2,484 results on '"Varner, Michael"'
Search Results
2. Short Term Coping-Behaviors and Postpartum Health in a Population-Based Study of Women with a Live Birth, Stillbirth, or Neonatal Death
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Stanhope, Kaitlyn K., Temple, Jeff R., Christiansen-Lindquist, Lauren, Dudley, Donald, Stoll, Barbara J., Varner, Michael, and Hogue, Carol J. R.
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- 2024
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3. Hypertensive disorders of pregnancy and subsequent risk of Alzheimer's disease and other dementias
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Schliep, Karen C, Shaaban, C Elizabeth, Meeks, Huong, Fraser, Alison, Smith, Ken R, Majersik, Jennifer J, Foster, Norman L, Wactawski‐Wende, Jean, Østbye, Truls, Tschanz, JoAnn, Padbury, James F, Sharma, Surrendra, Zhang, Yue, Facelli, Julio C, Abdelrahman, C Samir, Theilen, Lauren, and Varner, Michael W
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Reproductive Medicine ,Biomedical and Clinical Sciences ,Alzheimer's Disease Related Dementias (ADRD) ,Cerebrovascular ,Pregnancy ,Acquired Cognitive Impairment ,Aging ,Cardiovascular ,Maternal Morbidity and Mortality ,Alzheimer's Disease including Alzheimer's Disease Related Dementias (AD/ADRD) ,Brain Disorders ,Neurodegenerative ,Hypertension ,Women's Health ,Neurosciences ,Dementia ,Prevention ,Heart Disease ,Alzheimer's Disease ,Vascular Cognitive Impairment/Dementia ,Contraception/Reproduction ,Maternal Health ,Neurological ,Reproductive health and childbirth ,Good Health and Well Being ,Genetics ,Biological psychology - Abstract
IntroductionWomen with hypertensive disorders of pregnancy (HDP) have an increased risk of cardiovascular disease. Whether HDP is also associated with later-life dementia has not been fully explored.MethodsUsing the Utah Population Database, we performed an 80-year retrospective cohort study of 59,668 parous women.ResultsWomen with, versus without, HDP, had a 1.37 higher risk of all-cause dementia (95% confidence interval [CI]: 1.26, 1.50) after adjustment for maternal age at index birth, birth year, and parity. HDP was associated with a 1.64 higher risk of vascular dementia (95% CI: 1.19, 2.26) and 1.49 higher risk of other dementia (95% CI: 1.34, 1.65) but not Alzheimer's disease dementia (adjusted hazard ratio = 1.04; 95% CI: 0.87, 1.24). Gestational hypertension and preeclampsia/eclampsia showed similar increased dementia risk. Nine mid-life cardiometabolic and mental health conditions explained 61% of HDP's effect on subsequent dementia risk.DiscussionImproved HDP and mid-life care could reduce the risk of dementia.
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- 2023
4. Umbilical cord milking in nonvigorous infants: a cluster-randomized crossover trial.
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Underwood, Mark, Mazela, Jan, Kaempf, Joseph, Tomlinson, Mark, Gollin, Yvonne, Fulford, Kevin, Goff, Yvonne, Wozniak, Paul, Baker, Katherine, Rich, Wade, Morales, Ana, Varner, Michael, Poeltler, Debra, Vaucher, Yvonne, Mercer, Judith, Finer, Neil, El Ghormli, Laure, Rice, Madeline, Katheria, Anup, Clark, Erin, Yoder, Bradley, Schmölzer, Georg, Yan Law, Brenda, El-Naggar, Walid, Rittenberg, David, Sheth, Sheetal, Mohamed, Mohamed, Martin, Courtney, Vora, Farha, and Lakshminrusimha, Satyanarayana
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cord clamping ,cord milking ,newborn ,nonvigorous ,resuscitation ,Female ,Humans ,Infant ,Newborn ,Pregnancy ,Blood Transfusion ,Constriction ,Cross-Over Studies ,Hemoglobins ,Hypoxia-Ischemia ,Brain ,Infant ,Premature ,Placenta ,Umbilical Cord ,Umbilical Cord Clamping ,Infant ,Premature ,Diseases ,Infant ,Newborn ,Diseases - Abstract
BACKGROUND: Delayed cord clamping and umbilical cord milking provide placental transfusion to vigorous newborns. Delayed cord clamping in nonvigorous newborns may not be provided owing to a perceived need for immediate resuscitation. Umbilical cord milking is an alternative, as it can be performed more quickly than delayed cord clamping and may confer similar benefits. OBJECTIVE: We hypothesized that umbilical cord milking would reduce admission to the neonatal intensive care unit compared with early cord clamping in nonvigorous newborns born between 35 and 42 weeks gestation. STUDY DESIGN: This was a pragmatic cluster-randomized crossover trial of infants born at 35 to 42 weeks gestation in 10 medical centers in 3 countries between January 2019 and May 2021. The centers were randomized to umbilical cord milking or early cord clamping for approximately 1 year and then crossed over for an additional year or until the required number of consented subjects was reached. Waiver of consent as obtained in all centers to implement the intervention. Infants were eligible if nonvigorous at birth (poor tone, pale color, or lack of breathing in the first 15 seconds after birth) and were assigned to umbilical cord milking or early cord clamping according to their birth hospital randomization assignment. The baseline characteristics and outcomes were collected following deferred informed consent. The primary outcome was admission to the neonatal intensive care unit for predefined criteria. The main safety outcome was hypoxic-ischemic encephalopathy. Data were analyzed by the intention-to-treat concept. RESULTS: Among 16,234 screened newborns, 1780 were eligible (905 umbilical cord milking, 875 early cord clamping), and 1730 had primary outcome data for analysis (97% of eligible; 872 umbilical cord milking, 858 early cord clamping) either via informed consent (606 umbilical cord milking, 601 early cord clamping) or waiver of informed consent (266 umbilical cord milking, 257 early cord clamping). The difference in the frequency of neonatal intensive care unit admission using predefined criteria between the umbilical cord milking (23%) and early cord clamping (28%) groups did not reach statistical significance (modeled odds ratio, 0.69; 95% confidence interval, 0.41-1.14). Umbilical cord milking was associated with predefined secondary outcomes, including higher hemoglobin (modeled mean difference between umbilical cord milking and early cord clamping groups 0.68 g/dL, 95% confidence interval, 0.31-1.05), lower odds of abnormal 1-minute Apgar scores (Apgar ≤3, 30% vs 34%, crude odds ratio, 0.72; 95% confidence interval, 0.56-0.92); cardiorespiratory support at delivery (61% vs 71%, modeled odds ratio, 0.57; 95% confidence interval, 0.33-0.99), and therapeutic hypothermia (3% vs 4%, crude odds ratio, 0.57; 95% confidence interval, 0.33-0.99). Moderate-to-severe hypoxic-ischemic encephalopathy was significantly less common with umbilical cord milking (1% vs 3%, crude odds ratio, 0.48; 95% confidence interval, 0.24-0.96). No significant differences were observed for normal saline bolus, phototherapy, abnormal 5-minute Apgar scores (Apgar ≤6, 15.7% vs 18.8%, crude odds ratio, 0.81; 95% confidence interval, 0.62-1.06), or a serious adverse event composite of death before discharge. CONCLUSION: Among nonvigorous infants born at 35 to 42 weeks gestation, umbilical cord milking did not reduce neonatal intensive care unit admission for predefined criteria. However, infants in the umbilical cord milking arm had higher hemoglobin, received less delivery room cardiorespiratory support, had a lower incidence of moderate-to-severe hypoxic-ischemic encephalopathy, and received less therapeutic hypothermia. These data may provide the first randomized controlled trial evidence that umbilical cord milking in nonvigorous infants is feasible, safe and, superior to early cord clamping.
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- 2023
5. The association between perinatal depressive symptoms and child neurodevelopment
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Miller, Emily S., Costantine, Maged M., Mele, Lisa, Varner, Michael W., Reddy, Uma M., Wapner, Ronald J., Thorp, John M., Jr, Saade, George R., Tita, Alan T.N., Rouse, Dwight J., Sibai, Baha, Mercer, Brian M., Caritis, Steve N., and Casey, Brian M.
