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MINI REVIEW article

Front. Psychol., 02 August 2019
Sec. Developmental Psychology
This article is part of the Research Topic Risk and Protective Factors Associated with Early Adversity and Development: Evidence from Human and Animal Research View all 16 articles

Early Life Stress, Physiology, and Genetics: A Review

Nia Fogelman&#x;
Nia Fogelman*Turhan CanliTurhan Canli
  • Department of Psychology, Stony Brook University, Stony Brook, NY, United States

Early life stress (ELS) is a widely studied concept due to both its prevalent nature and its (presumed) detrimental consequences. In this review, we discuss the relationship between ELS and its underlying physiology spanning the sympathetic nervous system, hypothalamic-pituitary-adrenal axis, and markers of inflammation related to immune function in both human and animal literature. We also consider the potential role of genetic and epigenetic factors on the ELS-health outcome relationship. We conclude with recommendations to overcome identified shortcomings in a field that seeks to address the health consequences of ELS.

Introduction

Early life stress (ELS), including physical, sexual, and emotional forms of abuse and neglect experienced by the developing child (Centers for Disease Control and Prevention, 2018), has been linked to a host of physical and psychological sequelae into adulthood (Chapman et al., 2004; Gluckman et al., 2008; Middlebrooks and Audage, 2008; Pechtel and Pizzagalli, 2011). Such adverse experiences are surprisingly common, according to a large-scale epidemiological study on adverse childhood events, which reports that approximately 65% of people in the United States experienced at least one, and 12.5% experienced as many as four, adverse early life events (Middlebrooks and Audage, 2008). Given these statistics, a deeper understanding of the pathophysiology of ELS could produce better long-term prognosticators of adverse sequelae for vulnerable individuals, and promote the development of patient-centered interventions with specific strategies to mitigate the ill effects of ELS.

To elucidate the connection between ELS and negative health outcomes, research examined putative physiological mediators, including the sympathetic nervous system (SNS), the hypothalamic pituitary adrenal (HPA) axis, and cytokines linked to inflammation (Mayer, 2000; Pariante and Lightman, 2008). Dysregulation of these systems has been associated with a host of disorders in and of themselves (Cohen et al., 2000; Cowen, 2010; Lamers et al., 2013). In this review, we will examine the connections between ELS and these physiological pathways in both human adults and mature non-human animals. We will additionally consider the potential role of candidate gene polymorphisms and DNA methylation in genes linked to the stress response and to mood disorders as moderators of the ELS-negative health outcome relationship. Finally, we will offer recommendations for a growing field examining the effects of ELS into adulthood.

An Overview of Acute Stress Physiology and Inflammatory Markers

Stress promotes physiological responses across several different systems, most prominently the SNS, HPA axis, and immune system, which are heavily intertwined (Chrousos, 2009). For instance, brain regions processing sensory and psychological stressors activate preganglionic neurons in brain stem and spinal cord to activate the peripheral SNS. This then prepares the body to “fight or flee” by releasing catecholamines such as epinephrine and norepinephrine to increase heart rate and blood pressure. In parallel, stress activates the HPA axis, leading to the release of corticotropin-releasing factor (CRF) by the hypothalamus, followed by the release of adrenocorticotropin-releasing hormone (ACTH) onto CRH-R1 receptors from the pituitary, and subsequent release of glucocorticoids (including cortisol in humans and corticosterone in animals) from the adrenal glands (Lupien et al., 2009). Both activation of the SNS and HPA axis are correlated with inflammatory markers, including tumor necrosis factor-α (TNF-α), interferon-γ (IFN-γ), and interleukin-6 (IL-6) (Chrousos and Gold, 1992; Tsigos and Chrousos, 2002; Padgett and Glaser, 2003).

For the purposes of this review, we will focus on these and similar markers to assess the impact of ELS on stress physiology. Figure 1 presents an overview of these markers, their relationship to one another, and their potential changes in the presence of stress.

FIGURE 1
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Figure 1. ELS may impact gene methylation. ELS, working in conjunction with genetics, is associated with increased heart rate and inflammation. Evidence is inconsistent on the effects of catecholamines and signaling pathways associated with the HPA axis. The SNS, HPA axis, and immune system exhibit reciprocal effects on one another. Images adapted from open license image site smart.servier.com.

