Search

Your search keyword '"Nanette Okun"' showing total 83 results
Start Over Author "Nanette Okun"
83 results on '"Nanette Okun"'

1. Improving health equity through sustained academic partnership: development of a maternal-fetal medicine fellowship training program in Western Kenya

Author

David Nding'ori, MMed, Rachel F. Spitzer, MD, MPH, Julia Songok, MMed, Marie Buitendyk, MD, MSc, Pallavi Mishra, MMed, Wycliffe Kosgei, MMed, Bett Kipchumba, MMed, Mutindi Kakuti, MMed, Philip Tonui, MMed, Karen Fung-Kee-Fung, MD, MHPE, Heidi Leftwich, DO, Adrian Gardner, MD, MPH, Paul Nyongesa, MMed, and Nanette Okun, MD, MHsc

Subjects
global health, perinatal outcomes, maternal morbidity and mortality, Gynecology and obstetrics, RG1-991
Abstract

Low- and middle-income countries are underresourced in subspecialist care. This study describes a unique maternal-fetal medicine clinical fellowship training program at Moi University School of Medicine and Moi Teaching and Referral Hospital in Eldoret, Western Kenya. The first of its kind in Eastern Africa, it has met with success in the retention of highly qualified practitioners providing complex pregnancy care to a population that has been heretofore underserved.

Published
2024
Full Text
View/download PDF

2. Prevalence of Rheumatic Heart Disease and Other Cardiac Conditions in Low-Risk Pregnancies in Kenya: A Prospective Echocardiography Screening Study

Author

John W. Snelgrove, Joy Marsha Alera, Michael C. Foster, Kipchumba C. N. Bett, Gerald S. Bloomfield, Candice K. Silversides, Felix A. Barasa, Astrid Christoffersen-Deb, Heather C. Millar, Julie G. Thorne, Rachel F. Spitzer, Rajesh Vedanthan, and Nanette Okun

Subjects
rheumatic heart disease, pregnancy, echocardiography, epidemiology, kenya, africa, Diseases of the circulatory (Cardiovascular) system, RC666-701, Public aspects of medicine, RA1-1270
Abstract

Background: Rheumatic heart disease (RHD) in sub-Saharan Africa contributes to significant cardiac morbidity and mortality, yet prevalence estimates of RHD lesions in pregnancy are lacking. Objectives: Our first aim was to evaluate women using echocardiography to estimate the prevalence of RHD and other cardiac lesions in low-risk pregnancies. Our second aim was to assess the feasibility of screening echocardiography and its acceptability to patients. Methods: We prospectively recruited 601 pregnant women from a low-risk antenatal clinic at a tertiary care maternity centre in Western Kenya. Women completed a questionnaire about past medical history and cardiac symptoms. They underwent standardized screening echocardiography to evaluate RHD and non-RHD associated cardiac lesions. Our primary outcome was RHD-associated cardiac lesions and our secondary outcome was a composite of any clinically-relevant cardiac lesion or echocardiography finding. We also recorded duration of screening echocardiography and its acceptability among pregnant women in this sample. Results: The point prevalence of RHD-associated cardiac lesions was 5.0/1,000 (95% confidence interval: 1.0–14.5), and the point prevalence of all clinically significant lesions/findings was 21.6/1,000 (11.6–36.7). Mean screening time was seven minutes (SD 1.7, range: 4–17) for women without cardiac abnormalities and 13 minutes (SD 4.6, range: 6–23) for women with abnormal findings. Echocardiography was acceptable to women with 74.2% agreeing to participate. Conclusions: The prevalence of clinically-relevant cardiac lesions was moderately high in a low-risk population of pregnant women in Western Kenya.

Published
2021
Full Text
View/download PDF

5. Cost-effectiveness of noninvasive fetal RhD blood group genotyping in nonalloimmunized and alloimmunized pregnancies

Author

Olga Gajic‐Veljanoski, Chunmei Li, Alexis K. Schaink, Jennifer Guo, Nadine Shehata, George S. Charames, Barbra Vrijer, Gwen Clarke, Petros Pechlivanoglou, Nanette Okun, Rita Kandel, Joseph Dooley, Caroline Higgins, Vivian Ng, and Nancy Sikich

Subjects
Rh-Hr Blood-Group System, Genotype, Cost-Benefit Analysis, Rho(D) Immune Globulin, Immunology, Hematology, Fetal Blood, Rh Isoimmunization, Pregnancy, Prenatal Diagnosis, Blood Group Antigens, Immunology and Allergy, Humans, Female
Abstract

We sought to determine the cost-effectiveness of noninvasive fetal RhD blood group genotyping in nonalloimmunized and alloimmunized pregnancies in Canada.We developed two probabilistic state-transition (Markov) microsimulation models to compare fetal genotyping followed by targeted management versus usual care (i.e., universal Rh immunoglobulin [RhIG] prophylaxis in nonalloimmunized RhD-negative pregnancies, or universal intensive monitoring in alloimmunized pregnancies). The reference case considered a healthcare payer perspective and a 10-year time horizon. Sensitivity analysis examined assumptions related to test cost, paternal screening, subsequent pregnancies, other alloantibodies (e.g., K, Rh c/C/E), societal perspective, and lifetime horizon.Fetal genotyping in nonalloimmunized pregnancies (at per-sample test cost of C$247/US$311) was associated with a slightly higher probability of maternal alloimmunization (22 vs. 21 per 10,000) and a reduced number of RhIG injections (1.427 vs. 1.795) than usual care. It was more expensive (C$154/US$194, 95% Credible Interval [CrI]: C$139/US$175-C$169/US$213) and had little impact on QALYs (0.0007, 95%CrI: -0.01-0.01). These results were sensitive to the test cost (threshold achieved at C$88/US$111), and inclusion of paternal screening. Fetal genotyping in alloimmunized pregnancies (at test cost of C$328/US$413) was less expensive (-C$6280/US$7903, 95% CrI: -C$6325/US$7959 to -C$6229/US$7838) and more effective (0.19 QALYs, 95% CrI 0.17-0.20) than usual care. These cost savings remained robust in sensitivity analyses.Noninvasive fetal RhD genotyping saves resources and represents good value for the management of alloimmunized pregnancies. If the cost of genotyping is substantially decreased, the targeted intervention can become a viable option for nonalloimmunized pregnancies.

Published
2022

11. Comparing Maternal Serum Screening Markers Among IVF and Spontaneous Conceptions in Ontario Through Registry Data

Author

Beth K. Potter, Moya Johnson, Arthur Leader, Ann E. Sprague, Tianhua Huang, Deshayne B. Fell, Shelley Dougan, Nanette Okun, Andrea Lanes, and Mark Walker

Subjects
Adult, medicine.medical_specialty, Reproductive Techniques, Assisted, Pregnancy-associated plasma protein A, Population, Fertilization in Vitro, Reproductive technology, Human chorionic gonadotropin, 03 medical and health sciences, 0302 clinical medicine, Predictive Value of Tests, Pregnancy, Prenatal Diagnosis, Humans, Pregnancy-Associated Plasma Protein-A, Medicine, Registries, 030212 general & internal medicine, education, reproductive and urinary physiology, Ontario, education.field_of_study, 030219 obstetrics & reproductive medicine, urogenital system, business.industry, Obstetrics, Multiple of the median, Obstetrics and Gynecology, female genital diseases and pregnancy complications, Embryo transfer, Pregnancy Trimester, First, Pregnancy Trimester, Second, embryonic structures, Female, Down Syndrome, Nuchal Translucency Measurement, Alpha-fetoprotein, business, Serum screening, Biomarkers, hormones, hormone substitutes, and hormone antagonists
Abstract

Objective The objectives of this study were as follows: (1) to investigate the accuracy of IVF identification on the prenatal screening record from prenatal screening laboratories; (2) to compare the screening markers in IVF and non-IVF pregnancies in the population of Ontario; and (3) to propose more appropriate IVF adjustment factors for the Ontario population. Methods Two years of IVF treatment, data from all fertility clinics in Ontario were merged with the corresponding prenatal screening data from all five prenatal screening labs. New adjustment factors for IVF were developed for each maternal serum screening marker and nuchal translucency measurement. Means and SDs and linear regression models were reported for all prenatal screening records, as well as for records that had IVF identified through the prenatal screening requisition and records that were identified through the Canadian Assisted Reproductive Technologies Register (CARTR) Plus database. Results Significant differences between IVF and non-IVF groups on the basis of the prenatal screening requisition information and CARTR Plus information were found among the ethnicity-adjusted mean multiple of the medians for alpha fetoprotein, first trimester pregnancy-associated plasma protein A, second trimester unconjugated estradiol, first trimester human chorionic gonadotropin, total human chorionic gonadotropin, and dimeric inhibin A. Conclusion This study proposed alternate IVF adjustment factors that will produce more accurate screening results within the population of Ontario.

Published
2018

12. Noninvasive Fetal RhD Blood Group Genotyping: A Systematic Review of Economic Evaluations

Author

Nadine Shehata, Caroline Higgins, Chunmei Li, Alexis K. Schaink, Olga Gajic-Veljanoski, Jennifer Guo, Barbra de Vrijer, Vivian Ng, Nancy Sikich, Petros Pechlivanoglou, and Nanette Okun

Subjects
medicine.medical_specialty, Pregnancy, Fetus, Rh-Hr Blood-Group System, Genotype, medicine.diagnostic_test, Cost–benefit analysis, Obstetrics, business.industry, Cost effectiveness, Cost-Benefit Analysis, Obstetrics and Gynecology, Fetal Blood, Rh Isoimmunization, medicine.disease, Rhesus d, Data extraction, Prenatal Diagnosis, medicine, Humans, Female, business, Genotyping, Genetic testing
Abstract

Objective Noninvasive fetal rhesus D (RhD) blood group genotyping may prevent unnecessary use of anti-D immunoglobulin (RhIG) in non-alloimmunized RhD-negative pregnancies and can guide management of alloimmunized pregnancies. We conducted a systematic review of the economic literature to determine the cost-effectiveness of this intervention over usual care. Data Sources Systematic literature searches of bibliographic databases (Ovid MEDLINE, Embase, and Cochrane) until February 26, 2019, and auto-alerts until October 30, 2020, and of grey literature sources were performed to retrieve all English-language studies. Study Selection We included studies done in serologically confirmed non-alloimmunized or alloimmunized RhD-negative pregnancies, comparing costs and effectiveness of the intervention versus usual care. Data Extraction and Synthesis Two reviewers extracted data from the eligible studies and assessed their methodological quality (risk of bias) using the Quality of Health Economic Studies (QHES) and Drummond tools. We narratively synthesized findings. Our review included 8 economic studies that evaluated non-invasive fetal RhD genotyping followed by targeted RhIG prophylaxis in non-alloimmunized pregnancies. Five studies further considered a subsequent alloimmunized pregnancy. The cost-effectiveness of the intervention versus usual care (e.g., universal RhIG or prophylaxis conditional on results of paternal testing) for non-alloiummunized pregnancies was inconsistent. Two studies indicated greater benefits and lower costs for the intervention, and another 2 suggested a trade-off. In 4 studies, the intervention was less effective and costlier than alternatives. Three studies were determined to be of high quality by both tools. Two of these studies favoured the intervention, and one assessed benefits in quality-adjusted life-years. No study clearly examined the cost-effectiveness of repetitive use of fetal genotyping in multiple non-alloimmunized or alloimmunized pregnancies. The cost of genotyping was the most influential parameter. Conclusion The cost-effectiveness of noninvasive fetal RhD genotyping for non-alloimmunized pregnancies varies between studies. Potential savings from targeted management of alloimmunized pregnancies requires further research.

Published
2021

13. No 348-Directive clinique de la SOGC et du CCGM : mise à jour sur le dépistage prénatal de l’aneuploïdie fœtale, des anomalies fœtales et des issues défavorables de la grossesse

Author

Nanette Okun, R. Douglas Wilson, Isabelle De Bie, François Audibert, Jo-Ann Johnson, Christine M. Armour, David Chitayat, and Raymond H. Kim

Subjects
Gynecology, 03 medical and health sciences, medicine.medical_specialty, 030219 obstetrics & reproductive medicine, 0302 clinical medicine, business.industry, Obstetrics and Gynecology, Medicine, 030212 general & internal medicine, business
Published
2017

14. No. 348-Joint SOGC-CCMG Guideline: Update on Prenatal Screening for Fetal Aneuploidy, Fetal Anomalies, and Adverse Pregnancy Outcomes

Author

Jo-Ann Johnson, Nanette Okun, François Audibert, Isabelle De Bie, Christine M. Armour, Raymond H. Kim, R. Douglas Wilson, and David Chitayat

Subjects
medicine.medical_specialty, Genetic counseling, MEDLINE, Prenatal diagnosis, Cochrane Library, Congenital Abnormalities, 03 medical and health sciences, 0302 clinical medicine, Pregnancy, Prenatal Diagnosis, Humans, Medicine, 030212 general & internal medicine, Gynecology, 030219 obstetrics & reproductive medicine, medicine.diagnostic_test, business.industry, Obstetrics and Gynecology, Guideline, Aneuploidy, Pregnancy Complications, Systematic review, Cell-free fetal DNA, Family medicine, Amniocentesis, Female, business, Cell-Free Nucleic Acids, Biomarkers
Abstract

Objective To review the available prenatal screening options in light of the recent technical advances and to provide an update of previous guidelines in the field of prenatal screening. Intended Users Health care providers involved in prenatal screening, including general practitioners, obstetricians, midwives, maternal fetal medicine specialists, geneticists, and radiologists. Target Population All pregnant women receiving counselling and providing informed consent for prenatal screening. Evidence Published literature was retrieved through searches of Medline, PubMed, and the Cochrane Library in and prior to March 2016 using an appropriate controlled vocabulary (prenatal diagnosis, amniocentesis, chorionic villi sampling, non-invasive prenatal screening) and key words (prenatal screening, prenatal genetic counselling). Results were restricted to systematic reviews, randomized control trials/controlled clinical trials, and observational studies written in English and published from January 1985 to May 2016. Searches were updated on a regular basis and incorporated in the guideline. Grey (unpublished) literature was identified through searching the websites of health technology assessment and health technology-related agencies, clinical practice guideline collections, clinical trial registries, and national and international medical speciality societies. Guideline update Evidence will be reviewed 5 years after publication to determine whether all or part of the guideline should be updated. However, if important new evidence is published prior to the 5-year cycle, the review process may be accelerated for a more rapid update of some recommendations.

