The effects of an acute laboratory stressor on cortisol and sympathetic response in individuals with rheumatoid arthritis and osteoarthritis controls

Huyser, Bruce A.

January 1997

Thesis (Ph. D.)--University of Missouri-Columbia, 1997. / Typescript. Vita. Includes bibliographical references (leaves 45-56). Also available on the Internet.

The impact of proinflammatory cytokines upon adult hippocampal cell proliferation: implications for depression /

Sǧuin, Julie Anne,

January 1900

Thesis (M.Sc.) - Carleton University, 2007. / Includes bibliographical references (p. 66-91). Also available in electronic format on the Internet.

The role of the androgen receptor in anxiety-related behaviors, the hypothalamic pituitary adrenal axis, and sensorimotor gating studies in rodents with the testicular feminization mutation /

Zuloaga, Damian.

January 2008

Thesis (PH. D.)--Michigan State University. Dept. of Psychology, 2008. / Title from PDF t.p. (viewed on Sept. 8, 2009) Includes bibliographical references (p. 157-178). Also issued in print.

Evaluation of the effects of stress on the sympathetic nervous system and hypothalamic-pituitary-adrenal axis in cats with feline interstitial cystitis

Westropp, Jodi Lynn,

January 2005

Thesis (Ph. D.)--Ohio State University, 2005. / Title from first page of PDF file. Document formatted into pages; contains xii, 153 p.; also includes graphics (some col.) Includes bibliographical references (p. 132-153). Available online via OhioLINK's ETD Center

Seasonal plasticity of physiological systems, brain, and behavior

Pyter, Leah M,

January 2006

Thesis (Ph. D.)--Ohio State University, 2006. / Title from first page of PDF file. Includes bibliographical references (p. 198-229).