Early Life Stress, Sympathetic Nervous System, Hypothalamic-Pituitary-Adrenal Axis, and Inflammation in Humans

Several studies have found a relationship between ELS and cardiovascular/HPA axis effects. For instance, Dong et al. (2004) saw a direct relationship between ELS and ischemic heart disease later in life, although this was partially mediated by presence of additional psychological risk variables such as anger levels and depressed affect. Gatt et al. (2009) observed that an increase in the number of ELS events in healthy adult participants was associated with higher resting and activated heart rates. Similarly, Heim et al. (2000) reported elevated heart rate in response to the Trier Social Stress Test (TSST) in a group of depressed women who had experienced sexual and/or physical abuse early in life, compared to non-depressed women without ELS. Within the same group, depressed ELS women displayed heightened cortisol reactivity and dysregulated ACTH (the latter was seen in women with ELS regardless of depression status; Heim et al., 2000). In line with a heightened cortisol response, individuals in a community-based sample with ELS and a psychiatric history displayed poorer recovery and exhibited significantly stronger cortisol reactivity to a cognitive stress task, compared to the non-ELS group (Goldman-Mellor et al., 2012). Yet, others reported diminished cortisol associated with ELS. For instance, women who had experienced ELS showed lower baseline cortisol levels preceding a corticotropin-releasing factor (CRF) stimulation test (a bolus of CRF given in the afternoon), but produced a similar post-stressor cortisol response, compared to non-ELS controls (Heim et al., 2001). ELS was also associated with blunted cortisol in another common HPA outcome measure, the cortisol awakening response, in a different study (Li et al., 2015). Given the conflicting literature, we conducted a comprehensive meta-analysis, in which we found no significant association between early life stress and cortisol (Fogelman and Canli, 2018). We did, however, note strong heterogeneity across studies, suggesting that “type of stressor” may be an important moderator of subsequent cortisol physiology. For instance, experiencing abuse was associated with increased cortisol awakening response levels, suggesting that some forms of trauma may be more severe and hence have a more profound and lasting impact on physiology.

ELS is also associated with increased inflammation, both basally and in response to acute stress. One longitudinal study that followed participants since childhood, demonstrated a link between ELS and high-sensitivity C-reactive protein (hsCRP) levels (Danese et al., 2007). ELS was also associated with heightened IL-6 in response to the TSST (Carpenter et al., 2010) and with heightened IL-1β, IL-12, and TNF-α levels (Li et al., 2015) in healthy community samples. In a patient cohort of depressed individuals, there was no significant main effect between ELS and inflammatory markers; however, depressed patients displayed greater ELS and an increase in nuclear factor kappa-light-chain-enhancer of activated B cells (NF-κB) and IL-6 in response to the TSST (Pace et al., 2006).

In addition to ELS being linked to the SNS, HPA axis, and immune system, these systems have been shown to influence one another. For instance, Fagundes and Way (2014) proposed that increased sympathetic activity and dysregulated cortisol attributed to ELS may persist to low-grade inflammation over time. The “neuro-immune network” hypothesis by Nusslock and Miller (2016) puts forth the notion that ELS strengthens cortico-amygdala neural circuitry, thus “priming” and responding to heightened SNS, HPA axis, and immune function over time. Taken together, these findings suggest that ELS, at least in certain groups and under certain conditions, has a potent effect on mediating pathways related to the cardiovascular system/HPA axis and markers of inflammation.

Early Life Stress, The Hypothalamic-Pituitary-Adrenal Axis, and Inflammation in Animals

