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Δ9-Tetrahydrocannabinolic Acid markedly alleviates liver fibrosis and inflammation in mice

Beatriz Carmona-Hidalgo, Isabel González-Mariscal, Adela García-Martín, María E Prados, Francisco Ruiz-Pino, Giovanni Appendino, Manuel Tena-Sempere, Eduardo Muñoz
Key takeaways
  1. 01Δ9-THCA is a non-psychotropic cannabinoid found in raw cannabis
  2. 02Reduced fibrotic markers like Tenascin C and collagen in cell studies
  3. 03Alleviated liver inflammation and scarring in two different mouse models
  4. 04Improved metabolic health and reduced body weight in obese mice
  5. 05Suggests potential for treating NAFLD without the psychoactive effects of THC

Δ9-THCA may reduce liver scarring and inflammation in mice, suggesting potential for treating fatty liver disease without psychoactive effects.

Abstract

Background: Non-alcoholic fatty liver disease (NAFLD) is the most common liver disease in the Western world, and it is closely associated to obesity, type 2 diabetes mellitus, and dyslipidemia. Medicinal cannabis and some neutral cannabinoids have been suggested as a potential therapy for liver diseases.

Hypothesis: Δ9-tetrahydrocannabinolic acid (Δ9-THCA), the non-psychotropic precursor of Δ9-THC, is one of the most abundant cannabinoids presents in Cannabis Sativa. However, its biological activities have been poorly investigated. Herein, we studied the antifibrotic and antiinflammatory activities of Δ9-THCA in two different animal models of liver injury, providing a rationale for additional studies on the medicinal use of this cannabinoid in the treatment of liver fibrosis and the management of NAFLD.

Study design: The antifibrotic activity of Δ9-THCA in vitro was investigated in the cell lines LX-2 and NIH-3T3-Col1A2-luc. Non-alcoholic liver fibrosis was induced in mice by CCl4 treatment or, alternatively, by 23-week high fat diet (HFD) feeding. Δ9-THCA was administered daily intraperitoneally during the CCl4 treatment or during the last 3 weeks in HFD-fed mice.

Methods: TGFβ-induced profibrotic gene expression was analyzed by luciferase and qPCR assays. Liver fibrosis and inflammation were assessed by immunochemistry and qPCR. Blood glucose, insulin, leptin and triglyceride levels were measured in HFD mice.

Results: Δ9-THCA inhibited the expression of Tenascin C (TNC) and Col3A1 induced by TGFβ in LX-2 cells and the transcriptional activity of the Col1A2 promoter in fibroblasts. Δ9-THCA significantly attenuated CCl4-induced liver fibrosis and inflammation and reduced T cell and macrophage infiltration. Mice fed HFD for 23 weeks developed severe obesity (DIO), fatty liver and marked liver fibrosis, accompanied by immune cell infiltration. Δ9-THCA, significantly reduced body weight and adiposity, improved glucose tolerance, and drastically attenuated DIO-induced liver fibrosis and immune cell infiltration.

Conclusions: Δ9-THCA prevents TGFβ-induced fibrotic markers in vitro and liver inflammation and fibrogenesis in vivo, providing a rationale for additional studies on the medicinal use of this cannabinoid, as well as cannabis preparations containing it, for the treatment of liver fibrosis and the management of NAFLD.

Cite this study
APA
Beatriz Carmona-Hidalgo, Isabel González-Mariscal, Adela García-Martín, María E Prados, Francisco Ruiz-Pino, Giovanni Appendino, Manuel Tena-Sempere, & Eduardo Muñoz (2021). Δ9-Tetrahydrocannabinolic Acid markedly alleviates liver fibrosis and inflammation in mice. https://fasciaresearchdatabase.com/%ce%b49-tetrahydrocannabinolic-acid-markedly-alleviates-liver-fibrosis-and-inflammation-in-mice/
MLA
Beatriz Carmona-Hidalgo, et al. "Δ9-Tetrahydrocannabinolic Acid markedly alleviates liver fibrosis and inflammation in mice." 2021, https://fasciaresearchdatabase.com/%ce%b49-tetrahydrocannabinolic-acid-markedly-alleviates-liver-fibrosis-and-inflammation-in-mice/.
Chicago
Beatriz Carmona-Hidalgo et al. 2021. "Δ9-Tetrahydrocannabinolic Acid markedly alleviates liver fibrosis and inflammation in mice.". https://fasciaresearchdatabase.com/%ce%b49-tetrahydrocannabinolic-acid-markedly-alleviates-liver-fibrosis-and-inflammation-in-mice/