The hypothalamic-pituitary-adrenal (HPA) axis, the central neuroendocrine system governing the body's stress response, demonstrates significant dysfunction in progressive supranuclear palsy (PSP). This dysregulation contributes to disease progression through multiple pathways, including glucocorticoid-mediated neurotoxicity, circadian rhythm disruption, and autonomic stress integration failures. The HPA axis interacts extensively with the 4R-tau pathology characteristic of PSP, creating a bidirectional relationship where stress exacerbates neurodegeneration and neurodegeneration disrupts stress response systems.
PSP patients demonstrate characteristic patterns of HPA axis dysregulation that distinguish them from other neurodegenerative disorders. Understanding these alterations provides insight into disease mechanisms and identifies potential therapeutic targets for stress modulation approaches[hartmann1997].
The HPA axis functions as the body's central stress response system. The hypothalamus releases corticotropin-releasing hormone (CRH) in response to stress, stimulating the anterior pituitary to secrete adrenocorticotropic hormone (ACTH), which then triggers cortisol release from the adrenal cortex. This cascade operates through negative feedback loops involving the hippocampus and prefrontal cortex, which normally inhibit excessive glucocorticoid exposure. The system follows a robust circadian rhythm, with cortisol levels highest upon waking and lowest around midnight.
In PSP, this delicate regulatory system undergoes significant disruption at multiple levels. The tau pathology characteristic of PSP affects key brain regions that normally regulate HPA axis function, including the hypothalamus itself, the hippocampus, and the prefrontal cortex. This creates a cascading dysregulation where normal feedback mechanisms fail, leading to both elevated baseline cortisol and exaggerated stress responses[roohi2021].
PSP pathology affects several critical nodes in the HPA axis regulatory network. The hypothalamus, directly involved in CRH production and release, shows tau pathology in PSP patients. The hippocampus, essential for glucocorticoid negative feedback, demonstrates significant neuronal loss and tau burden. The prefrontal cortex, which modulates stress responses through top-down control, shows the characteristic frontal lobe syndrome of PSP. These combined lesions create a HPA axis that both overresponds to stress and fails to properly terminate the stress response[lucin2009].
The brainstem nuclei affected in PSP, including the locus coeruleus and raphe nuclei, also modulate HPA axis activity. These nuclei, which undergo significant degeneration in PSP, normally provide inhibitory and excitatory inputs to the hypothalamus that fine-tune the stress response. Their dysfunction removes important regulatory constraints on HPA axis activity, contributing to the dysregulated cortisol patterns observed in PSP patients.
Multiple studies have documented elevated baseline cortisol levels in PSP patients compared to age-matched controls. This hypercortisolemia appears specific to PSP among atypical parkinsonisms, distinguishing it from Parkinson's disease where cortisol patterns more closely resemble controls. The elevated baseline cortisol correlates with disease severity and duration, suggesting that HPA axis dysregulation worsens as PSP progresses[hartmann1997].
The source of elevated baseline cortisol likely involves multiple mechanisms. Hypothalamic CRH production appears increased in PSP, possibly due to loss of inhibitory inputs from affected brain regions. Pituitary sensitivity to CRH may be enhanced, leading to amplified ACTH responses. Adrenal function may also be altered, with enhanced cortisol production capacity even at baseline. The combination of central and peripheral changes creates a persistent hypercortisolemic state that accelerates neurodegeneration[sapolsky1985].
PSP patients demonstrate exaggerated cortisol responses to stressors, both physiological and psychological. The cortisol surge following standard stress challenges significantly exceeds that seen in healthy controls or patients with other neurodegenerative disorders. This hyperreactivity may relate to impaired negative feedback, as the hippocampus and prefrontal cortex that normally terminate the stress response are particularly vulnerable in PSP[cholerton2013].
The clinical implications of this hyperreactivity are substantial. Each stress-induced cortisol surge contributes to ongoing neurodegeneration through glucocorticoid-mediated mechanisms. Patients may experience worsening symptoms following relatively minor stressors, creating a negative cycle where stress triggers symptom exacerbation, which itself becomes a stressor. This cycle may accelerate disease progression and contribute to the characteristic rapid decline seen in PSP.
Glucocorticoids directly promote tau pathology through multiple mechanisms. Cortisol enhances tau phosphorylation at multiple sites, including those characteristic of PSP pathology. This phosphorylation reduces tau's ability to bind microtubules, leading to microtubule instability and impaired axonal transport. Glucocorticoid exposure also promotes tau aggregation, accelerating the formation of insoluble tau filaments that characterize PSP[chen2019].
The glucocorticoid-tau interaction creates a vicious cycle in PSP. Tau pathology itself disrupts HPA axis regulation, leading to elevated cortisol. Elevated cortisol then promotes additional tau pathology, accelerating neurodegeneration. This positive feedback loop may explain the rapid progression characteristic of PSP compared to other tauopathies where this interaction may be less pronounced.