In addition to studying the effects of ELS on health in human subjects, results from animal studies may offer helpful insights given the greater ability to manipulate experimental conditions and the simplified nature conditions surrounding ELS relative to human studies. Overall, experimental studies conducted in animal models of ELS tend to concur with human data suggesting heightened reactivity following ELS. For instance, one study found that rats who as pups had experienced maternal separation for either 15 or 180 min per day displayed higher levels of neuropeptide-y (a highly prevalent peptide associated with the CNS) than non-handled controls (Husum and Mathe, 2002), mirroring greater CNS reactivity we often see in human studies of ELS. In the same study, neuropeptide-y/CRF ratios were significantly lower in the maternal separation groups and the effect was dose dependent, such that more maternal separation was associated with lower ratios (Husum and Mathe, 2002); greater neuropeptide-y has been seen as protective in depression-like behavior in rats (Stogner and Holmes, 2000), therefore a lower ratio represents a concern for increased rates of depression-like behavior in the presence of ELS. Other maternal separation studies reported elevated heart rate and inflammatory responses to a physiological stressor (Loria et al., 2010), as well as elevated corticosterone, TNF-α, and IFN-γ levels, and increased production of anxiety-like behaviors (O’Mahony et al., 2009) in maternally deprived rats, compared to controls. In mice, ELS has also been linked with heightened basal corticosterone (Murgatroyd et al., 2009). These findings bolster concerns of up-regulation of physiological response, similar to that seen in human studies.

Yet, as with the human literature, reports on the impact of ELS on physiology are not always consistent. For instance, social isolation in early development was associated with lower corticosterone levels in a recovery period following restraint-stress exposure in adult rats (Lukkes et al., 2009). According to one review, rats and primates experiencing maternal separation early in life overall display heightened CRF, but diminished ACTH and glucocorticoid levels; in primates, these levels are initially elevated during development, suggesting that the timing of when measurements are obtained may be an important moderating factor (Pryce et al., 2002). On the whole, the animal literature mostly supports the conclusion that animal models of ELS produce later increases in SNS, HPA axis, and inflammatory markers. The larger degree of consistency across animal studies, compared to the human literature, may have been aided by greater experimental controls, more uniform models of ELS, and homogeneity in the choice of rodent strains.

Early Life Stress and Negative Health Outcomes: The Role of Genetics

Thus far, we have reviewed evidence surrounding ELS and its relationship to the SNS, HPA axis, and immune function, as these may be pathways to negative health later in life. However, ELS may also lead to poorer health outcomes through genetic mechanisms. Indeed, numerous studies have considered the role of genetics, both at the structural level of gene variants and at the level of epigenetic regulation of DNA expression (Heim and Binder, 2012). Variants of well-known candidate genes may potentially increase susceptibility to stressful environmental conditions, increasing risk for mood and anxiety disorders (Nugent et al., 2011). In a seminal longitudinal study of approximately 1,000 individuals, Caspi et al. (2003) reported a significant interaction between presence of the serotonin-transporter-linked polymorphic region (5-HTTLPR) S allele and life stress history predicting depressive symptoms. Later replication studies produced conflicting results and meta-analyses came to opposite conclusions. One the one hand, one meta-analysis concluded that ELS significantly interacted with presence of the S allele in 5-HTTLPR of SLC6A4 to predict greater stress sensitivity and risk of depression (Karg et al., 2011). On the other hand, a recent large-scale meta-analysis used harmonized analyses across 31 previously published datasets representing more than 38,000 individuals and failed to identify an interaction between the 5-HTTLPR S allele, life stress, and depression (Culverhouse et al., 2018). The authors concluded that “if an interaction exists in which the S allele of 5-HTTLPR increases risk of depression only in stressed individuals, then it is not broadly generalisable, but must be of modest effect size and only observable in limited situations” (p. 134).

Some other candidate genes included FKBP5 (a co-chaperone to glucocorticoid receptors as part of the HPA axis leading to stress response regulation and anxiety); the gene encoding the brain-derived neurotrophic factor, BDNF (hypothesized role in mood disorders; Nugent et al., 2011); and the oxytocin receptor gene, OXTR (oxytocin receptors are concentrated in the hypothalamus and dysregulation has been associated with depression and anxiety). For example, Binder et al. (2008) identified four SNPs in the FKBP5 gene interacting with ELS to predict heightened PTSD symptom severity; similar findings were reported by Klengel et al. (2013), however their results provided robust findings for only the rs1360780 SNP. Presence of the met allele in the val66met BDNF polymorphism in conjunction with ELS predicted greater depression and anxiety symptoms, although this was specifically mediated through diminished left prefrontal cortex brain volume and heightened heart rate (Gatt et al., 2009). The rs139832701 SNP in OXTR interacted with ELS to predict increased stress and depression scores (Myers et al., 2014).

