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Non-Toxic and Ultra-Small Biosilver Nanoclusters Trigger Apoptotic Cell Death in Fluconazole-Resistant Candida albicans via Ras Signaling

Version 2 2024-03-12, 18:07
Version 1 2023-10-19, 15:45
journal contribution
posted on 2024-03-12, 18:07 authored by Prateeksha, Braj Singh, Hesham El Enshasy, Essam Sholkamy, Ashraf Mostafa, Abd Hesham, Brahma Singh, Vijai Gupta, Farah Deeba, Rajesh Bajpai, Vivek Pandey, Alim Naqvi, Dalip Upreti, Nicholas Gathergood, Yueming Jiang
<p>Silver-based nanostructures are suitable for many biomedical applications, but to be useful therapeutic agents, the high toxicity of these nanomaterials must be eliminated. Here, we biosynthesize nontoxic and ultra-small silver nanoclusters (rsAg@NCs) using metabolites of usnioid lichen (a symbiotic association of algae and fungi) that exhibit excellent antimicrobial activity against fluconazole (FCZ)-resistant Candida albicans that is many times higher than chemically synthesized silver nanoparticles (AgNPs) and FCZ. The rsAg@NCs trigger apoptosis via reactive oxygen species accumulation that leads to the loss of mitochondrial membrane potential, DNA fragmentation, chromosomal condensation, and the activation of metacaspases. The proteomic analysis clearly demonstrates that rsAg@NCs exposure significantly alters protein expression. Most remarkable among the down-regulated proteins are those related to glycolysis, metabolism, free radical scavenging, anti-apoptosis, and mitochondrial function. In contrast, proteins involved in plasma membrane function, oxidative stress, cell death, and apoptosis were upregulated. Eventually, we also established that the apoptosis-inducing potential of rsAg@NCs is due to the activation of Ras signaling, which confirms their application in combating FCZ-resistant C. albicans infections.</p>

History

School affiliated with

  • School of Chemistry (Research Outputs)

Publication Title

Biomolecules

Volume

9

Issue

2

Pages/Article Number

47

Publisher

MDPI

ISSN

2218-273X

Date Submitted

2019-11-04

Date Accepted

2019-01-23

Date of First Publication

2019-01-29

Date of Final Publication

2019-01-29

ePrints ID

38698

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