Your search keyword '"Rex-Haffner, M. (Monika)"' showing total 2 results

1. Genome-wide copy number variant and high-throughput transcriptomics analyses of placental tissues underscore persisting child susceptibility in at-risk pregnancies cleared in standard genetic testing

Author

Czamara, D. (Darina), Cruceanu, C. (Cristiana), Lahti-Pulkkinen, M. (Marius), Dieckmann, L. (Linda), Ködel, M. (Maik), Sauer, S. (Susann), Rex-Haffner, M. (Monika), Sammallahti, S. (Sara), Kajantie, E. (Eero), Laivuori, H. (Hannele), Lahti, J. (Jari), Räikkönen, K. (Katri), Binder, E. B. (Elisabeth B.), Czamara, D. (Darina), Cruceanu, C. (Cristiana), Lahti-Pulkkinen, M. (Marius), Dieckmann, L. (Linda), Ködel, M. (Maik), Sauer, S. (Susann), Rex-Haffner, M. (Monika), Sammallahti, S. (Sara), Kajantie, E. (Eero), Laivuori, H. (Hannele), Lahti, J. (Jari), Räikkönen, K. (Katri), and Binder, E. B. (Elisabeth B.)

Abstract

Several studies have shown that children from pregnancies with estimated first-trimester risk based on fetal nuchal translucency thickness and abnormal maternal serum pregnancy protein and hormone levels maintain a higher likelihood of adverse outcomes, even if initial testing for known genetic conditions is negative. We used the Finnish InTraUterine cohort (ITU), which is a comprehensively characterized perinatal cohort consisting of 943 mothers and their babies followed throughout pregnancy and 18 months postnatally, including mothers shortlisted for prenatal genetic testing but cleared for major aneuploidies (cases: n = 544, 57.7%) and control pregnancies (n = 399, 42.3%). Using genome-wide genotyping and RNA sequencing of first-trimester and term placental tissue, combined with medical information from registry data and maternal self-report data, we investigated potential negative medical outcomes and genetic susceptibility to disease and their correlates in placenta gene expression. Case mothers did not present with higher levels of depression, perceived stress, or anxiety during pregnancy. Case children were significantly diagnosed more often with congenital malformations of the circulatory system (4.12 (95% CI [1.22–13.93]) higher hazard) and presented with significantly more copy number duplications as compared to controls (burden analysis, based on all copy number variants (CNVs) with at most 10% frequency, 823 called duplications in 297 cases versus 626 called duplications in 277 controls, p = 0.01). Fifteen genes showed differential gene expression (FDR < 0.1) in association with congenital malformations in first-trimester but not term placenta. These were significantly enriched for genes associated with placental dysfunction. In spite of normal routine follow-up prenatal testing results in early pregnancy, case children presented with an increased likelihood of negative outcomes, which should prompt vigilance in follow-up during pregnancy and

Published

2022

2. Cohort profile:InTraUterine sampling in early pregnancy (ITU), a prospective pregnancy cohort study in Finland:study design and baseline characteristics

Author

Kvist, T. (Tuomas), Sammallahti, S. (Sara), Lahti-Pulkkinen, M. (Marius), Cruceanu, C. (Cristiana), Czamara, D. (Darina), Dieckmann, L. (Linda), Tontsch, A. (Alina), Röh, S. (Simone), Rex-Haffner, M. (Monika), Wolford, E. (Eiina), Reynolds, R. (Rebecca), Eriksson, J. (Johan), Suomalainen-König, S. (Sanna), Laivuori, H. (Hannele), Kajantie, E. (Eero), Lahdensuo, E. (Eija), Binder, E. (Elisabeth), Räikkönen, K. (Katri), Kvist, T. (Tuomas), Sammallahti, S. (Sara), Lahti-Pulkkinen, M. (Marius), Cruceanu, C. (Cristiana), Czamara, D. (Darina), Dieckmann, L. (Linda), Tontsch, A. (Alina), Röh, S. (Simone), Rex-Haffner, M. (Monika), Wolford, E. (Eiina), Reynolds, R. (Rebecca), Eriksson, J. (Johan), Suomalainen-König, S. (Sanna), Laivuori, H. (Hannele), Kajantie, E. (Eero), Lahdensuo, E. (Eija), Binder, E. (Elisabeth), and Räikkönen, K. (Katri)

Abstract

Purpose: The InTraUterine sampling in early pregnancy (ITU) is a prospective pregnancy cohort study. The overarching aim of ITU is to unravel genomic, epigenomic, transcriptomic, endocrine, inflammatory and metabolic maternal-placental-fetal mechanisms involved in the programming of health and disease after exposure to prenatal environmental adversity, such as maternal malnutrition, cardiometabolic disorders, infections, medical interventions, mental disorders and psychosocial stress. This paper describes the study protocol, design and baseline characteristics of the cohort. Participants: We included 944 pregnant Finnish women, their partners and children born alive between April 2012 and December 2017. The women were recruited through the national, voluntary trisomy 21 screening between 9+0 and 21+6 gestational weeks. Of the participating women, 543 were screen positive and underwent fetal chromosomal testing. Test result of these women suggested no fetal chromosomal abnormality. Further, we recruited 401 women who were screen negative and who did not undergo fetal chromosomal testing. Findings to date: We have collected chorionic villi and amniotic fluid from the screen-positive women; blood, urine, buccal swabs and diurnal salivary samples from all women; blood and buccal swabs from all partners; and placenta, cord blood and buccal swabs from all newborns for analyses of the genome, epigenome, transcriptome, and endocrine, inflammatory and metabolic markers. These data are coupled with comprehensive phenotypes, including questions on demographic characteristics, health and well-being of the women and their partners during pregnancy and of the women and their children at the child’s age of 1.7 and 3 years. Data also come from patient records and nationwide registers covering health, lifestyle and medication data. Future plans: Multiple layers of ITU data allow integrative data analyses, which translate to biomarker identification and allow risk stratifica

Published

2022