Candidate gene studies have often been criticized for being statistically underpowered, and large-scale replication attempts have not supported previously reported gene-by-environment interactions. In addition to the Culverhouse et al. (2018) study, another recent large-state analysis imputed data (i.e., did not genotype directly, but inferred genotype from tagging single nucleotide polymorphisms) from large population-based and case-control samples (Ns ranging from 62,138 to 443,264 across subsamples) for 18 candidate genes (including SLC6A4 and BDNF, but not FKBP5 or OXTR) and also failed to find support for any main effect or interaction predicting depression (Border et al., 2019). These authors went further than Culverhouse et al. (2018), concluding “it is time for depression research to abandon historical candidate gene and candidate gene-by-environment interaction hypotheses” (p. 386).

The criticism of candidate genes raises important concerns about sample size and false positive results. Yet, it is also possible that analyses that are limited to DNA sequence variations and one specific disease outcome miss much of the complexity by which genes, life experience, and health outcomes are interrelated. For example, it is possible that additional mechanisms that have not been considered in the prior literature, such as alternative splicing of the human SLC6A4 (Bradley and Blakely, 1997), contribute to inconsistent findings across study population. The effects of alternative splicing, as well as epigenetic mechanisms (discussed next), would be evident at the level of mRNA or protein expression, for which there are currently only limited datasets available.

The current literature on epigenetics and life stress suggests important mechanisms linking ELS to epigenetic gene regulatory mechanisms, particularly DNA methylation. DNA methylation is the process by which a methyl group binds to, most typically, Cytosin-Guanine (CpG) sites on DNA and regulates its expression (for further information see Moore et al., 2013). Such methylation may be caused by life stress. As early as in utero, experiences related to maternal nutrition and health can lead to an increased risk for metabolic dysregulation (e.g., in insulin and leptin) later in life with ELS-induced adaptations in DNA methylation as a proposed pathway to such a relationship (Gluckman et al., 2008). Therefore, examining how ELS is associated with methylation may provide insight into one pathway toward dysregulation.

Several studies have reported increased DNA methylation in the presence of ELS. First reported in rats in a seminal study by Weaver et al. (2004), poor maternal care was linked to increased methylation of the glucocorticoid receptor (GR) gene promoter, reduced GR expression in the hippocampus, and increased adult stress reactivity, which could be reversed with administration of the histone deacetylase (HDAC) inhibitor trichostatin A (TSA). A study by McGowan et al. (2009) extended these findings to humans, showing increased GR methylation and reduced GR mRNA expression in the hippocampus of suicide victims with a history of childhood abuse, compared to suicide victims without childhood abuse and non-suicide controls. In other work, adult participants who had experienced physical abuse as children had higher SCL6A4 DNA methylation in blood relative to those who had not (Beach et al., 2010). Those with major depressive disorder (MDD) who had experienced ELS also exhibited a greater percentage of average methylation of SLC6A4 in blood cells compared to those with MDD who had not experienced ELS (Kang et al., 2013). In those with PTSD, the ELS group had a greater proportion of transcripts with methylated CpG sites in blood cells compared to the no ELS group (Mehta et al., 2013). Evidence for ELS and methylation exists across species as well. Rats that experienced abusive behavior during development by stressed mothers showed increased DNA methylation of BDNF in the prefrontal cortex at exons IV and IX (Roth et al., 2009). Finally, the presence of methylation may be a function of both genotype and the presence of ELS. For instance, Duman and Canli (2015) found that presence of the S allele in the serotonin-transporter-linked polymorphic region (5-HTTLPR) interacted with ELS to predict greater average methylation of SCL6A4 in blood samples; however, this did not correspond to downstream mRNA expression, suggesting more than just DNA methylation effects need to be considered. ELS interacted with rs1360780 in FKBP5 such that presence of the T allele in conjunction with ELS was associated with decreased methylation percentage of intron 7 in blood cells (Klengel et al., 2013). This evidence collectively suggests that methylation may represent one pathway to poorer health.

