This study comparatively characterized the phenolic profiles and in vitro cytotoxic activity of methanolic extracts from aerial and underground parts of eight Geranium species native to Serbia ( Geranium macrorrhizum , Geranium robertianum , Geranium phaeum , Geranium sanguineum , Geraniumpalustre , Geranium pyrenaicum , Geranium columbinum , and Geranium lucidum ). Phenolic constituents were analysed by LC‐PDA/MS, and cytotoxicity against human cancer cell lines (HeLa, PC‐3, HT‐29, Hs‐294T) and normal lung fibroblasts (MRC‐5) was evaluated using the MTT assay. Ellagitannins predominated, followed by phenolic acids and flavonols, with pronounced species‐ and organ‐specific variability. Some phenolics were identified for the first time in specific taxa and organs. Several extracts showed selective cytotoxicity, mainly against HeLa cells, with the strongest activity observed for underground parts of G. sanguineum (IC 50 = 2.52 µg/mL). Geraniin demonstrated selective cytotoxic effects. These findings highlight the chemical diversity and biological potential of the investigated Geranium species and support further mechanistic and in vivo studies.

01 Feb 2026·JOURNAL OF ETHNOPHARMACOLOGY

Multi-target therapeutics of geraniin from Geranium wilfordii Maxim. and related species: Mechanisms and applications

Review

Author: Zhang, Ping ; Wang, Long ; Zhang, Ting ; Ye, Qiang ; Chen, Yangxi ; Ao, Hui ; Zhong, Jie ; Cai, Jia ; Li, Jiaxin ; Zhu, Shunpeng ; Xu, Min

ETHNOPHARMACOLOGICAL RELEVANCE:

Erodii Herba Geranii Herba (also called Laoguancao in China) is the dried aerial part of Geranium wilfordii Maxim., Geranium carolinianum L. or Erodium stephanianum Willd. It has developed into a natural remedy known for its anti-inflammatory, analgesic and hepatoprotective properties, and widely recognized within traditional Chinese medicine (TCM) and its cultural context. Given the traditional applications of Erodii Herba Geranii Herba, which underscore its potential as a promising source of bioactive compounds for pharmaceutical development, geraniin-one of its principal active constituents-has attracted increasing attention for its prospective development and utilization. Previous studies have demonstrated that geraniin exhibits a broad spectrum of pharmacological activities, including metabolic regulation, organ protection mediated through anti-inflammatory and antioxidant mechanisms, as well as antitumor and antiviral effects. Nevertheless, a systematic review of these pharmacological activities and their underlying mechanisms remains lacking.

AIM OF THE STUDY:

This review focused on the pharmacological activities of geraniin and also summarized its availability, pharmacokinetics, and toxicity, thereby providing a solid theoretical foundation for its further development and practical utilization.

MATERIAL AND METHODS:

The literature included in this review was identified through searches conducted in the PubMed and China National Knowledge Infrastructure (CNKI) databases using the keywords "Geraniin", "Pharmacology", and "Pharmacokinetics". A total of 99 articles were retrieved, excluding review articles. The retrieved publications covered a period from 1974 to 2025.

RESULTS:

Geraniin demonstrated a range of pharmacological effects, including regulation of metabolism (glycolipid metabolism, blood pressure, and bone metabolism), protection of multiple organs (brain, cardiovascular, pulmonary, gastrointestinal, and renal systems), anti-tumor activity (against lung, breast, colorectal, and cervical cancers), and broad-spectrum antiviral properties. Notably, the multi-target actions of geraniin facilitated cross-disease modulation through involvement in the oxidative-inflammatory network (via NF-κB-Nrf2 and MAPK pathways) and the cell survival network (including PI3K/Akt and Wnt/β-catenin pathways), thereby underpinning its organ-protective effects, anti-tumor activity, and metabolic regulatory functions.

CONCLUSION:

These attributes suggested that geraniin held promise as a multi-targeted therapeutic agent. Thus, this paper elucidated the possibility of exploiting the resources of geraniin as a pharmaceutical product.

01 Jan 2026·CHEMISTRY & BIODIVERSITY

Isolation, Identification, and in Vitro Antitumor Activity of Polyphenols From Euryale ferox Salisb . Shell

Article

Author: Shan, Tiantian ; Lu, Xinyi ; Wang, Hongxun ; Jian, Xinru ; Yang, Yuhan ; Ge, Haotian ; Li, Longjie ; Wang, Limei

ABSTRACT:

The shell of Euryale ferox Salisb ., rich in polyphenols, has antitumor potential. We isolated and identified polyphenols from the shell and evaluated their in vitro antitumor activity. Compounds were extracted with 70% ethanol under ultrasound and purified by fractional extraction and silica gel chromatography, yielding three substances. Liquid chromatography–mass spectrometry (LC‐MS) and nuclear magnetic resonance confirmed the three compounds as ellagic acid, corilagin, and geraniin. High‐performance LC quantification showed corilagin and geraniin concentrations of 66.23 and 58.41 mg/g. In vitro experiments on cells showed the ethanol extract had strong inhibitory effects on cell proliferation (IC 50 : 68.56 µg/mL for HeLa, 78.09 µg/mL for A2780), and cell proliferation, migration, and invasion were regulated by the three compounds, exhibiting time‐ and dose‐dependent characteristics. Corilagin showed the strongest inhibitory effect on HeLa cell proliferation (74.61% at 48 h) and A2780 cell invasion (69.86%). Geraniin inhibited HeLa cell invasion (63.33%) and A2780 cell invasion (61.64%). This study determined the chemical structures of polyphenolic compounds from Euryale ferox Salisb . shell and their impact on tumor cell proliferation, migration, and invasion, offering evidence for developing antitumor drugs and insights for modernizing traditional Chinese medicinal resources.

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Indication	Highest Phase	Country/Location	Organization	Date
Tardive Dyskinesia	Preclinical	Taiwan Province	Mackay Junior College of Medicine, Nursing & Management	06 Jun 2025
Tardive Dyskinesia	Preclinical	Taiwan Province	Mackay Memorial Hospital	06 Jun 2025
stress oxidative	Preclinical	China	Jiangsu University	01 May 2025

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