Glucocorticoids enhance neuronal vulnerability through several complementary mechanisms. They reduce neuronal energy production by impairing mitochondrial function, making neurons more susceptible to metabolic stressors. Glucocorticoids also promote oxidative stress, generating reactive oxygen species that damage cellular components. Additionally, they impair autophagy and proteostasis, reducing the cell's ability to clear pathological proteins including 4R-tau aggregates[weir2020].
The hippocampus shows particular sensitivity to glucocorticoid-mediated neurotoxicity. Chronic glucocorticoid exposure leads to hippocampal neuron loss, which further impairs HPA axis negative feedback. This creates an accelerating cycle where initial hippocampal damage leads to glucocorticoid excess, which causes additional hippocampal damage. In PSP, this cycle likely contributes to the prominent memory and cognitive impairment seen in later disease stages.
The autonomic nervous system, intimately connected to HPA axis function, shows extensive dysfunction in PSP. Normal stress responses involve coordinated HPA axis and autonomic activation, with sympathetic activation accompanying cortisol release. In PSP, this coordination breaks down, leading to inappropriate autonomic responses to stress. Patients may experience paradoxical drops in blood pressure during stress, or excessive sympathetic activation with minimal provocation[sandusky2022].
The brainstem nuclei that coordinate autonomic responses, including the dorsal motor nucleus of the vagus and the nucleus of the solitary tract, undergo significant degeneration in PSP. These nuclei normally integrate HPA axis signals with autonomic outflow, creating appropriate physiological responses to stress. Their dysfunction leads to the autonomic instability characteristic of PSP, including orthostatic hypotension, urinary dysfunction, and thermoregulatory abnormalities.
The baroreceptor reflex, critical for blood pressure regulation during stress and posture changes, shows significant impairment in PSP. This dysfunction contributes to orthostatic hypotension, a common and disabling feature of PSP. The baroreflex normally provides rapid hemodynamic adjustments during stress, but this capacity is compromised by PSP-related brainstem pathology. Patients may experience dangerous blood pressure swings in response to even minor stressors, increasing fall risk and cardiovascular complications.
The normal cortisol circadian rhythm, with morning peak and nighttime nadir, shows significant disruption in PSP. Patients demonstrate flattened diurnal cortisol variation, with reduced morning peaks and insufficient nighttime suppression. This disruption likely reflects both hypothalamic pathology and the broader sleep-wake cycle abnormalities common in PSP. The flattened rhythm correlates with sleep disturbances, cognitive impairment, and overall disease severity.
The loss of robust cortisol rhythmicity has important implications for circadian function. Cortisol normally helps coordinate cellular metabolism and activity patterns throughout the body. When this coordination is disrupted, downstream systems including immune function, metabolic regulation, and neurotransmitter production may all be impaired. This global dysregulation may contribute to the multi-system involvement characteristic of PSP.
Sleep disturbances in PSP, including insomnia, sleep fragmentation, and rapid eye movement sleep behavior disorder, interact bidirectionally with HPA axis dysfunction. Poor sleep elevates baseline cortisol, while elevated cortisol disrupts sleep architecture. This creates a vicious cycle where sleep problems worsen HPA axis dysregulation, which in turn further impairs sleep. The resulting sleep fragmentation likely contributes to the excessive daytime sleepiness and cognitive impairment seen in PSP patients.
HPA axis dysfunction significantly contributes to cognitive impairment in PSP. Glucocorticoid-mediated hippocampal toxicity worsens memory dysfunction, while prefrontal cortex effects compound executive dysfunction. The characteristic "subcortical" cognitive profile of PSP, with prominent attention, planning, and working memory deficits, relates in part to glucocorticoid effects on prefrontal cortical function. Patients with evidence of greater HPA axis dysfunction show more severe cognitive impairment.
The HPA axis connects closely with mood regulation systems. Glucocorticoid elevations contribute to depression, anxiety, and emotional lability in PSP. The high prevalence of depression in PSP, estimated at 40-60%, likely relates in part to chronic glucocorticoid exposure. Anxiety and irritability may also reflect HPA axis overactivity. These neuropsychiatric symptoms significantly impact quality of life and may be amenable to stress-reduction and HPA axis-modulating interventions.
HPA axis dysfunction may accelerate disease progression through multiple mechanisms. Chronic glucocorticoid exposure promotes tau pathology, enhances neuronal vulnerability, and disrupts cellular homeostasis. The resulting neurodegeneration further impairs HPA axis regulation, creating a self-amplifying cycle of deterioration. Patients with greater HPA axis dysregulation may experience more rapid disease progression, suggesting this pathway as a potential therapeutic target.
Metyrapone inhibits 11β-hydroxylase, the enzyme that catalyzes the final step of cortisol synthesis in the adrenal cortex. This direct cortisol synthesis inhibition has been explored in Cushing's disease and shows potential for conditions with endogenous hypercortisolemia. In PSP, metyrapone could theoretically reduce glucocorticoid-mediated tau phosphorylation and neuronal vulnerability. However, no published trials have evaluated metyrapone specifically in PSP. Practical concerns include the risk of adrenal insufficiency, requires careful ACTH and cortisol monitoring, and potential for mineralocorticoid deficiency that may worsen orthostatic hypotension.
