,medicine.medical_specialty ,Down-Regulation ,Blood Pressure ,Gestational Age ,Logistic regression ,Risk Assessment ,Ultrasonography, Prenatal ,Umbilical Arteries ,Preeclampsia ,Young Adult ,03 medical and health sciences ,0302 clinical medicine ,Pre-Eclampsia ,Predictive Value of Tests ,Pregnancy ,Risk Factors ,Placenta ,medicine ,Birth Weight ,Humans ,Pregnancy-Associated Plasma Protein-A ,Radiology, Nuclear Medicine and imaging ,030212 general & internal medicine ,030219 obstetrics & reproductive medicine ,Obstetrics ,business.industry ,Serine Endopeptidases ,Infant, Newborn ,Obstetrics and Gynecology ,Ultrasonography, Doppler ,High-Temperature Requirement A Serine Peptidase 1 ,General Medicine ,medicine.disease ,Uterine Artery ,medicine.anatomical_structure ,Case-Control Studies ,Pregnancy Trimester, Second ,Infant, Small for Gestational Age ,Pediatrics, Perinatology and Child Health ,Nested case-control study ,Cohort ,Gestation ,Small for gestational age ,Female ,business ,Biomarkers - Abstract
Objective: The aim of this study was to investigate the potential utility of serum HtrA1 and HtrA3, serine proteases that are highly expressed in the developing placenta, at 15 and 20 weeks of gestation for predicting later development of adverse pregnancy outcomes of preeclampsia (PE), gestational hypertension (GHT), preterm birth (PTB), and small for gestational age (SGA) birth. Methods: This is a nested case control study of 665 samples (330 controls, 335 cases) from the Adelaide SCOPE cohort. The cases included were 92 PE, 71 GHT, 56 PTB, and 116 SGA. Samples were assessed by ELISA and data adjusted for maternal age, BMI, socioeconomic index, hCG, and smoking status. Multivariate logistic regression was performed with other biochemical and biophysical parameters available for these samples. Results: HtrA1 did not differ between the controls and cases. In contrast, HtrA3 was significantly lower at 15 weeks in pregnancies that later developed late-onset PE (LPE) or resulted in SGA birth, with an area under the ROC curve (AUC) of 0.716 and 0.790, respectively. The combination of HtrA3 with PAPP-A, uterine, and umbilical Doppler improved the AUC to 0.755 for LPE and 0.844 for SGA. Conclusion: HtrA3 at 15 weeks is associated with, and may be useful for, the early detection of LPE development and SGA birth.
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- 2019
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49. Pregnancy complications and cardiovascular disease risk perception: A qualitative study
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Prabha H. Andraweera, Zohra S. Lassi, Maleesa M. Pathirana, Michelle D. Plummer, Gus A. Dekker, Claire T. Roberts, and Margaret A. Arstall
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Pregnancy Complications ,Multidisciplinary ,Cardiovascular Diseases ,Pregnancy ,Postpartum Period ,Humans ,Female ,Perception ,Qualitative Research - Abstract
Objectives We aimed to assess women’s perceptions on the long-term risks for cardiovascular disease (CVD) after major pregnancy complications. Methods Women who experienced major pregnancy complications and those who experienced uncomplicated pregnancies were invited to participate in a qualitative study. Focus group discussions (FGDs) and self-administered questionnaires were used to explore: The knowledge of long-term sequelae after experiencing a major pregnancy complication; Importance of education on heart health; The practicality of referral to a clinic after pregnancy complications; Willingness for regular postpartum clinic visits after pregnancy complications. A thematic qualitative analysis was undertaken. Results 26 women participated in four FGDs. The majority of women did not know of the association between major pregnancy complications and CVD. The main views expressed were: Women who experience pregnancy complications should receive education on improving heart health; An appointment for the first CVD risk screening visit needs to be made prior to discharge from the delivery suite; Women will benefit by having the option to select between a hospital and a general-practitioner based model of follow up. Conclusions These views are important in developing postpartum strategies to reduce CVD risk among women who experience pregnancy complications.
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- 2022
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50. Young-Onset Gastrointestinal Adenocarcinoma Incidence and Survival Trends in the Northern Territory, Australia, with Emphasis on Indigenous Peoples
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Mia Shepherdson, Shalem Leemaqz, Gurmeet Singh, Courtney Ryder, Shahid Ullah, Karla Canuto, Joanne P. Young, Timothy J. Price, Ross A. McKinnon, Stephen J. Pandol, Claire T. Roberts, and Savio George Barreto
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Cancer Research ,Oncology ,outcomes ,morbidity ,mortality ,stomach ,pancreas ,colon ,Indigenous - Abstract
Background and Aims: A concerning rise in incidence of young-onset cancers globally led to the examination of trends in incidence and survival of gastrointestinal (GI) adenocarcinomas in the Northern Territory (NT), Australia, over a 28-year period, with a special emphasis on Indigenous peoples. Methods: This cross-sectional analysis of a prospective longitudinal database, NT Cancer Registry (1990–2017), includes all reported cases of GI (oesophagus, gastric, small intestinal, pancreas, colon, and rectum) adenocarcinomas. Poisson regression was used to estimate incidence ratio ratios, and survival was modelled using Cox proportional hazard models separately for people aged 18–50 years and >50 years. Results: A total of 1608 cases of GI adenocarcinoma were recorded during the time of the study. While the overall incidence in people 18–50 years remained unchanged over this time (p = 0.51), the rate in individuals aged >50 years decreased (IRR = 0.65 (95% CI 0.56–0.75; p < 0.0001)). Incidence rates were significantly less in females >50 years (IRR = 0.67 95% CI 0.59–0.75; p < 0.0001), and their survival was significantly better (HR = 0.84 (95%CI 0.72–0.98; p < 0.03)) compared to males. Overall survival across all GI subsites improved in both age cohorts, especially between 2010 and 2017 (HR = 0.45 (95%CI 0.29–0.72; p < 0.0007) and HR = 0.64 (95%CI 0.52–0.78; p < 0.0001), respectively) compared to 1990–1999, driven by an improvement in survival in colonic adenocarcinoma alone, as the survival remained unchanged in other GI subsites. The incidence was significantly lower in Indigenous patients compared to non-Indigenous patients, in both age cohorts (18–50 years IRR = 0.68 95% CI 0.51–0.91; p < 0.009 and >50 years IRR = 0.48 95% CI 0.40–0.57; p < 0.0001). However, Indigenous patients had worse survival rates (18–50 years HR = 2.06 95% CI 1.36–3.11; p < 0.0007 and >50 years HR = 1.66 95% CI 1.32–2.08; p < 0.0001). Conclusions: There is a trend towards an increased incidence of young-onset GI adenocarcinomas in the NT. Young Indigenous patients have lower incidence but worse survival across all GI subsites, highlighting significant health inequities in life expectancy. Targeted, culturally safe Indigenous community-focussed programs are needed for early detection and patient-centred management of GI adenocarcinomas.
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- 2022
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