Published
2017

15. Anomalies fœtales affectant le tube neural : Dépistage / diagnostic prénatal et prise en charge de la grossesse

Author

W. Kim MacDonald, Alain Gagnon, Lola Cartier, Jo-Ann Brock, François Audibert, Carla Campagnolo, Melanie Pastuck, June C. Carroll, Jo-Ann Johnson, R. Douglas Wilson, David Chitayat, Vanessa Popa, Sylvie Langlois, Nanette Okun, and Lynn Murphy-Kaulbeck

Subjects
Gynecology, Anencephaly, medicine.medical_specialty, Meningomyelocele, business.industry, Infant, Newborn, Obstetrics and Gynecology, Spina Bifida Occulta, Magnetic Resonance Imaging, Ultrasonography, Prenatal, Pregnancy, Evidence-Based Practice, Prenatal Diagnosis, Practice Guidelines as Topic, Amniocentesis, Humans, Medicine, Female, Neural Tube Defects, alpha-Fetoproteins, business, Spinal Dysraphism
Abstract

Resume Objectif Fournir, aux professionnels de la sante des domaines de l'obstetrique et de la genetique, des lignes directrices et des recommandations en ce qui a trait au depistage / diagnostic prenatal et a la prise en charge obstetricale du dysraphisme spinal ouvert / ferme (DSOF) chez le fœtus. Options La presente analyse englobe les techniques de depistage / diagnostic prenatal qui sont actuellement utilisees aux fins de la detection du DSOF, y compris le depistage des concentrations seriques en alphafoetoproteines chez la mere, l'echographie, l'imagerie par resonance magnetique visant le fœtus et l'amniocentese. Issues Ameliorer le depistage / diagnostic prenatal et la prise en charge obstetricale du DSOF, tout en prenant en consideration les soins offerts a la patiente, l'efficacite, les couts et les interventions de soins. Resultats La litterature publiee a ete recuperee par l'intermediaire de recherches menees dans PubMed ou MEDLINE, CINAHL et The Cochrane Library en novembre 2013 au moyen d'un vocabulaire controle et de mots cles appropries (p. ex. « prenatal screening », « congenital anomalies », « neural tube defects », « alpha-fetoprotein », « ultrasound scan », « magnetic resonance imaging »). Les resultats ont ete restreints aux analyses systematiques, aux essais comparatifs randomises / essais cliniques comparatifs et aux etudes observationnelles publies en anglais entre 1977 et 2012. Les recherches ont ete mises a jour de facon reguliere et ont ete integrees a la directive clinique jusqu'au 30 novembre 2013. La litterature grise (non publiee) a ete identifiee par l'intermediaire de recherches menees dans les sites Web d'organismes s'interessant a l'evaluation des technologies dans le domaine de la sante et d'organismes connexes, dans des collections de directives cliniques, dans des registres d'essais cliniques et aupres de societes de specialite medicale nationales et internationales. Une enquete en ligne menee aupres des praticiens de la sante a egalement fait l'objet d'une analyse. Valeurs La qualite des resultats est evaluee au moyen des criteres decrits dans le rapport du Groupe d'etude canadien sur les soins de sante preventifs (Tableau). Avantages, desavantages et couts La presente analyse permettra aux professionnels de la sante de mieux comprendre les methodes de depistage prenatal du DSOF dont nous disposons a l'heure actuelle, ainsi que les avantages et les risques qui sont associes a chacune de ces methodes, pour assurer la prise de decisions factuelles en ce qui concerne le depistage, le diagnostic et la prise en charge obstetricale du DSOF.

Published
2016

16. Prenatal Diagnosis Procedures and Techniques to Obtain a Diagnostic Fetal Specimen or Tissue: Maternal and Fetal Risks and Benefits

Author

R. Douglas Wilson, Alain Gagnon, François Audibert, Carla Campagnolo, June Carroll, Jo-Ann Brock, Karen Chong, Jo-Ann Johnson, William MacDonald, Nanette Okun, Melanie Pastuck, and Karine Vallee-Pouliot

Subjects
medicine.medical_specialty, Pregnancy, medicine.diagnostic_test, Obstetrics, business.industry, Genetic counseling, Directive Counseling, Obstetrics and Gynecology, Genetic Counseling, Prenatal diagnosis, Guideline, medicine.disease, Risk Assessment, Congenital Abnormalities, Systematic review, Prenatal Diagnosis, medicine, Amniocentesis, Humans, Female, Genetic Testing, business, Risk assessment, Genetic testing
Abstract

To provide maternity care providers and their patients with current evidence-based guidelines for maternal risk/benefit counselling for a prenatally identified at-risk pregnancy that requires ultrasound-guided prenatal diagnostic procedures and/or techniques for a genetic diagnosis and for subsequent pregnancy management decisions on questions such as level of obstetrical care provider, antenatal surveillance, location of care and delivery, and continuation or termination of pregnancy. This guideline is limited to maternal risk/benefit counselling and pregnancy management decisions for women who require, or are considering, an invasive ultrasound-guided procedure or technique for prenatal diagnosis.Pregnant women identified as having an increased risk of a fetal genetic abnormality secondary to the process of established prenatal screening protocols (maternal serum±imaging, high-risk cell-free DNA results, abnormal diagnostic fetal imaging, or a positive family history of an inherited condition). These women may require or request counselling about pregnancy risks and benefits of an invasive ultrasound-guided procedure to determine the etiology, diagnosis, and/or pathology for the possible fetal anomaly or anomalies.Published literature was retrieved through searches of Medline, PubMed, and the Cochrane Library in and prior to June 2014 using an appropriate controlled vocabulary (prenatal diagnosis, amniocentesis, chorionic villi sampling, cordocentesis) and key words (prenatal screening, prenatal genetic counselling, post-procedural pregnancy loss rate). Results were restricted to systematic reviews, randomized control trials/controlled clinical trials, and observational studies written in English and published from January 1985 to June 2014. Searches were updated on a regular basis and incorporated in the guideline to June 2014. Grey (unpublished) literature was identified through searching the websites of health technology assessment and health technology-related agencies, clinical practice guideline collections, clinical trial registries, and national and international medical speciality societies.The quality of evidence in this document was rated using the criteria described in the Report of the Canadian Task Force on Preventive Health Care (Table 1). Health benefits, side effects, and risks: Patient informed consent, knowledge translation, genetic prenatal risk assessment, anxiety relief, anxiety creation, advocacy, understanding or limitation for fetal testing, pregnancy management choice, pregnancy complication or loss, timely and improved care for birth of a neonate with recognized morbidity. Recommendations 1. The health care provider should counsel the at-risk pregnant woman on the different levels of genetic fetal testing in order for her to have a clear understanding and expectation of the level of testing and type of results that are offered. (III-B) 2. As part of the informed consent process, the health care provider should review with the at-risk pregnant woman the risks and benefits of in utero genetic diagnostic techniques associated with fetal genetic testing options. (III-A) 3. During risk/benefit counselling, the health care provider should advise that the best estimate of the pregnancy loss rate related to: a.amniocentesis is 0.5% to 1.0% (range 0.17 to 1.53%) (I) b.chorionic villus sampling is 0.5% to 1.0% (I) and c.cordocentesis or percutaneous umbilical blood sampling is 1.3% for fetuses with no anomalies and 1.3% to 25% for fetuses with single or multiple anomalies or intrauterine growth restriction. (II-2A).

Published
2015

17. 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

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

Subjects
Health Knowledge, Attitudes, Practice, Pediatrics, medicine.medical_specialty, Prenatal care, Cochrane Library, law.invention, Folic Acid, Randomized controlled trial, Pregnancy, law, Humans, Medicine, Anencephaly, Neural tube defect, business.industry, Spina bifida, Decision Trees, Obstetrics and Gynecology, Prenatal Care, medicine.disease, Systematic review, Dietary Supplements, Vitamin B Complex, Female, Preconception Care, business, Multivitamin
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 literature was retrieved through searches of PubMed, Medline, CINAHL, and the Cochrane Library in January 2011 using appropriate controlled vocabulary and key words (e.g., folic acid, prenatal multivitamins, folate sensitive birth defects, congenital anomaly risk reduction, pre-conception counselling). Results were restricted to systematic reviews, randomized control trials/controlled clinical trials, and observational studies published in English from 1985 and June 2014. Searches were updated on a regular basis and incorporated in the guideline to June 2014 Grey (unpublished) literature was identified through searching the websites of health technology assessment and health technology-related agencies, clinical practice guideline collections, clinical trial registries, and national and international medical specialty societies. Costs, risks, and benefits: The financial costs are those of daily vitamin supplementation and eating a healthy folate-enriched diet. The risks are of a reported association of dietary folic acid supplementation with fetal epigenetic modifications and with an increased likelihood of a twin pregnancy. These associations may require consideration before initiating folic acid supplementation. The benefit of folic acid oral supplementation or dietary folate intake combined with a multivitamin/micronutrient supplement is an associated decrease in neural tube defects and perhaps in other specific birth defects and obstetrical complications.The quality of evidence in the document was rated using the criteria described in the Report of the Canadian Task Force on Preventative Health Care (Table 1). Summary Statement In Canada multivitamin tablets with folic acid are usually available in 3 formats: regular over-the-counter multivitamins with 0.4 to 0.6 mg folic acid, prenatal over-the-counter multivitamins with 1.0 mg folic acid, and prescription multivitamins with 5.0 mg folic acid. (III) Recommendations 1. Women should be advised to maintain a healthy folate-rich diet; however, folic acid/multivitamin supplementation is needed to achieve the red blood cell folate levels associated with maximal protection against neural tube defect. (III-A) 2. All women in the reproductive age group (12-45 years of age) who have preserved fertility (a pregnancy is possible) should be advised about the benefits of folic acid in a multivitamin supplementation during medical wellness visits (birth control renewal, Pap testing, yearly gynaecological examination) whether or not a pregnancy is contemplated. Because so many pregnancies are unplanned, this applies to all women who may become pregnant. (III-A) 3. Folic acid supplementation is unlikely to mask vitamin B12 deficiency (pernicious anemia). Investigations (examination or laboratory) are not required prior to initiating folic acid supplementation for women with a risk for primary or recurrent neural tube or other folic acid-sensitive congenital anomalies who are considering a pregnancy. It is recommended that folic acid be taken in a multivitamin including 2.6 ug/day of vitamin B12 to mitigate even theoretical concerns. (II-2A) 4. Women at HIGH RISK, for whom a folic acid dose greater than 1 mg is indicated, taking a multivitamin tablet containing folic acid, should be advised to follow the product label and not to take more than 1 daily dose of the multivitamin supplement. Additional tablets containing only folic acid should be taken to achieve the desired dose. (II-2A) 5. Women with a LOW RISK for a neural tube defect or other folic acid-sensitive congenital anomaly and a male partner with low risk require a diet of folate-rich foods and a daily oral multivitamin supplement containing 0.4 mg folic acid for at least 2 to 3 months before conception, throughout the pregnancy, and for 4 to 6 weeks postpartum or as long as breast-feeding continues. (II-2A) 6. Women with a MODERATE RISK for a neural tube defect or other folic acid-sensitive congenital anomaly or a male partner with moderate risk require a diet of folate-rich foods and daily oral supplementation with a multivitamin containing 1.0 mg folic acid, beginning at least 3 months before conception. Women should continue this regime until 12 weeks' gestational age. (1-A) From 12 weeks' gestational age, continuing through the pregnancy, and for 4 to 6 weeks postpartum or as long as breast-feeding continues, continued daily supplementation should consist of a multivitamin with 0.4 to 1.0 mg folic acid. (II-2A) 7. Women with an increased or HIGH RISK for a neural tube defect, a male partner with a personal history of neural tube defect, or history of a previous neural tube defect pregnancy in either partner require a diet of folate-rich foods and a daily oral supplement with 4.0 mg folic acid for at least 3 months before conception and until 12 weeks' gestational age. From 12 weeks' gestational age, continuing throughout the pregnancy, and for 4 to 6 weeks postpartum or as long as breast-feeding continues, continued daily supplementation should consist of a multivitamin with 0.4 to 1.0 mg folic acid. (I-A). The same dietary and supplementation regime should be followed if either partner has had a previous pregnancy with a neural tube defect. (II-2A).