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- 2024
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6. Ocular Effects of Prenatal Carotenoid Supplementation in the Mother and Her Child: The Lutein and Zeaxanthin in Pregnancy (L-ZIP) Randomized Trial - Report Number 2
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Addo, Emmanuel K., Gorka, Joanna E., Allman, Susan J., Harrison, Deborah Y., Sharifzadeh, Mohsen, Hoffman, Robert O., Hartnett, M. Elizabeth, Varner, Michael W., and Bernstein, Paul S.
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- 2024
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7. Cardiovascular morbidity and mortality following hypertensive disorders of pregnancy
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Theilen, Lauren H., Varner, Michael W., Esplin, M. Sean, and Horne, Benjamin D.
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- 2024
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8. Mapping genetic susceptibility to spontaneous preterm birth: analysis of Utah pedigrees to find inherited genetic factors
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Workalemahu, Tsegaselassie, Clark, Erin A.S., Madsen, Michael J., Yu, Zhe, Dalton, Susan E., Esplin, M. Sean, Manuck, Tracy, Neklason, Deborah, Wu, Chen-Han Wilfred, Jorde, Lynn B., Camp, Nicola J., Silver, Robert M., and Varner, Michael W.
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- 2024
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9. Outcomes of induction vs prelabor cesarean delivery at
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Bushman, Elisa T., Grobman, William A., Bailit, Jennifer L., Reddy, Uma M., Wapner, Ronald J., Varner, Michael W., Thorp, John M., Jr, Caritis, Steve N., Prasad, Mona, Saade, George R., Sorokin, Yoram, Rouse, Dwight J., Blackwell, Sean C., and Tolosa, Jorge E.
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- 2023
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10. Systemic Effects of Prenatal Carotenoid Supplementation in the Mother and her Child: The Lutein and Zeaxanthin in Pregnancy (L-ZIP) Randomized Trial —Report Number 1
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Addo, Emmanuel K., Allman, Susan J., Arunkumar, Ranganathan, Gorka, Joanna E., Harrison, Deborah Y., Varner, Michael W., and Bernstein, Paul S.
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- 2023
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11. Antenatal Steroids and Cord Blood T-cell Glucocorticoid Receptor DNA Methylation and Exon 1 Splicing
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Carpenter, Jeanette R., Jablonski, Kathleen A., Koncinsky, Jordan, Varner, Michael W., Gyamfi-Bannerman, Cynthia, and Joss-Moore, Lisa A.
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- 2022
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12. Amniocentesis to diagnose congenital cytomegalovirus infection following maternal primary infection
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Dinsmoor, Mara J., Fette, Lida M., Hughes, Brenna L., Rouse, Dwight J., Saade, George R., Reddy, Uma M., Allard, Donna, Mallett, Gail, Thom, Elizabeth A., Gyamfi-Bannerman, Cynthia, Varner, Michael W., Goodnight, William H., Tita, Alan T.N., Costantine, Maged M., Swamy, Geeta K., Heyborne, Kent D., Chien, Edward K., Chauhan, Suneet P., El-Sayed, Yasser Y., Casey, Brian M., Parry, Samuel, Simhan, Hyagriv N., Napolitano, Peter G., and Macones, George A.
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- 2022
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13. An evaluation of seasonal maternal–neonatal morbidity related to trainee cycles
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Oben, Ayamo, McGee, Paula, Grobman, William A., Bailit, Jennifer L., Wapner, Ronald J., Varner, Michael W., Thorp, John M., Jr, Caritis, Steve N., Prasad, Mona, Saade, George R., Rouse, Dwight J., and Blackwell, Sean C.
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- 2022
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14. Overall and sex-specific risk factors for subjective cognitive decline: findings from the 2015–2018 Behavioral Risk Factor Surveillance System Survey
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Schliep, Karen C., Barbeau, William A., Lynch, Kristine E., Sorweid, Michelle K., Varner, Michael W., Foster, Norman L., and Qeadan, Fares
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- 2022
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15. Predicting the onset of Alzheimer’s disease and related dementia using Electronic Health Records: Findings from the Cache County Study on Memory in Aging (1995–2008)
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Schliep, Karen C., primary, Thornhill, Jeffrey, additional, Tschanz, JoAnn, additional, Facelli, Julio C., additional, Østbye, Truls, additional, Sorweid, Michelle K., additional, Smith, Ken R., additional, Varner, Michael, additional, Boyce, Richard D., additional, Brown, Christine J. Cliatt, additional, Meeks, Huong, additional, and Abdelrahman, Samir, additional
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- 2024
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16. Progression of Gestational Subclinical Hypothyroidism and Hypothyroxinemia to Overt Hypothyroidism After Pregnancy: Pooled Analysis of Data from Two Randomized Controlled Trials.
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Varner, Michael W., Mele, Lisa, Casey, Brian M., Peaceman, Alan M., Reddy, Uma M., Wapner, Ronald J., Thorp, John M., Saade, George R., Tita, Alan T. N., Rouse, Dwight J., Sibai, Baha M., Costantine, Maged M., Mercer, Brian M., and Caritis, Steve N.
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IODIDE peroxidase , *HYPOTHYROIDISM , *ODDS ratio , *SECONDARY analysis , *CONFIDENCE intervals - Abstract
Background: To examine the incidence of overt hypothyroidism 1 and 5 years after pregnancies where screening before 21 weeks identified subclinical hypothyroidism (SH) or hypothyroxinemia (HT). Methods: Secondary analysis of two multicenter treatment trials for either SH or HT diagnosed between 8 and 20 weeks gestation. Current analyses focus only on individuals randomized to the placebo groups in the two parallel studies. SH was diagnosed with thyrotropin (TSH) ≥4.0 mU/L and normal free T4 (fT4) (0.86–1.9 ng/dL). HT was diagnosed with normal TSH (0.08–3.99 mU/L) but fT4 <0.86 ng/dL. Serum from initial testing was stored for later thyroid peroxidase (TPO) antibody assay; results were not returned for clinical management. At 1 and 5 years after delivery, participants were asked whether they had either been diagnosed with or were being treated for a thyroid condition. Maternal serum was collected at these visits and thyroid function measured. Subsequent overt hypothyroidism was defined as TSH ≥4.0 mU/L with fT4 <0.86 ng/dL. Results: Data for 1- and 5-year follow-up were available in 307 of the 338 participants with SH and 229 of the 261 with HT. Subsequent hypothyroidism was more common both at year 1 (13.4% vs. 3.1%, p < 0.001) and year 5 (15.6% vs. 2.6%, p < 0.001) for participants with SH compared with those with HT. This progression was more common in individuals with TSH values >10 mIU/mL. Baseline TPO level >50 IU/mL in participants with SH was associated with higher rates of hypothyroidism at year 1 (26.7% vs. 6.5%, odds ratio [OR] = 5.3 [confidence interval (CI) 2.6–10.7]) and year 5 (30.5% vs. 7.5%, OR = 5.4 [CI: 2.8–10.6]) compared with those with TPO levels ≤50 IU/mL. For participants with HT, no differences in overt hypothyroidism were seen at 1 year related to baseline TPO level >50 IU/mL (1/10 (10%) vs. 6/218 (2.8%), OR = 3.9 [CI: 0.43–36.1]), but more participants with TPO levels >50 IU/mL developed hypothyroidism by year 5 (2/10 (20%) vs. 4/218 (1.8%), OR = 13.4 [CI: 2.1–84.1]). Conclusion: SH is associated with higher rates of overt hypothyroidism or thyroid replacement therapy within 5 years of delivery than is HT when these conditions are diagnosed in the first half of pregnancy. [ABSTRACT FROM AUTHOR]
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- 2024
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17. Low‐dose aspirin, maternal cardiometabolic health, and offspring respiratory health 9 to 14 years after delivery: Findings from the EAGeR Follow‐up Study.
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Shaaban, May, Shepelak, Zachary D., Stanford, Joseph B., Silver, Robert M., Mumford, Sunni L., Schisterman, Enrique F., Hinkle, Stefanie N., Nkoy, Flory L., Theilen, Lauren, Page, Jessica, Woo, Jessica G., Brown, Benjamin H., Varner, Michael W., and Schliep, Karen C.
