Back to the future: omnipresence of fetal influence on the human brain through the lifespan

Walhovd, Kristine B.; Krogsrud, Stine Kleppe; Amlien, Inge K.; Sørensen, Øystein; Wang, Yunpeng; Bråthen, Anne Cecilie Sjøli; Øverbye, Knut; Kransberg, Jonas; Mowinckel, Athanasia M.; Magnussen, Fredrik; Herud, Martine; Håberg, Asta; Fjell, Anders Martin; Vidal-Piñeiro, Dídac

doi:10.1101/2022.12.02.514196

Cited by 5 publications

(3 citation statements)

References 92 publications

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“…Cross-sectional measurement error. Measurement error σε was estimated as the average error across six different test-retest cohorts consisting of cognitively healthy adult participants, namely, the S2C (Walhovd et al, 2024), the preventAD (Orban et al, 2015), OASIS (Marcus et al, 2007), and GSP (Holmes et al, 2015) reliability subsets, and the HNU1 (Chen et al, 2015) and Maclaren (Maclaren et al, 2014) mean to the between-subject average for test-retest and to the within-subject average for densely scanned designs) were discarded. Measurement error (𝜎 𝑒 ) was estimated for a given subject (i) as the absolute difference between each measure estimated from both sessions divided by the mean of the two for test-retest designs (eq.…”

Section: Methodsmentioning

confidence: 99%

Reliability of structural brain change in cognitively healthy adult samples

Vidal-Piñeiro,

Sørensen,

Strømstad

et al. 2024

Preprint

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In neuroimaging research, tracking individuals over time is key to understanding the interplay between brain changes and genetic, environmental, or cognitive factors across the lifespan. Yet, the extent to which we can estimate the individual trajectories of brain change over time with precision remains uncertain. In this study, we estimated the reliability of structural brain change in cognitively healthy adults from multiple samples and assessed the influence of follow-up time and number of observations. Estimates of cross-sectional measurement error and brain change variance were obtained using the longitudinal FreeSurfer processing stream. Our findings showed, on average, modest longitudinal reliability with two years of follow-up. Increasing the follow-up time was associated with a substantial increase in longitudinal reliability while the impact of increasing the number of observations was comparatively minor. On average, 2-year follow-up studies require ≈2.7 and ≈4.0 times more individuals than designs with follow-ups of 4 and 6 years to achieve comparable statistical power. Subcortical volume exhibited higher longitudinal reliability compared to cortical area, thickness, and volume. The reliability estimates were comparable to those estimated from empirical data. The reliability estimates were affected by both the cohort’s age where younger adults had lower reliability of change, and the preprocessing pipeline where the FreeSurfer’s longitudinal stream was notably superior than the cross-sectional. Suboptimal reliability inflated sample size requirements and compromised the ability to distinguish individual trajectories of brain aging. This study underscores the importance of long-term follow-ups and the need to consider reliability in longitudinal neuroimaging research.

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Section: Methodsmentioning

confidence: 99%

Reliability of structural brain change in cognitively healthy adult samples

Vidal-Piñeiro,

Sørensen,

Strømstad

et al. 2024

Preprint

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“…It remains uncertain if estimates of morphometricity would be equally reduced. As a growing body of evidence demonstrates associations between perinatal and early-life factors and later brain development (Alnaes et al 2020;Walhovd et al 2023), we also included weight at birth.…”

Section: Outcome Measuresmentioning

confidence: 99%

Genetic and brain similarity independently predict childhood anthropometrics and socioeconomic markers

Dahl,

Eilertsen,

Rodriguez-Cabello

et al. 2023

Preprint

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Linking the developing brain with individual differences in clinical and demographic traits is challenging due to the substantial interindividual heterogeneity of brain anatomy and organization. Here we employ a novel approach that parses individual differences in both cortical thickness and common genetic variants, and assess their effects on a wide set of childhood traits. The approach uses a linear mixed model framework to obtain the unique effects of each type of similarity, as well as their covariance, with the assumption that similarity in cortical thickness may in part be driven by similarity in genetic variants. We employ this approach in a sample of 7760 unrelated children in the ABCD cohort baseline sample (mean age 9.9, 46.8% female). In general, significant associations between cortical thickness similarity and traits were limited to anthropometrics such as height (r2 = 0.11, SE = 0.01), weight (r2 = 0.12, SE = 0.01), and birth weight (r2 = 0.19, SE = 0.01), as well as markers of socioeconomic status such as local area deprivation (r2 = 0.06, SE = 0.01). Analyses of the contribution from common genetic variants to traits revealed contributions across included outcomes, albeit somewhat lower than previous reports, possibly due to the young age of the sample. No significant covariance of the effects of genetic and cortical thickness similarity was found. The present findings highlight the connection between anthropometrics as well as socioeconomic factors and the developing brain, which appear to be independent from individual differences in common genetic variants in this population-based sample. The approach provides a promising framework for analyses of neuroimaging genetics cohorts, which can be further expanded by including imaging derived phenotypes beyond cortical thickness.

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“…Data from the World Mental Health Surveys [1 ▪ ] indicate that the lifetime prevalence of any mental disorder is 28.6% for females and 29.8 for males, with age of onset often during childhood and adolescence [1 ▪ ]. A range of evidence – including brain imaging studies [2], genetic studies [3] and studies combining brain imaging and early gene expression [4] - indicate that mental disorders are associated with altered brain developmental processes even earlier, beginning in pregnancy. The period encompassing pregnancy and the first two years after birth -the perinatal period- has also been termed ‘the first 1000 days’ or ‘the first 1001 critical days’.…”

Section: Introductionmentioning

confidence: 99%

Current perspectives on perinatal mental health and neurobehavioral development: focus on regulation, coregulation and self-regulation

Van den Bergh,

Antonelli,

Stein

2024

Current Opinion in Psychiatry

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Purpose of review Perinatal mental health research provides an important perspective on neurobehavioral development. Here, we aim to review the association of maternal perinatal health with offspring neurodevelopment, providing an update on (self-)regulation problems, hypothesized mechanistic pathways, progress and challenges, and implications for mental health. Recent findings (1) Meta-analyses confirm that maternal perinatal mental distress is associated with (self-)regulation problems which constitute cognitive, behavioral, and affective social-emotional problems, while exposure to positive parental mental health has a positive impact. However, effect sizes are small. (2) Hypothesized mechanistic pathways underlying this association are complex. Interactive and compensatory mechanisms across developmental time are neglected topics. (3) Progress has been made in multiexposure studies. However, challenges remain and these are shared by clinical, translational and public health sciences. (4) From a mental healthcare perspective, a multidisciplinary and system level approach employing developmentally-sensitive measures and timely treatment of (self-)regulation and coregulation problems in a dyadic caregiver-child and family level approach seems needed. The existing evidence-base is sparse. Summary During the perinatal period, addressing vulnerable contexts and building resilient systems may promote neurobehavioral development. A pluralistic approach to research, taking a multidisciplinary approach to theoretical models and empirical research needs to be fostered.

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Back to the future: omnipresence of fetal influence on the human brain through the lifespan

Cited by 5 publications

References 92 publications

Reliability of structural brain change in cognitively healthy adult samples

Reliability of structural brain change in cognitively healthy adult samples

Genetic and brain similarity independently predict childhood anthropometrics and socioeconomic markers

Current perspectives on perinatal mental health and neurobehavioral development: focus on regulation, coregulation and self-regulation

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