如何利用突变文库鉴定白色念珠菌形成生物膜所需的基因。

UJEMI+ Pub Date : 2020-01-01 DOI:10.14288/UJEMI.V2I.193711
T. Anderson, Marcelio A. Shammami, Steven M. Taddei, Jonathan S. Finkel
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引用次数: 0

摘要

随着超过10亿的感染和病原体显示出胰腺癌等严重疾病,对病原真菌的研究从未像现在这样重要。2017年,美国在真菌疾病上花费了72亿美元。45亿美元用于75 055次住院治疗,26亿美元用于8 9932 230次门诊就诊。特别是念珠菌感染,成本为14亿美元。目前,可用的抗真菌药物种类很少,而且耐药性正在增长。生物膜形成所需基因的鉴定对新型抗真菌药物的开发至关重要。这篇综述详细介绍了如何识别、验证和表征白色念珠菌中有缺陷的生物膜形成突变体。这包括如何进行体外生物膜形成实验,如何使用改良的CRISPR-Cas9系统创建干净的缺失,如何检测以识别缺陷的潜在原因,以及如何创建互补菌株以确认突变缺陷。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
How to Use a Mutant Library to Identify Genes Required for Biofilm Formation in the Pathogenic Fungus Candida albicans.
With over 1 billion infections and the causative agents showing critical diseases such as pancreatic cancer, the study of pathogenic fungi has never been more critical. In 2017, the United States spent $7.2 billion on fungal diseases. $4.5 billion was allocated to 75,055 hospitalizations, while $2.6 billion went to 8,993,230 outpatient visits. For Candida infections specifically, the cost was $1.4 billion. Currently, there are few classes of antifungals available, and resistance is growing. The identification of genes required for biofilm formation is essential for new antifungal development. This review details how to identify, verify, and characterize defective biofilm formation mutants in C. albicans. This includes how to run an in vitro biofilm formation assay, how to create clean deletions using the modified CRISPR-Cas9 system, how to assay to identify the potential causes of the defect, and how to create complementation strains to confirm the mutant defect.
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