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MISCARRIAGE ,CHILDREN'S health ,MATERNAL health ,ASPIRIN ,HYPERCHOLESTEREMIA - Abstract
Background: Accumulating evidence shows that peri‐conceptional and in‐utero exposures have lifetime health impacts for mothers and their offspring. Objectives: We conducted a Follow‐Up Study of the Effects of Aspirin in Gestation and Reproduction (EAGeR) trial with two objectives. First, we determined if women who enrolled at the Utah site (N = 1001) of the EAGeR trial (2007–2011, N = 1228) could successfully be contacted and agree to complete an online questionnaire on their reproductive, cardio‐metabolic, and offspring respiratory health 9–14 years after original enrollment. Second, we evaluated if maternal exposure to low‐dose aspirin (LDA) during pregnancy was associated with maternal cardio‐metabolic health and offspring respiratory health. Methods: The original EAGeR study population included women, 18–40 years of age, who had 1–2 prior pregnancy losses, and who were trying to become pregnant. At follow‐up (2020–2021), participants from the Utah cohort completed a 13‐item online questionnaire on reproductive and cardio‐metabolic health, and those who had a live birth during EAGeR additionally completed a 7‐item questionnaire on the index child's respiratory health. Primary maternal outcomes included hypertension and hypercholesterolemia; primary offspring outcomes included wheezing and asthma. Results: Sixty‐eight percent (n = 678) of participants enrolled in the follow‐up study, with 10% and 15% reporting maternal hypertension and hypercholesterolemia, respectively; and 18% and 10% reporting offspring wheezing and asthma. We found no association between maternal LDA exposure and hypertension (risk difference [RD] −0.001, 95% confidence interval [CI] −0.05, 0.04) or hypercholesterolemia (RD −0.01, 95% CI −0.06, 0.05) at 9–14 years follow‐up. Maternal LDA exposure was not associated with offspring wheezing (RD −0.002, 95% CI −0.08, 0.08) or asthma (RD 0.13, 95% CI 0.11, 0.37) at follow‐up. Findings remained robust after considering potential confounding and selection bias. Conclusions: We observed no association between LDA exposure during pregnancy and maternal cardiometabolic or offspring respiratory health. [ABSTRACT FROM AUTHOR]
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- 2024
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18. Endometriosis Typology and Ovarian Cancer Risk.
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Barnard, Mollie E., Farland, Leslie V., Yan, Bin, Wang, Jing, Trabert, Britton, Doherty, Jennifer A., Meeks, Huong D., Madsen, Myke, Guinto, Emily, Collin, Lindsay J., Maurer, Kathryn A., Page, Jessica M., Kiser, Amber C., Varner, Michael W., Allen-Brady, Kristina, Pollack, Anna Z., Peterson, Kurt R., Peterson, C. Matthew, and Schliep, Karen C.
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OVARIAN cancer ,SALPINGECTOMY ,DISEASE risk factors ,ENDOMETRIOSIS ,ELECTRONIC health records ,CANCER patients ,REPRODUCTIVE history - Abstract
Key Points: Question: How do endometriosis subtypes influence ovarian cancer risk? Findings: Women with endometriosis had 4.2-fold higher ovarian cancer risk than those without endometriosis. Women with ovarian endometriomas and/or deep infiltrating endometriosis, compared with no endometriosis, had 9.7-fold higher risk. Associations between endometriosis subtypes and ovarian cancer histotypes were much greater for type I (endometrioid, clear cell, mucinous, and low-grade serous) compared with type II (high-grade serous) ovarian cancers. Meaning: Women with endometriosis, especially more severe subtypes, have a markedly increased ovarian cancer risk and may be an important population for targeted cancer screening and prevention studies. Importance: Endometriosis has been associated with an increased risk of ovarian cancer; however, the associations between endometriosis subtypes and ovarian cancer histotypes have not been well-described. Objective: To evaluate the associations of endometriosis subtypes with incidence of ovarian cancer, both overall and by histotype. Design, Setting, and Participants: Population-based cohort study using data from the Utah Population Database. The cohort was assembled by matching 78 893 women with endometriosis in a 1:5 ratio to women without endometriosis. Exposures: Endometriosis cases were identified via electronic health records and categorized as superficial endometriosis, ovarian endometriomas, deep infiltrating endometriosis, or other. Main Outcomes and Measures: Estimated adjusted hazard ratios (aHRs), adjusted risk differences (aRDs) per 10 000 women, and 95% CIs for overall ovarian cancer, type I ovarian cancer, and type II ovarian cancer comparing women with each type of endometriosis with women without endometriosis. Models accounted for sociodemographic factors, reproductive history, and past gynecologic operations. Results: In this Utah-based cohort, the mean (SD) age at first endometriosis diagnosis was 36 (10) years. There were 597 women with ovarian cancer. Ovarian cancer risk was higher among women with endometriosis compared with women without endometriosis (aHR, 4.20 [95% CI, 3.59-4.91]; aRD, 9.90 [95% CI, 7.22-12.57]), and risk of type I ovarian cancer was especially high (aHR, 7.48 [95% CI, 5.80-9.65]; aRD, 7.53 [95% CI, 5.46-9.61]). Ovarian cancer risk was highest in women with deep infiltrating endometriosis and/or ovarian endometriomas for all ovarian cancers (aHR, 9.66 [95% CI, 7.77-12.00]; aRD, 26.71 [95% CI, 20.01-33.41]), type I ovarian cancer (aHR, 18.96 [95% CI, 13.78-26.08]; aRD, 19.57 [95% CI, 13.80-25.35]), and type II ovarian cancer (aHR, 3.72 [95% CI, 2.31-5.98]; aRD, 2.42 [95% CI, −0.01 to 4.85]). Conclusions and Relevance: Ovarian cancer risk was markedly increased among women with ovarian endometriomas and/or deep infiltrating endometriosis. This population may benefit from counseling regarding ovarian cancer risk and prevention and could be an important population for targeted screening and prevention studies. This population-based cohort study investigates ovarian cancer risk in women with vs without endometriosis and the association between ovarian cancer histotypes and endometriosis subtypes. [ABSTRACT FROM AUTHOR]
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- 2024
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19. Is less more? Examining the relationship between food assistance benefit levels and childhood weight
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Reynolds, Megan M., Fox, Ashley M., Wen, Ming, and Varner, Michael W.
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- 2020
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20. Early Cardiac and Cerebral Hemodynamics with Umbilical Cord Milking Compared with Delayed Cord Clamping in Infants Born Preterm
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Katheria, Anup C., Szychowski, Jeff M., Essers, Jochen, Mendler, Marc R., Dempsey, Eugene M., Schmölzer, Georg M., Arnell, Kathy, Rich, Wade D., Hassen, Kasim, Allman, Phillip, Varner, Michael, Cutter, Gary R., and Finer, Neil
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- 2020
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21. Optimal timing of antenatal corticosteroid administration and preterm neonatal and early childhood outcomes
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Battarbee, Ashley N., Ros, Stephanie T., Esplin, M. Sean, Biggio, Joseph, Bukowski, Radek, Parry, Samuel, Zhang, Heping, Huang, Hao, Andrews, William, Saade, George, Sadovsky, Yoel, Reddy, Uma M., Varner, Michael W., and Manuck, Tracy A.
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- 2020
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22. Physical and cultural determinants of postpartum pelvic floor support and symptoms following vaginal delivery: a protocol for a mixed-methods prospective cohort study.
