Maternal plasma corticotrophin-releasing hormone and prediction of spontaneous preterm delivery. / CUHK electronic theses & dissertations collection

January 2001

Leung Tse Ngong. / Thesis (M.D.)--Chinese University of Hong Kong, 2001. / Includes bibliographical references (p. 169-197). / Electronic reproduction. Hong Kong : Chinese University of Hong Kong, [2012] System requirements: Adobe Acrobat Reader. Available via World Wide Web. / Mode of access: World Wide Web.

Obstetric Labor, Premature

Corticotropin-Releasing Hormone

alpha-Fetoproteins

Pregnancy Trimester, Second

Identification of a rational, physiologically based early biomarker and pathogenic pathway For preeclampsia

Santillan, Mark K.

01 May 2016

Preeclampsia is a hypertensive disorder of pregnancy that is diagnosed after the 20th week of gestation. It is defined by the American College of Obstetrics and Gynecology as de novo hypertension of at least 140/90 in a pregnant woman. Proteinuria with the hypertension is sufficient but not required for the diagnosis, especially if a woman displays severe symptoms such as headache, blurry vision, right upper quadrant pain, and low platelet count. Despite significant research, preeclampsia continues to kill 76,000 mothers and 500,000 babies per year worldwide. It causes short and long term consequences such as future metabolic and cardiovascular events for the mother and the child born during a pregnancy affected by preeclampsia. A delay in diagnosis and delayed access to appropriate care is a core cause of the preeclampsia related morbidity and severe mortality worldwide. Despite being in the medical literature since the time of the ancient Greeks, there is currently no significant predictive, preventative, therapeutic, and curative agent for preeclampsia except for an often preterm delivery of the fetus. The complex pathogenesis of preeclampsia has challenged the ability to effectively predict preeclampsia to decrease the delay in this diagnosis. Consequently, an early intervention or triage to higher level obstetric care is hindered. The lack of an early biomarker for preeclampsia also represents a major barrier to treat preeclampsia before major clinical symptoms emerge and the cycle of future cardiovascular risk for mom and baby begins. Novel, very early pregnancy predictive tests for preeclampsia may provide significant clinical utility. Furthermore, a biomarker that is linked with an early pathogenic mechanism in the first trimester development of preeclampsia would reveal a new avenue of early, first trimester intervention to treat and prevent this devastating disease. This work details the search for such a biomarker linked to an early initiator of the molecular pathogenesis of preeclampsia. These microRNA data highlight very important dysregulated mechanisms including immunologic, cell growth, and angiogenic mechanisms. T cells and the role of indoleamine 2,3 dioxygenase (IDO) is important in the early, maternal immune tolerance to the placenta and pregnancy. As poor placentation is a core cause of preeclampsia, a decreased immune tolerance to it is hypothesized to lead to preeclampsia. Furthermore, low IDO activity has been observed in the placentas of preeclamptic pregnancies which may make it a viable biomarker. These IDO-knock out mouse data, demonstrate that chronic IDO deficiency is sufficient to cause some of the core phenotypes of preeclampsia including renal dysfunction, vascular endothelial dysfunction, fetal growth restriction, and a slight increase in systolic blood pressure. This model does not completely phenocopy human preeclampsia. An investigation of early markers that are linked to vascular, immune, and renal abnormalities highlights the vasopressin pathway as a potential biomarker and early initiator of the pathogenesis of preeclampsia. These data demonstrate that copeptin, as a stable marker of vasopressin secretion, is robustly predictive of the development of late pregnancy human preeclampsia, as early as the 6th week of gestation. Furthermore, a mouse model with chronic infusion of vasopressin throughout mouse gestation phenocopies all the essential aspects of human preeclampsia: pregnancy specific hypertension, proteinuria, pathognomonic glomerular endotheliosis, fetal growth restriction, and increased fetal death. Further research must be done to elucidate the immunologic, vascular, and fetal programming phenotypes of this model. This work posits the possibility that the vasopressin pathway may provide new predictive, preventative, therapeutic, and potentially curative modalities for preeclampsia.

publicabstract

Animal Model

Biomarker

Early Prediction

First Trimester

Pathogenesis

Preeclampsia

Investigation of novel endocrine markers of early pregnancy and later pregnancy health

