Advertisement
Browse Subject Areas
?

Click through the PLOS taxonomy to find articles in your field.

For more information about PLOS Subject Areas, click here.

  • Loading metrics

Open Access

Peer-reviewed

Research Article

Diurnal Cortisol Patterns and Dexamethasone Suppression Test Responses in Healthy Young Adults Born Preterm at Very Low Birth Weight

  • Nina Kaseva ,

    nina.kaseva@fimnet.fi

    Affiliation Chronic Disease Prevention Unit, Department of Health, National Institute for Health and Welfare, Helsinki, Finland

  • Riikka Pyhälä,

    Affiliations Institute of Behavioural Sciences, University of Helsinki, Helsinki, Finland, Folkhälsan Research Centre, Helsinki, Finland

  • Anu-Katriina Pesonen,

    Affiliation Institute of Behavioural Sciences, University of Helsinki, Helsinki, Finland

  • Katri Räikkönen,

    Affiliation Institute of Behavioural Sciences, University of Helsinki, Helsinki, Finland

  • Anna-Liisa Järvenpää,

    Affiliation Children’s Hospital, Helsinki University Central Hospital and University of Helsinki, Helsinki, Finland

  • Sture Andersson,

    Affiliation Children’s Hospital, Helsinki University Central Hospital and University of Helsinki, Helsinki, Finland

  • Johan G. Eriksson,

    Affiliations Chronic Disease Prevention Unit, Department of Health, National Institute for Health and Welfare, Helsinki, Finland, Folkhälsan Research Centre, Helsinki, Finland, Department of General Practice and Primary Health Care, University of Helsinki and Helsinki University Hospital, Helsinki, Finland, Vasa Central Hospital, Vasa, Finland

  • Petteri Hovi,

    Affiliations Chronic Disease Prevention Unit, Department of Health, National Institute for Health and Welfare, Helsinki, Finland, Children’s Hospital, Helsinki University Central Hospital and University of Helsinki, Helsinki, Finland

  • Eero Kajantie

    Affiliations Chronic Disease Prevention Unit, Department of Health, National Institute for Health and Welfare, Helsinki, Finland, Children’s Hospital, Helsinki University Central Hospital and University of Helsinki, Helsinki, Finland, PEDEGO Research Group, Medical Research Center Oulu, Oulu University Hospital and University of Oulu, Oulu, Finland

Abstract

Background

Early life stress, such as painful and stressful procedures during neonatal intensive care after preterm birth, can permanently affect physiological, hormonal and neurobiological systems. This may contribute to altered programming of the hypothalamic-pituitary-adrenal axis (HPAA) and provoke changes in HPAA function with long-term health impacts. Previous studies suggest a lower HPAA response to stress in young adults born preterm compared with controls born at term. We assessed whether these differences in HPAA stress responsiveness are reflected in everyday life HPAA functioning, i.e. in diurnal salivary cortisol patterns, and reactivity to a low-dose dexamethasone suppression test (DST), in unimpaired young adults born preterm at very low birth weight (VLBW; <1500 g).

Methods

The participants were recruited from the Helsinki Study of Very Low Birth Weight Adults cohort study. At mean age 23.3 years (2.1 SD), 49 VLBW and 36 controls born at term participated in the study. For cortisol analyzes, saliva samples were collected on two consecutive days at 0, 15, 30 and 60 min after wake-up, at 12:00 h, 17:00 h and 22:00 h. After the last salivary sample of the first study day the participants were instructed to take a 0.5 mg dexamethasone tablet.

Results

With mixed-effects model no difference was seen in overall diurnal salivary cortisol between VLBW and control groups [13.9% (95% CI: -11.6, 47.0), P = 0.31]. Salivary cortisol increased similarly after awakening in both VLBW and control participants [mean difference -2.9% (29.2, 33.0), P = 0.85]. Also reactivity to the low-dose DST (awakening cortisol ratio day2/day1) was similar between VLBW and control groups [-1.1% (-53.5, 103.8), P = 0.97)].