Published
2015

18. RETIRED: Technical Update: Preimplantation Genetic Diagnosis and Screening

Author

Elias M. Dahdouh, Jacques Balayla, François Audibert, R. Douglas Wilson, Jo-Ann Brock, Carla Campagnolo, June Carroll, Karen Chong, Alain Gagnon, Jo-Ann Johnson, William MacDonald, Nanette Okun, Melanie Pastuck, and Karine Vallée-Pouliot

Subjects
Gynecology, medicine.medical_specialty, business.industry, MEDLINE, Obstetrics and Gynecology, Prenatal diagnosis, Reproductive technology, Cochrane Library, Preimplantation genetic diagnosis, Clinical trial, Systematic review, Medicine, Observational study, business, Intensive care medicine
Abstract

Objective To update and review the techniques and indications of preimplantation genetic diagnosis (PGD) and preimplantation genetic screening (PGS). Options Discussion about the genetic and technical aspects of preimplantation reproductive techniques, particularly those using new cytogenetic technologies and embryo-stage biopsy. Outcomes Clinical outcomes of reproductive techniques following the use of PGD and PGS are included. This update does not discuss in detail the adverse outcomes that have been recorded in association with assisted reproductive technologies. Evidence Published literature was retrieved through searches of The Cochrane Library and Medline in April 2014 using appropriate controlled vocabulary (aneuploidy, blastocyst/physiology, genetic diseases, preimplantation diagnosis/methods, fertilization in vitro) and key words (e.g., preimplantation genetic diagnosis, preimplantation genetic screening, comprehensive chromosome screening, aCGH, SNP microarray, qPCR, and embryo selection). Results were restricted to systematic reviews, randomized controlled trials/controlled clinical trials, and observational studies published from 1990 to April 2014. There were no language restrictions. Searches were updated on a regular basis and incorporated in the update to January 2015. Additional publications were identified from the bibliographies of retrieved articles. Grey (unpublished) literature was identified through searching the websites of health technology assessment and health technology-related agencies, clinical practice guideline collections, clinical trial registries, and national and international medical specialty societies. Values The quality of evidence in this document was rated using the criteria described in the Report of the Canadian Task Force on Preventive Health Care. (Table 1) Benefits, harms, and costs This update will educate readers about new preimplantation genetic concepts, directions, and technologies. The major harms and costs identified are those of assisted reproductive technologies. Summary Preimplantation genetic diagnosis is an alternative to prenatal diagnosis for the detection of genetic disorders in couples at risk of transmitting a genetic condition to their offspring. Preimplantation genetic screening is being proposed to improve the effectiveness of in vitro fertilization by screening for embryonic aneuploidy. Though FISH-based PGS showed adverse effects on IVF success, emerging evidence from new studies using comprehensive chromosome screening technology appears promising.

Published
2015

19. Facteurs génétiques à prendre en considération dans le cadre de l'examen gynécologique annuel

Author

Jo-Ann Brock, Lola Cartier, Jo-Ann Johnson, R. Douglas Wilson, François Audibert, Sylvie Langlois, Valérie Désilets, Lynn Murphy-Kaulbeck, Nanette Okun, Alain Gagnon, June C. Carroll, Melanie Pastuck, and Vyta Senikas

Subjects
Mayer rokitansky kuster hauser, Canada, Health Knowledge, Attitudes, Practice, business.industry, Genital Neoplasms, Female, Obstetrics and Gynecology, Genetic Counseling, Risk Assessment, Pedigree, Gynecology, Medicine, Humans, Female, Genetic Predisposition to Disease, Genetic Testing, Genetic risk, business, Humanities, Risk Reduction Behavior
Abstract

Resume Objectif Offrir aux medecins un survol des troubles genetiques courants qui devraient etre pris en consideration dans le cadre de l'examen gynecologique annuel d'une patiente, et ce, afin de determiner le risque que court celle-ci ou d'en venir a proceder a des examens particuliers ou a orienter la patiente vers un autre service de sous-specialite, en fonction de ses antecedents personnels ou familiaux. Options Ces renseignements d'ordre genetique peuvent etre utilises aux fins de la sensibilisation des patientes et du depistage ou du diagnostic de possibles maladies et/ou mutations. Issues L'utilisation de ces renseignements d'ordre genetique pourrait mener a l'amelioration de l'evaluation des risques et des avantages et a celle de la prise en charge dans le cadre de l'examen gynecologique annuel. Resultats Les etudes publiees en anglais, jusques et y compris en mai 2010, ont ete recuperees par l'intermediaire de recherches menees dans PubMed et la Cochrane Library au moyen d'un vocabulaire controle (« gynaecological diagnosis », « genetic inheritance ») et de mots cles (« genetic risk », « genetic mutation », « inheritance », « family history », « uterus », « ovary », « endometrial », « vagina », « colon », « gastric », « renal », « breast », « cardiac », « thrombophilia », « diabetes », « epilepsy », « leiomyomata uteri ») appropries. D'autres sources ont ete identifiees par l'intermediaire de recherches menees dans les sites Web d'organismes s'interessant a l'evaluation des technologies dans le domaine de la sante et d'organismes connexes, dans des collections de directives cliniques, dans des registres d'essais cliniques et aupres de societes de specialite medicale nationales et internationales. Valeurs Le niveau des resultats ne permet pas la formulation de recommandations factuelles. Avantages, desavantages et couts La presente opinion de comite ameliorera l'utilisation de nouvelles connaissances genetiques et leur application aux soins gynecologiques offerts annuellement aux femmes. Les occasions de gestion du risque et de diagnostic, pour ce qui est des troubles gynecologiques genetiques, s'en trouveront ameliorees. Une comprehension plus exhaustive des troubles genetiques pourrait entrainer une hausse de l'anxiete et du stress psychologique chez les femmes et les membres de leur famille. Commanditaire Societe des obstetriciens et gynecologues du Canada. Recommandations Le niveau des resultats ne permet pas la formulation de recommandations factuelles.

Published
2017

20. RETIRED: Prenatal Screening, Diagnosis, and Pregnancy Management of Fetal Neural Tube Defects

Author

R. Douglas Wilson, Francois Audibert, Jo-Ann Brock, Carla Campagnolo, June Carroll, Lola Cartier, David Chitayat, Alain Gagnon, Jo-Ann Johnson, Sylvie Langlois, W. Kim MacDonald, Lynn Murphy-Kaulbeck, Nanette Okun, Melanie Pastuck, and Vanessa Popa

Subjects
Adult, Male, Canada, medicine.medical_specialty, Pediatrics, Adolescent, MEDLINE, Cochrane Library, Ultrasonography, Prenatal, Young Adult, Pregnancy, Prenatal Diagnosis, Health care, medicine, Humans, Neural Tube Defects, Child, Intensive care medicine, medicine.diagnostic_test, business.industry, Pregnancy Outcome, Obstetrics and Gynecology, Guideline, Magnetic Resonance Imaging, Clinical trial, Systematic review, Child, Preschool, Quality of Life, Amniocentesis, Female, Observational study, alpha-Fetoproteins, business
Abstract

Objective To provide obstetrical and genetic health care practitioners with guidelines and recommendations for prenatal screening, diagnosis, and obstetrical management of fetal open and closed neural tube defects (OCNTD). Options This review includes prenatal screening and diagnostic techniques currently being used for the detection of OCNTD including maternal serum alpha fetoprotein screening, ultrasound, fetal magnetic resonance imaging, and amniocentesis. Outcomes To improve prenatal screening, diagnosis, and obstetrical management of OCNTD while taking into consideration patient care, efficacy, cost, and care procedures. Evidence Published literature was retrieved through searches of PubMed or MEDLINE, CINAHL, and The Cochrane Library in November, 2013, using appropriate controlled vocabulary and key words (e.g., prenatal screening, congenital anomalies, neural tube defects, alpha fetoprotein, ultrasound scan, magnetic resonance imaging). Results were restricted to systematic reviews, randomized control trials/controlled clinical trials, and observational studies published in English from 1977 to 2012. Searches were updated on a regular basis and incorporated in the guideline to November 30, 2013. Grey (unpublished) literature was identified through searching the websites of health technology assessment and health technology-related agencies, clinical practice guideline collections, clinical trial registries, and national and international medical specialty societies. An online survey of health care practitioners was also reviewed. Values The quality of evidence in this document was rated using the criteria described in the Report of the Canadian Task Force on Preventive Health Care (Table). Benefits, harms, and costs This review will provide health care practitioners with a better understanding of the available prenatal screening methods for OCNTD and the benefits and risks associated with each technique to allow evidenced-based decisions on OCNTD screening, diagnosis, and obstetrical management.

Published
2014

21. Beals syndrome (congenital contractural arachnodactyly): prenatal ultrasound findings and molecular analysis

Author

N. Meirowitz, D. Nanda, Nanette Okun, M. Inbar-Feigenberg, David Chitayat, and Ants Toi

Subjects
Adult, Male, musculoskeletal diseases, Proband, Marfan syndrome, Pathology, medicine.medical_specialty, Pediatrics, Contracture, Fibrillin-2, Gestational Age, Physical examination, Fibrillins, Ultrasonography, Prenatal, Diagnosis, Differential, Arachnodactyly, Prenatal ultrasound, Pregnancy, medicine, Humans, Point Mutation, Radiology, Nuclear Medicine and imaging, Congenital contractural arachnodactyly, Arthrogryposis, Arthrogryposis multiplex congenita, Radiological and Ultrasound Technology, medicine.diagnostic_test, business.industry, Microfilament Proteins, Obstetrics and Gynecology, General Medicine, medicine.disease, Reproductive Medicine, Female, Congenital contracture, Down Syndrome, business
Abstract

We report the prenatal findings in two cases of Beals syndrome. Both pregnancies presented with clinical features of arthrogryposis multiplex congenita/fetal akinesia syndrome (AMC/FAS), including clenched fists and multiple joint contractures on repeat prenatal ultrasound examinations. The first case was diagnosed as having Beals syndrome on physical examination shortly after birth and the diagnosis was confirmed by DNA analysis, shown as a point mutation in the fibrillin 2 (FBN2) gene. The second case was diagnosed with Beals syndrome following microarray analysis on amniocytes, which showed a deletion of the FBN2 gene. Although most cases with AMC/FAS carry a poor prognosis, Beals syndrome is consistent with normal cognitive development and a better prognosis. Thus, making the correct diagnosis is crucial, both pre- and postnatally, for accurate counseling and management.

Published
2014

22. RETIRED: Prenatal Invasive Procedures in Women With Hepatitis B, Hepatitis C, and/or Human Immunodeficiency Virus Infections

Author

Alain Gagnon, Gregory Davies, R. Douglas Wilson, Francois Audibert, Jo-Ann Brock, Carla Campagnolo, June Carroll, David Chitayat, Jo-Ann Johnson, William MacDonald, Lynn Murphy-Kaulbeck, Nanette Okun, and Melanie Pastuck

Subjects
Pediatrics, medicine.medical_specialty, HIV Infections, Cochrane Library, Risk Assessment, Pregnancy, Prenatal Diagnosis, medicine, Humans, Pregnancy Complications, Infectious, business.industry, Obstetrics and Gynecology, Hepatitis C, Guideline, Hepatitis B, medicine.disease, Clinical trial, Neonatal infection, Systematic review, Immunology, Amniocentesis, Female, business, Viral hepatitis
Abstract

Objective To review the risk of in utero infection through prenatal invasive procedures in women with hepatitis B, hepatitis C, and/or human immunodeficiency virus (HIV) infections. Outcomes Fetal and neonatal morbidity and mortality. Evidence Published literature was retrieved through searches of Medline, CINAHL, and the Cochrane Library using appropriate controlled vocabulary (amniocentesis, chorionic villus sampling, cordocentesis, fetal and neonatal infection) and key words (hepatitis B, hepatitis C, HIV). Results were restricted to systematic reviews, randomized control trials/controlled clinical trials, and observational studies from 2002 to 2012 published in English or French. (Studies from 1966 to 2002 were previously reviewed in Clinical Practice Guideline No. 123.) Searches were updated on a regular basis and incorporated in the guideline to February 2014. Grey (unpublished) literature was identified through searching the websites of health technology assessment and health technology-related agencies, clinical practice guideline collections, clinical trial registries, and national and international medical specialty societies. Values The quality of evidence in this document was rated using the criteria described in the Report of the Canadian Task Force on Preventive Health Care (Table).

Published
2014

23. 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

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

Subjects
Gynecology, medicine.medical_specialty, Neural tube defect, Folic acid, business.industry, Spina bifida, medicine, Obstetrics and Gynecology, medicine.disease, business
Published
2015

24. RETIRED: Investigation and Management of Non-immune Fetal Hydrops

Author

Valérie Désilets, François Audibert, R. Wilson, Francois Audibert, Jo-Ann Brock, June Carroll, Lola Cartier, Alain Gagnon, Jo-Ann Johnson, Sylvie Langlois, William MacDonald, Lynn Murphy-Kaulbeck, Nanette Okun, Melanie Pastuck, and Vyta Senikas

Subjects
Pediatrics, medicine.medical_specialty, business.industry, MEDLINE, Obstetrics and Gynecology, Guideline, Cochrane Library, medicine.disease, law.invention, Clinical trial, Systematic review, Randomized controlled trial, law, Hydrops fetalis, medicine, Observational study, business
Abstract

Objective To describe the current investigation and management of non-immune fetal hydrops, with a focus on treatable or recurring etiologies. Outcomes To provide better counselling and management in cases of prenatally diagnosed non-immune hydrops. Evidence Published literature was retrieved through searches of PubMed or MEDLINE, CINAHL, and The Cochrane Library in 2011 using key words (non-immune hydrops fetalis, fetal hydrops, fetal therapy, fetal metabolism). Results were restricted to systematic reviews, randomized controlled trials/controlled clinical trials, observational studies, and significant case reports. Additional publications were identified from the bibliographies of these articles. There were no date or language restrictions. Searches were updated on a regular basis and incorporated in the guideline to May 2012. Grey (unpublished) literature was identified through searching the websites of health technology assessment and health technology-related agencies, clinical practice guideline collections, clinical trial registries, and national and international medical specialty societies. Benefits, harms, and costs These guidelines educate readers about the causes of non-immune fetal hydrops and its prenatal counselling and management. It also provides a standardized approach to non-immune fetal hydrops, emphasizing the search for prenatally treatable conditions and recurrent genetic etiologies. Values The quality of evidence in this document was rated using the criteria described in the Report of the Canadian Task Force on Preventive Health Care (Table 1).

