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3. International variations in the gestational age distribution of births: An ecological study in 34 high-income countries

Author

Delnord, M., Mortensen, L., Hindori-Mohangoo, A.D., Blondel, B., Gissler, M., Kramer, M.R., Richards, J.L., Deb-Rinker, P., Rouleau, J., Morisaki, N., Nassar, N., Bolumar, F., Berrut, S., Nybo Andersen, A.M., Kramer, M.S., and Zeitlin, J.

Subjects
Life, Health, CH - Child Health, ELSS - Earth, Life and Social Sciences
Abstract

Background: Few studies have investigated international variations in the gestational age (GA) distribution of births. While preterm births (22-36 weeks GA) and early term births (37-38 weeks) are at greater risk of adverse health outcomes compared to full term births (39-40 weeks), it is not known if countries with high preterm birth rates also have high early term birth rates. We examined rate associations between preterm and early term births and mean term GA by mode of delivery onset. Methods: We used routine aggregate data on the GA distribution of singleton live births from up to 34 high-income countries/regions in 1996, 2000, 2004, 2008 and 2010 to study preterm and early term births overall and by spontaneous or indicated onset. Pearson correlation coefficients were adjusted for clustering in time trend analyses. Results: Preterm and early term births ranged from 4.1% to 8.2% (median 5.5%) and 15.6% to 30.8% (median 22.2%) of live births in 2010, respectively. Countries with higher preterm birth rates in 2004-2010 had higher early term birth rates (r > 0.50, P < 0.01) and changes over time were strongly correlated overall (adjusted-r=0.55, P < 0.01) and by mode of onset. Conclusion: Positive associations between preterm and early term birth rates suggest that common risk factors could underpin shifts in the GA distribution. Targeting modifiable population risk factors for delivery before 39 weeks GA may provide a useful preterm birth prevention paradigm. © 2018 The Author(s) 2018. Published by Oxford University Press on behalf of the European Public Health Association. All rights reserved.

Published
2018

4. Temporal Trends in Late Preterm and Early Term Birth Rates in 6 High-income Countries in North America and Europe and Association With Clinician-initiated Obstetric Interventions

Author

Richards, J.L., primary, Kramer, M.S., additional, Deb-Rinker, P., additional, Rouleau, J., additional, Mortensen, L., additional, Gissler, M., additional, Morken, N.H., additional, Skjærven, R., additional, Cnattingius, S., additional, Johansson, S., additional, Delnord, M., additional, Dolan, S.M., additional, Morisaki, N., additional, Tough, S., additional, Zeitlin, J., additional, and Kramer, M.R., additional

Published
2017
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5. Annotation of Human Chromosome 7 for Disease Research

Author

Scherer, S.W., Cheung, J., Nakabayashi, K., Vincent, J., Petek, E., Herbrick, J.A., Li, M., Skaug, J., Kolozsvari, D., Deb-Rinker, P., Carson, A., Hudek, A., Paterson, A., Osborne, L., Rommens, J., Boright, A., and Tsui, L.C.

Subjects
Human genetics -- Research, DNA -- Research, Chromosome mapping -- Methods, Biological sciences
Published
2001

7. Epigenetic modifications of SOX2 enhancers, SRR1 and SRR2, correlate with in vitro neural differentiation

Author

Sikorska, Marianna, Sandhu, J., Deb-Rinker, P., Jezierski, A., Leblanc, J., Charlebois, C., Ribecco-Lutkiewicz, Maria, Bani-Yaghoub, M., and Walker, P.

Subjects
glycoprotein, receptors, peptide, Canada, brain, receptor, molecular sequence data, membrane glycoproteins, cells, cultured, HMGB proteins, stem cells, transcription factors, DNA-binding proteins, Epigenesis, genetic, expression, genetics, molecular, gene, membrane, receptors, cytoplasmic and nuclear, comparative study, acetylation, mechanisms, DNA methylation, astrocytes, in vitro, DNA, cell, sequence, base sequence, enhancer elements, genetic, neuron, peptide, cell differentiation, neurogenesis, nuclear, calcium-binding proteins, soxb1 transcription factors, physiology, cytology, role, methylation, biosynthesis, protein, metabolism
Abstract

SOX2 is a key neurodevelopmental gene involved in maintaining the pluripotency of stem cells and proliferation of neural progenitors and astroglia. Two evolutionally conserved enhancers, SRR1 and SRR2, are involved in controlling SOX2 expression during neurodevelopment; however, the molecular mechanisms regulating their activity are not known. We have examined DNA methylation and histone H3 acetylation at both enhancers in NT2-D1 progenitors, neurons and astrocytes, to establish the role of epigenetic mechanisms in cell-type-specific SOX2 expression. This study showed that 1) unmethylated DNA and acetylated histones at both enhancers correlated with a high level of SOX2 expression in proliferating neural progenitors and 2) reversible modifications of the SRR1 element were observed during gene reexpression in astrocytes, whereas permanent epigenetic marks on the SRR2 enhancer were seen in neurons where the gene was silenced. Taken together, these results are clear illustrations of cell-type-specific epigenomes and suggest mechanisms by which they may be created and maintained

Published
2008

9. Variations in very preterm birth rates in 30 high-income countries: are valid international comparisons possible using routine data?