Conclusions

Diurnal cortisol patterns and reactivity to a low-dose DST in young adulthood were not associated with preterm birth.

Citation: Kaseva N, Pyhälä R, Pesonen A-K, Räikkönen K, Järvenpää A-L, Andersson S, et al. (2016) Diurnal Cortisol Patterns and Dexamethasone Suppression Test Responses in Healthy Young Adults Born Preterm at Very Low Birth Weight. PLoS ONE 11(9): e0162650. https://doi.org/10.1371/journal.pone.0162650

Editor: Umberto Simeoni, Centre Hospitalier Universitaire Vaudois, FRANCE

Received: May 13, 2016; Accepted: August 28, 2016; Published: September 12, 2016

Copyright: © 2016 Kaseva et al. This is an open access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.

Data Availability: All relevant data are within the paper. There are ethical and legal restrictions preventing the data from being made publicly available. Data can be made available from the he Helsinki Study of Very Low Birth Weight Adults cohort study. Possible data requests should be directed to the Chronic Disease Prevention Unit, National Institute for Health and Welfare, Helsinki directly to Dr Eero Kajantie (eero.kajantie@thl.fi). The requests may be subject to further ethics review and/or individual consent.

Funding: This study was supported by grants from the Medical Societies of Finland (Duodecim and Finska Läkaresällskapet to NK), the Finnish Foundation of Paediatric Research (to EK), Academy of Finland (grants 127437, 129306, 130326, 134791 and 263924 to EK), the Emil Aaltonen Foundation (to EK), the Jalmari and Rauha Ahokas Foundation (to EK), the Juho Vainio Foundation, the Novo Nordisk Foundation, the Signe and Ane Gyllenberg Foundation (to NK), the Sigrid Jusélius Foundation (to EK) and the Yrjö Jahnsson Foundation. The funders had no role in study design, data collection and analysis, decision to publish, or preparation of the manuscript.

Competing interests: The authors have declared that no competing interests exist.

Introduction

Cortisol secretion shows a diurnal pattern with a decrease from morning to evening levels [1]. This diurnal rhythm is an important marker of hypothalamic-pituitary-adrenal axis (HPAA) regulation [2], and it is established during the first year of life [3], in some infants even at 2 months of age [4]. It has been suggested that pre- and postnatal stress, and subsequent cortisol exposure, could alter and “program” HPAA function and thus affect health over the life course [5]. In infants born preterm, frequent invasive, painful and stressful treatment procedures performed during neonatal intensive care, are examples of such early life stress. Furthermore, the preterm infant with immature physiological systems, is particularly vulnerable during this time of early life stress and simultaneous programming of the stress systems [6].

Increased cortisol exposure, normally tightly regulated by the HPAA, is associated with development of several adverse health outcomes, including cardiovascular disease, osteoporosis and insulin resistance [7]. Similarly, preterm birth is linked with an increased risk for these conditions. As adults, individuals born preterm at very low birth weight (VLBW, ≤ 1500 g), have higher blood pressure [8,9], changes in lipid profile [9,10], lower mineral bone density [11,12] and impaired glucose regulation [12,13], compared with peers born at term. Based on current literature, HPAA functioning, especially in relation to stress responses, may be altered in those born preterm [1420], although the results have been inconsistent. Assuming that preterm birth provokes durable changes in adult HPAA function, this could modify adult health. To clarify the role of preterm birth on adult HPAA function we examined diurnal cortisol patterns and cortisol feedback inhibition by a low-dose dexamethasone suppression test (DST) in healthy young adults born preterm at VLBW and controls born at term.