Published
2013

25. Clinical outcomes after assisted reproductive technology in twin pregnancies: chorionicity-based comparison

Author

Gang Zou, Nanette Okun, Tao Duan, Xing Wei, Yan Chen, Jun Zhang, and Luming Sun

Subjects
Adult, Fetal Membranes, Premature Rupture, medicine.medical_specialty, Reproductive Techniques, Assisted, medicine.medical_treatment, Cholestasis, Intrahepatic, Logistic regression, Article, 03 medical and health sciences, 0302 clinical medicine, Pregnancy, Risk Factors, medicine, Humans, 030212 general & internal medicine, Retrospective Studies, Gynecology, 030219 obstetrics & reproductive medicine, Multidisciplinary, Assisted reproductive technology, Obstetrics, business.industry, Pregnancy Outcome, Retrospective cohort study, Odds ratio, medicine.disease, Confidence interval, Pregnancy Complications, Pregnancy, Twin, Gestation, Female, business, Premature rupture of membranes
Abstract

The chorionicity–based evaluation of the perinatal risk in twin pregnancies after assisted reproductive technology (ART) is lacking. A retrospective review was performed of all twin pregnancies monitored prenatally and delivered at our hospital between 2010 and 2014. Chorionicity was diagnosed by ultrasound examination at first trimester and confirmed by postnatal pathology. Pregnancy and perinatal outcomes were prospectively recorded. Adjusted odds ratios (aOR) with 95% confidence intervals (CI) were calculated in a logistic regression model. A total of 1153 twin pregnancies were analyzed. The occurrence of preterm premature rupture of membranes (PPROM) was 3 times as frequent in monochorionic diamniotic (MCDA) twin pregnancies after ART as in those spontaneous counterparts (aOR 3.0; 95%CI 1.1–3.2). The prevalence of intrahepatic cholestasis of pregnancies (ICP) was significantly higher in dichorionic diamniotic (DCDA) twin pregnancies following ART compared to spontaneous DCDA pregnancies (aOR 3.3; 95%CI 1.3–5.6). Perinatal outcomes did not differ between two conception methods, either in MCDA or DCDA twin pregnancies. Based on differentiation of chorionicity, ART is associated with the increased risk of PPROM in MCDA twin pregnancies and with a higher rate of ICP in DCDA twin gestations. ART does not increase adversity of perinatal outcomes in twin pregnancies.

Published
2016

26. RETIRED: Counselling Considerations for Prenatal Genetic Screening

Author

Lola Cartier, Lynn Murphy-Kaulbeck, R. Douglas Wilson, François Audibert, Jo-Ann Brock, June Carroll, Alain Gagnon, Jo-Ann Johnson, Sylvie Langlois, Nanette Okun, and Melanie Pastuck

Subjects
Pregnancy, Down syndrome, medicine.medical_specialty, medicine.diagnostic_test, business.industry, Obstetrics, Genetic counseling, Obstetrics and Gynecology, Aneuploidy, Prenatal care, medicine.disease, Prenatal screening, medicine, Trisomy, business, Genetic testing
Abstract

This document has been developed to aid clinicians in counselling patients about prenatal screening and to provide assistance in counselling about both positive and negative screening results.

Published
2012

27. RETIRED: Genetic Considerations for a Woman’s Annual Gynaecological Examination

Author

R. Douglas Wilson, Sylvie Langlois, François Audibert, Jo-Ann Brock, June Carroll, Lola Cartier, Valérie A. Désilets, Alain Gagnon, Jo-Ann Johnson, Lynn Murphy-Kaulbeck, Nanette Okun, Melanie Pastuck, and Vyta Senikas

Subjects
Gynecology, medicine.medical_specialty, Referral, business.industry, Specialty, Obstetrics and Gynecology, Guideline, Evidence-based medicine, Subspecialty, Clinical trial, Family medicine, medicine, Family history, business, Patient education
Abstract

Objective To provide the physician with an overview of common genetic conditions that should be considered during a women's annual gynaecological assessment to determine the patient's risk or to initiate specific testing or referral to another subspecialty service, depending on personal or family history. Options This genetic information can be used for patient education and possible disease and/or mutation screening or diagnosis. Outcomes The use of this genetic information may allow improved risk-benefit assessment and management at the annual gynaecological examination. Evidence Studies published in English up to and including May 2010 were retrieved through searches of PubMed and the Cochrane Library, using appropriate controlled vocabulary (gynaecological diagnosis, genetic inheritance) and key words (genetic risk, genetic mutation, inheritance, family history, uterus, ovary, endometrial, vagina, colon, gastric, renal, breast, cardiac, thrombophilia, diabetes, epilepsy, leiomyomata uteri). Other literature sources were identified through searching the web sites of health technology assessment and health technology assessment-related agencies, clinical practice guideline collections, clinical trial registries, and national and international medical specialty societies. Values The levels of evidence are not adequate for evidence-based recommendations to be made. Benefits, harms, and costs This committee opinion will enhance the use of new genetic knowledge and its application to the annual gynaecological care of women. Risk management and diagnostic opportunities for genetic gynaecological conditions will be improved. A more complete understanding of genetic conditions may increase anxiety and psychological stress for women and their families. Sponsors Society of Obstetricians and Gynaecologists of Canada.

Published
2012

28. Delayed Child-Bearing

Author

Valérie Désilets, Alain Gagnon, François Audibert, Suzanne Tough, Lola Cartier, Lynn Murphy-Kaulbeck, Jo-Ann Johnson, Jo-Ann BrockS, Nanette Okun, Sylvie Langlois, Claire Blight, and R. Douglas Wilson

Subjects
Adult, Male, Canada, medicine.medical_specialty, Reproductive Techniques, Assisted, medicine.medical_treatment, media_common.quotation_subject, Reproductive Behavior, Fertility, Reproductive technology, Paternal Age, Pregnancy, Risk Factors, Health care, medicine, Humans, Caesarean section, media_common, Assisted reproductive technology, business.industry, Obstetrics, Incidence, Pregnancy Outcome, Obstetrics and Gynecology, Guideline, Middle Aged, medicine.disease, Low birth weight, Female, medicine.symptom, business, Maternal Age
Abstract

To provide an overview of delayed child-bearing and to describe the implications for women and health care providers.Delayed child-bearing, which has increased greatly in recent decades, is associated with an increased risk of infertility, pregnancy complications, and adverse pregnancy outcome. This guideline provides information that will optimize the counselling and care of Canadian women with respect to their reproductive choices.Maternal age is the most important determinant of fertility, and obstetric and perinatal risks increase with maternal age. Many women are unaware of the success rates or limitations of assisted reproductive technology and of the increased medical risks of delayed child-bearing, including multiple births, preterm delivery, stillbirth, and Caesarean section. This guideline provides a framework to address these issues.Studies published between 2000 and August 2010 were retrieved through searches of PubMed and the Cochrane Library using appropriate key words (delayed child-bearing, deferred pregnancy, maternal age, assisted reproductive technology, infertility, and multiple births) and MeSH terms (maternal age, reproductive behaviour, fertility). The Internet was also searched using similar key words, and national and international medical specialty societies were searched for clinical practice guidelines and position statements. Data were extracted based on the aims, sample, authors, year, and results.The quality of evidence was rated using the criteria described in the Report of the Canadian Task Force on Preventive Health Care (Table 1).The Society of Obstetricians and Gynaecologists of Canada. RECOMMENDATIONS 1. Women who delay child-bearing are at increased risk of infertility. Prospective parents, especially women, should know that their fecundity and fertility begin to decline significantly after 32 years of age. Prospective parents should know that assisted reproductive technologies cannot guarantee a live birth or completely compensate for age-related decline in fertility. (II-2A) 2. A fertility evaluation should be initiated after 6 months of unprotected intercourse without conception in women 35 to 37 years of age, and earlier in women37 years of age. (II-2A) 3. Prospective parents should be informed that semen quality and male fertility deteriorate with advancing age and that the risk of genetic disorders in offspring increases. (II-2A) 4. Women ≥ 35 years of age should be offered screening for fetal aneuploidy and undergo a detailed second trimester ultrasound examination to look for significant fetal birth defects (particularly cardiac defects). (II-1A) 5. Delayed child-bearing is associated with increased obstetrical and perinatal complications. Care providers need to be aware of these complications and adjust obstetrical management protocols to ensure optimal maternal and perinatal outcomes. (II-2A) 6. All adults of reproductive age should be aware of the obstetrical and perinatal risks of advanced maternal age so they can make informed decisions about the timing of child-bearing. (II-2A) 7. Strategies to improve informed decision-making by prospective parents should be designed, implemented, and evaluated. These strategies should provide opportunity for adults to understand the potential medical, social, and economic consequences of child-bearing throughout the reproductive years. (III-B) 8. Barriers to healthy reproduction, including workplace policies, should be reviewed to optimize the likelihood of healthy pregnancies. (III-C).

Published
2012

29. RETIRED: Use of Array Genomic Hybridization Technology in Prenatal Diagnosis in Canada

Author

Alessandra Duncan, Sylvie Langlois, R. Douglas Wilson, François Audibert, Jo-Ann Brock, June Carroll, Lola Cartier, Alain Gagnon, Jo-Ann Johnson, Lynn Murphy-Kaulbeck, Nanette Okun, Melanie Pastuck, David Chitayat, Isabelle DeBie, Suzanne Demczuk, Valérie A. Désilets, Michael T. Geraghty, Janet Marcadier, Tanya N. Nelson, Vicky Siu, and David Skidmore

Subjects
Genetics, medicine.medical_specialty, business.industry, MEDLINE, Obstetrics and Gynecology, Prenatal diagnosis, Guideline, Clinical trial, Systematic review, Family medicine, Medicine, Copy-number variation, Advanced maternal age, business, Comparative genomic hybridization
Abstract

Objective To summarize for obstetrical care providers the current literature on array genomic hybridization in prenatal diagnosis and to outline the recommendations of the Canadian College of Medical Geneticists regarding the use of this new technology with respect to prenatal diagnosis. Evidence PubMed and Medline were searched for articles published in English between 2004 and 2010, using the key words DNA QF-PCR, quantitative fluorescent polymerase chain reaction, fetal chromosomal abnormalities, prenatal diagnosis, array genomic hybridization, fetal structural anomalies, and copy number variants Results were restricted to systematic reviews, randomized control trials/controlled clinical trials, and observational studies. Searches were updated on a regular basis, and articles were incorporated in the guideline to September 2011. Grey (unpublished) literature was identified through searching the websites of health technology assessment and health technology assessment-related agencies, clinical practice guideline collections, clinical trial registries, and national and international medical specialty societies. Values The quality of evidence in this document was rated using the criteria described in the Report of the Canadian Task Force on Preventive Health Care (Table 1). Recommendations 1.Array genomic hybridization is not recommended in pregnancies at low risk for a structural chromosomal abnormality; for example, advanced maternal age, positive maternal serum screen, previous trisomy, or the presence of "soft markers" on fetal ultrasound. (III-D) 2.Array genomic hybridization may be an appropriate diagnostic test in cases with fetal structural abnormalities detected on ultrasound or fetal magnetic resonance imaging; it could be done in lieu of a karyotype if rapid aneuploidy screening is negative and an appropriate turnaround time for results is assured. (II-2A) 3.Any pregnant woman who qualifies for microarray genomic hybridization testing should be seen in consultation by a medical geneticist before testing so that the benefits, limitations, and possible outcomes of the analysis can be discussed in detail. The difficulties of interpreting some copy number variants should also be discussed. This will allow couples to make an informed decision about whether or not they wish to pursue such prenatal testing. (III-A)

Published
2011

30. RETIRED: Fetal and Perinatal Autopsy in Prenatally Diagnosed Fetal Abnormalities With Normal Karyotype

Author

Valérie Désilets, Luc Laurier Oligny, R. Douglas Wilson, Victoria M. Allen, François Audibert, Claire Blight, Jo-Ann Brock, June Carroll, Lola Cartier, Alain Gagnon, Jo-Ann Johnson, Sylvie Langlois, Lynn Murphy-Kaulbeck, Nanette Okun, Melanie Pastuck, Donna Gilmour, Douglas Bell, George Carson, Owen Hughes, Caroline Le Jour, Dean Leduc, Nicholas Leyland, Paul Martyn, André Masse, Wendy Wolfman, William Ehman, Anne Biringer, Andrée Gagnon, Lisa Graves, Jonathan Hey, Jill Konkin, Francine Léger, and Cindy Marshall

Subjects
medicine.medical_specialty, business.industry, Obstetrics, MEDLINE, Obstetrics and Gynecology, Prenatal diagnosis, Guideline, Cochrane Library, law.invention, Surgery, Clinical trial, Systematic review, Randomized controlled trial, law, Medicine, Observational study, business
Abstract

Objective To review the information on fetal and perinatal autopsies, the process of obtaining consent, and the alternative informationgathering options following a prenatal diagnosis of nonchromosomal malformations, and to assist clinicians in providing postnatal counselling regarding fetal diagnosis and recurrence risks. Outcomes To provide better counselling about fetal and perinatal autopsies for women and families who are dealing with a prenatally diagnosed non-chromosomal fetal anomaly. Evidence Published literature was retrieved through searches of PubMed or Medline, CINAHL, and The Cochrane Library in 2009 and 2010, using appropriate key words (fetal autopsy, postmortem, autopsy, perinatal postmortem examination, autopsy protocol, postmortem magnetic resonance imaging, autopsy consent, tissue retention, autopsy evaluation). Results were restricted to systematic reviews, randomized controlled trials/controlled clinical trials, and observational studies. Additional publications were identified from the bibliographies of these articles. There were no date or language restrictions. Grey (unpublished) literature was identified through searching the websites of health technology assessment and health technology assessment-related agencies, clinical practice guideline collections, clinical trial registries, and national and international medical specialty societies. Benefits, harms, and costs This update educates readers about (1) the benefits of a fetal perinatal autopsy, (2) the consent process, and (3) the alternatives when the family declines autopsy. It also provides a standardized approach to fetal and perinatal autopsies, emphasizing pertinent additional sampling when indicated. Values The quality of evidence was rated using the criteria described in the Report of the Canadian Task Force on Preventive Health Care (Table 1).