Author

Delnord, M, Hindori‐Mohangoo, AD, Smith, LK, Szamotulska, K, Richards, JL, Deb‐Rinker, P, Rouleau, J, Velebil, P, Zile, I, Sakkeus, L, Gissler, M, Morisaki, N, Dolan, SM, Kramer, MR, Kramer, MS, Zeitlin, J, Haidinger, Gerald, Alexander, Sophie, Pavlou, Pavlos, and Mortensen, Laust

Subjects
PREMATURE labor, DURATION of pregnancy, PREMATURE infants, LABOR complications (Obstetrics), OBSTETRICAL emergencies, BIRTH rate, COMPARATIVE studies, GESTATIONAL age, RESEARCH methodology, EVALUATION of medical care, MEDICAL cooperation, PREGNANCY, RESEARCH, DEVELOPED countries, EVALUATION research
Abstract

Objective: Concerns about differences in registration practices across countries have limited the use of routine data for international very preterm birth (VPT) rate comparisons.Design: Population-based study.Setting: Twenty-seven European countries, the United States, Canada and Japan in 2010.Population: A total of 9 376 252 singleton births.Method: We requested aggregated gestational age data on live births, stillbirths and terminations of pregnancy (TOP) before 32 weeks of gestation, and information on registration practices for these births. We compared VPT rates and assessed the impact of births at 22-23 weeks of gestation, and different criteria for inclusion of stillbirths and TOP on country rates and rankings.Main Outcome Measures: Singleton very preterm birth rate, defined as singleton stillbirths and live births before 32 completed weeks of gestation per 1000 total births, excluding TOP if identifiable in the data source.Results: Rates varied from 5.7 to 15.7 per 1000 total births and 4.0 to 11.9 per 1000 live births. Country registration practices were related to percentage of births at 22-23 weeks of gestation (between 1% and 23% of very preterm births) and stillbirths (between 6% and 40% of very preterm births). After excluding births at 22-23 weeks, rate variations remained high and with a few exceptions, country rankings were unchanged.Conclusions: International comparisons of very preterm birth rates using routine data should exclude births at 22-23 weeks of gestation and terminations of pregnancy. The persistent large rate variations after these exclusions warrant continued surveillance of VPT rates at 24 weeks and over in high-income countries.Tweetable Abstract: International comparisons of VPT rates should exclude births at 22-23 weeks of gestation and terminations of pregnancy. [ABSTRACT FROM AUTHOR]

Published
2017
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14. Pre-conception Folic Acid and Multivitamin Supplementation for the Primary and Secondary Prevention of Neural Tube Defects and Other Folic Acid-Sensitive Congenital Anomalies

Author

Wilson, R. Douglas, Wilson, R. Douglas, Audibert, François, Brock, Jo-Ann, Carroll, June, Cartier, Lola, Gagnon, Alain, Johnson, Jo-Ann, Langlois, Sylvie, Murphy-Kaulbeck, Lynn, Okun, Nanette, Pastuck, Melanie, Deb-Rinker, Paromita, Dodds, Linda, Leon, Juan Andres, Lowell, Hélène, Luo, Wei, MacFarlane, Amanda, McMillan, Rachel, Moore, Aideen, Mundle, William, O’Connor, Deborah, Ray, Joel, and Van den Hof, Michiel

Abstract

To provide updated information on the pre- and post-conception use of oral folic acid with or without a multivitamin/micronutrient supplement for the prevention of neural tube defects and other congenital anomalies This will help physicians, midwives, nurses, and other health care workers to assist in the education of women about the proper use and dosage of folic acid/multivitamin supplementation before and during pregnancy.

Published
2015
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15. Temporal Trends in Late Preterm and Early Term Birth Rates in 6 High-Income Countries in North America and Europe and Association With Clinician-Initiated Obstetric Interventions

Author

Richards, Jennifer L., Kramer, Michael S., Deb-Rinker, Paromita, Rouleau, Jocelyn, Mortensen, Laust, Gissler, Mika, Morken, Nils-Halvdan, Skjærven, Rolv, Cnattingius, Sven, Johansson, Stefan, Delnord, Marie, Dolan, Siobhan M., Morisaki, Naho, Tough, Suzanne, Zeitlin, Jennifer, and Kramer, Michael R.

Abstract

(Abstracted from JAMA2016;316(4):410–419)Late-preterm and early-term births occurring spontaneously or through obstetric interventions including labor induction or cesarean delivery are a cause for concern because of consequent risks of adverse neonatal and childhood outcomes. Hence, recommendations in the United States have been to decrease nonmedically indicated or elective deliveries before 39 weeks.

Published
2016
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16. Supplémentation préconceptionnelle en acide folique / multivitamines pour la prévention primaire et secondaire des anomalies du tube neural et d’autres anomalies congénitales sensibles à l’acide folique

Author

Wilson, R. Douglas, Wilson, R. Douglas, Audibert, François, Brock, Jo-Ann, Carroll, June, Cartier, Lola, Gagnon, Alain, Johnson, Jo-Ann, Langlois, Sylvie, Murphy-Kaulbeck, Lynn, Okun, Nanette, Pastuck, Melanie, Deb-Rinker, Paromita, Dodds, Linda, Leon, Juan Andres, Lowell, Hélène, Luo, Wei, MacFarlane, Amanda, McMillan, Rachel, Moore, Aideen, Mundle, William, O’Connor, Deborah, Ray, Joel, and Van den Hof, Michiel

Abstract

Offrir des renseignements à jour sur l’utilisation pré et postconceptionnelle d’acide folique par voie orale, avec ou sans supplément de multivitamines / micronutriments, aux fins de la prévention des anomalies du tube neural et d’autres anomalies congénitales. Ces renseignements aideront les médecins, les sages-femmes, les infirmières et les autres professionnels de la santé à contribuer aux efforts de sensibilisation des femmes quant à l’utilisation et aux posologies adéquates de la supplémentation en acide folique / multivitamines, avant et pendant la grossesse.

Published
2015
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17. Molecular Characterization of a MSRV-like Sequence Identified by RDA from Monozygotic Twin Pairs Discordant for Schizophrenia

Author

Deb-Rinker, Paromita, Klempan, Timothy A., O'Reilly, Richard L., Torrey, E.Fuller, and Singh, Shiva M.