Άξονας υποθάλαμος-υπόφυση-επινεφρίδια και μεταβολικό σύνδρομο

Καζάκου, Παρασκευή

17 September 2012

Το μεταβολικό σύνδρομο, αποτελεί ένα σύνολο διαταραχών, όπως η κοιλιακή παχυσαρκία, η υπεργλυκαιμία, η χαμηλή HDL χοληστερόλη (HDL-C), τα αυξημένα τριγλυκερίδια (ΤRG) και η υπέρταση. Αν και η συχνότητα του παρουσιάζεται συνεχώς αυξανόμενη παγκοσμίως, η παθογένειά του, καθώς και τα διαγνωστικά κριτήρια, παραμένουν όχι σαφώς προσδιορισμένα. Φαίνεται να σχετίζεται με τη δραστηριότητα του άξονα ΥΥΕ, όμως ο υποκείμενος μηχανισμός παραμένει ασαφής. Σκοπός της παρούσης μελέτης ήταν να διερευνήσουμε τη λειτουργία του άξονα ΥΥΕ σε ασθενείς με μεταβολικό σύνδρομο και να εξετάσουμε αν η δραστηριότητα του άξονα ΥΥΕ σχετίζεται με τα επί μέρους στοιχεία του μεταβολικού συνδρόμου. Υλικό και Μέθοδος: Μελετήθηκαν 159 συνολικά άτομα, τα οποία χωρίστηκαν σε δύο ομάδες. Η πρώτη ομάδα (ομάδα ατόμων με μεταβολικό σύνδρομο) περιελάμβανε 86 άτομα με μεταβολικό σύνδρομο, 48 άνδρες και 38 γυναίκες, μέσης ηλικίας 52.2±7.6 έτη, mean±SD, και με δείκτη σωματικής μάζας 30.5±5.35 kg/m², mean±SD. Η δεύτερη ομάδα (ομάδα ελέγχου) περιελάμβανε 73 υγιή άτομα (μάρτυρες), 19 άνδρες και 54 γυναίκες, μέσης ηλικίας 49.9±7.5 έτη, mean±SD, και με δείκτη μάζας σώματος 27.9±4.42 kg/m², mean±SD. Οι δύο ομάδες ήταν συγκρίσιμες ως προς την ηλικία. Όλα τα άτομα υπεβλήθησαν σε δοκιμασία ανοχής 75g γλυκόζης από το στόμα (OGTT) μετά από νηστεία 12 ωρών, και δείγματα αίματος ελήφθησαν για τον προσδιορισμό της ACTH, της κορτιζόλης, της ινσουλίνης, του C-πεπτιδίου και της γλυκόζης. Τα επίπεδα κορτιζόλης ορού μετά από δοκιμασία ολονύκτιας καταστολής με 1mg δεξαμεθαζόνης (DXM) μετρήθηκαν και στις δύο ομάδες. Αποτελέσματα: Οι ασθενείς με μεταβολικό σύνδρομο είχαν στατιστικώς σημαντικά υψηλότερα επίπεδα κορτιζόλης ορού μετά από ολονύκτια δοκιμασία καταστολής με δεξαμεθαζόνη σε σχέση με τους υγιείς μάρτυρες. Καθ’όλη τη διάρκεια της δοκιμασίας ΟGTT τα επίπεδα της ΑCTH πλάσματος ήταν υψηλότερα στην ομάδα με μεταβολικό σύνδρομο σε σύγκριση με την ομάδα ελέγχου, ενώ τα επίπεδα κορτιζόλης ορού ήταν συγκρίσιμα μεταξύ των δύο ομάδων. Σε όλους τους χρόνους της δοκιμασίας OGTT τα επίπεδα της γλυκόζης, της ινσουλίνης και του C-πεπτιδίου ήταν στατιστικώς σημαντικά υψηλότερα στην ομάδα με μεταβολικό σύνδρομο σε σύγκριση με την ομάδα ελέγχου. Επίσης, η ΑCTH κατά τη δοκιμασία OGTT παρουσίασε στατιστικώς σημαντική θετική συσχέτιση με το μεταβολικό σύνδρομο και τα περισσότερα στοιχεία του, ενώ δεν βρέθηκε συσχέτιση μεταξύ της κορτιζόλης κατά τη διάρκεια της δοκιμασίας OGTT και του μεταβολικού συνδρόμου. Συμπεράσματα: Ο άξονας ΥΥΕ φαίνεται να είναι περισσότερο δραστήριος στους ασθενείς με μεταβολικό σύνδρομο, όπως αποδεικνύεται από τα υψηλότερα επίπεδα κορτιζόλης μετά από ολονύκτια δοκιμασία καταστολής με δεξαμεθαζόνη και τα αυξημένα επίπεδα ACTH κατά τη διάρκεια της δοκιμασίας OGTT. Το εύρημα αυτό ενισχύει την άποψη ότι υφίσταται «λειτουργική» υπερκορτιζολαιμία στην εκδήλωση του μεταβολικού συνδρόμου. / Metabolic syndrome (MetS) is correlated with the activity of Hypothalamic-Pituitary-Adrenal axis (HPA) but the underlying mechanism still remains elusive.The aim of this study was to investigate the HPA axis function in patients with MetS. Materials/Methods: This case-control study included 159 people. They were divided into 2 groups. The first group included 73 healthy volunteers (control group: 19 male, 54 female, mean±SD: 49.9±7.5 years old, with BMI: 27.9±4.42 kg/m2) and the second group included 86 patients with MetS (case group: 48 male, 38 female, mean±SD: 52.2±7.6 years old, with BMI: 30.5±5.35 kg/m2). An oral glucose tolerance test (OGTT) was performed for all subjects after a 12-h overnight fast, and blood samples were obtained for determination of ACTH, cortisol, insulin, C-peptide, and glucose levels. Serum cortisol after an overnight dexamethasone suppression test was determined in both groups. Results: Patients with MetS had serum cortisol levels after an overnight dexamethasone suppression test significantly higher than controls. During OGTT plasma ACTH levels were higher at all time points in patients with MetS compared to controls, whereas serum cortisol levels were comparable between the 2 groups. Plasma ACTH during OGTT was also correlated with most of the components of MetS. Conclusions: The HPA axis in patients with MetS seems to be more active as evidenced by the higher cortisol levels after the overnight dexamethasone suppression test and by the higher ACTH levels during OGTT. This functional hypercortisolism might be involved in the pathogenesis of the metabolic syndrome.

