TY - JOUR
T1 - Prenatal intimate partner violence exposure predicts infant biobehavioral regulation
T2 - Moderation by the brain-derived neurotrophic factor (BDNF) gene
AU - Martinez-Torteya, Cecilia
AU - Figge, Caleb J.
AU - Gilchrist, Michelle A.
AU - Muzik, Maria
AU - King, Anthony P.
AU - Sorenson, Matthew
N1 - Funding Information:
Doyle Colleen Cicchetti Dante Editors Martinez-Torteya Cecilia a b Figge Caleb J. a Gilchrist Michelle A. a Muzik Maria c King Anthony P. c Sorenson Matthew a a DePaul University b Universidad de Monterey c University of Michigan This research was supported in part by DePaul University Research Council grants. We thank the study participants and research staff, as well as Caitlin Karver for her technical assistance. Address correspondence and reprint requests to: Cecilia Martinez-Torteya, 2219 N Kenmore Ave. , Chicago , IL 60614 ; E-mail: [email protected] . 02 08 2018 08 2018 30 3
Publisher Copyright:
© Copyright 2018 Cambridge University Press.
PY - 2018/8/1
Y1 - 2018/8/1
N2 - The ability to regulate stress is a critical developmental milestone of early childhood that involves a set of interconnected behavioral and physiological processes and is influenced by genetic and environmental stimuli. Prenatal exposure to traumatic stress and trauma, including intimate partner violence (IPV), increases risk for offspring biobehavioral regulation problems during childhood and adolescence. Although individual differences in susceptibility to prenatal stress have been largely unexplored, a handful of studies suggest children with specific genetic characteristics are most vulnerable to prenatal stress. We evaluated the brain-derived neurotrophic factor Val66Met gene (BDNF) as a moderator of the effect of prenatal IPV exposure on infant temperamental and cortisol regulation in response to a psychosocial challenge. Ninety-nine mother-infant dyads recruited from the community were assessed when infants (51% female) were 11 to 14 months. Maternal reports of IPV during pregnancy and infant temperament were obtained, and infant saliva was collected for genotyping and to assess cortisol reactivity (before and after the Strange Situation Task). Significant genetic moderation effects were found. Among infants with the BDNF Met allele, prenatal IPV predicted worse temperamental regulation and mobilization of the cortisol response, while controlling for infant postnatal exposure to IPV, other maternal traumatic experiences, and infant sex. However, prenatal IPV exposure was not associated with temperamental or cortisol outcomes among infant carriers of the Val/Val genotype. Findings are discussed in relation to prenatal programming and biological susceptibility to stress.
AB - The ability to regulate stress is a critical developmental milestone of early childhood that involves a set of interconnected behavioral and physiological processes and is influenced by genetic and environmental stimuli. Prenatal exposure to traumatic stress and trauma, including intimate partner violence (IPV), increases risk for offspring biobehavioral regulation problems during childhood and adolescence. Although individual differences in susceptibility to prenatal stress have been largely unexplored, a handful of studies suggest children with specific genetic characteristics are most vulnerable to prenatal stress. We evaluated the brain-derived neurotrophic factor Val66Met gene (BDNF) as a moderator of the effect of prenatal IPV exposure on infant temperamental and cortisol regulation in response to a psychosocial challenge. Ninety-nine mother-infant dyads recruited from the community were assessed when infants (51% female) were 11 to 14 months. Maternal reports of IPV during pregnancy and infant temperament were obtained, and infant saliva was collected for genotyping and to assess cortisol reactivity (before and after the Strange Situation Task). Significant genetic moderation effects were found. Among infants with the BDNF Met allele, prenatal IPV predicted worse temperamental regulation and mobilization of the cortisol response, while controlling for infant postnatal exposure to IPV, other maternal traumatic experiences, and infant sex. However, prenatal IPV exposure was not associated with temperamental or cortisol outcomes among infant carriers of the Val/Val genotype. Findings are discussed in relation to prenatal programming and biological susceptibility to stress.
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U2 - 10.1017/S0954579418000329
DO - 10.1017/S0954579418000329
M3 - Article
C2 - 30068406
AN - SCOPUS:85051007468
SN - 0954-5794
VL - 30
SP - 1009
EP - 1021
JO - Development and psychopathology
JF - Development and psychopathology
IS - 3
ER -