Abstract

Retroviral-related amplicons were used in modified RDA to identify four sequences from affected members of three pairs of monozygotic twins discordant for schizophrenia. One sequence (schizophrenia associated retrovirus, SZRV-1, GenBank Accession No. AF135487) is characterized here. It is similar to two known sequences of retroviral origin: multiple sclerosis-associated retrovirus, MSRV (GenBank Accession No. AF009668), and ERV-9 (GenBank Accession No. S77575). It is present in multiple copies in the human genome and has been localized to six different chromosomal sites. A zooblot shows that this multicopy sequence is predominant in the primate lineage and present in rhesus monkeys and humans. SZRV-1 is expressed as a 9-kb RNA band in the placenta. This could offer support to the hypothesis that retroviral sequences transposing during fetal growth may alter neurodevelopmental genes and cause diseases, although its direct involvement in the causation of schizophrenia remains to be established.

Published
1999
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18. Severe Maternal Morbidity in Canada: Temporal Trends and Regional Variations, 2003-2016

Author

Dzakpasu, Susie, Deb-Rinker, Paromita, Arbour, Laura, Darling, Elizabeth K., Kramer, Michael S., Liu, Shiliang, Luo, Wei, Murphy, Phil A., Nelson, Chantal, Ray, Joel G., Scott, Heather, VandenHof, Michiel, and Joseph, K.S.

Abstract

This study sought to quantify temporal trends and provincial and territorial variations in severe maternal morbidity (SMM) in Canada.

Published
2019
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20. Risk of latent and active tuberculosis infection in travellers: a systematic review and meta-analysis.

Author

Diefenbach-Elstob TR, Alabdulkarim B, Deb-Rinker P, Pernica JM, Schwarzer G, Menzies D, Shrier I, Schwartzman K, and Greenaway C

Subjects
Health Personnel, Humans, Incidence, Prevalence, Risk Factors, Travel, Latent Tuberculosis epidemiology, Tuberculosis epidemiology
Abstract

Introduction: Achieving tuberculosis (TB) elimination in low TB incidence countries requires identification and treatment of individuals at risk for latent TB infection (LTBI). Persons travelling to high TB incidence countries are potentially at risk for TB exposure. This systematic review and meta-analysis estimates incident LTBI and active TB among individuals travelling from low to higher TB incidence countries., Methods: Five electronic databases were searched from inception to 18 February 2020. We identified incident LTBI and active TB among individuals travelling from low (<10 cases/100 000 population) to intermediate (10-100/100 000) or high (>100/100 000) TB incidence countries. We conducted a meta-analysis and meta-regression using a random effects model of log-transformed proportions (cumulative incidence). Subgroup analyses investigated the impact of travel duration, travel purpose and TB incidence in the destination country., Results: Our search identified 799 studies, 120 underwent full-text review, and 10 studies were included. These studies included 1 154 673 travellers observed between 1994 and 2013, comprising 443 health care workers (HCW), 1 068 636 military personnel and 85 594 general travellers/volunteers. We did not identify any studies that estimated incidence of LTBI or active TB among people travelling to visit friends and relatives (VFRs). The overall cumulative incidence of LTBI was 2.3%, with considerable heterogeneity. Among individuals travelling for a mean/median of up to 6 months, HCWs had the highest cumulative incidence of LTBI (4.3%), whereas the risk was lower for military (2.5%) and general travellers/volunteers (1.6%). Meta-regression did not identify a difference in incident LTBI based on travel duration and TB incidence in the destination country. Five studies reported cases of active TB, with an overall pooled estimate of 120.7 cases per 100 000 travellers., Conclusions: We found that travelling HCWs were at highest risk of developing LTBI. Individual risk activities and travel purpose were most associated with risk of TB infection acquired during travel., (© International Society of Travel Medicine 2020. All rights reserved. For Permissions, please e-mail: journals.permissions@oup.com.)

Published
2021
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21. Severe maternal morbidity surveillance: Monitoring pregnant women at high risk for prolonged hospitalisation and death.

Author

Dzakpasu S, Deb-Rinker P, Arbour L, Darling EK, Kramer MS, Liu S, Luo W, Murphy PA, Nelson C, Ray JG, Scott H, VandenHof M, and Joseph KS

Subjects
Adult, Canada epidemiology, Cause of Death, Epidemiological Monitoring, Female, Humans, Mortality, Outcome Assessment, Health Care methods, Outcome Assessment, Health Care standards, Pregnancy, Risk Factors, Severity of Illness Index, Length of Stay statistics & numerical data, Maternal Mortality, Obstetric Labor Complications classification, Obstetric Labor Complications mortality, Pregnancy Complications classification, Pregnancy Complications epidemiology, Pregnancy, High-Risk, Public Health Surveillance methods
Abstract