Published
2011

31. Prenatal Screening for Fetal Aneuploidy in Singleton Pregnancies

Author

David Chitayat, Sylvie Langlois, R. Douglas Wilson, François Audibert, Claire Blight, Jo-Ann Brock, Lola Cartier, June Carroll, Valerie A. Désilets, Alain Gagnon, Jo-Ann Johnson, Lynn Murphy-Kaulbeck, Nanette Okun, Melanie Pastuck, Vyta Senikas, Isabelle DeBie, Suzanne Demczuk, Michael T Geraghty, Janet Marcadier, Tanya N. Nelson, David Skidmore, and Vicky Siu

Subjects
Adult, Canada, medicine.medical_specialty, Down syndrome, Pregnancy-associated plasma protein A, Aneuploidy, Gestational Age, Trisomy, Prenatal diagnosis, Ultrasonography, Prenatal, Pregnancy, Risk Factors, Prenatal Diagnosis, medicine, Humans, Pregnancy-Associated Plasma Protein-A, Chorionic Gonadotropin, beta Subunit, Human, Genetic Testing, Randomized Controlled Trials as Topic, Gynecology, Obstetrics, business.industry, Singleton, Obstetrics and Gynecology, Gestational age, medicine.disease, Review Literature as Topic, Female, alpha-Fetoproteins, Down Syndrome, Chromosomes, Human, Pair 18, Nuchal Translucency Measurement, business, Biomarkers, Maternal Age
Abstract

To develop a Canadian consensus document on maternal screening for fetal aneuploidy (e.g., Down syndrome and trisomy 18) in singleton pregnancies.Pregnancy screening for fetal aneuploidy started in the mid 1960s, using maternal age as the screening test. New developments in maternal serum and ultrasound screening have made it possible to offer all pregnant patients a non-invasive screening test to assess their risk of having a fetus with aneuploidy to determine whether invasive prenatal diagnostic testing is necessary. This document reviews the options available for non-invasive screening and makes recommendations for Canadian patients and health care workers.To offer non-invasive screening for fetal aneuploidy (trisomy 13, 18, 21) to all pregnant women. Invasive prenatal diagnosis would be offered to women who screen above a set risk cut-off level on non-invasive screening or to pregnant women whose personal, obstetrical, or family history places them at increased risk. Currently available non-invasive screening options include maternal age combined with one of the following: (1) first trimester screening (nuchal translucency, maternal age, and maternal serum biochemical markers), (2) second trimester serum screening (maternal age and maternal serum biochemical markers), or (3) 2-step integrated screening, which includes first and second trimester serum screening with or without nuchal translucency (integrated prenatal screen, serum integrated prenatal screening, contingent, and sequential). These options are reviewed, and recommendations are made.Studies published between 1982 and 2009 were retrieved through searches of PubMed or Medline and CINAHL and the Cochrane Library, using appropriate controlled vocabulary and key words (aneuploidy, Down syndrome, trisomy, prenatal screening, genetic health risk, genetic health surveillance, prenatal diagnosis). Results were restricted to systematic reviews, randomized controlled trials, and relevant observational studies. There were no language restrictions. Searches were updated on a regular basis and incorporated in the guideline to August 2010. Grey (unpublished) literature was identified through searching the websites of health technology assessment and health technology assessment-related agencies, clinical practice guideline collections, clinical trial registries, and national and international medical specialty societies. The previous Society of Obstetricians and Gynaecologists of Canada guidelines regarding prenatal screening were also reviewed in developing this clinical practice guideline.The quality of evidence was rated using the criteria described in the Report of the Canadian Task Force on Preventive Health Care.This guideline is intended to reduce the number of prenatal invasive procedures done when maternal age is the only indication. This will have the benefit of reducing the numbers of normal pregnancies lost because of complications of invasive procedures. Any screening test has an inherent false-positive rate, which may result in undue anxiety. It is not possible at this time to undertake a detailed cost-benefit analysis of the implementation of this guideline, since this would require health surveillance and research and health resources not presently available; however, these factors need to be evaluated in a prospective approach by provincial and territorial initiatives. RECOMMENDATIONS 1. All pregnant women in Canada, regardless of age, should be offered, through an informed counselling process, the option of a prenatal screening test for the most common clinically significant fetal aneuploidies in addition to a second trimester ultrasound for dating, assessment of fetal anatomy, and detection of multiples. (I-A) 2. Counselling must be non-directive and must respect a woman's right to accept or decline any or all of the testing or options offered at any point in the process. (III-A) 3. Maternal age alone is a poor minimum standard for prenatal screening for aneuploidy, and it should not be used a basis for recommending invasive testing when non-invasive prenatal screening for aneuploidy is available. (II-2A) 4. Invasive prenatal diagnosis for cytogenetic analysis should not be performed without multiple marker screening results except for women who are at increased risk of fetal aneuploidy (a) because of ultrasound findings, (b) because the pregnancy was conceived by in vitro fertilization with intracytoplasmic sperm injection, or (c) because the woman or her partner has a history of a previous child or fetus with a chromosomal abnormality or is a carrier of a chromosome rearrangement that increases the risk of having a fetus with a chromosomal abnormality. (II-2E) 5. At minimum, any prenatal screen offered to Canadian women who present for care in the first trimester should have a detection rate of 75% with no more than a 3% false-positive rate. The performance of the screen should be substantiated by annual audit. (III-B) 6. The minimum standard for women presenting in the second trimester should be a screen that has a detection rate of 75% with no more than a 5% false-positive rate. The performance of the screen should be substantiated by annual audit. (III-B) 7. First trimester nuchal translucency should be interpreted for risk assessment only when measured by sonographers or sonologists trained and accredited for this service and when there is ongoing quality assurance (II-2A), and it should not be offered as a screen without biochemical markers in singleton pregnancies. (I-E) 8. Evaluation of the fetal nasal bone in the first trimester should not be incorporated as a screen unless it is performed by sonographers or sonologists trained and accredited for this service and there is ongoing quality assurance. (II-2E) 9. For women who undertake first trimester screening, second trimester serum alpha fetoprotein screening and/or ultrasound examination is recommended to screen for open neural tube defects. (II-1A) 10. Timely referral and access is critical for women and should be facilitated to ensure women are able to undergo the type of screening test they have chosen as first trimester screening. The first steps of integrated screening (with or without nuchal translucency), contingent, or sequential screening are performed in an early and relatively narrow time window. (II-1A) 11. Ultrasound dating should be performed if menstrual or conception dating is unreliable. For any abnormal serum screen calculated on the basis of menstrual dating, an ultrasound should be done to confirm gestational age. (II-1A) 12. The presence or absence of soft markers or anomalies in the 18- to 20-week ultrasound can be used to modify the a priori risk of aneuploidy established by age or prior screening. (II-2B) 13. Information such as gestational dating, maternal weight, ethnicity, insulin-dependent diabetes mellitus, and use of assisted reproduction technologies should be provided to the laboratory to improve accuracy of testing. (II-2A) 14. Health care providers should be aware of the screening modalities available in their province or territory. (III-B) 15. A reliable system needs to be in place ensuring timely reporting of results. (III-C) 16. Screening programs should be implemented with resources that support audited screening and diagnostic laboratory services, ultrasound, genetic counselling services, patient and health care provider education, and high quality diagnostic testing, as well as resources for administration, annual clinical audit, and data management. In addition, there must be the flexibility and funding to adjust the program to new technology and protocols. (II-3B).

Published
2011

32. Prenatal Screening for and Diagnosis of Aneuploidy in Twin Pregnancies

Author

François Audibert, Alain Gagnon, R. Douglas Wilson, Claire Blight, Jo-Ann Brock, Lola Cartier, Valerie A. Désilets, Jo-Ann Johnson, Sylvie Langlois, Lynn Murphy-Kaulbeck, Nanette Okun, Melanie Pastuck, Vyta Senikas, David Chitayat, Michael T. Geraghty, Janet Marcadier, Tanya N. Nelson, David Skidmore, Vicky Siu, and Frederique Tihy

Subjects
Down syndrome, medicine.medical_specialty, medicine.diagnostic_test, business.industry, Obstetrics, Obstetrics and Gynecology, Chorionic villus sampling, Aneuploidy, Prenatal diagnosis, medicine.disease, Prenatal screening, medicine, Amniocentesis, business, Trisomy, Twin Pregnancy
Abstract

Objective To provide a Canadian consensus document with recommendations on prenatal screening for and diagnosis of fetal aneuploidy (e.g., Down syndrome and trisomy 18) in twin pregnancies.

Published
2011

33. Échographie et grossesse gémellaire

Author

Lucie Morin, Kenneth Lim, Stephen Bly, Kimberly Butt, Yvonne M. Cargill, Gregory Davies, Nanette Denis, Robert Gagnon, Marja Anne Hietala-Coyle, Annie Ouellet, Shia Salem, Vyta Senikas, Jon Barrett, R. Douglas Wilson, François Audibert, Jo-Ann Brock, June Carroll, Lola Cartier, Alain Gagnon, Jo-Ann Johnson, Sylvie Langlois, Lynn Murphy-Kaulbeck, Nanette Okun, Melanie Pastuck, Lynda Hudon, Melanie Basso, Hayley Bos, Joan M. Crane, Marie-France Delisle, Savas Menticoglou, William Mundle, Tracy Pressey, Christy Pylypjuk, Anne Roggensack, and Frank Sanderson

Subjects
business.industry, Obstetrics and Gynecology, Medicine, business, Humanities
Abstract

Resume Objectif Analyser la litterature portant sur l'utilisation de l'echographie diagnostique dans la prise en charge des grossesses gemellaires. Formuler des recommandations quant a la meilleure facon d'utiliser l'echographie dans les cas de grossesse gemellaire. Issues Baisse des taux de mortalite et de morbidite perinatales, ainsi que des taux de morbidite neonatale a court et a long terme, dans les cas de grossesse gemellaire. Optimisation du recours a l'echographie dans les cas de grossesse gemellaire. Resultats La litterature publiee a ete recuperee par l'intermediaire de recherches menees dans PubMed et The Cochrane Library, en 2008 et en 2009, au moyen d'un vocabulaire controle (p. ex. « twin », « ultrasound », « cervix », « prematurity ») et de mots cles (p. ex. « acardiac », « twin », « reversed arterial perfusion », « twin-to-twin transfusion syndrome », « amniotic fluid ») adequats. Les resultats ont ete restreints aux analyses systematiques, aux essais comparatifs randomises / essais cliniques comparatifs et aux etudes observationnelles. Aucune restriction n'a ete imposee en matiere de date. Les etudes ont ete restreintes a celles qui disposaient d'un resume ou d'un texte en francais ou en anglais. Les recherches ont ete mises a jour de facon reguliere et integrees a la directive clinique jusqu'en septembre 2009. La litterature grise (non publiee) a ete identifiee par l'intermediaire de recherches menees dans les sites Web d'organismes s'interessant a l'evaluation des technologies dans le domaine de la sante et d'organismes connexes, dans des collections de directives cliniques, dans des registres d'essais cliniques et aupres de societes de specialite medicale nationales et internationales. Valeurs Les donnees recueillies ont ete analysees par le comite d'imagerie diagnostique de la Societe des obstetriciens et gynecologues du Canada, avec l'apport des membres du comite de medecine fœto-maternelle et du comite de genetique de la SOGC. Les recommandations ont ete formulees conformement aux lignes directrices elaborees par le Groupe d'etude canadien sur les soins de sante preventifs (Tableau 1). Avantages, desavantages et couts La facilitation et l'optimisation du recours a l'echographie dans les cas de grossesse gemellaire constituent les avantages auxquels l'on s'attend de la presente directive clinique.

Published
2011

34. RETIRED: Genetic Considerations for a Woman’s Pre-conception Evaluation

Author

R. Douglas Wilson, François Audibert, Jo-Ann Brock, Lola Cartier, Valerie A. Désilets, Alain Gagnon, Jo-Ann Johnson, Sylvie Langlois, Lynn Murphy-Kaulbeck, Nanette Okun, and Melanie Pastuck

Subjects
medicine.medical_specialty, business.industry, Genetic counseling, Specialty, MEDLINE, Obstetrics and Gynecology, Health technology, Prenatal diagnosis, Disease, Family medicine, Health care, medicine, Psychiatry, business, Patient education
Abstract

Objective To give health care providers information about the genetic information that can be used as part of health surveillance for women undergoing a pre-conception evaluation for genetic risk assessment and possible genetic screening or testing. Options This genetic information can be used for patient education and possible prenatal testing. Outcomes The use of this genetic information may allow improved risk-benefit assessment for pre-conception counselling for individual patients and their families. Evidence PubMed or Medline and the Cochrane Database were searched in November 2009, using appropriate key words (preconception, genetic disease, maternal, family history, genetic health risk, genetic health surveillance, prenatal screening, prenatal diagnosis, birth defects, and teratogen). Grey (unpublished) literature was identified through searching the websites of health technology assessment and health technology assessment-related agencies, clinical practice guideline collections, and national and international medical specialty societies. Benefits, harms, and costs The benefits for the patient and her family include understanding of possible genetic risk and enhanced pregnancy outcomes. The harm includes increased anxiety or psychological stress associated with the possibility of identifying genetic risks. Validation The evidence obtained was reviewed by the Genetics Committee of the Society of Obstetricians and Gynaecologists of Canada.