Μεταβολικό σύνδρομο

616.399

Hypothalamic-pituitary-adrenal axis

Metabolic syndrome

Maternal Depression and Stress Response The Effect on Offspring in Emerging Adulthood

January 2011

abstract: Dysregulated cortisol has been linked to a variety of adverse physical and psychological consequences. Stressors in the childhood family environment can influence cortisol activity throughout development. For example, research has shown that both infants and children of depressed mothers exhibit altered levels of cortisol compared to infants and children of non-depressed mothers. It is unclear, however, whether exposure to maternal depression in childhood and adolescence is related to cortisol activity at later stages of development. The current study examined the longitudinal relation between maternal depressive symptoms during late childhood (9-12 years old) and adolescence (15-19 years old) and cortisol activity in offspring in young adulthood (24- 28 years old) in a sample of 40 young adults and their mothers. Maternal depressive symptoms were prospectively assessed at four time points across the 15 year study. Cortisol samples were collected from young adult offspring at the final time point. Findings revealed that higher levels of maternal depressive symptoms during late childhood were associated with lower total cortisol output in young adulthood. Results suggest that attenuated cortisol levels, which put these young adults at risk for a variety of stress-related physical and psychological illnesses, may be a long-term consequence of exposure to maternal depression,. Depressive symptoms in mothers during their child's adolescence, however, did not relate to cortisol output. These findings suggest a sensitive period in late childhood during which the development of HPA activity may be susceptible to the environmental stressor of maternal depression. / Dissertation/Thesis / M.A. Psychology 2011

Psychology

Psychobiology

Child Development

Cortisol

Hypothalamic Pituitary Adrenal Axis

Maternal Depression

Manque de sommeil et maladies métaboliques / Sleep and metabolic diseases

Guyon, Aurore

16 December 2013

La réduction du temps de sommeil est un phénomène de plus en plus courant. Un faisceau de données expérimentales et épidémiologiques suggère qu'un manque de sommeil pourrait être un facteur de risque d'obésité et de diabète. Dans un premier temps, puisque des modifications de l'axe Hypothalamo-Hypophyso-Surrénalien (HHS) pourraient sous- tendre la relation entre le manque de sommeil et les maladies métaboliques, j'ai évalué les effets de 2 nuits courtes sur ce système chez des jeunes hommes en bonne santé. Nous avons montré que 2 nuits de 4h au lit altéraient l'activité spontanée et la réactivité de l'axe HHS et que l'ampleur des altérations était corrélée à l'importance de la privation de sommeil. Dans un deuxième temps, j'ai tenté de déterminer si une extension de sommeil pouvait avoir des effets bénéfiques chez des jeunes obèses dormant habituellement peu. Nos résultats préliminaires montrent que par simple extension du temps passé au lit, des obèses dormant habituellement 6h, étaient capables de dormir 8h, une durée associée au plus faible risque d'obésité dans les études épidémiologiques, que leur appétit pour les aliments gras et salés et le grignotage diminuaient, que leurs taux de polypeptide pancréatique, une hormone anorexigène, étaient augmentés, et que leur prise calorique lors d'un buffet à volonté était d'autant plus diminuée que leur temps de sommeil était augmenté. Ce travail souligne l'importance d'une durée de sommeil suffisante pour une bonne santé métabolique et suggère que l'optimisation du sommeil pourrait constituer une alternative peu coûteuse pour la prévention et la prise en charge des maladies métaboliques / Voluntary sleep restriction is increasingly common in modern socities. Evidence from epidemiological and experimental studies suggest that sleep loss may be a risk factor for obesity and type 2 diabetes. First, since the modifications in Hypothalamic-Pituitary-adrenal (HPA) axis activity may underlie the relationship between sleep loss and metabolic diseases, 1 evaluated the effect of 2 short nights on this system in healthy lean young men. We showed that 2 nights of 4h in bed impaired spontaneous activity and the reactivity of the HPA axis and that the magnitude of these alterations was related of the severity of sleep loss. 1n a second step, 1 sought to determine if sleep extension could have a beneficial effect in young obese short sleepers. Our preliminary results showed that, by a simple bedtime extension, obese subjects usually sleeping 6h were able to sleep 8h, a duration associated with the lowest risk obesity risk in epidemiological studies. Moreover, their appetite for sweets and fat food, and snacking were decreased, the levels of pancreatic polypeptide, an anorexigenic hormone, were increased and the more they slept, the less they consumed calories at an ad libitum buffet. This work highlights the importance of getting enough sleep to maintain a good metabolic health and suggest that sleep optimization may have implications for novel public health interventions