Background: There is no international consensus on the definition and components of severe maternal morbidity (SMM)., Objectives: To propose a comprehensive definition of SMM, to create an empirically justified list of SMM types and subtypes, and to use this to examine SMM in Canada., Methods: Severe maternal morbidity was defined as a set of heterogeneous maternal conditions known to be associated with severe illness and with prolonged hospitalisation or high case fatality. Candidate SMM types/subtypes were evaluated using information on all hospital deliveries in Canada (excluding Quebec), 2006-2015. SMM rates for 2012-2016 were quantified as a composite and as SMM types/subtypes. Rate ratios and population attributable fractions (PAF) associated with overall and specific SMM types/subtypes were estimated in relation to length of hospital stay (LOS > 7 days) and case fatality., Results: There were 22 799 cases of SMM subtypes (among 1 418 545 deliveries) that were associated with a prolonged LOS or high case fatality. Between 2012 and 2016, the composite SMM rate was 16.1 (95% confidence interval [CI] 15.9, 16.3) per 1000 deliveries. Severe pre-eclampsia and HELLP syndrome (514.6 per 100 000 deliveries), and severe postpartum haemorrhage (433.2 per 100 000 deliveries) were the most common SMM types, while case fatality rates among SMM subtypes were highest among women who had cardiac arrest and resuscitation (241.1 per 1000), hepatic failure (147.1 per 1000), dialysis (67.6 per 1000), and cerebrovascular accident/stroke (51.0 per 1000). The PAF for prolonged hospital stay related to SMM was 17.8% (95% CI 17.3, 18.3), while the PAF for maternal death associated with SMM was 88.0% (95% CI 74.6, 94.4)., Conclusions: The proposed definition of SMM and associated list of SMM subtypes could be used for standardised SMM surveillance, with rate ratios and PAFs associated with specific SMM types/subtypes serving to inform clinical practice and public health policy., (© 2019 The Authors. Paediatric and Perinatal Epidemiology Published by John Wiley & Sons Ltd.)

Published
2020
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22. Prevalence of Severe Maternal Morbidity and Factors Associated With Maternal Mortality in Ontario, Canada.

Author

Ray JG, Park AL, Dzakpasu S, Dayan N, Deb-Rinker P, Luo W, and Joseph KS

Subjects
Adolescent, Adult, Cross-Sectional Studies, Female, Humans, Maternal Mortality, Middle Aged, Morbidity, Ontario epidemiology, Pregnancy, Prevalence, Risk Factors, Young Adult, Pregnancy Complications epidemiology, Pregnancy Complications mortality, Pregnancy Outcome epidemiology
Abstract

Importance: Severe maternal morbidity is defined by potentially life-threatening conditions. The association between the number of severe maternal morbidity (SMM) indicators and maternal death is not known., Objective: To quantify the association between the number of SMM indicators and maternal mortality., Design, Setting, and Participants: This population-based cohort study used provincial databases for data on all live birth and stillbirth hospital deliveries among women in Ontario, Canada, from April 1, 2002, to February 18, 2017. Excluded from this cohort were those with invalid identification number, non-Ontario residency, maternal age younger than 10 years or older than 55 years or unknown, or gestational age fewer than 20 weeks or unknown as well as any out-of-hospital births, ectopic pregnancies, or spontaneous or induced abortions., Exposures: Number of SMM indicators identified between 20 weeks' gestation and 42 days after the index delivery., Main Outcomes and Measures: Maternal death occurring from delivery to 42 days after the index delivery., Results: Of the 1 953 943 total births among 1 211 396 women, 181 maternal deaths occurred within 42 days after birth, a rate of 9.3 per 100 000 births. Of the 181 women who died, 123 (68.0%) had at least 1 SMM indicator compared with 1.7% (33 152) of women who survived. Standardized differences suggested that women who died, compared with the women who lived, were older (mean [SD] age, 31.0 [6.2] years vs 30.1 [5.5] years; standardized difference, 0.15) and more likely to reside in a lower-income area (99 [54.7%] vs 832 231 [42.6%]; standardized difference, 0.24), be nulliparous (93 [51.4%] vs 880 386 [45.1%]; standardized difference, 0.13), and be of Afro-Caribbean origin (12 [6.6%] vs 64 948 [3.3%]; standardized difference, 0.15). The most frequent SMM indicators were intensive care unit admission (81 [44.8%]), invasive ventilation (77 [42.5%]), cardiac conditions (69 [38.1%]), complications of obstetric surgery or procedures (32 [17.7%]), and postpartum hemorrhage with blood transfusion (31 [17.1%]). The rate of maternal mortality increased exponentially with the number of SMM indicators: 0 indicators (3.0 per 100 000 births), 1 (71.7 per 100 000 births), 2 (385.9 per 100 000 births), 3 (1274.2 per 100 000 births), 4 (2236.8 per 100 000 births), 5 (4285.7 per 100 000 births), and 6 or more (9422.5 per 100 000 births). Adjusted relative risks for maternal death ranged from 20.1 (95% CI, 11.6-34.7) with 1 SMM indicator to 2192.0 (95% CI, 1287.0-3735.0) with 6 or more SMM indicators compared with 0 indicators., Conclusions and Relevance: Maternal death may be associated with the number of SMM indicators and occur in certain identifiable groups of women; targeting preventable SMM indicators or limiting their progression may reduce the number of maternal deaths.

Published
2018
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23. At-a-glance - How Healthy are Canadians? A brief update.

Author

Branchard B, Deb-Rinker P, Dubois A, Lapointe P, O'Donnell S, Pelletier L, and Williams G

Subjects
Anxiety Disorders epidemiology, Canada epidemiology, Cardiovascular Diseases mortality, Chronic Disease trends, Diabetes Mellitus mortality, Health Status Indicators, Humans, Mood Disorders epidemiology, Neoplasms mortality, Respiratory Tract Diseases mortality, Cardiovascular Diseases epidemiology, Diabetes Mellitus epidemiology, Health Risk Behaviors, Health Status, Neoplasms epidemiology, Respiratory Tract Diseases epidemiology
Abstract

Competing Interests: The authors have no conflicts of interest to disclose.

Published
2018
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24. An International Comparison of Death Classification at 22 to 25 Weeks' Gestational Age.

