Appraising the "entourage Effect": Antitumor Action of a Pure Cannabinoid Versus a Botanical Drug Preparation in Preclinical Models of Breast Cancer

Overview

Journal Biochem Pharmacol

Specialties Biochemistry
Pharmacology

Date 2018 Jun 26

PMID 29940172

Citations 75

Authors

Sandra Blasco-Benito

Marta Seijo-Vila

Miriam Caro-Villalobos

Isabel Tundidor

Clara Andradas

Elena Garcia-Taboada

Jeff Wade

Stewart Smith

Manuel Guzman

Eduardo Perez-Gomez

Mara Gordon

Cristina Sanchez

Affiliations

Soon will be listed here.

Abstract

Breast cancer is the second leading cause of death among women. Although early diagnosis and development of new treatments have improved their prognosis, many patients present innate or acquired resistance to current therapies. New therapeutic approaches are therefore warranted for the management of this disease. Extensive preclinical research has demonstrated that cannabinoids, the active ingredients of Cannabis sativa, trigger antitumor responses in different models of cancer. Most of these studies have been conducted with pure compounds, mainly Δ-tetrahydrocannabinol (THC). The cannabis plant, however, produces hundreds of other compounds with their own therapeutic potential and the capability to induce synergic responses when combined, the so-called "entourage effect". Here, we compared the antitumor efficacy of pure THC with that of a botanical drug preparation (BDP). The BDP was more potent than pure THC in producing antitumor responses in cell culture and animal models of ER+/PR+, HER2+ and triple-negative breast cancer. This increased potency was not due to the presence of the 5 most abundant terpenes in the preparation. While pure THC acted by activating cannabinoid CB receptors and generating reactive oxygen species, the BDP modulated different targets and mechanisms of action. The combination of cannabinoids with estrogen receptor- or HER2-targeted therapies (tamoxifen and lapatinib, respectively) or with cisplatin, produced additive antiproliferative responses in cell cultures. Combinations of these treatments in vivo showed no interactions, either positive or negative. Together, our results suggest that standardized cannabis drug preparations, rather than pure cannabinoids, could be considered as part of the therapeutic armamentarium to manage breast cancer.

Citing Articles

Extraction, GC-MS analysis, cytotoxic, anti-inflammatory and anticancer potential of female flower; , and .

Safir W, Malik A, Saadia H, Zahid A, Li J Front Pharmacol. 2025; 16:1546062.

PMID: 40008130 PMC: 11850312. DOI: 10.3389/fphar.2025.1546062.

Cannabinoids as Promising Inhibitors of HER2-Tyrosine Kinase: A Novel Strategy for Targeting HER2-Positive Ovarian Cancer.

Lamtha T, Jongkon N, Lertvanithphol T, Horprathum M, Seetaha S, Choowongkomon K ACS Omega. 2025; 10(6):6191-6200.

PMID: 39989803 PMC: 11840771. DOI: 10.1021/acsomega.4c11108.

Acute and prolonged toxicity assessment of extract in rodents and lagomorphs.

Costa A, Gasparotto Jr A, Garcia A, Pereira C, Lourenco E, Joaquim H Toxicol Rep. 2025; 14:101918.

PMID: 39917037 PMC: 11800086. DOI: 10.1016/j.toxrep.2025.101918.

L. Extract Increases COX-1, COX-2 and TNF-α in the Hippocampus of Rats with Neuropathic Pain.

Bartkowiak-Wieczorek J, Jamka M, Kujawski R, Holysz M, Bienert A, Czora-Poczwardowska K Molecules. 2025; 30(1.

PMID: 39795254 PMC: 11721898. DOI: 10.3390/molecules30010194.

Research and Clinical Practice Involving the Use of Products, with Emphasis on Cannabidiol: A Narrative Review.

Simei J, Souza J, Pedrazzi J, Guimaraes F, Campos A, Zuardi A Pharmaceuticals (Basel). 2025; 17(12.

PMID: 39770486 PMC: 11677192. DOI: 10.3390/ph17121644.