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Last update 11 Oct 2025

Harmaline

Last update 11 Oct 2025

Overview

R&D Status

Clinical Result

Translational Medicine

Overview

Basic Info

Drug Type

Small molecule drug

Synonyms

HAR

Target

MARK4

Action

inhibitors

Mechanism

MARK4 inhibitors(microtubule affinity regulating kinase 4 inhibitors)

Therapeutic Areas

Nervous System Diseases

Active Indication

Alzheimer Disease

Inactive Indication-

Originator Organization

University of Hail

Active Organization

University of Hail

Inactive Organization-

License Organization-

Drug Highest PhasePreclinical

First Approval Date-

Regulation-

Structure/Sequence

Molecular FormulaC13H14N2O

InChIKeyRERZNCLIYCABFS-UHFFFAOYSA-N

CAS Registry304-21-2

Clinical Trials associated with Harmaline

CTRI/2018/04/013398

/ Not yet recruitingPhase 2IIT

An Open Labeled, Active Controlled, Randomized, Parallel Group Study Of Efficacy Of Nano Haritaki In Malavshtambha Vis-Ã?-Vis Functional Constipation

Start Date01 Jun 2018

Sponsor / Collaborator-

100 Clinical Results associated with Harmaline

100 Translational Medicine associated with Harmaline

100 Patents (Medical) associated with Harmaline

1,412

Literatures (Medical) associated with Harmaline

01 Dec 2025·TOXICON

Chemical fingerprinting of Peganum harmala seeds via UV–Vis, XRD, TGA, FTIR, and GC-MS techniques; In vitro assessment of cytotoxic properties

Article

Author: Sunil, Sreya ; P, Amruth

Peganum harmala L., a perennial herb traditionally valued for medicinal and ritual uses, was comprehensively profiled to elucidate its chemical composition and cytotoxic potential. Methanolic seed extracts contained diverse primary and secondary metabolites, including alkaloids, flavonoids, saponins, glycosides, steroids, proteins, and carbohydrates. Proximate analysis revealed high moisture (45.88 %) and crude fibre (18.39 %) with moderate fat (14.74 %) and protein (7.67 %) levels. Spectroscopic studies supported the presence of β-carboline alkaloids: FTIR spectra showed characteristic functional group vibrations, UV-Vis displayed a strong absorption at 440 nm, and X-ray diffraction revealed semi-crystalline patterns enriched in harmine and harmaline. GC-MS provided definitive chemical identification, detecting harmine (53.13 %) and harmaline (39.12 %) as major constituents. Thermal analyses (TGA-DTA and DTG) indicated multiphase decomposition typical of complex organic matrices. Cytotoxicity assessment using the MTT assay on L929 fibroblast cells demonstrated a dose-dependent decline in cell viability, with an LC₅₀ of 243.9 μg/mL, signifying moderate-high cytotoxic potential. These findings validate the ethnomedicinal significance of P. harmala and underscore its promise for phytomedicine, nutraceutical applications, and pharmaceutical research, while highlighting the necessity of standardized and regulated use to ensure efficacy and safety.

18 Aug 2025·NATURAL PRODUCT RESEARCH

Exploring the antimitotic, thrombolytic, and cytotoxic properties of lasiosiphon glaucus or gnidia glauca (fresen.) gilg leaf alkaloid extract: insights from experimental and in silico investigations

Article

Author: Kumar, Vadlapudi ; Valleti, Poorna Vivek ; Vijendra Dittekoppa, Poornima ; CM, Anuradha ; Gopalappa, Ranjitha ; Ramayanam, Pradeep Kumar

Plant alkaloids are nitrogen containing secondary metabolites that have wide range of biological properties including anticancer activity. 'Lasiosiphon glaucus', or 'Gnidia glauca (Fresen.) Gilg,' known for its biological properties, requires exploration to evaluate cytotoxic and anticancer effects. The present study is aimed to evaluate L. glaucus leaf alkaloid extract (LgLAE) for antimitotic, thrombolytic, and cytotoxic properties. LgLAE demonstrated comparable antimitotic efficacy to methotrexate in Allium cepa root meristematic cells. Thrombolytic evaluation showed a maximum observed clot lysis of 41.39 ± 0.21% at 2 mg/100 µL. Cytotoxicity assay shows greater inhibition of MCF-7 (144.51 μg/mL) cancer cell proliferation than MCF-10A cells (409.86 μg/mL), indicating potential cancer-specific effects. Computational analysis revealed strong binding affinities between L. glaucus alkaloids (Ergocristine, Solasodine, Solanocapsine, Delphinine, and Harmidine) and relevant receptors. These findings highlight L. glaucus contains valuable natural compounds with pharmacological effects, particularly in antimitotic, thrombolytic, and cytotoxic effects, it essential for further investigation for cancer treatment.

01 Jul 2025·FOOD AND CHEMICAL TOXICOLOGY

Bavachinin causes cholestasis by down-regulating BAAT expression and disrupting glycocholic acid synthesis in human liver organoids

Article

Author: Chen, Xiaomeng ; Zhao, Xinyan ; Wang, Xue ; Su, Yu ; Liu, Lin ; Jia, Jidong

Psoraleae Fructus (Bu Gu Zhi, BGZ) is extensively utilized for dermatological and osseous disorders in China. BGZ-induced liver injury has become one of the major concerns, which predominantly cause cholestasis, with the pathogenesis not being fully elucidated. Currently, studies on hepatotoxic mechanisms of BGZ have mainly been conducted on 2D cell culture systems or rodent models, which may not fully encapsulate human pathophysiology. Therefore, we generated human liver organoids (HLOs) from healthy donor(s) for living-related liver transplantation to explore the hepatotoxic mechanism. We identified bavachinin (BVC) as the most hepatotoxic component for cholestasis. After validating by CLF tests, we identified BVC caused cholestasis by down-regulating BAAT, which catalyzes the amidation of bile acids. We also found that up-regulating BAAT with harmaline could mitigate cholestasis and enhance cell viabilities in HLOs. We further demonstrated that glycocholic acid (GCA) levels decreased in BVC-treated HLOs. Supplementation of GCA to BVC-treated HLOs significantly improved cell viabilities. Collectively, our data suggested that BVC impaired the GCA synthesis by down-regulating the expression of BAAT, thereby inducing cholestasis.

100 Deals associated with Harmaline

R&D Status

10 top R&D records.

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Indication	Highest Phase	Country/Location	Organization	Date
Alzheimer Disease	Preclinical	Saudi Arabia	University of Hail	01 Oct 2022

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Harmaline

Overview

Basic Info

Structure/Sequence

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R&D Status

Clinical Result

Translational Medicine

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Core Patent

Clinical Trial

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Regulation