Tong, Stephen

January 2004

Abstract not available

Obstetrical endocrinology

Biochemical markers

Pregnancy -- Trimester, First

Pregnancy -- Complications

Miscarriage

Twins

Activin

A Rare Case of Acute Promyelocytic Leukemia in Pregnancy

Franklyn, Lindsey, Mhadgut, Hemendra, Sinha, Alok, Singal, Sakshi

28 April 2020

Acute promyelocytic leukemia (APL) is a clinically distinct and rare type of acute myeloid leukemia and represents an oncologic emergency. Even rarer is the incidence of APL in pregnancy with less than 60 cases described in the literature. A 33-year-old pregnant female at 34 week gestation presented to hospital with reports of abdominal pain. On admission she was found to have acute onset pancytopenia with a WBC count of 1.2, Hemoglobin of 9.7g/dl, and platelet count of 26000. Initial history, exam, and investigations including a peripheral smear, coagulation panel, liver function, vitamin b12 and folate levels did not reveal possible etiology of pancytopenia. Given worsening pancytopenia, bone marrow biopsy was done which showed 58% promyelocytes and 11% blasts with numerous Auer rods present. Cytogenetics showed abnormal female karyotype with t(15:17) and FISH analysis revealed PML/RARA fusion in 76.5% of analyzed cells. The above findings were diagnostic of APL. After multidisciplinary discussion with high risk obstetrics physician, it was decided to immediately induce labor for immediate initiation of treatment of APL. She had a prolonged labor requiring aggressive blood product support and initiation of All trans retinoic acid (ATRA) before delivery given concerns of coagulopathy. Induction treatment with Arsenic trioxide (ATO) was started the day after her delivery. Repeat bone marrow biopsy on day 24 showed complete morphologic remission. Shortly thereafter, she started cycle 1 of consolidation with ATRA and arsenic trioxide. APL is characterized by a translocation between chromosome 15 and 17. Coagulopathy is a pathognomonic feature of this leukemia and often the reason for high mortality in early course of disease. APL when treated with ATRA and ATO, has excellent remission rate and 99% overall survival at 2 years. APL in pregnancy is associated with increased risk of preterm delivery, perinatal mortality, and miscarriage. Following pregnancy, there is an increased risk of bleeding, infection, or placental abruption. ATRA, one of the pillars around which treatment of APL revolves, is highly teratogenic during the first trimester and has low risk later in pregnancy. Treatment is directed by the trimester of pregnancy. Termination of pregnancy or treatment with single agent conventional chemotherapy is preferred in the first trimester whereas treatment with ATRA prior to delivery and use of chemotherapy after delivery is the preferred approach in the 2nd and 3rd trimester. This case is an example of individualized approach with a multidisciplinary team need in the setting of scarce data.

Acute Promyelocytic Leukemia

APL

3rd-trimester pregnancy

ATRA

ATO

Cancer or Carcinogenesis

Effect of Time-Lapse Scheduling on Mathematics Achievement

Ross, John E., 1926-

05 1900

The purposes of the study were to (a) determine whether there was a significant difference in the mathematics achievement of students which may be attributed to any of the nine variations in trimester scheduling during the two-year period, and (b) to analyze the implications of trimester scheduling as they apply to teachers, counselors, and administrators in the middle school program. On the basis of careful treatment and analysis of data collected to ascertain the effect of time-lapse scheduling on mathematics achievement in arithmetic computation, arithmetic concepts, and arithmetic applications, the following conclusions, limited to the population studied, were drawn: 1. None of the nine time-lapse schedules had a significant differential effect on mathematics achievement. 2. The results of this study may be generalized to include the high, middle, and low achievement segments of the target population of students in all middle schools in the school district of this study. 3. Middle school administrators and counselors may schedule students into any convenient sequence of courses without fear of relative detrimental consequences to mathematics achievement. 4. Teachers need not be concerned that "learning loss" in mathematics due to different time-lapse schedules of the students will require different amounts of review prior to beginning work in a new trimester. 5. The Intensified Learning Plan is a viable program in mathematics in the school district's middle school plan of organization and scheduling.

trimester scheduling

mathematical achievement

School year.

Academic achievement.

