Differential Phosphorylation Provides a Switch to Control How α-Arrestin Rod1 Down-regulates Mating Pheromone Response in <i>Saccharomyces cerevisiae</i>

Alvaro, Christopher G.; Aindow, Ann; Thorner, Jeremy

doi:10.1534/genetics.115.186122

Cited by 38 publications

(54 citation statements)

References 104 publications

(170 reference statements)

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“…Several examples have been reported in the literature, such as the nitrogen-dependent regulation of Ldb19 (Art1) by the TOR-dependent Npr1 protein kinase and the carbon source-dependent regulation of Rod1 (Art4) by the Snf1 kinase (12,16,19). This latter case was shown to be involved in the regulation of the Jen1 lactate transporter, the Ste2 pheromone receptor, and the Hxt1 and Hxt3 hexose permeases (15)(16)(17).…”

Section: Discussionmentioning

confidence: 99%

Regulation of the Yeast Hxt6 Hexose Transporter by the Rod1 α-Arrestin, the Snf1 Protein Kinase, and the Bmh2 14-3-3 Protein

Llopis-Torregrosa

Ferri-Blázquez

Adam‐Artigues

et al. 2016

Journal of Biological Chemistry

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Cell viability requires adaptation to changing environmental conditions. Ubiquitin-mediated endocytosis plays a crucial role in this process, because it provides a mechanism to remove transport proteins from the membrane. Arrestin-related trafficking proteins are important regulators of the endocytic pathway in yeast, facilitating selective ubiquitylation of target proteins by the E3 ubiquitin ligase, Rsp5. Specifically, Rod1 (Art4) has been reported to regulate the endocytosis of both the Hxt1, Hxt3, and Hxt6 glucose transporters and the Jen1 lactate transporter. Also, the AMP kinase homologue, Snf1, and 14-3-3 proteins have been shown to regulate Jen1 via Rod1. Here, we further characterized the role of Rod1, Snf1, and 14-3-3 in the signal transduction route involved in the endocytic regulation of the Hxt6 high affinity glucose transporter by showing that Snf1 interacts specifically with Rod1 and Rog3 (Art7), that the interaction between the Bmh2 and several arrestin-related trafficking proteins may be modulated by carbon source, and that both the 14-3-3 protein Bmh2 and the Snf1 regulatory domain interact with the arrestin-like domain containing the N-terminal half of Rod1 (amino acids 1-395). Finally, using both co-immunoprecipitation and bimolecular fluorescence complementation, we demonstrated the interaction of Rod1 with Hxt6 and showed that the localization of the Rod1-Hxt6 complex at the plasma membrane is affected by carbon source and is reduced upon overexpression of SNF1 and BMH2.An important component of the maintenance of cellular homeostasis and stress responses is the regulation of the composition of plasma membrane proteins responsible for the uptake and extrusion of nutrients and other nonpermeable small molecules. The general mechanisms controlling this regulatory process are highly conserved among eukaryotic organisms and involve both transcriptional regulation and modulation of the balance of secretion, recycling, and degradation of individual transporter proteins in response to changes in the extracellular environment (reviewed in Ref. 1). Regulated endocytosis, one important step in this process, has been well studied in both mammals and yeast, unveiling many mechanistic similarities that establish yeast as a relevant model system.In Saccharomyces cerevisiae, plasma membrane transporters that need to be down-regulated are ubiquitylated by the Rsp5 E3 ubiquitin ligase, endocytosed, sorted into multivesicular bodies in a process requiring the ESCRT machinery, and finally are delivered to the vacuole for degradation (2-5). Transporter ubiquitylation by the HECT family Rsp5 E3 ubiquitin ligase is mediated by one or more of several adaptor proteins that confer specificity and ensure the correct regulation of targeted proteins in response to changes in the extracellular environment (reviewed in Refs. 6). At least 18 Rsp5 adaptor proteins have been described, each having specificity for a subset of transport proteins and acting in response to specific stimuli.The molecular mechanisms governing th...