Author

Smith LK, Morisaki N, Morken NH, Gissler M, Deb-Rinker P, Rouleau J, Hakansson S, Kramer MR, and Kramer MS

Subjects
Canada, Female, Finland, Gestational Age, Humans, Infant, Infant, Newborn, Japan, Norway, Pregnancy, Registries, Survival Rate, Sweden, United Kingdom, United States, Fetal Death, Infant Mortality
Abstract

Objectives: To explore international differences in the classification of births at extremely low gestation and the subsequent impact on the calculation of survival rates., Methods: We used national data on births at 22 to 25 weeks' gestation from the United States (2014; n = 11 144), Canada (2009-2014; n = 5668), the United Kingdom (2014-2015; n = 2992), Norway (2010-2014; n = 409), Finland (2010-2015; n = 348), Sweden (2011-2014; n = 489), and Japan (2014-2015; n = 2288) to compare neonatal survival rates using different denominators: all births, births alive at the onset of labor, live births, live births surviving to 1 hour, and live births surviving to 24 hours., Results: For births at 22 weeks' gestation, neonatal survival rates for which we used live births as the denominator varied from 3.7% to 56.7% among the 7 countries. This variation decreased when the denominator was changed to include stillbirths (ie, all births [1.8%-22.3%] and fetuses alive at the onset of labor [3.7%-38.2%]) or exclude early deaths and limited to births surviving at least 12 hours (50.0%-77.8%). Similar trends were seen for infants born at 23 weeks' gestation. Variation diminished considerably at 24 and 25 weeks' gestation., Conclusions: International variation in neonatal survival rates at 22 to 23 weeks' gestation diminished considerably when including stillbirths in the denominator, revealing the variation arises in part from differences in the proportion of births reported as live births, which itself is closely connected to the provision of active care., Competing Interests: POTENTIAL CONFLICT OF INTEREST: The authors have indicated they have no potential conflicts of interest to disclose., (Copyright © 2018 by the American Academy of Pediatrics.)

Published
2018
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25. International variations in the gestational age distribution of births: an ecological study in 34 high-income countries.

Author

Delnord M, Mortensen L, Hindori-Mohangoo AD, Blondel B, Gissler M, Kramer MR, Richards JL, Deb-Rinker P, Rouleau J, Morisaki N, Nassar N, Bolumar F, Berrut S, Nybo Andersen AM, Kramer MS, and Zeitlin J

Subjects
Australia epidemiology, Canada epidemiology, Europe epidemiology, Female, Humans, Income, Infant, Newborn, Japan epidemiology, Male, United States epidemiology, Developed Countries statistics & numerical data, Gestational Age, Premature Birth epidemiology, Term Birth
Abstract

Background: Few studies have investigated international variations in the gestational age (GA) distribution of births. While preterm births (22-36 weeks GA) and early term births (37-38 weeks) are at greater risk of adverse health outcomes compared to full term births (39-40 weeks), it is not known if countries with high preterm birth rates also have high early term birth rates. We examined rate associations between preterm and early term births and mean term GA by mode of delivery onset., Methods: We used routine aggregate data on the GA distribution of singleton live births from up to 34 high-income countries/regions in 1996, 2000, 2004, 2008 and 2010 to study preterm and early term births overall and by spontaneous or indicated onset. Pearson correlation coefficients were adjusted for clustering in time trend analyses., Results: Preterm and early term births ranged from 4.1% to 8.2% (median 5.5%) and 15.6% to 30.8% (median 22.2%) of live births in 2010, respectively. Countries with higher preterm birth rates in 2004-2010 had higher early term birth rates (r > 0.50, P < 0.01) and changes over time were strongly correlated overall (adjusted-r = 0.55, P < 0.01) and by mode of onset., Conclusion: Positive associations between preterm and early term birth rates suggest that common risk factors could underpin shifts in the GA distribution. Targeting modifiable population risk factors for delivery before 39 weeks GA may provide a useful preterm birth prevention paradigm.

Published
2018
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26. Variations in very preterm birth rates in 30 high-income countries: are valid international comparisons possible using routine data?

Author

Delnord M, Hindori-Mohangoo AD, Smith LK, Szamotulska K, Richards JL, Deb-Rinker P, Rouleau J, Velebil P, Zile I, Sakkeus L, Gissler M, Morisaki N, Dolan SM, Kramer MR, Kramer MS, and Zeitlin J

Subjects
Canada epidemiology, Developed Countries, Europe epidemiology, Female, Gestational Age, Humans, Infant, Newborn, Japan epidemiology, Pregnancy, United States epidemiology, Birth Rate, Pregnancy Outcome epidemiology, Premature Birth epidemiology
Abstract

Objective: Concerns about differences in registration practices across countries have limited the use of routine data for international very preterm birth (VPT) rate comparisons., Design: Population-based study., Setting: Twenty-seven European countries, the United States, Canada and Japan in 2010., Population: A total of 9 376 252 singleton births., Method: We requested aggregated gestational age data on live births, stillbirths and terminations of pregnancy (TOP) before 32 weeks of gestation, and information on registration practices for these births. We compared VPT rates and assessed the impact of births at 22-23 weeks of gestation, and different criteria for inclusion of stillbirths and TOP on country rates and rankings., Main Outcome Measures: Singleton very preterm birth rate, defined as singleton stillbirths and live births before 32 completed weeks of gestation per 1000 total births, excluding TOP if identifiable in the data source., Results: Rates varied from 5.7 to 15.7 per 1000 total births and 4.0 to 11.9 per 1000 live births. Country registration practices were related to percentage of births at 22-23 weeks of gestation (between 1% and 23% of very preterm births) and stillbirths (between 6% and 40% of very preterm births). After excluding births at 22-23 weeks, rate variations remained high and with a few exceptions, country rankings were unchanged., Conclusions: International comparisons of very preterm birth rates using routine data should exclude births at 22-23 weeks of gestation and terminations of pregnancy. The persistent large rate variations after these exclusions warrant continued surveillance of VPT rates at 24 weeks and over in high-income countries., Tweetable Abstract: International comparisons of VPT rates should exclude births at 22-23 weeks of gestation and terminations of pregnancy., (© 2016 Royal College of Obstetricians and Gynaecologists.)