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Nygaard, Ingrid E, Clark, Erin, Clark, Lauren, Egger, Marlene J, Hitchcock, Robert, Hsu, Yvonne, Norton, Peggy, Sanchez-Birkhead, Ana, Shaw, Janet, Sheng, Xiaoming, and Varner, Michael
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Pelvic Floor ,Humans ,Fecal Incontinence ,Urinary Incontinence ,Delivery ,Obstetric ,Prospective Studies ,Postpartum Period ,Pregnancy ,Parturition ,Qualitative Research ,Cultural Characteristics ,Quality of Life ,Adult ,Utah ,Female ,Sexual Dysfunction ,Physiological ,Muscle Strength ,Pelvic Organ Prolapse ,Pelvic Floor Disorders ,Social Determinants of Health ,Pelvic organ prolapse ,childbirth injury ,intra-abdominal pressure ,pelvic floor disorders ,physical activity ,urinary incontinence ,Delivery ,Obstetric ,Sexual Dysfunction ,Physiological ,Clinical Sciences ,Public Health and Health Services ,Other Medical and Health Sciences - Abstract
IntroductionPelvic floor disorders (PFDs), including pelvic organ prolapse (POP), stress and urgency urinary incontinence, and faecal incontinence, are common and arise from loss of pelvic support. Although severe disease often does not occur until women become older, pregnancy and childbirth are major risk factors for PFDs, especially POP. We understand little about modifiable factors that impact pelvic floor function recovery after vaginal birth. This National Institutes of Health (NIH)-funded Program Project, 'Bridging physical and cultural determinants of postpartum pelvic floor support and symptoms following vaginal delivery', uses mixed-methods research to study the influences of intra-abdominal pressure, physical activity, body habitus and muscle fitness on pelvic floor support and symptoms as well as the cultural context in which women experience those changes.Methods and analysisUsing quantitative methods, we will evaluate whether pelvic floor support and symptoms 1 year after the first vaginal delivery are affected by biologically plausible factors that may impact muscle, nerve and connective tissue healing during recovery (first 8 weeks postpartum) and strengthening (remainder of the first postpartum year). Using qualitative methods, we will examine cultural aspects of perceptions, explanations of changes in pelvic floor support, and actions taken by Mexican-American and Euro-American primipara, emphasising early changes after childbirth. We will summarise project results in a resource toolkit that will enhance opportunities for dialogue between women, their families and providers, and across lay and medical discourses. We anticipate enrolling up to 1530 nulliparous women into the prospective cohort study during the third trimester, following those who deliver vaginally 1 year postpartum. Participants will be drawn from this cohort to meet the project's aims.Ethics and disseminationThe University of Utah and Intermountain Healthcare Institutional Review Boards approved this study. Data are stored in a secure password-protected database. Papers summarising the primary results and ancillary analyses will be published in peer-reviewed journals.
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- 2017
23. Onset of human preterm and term birth is related to unique inflammatory transcriptome profiles at the maternal fetal interface
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Bukowski, Radek, Sadovsky, Yoel, Goodarzi, Hani, Zhang, Heping, Biggio, Joseph R, Varner, Michael, Parry, Samuel, Xiao, Feifei, Esplin, Sean M, Andrews, William, Saade, George R, Ilekis, John V, Reddy, Uma M, and Baldwin, Donald A
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Biological Sciences ,Biomedical and Clinical Sciences ,Bioinformatics and Computational Biology ,Midwifery ,Health Sciences ,Reproductive Medicine ,Clinical Research ,Preterm ,Low Birth Weight and Health of the Newborn ,Pediatric ,Human Genome ,Genetics ,Contraception/Reproduction ,Infant Mortality ,Perinatal Period - Conditions Originating in Perinatal Period ,Aetiology ,2.1 Biological and endogenous factors ,Reproductive health and childbirth ,Good Health and Well Being ,Pregnancy ,Pretrem labor ,Labor ,Gene expression ,Transcriptomics ,Medical and Health Sciences - Abstract
BackgroundPreterm birth is a main determinant of neonatal mortality and morbidity and a major contributor to the overall mortality and burden of disease. However, research of the preterm birth is hindered by the imprecise definition of the clinical phenotype and complexity of the molecular phenotype due to multiple pregnancy tissue types and molecular processes that may contribute to the preterm birth. Here we comprehensively evaluate the mRNA transcriptome that characterizes preterm and term labor in tissues comprising the pregnancy using precisely phenotyped samples. The four complementary phenotypes together provide comprehensive insight into preterm and term parturition.MethodsSamples of maternal blood, chorion, amnion, placenta, decidua, fetal blood, and myometrium from the uterine fundus and lower segment (n = 183) were obtained during cesarean delivery from women with four complementary phenotypes: delivering preterm with (PL) and without labor (PNL), term with (TL) and without labor (TNL). Enrolled were 35 pregnant women with four precisely and prospectively defined phenotypes: PL (n = 8), PNL (n = 10), TL (n = 7) and TNL (n = 10). Gene expression data were analyzed using shrunken centroid analysis to identify a minimal set of genes that uniquely characterizes each of the four phenotypes. Expression profiles of 73 genes and non-coding RNA sequences uniquely identified each of the four phenotypes. The shrunken centroid analysis and 10 times 10-fold cross-validation was also used to minimize false positive finings and overfitting. Identified were the pathways and molecular processes associated with and the cis-regulatory elements in gene's 5' promoter or 3'-UTR regions of the set of genes which expression uniquely characterized the four phenotypes.ResultsThe largest differences in gene expression among the four groups occurred at maternal fetal interface in decidua, chorion and amnion. The gene expression profiles showed suppression of chemokines expression in TNL, withdrawal of this suppression in TL, activation of multiple pathways of inflammation in PL, and an immune rejection profile in PNL. The genes constituting expression signatures showed over-representation of three putative regulatory elements in their 5'and 3' UTR regions.ConclusionsThe results suggest that pregnancy is maintained by downregulation of chemokines at the maternal-fetal interface. Withdrawal of this downregulation results in the term birth and its overriding by the activation of multiple pathways of the immune system in the preterm birth. Complications of the pregnancy associated with impairment of placental function, which necessitated premature delivery of the fetus in the absence of labor, show gene expression patterns associated with immune rejection.
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- 2017
24. Umbilical Cord Collection and Drug Testing to Estimate Prenatal Substance Exposure in Utah
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Smid, Marcela C., Allshouse, Amanda A., McMillin, Gwendolyn A., Nunez, Kendyl, Cavin, Tyler, Worden, Joseph, Buchi, Karen, Muniyappa, Bhanu, Varner, Michael W., Cochran, Gerald, and Metz, Torri D.
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- 2022
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25. 26 - Pregnancy as a Window to Future Maternal and Child Health
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Theilen, Lauren H., Adesomo, Adebayo A., and Varner, Michael W.
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- 2025
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26. Umbilical cord milking in nonvigorous infants: a cluster-randomized crossover trial
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Katheria, Anup C., Clark, Erin, Yoder, Bradley, Schmölzer, Georg M., Yan Law, Brenda Hiu, El-Naggar, Walid, Rittenberg, David, Sheth, Sheetal, Mohamed, Mohamed A., Martin, Courtney, Vora, Farha, Lakshminrusimha, Satyan, Underwood, Mark, Mazela, Jan, Kaempf, Joseph, Tomlinson, Mark, Gollin, Yvonne, Fulford, Kevin, Goff, Yvonne, Wozniak, Paul, Baker, Katherine, Rich, Wade, Morales, Ana, Varner, Michael, Poeltler, Debra, Vaucher, Yvonne, Mercer, Judith, Finer, Neil, El Ghormli, Laure, and Rice, Madeline Murguia
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- 2023
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27. Is immunohistochemistry-based screening for Lynch syndrome in endometrial cancer effective? The consent's the thing
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Gudgeon, James M., Varner, Michael W., Hashibe, Mia, and Williams, Marc S.
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- 2019
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28. Noninvasive Prediction of Congenital Cytomegalovirus Infection After Maternal Primary Infection
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Rouse, Dwight J., Fette, Lida M., Hughes, Brenna L., Saade, George R., Dinsmoor, Mara J., Reddy, Uma M., Pass, Robert, Allard, Donna, Mallett, Gail, Clifton, Rebecca G., Saccoccio, Frances M., Permar, Sallie R., Gyamfi-Bannerman, Cynthia, Varner, Michael W., Goodnight, William H., Tita, Alan T. N., Costantine, Maged M., Swamy, Geeta K., Heyborne, Kent D., Chien, Edward K., Chauhan, Suneet P., El-Sayed, Yasser Y., Casey, Brian M., Parry, Samuel, Simhan, Hyagriv N., Napolitano, Peter G., and Macones, George A.
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- 2022
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29. Impaired Awareness of Hypoglycemia Continues to be a Risk Factor for Severe Hypoglycemia Despite the Use of Continuous Glucose Monitoring System in Type 1 Diabetes
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Lin, Yu Kuei, Hung, Man, Sharma, Anu, Chan, Owen, Varner, Michael W., Staskus, Gitana, and Fisher, Simon J.
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- 2019
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30. Principles of Pharmacokinetics in the Pregnant Woman and Fetus
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Ward, Robert M. and Varner, Michael W.
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- 2019
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31. Exploring the associations between microRNA expression profiles and environmental pollutants in human placenta from the National Children's Study (NCS).
