Biological mechanisms underlying psychosocial stress response: The consequences of prenatal maternal distress and childhood maltreatment on the endocrine and immune systems

dc.contributor
Universitat de Barcelona. Departament de Biologia Evolutiva, Ecologia i Ciències Ambientals
dc.contributor.author
Castro Quintas, Águeda
dc.date.accessioned
2024-03-26T10:18:47Z
dc.date.available
2024-03-26T10:18:47Z
dc.date.issued
2024-02-26
dc.identifier.uri
http://hdl.handle.net/10803/690424
dc.description
Programa de Doctorat en Biomedicina
ca
dc.description.abstract
[eng] During critical periods of development, psychosocial stress experiences may alter key neural networks of the human brain, with long-lasting effects on behavior and mental health. However, the specific biological mechanisms through which early life stress impacts on present and future mental health are still not well understood. Hypothalamic-pituitary-adrenal (HPA) axis is the principal sensor and regulator of stress response. Its modulation begins early in development through fetus-placental dialogue and continues during postnatal life, from childhood to adolescence, being especially sensitive to early life’s adversities. Thus, HPA axis programming during prepostnatal developmental periods is proposed as a plausible mechanism of early sensitization that undermine future HPA axis functioning and associated mental disorders. Moreover, it should not be forgotten that the HPA axis dialogues with the immune system, exhibiting a bidirectional interaction. In this framework, the present dissertation aimed to disentangle the impact of psychosocial stress exposure during early sensitive periods of pre-postnatal brain development on HPA axis and immunity system. Cortisol (the HPA axis ultimate effector) and secretory immunoglobulin A (s-IgA) (an immunoglobulin of the mucosal surfaces) were selected in this thesis, respectively, as putative biomarkers of the endocrine and immune response to early psychosocial stress exposure in early life. The study of two mother/infant dyad cohorts, the Intramural_Maternal_Epi_project cohort and the COGESCOV-19 cohort, enable us to explore the respectively effects of the maternal distress and SARS-CoV-2 infection during pregnancy on the newborn’s early stress reactivity. In Intramural_Maternal_Epi_project, we observed that the presence of depressive symptoms flattened the maternal cortisol circadian pattern, especially during the second trimester of pregnancy. Furthermore, elevated maternal cortisol levels in mid-late pregnancy were associated with poor birth outcomes, including prematurity and low weight percentile at birth. These results underscore the importance of early detection of depressive symptoms, which are often manifested as a subclinical condition during pregnancy. Another hypothesis we tested with this cohort was based on the premise that maternal distress during pregnancy could influence DNA methylation patterns in placenta. Specifically, we studied the DNA methylation of FKBP5, NR3C1 and HSD11B2 genes in two different placental layers: maternal decidua and chorionic villi. We observed that while maternal cortisol levels in early pregnancy were associated with an increase in DNA methylation of CpG islands of NR3C1 gene and a decrease in DNA methylation of CpG islands of FKBP5 gene in the chorionic villi, at the level of the maternal decidua it was the increase in DNA methylation (at specific CpG sites of FKBP5 gene) that was strongly associated with the lower gestational age of the newborn at birth. Thus, stress during the pregnancy, and its associated cortisol levels could influence placental epigenetic signatures differently depending on the time of exposure, the placental layer, and the gene of study. Complementarily, we could explore the putative consequences of maternal exposure to SARS-CoV-2 during pregnancy in the neurodevelopmental outcomes of offspring, thanks to the COGESCOV-19 cohort. In this regard, we observed that infants born to mothers exposed to SARS-CoV-2 (serologically positive) showed poorer responses in items related to regulation and motor system domains (NBAS-Brazelton scale) at seven weeks old. This effect was especially evident in infants whose mothers were infected in the third trimester. Considering the magnitude of COVID-19 pandemic, children born to mothers infected during pregnancy, particularly in late pregnancy, should undergo additional longitudinal screening for neurodevelopmental milestones. On the other hand, in this thesis, we had the opportunity to explore the effect of the most severe psychosocial stress condition for a child, such as exposure to maltreatment during their early years of life. Our research was made possible thanks to Epi_young_stress cohort, which consists of a representative number of children and adolescents from the general population (aged between 7 and 17 years). This cohort has been recruited through the collaboration of various child and adolescent psychiatry units nationwide and includes both children with a current psychiatric diagnosis and a control group. For all subjects, the history of childhood maltreatment was thoroughly examined, and the Trier Social Stress Test for children (TSST-C) was also administered to assess the reactivity of the HPA axis to acute stress in this population. Regarding the functioning of the HPA axis in this young population, although children with maltreatment showed higher basal cortisol levels compared to those not exposed to maltreatment, when subjected to the acute stressor (TSST-C), they exhibited a flattened cortisol response but higher perceived anxiety. Noticeably, we also observed a dose-response relationship between the frequency and severity of the maltreatment and cortisol dysregulation. Furthermore, and in relation with putative immunity biomarkers in front psychosocial stress, we described that the acute exposure to the stress test was able to stimulate the secretion of s-IgA in young subjects after puberty. Additionally, concerning immune markers in response to acute stress, we found that exposure to the acute stressor (TSST-C) was able to stimulate the secretion