Prenatal Epigenetics: Trauma and Outcomes of Labor Dysfunction Restricted; Files Only

Abstract

Black pregnant people are disproportionately affected by trauma exposure, post-traumatic stress disorder (PTSD), and maternal morbidity and mortality. PTSD has been associated with increased risk for maternal morbidity and mortality; however, little is known about the physiologic mechanisms by which PTSD may contribute to poor perinatal outcomes. PTSD is associated with dysregulation of stress physiology systems, including the hypothalamic-pituitary- adrenal axis, the oxytocin system, and immunologic function which are integral to labor progress. Labor dysfunction, defined as labor dystocia and unplanned cesarean birth, is a primary contributor to maternal morbidity and mortality. Thus, in the first paper of this dissertation I examined associations among childhood maltreatment, labor duration, and synthetic oxytocin requirements for vaginal birth in a sample of Black birthing people. In that sample, among those who had induced labor, associations were found between childhood emotional and physical abuse and labor duration in adjusted models. Additionally, there were associations between childhood physical abuse with higher intrapartum synthetic oxytocin dose, duration, and mean dose per hour. In the second chapter, in a sample of Black pregnant people getting prenatal care at a birth center or hospital, I evaluated relationships among childhood maltreatment, life course trauma exposure, PTSD symptoms and labor dystocia and unplanned cesarean birth. In the total induction of labor sample, PTSD symptoms and provisional PTSD were associated with labor dystocia but not unplanned cesarean birth. In the third paper, a subset of participants from the second paper who gave prenatal blood samples for epigenetic analyses were evaluated. Associations were found between PTSD symptom total score and DNA methylation at cg16373697 in the SLC14A2 gene, which is involved with renal function and hypertension. Associations were also found between labor dystocia and DNA methylation at cg18718657 in the FKBP2 gene, which is involved in complement cascade and proinsulin protein folding and trafficking. CpG sites associated (P<.05) with PTSD symptom score were 2.3 times more likely to also be associated with labor dystocia. Overall, the results in this dissertation highlights relationships among childhood maltreatment, trauma exposure, PTSD, differences in DNA methylation, and labor dystocia in multiple cohorts of Black pregnant people.

Table of Contents

 Table of Contents

CHAPTER 1: INTRODUCTION: TRAUMA, POST TRAUMATIC STRESS DISORDER, AND LABOR DYSFUNCTION 1

Context and Authors’ Contribution 1

Trauma as a Social Determinant of Health: Prevalence and Health Outcomes 2

Post Traumatic Stress Disorder 2

Disparities in Trauma Exposure, Post Traumatic Stress Disorder, and Maternal Morbidity and Mortality 3

Labor Dysfunction 4

Trauma and Labor Dysfunction Outcomes 4

Influence of Maternal Trauma Exposure from Adulthood on Labor Dystocia and Unplanned Cesarean Birth 5

Influence of Maternal Trauma Exposure from Childhood on Labor Dystocia and Unplanned Cesarean Birth 9

Trauma, Epigenetics, and Pregnancy 18

Physiology of Normal Parturition in Humans 19

Preparation and Labor Initiation 19

Physiology of Uterine Activity and Endurance in Labor 20

Trauma, Stress, and Immunologic Dysregulation in Pregnancy and Labor 23

Trauma, Stress and Oxytocin System in Pregnancy and Labor 25

Trauma and Stress Related Disorders and HPA-Axis in Pregnancy 28

Purpose 30

Conceptual Framework: Trauma, Allostatic Load, and Perinatal Outcomes 31

Specific Aims 31

Summary 33

CHAPTER 2: CHILDHOOD MALTREATMENT, LABOR DURATION, AND INTRAPARTUM SYNTHETIC OXYTOCIN DOSE AND DURATION: A POTENTIAL OXYTOCIN-LINKED CONTRIBUTOR TO LABOR OUTCOMES IN BLACK BIRTHING PEOPLE 44

Context, Authors’ Contribution, And Acknowledgement of Reproduction 44

Abstract 45

INTRODUCTION 46

Childhood Trauma and the Oxytocin System 47

Childhood Trauma and Labor Duration 48

METHODS 49

Results 54

Participants Demographics 54

Associations Between Childhood Maltreatment and Labor Duration 56

Clinical Interpretation 58

Associations Between Childhood Maltreatment and Intrapartum Synthetic Oxytocin Requirements 60

DISCUSSION 62

Strengths, Limitations, and Future Directions 63

CONCLUSION 65

CHAPTER 3: TRAUMA EXPOSURE, POST TRAUMATIC STRESS DISORDER AND OUTCOMES OF LABOR DYSFUNCTION IN A SAMPLE OF BLACK PREGNANT PEOPLE 70

Context and Authors’ Contribution 70

Abstract 71

Maternal Trauma Exposure and Labor Dystocia 73

Maternal Trauma Exposure and Unplanned Cesarean 76

Trauma Exposure and Labor Dysfunction Outcomes in Black Pregnant Populations in the United States 80

Methods 81

Results 87

Participant Demographics 87

Associations Between TEI-LEC Harmonized Scale, Childhood Trauma Questionnaire, and PCL-5 Score and Labor Dysfunction Outcomes in the Total Sample and Stratified by Mode of Labor Onset 91

Associations Between PTSD, Trauma Exposure, and Labor Dysfunction Outcomes in the Total Sample Stratified by Prenatal Care Site and Mode of Labor Onset 95

Discussion 98

Strengths, Limitations, and Future Directions 100

Conclusion 103

CHAPTER 4: RELATIONSHIPS BETWEEN PTSD, DNA METHYLATION AND LABOR DYSFUNCTION OUTCOMES IN A COHORT OF BLACK PREGNANT PEOPLE 111

Context and Authors’ Contribution 111

Abstract 112

Introduction 113

Methods 116

Results 122

Trauma Exposure, Provisional PTSD and Differential DNA Methylation 124

Post Traumatic Stress Disorder Symptoms Associated with Methylation at cg16373697 in SLC14A2 Gene 124

Methylation at cg16373697 in SLC14A2 Gene Associated with Hypertensive Disorders of Pregnancy 126

Labor Dystocia Associated with Methylation in cg18718657 in FKBP2 Gene 126

Enrichment Test for CpGs Associated with PCL-5 Score and Labor Dystocia 128

Relationships Between PCL-5 Total Score, Epigenetic Biomarker Proxies, and Metabolic Risk Score 128

Relationships Between DNAm at cg18718657, Labor Dystocia Metabolic Risk Score, Epigenetic Biomarker Proxies, and Metabolic Risk Score 130

Discussion 132

Strengths, Limitations, and Future Directions 135

CHAPTER 5: SYNTHESIS AND FUTURE DIRECTIONS 146

Context and Authors’ Contribution 146

Introduction 147

Theoretical Framework 147

Summary of the Study Findings 148

Contributions to the Literature 155

Study Limitations and Strengths 157

Implications for Clinical Practice and Future Research 158

About this Dissertation

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School	Laney Graduate School
Department	Nursing
Degree	Ph.D.
Submission	Dissertation
Language	English
Research Field	Biology, Genetics Psychology, Behavioral Sciences Health Sciences, Nursing
关键词	Pregnancy Labor Dysfunction Epigenetics Posttraumatic Stress Disorder Health Equity Trauma
Committee Chair / Thesis Advisor	Dr. Nicole Carlson, Emory University
Committee Members	Dr. Alicia Smith, Emory University Dr. Alexis Dunn-Amore, New York University Dr. Vasiliki Michopoulos, Emory University Dr. Madelyn Houser, Emory University

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