Published
2017
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27. Temporal Trends in Late Preterm and Early Term Birth Rates in 6 High-Income Countries in North America and Europe and Association With Clinician-Initiated Obstetric Interventions.

Author

Richards JL, Kramer MS, Deb-Rinker P, Rouleau J, Mortensen L, Gissler M, Morken NH, Skjærven R, Cnattingius S, Johansson S, Delnord M, Dolan SM, Morisaki N, Tough S, Zeitlin J, and Kramer MR

Subjects
Canada epidemiology, Denmark epidemiology, Developing Countries, Female, Finland epidemiology, Gestational Age, Humans, Maternal Age, Norway epidemiology, Obstetric Labor, Premature epidemiology, Obstetrics trends, Pregnancy, Retrospective Studies, Sweden epidemiology, United States epidemiology, Cesarean Section trends, Labor, Induced trends, Obstetric Labor, Premature therapy, Term Birth
Abstract

Importance: Clinicians have been urged to delay the use of obstetric interventions (eg, labor induction, cesarean delivery) until 39 weeks or later in the absence of maternal or fetal indications for intervention., Objective: To describe recent trends in late preterm and early term birth rates in 6 high-income countries and assess association with use of clinician-initiated obstetric interventions., Design: Retrospective analysis of singleton live births from 2006 to the latest available year (ranging from 2010 to 2015) in Canada, Denmark, Finland, Norway, Sweden, and the United States., Exposures: Use of clinician-initiated obstetric intervention (either labor induction or prelabor cesarean delivery) during delivery., Main Outcomes and Measures: Annual country-specific late preterm (34-36 weeks) and early term (37-38 weeks) birth rates., Results: The study population included 2,415,432 Canadian births in 2006-2014 (4.8% late preterm; 25.3% early term); 305,947 Danish births in 2006-2010 (3.6% late preterm; 18.8% early term); 571,937 Finnish births in 2006-2015 (3.3% late preterm; 16.8% early term); 468,954 Norwegian births in 2006-2013 (3.8% late preterm; 17.2% early term); 737,754 Swedish births in 2006-2012 (3.6% late preterm; 18.7% early term); and 25,788,558 US births in 2006-2014 (6.0% late preterm; 26.9% early term). Late preterm birth rates decreased in Norway (3.9% to 3.5%) and the United States (6.8% to 5.7%). Early term birth rates decreased in Norway (17.6% to 16.8%), Sweden (19.4% to 18.5%), and the United States (30.2% to 24.4%). In the United States, early term birth rates decreased from 33.0% in 2006 to 21.1% in 2014 among births with clinician-initiated obstetric intervention, and from 29.7% in 2006 to 27.1% in 2014 among births without clinician-initiated obstetric intervention. Rates of clinician-initiated obstetric intervention increased among late preterm births in Canada (28.0% to 37.9%), Denmark (22.2% to 25.0%), and Finland (25.1% to 38.5%), and among early term births in Denmark (38.4% to 43.8%) and Finland (29.8% to 40.1%)., Conclusions and Relevance: Between 2006 and 2014, late preterm and early term birth rates decreased in the United States, and an association was observed between early term birth rates and decreasing clinician-initiated obstetric interventions. Late preterm births also decreased in Norway, and early term births decreased in Norway and Sweden. Clinician-initiated obstetric interventions increased in some countries but no association was found with rates of late preterm or early term birth.

Published
2016
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28. Differences in perinatal and infant mortality in high-income countries: artifacts of birth registration or evidence of true differences?

Author

Deb-Rinker P, León JA, Gilbert NL, Rouleau J, Andersen AM, Bjarnadóttir RI, Gissler M, Mortensen LH, Skjærven R, Vollset SE, Zhang X, Shah PS, Sauve RS, Kramer MS, and Joseph KS

Subjects
Birth Weight, Canada epidemiology, Gestational Age, Humans, Infant, Infant, Newborn, Retrospective Studies, Scandinavian and Nordic Countries epidemiology, United States epidemiology, Birth Certificates, Fetal Mortality, Infant Mortality, Vital Statistics
Abstract

Background: Variation in birth registration criteria may compromise international comparisons of fetal and infant mortality. We examined the effect of birth registration practices on fetal and infant mortality rates to determine whether observed differences in perinatal and infant mortality rates were artifacts of birth registration or reflected true differences in health status., Methods: A retrospective population-based cohort study was done using data from Canada, United States, Denmark, Finland, Iceland, Norway, and Sweden from 1995-2005. Main outcome measures included live births by gestational age and birth weight; gestational age-and birth weight-specific stillbirth rates; neonatal, post-neonatal, and cause-specific infant mortality., Results: Proportion of live births <22 weeks varied substantially: Sweden (not reported), Iceland (0.00%), Finland (0.001%), Denmark (0.01%), Norway (0.02%), Canada (0.07%) and United States (0.08%). At 22-23 weeks, neonatal mortality rates were highest in Canada (892.2 per 1000 live births), Denmark (879.3) and Iceland (1000.0), moderately high in the United States (724.1), Finland (794.3) and Norway (739.0) and low in Sweden (561.2). Stillbirth:live birth ratios at 22-23 weeks were significantly lower in the United States (79.2 stillbirths per 100 live births) and Finland (90.8) than in Canada (112.1), Iceland (176.2) and Norway (173.9). Crude neonatal mortality rates were 83% higher in Canada and 96% higher in the United States than Finland. Neonatal mortality rates among live births ≥ 28 weeks were lower in Canada and United States compared with Finland. Post-neonatal mortality rates were higher in Canada and United States than in Nordic countries., Conclusions: Live birth frequencies and stillbirth and neonatal mortality patterns at the borderline of viability are likely due to differences in birth registration practices, although true differences in maternal, fetal and infant health cannot be ruled out. This study emphasises the need for further standardisations, in order to enhance the relevance of international comparisons of infant mortality.

