Abstract
The fungal pathogen Cryptococcus neoformans relies on post-transcriptional mechanisms of gene regulation to adapt to stressors it encounters in the human host, such as oxidative stress and nutrient limitation. The kinase Gcn2 regulates translation in response to stress by phosphorylating the initiation factor eIF2, and it is a crucial factor in withstanding oxidative stress in C. neoformans, and amino acid limitation in many fungal species. However, little is known about the role of Gcn2 in nitrogen limitation in C. neoformans. In this study, we demonstrate that Gcn2 is required for C. neoformans to utilize methionine as a source of nitrogen, and that the presence of methionine as a sole nitrogen source induces eIF2 phosphorylation. The stress imposed by methionine leads to an oxidative stress response at both the levels of transcription and translation, as seen through polysome profiling as well as increased abundance of select oxidative stress response transcripts. The transcription factor Gcn4 is also required for methionine utilization and oxidative stress resistance, and RT-qPCR data suggests that it regulates expression of certain transcripts in response to oxidative stress. The results of this study suggest a connection between nitrogen metabolism and oxidative stress in C. neoformans that is mediated by Gcn4, possibly indicating the presence of a compound stress response in this clinically important fungal pathogen.
Highlights
Cryptococcus neoformans is a basidiomycetous fungus that is found ubiquitously in the environment and is an opportunistic pathogen in humans
We began by determining whether Gcn2 and eIF2 phosphorylation were required to regulate nitrogen metabolism in C. neoformans
In order to adapt to the stressors, C. neoformans relies on post-transcriptional regulation of gene expression at the levels of both mRNA processing and translation (Bloom et al, 2017)
Summary
Cryptococcus neoformans is a basidiomycetous fungus that is found ubiquitously in the environment and is an opportunistic pathogen in humans. C. neoformans is a causative agent of cryptococcosis and is responsible for up to 250,000 deaths annually (Rajasingham et al, 2017). Immunocompromised individuals such as those living with HIV/AIDs and with organ transplants are susceptible. Advances have been made in antiretroviral therapy and other health interventions, C. neoformans infection is still prevalent in developing regions of the world with limited resources and access to healthcare. Growing resistance to current antifungal drugs highlights the need for the development of new therapeutics to treat cryptococcal infections (Smith et al, 2015; Rajasingham et al, 2017; Zafar et al, 2019).
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