Quitting Smoking During Pregnancy and Birth Outcomes: Evidence of Gains Following Cessation by Third Trimester

Bailey, Beth, McCook, Judy G., Clements, Andrea, McGrady, Lana

01 June 2011

No description available.

quitting smoking

pregnancy

gains

third trimester

College of Nursing

Family Medicine

Psychology

Postpartum care and diastasis recti abdominis recovery: an occupational therapist’s continuing education course

Winters, Sharon Hope

08 May 2023

American maternal health is a concern and has even been described as a “crisis” (Gingrey, 2020). The US is an outlier in maternal health in comparison to other industrialized countries with more than a 50% increase in maternal death rates comparatively speaking (Taylor et al., 2022). A significant change in postpartum care must occur. Hope Health Today LLC, the proposed continuing education Limited Liability Company (LLC), will be the catalyst to this health care change. Hope Health Today LLC’s initial continuing education program will positively educate healthcare providers to better serve this at-risk population. Hope Health Today LLC will provide professional education for licensed occupational therapists, physical therapists, physicians, nurses, and midwives. The initial continuing education (CEU) course will be a holistic guide for Diastasis Recti Abdominis (DRA) recovery and postpartum care. The course will cover pelvic floor and deep core anatomy, a 20-week diastasis recti abdominis recovery program, postpartum body mechanics, breast feeding positions, roles and interpersonal relationships, signs of postpartum depression, and return to intimacy. HopeHealth Today LLC aims to make a positive impact for postpartum families. Making a change at the policy level through American College of Obstetrics and Gynecology (ACOG) to provide a 4-week pelvic floor therapy referral to all postpartum patients. Hope Health Today LLC will advance the profession of occupational therapy through advocating for a women’s health board certification through American Occupational Therapy Association (AOTA) and improving quality postpartum patient outcomes through providing research based continuing education for health care providers. HopeHealth TodayLLC will educate the public through social media. HopeHealth TodayLLC will advance the current state of postpartum care. The ambition of this company is to educate the public to know what to expect from their women’s health providers and what to ask for if care is not reaching appropriate standards.

Continuing education

4th trimester

Abdominal binding

Muscle recovery

Muscle strengthening

Pelvic floor therapy

Interrelationships between stress, dietary intake, and plasma ascorbic acid during pregnancy

McFarland, Mary Ann

January 1982

The relationships between stress, ascorbic acid status, and the adequacy of nutrient intake during the third trimester of pregnancy were studied. Adequacy of nutrient and ascorbic acid intake were measured by diet histories and 24 hour recalls. Plasma ascorbic acid and cortisol levels were determined. Stress was assessed by Spielberger State-Trait Anxiety Inventories (STAI) and Symptom Checklists (SCL). Factors which may affect stress were assessed by a General Background Information Questionnaire. All subjects had acceptable plasma ascorbic acid levels (0.48 - 1.64). A-State and A-Trait scores, X̄ = 1.55 and X̄ = 1.63 respectively, indicated the majority of subjects to be little stressed. There were positive significant correlations between age and cortisol, A-State and A-Trait measures of STAI, nutritional scores from diet histories and plasma cortisol. Significant negative correlations were obtained between month of pregnancy and plasma ascorbic acid levels, total ascorbic acid intake and A-State measurements of STAI, A-State measurements and income, A-State measurements and education, and A-State measurements and ascorbic intake as calculated from diet histories. There was no significant correlations between STAI, measurements and cortisol, plasma ascorbic acid and cortisol, and STAI measurements and plasma ascorbic acid. This study showed no conclusive evidence that ascorbic acid status or nutrient intake were affected by psychological stress. / Master of Science

LD5655.V855 1982.M333

Pregnancy -- Nutritional aspects

Pregnancy -- Psychological aspects

Pregnancy -- Trimester, Third

Implications of False-Positive Trisomy 18 or 21 Screening Test Results in Predicting Adverse Pregnancy Outcomes

Huang, Pinchia

13 October 2009

No description available.

African Americans

Biomedical Research

Genetics

Health Care

Minority and Ethnic Groups

Obstetrics

prental screeening test

quad screens

first trimester screens

second trimester screens

first check

pregnancy complications

adverse pregnancy outcomes

obstetric complications

African American pregnancy

intrauterine growth retardation

Dépistage précoce du diabète gestationnel / Early screening of gestational diabetes mellitus

