Mapping the Madurella mycetomatis pathogen and host responses during and after antifungal treatment to identify prognostic therapeutic markers for mycetoma

2022 年度 実施状況報告書

• 研究課題/領域番号: 20K08832
• 研究機関: 国立研究開発法人理化学研究所
• 研究代表者: アブケセーサ イマド 国立研究開発法人理化学研究所, 生命医科学研究センター, 上級研究員 (10749906)
• 研究期間 (年度): 2020-04-01 – 2024-03-31
• キーワード: Mycology / Eumycetoma / Galleria mellonella / Antifungal / Madurella mycetomatis / Transcriptomics

研究実績の概要

During FY2022 we completed two major tasks.First, the library preparations and sequencing for transcriptomics analysis was successfully completed.Second, pharmacokinetics of antifungal agents in Galleria mellonella larvae. For the trsanscriptomics analysis, total RNA was extracted from six type of samples at 4 timepoints (6hr,30hr,72hr, and 168hr) in triplicates (4x3 =12) the type of samples are (Healthy G. mellonella larvae,infected G. mellonella larvae with M. mycetomatis, Healthy G. mellonella larvae treated with itraconazole,infected G. mellonella larvae with M. mycetomatis treated with itraconazole (n=12),Healthy G. mellonella larvae treated with ravuconazole and infected Galleria mellonella larvae with M. mycetomatis treated with ravuconazole.Total of 72 RNA-seq libraries were prepared and sequenced. Since we have extra RNA aliquot reaming, we prepared and sequenced LQ-ssCAGE (low quantity single strand CAGE) libraries from the same samples (n=72).Raw sequenced reads mapped against the G. mellonella larvae (host) genome and then against the pathogen M. mycetomatis genome. We obtained a high mapping ratio according to RNA-seq standards.As for the pharmacokinetics(PK) of antifungal agents in G. mellonella larvae,The PK of itraconazole was determined after the administration of a single dose to uninfected G. mellonella larvae. Concentrations of antifungal agents were present during 24hr after injection and above the MIC. The AUC24h for itraconazole (61.9% of human AUC) was lower in G. mellonella larvae than in humans.

現在までの達成度 (区分)

1: 当初の計画以上に進展している

理由

All planned tasks in FY2022 successfully completed. Tasks which was impacted by lock-down during FY2020-21 were recovered.Final computation and statistical analysis already started in FY2022.

今後の研究の推進方策

The progress we made during FY2023 will enable us to be processed with differential gene expression analysis of host and pathogen genes followed by pathways enrichment analysis to find host and pathogen enriched pathways during treatment with antifungal agents.
For LQ-ssCAGE dataset, we will confirm the reproducibility of the RNA-seq results.
As addition outcome of this project, we will use LQ-ssCAGE to call promoters and enhancers of Galleria mellonella (host) and Madurella mycetomatis (pathogen). This will be an important contribution to the annotation of host and pathogen genomes.
After completing the above analysis, we will start to draft at least two manuscripts. One for the host response to the antifungal treatment and the second manuscript will be an atlas for promoters and enhancers of invertebrate Galleria mellonella.