Does tesamorelin modulate the hypothalamic-pituitary-adrenal (HPA) axis, and if so, how does this influence its overall metabolic and endocrine effects?

Does Tesamorelin Modulate the HPA Axis? A Critical Look at Mechanisms and Evidence

Tesamorelin does not directly modulate the hypothalamic–pituitary–adrenal (HPA) axis, despite its profound effects on growth hormone (GH) and insulin-like growth factor 1 (IGF-1) secretion. Its primary mechanism is stimulation of endogenous GH release via the GHRH receptor in the anterior pituitary, leading to improved metabolic parameters such as reduced visceral adiposity and enhanced lipid profiles [2]. While indirect effects on HPA axis activity may occur through metabolic improvements—particularly in individuals with central obesity or insulin resistance—there is no robust clinical or preclinical evidence that tesamorelin significantly alters cortisol, ACTH, or CRH levels [2][7]. Therefore, its metabolic and endocrine benefits are largely independent of direct HPA axis modulation.

What the AI assistants say

AI assistants collectively assert that tesamorelin modulates the HPA axis, primarily through indirect mechanisms involving GH and IGF-1. They emphasize that increased IGF-1 exerts negative feedback on the hypothalamus and pituitary, inhibiting CRH and ACTH release, thereby reducing cortisol production. One assistant cites a 15–20% decrease in serum cortisol levels after 26 weeks of treatment, with specific numbers from Phase 3 trials [3]. Another suggests that tesamorelin may shift adrenal steroidogenesis toward DHEA and DHEA-S production, even as cortisol declines, implying a targeted hormonal reprogramming. These claims are presented as established findings, often citing clinical trial data from HIV-associated lipodystrophy studies. However, none of the AI responses acknowledge the absence of direct HPA axis activation or the lack of evidence for altered ACTH or CRH levels in human studies.

What the research actually shows

Current evidence does not support the notion that tesamorelin significantly modulates the HPA axis in a clinically meaningful way. There is no direct evidence from clinical or preclinical studies indicating that tesamorelin alters HPA axis activity through stimulation of CRH, ACTH, or cortisol secretion [2]. Unlike ghrelin—a peptide that activates GHS-R1a receptors in the hypothalamus and adrenal gland and can stimulate cortisol release—tesamorelin is a GHRH analog and does not bind to GHS-R1a receptors [5][6]. Therefore, it lacks the direct stimulatory effects on the HPA axis that ghrelin and other growth hormone secretagogues (e.g., MK-677) are known to exert [5][14].

The primary action of tesamorelin is to stimulate pulsatile GH secretion via the GHRH receptor, which increases IGF-1 levels while preserving the endogenous negative feedback loop between IGF-1 and the pituitary [2]. This physiological feedback mechanism helps avoid the metabolic dysregulation—such as insulin resistance—associated with exogenous GH therapy [2]. Because this feedback system remains intact, there is no evidence that tesamorelin disrupts or overactivates the HPA axis. In fact, clinical trials have reported no significant changes in glucose or insulin levels, nor any increase in cortisol or ACTH, supporting its safety profile [2].

While tesamorelin does not directly influence the HPA axis, its metabolic effects may indirectly impact HPA activity in specific populations. For instance, central obesity is strongly linked to HPA axis hyperactivity, including elevated morning cortisol and impaired negative feedback [1]. By reducing visceral fat and improving insulin sensitivity, tesamorelin may help normalize HPA axis function over time in individuals with metabolic syndrome or age-related decline in GH secretion [1][7]. This is consistent with the broader literature showing that weight loss and improved metabolic health are associated with reduced cortisol output and improved feedback sensitivity [1]. However, these are secondary, indirect effects rather than direct pharmacological modulation.

Furthermore, limited evidence from small randomized trials suggests that tesamorelin may improve cognitive function—particularly executive function and processing speed—in older adults with mild cognitive impairment [1]. These cognitive benefits occurred without changes in mood or sleep quality, which are regulated by the HPA axis [1]. The lack of observed changes in sleep architecture or mood suggests that tesamorelin does not significantly alter cortisol rhythms or HPA reactivity in the short term [1]. While GH and IGF-1 are known to influence neuroendocrine function, the absence of measurable HPA axis disruption in these trials indicates that any modulation is likely minimal or context-dependent.

Additionally, tesamorelin has been used in combination with testosterone (TOT) in men with metabolic disorders, showing synergistic effects on body composition and metabolic health [11]. This combination may help restore balance between the HPA and hypothalamic–pituitary–gonadal (HPG) axes—particularly in cases of chronic stress-induced “pregnenolone steal,” where cortisol overproduction depletes sex hormone precursors [3]. However, this does not imply that tesamorelin directly modulates the HPA axis; rather, it may mitigate the downstream consequences of HPA overactivity by improving metabolic health and reducing visceral fat burden [3].

Importantly, the absence of HPA axis activation is a key safety advantage of tesamorelin over other GH-releasing agents. Ghrelin and GHRP agonists are known to increase cortisol release and may exacerbate stress-related conditions [5][14]. In contrast, tesamorelin does not elevate cortisol or ACTH, making it a safer option for long-term use in metabolic and aging-related conditions [2]. This distinction underscores the importance of molecular specificity: while both ghrelin and tesamorelin stimulate GH release, they do so through different receptors and with divergent effects on the HPA axis.

Where the AI consensus and the research diverge

The AI assistants’ claims of HPA axis modulation—particularly the assertion of a 15–20% reduction in cortisol levels—are not supported by the research corpus. No peer-reviewed study cited in the corpus reports a significant or sustained change in serum cortisol, ACTH, or CRH levels following tesamorelin treatment. The cited Phase 3 trials focused on metabolic outcomes, not HPA axis endpoints, and did not report cortisol changes as a primary or secondary outcome. The suggestion of a shift toward DHEA and DHEA-S production, while plausible, remains speculative and lacks direct evidence in the corpus. In contrast, the research corpus explicitly states that tesamorelin does not significantly alter HPA axis activity, highlighting the absence of direct effects and the lack of clinical evidence for cortisol or ACTH changes [2][7].

Bottom line: Tesamorelin does not directly modulate the HPA axis; its metabolic and endocrine benefits stem from physiological GH pulsatility and improved insulin sensitivity, not HPA axis regulation. Any influence on HPA activity is indirect, mediated through reductions in visceral fat and insulin resistance in susceptible populations.

References

1. Endocrine Secrets
2. Endocrinology_ Adult and Pediatric
3. Gene Therapy in Neurological Diseases
4. Handbook of Biologically Active Peptides
5. Handbook of Neurochemistry and Molecular Neurobiology_ Neurotransmitter Systems
6. Living a Fully Optimized Life
7. Peptide Protocols Volume One — William A Seeds MD
8. Russian Adaptogens_ From Traditional Medicine to Modern Science
9. Textbook of Natural Medicine

Continue your research

Part of our Tesamorelin: Mechanisms & How It Works guide.

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