Methods

Participants

The data come from the Helsinki Study of Very Low Birth Weight Adults, a case-control cohort which has previously been described in detail [13]. The original cohort included 335 subjects born preterm at VLBW during 1978–1985 and discharged alive from the neonatal intensive care unit serving one regional area in southern Finland, and 314 controls born at term, group-matched for sex, age and birth hospital. In 2004–2005, those 255 VLBW and 314 control subjects who were residing in the greater Helsinki area were invited to participate in a clinical examination. Of these invited subjects, 166 VLBW and 172 controls chose to participate. During 2005 a random sample among the participants (166 VLBW and 172 controls) of the cohort’s first clinical visit in 2004–2005 was invited to participate in the current study, selected as previously described [20]. Briefly, we excluded individuals who 1) used glucocorticoids, 2) had a nightshift during the previous week or 3) were unable to stand or manage without an assistant. A total of 49 VLBW (26 men and 23 women) and 36 controls (14 men and 22 women) provided adequate salivary samples and were included in the analyses (Fig 1). Anthropometry was measured and all participants completed a detailed questionnaire regarding health status, including smoking habits, medical history and medications.

thumbnail
Download:
Fig 1. Flow chart of the study population.

https://doi.org/10.1371/journal.pone.0162650.g001

Ethics.

The study was performed according to the Declaration of Helsinki. The Ethics Committee of the Helsinki and Uusimaa Hospital District approved the study protocol. Written informed consent was obtained from each participant.

Non-participant analysis.

We compared perinatal and current descriptive characteristics between the participants of this study (49 VLBW and 36 controls) and the group they were recruited from (Fig 1), i.e. the remaining cohort that previously participated in a clinical examination (117 VLBW and 136 controls) (13). The sample was comparable to the birth cohort in terms of gestational age, birth weight, sex, incidence of pre-eclampsia and multiple pregnancy (all P-values ≥ 0.1). Of the sample, 47% of VLBW participants were small for gestational age (SGA) [21] compared to 28% in the group they were recruited from (P = 0.03). Age, daily smoking, hormonal contraception use, parental education, adult height and body mass index (BMI) were also similar between the participants of the current study and the group they were recruited from (all P-values ≥ 0.1).

Measures and procedures

As a marker of HPAA function we used diurnal salivary cortisol profiles. We collected saliva samples using Salivette® (Sarstedt, Nümbrecht, Germany) on two consecutive days at 0, 15, 30 and 60 min after wake-up, at 12:00 h, 17:00 h and 22:00 h.

After the last salivary sample of the first study day, at 22:00 h, the participants were instructed to take a 0.5 mg dexamethasone tablet. The cortisol response to the DST was calculated as the difference between log-transformed awakening cortisol on days 2 and 1, back-transformed to indicate the Day 2/ Day 1 ratio. We chose this dose of dexamethasone because our aim was to assess individual variation in normal HPAA suppression rather than to assess endocrine disorders, for which higher doses are used in routine endocrine practice.

The cortisol concentrations were determined using a competitive solid-phase, time-resolved fluorescence immunoassay with fluorometric end point detection (DELFIA, Wallac, Turku, Finland). Cortisol measurements were assayed in duplicate (University of Trier, Germany).

Statistical analyses.

All statistical analyses were conducted with IBM SPSS Statistics 21 (SPSS Inc., Chicago, IL, USA). The significance level was set to two-tailed P < 0.05. We compared descriptive characteristics between VLBW and control groups with t-test (continuous variables) and χ2-test (categorical variables).

To attain normality, cortisol concentrations were log-transformed. We analyzed overall diurnal cortisol with mixed-effects models, which has the advantage of taking into account within-subject correlation in studies with repeated measurements. We adjusted for age and sex in model 1; for age, sex and childhood socioeconomic status (SES; highest parental education) and maternal smoking during pregnancy in model 2; and for age, sex, highest parental education, maternal smoking during pregnancy, BMI, smoking and use of hormonal contraception in model 3. We additionally adjusted for menstrual cycle phase in model 4 if data was available. The results are presented as mean differences (%) and 95% confidence intervals (CI) between VLBW and control groups.

