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Humanin

HN, S14G-Humanin

Quick Stats
Studies 491
Trials 100
Score 1
2011 pubmed 73 citations

Self-assembled polymersomes conjugated with lactoferrin as novel drug carrier for brain delivery.

Yu. Yuan Y; Pang. Zhiqing Z; Lu. Wei W; Yin. Qi Q; Gao. Huile H; Jiang. Xinguo X

Key Findings

  • About 101 lactoferrin molecules per polymersome gave the highest brain uptake in mice.
  • S14G‑humanin packaged in these carriers reduced cell‑death markers (Bax, caspase‑3) in rat hippocampus after amyloid exposure.
  • Choline acetyltransferase activity increased, suggesting better neuronal function.

Practical Outcomes

  • The study shows a promising way to get humanin into the brain, but the technology is still experimental and not ready for DIY use. It may guide future brain‑targeted supplement designs, but for now there’s no actionable protocol for biohackers.

Summary

Scientists made tiny carriers that can cross the brain’s protective barrier and deliver a neuro‑protective version of the humanin peptide. In mice they found the best amount of a targeting protein (lactoferrin) on the carrier, and in rats the peptide helped protect brain cells from damage caused by an Alzheimer‑related protein. However, making these carriers requires advanced lab work and IV injection, so it isn’t something you can try at home right now.

Abstract

To develop a novel brain drug delivery system based on self-assembled poly(ethyleneglycol)-poly (D,L-lactic-co-glycolic acid) (PEG-PLGA) polymersomes conjugated with lactoferrin (Lf-POS). The brain delivery properties of Lf-POS were investigated and optimized. Three formulations of Lf-POS, with different densities of lactoferrin on the surface of polymersomes, were prepared and characterized. The brain delivery properties in mice were investigated using 6-coumarin as a fluorescent probe loaded in Lf-POS (6-coumarin-Lf-POS). A neuroprotective peptide, S14G-humanin, was incorporated into Lf-POS (SHN-Lf-POS); a protective effect on the hippocampuses of rats treated by Amyloid-β(25-35) was investigated by immunohistochemical analysis. The results of brain delivery in mice demonstrated that the optimized number of lactoferrin conjugated per polymersome was 101. This obtains the greatest blood-brain barrier (BBB) permeability surface area(PS) product and percentage of injected dose per gram brain (%ID/g brain). Immunohistochemistry revealed the SHN-Lf-POS had a protective effect on neurons of rats by attenuating the expression of Bax and caspase-3 positive cells. Meanwhile, the activity of choline acetyltransferase (ChAT) had been increased compared with negative controls. These results suggest that lactoferrin functionalized self-assembled PEG-PLGA polymersomes could be a promising brain-targeting peptide drug delivery system via intravenous administration.

Study Information

Provider

pubmed

Year

2011

Date

2011-10-07T00:00:00.000Z

DOI

10.1007/s11095-011-0513-7

Citations

73

References

43