Published
2011

35. Archivée: Considérations génétiques pour ce qui est de l’évaluation préconceptionnelle chez la femme

Author

R. Douglas Wilson, François Audibert, Jo-Ann Brock, Lola Cartier, Valérie A. Désilets, Alain Gagnon, Jo-Ann Johnson, Sylvie Langlois, Lynn Murphy-Kaulbeck, Nanette Okun, and Melanie Pastuck

Subjects
Gynecology, medicine.medical_specialty, Prenatal screening, business.industry, Obstetrics and Gynecology, Medicine, business
Abstract

Resume Objectif Offrir aux fournisseurs de soins de sante des renseignements au sujet des donnees genetiques qui peuvent etre utilisees dans le cadre de la surveillance de la sante pour les femmes qui subissent une evaluation preconceptionnelle visant a determiner le risque genetique et la possibilite de proceder a un depistage ou a des tests genetiques. Options Ces donnees genetiques peuvent etre utilisees aux fins de la sensibilisation des patientes et du depistage prenatal potentiel. Issues L'utilisation de ces donnees genetiques pourrait permettre l'amelioration de l'evaluation des risques et des avantages pour ce qui est du counseling preconceptionnel a l'intention des patientes et de leur famille. Resultats Des recherches ont ete menees dans PubMed ou Medline et la base de donnees Cochrane en novembre 2009, au moyen de mots cles appropries (« pre-conception », « genetic disease », « maternal, family history », « genetic health risk », « genetic health surveillance », « prenatal screening », « prenatal diagnosis », « birth defects » et « teratogen »). La litterature grise (non publiee) a ete identifiee par l'intermediaire de recherches menees dans les sites Web d'organismes s'interessant a l'evaluation des technologies dans le domaine de la sante et d'organismes connexes, dans des collections de directives cliniques, dans des registres d'essais cliniques et aupres de societes de specialite medicale nationales et internationales. Avantages, desavantages et couts Parmi les avantages pour la patiente et sa famille, on trouve la comprehension d'un possible risque genetique et l'obtention de meilleures issues de grossesse. Parmi les desavantages, on trouve une hausse de l'anxiete ou du stress psychologique associe a la possibilite d'identifier des risques genetiques. Validation Les resultats obtenus ont ete analyses par le comite de genetique de la Societe des obstetriciens et gynecologues du Canada.

Published
2011

37. Placental size and the prediction of severe early-onset intrauterine growth restriction in women with low pregnancy-associated plasma protein-A

Author

Gordon C. S. Smith, David Chitayat, L. K. Proctor, Nanette Okun, Sarah Keating, John Kingdom, Rory Windrim, and Meghana Toal

Subjects
Gynecology, Pregnancy, medicine.medical_specialty, Radiological and Ultrasound Technology, Pregnancy-associated plasma protein A, business.industry, Obstetrics, Obstetrics and Gynecology, Intrauterine growth restriction, General Medicine, Placental insufficiency, medicine.disease, Reproductive Medicine, Premature birth, medicine.artery, Medicine, Small for gestational age, Gestation, Radiology, Nuclear Medicine and imaging, business, Uterine artery
Abstract

Objectives Screening studies for trisomy 21 demonstrate that low maternal serum pregnancy-associated plasma protein-A (PAPP-A) at 11–13 weeks’ gestation is associated with stillbirth, intrauterine growth restriction (IUGR) and pre-eclampsia in chromosomally normal fetuses. However, the strength of these associations is too weak to justify screening for these placental insufficiency syndromes. Our objective was to evaluate placental size and uterine artery (UtA) Doppler imaging as second-stage screening tests for women with low PAPP-A. Methods We prospectively studied 90 normal singleton pregnancies with first-trimester PAPP-A ≤ 0.30 multiples of the median. Maternal serum α-fetoprotein (AFP) at 15–18 weeks’ gestation, and second-trimester placental size and UtA Doppler indices were assessed as predictors of pregnancy outcome. Results The risks of IUGR, preterm delivery before 32 weeks’ gestation and stillbirth were significantly associated with small placental size (relative risk (RR), 3.96; 95% CI, 2.21–5.98; RR, 3.96; 95% CI, 2.21–5.98; and RR, 6.44, 95% CI, 2.74–14.54, respectively) and elevated AFP (RR, 3.67; 95% CI, 1.78–7.71; RR, 2.48; 95% CI, 1.23–4.94; and RR, 5.14; 95% CI, 1.66–16.85, respectively), but not with abnormal UtA Doppler indices. The combination of elevated AFP and small placental size further increased the risk of IUGR (RR, 4.88; 95% CI, 2.88–5.31), delivery before 32 weeks’ gestation (RR, 4.25; 95% CI, 2.38–4.98) and stillbirth (RR, 7.44; 95% CI, 3.04–3.75). Conclusions Small placental size and elevated AFP, but not UtA Doppler indices, identify women with low PAPPA at high risk of IUGR, extreme preterm delivery and stillbirth. These additional screening tests may directly improve perinatal outcomes in women with low PAPP-A. Copyright  2009 ISUOG. Published by John Wiley & Sons, Ltd.

Published
2009

38. Screening for Placental Insufficiency in High-risk Pregnancies: Is Earlier Better?

Author

Nanette Okun, Jodie M Dodd, John Kingdom, S.L. Costa, Rory Windrim, L. K. Proctor, J.-A. Johnson, and Meghana Toal

Subjects
Adult, medicine.medical_specialty, HELLP syndrome, Placenta, Intrauterine growth restriction, Pilot Projects, Placental insufficiency, Young Adult, Predictive Value of Tests, Pregnancy, Risk Factors, medicine, Humans, Mass Screening, Prospective Studies, Prospective cohort study, Gynecology, business.industry, Obstetrics, Uterine artery doppler, Obstetrics and Gynecology, Ultrasonography, Doppler, Arteries, Middle Aged, Placental Insufficiency, medicine.disease, Pregnancy Trimester, First, Early Diagnosis, Reproductive Medicine, Pregnancy Trimester, Second, Gestation, Female, business, Alpha-fetoprotein, Developmental Biology
Abstract

To compare a profile of placental function between the first and second trimesters in pregnancies at high risk of adverse perinatal outcomes attributable to placental insufficiency.Prospective cohort study in 61 singleton pregnancies. Uterine artery Doppler and placental morphology (shape and texture) were determined at 11-13(+6) weeks and at 18-23(+6) weeks. First trimester (pregnancy-associated placental protein-A [PAPP-A]) and second trimester (total hCG and alpha fetoprotein [AFP]) serum biochemistry were determined. The two screening periods were compared for the prediction of a range of severe adverse perinatal outcomes (intrauterine growth restriction [IUGR], abruption, severe pre-eclampsia/HELLP syndrome, delivery32 weeks, or stillbirth).Adverse perinatal outcomes occurred in 14 (23%) women; 3 (4.9%) losses20 weeks, 2 (3.3%) stillbirths20 weeks, 4 (6.6%) IUGR, 7 (11.5%) severe pre-eclampsia/HELLP syndrome, and 10 (16.4%) deliveries32 weeks. Abnormal second trimester placental morphology was significantly associated with adverse outcome [+LR: 3.6, 95% CI: 1.3-8.5; -LR: 0.63, 95% CI: 0.36-0.93; p=0.025], as wasor = 1 abnormal second trimester tests [+LR: 5.9, 95% CI: 1.6-24; -LR: 0.68, 95% CI: 0.59-0.89; p=0.005] oror = 2 abnormal second trimester tests [+LR: 3.6, 95% CI: 1.3-7.7; -LR: 0.58, 95% CI: 0.27-0.94; p=0.035]. No combination of first trimester tests significantly predicted severe adverse perinatal outcomes. A study sample size of 822 women with similar high-risk characteristics would be needed in order to refute the conclusion that present methods of first trimester screening are not inferior to second trimester screening for severe placental insufficiency (p=0.05, power 80%, z-test).In clinically high-risk pregnancies, prediction of adverse perinatal outcomes using placental function testing is more effective in the second compared with the first trimester.

Published
2008

39. Breech Presentation: a Random Event 01 an Explainable Phenomenon?

Author

Nanette Okun and Doreen J. Bartlett

Subjects
Developmental Neuroscience, business.industry, Breech presentation, Phenomenon, Pediatrics, Perinatology and Child Health, MEDLINE, Medicine, Random event, Neurology (clinical), Medical emergency, business, medicine.disease, Social psychology
Published
2008

40. Resistance exercise decreases the need for insulin in overweight women with gestational diabetes mellitus

Author

Bryan F. Mitchell, Gabrielle N Brankston, Nanette Okun, and Edmond A. Ryan

Subjects
Adult, medicine.medical_specialty, Weight Lifting, medicine.medical_treatment, Physical exercise, Overweight, Pregnancy, Diabetes mellitus, Internal medicine, Diabetes Mellitus, medicine, Humans, Hypoglycemic Agents, Insulin, Obesity, Dose-Response Relationship, Drug, business.industry, Obstetrics and Gynecology, medicine.disease, Exercise Therapy, Gestational diabetes, Diabetes, Gestational, Endocrinology, Female, medicine.symptom, business, Body mass index
Abstract

This study examines the effects of circuit-type resistance training on the need for insulin in women with gestational diabetes mellitus.Thirty-two patients with gestational diabetes mellitus were randomly assigned either to a group that was treated with diet alone or to a group that was treated with diet plus resistance exercise.The number of women whose condition required insulin therapy was the same, regardless of treatment. However, a subgroup analysis that examined only overweight women (prepregnant body mass index,25 kg/m(2)) showed a lower incidence of insulin use in the diet-plus-exercise group (P.05). Women in the diet-plus-exercise group were prescribed less insulin (P.05) and showed a longer delay from diagnosis to the initiation of insulin therapy (P.05), compared with the diet-alone group.Resistance exercise training may help to avoid insulin therapy for overweight women with gestational diabetes mellitus.

Published
2004

41. Archivée: Autopsies foetales et périnatales dans les cas d’anomalies foetales diagnostiquées avant la naissance en présence d’un caryotype normal

Author

Valérie Désilets, Luc Laurier Oligny, R. Douglas Wilson, Victoria M. Allen, François Audibert, Claire Blight, Jo-Ann Brock, Lola Cartier, June Carroll, Alain Gagnon, Jo-Ann Johnson, Sylvie Langlois, Lynn Murphy-Kaulbeck, Nanette Okun, Melanie Pastuck, Donna Gilmour, Douglas Bell, George Carson, Owen Hughes, Caroline Le Jour, Dean Leduc, Nicholas Leyland, Paul Martyn, André Masse, Wendy Wolfman, William Ehman, Anne Biringer, Andrée Gagnon, Lisa Graves, Jonathan Hey, Jill Konkin, Francine Léger, and Cindy Marshall

Subjects
Perinatal autopsy, business.industry, Obstetrics and Gynecology, Medicine, business, Humanities
Abstract

Resume Objectif Analyser les donnees au sujet des autopsies foetales et perinatales, le processus d'obtention du consentement et les autres options de collecte de donnees a la suite d'un diagnostic prenatal de malformations non chromosomiques, ainsi qu'aider les cliniciens a offrir des services de counseling postnatal a propos du diagnostic foetal et des risques de recurrence.Criteres d'evaluation des resultats et de classifcation des recommandations, fondes sur ceux du Groupe d'etude canadien sur les soins de sante preventifsNiveaux de resultats*Categories de recommandations† I:Resultats obtenus dans le cadre d'au moins un essai comparatif convenablement randomise II-1:Resultats obtenus dans le cadre d'essais comparatifs non randomises bien concus II-2:Resultats obtenus dans le cadre d'etudes de cohortes (prospectives ou retrospectives) ou d'etudes analytiques cas-temoins bien concues, realisees de preference dans plus d'un centre ou par plus d'un groupe de recherche II-3:Resultats decoulant de comparaisons entre differents moments ou differents lieux, ou selon qu'on a ou non recours a une intervention Des resultats de premiere importance obtenus dans le cadre d'etudes non comparatives (par exemple, les resultats du traitement a la penicilline, dans les annees 1940) pourraient en outre fgurer dans cette categorie III:Opinions exprimees par des sommites dans le domaine, fondees sur l'experience clinique, etudes descriptives ou rapports de comites d'experts A.On dispose de donnees suffsantes pour appuyer la mesure clinique de prevention B.On dispose de donnees acceptables pour appuyer la mesure clinique de prevention C.Les donnees existantes sont contradictoires et ne permettent pas de formuler une recommandation pour ou contre l'usage de la mesure clinique de prevention; cependant, d'autres facteurs peuvent infuer sur la prise de decision D.On dispose de donnees acceptables pour deconseiller la mesure clinique de prevention E.On dispose de donnees suffsantes pour deconseiller la mesure clinique de prevention F.Les donnees sont insuffsantes (d'un point de vue qantitatif ou qualitatif) et ne permettent pas de formuler une recommandation; cependant, d'autres facteurs peuvent infuer sur la prise de decision Woolf SH, Battista RN, Angerson GM, Logan AG, Eel W « Canadian Task Force on Preventive Health Care New grades for recommendations from the Canadian Task Force on Preventive Health Care », CMAJ, vol 169, 2003, p 207–8*La qualite des resultats signales dans les presentes directives cliniques a ete etablie conformement aux criteres d'evaluation des resultats presentes dans le Rapport du Groupe d'etude canadien sur les soins de sante preventifs†Les recommandations que comprennent les presentes directives cliniques ont ete classees conformement a la methode de classifcation decrite dans le Rapport du Groupe d'etude canadien sur les soins de sante preventif Issues Mieux conseiller les patientes et leur famille qui font face a un diagnostic prenatal d'anomalie foetale non chromosomique au sujet des autopsies foetales et perinatales. Resultats La litterature publiee a ete recuperee par l'intermediaire de recherches menees dans PubMed ou MEDLINE, CINAHL et The Cochrane Library en 2009 et en 2010, au moyen de mots cles adequats (« fetal autopsy », « postmortem », « autopsy », « perinatal postmortem examination », « autopsy protocol », « postmortem magnetic resonance imaging », « autopsy consent », « tissue retention », « autopsy evaluation »). Les resultats ont ete restreints aux analyses systematiques, aux essais comparatifs randomises / essais cliniques comparatifs et aux etudes observationnelles. Des publications additionnelles ont ete identifiees a partir des bibliographies de ces articles. Aucune restriction n'a ete imposee en matiere de date ou de langue. La litterature grise (non publiee) a ete identifiee par l'intermediaire de recherches menees dans les sites Web d'organismes s'interessant a l'evaluation des technologies dans le domaine de la sante et d'organismes connexes, dans des collections de directives cliniques, dans des registres d'essais cliniques et aupres de societes de specialite medicale nationales et internationales. Avantages, desavantages et couts La presente mise a jour renseigne les lecteurs au sujet (1) des avantages de la tenue d'une autopsie foetale ou perinatale, (2) du processus de consentement et (3) des solutions de rechange face au refus de la famille de proceder a une autopsie. Elle offre egalement une approche standardisee envers les autopsies foetales et perinatales, en mettant l'accent sur les prelevements additionnels pertinents, le cas echeant. Valeurs La qualite des resultats a ete evaluee au moyen des criteres decrits dans le rapport du Groupe d'etude canadien sur les soins de sante preventifs (Tableau 1).