We tested if VLBW and control groups have different trajectories of diurnal cortisol by including an interaction term with sampling time (time*VLBW status). We also assessed sex differences by interaction terms (sex*VLBW status and sex*time*VLBW status).

To compare common indicators of diurnal cortisol patterns, i.e. awakening, peak after awakening, cortisol awakening response (CAR) and 22:00 h concentrations, we used multiple linear regression models. CAR describes the increase in cortisol concentration 30–45 min after awakening and reflects the adrenal capacity to stress response [22]. The CAR was calculated as 1) peak after awakening minus value at awakening and 2) as the area under the curve (AUC), calculated from the first four salivary samples (0, 15, 30 and 60 min post awakening). Diurnal AUC was calculated from all seven salivary samples collected (0, 15, 30 and 60 min post awakening and 12:00, 17:00 and 22:00 h).

Results

Within the VLBW group, gestational age ranged between 24.1 and 35.6 weeks (mean 29.4 weeks), and within controls between 38.0 and 42.3 weeks (mean 40.2 weeks). Birth weights ranged between 600 and 1500 g (mean 1099 g) and between 2880 and 4900 g (mean 3641 g), respectively. Detailed descriptive characteristics of the participants are shown in Table 1.

thumbnail
Download:
Table 1. Descriptive characteristics of the participants.

https://doi.org/10.1371/journal.pone.0162650.t001

Cortisol awakening response (CAR)

As expected, salivary cortisol increased after awakening in both VLBW and control groups (Table 2). We found no differences in CAR between VLBW and control groups [-2.9% (95% CI: 29.2, 33.0), P = 0.85].

thumbnail
Download:
Table 2. Diurnal salivary cortisol of the study participants, before (Day 1) and after (Day 2) a low-dose dexamethasone suppression test.

https://doi.org/10.1371/journal.pone.0162650.t002

Diurnal cortisol

Diurnal cortisol patterns were similar in VLBW and control groups (Fig 2). With mixed model no difference was seen in overall diurnal cortisol [13.9% (95% CI: -11.6, 47.0), P 0.31] when adjusting for age and sex. Further adjusting for childhood socioeconomic status in model 2; BMI, smoking and use of hormonal contraception in model 3 and for menstrual cycle phase in model 4 did not change the results (Table 3, all P-values ≥ 0.31). Also diurnal AUC and evening cortisol were similar in both groups (Table 2).

thumbnail
Download:
Fig 2. Diurnal cortisol patterns and dexamethasone suppression test responses of the participants.

Diurnal salivary cortisol concentrations during Day 1 and after a low-dose dexamethasone suppression test (Day 2) among adults born preterm at very low birth weight (VLBW; <1500g) (continuous lines) and controls born at term (dashed lines).

https://doi.org/10.1371/journal.pone.0162650.g002

thumbnail
Download:
Table 3. Mixed model results, showing overall differences in daily salivary cortisol concentrations between very low birth weight (VLBW, <1500g) and control participants, presented as mean differences (95% CI).

https://doi.org/10.1371/journal.pone.0162650.t003

Dexamethasone suppression test

After the low-dose DST we found a lower CAR in the VLBW group (1.4 vs. 2.3, P = 0.04, Table 2), this difference did not remain statistically significant after further adjusting for confounders in models 2–4. Also the awakening and diurnal AUC were similar in both groups (P ≥ 0.68).

Men and women

We tested for sex, group and time interactions. No two-way or three-way interactions were found in analyses of any outcome measures (mixed model P-values for interaction terms across the different adjustment models were as follows: sex*VLBW status ≥ 0.67; time*VLBW status ≥ 0.33; sex*time*VLBW status ≥ 0.57) and therefore the results are presented with men and women combined. As sex differences are a common characteristic of HPAA stress response studies, we reran all analyses with men and women separately (Table 3). Overall diurnal cortisol, comparing men only [8.8% (95% CI: -31.3, 72.2), P = 0.71], and women only [18.8% (95% CI:-11.8, 60.0) P = 0.25], showed no significant differences between VLBW and control groups.