Published
2015
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29. Involvement of NOS3 in RA-Induced neural differentiation of human NT2/D1 cells.

Author

Jezierski A, Deb-Rinker P, Sodja C, Walker PR, Ly D, Haukenfrers J, Sandhu JK, Bani-Yaghoub M, and Sikorska M

Subjects
5' Untranslated Regions genetics, Acetylation, Cell Cycle drug effects, Cell Cycle physiology, Cell Line, Tumor cytology, Cell Line, Tumor drug effects, Cell Nucleus enzymology, Chromatin Immunoprecipitation, CpG Islands genetics, DNA Methylation, Enzyme Induction drug effects, Gene Expression Regulation, Developmental drug effects, Histones metabolism, Humans, Nerve Tissue Proteins antagonists & inhibitors, Nerve Tissue Proteins biosynthesis, Nerve Tissue Proteins genetics, Neurogenesis physiology, Neuroglia cytology, Neurons cytology, Nitric Oxide physiology, Nitric Oxide Donors pharmacology, Nitric Oxide Synthase Type I biosynthesis, Nitric Oxide Synthase Type I genetics, Nitric Oxide Synthase Type III antagonists & inhibitors, Nitric Oxide Synthase Type III biosynthesis, Nitric Oxide Synthase Type III genetics, Ornithine analogs & derivatives, Ornithine pharmacology, Protein Processing, Post-Translational, RNA, Messenger biosynthesis, RNA, Messenger genetics, Teratocarcinoma pathology, Triazenes pharmacology, Nerve Tissue Proteins physiology, Neurogenesis drug effects, Nitric Oxide Synthase Type III physiology, Tretinoin pharmacology
Abstract

Nitric oxide (NO) plays a key role in neurogenesis as a regulator of cell proliferation and differentiation. NO is synthesized from the amino acid L-arginine by nitric oxide synthases (NOS1, NOS2, and NOS3), which are encoded by separate genes and display different tissue distributions. We used an in vitro model of RA-induced neural differentiation of NT2 cells to examine which of the three NO-synthesizing enzymes is involved in this process. The results revealed a transient induction of NOS3 (known as the constitutively expressed endothelial nitric oxide synthase; eNOS) during the time course of the RA treatment. The peak of gene expression and the nuclear presence of NOS3 protein coincided with cell cycle exit of NT2-derived neuronal precursors. The subsequent analysis of cytosine methylation and histone H3 acetylation of the human NOS3 5' regulatory sequences indicated that epigenetic modifications, especially upstream of the proximal promoter (-734 to -989, relative to exon 2 TSS at +1), were also taking place. NOS1 was expressed only in the differentiated neurons (NT2-N), whereas NOS2 was not expressed at all in this cellular model. Thus, a burst of NO production, possibly required to inhibit neural cell proliferation, was generated by the transient expression of NOS3. This pattern of gene expression, in turn, required epigenetic remodeling of its regulatory region., (Copyright © 2012 Wiley Periodicals, Inc.)

Published
2012
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30. Epigenetic modifications of SOX2 enhancers, SRR1 and SRR2, correlate with in vitro neural differentiation.

Author

Sikorska M, Sandhu JK, Deb-Rinker P, Jezierski A, Leblanc J, Charlebois C, Ribecco-Lutkiewicz M, Bani-Yaghoub M, and Walker PR

Subjects
Acetylation, Astrocytes cytology, Astrocytes metabolism, Base Sequence, Calcium-Binding Proteins genetics, Cells, Cultured, DNA Methylation, DNA-Binding Proteins genetics, DNA-Binding Proteins metabolism, HMGB Proteins genetics, HMGB Proteins metabolism, Humans, Membrane Glycoproteins genetics, Molecular Sequence Data, Neurons metabolism, Receptors, Cytoplasmic and Nuclear genetics, Receptors, Peptide genetics, SOXB1 Transcription Factors, Stem Cells cytology, Stem Cells metabolism, Transcription Factors genetics, Transcription Factors metabolism, Calcium-Binding Proteins physiology, Cell Differentiation physiology, DNA-Binding Proteins biosynthesis, Enhancer Elements, Genetic physiology, Epigenesis, Genetic physiology, HMGB Proteins biosynthesis, Membrane Glycoproteins physiology, Neurons cytology, Receptors, Cytoplasmic and Nuclear physiology, Receptors, Peptide physiology, Transcription Factors biosynthesis
Abstract

SOX2 is a key neurodevelopmental gene involved in maintaining the pluripotency of stem cells and proliferation of neural progenitors and astroglia. Two evolutionally conserved enhancers, SRR1 and SRR2, are involved in controlling SOX2 expression during neurodevelopment; however, the molecular mechanisms regulating their activity are not known. We have examined DNA methylation and histone H3 acetylation at both enhancers in NT2-D1 progenitors, neurons and astrocytes, to establish the role of epigenetic mechanisms in cell-type-specific SOX2 expression. This study showed that 1) unmethylated DNA and acetylated histones at both enhancers correlated with a high level of SOX2 expression in proliferating neural progenitors and 2) reversible modifications of the SRR1 element were observed during gene reexpression in astrocytes, whereas permanent epigenetic marks on the SRR2 enhancer were seen in neurons where the gene was silenced. Taken together, these results are clear illustrations of cell-type-specific epigenomes and suggest mechanisms by which they may be created and maintained., ((c) 2008 Wiley-Liss, Inc.)

