SGD Paper Help



Lopez-Garcia B, et al.  (2010) A genomic approach highlights common and diverse effects and determinants of susceptibility on the yeast Saccharomyces cerevisiae exposed to distinct antimicrobial peptides. BMC Microbiol 10():289

Abstract: ABSTRACT: BACKGROUND: The mechanism of action of antimicrobial peptides (AMP) was initially correlated with peptide membrane permeation properties. However, recent evidences indicate that action of a number of AMP is more complex and involves specific interactions at cell envelopes or with intracellular targets. In this study, a genomic approach was undertaken on the model yeast Saccharomyces cerevisiae to characterize the antifungal effect of two unrelated AMP. RESULTS: Two differentiated peptides were used: the synthetic cell-penetrating PAF26 and the natural cytolytic melittin. Transcriptomic analyses demonstrated distinctive gene expression changes for each peptide. Quantitative RT-PCR confirmed differential expression of selected genes. Gene onthology (GO) annotation of differential gene lists showed that the unique significant terms shared by treatment with both peptides were related to the cell wall (CW). Assays with mutants lacking CW related genes including those of MAPK signaling pathways revealed genes having influence on sensitivity to peptides. Fluorescence microscopy and flow cytometry demonstrated PAF26 interaction with cells and internalization that correlated with cell killing in sensitive CW-defective mutants such as [increment]ecm33 or [increment]ssd1. GO annotation also showed differential responses between peptides, which included ribosomal biogenesis, ARG genes from the metabolism of amino groups (specifically induced by PAF26), or the reaction to unfolded protein stress. Susceptibility of deletion mutants confirmed the involvement of these processes. Specifically, mutants lacking ARG genes from the metabolism of arginine pathway were markedly more resistant to PAF26 and had a functional CW. In the deletant in the arginosuccinate synthetase (ARG1) gene, PAF26 interaction occurred normally, thus uncoupling peptide interaction from cell killing. The previously described involvement of the glycosphingolipid gene IPT1 was extended to the peptides studied here. CONCLUSIONS: Reinforcement of CW is a general response common after exposure to distinct AMP, and likely contributes to shield cells from peptide interaction. However, a weakened CW is not necessarily indicative of a higher sensitivity to AMP. Additional processes modulate susceptibility to specific peptides, exemplified in the involvement of the metabolism of amino groups in the case of PAF26. The relevance of the response to unfolded protein stress or the sphingolipid biosynthesis, previously reported for other unrelated AMP, was also independently confirmed.

Status: Published Type: Journal Article PubMed ID: 21078184

Topics addressed in this paper

Number of different genes curated to this paper: 56

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Topics Topics not linked to Genes Genes linked to topics (#1 - 10 )
ALB1 ARG1 ARG2 ARG3 ARG4 ARG5,6 ARG7 BTN2 CAR1 CGR1
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Topics Genes linked to topics (#11 - 20 )
CIS3 CUP1-1 CUP1-2 DBP2 DSE2 ECM33 FKS1 GUF1 HOG1 HOT1
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Topics Genes linked to topics (#21 - 30 )
HSC82 HSP150 IPT1 MCR1 MID2 MLP1 MSN2 NOP1 NOP16 NTH1
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Topics Genes linked to topics (#31 - 40 )
PBS2 PIR1 PIR3 PLB1 PSO2 PTC3 RHO1 RLM1 RPL14A RPL1A
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Topics Genes linked to topics (#41 - 50 )
SED1 SLT2 SSD1 SSK1 SSK2 STE11 STE5 STE7 TOS1 UTP23
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Topics Genes linked to topics (#51 - 56 )
YAP1 YHC3 YLR162W YNL190W YPD1 YPQ1
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