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Kisspeptin-10

KP-10, Metastin (45-54), Kisspeptin-10 (human), KiSS-1

Quick Stats
Studies 877
Trials 47
Score 2
2018 pubmed 99 citations

Central precocious puberty: From genetics to treatment.

Aguirre. Rebecca Schneider RS; Eugster. Erica A EA

Key Findings

  • Kisspeptin signaling is essential for starting puberty and mutations can lead to early activation (CPP).
  • Genetic variants in kisspeptin, MKRN3, and DLK1 are linked to both sporadic and familial cases of CPP.
  • GnRH analogs remain the standard treatment, with newer extended‑release formulations under development and no known long‑term side effects so far.

Practical Outcomes

  • For biohackers, the main takeaway is that kisspeptin is a powerful trigger of the reproductive hormone cascade, but manipulating it in healthy adults for performance or longevity is not supported by this study. The research reinforces that current CPP treatments are safe and effective, but it does not provide new dosing strategies or protocols relevant to adult health optimization.

Summary

The paper explains that early puberty (central precocious puberty) happens when the brain's hormone system turns on too soon, and that the kisspeptin pathway is a key driver of this process. Mutations in kisspeptin and related genes can cause this condition. Treatment usually involves GnRH analog drugs to pause puberty and protect height, and newer long‑acting versions are being developed.

Abstract

Central precocious puberty (CPP) results from early activation of the hypothalamic - pituitary -gonadal (HPG) axis and follows the same sequence as normal puberty. While many factors involved in pubertal initiation remain poorly understood, the kisspeptin system is known to play a key role. Currently, mutations in the kisspeptin system, MKRN3, and DLK1 have been identified in sporadic and familial cases of CPP. The diagnosis is based on physical exam findings indicating advancing puberty and on laboratory tests confirming central HPG axis activation. GnRH analogs are the mainstay of treatment and are used with the goal of height preservation. Newer extended release formulations continue to be developed. Currently there is no evidence of long-term complications associated with treatment. However, many areas remain to be explored such as targeted therapies and aspects of clinical management. Further investigation into psychological effects and additional data regarding long-term outcomes, particularly in males, is needed.

Study Information

Provider

pubmed

Year

2018

Date

2018-05-26T00:00:00.000Z

DOI

10.1016/j.beem.2018.05.008

Citations

99

References

69