Desensitization of gonadotropin responses to kisspeptin in the female rat: analyses of LH and FSH secretion at different developmental and metabolic states.
Roa. J J; Vigo. E E; García-Galiano. D D; Castellano. J M JM; Navarro. V M VM; Pineda. R R; Diéguez. C C; Aguilar. E E; Pinilla. L L; Tena-Sempere. M M
Key Findings
- Continuous kisspeptin-10 causes a brief LH surge followed by rapid decline in adult female rats
- FSH stays elevated during ongoing kisspeptin infusion, but under‑nutrition shortens this response
- Undernutrition prolongs LH elevation and mimics leptin’s effect, while leptin does not replicate the FSH pattern
- In pubertal females, both LH and FSH stay high for a week of infusion, especially with subnutrition
- Gonadotropin‑releasing hormone response remains intact, indicating desensitization occurs upstream of the pituitary
Practical Outcomes
- For biohackers, this suggests that continuous kisspeptin dosing may quickly lose its LH‑boosting effect and could lead to hormone desensitization, especially if nutritional status is altered. Intermittent or pulsed dosing might be needed to maintain efficacy, and any protocol should consider the user’s energy balance or leptin levels. However, because the study is in rats with brain infusion, direct translation to human oral or injectable use is uncertain and requires caution.
Summary
In female rats, giving kisspeptin-10 continuously into the brain first spikes the hormone LH, but then it quickly falls back to normal, while another hormone, FSH, stays high for longer. How much the rats were fed changes these effects – under‑feeding keeps LH high longer and shortens the FSH rise. The pituitary gland still works fine, so the drop‑off happens before that point. These results show that constant kisspeptin isn’t a simple way to boost reproductive hormones and that nutrition matters.
Abstract
Kisspeptins have emerged as potent elicitors of gonadotropin secretion and, therefore, putative targets for pharmacological intervention. In this context, desensitization of gonadotropin responses to continuous administration of kisspeptins has begun to be characterized, but information so far available is mostly restricted to LH responses in males, whereas the similar phenomenon in females, of obvious therapeutic interest, remains virtually unexplored. We report herein LH and FSH responses to continuous intracerebral administration of kisspeptin in female rats at different developmental and metabolic states. Infusion of kisspeptin-10 to adult female rats induced a transient elevation in serum LH concentrations, followed by a precipitous drop and normalization of LH levels thereafter. Elevation of LH after kisspeptin infusion was prolonged in underfed animals; a phenomenon mimicked by leptin administration. Conversely, FSH levels were persistently heightened along continuous kisspeptin infusion, but duration of this response was shortened by undernutrition. In pubertal females, LH and FSH levels remained elevated at the end of a 7-day infusion of kisspeptin; responses whose magnitude was augmented by subnutrition but not mimicked by leptin. In all settings, terminal gonadotropin-releasing hormone responses were fully preserved, suggesting that eventual desensitization must occur upstream from the pituitary. In summary, our current data document the pharmacological consequences of continuous administration of kisspeptin to female rats, with remarkable differences being detected between LH and FSH responses, in different developmental and metabolic states. These observations of potential pharmacological interest might help also to delineate the physiological roles of kisspeptins in the dynamic regulation of gonadotropin secretion in the female.
Study Information
pubmed
2008
2008-04-15T00:00:00.000Z
10.1152/ajpendo.90240.2008
102
49