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Li, Qian, Kappil, Maya A, Li, An, Dassanayake, Priyanthi S, Darrah, Thomas H, Friedman, Alan E, Friedman, Michelle, Lambertini, Luca, Landrigan, Philip, Stodgell, Christopher J, Xia, Yulin, Nanes, Jessica A, Aagaard, Kjersti M, Schadt, Eric E, Murray, Jeff C, Clark, Edward B, Dole, Nancy, Culhane, Jennifer, Swanson, James, Varner, Michael, Moye, Jack, Kasten, Carol, Miller, Richard K, and Chen, Jia
- Subjects
Placenta ,Humans ,Arsenic ,Cadmium ,Lead ,Mercury ,Benzhydryl Compounds ,Polychlorinated Biphenyls ,Dichlorodiphenyldichloroethane ,Phenols ,MicroRNAs ,Environmental Pollutants ,Gene Expression Regulation ,Pregnancy ,Female ,Male ,Halogenated Diphenyl Ethers ,Genetic Association Studies ,birth cohort ,environmental pollutants ,epigenetics ,microRNA ,placenta ,Pediatric ,Pediatric Research Initiative ,Biotechnology ,Genetics ,Clinical Research ,Biochemistry and Cell Biology ,Medical Biochemistry and Metabolomics ,Developmental Biology - Abstract
The placenta is the principal regulator of the in utero environment, and disruptions to this environment can result in adverse offspring health outcomes. To better characterize the impact of in utero perturbations, we assessed the influence of known environmental pollutants on the expression of microRNA (miRNA) in placental samples collected from the National Children's Study (NCS) Vanguard birth cohort. This study analyzed the expression of 654 miRNAs in 110 term placentas. Environmental pollutants measured in these placentas included dichlorodiphenyldichloroethylene (DDE), bisphenol A (BPA), polybrominated diphenyl ethers (PBDEs), polychlorinated biphenyls (PCBs), arsenic (As), mercury (Hg), lead (Pb), and cadmium (Cd). A moderated t-test was used to identify a panel of differentially expressed miRNAs, which were further analyzed using generalized linear models. We observed 112 miRNAs consistently expressed in >70% of the samples. Consistent with the literature, miRNAs located within the imprinted placenta-specific C19MC cluster, specifically mir-517a, mir-517c, mir-522, and mir-23a, are among the top expressed miRNA in our study. We observed a positive association between PBDE 209 and miR-188-5p and an inverse association between PBDE 99 and let-7c. Both PCBs and Cd were positively associated with miR-1537 expression level. In addition, multiple let-7 family members were downregulated with increasing levels of Hg and Pb. We did not observe DDE or BPA levels to be associated with placental miRNA expression. This is the first birth cohort study linking environmental pollutants and placental expression of miRNAs. Our results suggest that placental miRNA profiles may signal in utero exposures to environmental chemicals.
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- 2015
32. A Trial of Hyperimmune Globulin to Prevent Congenital Cytomegalovirus Infection
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Hughes, Brenna L., Clifton, Rebecca G., Rouse, Dwight J., Saade, George R., Dinsmoor, Mara J., Reddy, Uma M., Pass, Robert, Allard, Donna, Mallett, Gail, Fette, Lida M., Gyamfi-Bannerman, Cynthia, Varner, Michael W., Goodnight, William H., Tita, Alan T. N., Costantine, Maged M., Swamy, Geeta K., Gibbs, Ronald S., Chien, Edward K., Chauhan, Suneet P., El-Sayed, Yasser Y., Casey, Brian M., Parry, Samuel, Simhan, Hyagriv N., Napolitano, Peter G., and Macones, George A.
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- 2022
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33. 1172 The Integration of Prenatal Data Into the Neonatal Research Network (NRN) Survival Probability Estimator
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Varner, Michael W., primary
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- 2024
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34. LB02 Long Term Outcomes for The Milking In Non-Vigorous Infants (MINVI) Trial
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Katheria, Anup, primary, El Ghormli, Laure, additional, Clark, Erin A., additional, Yoder, Bradley, additional, Schmölzer, Georg, additional, Law, Brenda, additional, El-Naggar, Walid, additional, Rittenberg, David, additional, Sheth, Sheetal, additional, Martin, Courtney, additional, Vora, Farha, additional, Lakshminrusimha, Satyan, additional, Underwood, Mark, additional, Mazela, Jan, additional, Kaempf, Joseph, additional, Tomlinson, Mark, additional, Gollin, Yvonne, additional, Rich, Wade, additional, Morales, Ana, additional, Varner, Michael W., additional, Poeltler, Debra, additional, Vaucher, Yvonne, additional, Mercer, Judith, additional, Finer, Neil, additional, and Rice, Madeline, additional
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- 2024
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35. Source of variation in cost of obstetrical care for low-risk nulliparas at term
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Einerson, Brett D., primary, Allshouse, Amanda A., additional, Sandoval, Grecio, additional, Nelson, Richard E., additional, Esplin, M. Sean, additional, Varner, Michael, additional, Grobman, William A., additional, and Metz, Torri D., additional
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- 2024
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36. Comparison of Cesarean Deliveries in a Multicenter U.S. Cohort Using the 10-Group Classification System.
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Pasko, Daniel N., McGee, Paula, Grobman, William A., Bailit, Jennifer L., Reddy, Uma M., Wapner, Ronald J., Varner, Michael W., Thorp Jr., John M., Caritis, Steve N., Prasad, Mona, Saade, George R., Sorokin, Yoram, Rouse, Dwight J., and Tolosa, Jorge E.
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CESAREAN section ,SECONDARY analysis ,DATA analysis ,RESEARCH funding ,LOGISTIC regression analysis ,HOSPITALS ,DESCRIPTIVE statistics ,INDUCED labor (Obstetrics) ,STATISTICS ,RESEARCH ,COMPARATIVE studies ,FETAL presentation - Abstract
Objective We sought to (1) use the Robson 10-Group Classification System (TGCS), which classifies deliveries into 10 mutually exclusive groups, to characterize the groups that are primary contributors to cesarean delivery frequencies, (2) describe inter-hospital variations in cesarean delivery frequencies, and (3) evaluate the contribution of patient characteristics by TGCS group to hospital variation in cesarean delivery frequencies. Study Design This was a secondary analysis of an observational cohort of 115,502 deliveries from 25 hospitals between 2008 and 2011. The TGCS was applied to the cohort and each hospital. We identified and compared the TGCS groups with the greatest relative contributions to cohort and hospital cesarean delivery frequencies. We assessed variation in hospital cesarean deliveries attributable to patient characteristics within TGCS groups using hierarchical logistic regression. Results A total of 115,211 patients were classifiable in the TGCS (99.7%). The cohort cesarean delivery frequency was 31.4% (hospital range: 19.1–39.3%). Term singletons in vertex presentation with a prior cesarean delivery (group 5) were the greatest relative contributor to cohort (34.8%) and hospital cesarean delivery frequencies (median: 33.6%; range: 23.8–45.5%). Nulliparous term singletons in vertex (NTSV) presentation (groups 1 [spontaneous labor] and 2 [induced or absent labor]: 28.9%), term singletons in vertex presentation with a prior cesarean delivery (group 5: 34.8%), and preterm singletons in vertex presentation (group 10: 9.8%) contributed to 73.2% of the relative cesarean delivery frequency for the cohort and were correlated with hospital cesarean delivery frequencies (Spearman's rho = 0.96). Differences in patient characteristics accounted for 34.1% of hospital-level cesarean delivery variation in group 2. Conclusion The TGCS highlights the contribution of NTSV presentation to cesarean delivery frequencies and the impact of patient characteristics on hospital-level variation in cesarean deliveries among nulliparous patients with induced or absent labor. Key Points We report on the cesarean delivery frequencies in a multicenter U.S. cohort. NTSV gestations (groups 1 and 2) are a primary driver of cesarean deliveries. Patient characteristics contributed most to hospital variation in cesarean deliveries in group 2. [ABSTRACT FROM AUTHOR]
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- 2024
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37. Association of Maternal Body Mass Index and Maternal Morbidity And Mortality.
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Dinsmoor, Mara J., Ugwu, Lynda G., Bailit, Jennifer L., Reddy, Uma M., Wapner, Ronald J., Varner, Michael W., Thorp Jr., John M., Caritis, Steve N., Prasad, Mona, Tita, Alan T.N., Saade, George R., Sorokin, Yoram, Rouse, Dwight J., Blackwell, Sean C., and Tolosa, Jorge E.