Obésité

Diabète

Sommeil

Axe Hypothalamo-Hypophyso-Surrénalien

Obesity

Diabetes

Sleep

Hypothalamic-Pituitary-Adrenal axis

612.8

Examining Multiple Sleep Behaviors and Diurnal Patterns of Salivary Cortisol and Alpha-Amylase: Within- and Between-Person Associations

January 2015

abstract: Sleep is essential for physical and psychological health. Sleep has also been linked to the daily patterns of key stress-responsive physiological systems, specifically the hypothalamic-pituitary-adrenal (HPA) axis and autonomic nervous system (ANS). Extant research examining sleep and diurnal patterns of cortisol, the primary end product of the HPA axis, is inconsistent. Moreover, it is not clear how specific aspects of sleep behavior (e.g., sleep duration, sleep quality, sleep variability) are related to specific components of diurnal cortisol rhythms. Salivary alpha-amylase (sAA) has been recognized as a surrogate marker of ANS activity, but limited research has explored relations between sleep and sAA diurnal rhythms. The current study utilized a modified ecological momentary assessment protocol to examine within- and between-person relations between multiple facets of sleep behavior using multiple methods (e.g., subjective report, actigraphy) and salivary cortisol and sAA. First year college students (N = 76) provided saliva samples and diary entries five times per day over the course of three days. Sleep was assessed via questionnaire, through daily diaries, and monitored objectively using actigraphy over a four day period. Between-person results revealed that shorter average sleep duration and greater sleep variability was related to lower levels of waking cortisol and flatter diurnal slopes across the day. Within-person results revealed that on nights when individuals slept for shorter durations than usual they also had lower levels of waking cortisol the next day. Sleep was not related to the cortisol awakening response (CAR) or diurnal patterns of sAA, in either between-person or within-person analyses. However, typical sleep behaviors measured via questionnaire were related to waking levels of sAA. Overall, this study provides a greater understanding of how multiple components of sleep, measured in naturalistic environments, is related to cortisol and sAA diurnal rhythms, and how day-to-day, within-person changes in sleep duration contribute to daily variations in cortisol. / Dissertation/Thesis / Masters Thesis Psychology 2015

