Brazilian Red Propolis and Its Active Constituent 7-O-methylvestitol Impair Early and Late Stages of Toxoplasma gondii Infection in Human Placental Models.

巴西红蜂胶及其活性成分 7-O-甲基蜂胶醇可抑制人类胎盘模型中弓形虫感染的早期和晚期阶段

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作者:Teixeira Samuel Cota, de Souza Guilherme, Dos Santos Natalia Carine Lima, de Oliveira Rafael Martins, Silva Nagela Bernadelli Sousa, de Lima Junior Joed Pires, Rosini Alessandra Monteiro, Luz Luana Carvalho, Martínez Aryani Felixa Fajardo, Almeida Marcos Paulo Oliveira, Faria Guilherme Vieira, Alves Rosiane Nascimento, Gomes Angelica Oliveira, Ambrosio Maria Anita Lemos Vasconcelos, Veneziani Rodrigo Cassio Sola, Bastos Jairo Kenupp, Mineo José Roberto, Martins Carlos Henrique Gomes, Ferro Eloisa Amália Vieira, Barbosa Bellisa Freitas
Toxoplasma gondii is a globally distributed protozoan parasite and a major cause of congenital infections, particularly in South America. Current therapies for congenital toxoplasmosis are limited by toxicity, long treatment regimens, and suboptimal efficacy, highlighting the urgent need for safer and more effective alternatives. In this study, we evaluated the antiparasitic effects of crude ethanolic extract of Brazilian Red Propolis (BRP) and its isolated compounds, focusing on 7-O-methylvestitol, in human trophoblast (BeWo) cells and third-trimester placental explants. Both BRP and 7-O-methylvestitol significantly reduced T. gondii adhesion, invasion, and intracellular replication, without compromising host cell viability. Ultrastructural analyses revealed irreversible parasite damage, and cytokine profiling demonstrated immunomodulatory effects, with enhanced production of interleukin (IL)-6, IL-8, and macrophage migration inhibitory factor (MIF) in BeWo cells and downregulation of IL-6, MIF, and tumor Necrosis Factor (TNF) in infected placental villi. Notably, 7-O-methylvestitol reproduced and, in some assays, surpassed the antiparasitic activity of BRP, suggesting it as a key bioactive constituent responsible for the therapeutic potential of the extract. These findings support the identification of 7-O-methylvestitol as a promising lead compound for structure-based drug design and repositioning strategies, advancing the development of novel, safe, and targeted therapies against congenital toxoplasmosis.

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