of s-IgA in young subjects, but only after puberty. However, although s-IgA reactivity to acute stress was not observed in prepubescent children, when the presence of maltreatment was observed, these children had developed this immune response capability, suggesting that complex trauma could anticipates the immune maturation. Finally, considering our previous result that salivary s-IgA quickly rises after acute stress exposure, we wanted to know if salivary s-IgA could be a new promising biomarker of psychosocial stress reactivity in young population. A systematic review of the available scientific literature revealed that s-IgA can be considered a reliable biomarker of acute stress in under 18 population. However, further research is needed to specifically determine how psychosocial stress impacts on s-IgA circadian rhythm and basal levels. Together, the results of this thesis support the notion that psychosocial stress during prenatal and child-juvenile periods could alter endocrine and immune systems regulation, modifying early behavioral dimensions and the reactivity to stress, which might increase the risk of future mental health problems.
ca
dc.description.abstract
[spa] Durante los periodos más precoces y sensibles del desarrollo del sistema nervioso central (SNC), la exposición al estrés psicosocial puede alterar los sistemas biológicos para el futuro funcionamiento adaptativo del sujeto. El cortisol (último efector del eje Hipotalámico Hipofisario Adrenal (HHA)) y la inmunoglobulina A secretora (s-IgA) se seleccionaron en esta tesis, respectivamente, como posibles biomarcadores de respuesta al estrés psicosocial en las primeras etapas de la vida. Se pudo estudiar el papel del distrés materno durante el embarazo, y su posible asociación con en el comportamiento y la reactividad ante el estrés del recién nacido, gracias a dos cohortes de diadas madre/niño seguidas durante el embarazo y hasta las primeras semanas postnatales: la cohorte del Intramural_Maternal_Epi_project y la cohorte COGESTCOV-19. En primer lugar, pudimos constatar que el patrón diurno de cortisol estaba desregulado en mujeres con síntomas de depresión, especialmente durante en el segundo trimestre del embarazo. Así mismo se observó que altos niveles de cortisol en esta etapa del embarazo se asociaban con prematuridad y bajo peso al nacer. Por otra parte, se pudo comprobar que los niveles altos de cortisol materno al principio del embarazo podrían asociarse con un perfil de metilación del ADN específico en genes placentarios implicados en la regulación del cortisol, incrementando el riesgo de un parto adelantado. Finalmente, se estudiaron las consecuencias de la infección materna por SARS-COV-2 durante el embarazo en las respuestas motoras y de regulación ante los estímulos del test de Brazelton en los niños a las 7 semanas de vida, constatando un mayor efecto si la infección afectaba al último trimestre de embarazo. Por otro lado, el estudio de una cohorte de niños/as y adolescentes con y sin patología mental (cohorte del proyecto Epi_young_stress) nos permitió analizar el papel del maltrato infantil en la posible sensibilización temprana del eje HHA y del sistema inmunitario de los sujetos expuestos. Para testar esta posible sensibilización, en este estudio se indujo estrés psicosocial agudo a todos los sujetos de la cohorte, mediante un protocolo de laboratorio cuasi experimental: el test de estrés psicosocial Trier para niños (TSST-C). Los niños/as y adolescentes expuestos a maltrato mostraron mayores niveles de cortisol basales y una hiporreactividad del eje HHA al TSST-C, a pesar de mostrar una mayor percepción de ansiedad ante estrés psicosocial agudo comparados con los niños no expuestos a maltrato. También se observó una relación dosis-efecto entre la exposición y severidad del maltrato y la desregulación del eje HHA. Además, el estrés psicosocial estimuló la secreción de s-IgA, pero sólo después de la pubertad. Sin embargo, los niños/as expuestos a maltrato infantil mostraron secreción de la s-IgA ante estrés psicosocial de forma similar a los adolescentes, sugiriendo una anticipación de la maduración del sistema inmune en los niños maltratados. El uso de la s-IgA como posible biomarcador de estrés agudo y crónico en etapas tempranas de la vida fue estudiado y discutido mediante una revisión sistemática. En conjunto, los resultados de esta tesis sostienen que la exposición al estrés psicosocial durante los periodos tempranos del desarrollo del SNC (prenatal, infancia y adolescencia) podrían alterar la respuesta al estrés de los sistemas endocrino e inmune, modificando algunos rasgos de la conducta temprana en el recién nacido y aumentando el riesgo de futuros problemas de salud mental.
ca
dc.format.extent
249 p.
ca
dc.language.iso
eng
ca
dc.publisher
Universitat de Barcelona
dc.rights.license
L'accés als continguts d'aquesta tesi queda condicionat a l'acceptació de les condicions d'ús establertes per la següent llicència Creative Commons: http://creativecommons.org/licenses/by-nc-nd/4.0/
ca
dc.rights.uri
http://creativecommons.org/licenses/by-nc-nd/4.0/
*
dc.source
TDX (Tesis Doctorals en Xarxa)
dc.subject
Embaràs
ca
dc.subject
Embarazo
ca
dc.subject
Pregnancy
ca
dc.subject
Maltractament infantil
ca
dc.subject
Maltrato infantil
ca
dc.subject
Child abuse
ca
dc.subject
Hormones pituïtàries
ca
dc.subject
Hormonas hipofisarias
ca
dc.subject
Pituitary hormones
ca
dc.subject
Immunoglobulina A
ca
dc.subject
Inmunoglobulina A
ca
dc.subject
Immunoglobulin A
ca
dc.subject
Placenta
ca
dc.subject.other
Ciències Experimentals i Matemàtiques
ca
dc.title
Biological mechanisms underlying psychosocial stress response: The consequences of prenatal maternal distress and childhood maltreatment on the endocrine and immune systems
ca
dc.type
info:eu-repo/semantics/doctoralThesis
dc.type
info:eu-repo/semantics/publishedVersion
dc.subject.udc
577
ca
dc.contributor.director
Fañanás Saura, Lourdes
dc.contributor.tutor
Fañanás Saura, Lourdes
dc.embargo.terms
cap
ca
dc.rights.accessLevel
info:eu-repo/semantics/openAccess


Documents

ACQ_PhD_THESIS.pdf

20.37Mb PDF

This item appears in the following Collection(s)