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IGF-1

Insulin-like Growth Factor 1, Somatomedin C

Quick Stats
Studies 92
Trials 100
Score 2
2025 pubmed

Network pharmacology reveals Ficus. Carica. L latex as a potential therapeutic agent for gastric ulcers by modulating inflammation and promoting repair.

Shady. Nourhan Hisham NH; Hisham. Mohamed M; Abdullah. Hend Samy HS; Maher. Sherif A SA; Albohy. Amgad A; Elrehany. Mahmoud A MA; Sayed. Ahmed M AM; Allehyani. Esam S ES; Khowdiary. Manal M MM; Shawky. Ahmed M AM; Abdelmohsen. Usama Ramadan UR

Key Findings

  • Fig latex reduced ulcer severity and lowered the ulcer index in rats
  • It decreased inflammatory markers (IL‑6, TNF‑α, IL‑1β) and lowered IGF‑1 gene expression
  • It increased healing‑related genes (EGF, KGF) and showed antioxidant activity

Practical Outcomes

  • The findings hint that fig latex could be a natural aid for gut health and might modestly lower IGF‑1 activity, which some biohackers view as beneficial for longevity. However, the evidence is limited to animal models, so there’s no clear dosage or safety guidance for humans yet. Until more research is done, it’s not ready for direct supplementation.

Summary

A study in rats found that latex from the common fig tree (Ficus carica) helps heal stomach ulcers caused by a drug, partly by lowering inflammation and reducing the activity of IGF‑1 and other harmful genes while boosting healing factors. The extract also showed antioxidant properties and contains several compounds that might be responsible for these effects.

Abstract

The primary objective of our research is to investigate the gastroprotective impact of Ficus. carica L. latex extract (FCL). Metabolic profiling based on HR- LCMS for the extract led to the annotation of 20 compounds. Additionally, the gastro-protective activity of the latex extract was evaluated in vivo using male albino rats. FCL significantly alleviated the indomethacin-induced ulceration and reduced the ulcer index. Furthermore, the inflammation caused by indomethacin was seen to diminish due to the downregulation of the production of certain genes (IL-6, and TNF-α, IL-1β). Besides, FCL considerably reduced the elevated TGF-β, and IGF-1, COX-2 relative gene expression. Likewise, FCL dramatically raised EGF and KGF relative gene expression, demonstrating its beneficial impact in ulcer healing. The antioxidant ability of FCL was assessed by in vitro experiments utilizing hydrogen peroxide and superoxide radical scavenging, which demonstrated significant antioxidant capacity. Employing network pharmacology, we identified 10 hub genes central to peptic ulcer disease and conducted molecular docking studies screening interactions between FCL extract compounds and these hubs along with anti-inflammatory targets including FGFR, TGF-βR, IGFR-1R and IL-1R1 involved in ulcer healing. Additionally, an in-silico study using annotated FCL compounds highlighted Ficuseptin-C, Ficuseptin-B and Ficusin-A in the extract may contribute to its antiulcer properties. The present study highlighted the potential of FCL as a promising natural gastro-protective agent.

Study Information

Provider

pubmed

Year

2025

Date

2025-12-02T00:00:00.000Z

DOI

10.1371/journal.pone.0333777

References

50