History of depression

Of the participants, 6 (12.2%) VLBW and 5 (13.9%) controls had history of depression diagnosed by a physician. We reran all the analyses after excluding the VLBW and control participants with diagnosed depression. The results remained similar.

Small and appropriate for gestational age

Within the VLBW group 23 (46.9%) participants were born SGA. We reran all the analyses comparing those 23 VLBW born SGA with the 26 born appropriate for gestational age (AGA, birth weight ≥ -2SD). There were no significant differences in diurnal cortisol or DST responses between SGA and AGA VLBW participants (Table 3).

Discussion

We found no difference in diurnal salivary cortisol patterns in healthy VLBW and control young adults. The results remained after adjustment for important confounders, including age, sex, SES, BMI, smoking, use of hormonal contraception and menstrual cycle phase, as applicable. We further found no difference in the response to a low-dose DST between VLBW and control groups, measured as overall cortisol and AUC (awakening and diurnal). The lower awakening cortisol after the low-dose DST attained nominal statistical significance, but this finding was attenuated after adjustment for confounders.

Neonatal exposure to stress or maternal cortisol can permanently modify HPAA function, and thereby have long-term health impacts [23,24]. Our finding of similar diurnal cortisol patterns in VLBW and control groups suggest similar HPAA function in everyday situations. This is an important finding, taking into account the higher risk of disease and increased risk factors largely reported in VLBW adults [8,9,12,13]. Although prior studies on the effects of preterm birth on diurnal cortisol patterns have been few, one study recently reported lower waking cortisol (P<0.039) and attenuated diurnal cortisol decline from waking to bedtime (P<0.035) in prematurely born men, aged 21–23 years, compared with term-born men [25]. In line with our findings, Lee et al. also reported similar waking cortisol and diurnal cortisol patterns in prematurely born women compared with term-born controls [25]. In contrast to these findings, in an explorative examination, another study showed that individuals born preterm or with small birth weight (< 2500g) had higher evening and total cortisol levels at 43 years of age [26]. We are unaware of any further similar studies in adults. However, Grunau et al. measured hair cortisol levels, an integrated index of endogenous HPAA activity, in preterm children at seven years of age, and reported lower hair cortisol levels in preterm compared to term-born children [18]. This finding suggests persistent alteration of stress system programming in preterm children extending into school age.

Interindividual variations in cortisol concentrations are considerable. We previously reported 17.2% lower plasma cortisol responses [(95% CI: -28.9, -3.5) P = 0.02] after a standardized stressor, the Trier Social Stress Test [27], in the same VLBW adults we now report on, when compared with controls born at term [20]. The 95% CI’s of this finding of lower cortisol responses after stress fit in the 95% CI’s of the current results, and we are unable to detect such small differences in this study.

There are limitations to our study. Notably, the sample size is relatively small. This may diminish possibilities of finding associations in subgroups, i.e. evaluation of sexes separately. Furthermore, a higher proportion of the VLBW participants of the current study were born SGA, 47% compared to 28%, than in the group they were recruited from. Lifetime stressful experiences and current perceived stress affect HPAA function and we were unable to control for these factors in the analyses.

Strengths of our study include collecting seven cortisol samples in duplicate on two consecutive days. We were able to adjust for important confounders in the analyses, including use of hormonal contraception. A strength of our study population is the age-, sex- and birth hospital-matched control group.

Conclusions

Our study contribute to the growing literature on the effects of early life stress on later HPAA functioning. To conclude, although previous literature suggests that HPAA stress response is altered in VLBW individuals [1420], diurnal cortisol patterns in everyday situations and after a low-dose DST challenge seem similar in healthy VLBW and control young adults.

Acknowledgments

We are grateful to all the participants of this study.

