Proline catabolism is a key factor facilitating Candida albicans pathogenicity

Autor:in

Silao, Fitz Gerald; Jiang, Tonglei; Bereczky-Veress, Biborka; Kuhbacher, A.; Ryman, Kicki; Uwamohoro, Nathalie; Jenull, Sabrina; Nogueira, Filomena; Ward, Meliza; Lion, Thomas; Urban, Constantin; Rupp, Steffen; kuchler, karl; Chen, Chang-Bin; Peuckert, Christiane; Ljungdahl, Per

Abstrakt

Candida albicans is listed as one of four "critical priority" fungal pathogens by the World Health Organization (WHO). Intriguingly, C. albicans is a natural commensal organism thriving in symbiosis with other components of the human microflora. Given the opportunistic character of C. albicans, it is important to understand how nutrient availability within host microenvironments contribute to the transition from commensal to pathogenic growth. Here, we report that proline is catabolized by C. albicans as an important energy source, a characteristic that is conserved among other pathogenic Candida species, including the multidrug resistant C. glabrata and C. auris. Using different infection models and applying a state-of-the-art intravital imaging technique to visualize C. albicans cells infecting kidneys in a living mouse, we observed that strains unable to utilize proline exhibit significantly reduced virulence and filamentous hyphal growth. Genetic dissection of the Proline UTilization (PUT) pathway and deciphering the control mechanisms governing proline use led to the discovery that proline is toxic to cells unable to catabolize this amino acid. Our findings provide novel insights implicating proline metabolism as a key determinant of pathogenic fungal growth.

Dokumententyp

Originalarbeit

Open Access Type

Gold

DOI

10.1371/journal.ppat.1011677

PubMed ID

MEDLINE:37917600