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Anti-Toxoplasma gondii Effects of Lipopeptide Derivatives of Lycosin-I.


ABSTRACT: Toxoplasmosis, caused by Toxoplasma gondii (T. gondii), is a serious zoonotic parasitic disease. We previously found that Lycosin-I exhibited anti-T. gondii activity, but its serum stability was not good enough. In this study, we aimed to improve the stability and activity of Lycosin-I through fatty acid chain modification, so as to find a better anti-T. gondii drug candidate. The α/ε-amino residues of different lysine residues of Lycosin-I were covalently coupled with lauric acid to obtain eight lipopeptides, namely L-C12, L-C12-1, L-C12-2, L-C12-3, L-C12-4, L-C12-5, L-C12-6, and L-C12-7. Among these eight lipopeptides, L-C12 showed the best activity against T. gondii in vitro in a trypan blue assay. We then conjugated a shorter length fatty chain, aminocaproic acid, at the same modification site of L-C12, namely L-an. The anti-T. gondii effects of Lycosin-I, L-C12 and L-an were evaluated via an invasion assay, proliferation assay and plaque assay in vitro. A mouse model acutely infected with T. gondii tachyzoites was established to evaluate their efficacy in vivo. The serum stability of L-C12 and L-an was improved, and they showed comparable or even better activity than Lycosin-I did in inhibiting the invasion and proliferation of tachyzoites. L-an effectively prolonged the survival time of mice acutely infected with T. gondii. These results suggest that appropriate fatty acid chain modification can improve serum stability and enhance anti-T. gondii effect of Lycosin-I. The lipopeptide derivatives of Lycosin-I have potential as a novel anti-T. gondii drug candidate.

SUBMITTER: Liu X 

PROVIDER: S-EPMC10467082 | biostudies-literature | 2023 Jul

REPOSITORIES: biostudies-literature

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Anti-<i>Toxoplasma gondii</i> Effects of Lipopeptide Derivatives of Lycosin-I.

Liu Xiaohua X   Zhang Peng P   Liu Yuan Y   Li Jing J   Yang Dongqian D   Liu Zhonghua Z   Jiang Liping L  

Toxins 20230726 8


Toxoplasmosis, caused by <i>Toxoplasma gondii</i> (<i>T. gondii</i>), is a serious zoonotic parasitic disease. We previously found that Lycosin-I exhibited anti-<i>T. gondii</i> activity, but its serum stability was not good enough. In this study, we aimed to improve the stability and activity of Lycosin-I through fatty acid chain modification, so as to find a better anti-<i>T. gondii</i> drug candidate. The α/ε-amino residues of different lysine residues of Lycosin-I were covalently coupled wit  ...[more]

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