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POISSON distribution ,BODY mass index ,SECONDARY analysis ,RESEARCH funding ,HYPERTENSION ,SMOKING ,MATERNAL mortality ,CAUSES of death ,MULTIVARIATE analysis ,DESCRIPTIVE statistics ,DISEASES ,LONGITUDINAL method ,INTENSIVE care units ,PARITY (Obstetrics) ,CONFIDENCE intervals ,OBESITY ,REGRESSION analysis ,PREGNANCY - Abstract
Objective This study aimed to assess the association of maternal body mass index (BMI) with a composite of severe maternal outcomes. Study Design Secondary analysis of a cohort of deliveries on randomly selected days at 25 hospitals from 2008 to 2011. Data on comorbid conditions, intrapartum events, and postpartum course were collected. The reference group (REF, BMI: 18.5–29.9kg/m
2 ), obese (OB; BMI: 30–39.9kg/m2 ), morbidly obese (MO; BMI: 40–49.9kg/m2 ), and super morbidly obese (SMO; BMI ≥ 50kg/m2 ) women were compared. The composite of severe maternal outcomes was defined as death, intensive care unit (ICU) admission, ventilator use, deep venous thrombosis/pulmonary embolus (DVT/PE), sepsis, hemorrhage, disseminated intravascular coagulation (DIC), unplanned operative procedure, or stroke. Patients in the REF group were matched 1:1 with those in all other obesity groups based on propensity score using the baseline characteristics of age, race/ethnicity, previous cesarean, preexisting diabetes, chronic hypertension, parity, cigarette use, and insurance status. Multivariable Poisson's regression was used to estimate adjusted relative risks (aRRs) and 95% confidence intervals (CIs) for the association between BMI and the composite outcome. Because cesarean delivery may be in the causal pathway between obesity and adverse maternal outcomes, models were then adjusted for mode of delivery to evaluate potential mediation. Results A total of 52,162 pregnant patients are included in the analysis. Risk of composite maternal outcomes was increased for SMO compared with REF but not for OB and MO [OB: aRR=1.06, 95% CI: 0.99–1.14; MO: aRR=1.10, 95% CI: 0.97–1.25; SMO: aRR=1.32, 95% CI: 1.02–1.70]. However, in the mediation analysis, cesarean appears to mediate 46% (95% CI: 31–50%) of the risk of severe morbidity for SMO compared with REF. Conclusion Super morbid obesity is significantly associated with increased serious maternal morbidity and mortality; however, cesarean appears to mediate this association. Obesity and morbid obesity are not associated with maternal morbidity and mortality. Key Points Super morbid obesity is associated with increased morbidity. Cesarean appears to mediate the association between super morbid obesity and morbidity. Obesity and morbid maternal obesity are not associated with morbidity. [ABSTRACT FROM AUTHOR]- Published
- 2024
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38. DLK1: A Novel Biomarker of Placental Insufficiency in Stillbirth and Live Birth.
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Page, Jessica M., Allshouse, Amanda A., Gaffney, Jessica E., Roberts, Victoria H. J., Thorsten, Vanessa, Gibbins, Karen J., Dudley, Donald J., Saade, George, Goldenberg, Robert L., Stoll, Barbara J., Hogue, Carol J., Bukowski, Radek, Parker, Corette, Conway, Deborah, Reddy, Uma M., Varner, Michael W., Frias, Antonio E., and Silver, Robert M.
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FETAL malnutrition ,CROSS-sectional method ,PLACENTA ,SMALL for gestational age ,CALCIUM-binding proteins ,FETAL growth retardation ,LOGISTIC regression analysis ,ENZYME-linked immunosorbent assay ,PREGNANCY outcomes ,PERINATAL death ,DESCRIPTIVE statistics ,ODDS ratio ,GESTATIONAL age ,RESEARCH ,GROWTH factors ,COMPARATIVE studies ,BIOMARKERS ,MEMBRANE proteins ,REGRESSION analysis - Abstract
Objective Delta-like homolog 1 (DLK1) is a growth factor that is reduced in maternal sera in pregnancies with small for gestational age neonates. We sought to determine if DLK1 is associated with stillbirth (SB), with and without placental insufficiency. Study Design A nested case-control study was performed using maternal sera from a multicenter case-control study of SB and live birth (LB). SB and LB were stratified as placental insufficiency cases (small for gestational age <5% or circulatory lesions on placental histopathology) or normal placenta controls (appropriate for gestational age and no circulatory lesions). Enzyme-linked immunosorbent assay (ELISA) was used to measure DLK1. The mean difference in DLK1 was compared on the log scale in an adjusted linear regression model with pairwise differences, stratified by term/preterm deliveries among DLK1 results in the quantifiable range. In exploratory analysis, geometric means were compared among all data and the proportion of "low DLK1" (less than the median value for gestational age) was compared between groups and modeled using linear and logistic regression, respectively. Results Overall, 234 SB and 234 LB were analyzed; 246 DLK1 values were quantifiable within the standard curve. Pairwise comparisons of case and control DLK1 geometric means showed no significant differences between groups. In exploratory analysis of all data, adjusted analysis revealed a significant difference for the LB comparison only (SB: 71.9 vs. 99.1 pg/mL, p = 0.097; LB: 37.6 vs. 98.1 pg/mL, p = 0.005). In exploratory analysis of "low DLK1," there was a significant difference between the odds ratio of having "low DLK1" between preterm cases and controls for both SB and LB. There were no significant differences in geometric means nor "low DLK1" between SB and LB. Conclusion In exploratory analysis, more placental insufficiency cases in preterm SB and LB had "low DLK1." However, low DLK1 levels were not associated with SB. Key Points Maternally circulating DLK1 is correlated with placental insufficiency. Maternally circulating DLK1 is not correlated with SB. DLK1 is a promising marker for placental insufficiency. [ABSTRACT FROM AUTHOR]
- Published
- 2024
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39. Outcomes in Twins Compared With Singletons Subsequent to Preterm Prelabor Rupture of Membranes
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Fishel Bartal, Michal, Ugwu, Lynda G., Grobman, William A., Bailit, Jennifer L., Reddy, Uma M., Wapner, Ronald J., Varner, Michael W., Thorp, John M., Jr, Caritis, Steve N., Prasad, Mona, Tita, Alan T. N., Saade, George R., and Rouse, Dwight J.
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- 2021
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40. Thrombotic markers in pregnant patients with and without SARS-CoV-2 infection
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Bruno, Ann, additional, Allshouse, Amanda, additional, Benson, Ashley E, additional, Yost, Christian, additional, Metz, Torri, additional, Varner, Michael, additional, Silver, Robert M, additional, and Branch, D. Ware, additional
- Published
- 2023
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41. Umbilical Cord Milking Versus Delayed Cord Clamping in Infants 28 to 32 Weeks: A Randomized Trial
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Katheria, Anup, primary, Szychowski, Jeff, additional, Carlo, Waldemar A, additional, Subramaniam, Akila, additional, Reister, Frank, additional, Essers, Jochen, additional, Vora, Farha, additional, Martin, Courtney, additional, Schmölzer, Georg M., additional, Law, Brenda, additional, Dempsey, Eugene, additional, O’Donoghue, Keelin, additional, Kaempf, Joseph, additional, Tomlinson, Mark, additional, Fulford, Kevin, additional, Folsom, Bergen, additional, Karam, Simon, additional, Morris, Rachael, additional, Yanowitz, Toby, additional, Beck, Stacy, additional, Clark, Erin, additional, DuPont, Tara, additional, Biniwale, Manoj, additional, Ramanathan, Rangasamy, additional, Bhat, Shazia, additional, Hoffman, Matthew, additional, Chouthai, Nitin, additional, Bany-Mohammed, Fayez, additional, Mydam, Janardhan, additional, Narendran, Vivek, additional, Wertheimer, Fiona, additional, Gollin, Yvonne, additional, Vaucher, Yvonne, additional, Arnell, Kathy, additional, Varner, Michael, additional, Cutter, Gary, additional, Wilson, Nicole, additional, Rich, Wade, additional, and Finer, Neil, additional
- Published
- 2023
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42. Intrapartum Resuscitation Interventions for Category II Fetal Heart Rate Tracings and Improvement to Category I
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Reddy, Uma M., Weiner, Steven J., Saade, George R., Varner, Michael W., Blackwell, Sean C., Thorp, John M., Jr, Tita, Alan T.N., Miller, Russell S., Peaceman, Alan M., McKenna, David S., Chien, Edward K. S., Rouse, Dwight J., El-Sayed, Yasser Y., Sorokin, Yoram, and Caritis, Steve N.
