多细胞生物
生物
金念珠菌
表型
胞质分裂
微生物学
酵母
基因
细胞生物学
萌芽
细胞
遗传学
细胞分裂
抗真菌
作者
Jian Bing,Zhangyue Guan,Tianhong Zheng,Craig L. Ennis,Clarissa J. Nobile,Changbin Chen,Haiqing Chu,Guanghua Huang
标识
DOI:10.1038/s41467-024-46786-8
摘要
Abstract Candida auris has become a serious threat to public health. The mechanisms of how this fungal pathogen adapts to the mammalian host are poorly understood. Here we report the rapid evolution of an adaptive C. auris multicellular aggregative morphology in the murine host during systemic infection. C. auris aggregative cells accumulate in the brain and exhibit obvious advantages over the single-celled yeast-form cells during systemic infection. Genetic mutations, specifically de novo point mutations in genes associated with cell division or budding processes, underlie the rapid evolution of this aggregative phenotype. Most mutated C. auris genes are associated with the regulation of cell wall integrity, cytokinesis, cytoskeletal properties, and cellular polarization. Moreover, the multicellular aggregates are notably more recalcitrant to the host antimicrobial peptides LL-37 and PACAP relative to the single-celled yeast-form cells. Overall, to survive in the host, C. auris can rapidly evolve a multicellular aggregative morphology via genetic mutations.
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