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Humanin

HN, S14G-Humanin

Quick Stats
Studies 491
Trials 100
Score 2
2014 pubmed 8 citations

Genome expression analysis by suppression subtractive hybridization identified overexpression of Humanin, a target gene in gastric cancer chemoresistance.

Mottaghi-Dastjerdi. Negar N; Soltany-Rezaee-Rad. Mohammad M; Sepehrizadeh. Zargham Z; Roshandel. Gholamreza G; Ebrahimifard. Farzaneh F; Setayesh. Neda N

Key Findings

  • Humanin isoforms are the most over‑expressed genes in gastric cancer tissue compared to normal tissue
  • Humanin isoform 3 shows the highest increase, about 4‑fold over normal levels
  • Elevated humanin may contribute to chemotherapy resistance, making it a potential target for new cancer therapies

Practical Outcomes

  • If you’re experimenting with humanin for anti‑aging or metabolic benefits, be aware that high levels could potentially aid cancer cell survival. Until more safety data are available, it’s prudent to avoid chronic high‑dose humanin supplementation, especially if you have a personal or family history of cancer.

Summary

The study found that the small peptide humanin is produced at much higher levels in stomach cancer cells and may help those cells resist chemotherapy, suggesting that blocking humanin could improve cancer treatment. For biohackers, this means that taking humanin supplements might carry a risk of supporting cancer cell survival, so caution is advised, especially for anyone with cancer risk or existing disease.

Abstract

In cancer cells, apoptosis is an important mechanism that influences the outcome of chemotherapy and the development of chemoresistance. To find the genes involved in chemoresistance and the development of gastric cancer, we used the suppression subtractive hybridization method to identify the genes that are overexpressed in gastric cancer tissues compared to normal gastric tissues. In the suppression subtractive hybridization library we constructed, the most highly overexpressed genes were humanin isoforms. Humanin is a recently identified endogenous peptide that has anti-apoptotic activity and has been selected for further study due to its potential role in the chemoresistance of gastric cancer. Upregulation of humanin isoforms was also observed in clinical samples by using quantitative real-time PCR. Among the studied isoforms, humanin isoform 3, with an expression level of 4.166 ± 1.44 fold, was the most overexpressed isoform in GC. The overexpression of humanin in gastric cancer suggests a role for chemoresistance and provides new insight into the biology of gastric cancer. We propose that humanin isoforms are novel targets for combating chemoresistance in gastric cancer.

Study Information

Provider

pubmed

Year

2014

Date

2014-01-08T00:00:00.000Z

DOI

10.1186/2008-2231-22-14

Citations

8