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- 2021
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43. Relationship Between Maternal Economic Vulnerability and Childhood Neurodevelopment at 2 and 5 Years of Life
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Premkumar, Ashish, Mele, Lisa, Casey, Brian M., Varner, Michael W., Sorokin, Yoram, Wapner, Ronald J., Thorp, John M., Jr, Saade, George R., Tita, Alan T.N., Rouse, Dwight J., Sibai, Baha, Costantine, Maged M., Mercer, Brian M., Tolosa, Jorge E., and Caritis, Steve N.
- Published
- 2021
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44. Hepatitis C Virus Antibody Screening in a Cohort of Pregnant Women: Identifying Seroprevalence and Risk Factors
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Prasad, Mona, Saade, George R., Sandoval, Grecio, Hughes, Brenna L., Reddy, Uma M., Mele, Lisa, Salazar, Ashley, Varner, Michael W., Gyamfi-Bannerman, Cynthia, Thorp, John M., Jr, Tita, Alan T. N., Swamy, Geeta K., Chien, Edward K., Casey, Brian M., Peaceman, Alan M., El-Sayed, Yasser Y., Iams, Jay D., Gibbs, Ronald S., Sibai, Baha, Wiese, Nicholas, Kamili, Saleem, and Macones, George A.
- Published
- 2020
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45. Effect of Thyroxine Therapy on Depressive Symptoms Among Women With Subclinical Hypothyroidism
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Costantine, Maged M., Smith, Karen, Thom, Elizabeth A., Casey, Brian M., Peaceman, Alan M., Varner, Michael W., Sorokin, Yoram, Reddy, Uma M., Wapner, Ronald J., Boggess, Kim, Tita, Alan T.N., Rouse, Dwight J., Sibai, Baha, Iams, Jay D., Mercer, Brian M., Tolosa, Jorge E., Caritis, Steve N., and VanDorsten, J. Peter
- Published
- 2020
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46. Risk-adjusted models for adverse obstetric outcomes and variation in risk-adjusted outcomes across hospitals
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Bailit, Jennifer L, Grobman, William A, Rice, Madeline Murguia, Spong, Catherine Y, Wapner, Ronald J, Varner, Michael W, Thorp, John M, Leveno, Kenneth J, Caritis, Steve N, Shubert, Phillip J, Tita, Alan T, Saade, George, Sorokin, Yoram, Rouse, Dwight J, Blackwell, Sean C, Tolosa, Jorge E, Van Dorsten, J Peter, and Network, Eunice Kennedy Shriver National Institute of Child Health and Human Development Maternal–Fetal Medicine Units
- Subjects
Reproductive Medicine ,Biomedical and Clinical Sciences ,Good Health and Well Being ,Adult ,Cohort Studies ,Delivery ,Obstetric ,Female ,Hospitals ,Humans ,Infant ,Newborn ,Lacerations ,Models ,Statistical ,Multivariate Analysis ,Obstetric Labor Complications ,Outcome Assessment ,Health Care ,Perineum ,Peripartum Period ,Postpartum Hemorrhage ,Pregnancy ,Pregnancy Complications ,Cardiovascular ,Pregnancy Complications ,Infectious ,Puerperal Infection ,Quality Improvement ,Risk Adjustment ,United States ,Venous Thromboembolism ,Young Adult ,obstetrics ,performance improvement ,quality ,risk adjustment ,Eunice Kennedy Shriver National Institute of Child Health and Human Development Maternal–Fetal Medicine Units Network ,Paediatrics and Reproductive Medicine ,Obstetrics & Reproductive Medicine ,Reproductive medicine - Abstract
ObjectiveRegulatory bodies and insurers evaluate hospital quality using obstetrical outcomes, however meaningful comparisons should take preexisting patient characteristics into account. Furthermore, if risk-adjusted outcomes are consistent within a hospital, fewer measures and resources would be needed to assess obstetrical quality. Our objective was to establish risk-adjusted models for 5 obstetric outcomes and assess hospital performance across these outcomes.Study designWe studied a cohort of 115,502 women and their neonates born in 25 hospitals in the United States from March 2008 through February 2011. Hospitals were ranked according to their unadjusted and risk-adjusted frequency of venous thromboembolism, postpartum hemorrhage, peripartum infection, severe perineal laceration, and a composite neonatal adverse outcome. Correlations between hospital risk-adjusted outcome frequencies were assessed.ResultsVenous thromboembolism occurred too infrequently (0.03%; 95% confidence interval [CI], 0.02-0.04%) for meaningful assessment. Other outcomes occurred frequently enough for assessment (postpartum hemorrhage, 2.29%; 95% CI, 2.20-2.38, peripartum infection, 5.06%; 95% CI, 4.93-5.19, severe perineal laceration at spontaneous vaginal delivery, 2.16%; 95% CI, 2.06-2.27, neonatal composite, 2.73%; 95% CI, 2.63-2.84). Although there was high concordance between unadjusted and adjusted hospital rankings, several individual hospitals had an adjusted rank that was substantially different (as much as 12 rank tiers) than their unadjusted rank. None of the correlations between hospital-adjusted outcome frequencies was significant. For example, the hospital with the lowest adjusted frequency of peripartum infection had the highest adjusted frequency of severe perineal laceration.ConclusionEvaluations based on a single risk-adjusted outcome cannot be generalized to overall hospital obstetric performance.
- Published
- 2013
47. Bisphenol A and phthalates and endometriosis: the Endometriosis: Natural History, Diagnosis and Outcomes Study.
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Buck Louis, Germaine, Peterson, C, Chen, Zhen, Sundaram, Rajeshwari, Stanford, Joseph, Varner, Michael, Kennedy, Anne, Sun, Liping, Wang, Lei, Guo, Ying, Kannan, Kurunthachalam, Giudice, Linda, Fujimoto, Victor, and Croughan, Mary
- Subjects
Adult ,Benzhydryl Compounds ,Biomarkers ,Cohort Studies ,Endometriosis ,Environmental Pollutants ,Female ,Humans ,Laparoscopy ,Phenols ,Phthalic Acids ,Treatment Outcome - Abstract
OBJECTIVE: To explore the relation between bisphenol A and 14 phthalate metabolites and endometriosis. DESIGN: Matched cohort design. SETTING: Fourteen clinical centers. PATIENT(S): The operative cohort comprised 495 women undergoing laparoscopy/laparotomy, whereas the population cohort comprised 131 women matched on age and residence. INTERVENTION(S): None. MAIN OUTCOME MEASURE(S): Surgically visualized or pelvic magnetic resonance imaging diagnosed endometriosis in the two cohorts, respectively. RESULT(S): Odds ratios (OR) and 95% confidence intervals (CIs) were estimated using logistic regression adjusting for age, body mass index, and creatinine. In the population cohort, six phthalate metabolites-mono-n-butyl phthalate, mono-[(2-carboxymethyl) hexyl] phthalate, mono (2-ethyl-5-carboxyphentyl) phthalate, mono (2-ethylhexyl) phthalate, mono (2-ethyl-5-hydroxyhexyl) phthalate, and mono (2-ethyl-5-oxohexyl) phthalate-were significantly associated with an approximately twofold increase in the odds of an endometriosis diagnosis. Two phthalates were associated with endometriosis in the operative cohort when restricting to visualized and histologic endometriosis (monooctyl phthalate; OR 1.38; 95% CI 1.10-1.72) or when restricting comparison women to those with a postoperative diagnosis of a normal pelvis [mono (2-ethylhexyl) phthalate; OR 1.35; 95% CI 1.03-1.78]. CONCLUSION(S): Select phthalates were associated with higher odds of an endometriosis diagnosis for women with magnetic resonance imaging-diagnosed endometriosis. The lack of consistency of findings across cohorts underscores the impact of methodology on findings.