Ketoconazole, an azole antifungal, also inhibits 11β-hydroxylase and has been used off-label for cortisol suppression. Beyond cortisol synthesis inhibition, ketoconazole has additional properties including inhibition of testosterone synthesis, which may be relevant given that testosterone may interact with tau pathology. The drug requires liver function monitoring and has multiple drug interactions. Like metyrapone, specific PSP trials are lacking.
Mifepristone is a glucocorticoid receptor antagonist that blocks the effects of cortisol at the receptor level. This approach preserves cortisol synthesis but prevents downstream glucocorticoid-mediated effects including tau phosphorylation and neuronal toxicity. Mifepristone has been explored in Cushing's syndrome and in Alzheimer's disease cognitive outcomes. The principal concern is potential for adrenal crisis if cortisol levels remain elevated while receptors are blocked. In PSP, this dual-action approach (reducing synthesis with antagonist effect) may be theoretically beneficial but remains untested.
Fludrocortisone is a synthetic mineralocorticoid that acts on mineralocorticoid receptors in the kidney to enhance sodium retention and increase blood volume. In PSP, fludrocortisone may help address orthostatic hypotension through volume expansion rather than direct vasoconstriction. However, mineralocorticoid receptor activation also affects stress response regulation through extra-renal tissues. The drug requires monitoring for hypertension, hypokalemia, and fluid overload. Fludrocortisone has been used in Parkinson's disease for autonomic dysfunction with mixed results.
Selective glucocorticoid receptor modulators (SGRMs) represent an emerging class that can have tissue-specific agonist or antagonist effects. These compounds may preserve beneficial glucocorticoid effects while blocking harmful ones. In theory, SGRMs could allow necessary glucocorticoid function (anti-inflammatory, metabolic) while blocking hippocampal toxicity and tau phosphorylation effects. Compound development remains early-stage.
Mindfulness-based stress reduction (MBSR) programs have shown cortisol-lowering effects in multiple populations. An 8-week MBSR protocol significantly reduces morning cortisol and improves stress coping. While not PSP-specific, these interventions are low-risk and may provide symptom benefits beyond cortisol reduction including improved mood and reduced anxiety.
Progressive muscle relaxation, guided imagery, and breathing exercises may reduce acute cortisol responses to stressors. Caregiver education to minimize unnecessary stressors and optimize daily routines may help maintain lower cortisol states. Environmental modifications to reduce fall risk and sudden surprises can help prevent stress-induced cortisol spikes.
Sleep disturbances in PSP elevate baseline cortisol, while elevated cortisol disrupts sleep. Optimizing sleep hygiene may help restore more normal cortisol rhythms. Strategies include consistent sleep scheduling, limited caffeine, reduced evening light exposure, and treatment of REM sleep behavior disorder if present.
Regular moderate exercise helps regulate HPA axis function and improves stress tolerance. However, excessive or intense exercise may elevate cortisol, particularly in poorly conditioned individuals. TheOptimal exercise in PSP involves consistent, moderate aerobic activity within functional abilities, such as supervised treadmill training or cycling.
Dietary factors that stabilize glucose and cortisol include adequate protein and complex carbohydrates. Extended periods without food may trigger cortisol release. Nutritional timing (smaller, more frequent meals) may help maintain metabolic stability.
Clinical trials targeting HPA axis dysfunction in PSP face several challenges: lack of validated PSP-specific cortisol biomarkers, heterogeneity in HPA axis abnormalities across patients, difficulty separating primary from secondary HPA axis effects, and the complexity of the HPA axis negative feedback system. Patient selection based on demonstrated HPA axis dysregulation (elevated morning cortisol, failed dexamethasone suppression) may improve signal detection.
Potential outcome measures for HPA axis-targeted trials include:
In PSP, cortisol abnormalities correlate with specific biomarkers:
The correlations between cortisol and tau pathology support the biological rationale for targeting HPA axis dysfunction in PSP. Patients with greater HPA axis disturbance may represent a subgroup that benefits most from cortisol-modifying interventions.
HPA axis measures may serve as biomarkers in PSP. Morning cortisol levels, cortisol awakening response, and dexamethasone suppression test results all show abnormal patterns in PSP and may correlate with disease severity or progression. These measures are relatively non-invasive and could potentially be used for patient stratification or treatment monitoring. However, standardization across studies remains challenging.
Understanding HPA axis dysfunction in PSP identifies potential therapeutic targets. CRH receptor antagonists might dampen excessive stress responses. Glucocorticoid receptor modulators could potentially preserve necessary glucocorticoid function while blocking harmful effects. Downstream interventions targeting glucocorticoid-mediated tau phosphorylation or neuronal vulnerability represent additional therapeutic possibilities. Successful development of these approaches would require careful attention to the complex physiology of the HPA axis system.