Published
2008
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31. Sequential DNA methylation of the Nanog and Oct-4 upstream regions in human NT2 cells during neuronal differentiation.

Author

Deb-Rinker P, Ly D, Jezierski A, Sikorska M, and Walker PR

Subjects
5' Flanking Region, Cell Differentiation drug effects, Cell Line, Down-Regulation, Humans, Nanog Homeobox Protein, Octamer Transcription Factor-3, Polymerase Chain Reaction, Promoter Regions, Genetic, Regulatory Sequences, Nucleic Acid, Tretinoin pharmacology, Cell Differentiation genetics, DNA Methylation, DNA-Binding Proteins genetics, Homeodomain Proteins genetics, Neurons cytology, Transcription Factors genetics
Abstract

Human NT2 cells, which differentiate into neurons and astrocytes, initially express and then permanently down-regulate Nanog and Oct-4 (POU5F1). We investigated the relationship between the expression of these genes and the methylation state of their 5'-flanking regions. Gene expression and DNA methylation were assayed with quantitative polymerase chain reaction and bisulfite genomic sequencing, respectively. Retinoic acid-induced differentiation of NT2 cells to neurons is accompanied by a sequential decrease in the expression of both genes, paralleled by sequential epigenetic modification of their upstream regions. This is the first report demonstrating changes in DNA methylation in the promoter regions of Nanog and Oct-4 in a human cell line.

Published
2005
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32. Molecular characterization of a 2.7-kb, 12q13-specific, retroviral-related sequence isolated by RDA from monozygotic twin pairs discordant for schizophrenia.

Author

Deb-Rinker P, O'Reilly RL, Torrey EF, and Singh SM

Subjects
Base Sequence, Chromosome Mapping, Chromosomes, Artificial, Bacterial, DNA blood, DNA isolation & purification, DNA Methylation, Databases, Genetic, Female, Genome, Humans, In Situ Hybridization, Fluorescence, Male, Molecular Sequence Data, Sequence Analysis, DNA, Chromosomes, Human, Pair 12, Endogenous Retroviruses genetics, Genetic Techniques, Schizophrenia genetics, Twins, Monozygotic genetics
Abstract

This report deals with the molecular characterization of a representational difference analysis (RDA)-derived sequence (SZRV-2, GenBank accession No. AF135486; Genome Database accession Nos. 7692183 and 7501402) from three monozygotic twin pairs discordant for schizophrenia (MZD). The results suggest that it is a primate-specific, heavily methylated, and placentally expressed (-7-kb mRNA) endogenous retroviral-related (ERV) sequence of the human genome. We have mapped this sequence to 12q13 using two SZRV-2 positive BAC clones (4K11 (Genome Survey Sequence Database No. 1752076; GenBank accession No. AZ301773) and 501H16) by fluorescence in situ hybridization. End sequencing of the 4K11 BAC clone has allowed identification of nearby genes from the human genome database at NCBI that may be of interest in schizophrenia research. These include viral-related sequences (potential hot spots for insertions), developmental, channel, and signal transduction genes, as well as genes affecting expression of certain receptors in neurons. Furthermore, when used as a probe on Southern blots, SZRV-2 detected no difference between schizophrenia patients from southwestern Ontario and their matched controls. However, it identified aberrant methylation in one of the eight patients and none of the 21 unaffected controls. Although additional experiments will be required to establish the significance, if any, of SZRV-2 methylation in the complex etiology of schizophrenia, molecular results included offer a novel insight into the role of retroviral-related sequences in the origin, organization, and regulation of the human genome.

Published
2002
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33. Molecular genetic studies of human chromosome 7 in Russell-Silver syndrome.

Author

Nakabayashi K, Fernandez BA, Teshima I, Shuman C, Proud VK, Curry CJ, Chitayat D, Grebe T, Ming J, Oshimura M, Meguro M, Mitsuya K, Deb-Rinker P, Herbrick JA, Weksberg R, and Scherer SW

Subjects
Amino Acid Sequence, Animals, Body Height genetics, Chromosome Aberrations, Cytogenetic Analysis, Facies, Humans, Hybrid Cells, In Situ Hybridization, Fluorescence, Mice, Molecular Sequence Data, Sequence Analysis, DNA, Sequence Homology, Amino Acid, Syndrome, Abnormalities, Multiple genetics, Chromosomes, Human, Pair 7
Abstract

Russell-Silver syndrome (RSS) is a form of congenital short stature characterized by severe growth retardation and variable dysmorphic features. In some RSS individuals, alterations in imprinted genes may be involved because approximately 7% of sporadic patients have been observed to have maternal uniparental disomy (mUPD) of chromosome 7. RSS patients with structural abnormalities of chromosome 7 have also been described. In these individuals the chromosome rearrangement could disrupt the balance of imprinted genes, contribute to a recessive form of RSS, or lead to haploinsufficiency of a crucial developmental gene product. Because the mechanism and molecular defects on chromosome 7 causing RSS are still unknown, we tested our collection of 77 RSS families for mUPD7 and were able to identify three new cases. We also characterized two RSS patients with de novo cytogenetic abnormalities involving the short arm of chromosome 7. One had a partial duplication [46, XX, dup(7)(p12 p14)] and the second contained a paracentric inversion [46, XY, inv(7)(p14 p21)]. Fluorescence in situ hybridization (FISH) mapping revealed that the breakpoints on 7p14 were localized to the same novel gene, C7orf10, which encompasses >700 kb of DNA. We also identified other transcription units from this immediate region, but all seem to be biallelically expressed when using a somatic cell hybrid assay.

Published
2002
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