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- 2013
48. Bisphenol A and phthalates and endometriosis: the Endometriosis: Natural History, Diagnosis and Outcomes Study
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Louis, Germaine M Buck, Peterson, C Matthew, Chen, Zhen, Croughan, Mary, Sundaram, Rajeshwari, Stanford, Joseph, Varner, Michael W, Kennedy, Anne, Giudice, Linda, Fujimoto, Victor Y, Sun, Liping, Wang, Lei, Guo, Ying, and Kannan, Kurunthachalam
- Subjects
Reproductive Medicine ,Biomedical and Clinical Sciences ,Prevention ,Clinical Research ,Contraception/Reproduction ,Endometriosis ,Pain Research ,Reproductive health and childbirth ,Adult ,Benzhydryl Compounds ,Biomarkers ,Cohort Studies ,Environmental Pollutants ,Female ,Humans ,Laparoscopy ,Phenols ,Phthalic Acids ,Treatment Outcome ,Bisphenol A ,endometriosis ,endocrine disrupting chemicals ,epidemiology ,phthalates ,Clinical Sciences ,Paediatrics and Reproductive Medicine ,Public Health and Health Services ,Obstetrics & Reproductive Medicine ,Reproductive medicine - Abstract
ObjectiveTo explore the relation between bisphenol A and 14 phthalate metabolites and endometriosis.DesignMatched cohort design.SettingFourteen clinical centers.Patient(s)The operative cohort comprised 495 women undergoing laparoscopy/laparotomy, whereas the population cohort comprised 131 women matched on age and residence.Intervention(s)None.Main outcome measure(s)Surgically visualized or pelvic magnetic resonance imaging diagnosed endometriosis in the two cohorts, respectively.Result(s)Odds ratios (OR) and 95% confidence intervals (CIs) were estimated using logistic regression adjusting for age, body mass index, and creatinine. In the population cohort, six phthalate metabolites-mono-n-butyl phthalate, mono-[(2-carboxymethyl) hexyl] phthalate, mono (2-ethyl-5-carboxyphentyl) phthalate, mono (2-ethylhexyl) phthalate, mono (2-ethyl-5-hydroxyhexyl) phthalate, and mono (2-ethyl-5-oxohexyl) phthalate-were significantly associated with an approximately twofold increase in the odds of an endometriosis diagnosis. Two phthalates were associated with endometriosis in the operative cohort when restricting to visualized and histologic endometriosis (monooctyl phthalate; OR 1.38; 95% CI 1.10-1.72) or when restricting comparison women to those with a postoperative diagnosis of a normal pelvis [mono (2-ethylhexyl) phthalate; OR 1.35; 95% CI 1.03-1.78].Conclusion(s)Select phthalates were associated with higher odds of an endometriosis diagnosis for women with magnetic resonance imaging-diagnosed endometriosis. The lack of consistency of findings across cohorts underscores the impact of methodology on findings.
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- 2013
49. Risk factors associated with endometriosis: importance of study population for characterizing disease in the ENDO Study.
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Peterson, C Matthew, Johnstone, Erica B, Hammoud, Ahmad O, Stanford, Joseph B, Varner, Michael W, Kennedy, Anne, Chen, Zhen, Sun, Liping, Fujimoto, Victor Y, Hediger, Mary L, Buck Louis, Germaine M, and ENDO Study Working Group
- Subjects
ENDO Study Working Group ,Pelvis ,Humans ,Infertility ,Endometriosis ,Dysmenorrhea ,Pelvic Pain ,Magnetic Resonance Imaging ,Laparoscopy ,Laparotomy ,Incidence ,Logistic Models ,Odds Ratio ,Risk Factors ,Case-Control Studies ,Cohort Studies ,Prospective Studies ,Gravidity ,Parity ,Pregnancy ,Adolescent ,Adult ,Female ,Young Adult ,Pain Research ,Contraception/Reproduction ,Clinical Research ,Prevention ,Detection ,screening and diagnosis ,4.1 Discovery and preclinical testing of markers and technologies ,Reproductive health and childbirth ,Good Health and Well Being ,Body mass index ,dysmenorrhea ,endometriosis ,epidemiology ,infertility ,laparoscopy ,magnetic resonance imaging ,risk factors ,Paediatrics and Reproductive Medicine ,Obstetrics & Reproductive Medicine - Abstract
ObjectiveWe sought to identify risk factors for endometriosis and their consistency across study populations in the Endometriosis: Natural History, Diagnosis, and Outcomes (ENDO) Study.Study designIn this prospective matched, exposure cohort design, 495 women aged 18-44 years undergoing pelvic surgery (exposed to surgery, operative cohort) were compared to an age- and residence-matched population cohort of 131 women (unexposed to surgery, population cohort). Endometriosis was diagnosed visually at laparoscopy/laparotomy or by pelvic magnetic resonance imaging in the operative and population cohorts, respectively. Logistic regression estimated the adjusted odds ratios (AORs) and 95% confidence intervals (CIs) for each cohort.ResultsThe incidence of visualized endometriosis was 40% in the operative cohort (11.8% stage 3-4 by revised criteria from the American Society for Reproductive Medicine), and 11% stage 3-4 in the population cohort by magnetic resonance imaging. An infertility history increased the odds of an endometriosis diagnosis in both the operative (AOR, 2.43; 95% CI, 1.57-3.76) and population (AOR, 7.91; 95% CI, 1.69-37.2) cohorts. In the operative cohort only, dysmenorrhea (AOR, 2.46; 95% CI, 1.28-4.72) and pelvic pain (AOR, 3.67; 95% CI, 2.44-5.50) increased the odds of diagnosis, while gravidity (AOR, 0.49; 95% CI, 0.32-0.75), parity (AOR, 0.42; 95% CI, 0.28-0.64), and body mass index (AOR, 0.95; 95% CI, 0.93-0.98) decreased the odds of diagnosis. In all sensitivity analyses for different diagnostic subgroups, infertility history remained a strong risk factor.ConclusionAn infertility history was a consistent risk factor for endometriosis in both the operative and population cohorts of the ENDO Study. Additionally, identified risk factors for endometriosis vary based upon cohort selection and diagnostic accuracy. Finally, endometriosis in the population may be more common than recognized.
- Published
- 2013
50. Perfluorochemicals and Endometriosis
- Author
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Louis, Germaine M Buck, Peterson, C Matthew, Chen, Zhen, Hediger, Mary L, Croughan, Mary S, Sundaram, Rajeshwari, Stanford, Joseph B, Fujimoto, Victor Y, Varner, Michael W, Giudice, Linda C, Kennedy, Anne, Sun, Liping, Wu, Qian, and Kannan, Kurunthachalam
- Subjects
Clinical Research ,Endometriosis ,Adolescent ,Adult ,Caprylates ,Environmental Exposure ,Environmental Pollutants ,Female ,Fluorocarbons ,Humans ,San Francisco ,Utah ,Young Adult ,Statistics ,Public Health and Health Services ,Epidemiology - Abstract
BackgroundEnvironmental chemicals may be associated with endometriosis. No published research has focused on the possible role of perfluorochemicals (PFCs) despite their widespread presence in human tissues.MethodsWe formulated two samples. The first was an operative sample comprising 495 women aged 18-44 years scheduled for laparoscopy/laparotomy at one of 14 participating clinical sites in the Salt Lake City or San Francisco area, 2007-2009. The second was a population-based sample comprising 131 women matched to the operative sample on age and residence within a 50-mile radius of participating clinics. Interviews and anthropometric assessments were conducted at enrollment, along with blood collection for the analysis of nine PFCs, which were quantified using liquid chromatography-tandem mass spectrometry. Endometriosis was defined based on surgical visualization (in the operative sample) or magnetic resonance imaging (in the population sample). Using logistic regression, we estimated odds ratios (ORs) and 95% confidence intervals (CIs) for each PFC (log-transformed), adjusting for age and body mass index, and then parity.ResultsSerum perfluorooctanoic acid (PFOA; OR = 1.89 [95% CI = 1.17-3.06]) and perfluorononanoic acid (2.20 [1.02-4.75]) were associated with endometriosis in the operative sample; findings were moderately attenuated with parity adjustment (1.62 [0.99-2.66] and 1.99 [0.91-4.33], respectively). Perfluorooctane sulfonic acid (1.86 [1.05-3.30]) and PFOA (2.58 [1.18-5.64]) increased the odds for moderate/severe endometriosis, although the odds were similarly attenuated with parity adjustment (OR = 1.50 and 1.86, respectively).ConclusionsSelect PFCs were associated with an endometriosis diagnosis. These associations await corroboration.
- Published
- 2012
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