Literature DB >> 33397721

Small-molecule inhibitors for the Prp8 intein as antifungal agents.

Zhong Li1, Anil Mathew Tharappel1, Jimin Xu2, Yuekun Lang1, Cathleen M Green3, Jing Zhang1, Qishan Lin4, Sudha Chaturvedi1,5, Jia Zhou2, Marlene Belfort6,5, Hongmin Li7,5,8.   

Abstract

Self-splicing proteins, called inteins, are present in many human pathogens, including the emerging fungal threats Cryptococcus neoformans (Cne) and Cryptococcus gattii (Cga), the causative agents of cryptococcosis. Inhibition of protein splicing in Cryptococcus sp. interferes with activity of the only intein-containing protein, Prp8, an essential intron splicing factor. Here, we screened a small-molecule library to find addititonal, potent inhibitors of the Cne Prp8 intein using a split-GFP splicing assay. This revealed the compound 6G-318S, with IC50 values in the low micromolar range in the split-GFP assay and in a complementary split-luciferase system. A fluoride derivative of the compound 6G-318S displayed improved cytotoxicity in human lung carcinoma cells, although there was a slight reduction in the inhibition of splicing. 6G-318S and its derivative inhibited splicing of the Cne Prp8 intein in vivo in Escherichia coli and in C. neoformans Moreover, the compounds repressed growth of WT C. neoformans and C. gattii In contrast, the inhibitors were less potent at inhibiting growth of the inteinless Candida albicans Drug resistance was observed when the Prp8 intein was overexpressed in C. neoformans, indicating specificity of this molecule toward the target. No off-target activity was observed, such as inhibition of serine/cysteine proteases. The inhibitors bound covalently to the Prp8 intein and binding was reduced when the active-site residue Cys1 was mutated. 6G-318S showed a synergistic effect with amphotericin B and additive to indifferent effects with a few other clinically used antimycotics. Overall, the identification of these small-molecule intein-splicing inhibitors opens up prospects for a new class of antifungals.

Entities:  

Keywords:  Cryptococcus; Prp8 intein; antifungal; protein splicing; small-molecule inhibitor

Mesh:

Substances:

Year:  2021        PMID: 33397721      PMCID: PMC7812778          DOI: 10.1073/pnas.2008815118

Source DB:  PubMed          Journal:  Proc Natl Acad Sci U S A        ISSN: 0027-8424            Impact factor:   11.205


  75 in total

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Journal:  Protein Eng Des Sel       Date:  2014-08       Impact factor: 1.650

6.  Förster resonance energy transfer-based cholesterolysis assay identifies a novel hedgehog inhibitor.

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Authors:  Matthew Brecher; Zhong Li; Binbin Liu; Jing Zhang; Cheri A Koetzner; Adham Alifarag; Susan A Jones; Qishan Lin; Laura D Kramer; Hongmin Li
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2.  Calcimycin Inhibits Cryptococcus neoformans In Vitro and In Vivo by Targeting the Prp8 Intein Splicing.

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4.  Nanomolar, Noncovalent Antagonism of Hedgehog Cholesterolysis: Exception to the "Irreversibility Rule" for Protein Autoprocessing Inhibition.

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Review 6.  Inteins as Drug Targets and Therapeutic Tools.

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Journal:  Front Mol Biosci       Date:  2022-02-08

7.  Cryptococcus neoformans Prp8 Intein: An In Vivo Target-Based Drug Screening System in Saccharomyces cerevisiae to Identify Protein Splicing Inhibitors and Explore Its Dynamics.

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