Author Contributions

  1. Conceptualization: A-KP KR A-LJ SA JGE PH EK.
  2. Data curation: NK RP PH EK.
  3. Formal analysis: NK PH EK.
  4. Funding acquisition: NK A-KP KR SA JGE EK.
  5. Investigation: RP A-KP KR.
  6. Methodology: RP A-KP KR EK.
  7. Project administration: A-KP KR A-LJ SA JGE EK.
  8. Resources: SA JGE EK.
  9. Supervision: EK.
  10. Visualization: NK.
  11. Writing – original draft: NK.
  12. Writing – review & editing: RP A-KP KR A-LJ SA JGE PH EK.

References

  1. 1. Sherman B, Wysham C, Pfohl B. Age-related changes in the circadian rhythm of plasma cortisol in man. J Clin Endocrinol Metab 1985 Sep;61(3):439–443. pmid:4019712
  2. 2. Rosmalen JG, Oldehinkel AJ, Ormel J, de Winter AF, Buitelaar JK, Verhulst FC. Determinants of salivary cortisol levels in 10–12 year old children; a population-based study of individual differences. Psychoneuroendocrinology 2005 Jun;30(5):483–495. pmid:15721059
  3. 3. Tollenaar MS, Jansen J, Beijers R, Riksen-Walraven JM, de Weerth C. Cortisol in the first year of life: normative values and intra-individual variability. Early Hum Dev 2010 Jan;86(1):13–16. pmid:20051312
  4. 4. de Weerth C, Zijl RH, Buitelaar JK. Development of cortisol circadian rhythm in infancy. Early Hum Dev 2003 Aug;73(1–2):39–52. pmid:12932892
  5. 5. Kajantie E, Räikkönen K. Early life predictors of the physiological stress response later in life. Neurosci Biobehav Rev 2010 Sep;35(1):23–32. pmid:19931557
  6. 6. Matthews SG. Early programming of the hypothalamo-pituitary-adrenal axis. Trends Endocrinol Metab 2002 Nov;13(9):373–380. pmid:12367818
  7. 7. McEwen BS. Protective and damaging effects of stress mediators. N Engl J Med 1998 Jan 15;338(3):171–179. pmid:9428819
  8. 8. de Jong F, Monuteaux MC, van Elburg RM, Gillman MW, Belfort MB. Systematic review and meta-analysis of preterm birth and later systolic blood pressure. Hypertension 2012 Feb;59(2):226–234. pmid:22158643
  9. 9. Parkinson JR, Hyde MJ, Gale C, Santhakumaran S, Modi N. Preterm birth and the metabolic syndrome in adult life: a systematic review and meta-analysis. Pediatrics 2013 Apr;131(4):e1240–63. pmid:23509172
  10. 10. Hovi P, Kajantie E, Soininen P, Kangas AJ, Järvenpää AL, Andersson S, et al. Lipoprotein subclass profiles in young adults born preterm at very low birth weight. Lipids Health Dis 2013 Apr 30;12:57-511X-12-57.
  11. 11. Hovi P, Andersson S, Järvenpää AL, Eriksson JG, Strang-Karlsson S, Kajantie E, et al. Decreased bone mineral density in adults born with very low birth weight: a cohort study. PLoS Med 2009 Aug;6(8):e1000135. pmid:19707270
  12. 12. Smith CM, Wright NP, Wales JK, Mackenzie C, Primhak RA, Eastell R, et al. Very low birth weight survivors have reduced peak bone mass and reduced insulin sensitivity. Clin Endocrinol (Oxf) 2011 Oct;75(4):443–449.
  13. 13. Hovi P, Andersson S, Eriksson JG, Järvenpää AL, Strang-Karlsson S, Mäkitie O, et al. Glucose regulation in young adults with very low birth weight. N Engl J Med 2007 May 17;356(20):2053–2063. pmid:17507704
  14. 14. Buske-Kirschbaum A, Krieger S, Wilkes C, Rauh W, Weiss S, Hellhammer DH. Hypothalamic-pituitary-adrenal axis function and the cellular immune response in former preterm children. J Clin Endocrinol Metab 2007 Sep;92(9):3429–3435. pmid:17566098