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Section: Discussionmentioning

confidence: 99%

Regulation of the Yeast Hxt6 Hexose Transporter by the Rod1 α-Arrestin, the Snf1 Protein Kinase, and the Bmh2 14-3-3 Protein

Llopis-Torregrosa

Ferri-Blázquez

Adam‐Artigues

et al. 2016

Journal of Biological Chemistry

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“…Glucose-induced inactivation of Jen1 requires the ␣-arrestin, Rod1/Art4. Activity of Rod1 is regulated by the phosphorylation state, which is modulated by Snf1 kinase and type 1 protein phosphatase (Glc7-Reg1) (14,15). In the absence of glucose, Rod1 is phosphorylated by Snf1 kinase, which facilitates binding to the 14-3-3 proteins (Bmh1/2) to inhibit its interaction with Jen1 (14).…”

mentioning

confidence: 99%

The C-terminal region of the yeast monocarboxylate transporter Jen1 acts as a glucose signal–responding degron recognized by the α-arrestin Rod1

Fujita

Sato

Kasai

et al. 2018

Journal of Biological Chemistry

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In response to changes in nutrient conditions, cells rearrange the composition of plasma membrane (PM) transporters to optimize their metabolic flux. Not only transcriptional gene regulation, but also inactivation of specific transporters is important for fast rearrangement of the PM. In eukaryotic cells, endocytosis plays a role in transporter inactivation, which is triggered by ubiquitination of these transporters. The Nedd4 family E3 ubiquitin ligase is responsible for ubiquitination of the PM transporters and requires that a series of α-arrestin proteins are targeted to these transporters. The mechanism by which an α-arrestin recognizes its cognate transporters in response to environmental signals is of intense scientific interest. Excess substrates or signal transduction pathways are known to initiate recognition of transporters by α-arrestins. Here, we identified an endocytic-sorting signal in the monocarboxylate transporter Jen1 from yeast (), whose endocytic degradation depends on the Snf1-glucose signaling pathway. We found that the C-terminal 20-amino acid-long region of Jen1 contains an amino acid sequence required for association of Jen1 to the α-arrestin Rod1, as well as lysine residues important for glucose-induced Jen1 ubiquitination. Notably, fusion of this region to the methionine permease, Mup1, whose endocytosis is normally induced by excess methionine, was sufficient for Mup1 to undergo glucose-induced, Rod1-mediated endocytosis. Taken together, our results demonstrate that the Jen1 C-terminal region acts as a glucose-responding degron for α-arrestin-mediated endocytic degradation of Jen1.

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“…Deletion of YPK1 led to the lowest transformation efficiencies out of all mutant strains we tested in this study. However, further work is needed to clarify the exact role of Ypk1 in DNA uptake because Ypk1 also regulates at least one α‐arrestin (Alvaro, Aindow, & Thorner, ), it impinges on actin dynamics (Niles & Powers, ), and it is involved in the heat stress response (Sun et al., ). The hypotheses that eisosomes mark sites of endocytosis and that transformation is facilitated by endocytosis have one point in common: In both cases, these types of endocytosis differ from well‐studied endocytic pathways, such as clathrin‐mediated endocytosis that originates at actin patches (Kawai et al., ; Ziółkowska, Christiano, & Walther, ).…”

Section: Discussionmentioning

confidence: 99%

Yeast transformation efficiency is enhanced by TORC1‐ and eisosome‐dependent signaling

Kuemmel

Skoufou-Papoutsaki

et al. 2018

MicrobiologyOpen

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Transformation of baker's yeast ( Saccharomyces cerevisiae ) plays a key role in several experimental techniques, yet the molecular mechanisms underpinning transformation are still unclear. The addition of amino acids to the growth and transformation medium increases transformation efficiency. Here, we show that target of rapamycin complex 1 ( TORC 1) activated by amino acids enhances transformation via ubiquitin‐mediated endocytosis. We created mutants of the TORC 1 pathway, alpha‐arrestins, and eisosome‐related genes. Our results demonstrate that the TORC 1‐Npr1‐Art1/Rsp5 pathway regulates yeast transformation. Based on our previous study, activation of this pathway results in up to a 200‐fold increase in transformation efficiency, or greater. Additionally, we suggest DNA may be taken up by domains at the membrane compartment of Can1 ( MCC ) in the plasma membrane formed by eisosomes. Yeast studies on transformation could be used as a platform to understand the mechanism of DNA uptake in mammalian systems, which is clinically relevant to optimize gene therapy.

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Differential Phosphorylation Provides a Switch to Control How α-Arrestin Rod1 Down-regulates Mating Pheromone Response in Saccharomyces cerevisiae

Cited by 38 publications

References 104 publications

Regulation of the Yeast Hxt6 Hexose Transporter by the Rod1 α-Arrestin, the Snf1 Protein Kinase, and the Bmh2 14-3-3 Protein

Regulation of the Yeast Hxt6 Hexose Transporter by the Rod1 α-Arrestin, the Snf1 Protein Kinase, and the Bmh2 14-3-3 Protein

The C-terminal region of the yeast monocarboxylate transporter Jen1 acts as a glucose signal–responding degron recognized by the α-arrestin Rod1

Yeast transformation efficiency is enhanced by TORC1‐ and eisosome‐dependent signaling

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