Published
2011

42. Recours à une méthode ADN (QF-PCR) dans le diagnostic prénatal des aneuploïdies fœtales

Author

Sylvie Langlois, Alessandra Duncan, R. Douglas Wilson, François Audibert, Jo-Ann Brock, June Carroll, Lola Cartier, Valérie A. Désilets, Alain Gagnon, Jo-Ann Johnson, Lynn Murphy-Kaulbeck, Nanette Okun, Melanie Pastuck, David Chitayat, Isabelle DeBie, Suzanne Demczuk, Michael T Geraghty, Janet Marcadier, Tanya N. Nelson, Vicky Siu, and David Skidmore

Subjects
Gynecology, medicine.medical_specialty, business.industry, medicine, Obstetrics and Gynecology, business
Abstract

Resume Objectif Offrir aux fournisseurs de soins de sante canadiens des donnees actuelles sur l'utilisation de l'amplification en chaine par polymerase fluorescente quantitative (QF-PCR) ou d'une technologie equivalente dans le diagnostic prenatal des anomalies chromosomiques fœtales. Options Au cours des dernieres decennies, le diagnostic prenatal des anomalies chromosomiques fœtales a repose sur l'analyse cytogenetique conventionnelle de cultures d'amniocytes, de villosites choriales ou de sang fœtal. Au cours des quelques dernieres annees, la validite clinique d'une nouvelle technique (la QF-PCR) pour ce qui est de la detection des aneuploidies courantes a ete signalee par un certain nombre de chercheurs. Cette technique dispose de l'avantage de fournir rapidement des resultats pour le diagnostic ou l'exclusion de l'aneuploidie en ce qui concerne les chromosomes 13, 18, 21, X ou Y II est maintenant possible de choisir d'avoir recours a une analyse chromosomique standard ou a la QF-PCR pour le diagnostic prenatal des anomalies chromosomiques (ou encore de mener ces deux tests), en fonction de l'indication clinique du depistage. Le present document analyse l'utilite clinique de la QF-PCR et formule des recommandations quant a son utilisation dans le cadre des soins offerts aux patientes canadiennes. Resultats Des recherches ont ete menees dans Medline et PubMed afin d'en tirer les articles publies en anglais entre janvier 2000 et decembre 2010 qui presentaient des donnees issues de la comparaison entre la QF-PCR et l'analyse cytogenetique standard des prelevements prenataux. Une deuxieme recherche a ete menee pour identifier les publications en anglais qui offraient des resultats d'analyses cytogenetiques menees sur des prelevements prenataux chez des femmes exposees a un risque accru d'aneuploidie fœtale en raison de leur âge, de resultats anormaux a la suite du depistage prenatal ou de marqueurs faibles echographiques fœtaux semblant indiquer un risque accru d'aneuploidie. Ces publications ont ete incluses lorsqu'elles offraient des renseignements detailles sur les anomalies detectees, peu importe si un depistage rapide de l'aneuploidie avait ete mene. Les resultats ont ete restreints aux analyses systematiques, aux essais comparatifs randomises et aux etudes observationnelles pertinentes. La litterature grise (non publiee) a ete identifiee par l'intermediaire de recherches menees dans les sites Web d'organismes s'interessant a l'evaluation des technologies dans le domaine de la sante et d'organismes connexes, dans des collections de directives cliniques, dans des registres d'essais cliniques et aupres de societes de specialite medicale nationales et internationales. Les directives cliniques precedemment publiees par la Societe des obstetriciens et gynecologues du Canada au sujet du depistage prenatal ont egalement ete analysees dans le cadre de l'elaboration de la presente directive clinique. Valeurs La qualite des resultats a ete evaluee au moyen des criteres decrits dans le rapport du Groupe d'etude canadien sur les soins de sante preventifs (Tableau). Avantages, desavantages et couts La presente directive clinique fait la promotion du recours a un test ADN rapide de depistage de l'aneuploidie chez les femmes exposees a un risque accru de connaitre une grossesse affectee par une aneuploidie courante. La mise en oeuvre d'un tel test aura l'avantage de fournir rapidement des resultats precis aux femmes exposees a un risque accru de syndrome de Down, de trisomie 13, de trisomie 18, d'aneuploidie ou de triploidie des chromosomes sexuels. Elle favorisera egalement une meilleure utilisation des ressources laboratoires et la reduction des couts lies au diagnostic prenatal. Cependant, un faible pourcentage de grossesses presentant une anomalie chromosomique potentiellement significative sur le plan clinique, bien que detectables au moyen de methodes cytogenetiques conventionnelles, passeront inapercues au moment de la mise en oeuvre de la QF-PCR. Recommandations 1. La QF-PCR est un moyen fiable de detecter les trisomies et devrait remplacer l'analyse cytogenetique conventionnelle lorsque le depistage prenatal n'est mene qu'en raison d'un risque accru d'aneuploidie affectant les chromosomes 13, 18, 21, X ou Y. Comme pour tout autre test, les services de counseling pretest devraient comprendre une discussion sur les avantages et les limites de ce test. Au cours de la periode initiale d'utilisation, l'offre d'une formation aux fournisseurs de soins de sante s'averera necessaire. (II-2A) 2. L'analyse cytogenetique conventionnelle et la QF-PCR devraient toutes deux etre mises en oeuvre dans tous les cas de diagnostic prenatal demande en raison de la constatation echographique d'une anomalie foetale (y compris une mesure accrue de la clarte nucale > 3,5 mm) ou de la presence d'un remaniement chromosomique familial. (II-2A) 3. Le suivi cytogenetique des resultats de QF-PCR indiquant des trisomies 13 et 21 est recommande pour ecarter la presence possible de translocations robertsoniennes hereditaires. Toutefois, la decision de mettre en oeuvre, pour tous les cas, une culture d'appoint qui permettrait la tenue d'un depistage cytogenetique traditionnel (lorsque cela s'avererait indique en raison de donnees cliniques ou de laboratoire additionnelles) devrait etre prise par chacun des centres offrant le depistage, en fonction de l'experience et des ressources cliniques et de laboratoire locales. (III-A) 4. D'autres technologies de detection rapide de l'aneuploidie etant en mesure d'offrir un rendement semblable ou ameliore (pour ce qui est de la detection des trisomies 13, 18 et 21, et de l'aneuploidie des chromosomes sexuels) pourraient en venir a remplacer la QF-PCR. (III-A)

Published
2011

43. Dépistage et diagnostic prénatals de l’aneuploïdie en ce qui concerne les grossesses gémellaires

Author

François Audibert, Alain Gagnon, R. Douglas Wilson, Claire Blight, Jo-Ann Brock, Lola Cartier, Valérie A. Désilets, Jo-Ann Johnson, Sylvie Langlois, Lynn Murphy-Kaulbeck, Nanette Okun, Melanie Pastuck, Vyta Senikas, David Chitayat, Michael T. Geraghty, Janet Marcadier, Tanya N. Nelson, David Skidmore, Vicky Siu, and Frédérique Tihy

Subjects
Gynecology, medicine.medical_specialty, Prenatal screening, medicine.diagnostic_test, Nuchal translucency, business.industry, Amniocentesis, medicine, Obstetrics and Gynecology, Chorionic villus sampling, Prenatal diagnosis, business, Twin Pregnancy
Published
2011

44. Dépistage prénatal de l’aneuploïdie fœtale en ce qui concerne les grossesses monofœtales

Author

David Chitayat, Sylvie Langlois, R. Douglas Wilson, François Audibert, Claire Blight, Jo-Ann Brock, Lola Cartier, June Carroll, Valérie A. Désilets, Alain Gagnon, Jo-Ann Johnson, Lynn Murphy-Kaulbeck, Nanette Okun, Melanie Pastuck, Vyta Senikas, Isabelle DeBie, Suzanne Demczuk, Valerie A. Désilets, Michael T. Geraghty, Janet Marcadier, Tanya N. Nelson, David Skidmore, and Vicky Siu

Subjects
Gynecology, Down syndrome, medicine.medical_specialty, Prenatal screening, business.industry, medicine, Obstetrics and Gynecology, Aneuploidy, Prenatal diagnosis, medicine.disease, Trisomy, business
Published
2011

45. Prospective study of intracranial translucency and the posterior brain in normal fetuses at the 11- to 13-week scan

Author

Katherine Fong, Jana Dengler, Ants Toi, Ravi Menezes, Nanette Okun, and Yasser Karimzad

Subjects
Adult, medicine.medical_specialty, Adolescent, Intraclass correlation, Fetal position, Retroverted uterus, Ultrasonography, Prenatal, Young Adult, Pregnancy, medicine, Humans, Radiology, Nuclear Medicine and imaging, Prospective Studies, Prospective cohort study, Measurement reproducibility, Observer Variation, Fetus, Brain Mapping, Radiological and Ultrasound Technology, Spina bifida, business.industry, Gestational age, Brain, Reproducibility of Results, Middle Aged, medicine.disease, Surgery, Pregnancy Trimester, First, Female, business, Nuclear medicine, Nuchal Translucency Measurement
Abstract

Objectives To evaluate the ability of sonographers to prospectively identify intracranial translucency and posterior brain structures at 11 to 13 weeks and to evaluate measurement reproducibility of brain stem and brain stem–occipital bone diameters on stored images. Methods After specific training for intracranial translucency visualization, 10 nonphysician sonographers prospectively identified intracranial translucency at the 11- to 13-week scan, noting whether intracranial translucency was present, absent, or uncertain. If absent/uncertain, they documented the reason as spina bifida or an inadequate image (with reasons for the inadequate image). Measurements of brain stem and brain stem–occipital bone diameters were performed on stored images. Fifty randomly selected cases were reviewed for intraobserver and interobserver variability. Results In 313 singleton pregnancies, the posterior brain including intracranial translucency was evaluated; 293 (93.6%) had known pregnancy outcomes. None had open spina bifida, but 7 had chromosomal or congenital abnormalities. In the remaining 286 normal fetuses, intracranial translucency was seen in 275 (96%) and uncertain in 11 (4%), due to inadequate images (top 3 reasons were fetal position [n = 8], obesity [n = 5], and retroverted uterus [n = 4]). Fetal position and gestational age were significantly associated with intracranial translucency visualization (P < .05). Intraobserver and interobserver agreement rates were moderate for measurements of brain stem diameter (intraclass correlation coefficients, 0.59 and 0.57) and substantial for brain stem–occipital bone diameter (intraclass correlation coefficients, 0.76 and 0.61). Bland-Altman analysis revealed negligible intraobserver and interobserver differences in brain stem and brain stem–occipital bone diameter measurements. Conclusions Intracranial translucency can be prospectively identified by trained sonographers in 96% of normal fetuses at 11 to 13 weeks. Measurements of brain stem and brain stem–occipital bone diameters are reproducible.

Published
2014

46. Current practices in the prediction and prevention of preterm birth in patients with higher-order multiple gestations

Author

Dan Farine, Nanette Okun, Emily Baker, and Tiffany Hunter

Subjects
Tocolytic agent, medicine.medical_specialty, Pediatrics, Canada, medicine.medical_treatment, Psychological intervention, Bed rest, Risk Assessment, Adrenal Cortex Hormones, Pregnancy, Surveys and Questionnaires, medicine, Humans, Practice Patterns, Physicians', Cerclage, Cervical, Response rate (survey), Obstetrics, business.industry, Obstetrics and Gynecology, medicine.disease, Perinatology, Confidence interval, Cervical Length Measurement, Tocolytic Agents, Gestation, Premature Birth, Female, Pregnancy, Multiple, business, Bed Rest
Abstract

Objective We sought to determine the interventions utilized by maternal-fetal medicine specialists in the prediction and prevention of preterm labor in higher-order multiple (HOM) gestations. Study Design Online questionnaires and email surveys were sent to all the maternal-fetal medicine specialists in Canada (n = 122). Questionnaire items included interventions physicians routinely recommended for HOM gestations including: (1) bed rest; (2) cervical length measurement on transvaginal ultrasound; (3) corticosteroids use; (4) cerclage; and (5) tocolytic therapy. Results Response rate was 66% (81/122), with 68% of respondents in practice for >10 years. Of physicians, 91% did not routinely recommend bed rest (95% confidence interval [CI], 84.7–97.2). In all, 82% (95% CI, 73.63–90.4%) recommended routine cervical length assessment with 32.3% (95% CI, 20.7–43.2) and 37.1% (95% CI, 25.3–48.6) of this group suggesting assessment at 16-18 and 19-21 weeks, respectively. Frequency of assessment varied from biweekly (53.3%; 95% CI, 40.9–65.0), to monthly (23.3%; 95% CI, 12.8–33.1), to a single measurement repeated only if abnormal (12.5%; 95% CI, 4.5–20.8). In all, 28% (95% CI, 18.2–37.8) recommended routine administration of corticosteroids for lung maturation. Timing of administration varied, with 24% initiating steroids between 24-26 weeks, 59% between 27-28 weeks, and 17% after 28 weeks. None reported routine cerclage placement. However, 71% (95% CI, 61.1–80.8) would perform cerclage based on history or ultrasound. Of respondents, 81% (95% CI, 72.4–89.5) would consider using tocolytic agents for threatened preterm labor including calcium channel blockers (94%), nonsteroidal antiinflammatory drugs (5%), and nitroglycerin transdermal patch (24%). Conclusion The variable practice guidelines and paucity of data for management of HOM pregnancy places the onus on individual practitioners to develop their own management schemes. This results in heterogeneous management, which is based on conflicting international guidelines, studies, expert opinion, or past experience.

