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Kisspeptin-10

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

Quick Stats
Studies 877
Trials 47
Score 2
2016 pubmed

Dynamic Regulation of Hypothalamic DMXL2, KISS1, and RFRP Expression During Postnatal Development in Non-Human Primates.

Wahab. Fazal F; Drummer. Charis C; Schlatt. Stefan S; Behr. Rüdiger R

Key Findings

  • Kiss1 (kisspeptin) mRNA levels rise from newborn to infant and again from juvenile to pubertal and adult stages.
  • DMXL2 expression mirrors the kisspeptin pattern, increasing in infantile and post‑pubertal periods.
  • RFRP (GnIH) transcript levels peak during the prepubertal (juvenile) stage.

Practical Outcomes

  • For biohackers, the data suggest kisspeptin naturally spikes around puberty, hinting that timing could matter if you ever consider kisspeptin supplementation for hormone modulation. However, the study provides no dosage, safety, or efficacy info for humans, so it’s not a ready‑to‑use protocol. More human‑focused research is needed before applying these findings to longevity or performance strategies.

Summary

The study looked at how the brain chemicals kisspeptin, DMXL2, and a hormone‑blocking factor (RFRP) change as baby marmoset monkeys grow up. It found that kisspeptin and DMXL2 levels are low at birth, rise during early childhood, dip before puberty, then go up again at puberty and adulthood. The hormone‑blocking factor spikes just before puberty. This tells us that kisspeptin naturally increases when the reproductive system is maturing, but the research was done in monkeys and didn’t test any treatments in people.

Abstract

The neurobiological mechanism of puberty onset in primates is currently only partly understood. A recent study reported an important role of Dmx-like 2 (DMXL2), a gene encoding rabconnectin-3α vesicular protein, in human subjects with mental retardation and neuroendocrine impairment of reproduction. To further characterize the potential role of DMXL2 in the regulation of reproduction, we analyzed the expression of DMXL2 in hypothalami of newborn, infantile, juvenile, pubertal, and postpubertal female and male common marmoset monkeys. Additionally, as the relative hypothalamic levels of gonadotropin-inhibitory hormone (GnIH) transcript during postnatal development are unknown in primates, we also quantified messenger RNA (mRNA) levels of RFRP, a gene encoding GnIH. Moreover, the transcript levels of kisspeptin, a well-known regulator of the hypothalamic neurohormonal axis controlling reproduction, were also checked. Transcript and protein levels of DMXL2 and Kiss1 transcript levels increase from the newborn to the infantile and from the juvenile (prepubertal) to the pubertal and the postpubertal period. We also noted a clear upsurge in RFRP transcript levels in the prepubertal period. In conclusion, the hypothalamic expressions of Kiss1 and DMXL2 mRNA increase during infantile, pubertal, and adult stages compared to newborn and juvenile stages in common marmoset monkeys. In contrast, the expression of RFRP mRNA upsurges in juvenile monkeys. Further mechanistic studies are needed to characterize the potential inhibitory role of the GnIH-GPR147 signaling in the prepubertal period and the role of DMXL2 in the molecular cascade regulating the neuroendocrine reproductive axis in primates.

Study Information

Provider

pubmed

Year

2016

Date

2016-12-12T00:00:00.000Z

DOI

10.1007/s12035-016-0329-x