Mahdavian, Masoud

January 2015

Résumé : L’aggravation de certaines caractéristiques cliniques des femmes enceintes (âge, poids) et l’augmentation de la prévalence du diabète gestationnel (DG) poussent à dépister le DG le plus tôt possible pour éviter chez la mère et le fœtus les complications à court et à long terme. Le dépistage du DG est recommandé à 24-28 semaines de grossesse, et le plus souvent un test de tolérance à 50g de glucose (TTG) est réalisé. Pour les femmes qui ont des facteurs de risque, ce test doit être effectué plus précocement, habituellement pendant le premier trimestre de la grossesse. Cette dernière recommandation est peu suivie, d’autant qu’il n’y a pas de consensus international sur le dépistage du DG pendant le premier trimestre de la grossesse. Objectifs. 1) Définir au premier trimestre de la grossesse la valeur de la glycémie du TTG qui prédit le diagnostic de DG à 24-28 semaines avec une sensibilité et une spécificité optimales à l’aide d’une courbe ROC. 2) Déterminer si la glycémie du TTG au premier trimestre est un facteur prédictif indépendant du DG. Méthodes. Étude prospective de cohorte. Les facteurs d'inclusion étaient : âge ≥ 18 ans et âge gestationnel entre 6 et 13 semaines après la dernière menstruation. Les TTG ont été effectués à la première visite prénatale. Une deuxième visite était programmée à 24-28 semaines pour faire une hyperglycémie provoquée par voie orale (HGPO) et donc un éventuel diagnostic de DG. Les critères utilisés pour ce diagnostic étaient ceux de l’Association américaine du diabète. Résultats. Les TTG ont été faits à 9,1±2,0 semaines et les HGPO à 26.5±1.1semaines chez 1180 femmes (28,2±4,4 ans, IMC : 25,2±5,5 kg/m[indice supérieur 2]). Un DG a été diagnostiqué chez 100 (8,4%) participantes. La valeur de glycémie du TTG à 5,6 mmol/L a prédit le DG avec une sensibilité de 84,1% et une spécificité de 62,3%, tandis que la valeur prédictive positive était de 0,121 et la valeur prédictive négative de 0,985. Cette valeur de 5,6 était indépendamment associée au DG (OR=2,806, IC 95%: 1,98 à 3,97, p <0,001). Comparé à d'autres facteurs de risque, le TTG était le plus puissant prédicteur indépendant du DG (OR=1,767, IC 95%: 1,52 à 2,05, p <0,001). Conclusions. Au premier trimestre, la valeur glycémie de 5.6 mmol/L du TTG prédit avec une bonne sensibilité et spécificité l’apparition d’un DG à 24-28 semaines. La glycémie du TTG au premier trimestre est le plus puissant prédicteur indépendant de DG. / Abstract : The changes in clinical characteristics of pregnant women and an increase in the prevalence of gestational diabetes mellitus (GDM) warrant the importance of screening as early as possible in order to possibly prevent short and long-term complications in both the mother and fetus. GDM screening is recommended at 24-28 weeks of pregnancy, using a 50g glucose challenge test (GCT) although women with multiple risk factors are expected to be assessed “early” in pregnancy, a recommendation poorly followed. Most importantly, there is no universal agreement currently in place for GDM screening, particularly during the first trimester of pregnancy. Objectives. 1) To define the cut-off value of GCT during the first trimester in order to predict GDM diagnosed at 24-28 weeks of gestation with optimal sensitivity and specificity using ROC curve. 2) To determine if GCT during the first trimester of pregnancy is an independent predictor of GDM diagnosed at 24-28 weeks gestation. Methods. This is a prospective cohort study. Women were recruited at their first prenatal visit. Inclusion factors were: age ≥ 18 years and gestational age between 6 and 13 weeks from their last menstrual period. GCT were performed at the first prenatal visit. The second visit was scheduled at 24-28 weeks for the diagnostic 75g oral glucose tolerance test (OGTT). GDM diagnosis was made in accordance with the American Diabetes Association guidelines. A variety of statistical analysis including multivariate logistic regression models and ROC curve were used to address the aims of the study. Results. Participants (n=1180, age: 28.2±4.4 years, BMI: 25.2±5.5 kg/m[superscript 2]) underwent GCT at 9.1±2.0 weeks and OGTT at 26.5±1.1 weeks of gestation. GDM was diagnosed in 100 (8.4%) women. The cut-off value of 5.6 mmol/L predicted GDM with 84.1% (75.4-92.7) sensitivity, 62.3% (59.5-65.1) specificity, while the positive predictive value was 0.121 (0.091-0.150) and the negative predictive value was 0.985 (0.975-0.994). This 5.6 value was independently associated with GDM (OR=2.806, 95% CI: 1.98-3.97, p<0.001). Compared to other risk factors, GCT was the strongest independent predictor of GDM (OR=1.767, 95% CI: 1.52-2.05, p<0.001). Conclusions. The cut-off value of 5.6 mmol/L has the optimal sensitivity and specificity for the GCT during the first trimester to predict GDM at 24-28 weeks of gestation according to ADA guidelines. GCT during the first trimester is the strongest independent predictor of GDM at 24-28 weeks of gestation.

Diabète gestationnel

DG

Dépistage

1er trimestre

Grossesse

TTG

OGTT

Gestational diabetes mellitus

GDM

Screening

1st trimester

Pregnancy