Published
2014

47. Pregnancy outcomes after assisted human reproduction

Author

Nanette Okun, Sony Sierra, R. Douglas Wilson, Francois Audibert, Jo-Ann Brock, Carla Campagnolo, June Carroll, Lola Cartier, David Chitayat, Alain Gagnon, Jo-Ann Johnson, Sylvie Langlois, Lynn Murphy-Kaulbeck, W. Kim MacDonald, Melanie Pastuck, Lih Yeen Tan, Valda Poplak, and Helen Robson

Subjects
Male, medicine.medical_specialty, Canada, Reproductive Techniques, Assisted, medicine.medical_treatment, MEDLINE, Genetic Counseling, Fertilization in Vitro, Cochrane Library, law.invention, Congenital Abnormalities, Genomic Imprinting, Randomized controlled trial, law, Pregnancy, Risk Factors, Single Embryo Transfer, Medicine, Humans, Genetic Testing, Sperm Injections, Intracytoplasmic, Infertility, Male, Preimplantation Diagnosis, Gynecology, Chromosome Aberrations, Assisted reproductive technology, business.industry, Infant, Newborn, Pregnancy Outcome, Obstetrics and Gynecology, Guideline, Infant, Low Birth Weight, Clinical trial, Systematic review, Family medicine, Premature Birth, Observational study, Female, Pregnancy, Multiple, business, Maternal Age
Abstract

To review the effect of assisted human reproduction (AHR) on perinatal outcomes, to identify areas requiring further research with regard to birth outcomes and AHR, and to provide guidelines to optimize obstetrical management and counselling of prospective Canadian parents.This document compares perinatal outcomes of different types of AHR pregnancies with each other and with those of spontaneously conceived pregnancies. Clinicians will be better informed about the adverse outcomes that have been documented in association with AHR, including obstetrical complications, adverse perinatal outcomes, multiple gestations, structural congenital abnormalities, chromosomal abnormalities, and imprinting disorders.Published literature was retrieved through searches of MEDLINE and the Cochrane Library from January 2005 to December 2012 using appropriate controlled vocabulary and key words (assisted reproduction, assisted reproductive technology, ovulation induction, intracytoplasmic sperm injection, embryo transfer, and in vitro fertilization). Results were not restricted to systematic reviews, randomized control trials/controlled clinical trials, and observational studies; studies of all designs published in English from January 2005 to December 2012 were reviewed, and additional publications were identified from the bibliographies of these articles. Searches were updated on a regular basis and incorporated in the guideline to August 2013. Grey (unpublished) literature was identified through searching the websites of health technology assessment and health technology assessment-related agencies, clinical practice guideline collections, clinical trial registries, and national and international medical specialty societies.The quality of evidence in this document was rated using the criteria described in the Report of the Canadian Task Force on Preventive Health Care (Table 1). Summary Statements 1. There is increasing evidence that infertility or subfertility is an independent risk factor for obstetrical complications and adverse perinatal outcomes, even without the addition of assisted human reproduction. (II-2) 2. The relative risk for an imprinting phenotype such as Silver-Russell syndrome, Beckwith-Wiedemann syndrome, or Angelman syndrome is increased in the assisted reproduction population, but the actual risk for one of these phenotypes to occur in an assisted pregnancy is estimated to be low, at less than 1 in 5000. The exact biological etiology for this increased imprinting risk is likely heterogeneous and requires more research. (II-2) Recommendations 1. All men with severe oligozoospermia or azoospermia (sperm count5 million/hpf) should be offered genetic/clinical counselling, karyotype assessment for chromosomal abnormalities, and Y-chromosome microdeletion testing prior to in vitro fertilization with intracytoplasmic sperm injection. (II-2A) 2. All men with unexplained obstructive azoospermia should be offered genetic/clinical counselling and genetic testing for cystic fibrosis prior to in vitro fertilization with intracytoplasmic sperm injection. (II-2A) 3. Multiple pregnancy is the most powerful predictive factor for adverse maternal, obstetrical, and perinatal outcomes. Couples should be thoroughly counselled about the significant risks of multiple pregnancies associated with all assisted human reproductive treatments. (II-2A) 4. The benefits and cumulative pregnancy rates of elective single embryo transfer support a policy of using this protocol in couples with good prognosis for success, and elective single embryo transfer should be strongly encouraged in this population. (II-2A) 5. To reduce the incidence of multiple pregnancy, health care policies that support public funding for assisted human reproduction, with regulations promoting best practice regarding elective single embryo transfer, should be strongly encouraged. (II-2A) 6. Among singleton pregnancies, assisted reproductive technology is associated with increased risks of preterm birth and low birth weight infants, and ovulation induction is associated with an increased risk of low birth weight infants. Until sufficient research has clarified the independent roles of infertility and treatment for infertility, couples should be counselled about the risks associated with treatment. (II-2B) There is a role for closer obstetric surveillance of women who conceive with assisted human reproduction. (III-L) 7. There is growing evidence that pregnancy outcomes are better for cryopreserved embryos fertilized in vitro than for fresh embryo transfers. This finding supports a policy of elective single embryo transfer for women with a good prognosis (with subsequent use of cryopreserved embryos as necessary), and may reassure women who are considering in vitro fertilization. (II-2A) 8. Women and couples considering assisted human reproduction and concerned about perinatal outcomes in singleton pregnancies should be advised that (1) intracytoplasmic sperm injection does not appear to confer increased adverse perinatal or maternal risk over standard in vitro fertilization, and (2) the use of donor oocytes increases successful pregnancy rates in selected women, but even when accounting for maternal age, can increase the risks of low birth weight and preeclampsia. (II-2B) 9. Any assisted reproductive technology procedure should be prefaced by a discussion of fetal outcomes and the slight increase in the risk of congenital structural abnormalities, with emphasis on known confounding factors such as infertility and body mass index. (II-2B) 10. In pregnancies achieved by artificial reproductive technology, routine anatomic ultrasound for congenital structural abnormalities is recommended between 18 and 22 weeks. (II-2A) 11. Pregnancies conceived by intracytoplasmic sperm injection may be at increased risk of chromosomal aberrations, including sex chromosome abnormalities. Diagnostic testing should be offered after appropriate counselling. (II-2A) 12. The possible increased risk for late onset cancer due to gene dysregulation for tumour suppression requires more long-term follow-up before the true risk can be determined. (III-A) 13. The clinical application of preimplantation genetic testing in fertile couples must balance the benefits of avoiding disease transmission with the medical risks and financial burden of in vitro fertilization. (III-B) 14. Preimplantation screening for aneuploidy is associated with inconsistent findings for improving pregnancy outcomes. Any discussion of preimplantation genetic screening with patients should clarify that there is no adequate information on the long-term effect of embryo single cell biopsy. (I-C).

Published
2014

48. Is Transperineal Ultrasonography of Cervical Length in Pregnant Women as Accurate as Endovaginal Ultrasonography? A Prospective, Blinded Comparison of Level of Agreement of Two Techniques

Author

Shelin Tkatch, Damon C. Mayes, Trevor Cohen, Nestor Demianczuk, and Nanette Okun

Subjects
Cervix length, medicine.medical_specialty, business.industry, Transperineal ultrasonography, Concordance, Preterm labour, Endovaginal ultrasonography, Medicine, Radiology, business, Cervical length, Blinded study, Cervical Length Measurement
Abstract

Objectives : To assess the accuracy of transperineal compared to endovaginal sonographic measurement of cervix length, and to assess the feasibility of an obstetrical resident attaining competence in transperineal sonographic measurement of cervix length. Methods : After attaining appropriate concordance in measurement between the three participating investigators (one obstetrical resident and two experienced sonographers), a prospective, blinded study was performed. Paired endovaginal and transperineal cervix length measurements were performed on 123 consenting pregnant women. Results : Concordance between the three investigators was easily established, demonstrating competence in transperineal cervix length measurement by the obstetrical resident. Although there was 85 percent correlation between endovaginal and transperineal cervix length measurements, the predetermined acceptante difference between the two measurements (1-5 mm) was not obtained, demonstrating that transperineal cervical length measurements are not as accurate as endovaginal measurements. ln addition, 15 percent of transperineal assessments were of insufficient quality for interpretations. Conclusions : Transperineal measurements are more difficult to perform well, the quality of the measurements are more often unacceptable, and they may not be as accurate or reliable as endovaginal measurements. It is a realistic objective for obstetrical residents to become competent in sonographic cervix length measurement, suggesting that it could be feasible for residents to perform endovaginal cervix length measurements in a labour and delivery setting for the assessment of women with symptoms of threatened preterm labour.

Published
2001

49. Early motor development of breech- and cephalic-presenting infants

Author

Paul Byrne, Doreen J. Bartlett, Joe Watt, Martha C. Piper, and Nanette Okun

Subjects
Male, Pediatrics, medicine.medical_specialty, Neurological assessment, Child Development, Pregnancy, Breech presentation, Humans, Medicine, Prospective Studies, Breech Presentation, reproductive and urinary physiology, Motor skill, Psychomotor learning, Cesarean Section, business.industry, Infant, Newborn, Infant, Obstetrics and Gynecology, Motor Skills, Gestation, Female, Analysis of variance, Vertex Presentation, business, Cohort study
Abstract

This study was conducted to determine whether breech-presenting infants have a different pattern of early neuromotor development than cephalic-presenting infants--regardless of mode of delivery-thus explaining both the failure to assume cephalic version at the end of gestation and the higher rates of childhood motor impairments associated with breech presentation.Ninety morphologically normal, term, breech-presenting singletons with birthweights greater than 2,500 g were paired with a similar cephalic-presenting infant, matched for gender and mode of delivery (n = 180; 100 delivered abdominally and 80 delivered vaginally). Data on neurological status (Neurological Assessment of the Preterm and Full-term Newborn Infant) and motor performance (Alberta Infant Motor Scale, Peabody Developmental Motor Scales, and age of walking) were collected prospectively over the first 18 months of life. This study was designed with a power of .80 to detect a "medium" effect size for motor development using the Alberta Infant Motor Scale. The data were analyzed using analysis of variance techniques.Breech-presenting infants had minor transient differences compared with cephalic-presenting infants. First, they had more open popliteal angles at birth (P.001). Second, they had significantly lower motor scores at 6 weeks than the normative sample (P.001). At 18 months, three infants were diagnosed with neurological problems, all of whom were delivered electively in the cesarean-breech group.As a group, breech-presenting infants do not have a persistent, inherently different pattern of motor development than cephalic-presenting infants. Mode of delivery did not explain the excess neuromotor impairment detected in the subgroup of breech infants.

Published
2000

50. Technical factors in early amniocentesis predict adverse outcome. Results of the Canadian early (EA) versus mid-trimester (MA) amniocentesis trial

Author

B. A. Armson, R. Benzie, Nanette Okun, Jo-Ann Johnson, Jerome Dansereau, Christopher Harman, R. Natale, J. Singer, Elizabeth J.T. Winsor, Patrick Mohide, M. F. Ho, and R. D. Wilson

Subjects
Gynecology, Pregnancy, medicine.medical_specialty, medicine.diagnostic_test, business.industry, Obstetrics, Obstetrics and Gynecology, Chorionic villus sampling, Prenatal diagnosis, Abortion, medicine.disease, law.invention, Randomized controlled trial, law, medicine, Amniocentesis, Maternal hypertension, Gestation, business, Genetics (clinical)
Abstract

The purpose of this study was to identify risk factors for fetal loss and other pregnancy complications associated with genetic amniocentesis. Data were acquired in the Canadian Early Amniocentesis Trial (CEMAT), a multicentered (12) prospective, randomized trial comparing continuous ultrasound-guided early amniocentesis (EA) and mid-trimester amniocentesis (MA) (CEMAT Group, 1998). Details of the procedure were recorded and analysed by allocation (EA versus MA), operator and centre, and correlated with pregnancy outcome. A total of 62 spontaneous pregnancy losses occurred between the procedure and 20 weeks' gestation among the 3691 patients who received their procedures within the allocated window (EA=53/1916, MA=9/1775). Technical factors correlating with these losses included procedures 'judged to be difficult' by the operator, and post-procedure amniotic fluid leakage or bleeding. Maternal risk factors included maternal hypertension (fetal loss 11. 1 per cent, compared with non-hypertensive women, 2.6 per cent) increased body mass index (BMI) and gravidity of three or greater. Allocation to EA was predictive of fetal loss, as well as failed procedure, multiple needle insertions, amniotic fluid leakage, failed culture and talipes equinovarus, in excess compared with MA. In conclusion, in this large prospective randomized trial evaluating amniocentesis, specific maternal, fetal and procedural variables were found to be predictive of fetal loss and adverse pregnancy outcome. Performing amniocentesis before 13 weeks' gestation (EA) was the major predictive factor for adverse outcome. These data suggest that first-trimester chorionic villus sampling (CVS) and MA will likely remain the invasive procedures of choice for evaluation of fetal karyotype.

Published
1999

Catalog

Books, media, physical & digital resources
See catalog results