  15. 15. Grunau RE, Haley DW, Whitfield MF, Weinberg J, Yu W, Thiessen P. Altered basal cortisol levels at 3, 6, 8 and 18 months in infants born at extremely low gestational age. J Pediatr 2007 Feb;150(2):151–156. pmid:17236892
  16. 16. Grunau RE, Tu MT, Whitfield MF, Oberlander TF, Weinberg J, Yu W, et al. Cortisol, behavior, and heart rate reactivity to immunization pain at 4 months corrected age in infants born very preterm. Clin J Pain 2010 Oct;26(8):698–704. pmid:20664338
  17. 17. Brummelte S, Grunau RE, Zaidman-Zait A, Weinberg J, Nordstokke D, Cepeda IL. Cortisol levels in relation to maternal interaction and child internalizing behavior in preterm and full-term children at 18 months corrected age. Dev Psychobiol 2011 Mar;53(2):184–195. pmid:21298633
  18. 18. Grunau RE, Cepeda IL, Chau CM, Brummelte S, Weinberg J, Lavoie PM, et al. Neonatal pain-related stress and NFKBIA genotype are associated with altered cortisol levels in preterm boys at school age. PLoS One 2013 Sep 16;8(9):e73926. pmid:24066085
  19. 19. de Graaf J, van den Akker EL, van Lingen RA, Groot Jebbink LJ, de Jong FH, Grunau RE, et al. Five-year follow-up of effects of neonatal intensive care and morphine infusion during mechanical ventilation on diurnal cortisol rhythm. J Pediatr 2014 Sep;165(3):459–463.e2. pmid:24996988
  20. 20. Kaseva N, Wehkalampi K, Pyhälä R, Moltchanova E, Feldt K, Pesonen AK, et al. Blunted hypothalamic-pituitary-adrenal axis and insulin response to psychosocial stress in young adults born preterm at very low birth weight. Clin Endocrinol (Oxf) 2014 Jan;80(1):101–106.
  21. 21. Pihkala J, Hakala T, Voutilainen P, Raivio K. Characteristic of recent fetal growth curves in Finland. Duodecim 1989;105(18):1540–1546. pmid:2680445
  22. 22. Kudielka BM, Wust S. Human models in acute and chronic stress: assessing determinants of individual hypothalamus-pituitary-adrenal axis activity and reactivity. Stress 2010 Jan;13(1):1–14. pmid:20105052
  23. 23. Räikkönen K, Seckl JR, Heinonen K, Pyhälä R, Feldt K, Jones A, et al. Maternal prenatal licorice consumption alters hypothalamic–pituitary–adrenocortical axis function in children. Psychoneuroendocrinology 2010 11;35(10):1587–1593. pmid:20510523
  24. 24. Reynolds RM, Labad J, Buss C, Ghaemmaghami P, Räikkönen K. Transmitting biological effects of stress in utero: implications for mother and offspring. Psychoneuroendocrinology 2013 Sep;38(9):1843–1849. pmid:23810315
  25. 25. Lee J, Fried R, Thayer Z, Kuzawa CW. Preterm delivery as a predictor of diurnal cortisol profiles in adulthood: evidence from Cebu, Philippines. Am J Hum Biol 2014 Sep-Oct;26(5):598–602. pmid:24898414
  26. 26. Gustafsson PE, Janlert U, Theorell T, Hammarstrom A. Is body size at birth related to circadian salivary cortisol levels in adulthood? Results from a longitudinal cohort study. BMC Public Health 2010 Jun 17;10:346-2458-10-346.
  27. 27. Kirschbaum C, Pirke KM, Hellhammer DH. The 'Trier Social Stress Test'-a tool for investigating psychobiological stress responses in a laboratory setting. Neuropsychobiology 1993;28(1–2):76–81. pmid:8255414