Hepatoprotective Activity, In Silico Analysis, and Molecular Docking Study of Verbascoside from Leucophyllum frutescens in Rats with Post-Necrotic Liver Damage

Author:

Jaramillo-Morales Osmar Antonio1ORCID,Díaz-Cervantes Erik2ORCID,Via Lisa Dalla3ORCID,Garcia-Argaez Aida Nelly3,Espinosa-Juárez Josué Vidal4ORCID,Ovando-Zambrano José Carlos4,Muñoz-Pérez Victor Manuel5ORCID,Valadez-Vega Carmen5ORCID,Bautista Mirandeli5ORCID

Affiliation:

1. Life Sciences Division, Nursing and Obstetrics Department, Campus Irapuato-Salamanca, University of Guanajuato, Ex Hacienda el Copal, km. 9 Carretera Irapuato-Silao, A.P. 311, Irapuato 36500, Guanajuato, Mexico

2. Departamento de Alimentos, Centro Interdisciplinario del Noreste, Universidad de Guanajuato, Tierra Blanca 37975, Guanajuato, Mexico

3. Department of Pharmaceutical and Pharmacological Sciences, University of Padova, via F. Marzolo 5, 35131 Padova, Italy

4. School of Chemical Sciences, Autonomous University of Chiapas, Ocozocoautla de Espinosa 29140, Chiapas, Mexico

5. Academic Area of Pharmacy, Health Sciences Institute, Autonomous of Hidalgo State University, Circuito Ex-Hacienda La Concepción, Km 1.5, San Agustín Tlaxiaca 42160, Hidalgo, Mexico

Abstract

There is an urgent need for scientists to verify the pharmacological properties of medicinal plants. Leucophyllum frutescens (Lf) belongs to the family Scrophulariaceae, and it is used in the treatment of airway diseases such as cough, tuberculosis, and asthma. The methanolic extract of the aerial parts of Lf allows for the isolation and identification of verbascoside (Vb). This study aimed to evaluate the hepatoprotective effect of Vb, a caffeoyl phenylethanoid glycoside (CPG), on post-necrotic liver damage induced by thioacetamide (TA) via in vivo and in silico studies, with the latter considering a cancerous process. The aerial parts of Lf were extracted by maceration using hexane methanol (5 L/500 g/8 days). Vb was isolated from methanol extract at approximately 30%. Wistar rats were intragastrically pretreated or not with a single dose of Vb (20 mg/kg) for four days. On the fourth day, a single dose of TA (6.6 mmol/kg) was intraperitoneally injected. Blood samples and parameters related to liver damage, like AST and ALT, were obtained. Vb significantly reduced the level of liver injury following thioacetamide-induced necrosis. This was corroborated by in silico assay and docking studies, demonstrating that Vb can interact with a HeLa target through hydrogen bonds and electrostatic interactions, achieving better performance than commercial chemotherapeutic Taxol®, by 0.34 kcal/mol. AST and ALT were significantly lower in the rats pretreated with Vb. Furthermore, Vb did not induce cytotoxicity and had a median lethal dose (LD50) greater than 5000 mg/kg. These results suggest that Vb may be used as an alternative to reduce liver damage.

Funder

CONACYT, Mexico

University of Padova -Dotazione Ordinaria Ricerca

Convocatoria Institucional de Investigación Científica

Publisher

MDPI AG

Subject

Pharmaceutical Science

Reference55 articles.

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