Psychology

Psychobiology

actigraphy

cortisol

hypothalamic-pituitary-adrenal axis

salivary alpha-amylase

sleep

Role of 5α-reductase type 1 in modifying anxiety, appetite and the HPA axis

Di Rollo, Emma Margaret

January 2014

Glucocorticoid excess is associated with adverse effects on a number of physiological parameters, leading to obesity, dysfunction of the hypothalamic-pituitary- adrenal (HPA) axis and behavioural changes such as anxiety and impaired learning and memory. Circulating and local tissue glucocorticoid levels are tightly controlled by the HPA axis but an additional level of control exists in tissues such as brain, liver and adipose tissue. In these structures, enzymes including 5α-reductase 1 (5αR1), catalyse the conversion of corticosterone to A-ring reduced metabolites, which have a different spectrum of activities. This thesis investigates the role of 5αR1 in regulating central glucocorticoid actions which control HPA axis function and behaviour in a mouse model with genetic disruption of 5αR1 (5αR1-KO). Preliminary data showed 5αR1-KO mice were susceptible to developing insulin resistance and obesity and had reduced HPA axis responses to acute stress. Additionally, male 5αR1-KO mice were more prone to obesity than wild-type (WT) when fed a high-fat diet whilst female 5αR1-KO mice gained more weight than WT even on a normal chow diet. Intriguingly, female 5αR1-KO mice subjected to social isolation stress lost this extra weight and became comparable to WT controls. This study tested the hypothesis that 5αR1-KO mice are less able to inactivate glucocorticoids in the periphery and within tissues, resulting in a predisposition to metabolic disturbances and behavioural alterations. These were hypothesised to include hyperphagia, weight gain, impaired stress responses, anxiety (exacerbated by environmental stress) and cognitive deficits. It was also thought that many of these features would be more pronounced in female vs. male mice. The main aims of this study were to determine if 5αR1-KO induced weight gain and if this was correlated to altered gene expression of key hypothalamic neuropeptides which regulate appetite, to determine the central mechanisms which underpin attenuated HPA axis responses to acute stress and to determine whether behaviours such as anxiety and learning and memory ability are affected by global 5αR1 loss. It was hypothesised that female 5αR1-KO mice have increased appetite and reduced locomotor activity compared with WT and male 5αR1-KOs. However, male 5αR1- KO mice (on a mixed genetic background, C57Bl/6j/SvEv/129) were hyperphagic on a normal chow diet but did not gain extra weight, while female 5αR1-KO mice gained more weight vs. WT despite hypophagia. Free ambulatory activity was unaffected by genotype in either sex. Male 5αR1-KO mice appeared less anxious but responses of female 5αR1-KO mice in tests of anxiety did not differ from WT controls. Mice lacking 5αR1 generally had a poorer metabolic profile with impaired glucose tolerance and hyperinsulinaemia; with hepatic steatosis evident in female mice. There was evidence of compensatory changes in hypothalamic orexigenic and anorexigenic peptides. Phenotypes were sexually dimorphic such that male mice had a poorer metabolic profile vs. females, which was particularly marked in male 5αR1- KO animals. 5αR1-KO mice were previously shown to have attenuated HPA axis responses to acute stress and it was hypothesised that disruption of 5αR1 would result in altered expression of genes related HPA axis regulation with a view to increased negative feedback. Here, male and female 5αR1-KO mice demonstrated altered corticosteroid receptor expression within the hippocampus and the pituitary, two key structures in the HPA cascade. In situ hybridisation showed reduced mRNA for MR in the hippocampus and for Crh in the hypothalamus of 5αR1-KO mice. These modifications along with decreased Crhr-1 mRNA (CRH‘s main receptor) may be due to a lack of corticosterone metabolism within the brain resulting in enhanced negative feedback and reduced HPA axial drive. In order to study behaviour in detail and also to test whether potential central glucocorticoid excess may predispose to cognitive decline with ageing, a separate cohort of female 5αR1-KO backcrossed onto a uniform C57Bl/6j background was studied both when young (6 months) and when aged (14-15 months). Additionally, mice were housed in either groups or singly (social isolation) to investigate the potentially additive effects of environmental stress. It was hypothesised that local glucocorticoid increases in the brains of 5αR1-KO mice would be associated with anxiety and cognitive deficiencies and that these phenotypes would be exaggerated by the stress of social isolation as well as ageing. Behavioural differences were not observed at 6 months of age. However aged, 5αR1-KO mice housed singly showed increased anxiety and had higher plasma corticosterone levels than group-housed mice. Moreover, aged mice lacking 5αR1 performed less well than WT in tests of memory and had a marginally greater cognitive decline when learning ability at 14- 15 months old was compared to that of the same animals tested at 6 months old. Overall, mice with global 5αR1 loss appeared susceptible to anxiety as well as some degree of age-associated cognitive impairment, but only when subjected to social isolation stress which is a known chronic stressor. The final set of experiments aimed to determine the effect of mouse strain on 5αR1- KO phenotypes. It was hypothesised that glucocorticoid clearance would be attenuated to a lesser degree in 5αR1-KO mice bred onto a congenic C57Bl/6j strain compared to those of the mixed strain and that this would manifest as less disruption of metabolism and less suppression of HPA axis stress responses. Although social isolation again induced weight-loss in female mice and more so in 5αR1-KO animals, mice on the C57Bl/6j background strain did not show dampened HPA axis responses to acute stress as seen previously. It was subsequently shown in adrenalectomised mice that animals bred on the C57Bl/6j strain cleared active corticosterone from plasma and liver faster than mixed strain mice. This may have rendered mixed strain 5αR1-KO mice more susceptible to excessive corticosterone levels producing a more exaggerated phenotype in this group. In conclusion, these data suggest a role for the enzyme 5αR1 in modifying glucocorticoid concentrations in the brain and liver, influencing not only metabolic and peripheral effects such as weight gain and insulin resistance, but also in modifying cognition, appetite stimulation and affective behaviours. It has been highlighted that outside factors such as housing and age can modify these phenotypes and are important considerations for future studies. This study has also highlighted the importance of choosing an appropriate genetic background for genetically modified animals since phenotypes can be enhanced or attenuated depending on strain. Finally, 5αR inhibitors are used to treat disorders such as benign prostatic hyperplasia in men, and it is important to consider that these drugs may have a wide array of associated side effects both systemically and in the central nervous system.

612.8