Conclusions and Future Recommendations

It is now widely accepted that ELS is linked to significant adverse sequelae in adulthood (Enoch, 2011; Shonkoff et al., 2012). However, this association needs to be better understood in its nuances. For instance, different types of ELS may be differentially associated with health risk; although most forms of ELS are associated with increased risk of psychopathology, surprisingly, this association was weaker for forms of physical neglect (Carr et al., 2013). This may stem from discrepancies in the severity of ELS types or from differences in the response (or lack thereof) to different ELS types. Negative consequences of ELS may be most pronounced when the stress takes on its most severe forms (Caspi et al., 2003; Kendler et al., 2004), when there are numerous instances of ELS (Heim et al., 2002; Dube et al., 2003; Myers et al., 2014), or in the context of other moderating factors. This includes, but is certainly not limited to, genetic disposition (Nugent et al., 2011) and ELS-related epigenetic modifications of genes involved in the stress systems (Heim and Binder, 2012).

Another consideration is that ELS perhaps does not present a unique threat to underlying physiology relative to other forms of stress. In one area of thought, ELS is unique because it takes place during developmentally sensitive periods, where underlying physiology later in life is particularly vulnerable to stressful experiences (Lupien et al., 2009). However, other evidence calls into doubt the singular role of ELS in that some forms of stress have a profound impact regardless of their timing. For example, sexual abuse, whether it occurs early in life or later on in adulthood, has been linked to a host of somatic disorders, including gastrointestinal problems and chronic pain (Paras et al., 2009). Similarly, an increase in stressful life events (regardless of age that the stressors occurred) was associated with increased depression (Risch et al., 2009) and evidence exists that such lifelong stress interacts with the presence of the S allele on 5-HTTLPR to predict increased rates of depression (Caspi et al., 2003), although this finding continues to generate debate (Karg et al., 2011; Culverhouse et al., 2018). Further complicating this narrative is the notion that different types of ELS co-occur (Merrick et al., 2018). Therefore, the detrimental effects of stress may not be restricted to the early developmental period, but rather might be determined by severity and number of different stressors.

Based on these considerations, we make three recommendations for the field to advance: (1) begin with rigorous operational definitions of ELS, thus making it easier to measure and compare findings across studies. At present, there are numerous methodologies to measure ELS (e.g., questionnaires (Bernstein et al., 1994), interview methods (Bremner et al., 2000), or by asking a social worker or caregiver if previous abuse has occurred), all potentially introducing unique variance that may help explain some of the inconsistent results. Showing correlations between instrument types within the same study (e.g., validating a social worker’s report with a high score on a standardized questionnaire by the trauma survivor) may set a gold standard to interpret any findings. (2) Consider ELS in a larger genetic and environmental context. This would span genetic profiles for multiple genes of interest or polygenic risk scores (for further information see Dudbridge, 2013), as well as current stressors in the person’s life and presence of social support (Heim et al., 2008; Daskalakis et al., 2013). (3) Conduct research in ways that mitigate, reframe, or reverse the consequences of ELS. Teaching children appropriate coping mechanisms and building social networks (Werner, 1995) may act as deterrents to these negative outcomes. Likewise, in applying lessons from the animal literature, environmental enrichment (i.e., cognitive stimulation and physical activity) may act as another mechanism to help mitigate negative effects (Fox et al., 2006).

Author Contributions

NF wrote the initial draft. TC revised the initial draft. Both TC and NF conceptualized the material for review.

Conflict of Interest Statement

The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest.

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Keywords: early life stress, sympathetic nervous system, hypothalamic-pituitary-adrenal axis, inflammation, genetics, epigenetics

Citation: Fogelman N and Canli T (2019) Early Life Stress, Physiology, and Genetics: A Review. Front. Psychol. 10:1668. doi: 10.3389/fpsyg.2019.01668

Received: 23 December 2018; Accepted: 02 July 2019;
Published: 02 August 2019.

Edited by:

Rosario Montirosso, Eugenio Medea (IRCCS), Italy

Reviewed by:

Richard G. Hunter, University of Massachusetts Boston, United States
Eva Unternaehrer, Universität Konstanz, Germany

Present address:

Nia Fogelman, Department of Psychiatry, Yale University School of Medicine, New Haven, CT, United States

Copyright © 2019 Fogelman and Canli. This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.

*Correspondence: Nia Fogelman, nia.fogelman@yale.edu

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