Does inter-organellar proteostasis impact yeast quality and performance during beer fermentation?
| Autor(a) principal: | |
|---|---|
| Data de Publicação: | 2020 |
| Outros Autores: | , |
| Tipo de documento: | Artigo |
| Idioma: | eng |
| Título da fonte: | Repositório Institucional da UFRGS |
| Texto Completo: | http://hdl.handle.net/10183/274310 |
Resumo: | During beer production, yeast generate ethanol that is exported to the extracellular environment where it accumulates. Depending on the initial carbohydrate concentration in the wort, the amount of yeast biomass inoculated, the fermentation temperature, and the yeast attenuation capacity, a high concentration of ethanol can be achieved in beer. The increase in ethanol concentration as a consequence of the fermentation of high gravity (HG) or very high gravity (VHG) worts promotes deleterious pleiotropic effects on the yeast cells. Moderate concentrations of ethanol (5% v/v) change the enzymatic kinetics of proteins and affect biological processes, such as the cell cycle and metabolism, impacting the reuse of yeast for subsequent fermentation. However, high concentrations of ethanol (> 5% v/v) dramatically alter protein structure, leading to unfolded proteins as well as amorphous protein aggregates. It is noteworthy that the effects of elevated ethanol concentrations generated during beer fermentation resemble those of heat shock stress, with similar responses observed in both situations, such as the activation of proteostasis and protein quality control mechanisms in different cell compartments, including endoplasmic reticulum (ER), mitochondria, and cytosol. Despite the extensive published molecular and biochemical data regarding the roles of proteostasis in different organelles of yeast cells, little is known about how this mechanism impacts beer fermentation and how different proteostasis mechanisms found in ER, mitochondria, and cytosol communicate with each other during ethanol/fermentative stress. Supporting this integrative view, transcriptome data analysis was applied using publicly available information for a lager yeast strain grown under beer production conditions. The transcriptome data indicated upregulation of genes that encode chaperones, co chaperones, unfolded protein response elements in ER and mitochondria, ubiquitin ligases, proteasome components, N-glycosylation quality control pathway proteins, and components of processing bodies (p-bodies) and stress granules (SGs) during lager beer fermentation. Thus, the main purpose of this hypothesis and theory manuscript is to provide a concise picture of how inter-organellar proteostasis mechanisms are connected with one another and with biological processes that may modulate the viability and/or vitality of yeast populations during HG/VHG beer fermentation and serial repitching. |
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Telini, Bianca de PaulaMenoncin, MarceloBonatto, Diego2024-03-28T06:23:32Z20201664-8021http://hdl.handle.net/10183/274310001172059During beer production, yeast generate ethanol that is exported to the extracellular environment where it accumulates. Depending on the initial carbohydrate concentration in the wort, the amount of yeast biomass inoculated, the fermentation temperature, and the yeast attenuation capacity, a high concentration of ethanol can be achieved in beer. The increase in ethanol concentration as a consequence of the fermentation of high gravity (HG) or very high gravity (VHG) worts promotes deleterious pleiotropic effects on the yeast cells. Moderate concentrations of ethanol (5% v/v) change the enzymatic kinetics of proteins and affect biological processes, such as the cell cycle and metabolism, impacting the reuse of yeast for subsequent fermentation. However, high concentrations of ethanol (> 5% v/v) dramatically alter protein structure, leading to unfolded proteins as well as amorphous protein aggregates. It is noteworthy that the effects of elevated ethanol concentrations generated during beer fermentation resemble those of heat shock stress, with similar responses observed in both situations, such as the activation of proteostasis and protein quality control mechanisms in different cell compartments, including endoplasmic reticulum (ER), mitochondria, and cytosol. Despite the extensive published molecular and biochemical data regarding the roles of proteostasis in different organelles of yeast cells, little is known about how this mechanism impacts beer fermentation and how different proteostasis mechanisms found in ER, mitochondria, and cytosol communicate with each other during ethanol/fermentative stress. Supporting this integrative view, transcriptome data analysis was applied using publicly available information for a lager yeast strain grown under beer production conditions. The transcriptome data indicated upregulation of genes that encode chaperones, co chaperones, unfolded protein response elements in ER and mitochondria, ubiquitin ligases, proteasome components, N-glycosylation quality control pathway proteins, and components of processing bodies (p-bodies) and stress granules (SGs) during lager beer fermentation. Thus, the main purpose of this hypothesis and theory manuscript is to provide a concise picture of how inter-organellar proteostasis mechanisms are connected with one another and with biological processes that may modulate the viability and/or vitality of yeast populations during HG/VHG beer fermentation and serial repitching.application/pdfengFrontiers in Genetics. Lausanne. Vol. 11 (Jan. 2020), e2, 15 p.ProteostaseLevedura cervejeiraTranscriptomaEthanol stressBeer fermentationInter-organellar communicationDoes inter-organellar proteostasis impact yeast quality and performance during beer fermentation?Estrangeiroinfo:eu-repo/semantics/articleinfo:eu-repo/semantics/publishedVersioninfo:eu-repo/semantics/openAccessreponame:Repositório Institucional da UFRGSinstname:Universidade Federal do Rio Grande do Sul (UFRGS)instacron:UFRGSTEXT001172059.pdf.txt001172059.pdf.txtExtracted Texttext/plain84782http://www.lume.ufrgs.br/bitstream/10183/274310/2/001172059.pdf.txta3ebd0b40f8266f471ade221eec72658MD52ORIGINAL001172059.pdfTexto completo (inglês)application/pdf2668804http://www.lume.ufrgs.br/bitstream/10183/274310/1/001172059.pdfa519d60c3463e93a1ba795dba70f0be5MD5110183/2743102024-03-29 06:17:20.273238oai:www.lume.ufrgs.br:10183/274310Repositório de PublicaçõesPUBhttps://lume.ufrgs.br/oai/requestopendoar:2024-03-29T09:17:20Repositório Institucional da UFRGS - Universidade Federal do Rio Grande do Sul (UFRGS)false |
| dc.title.pt_BR.fl_str_mv |
Does inter-organellar proteostasis impact yeast quality and performance during beer fermentation? |
| title |
Does inter-organellar proteostasis impact yeast quality and performance during beer fermentation? |
| spellingShingle |
Does inter-organellar proteostasis impact yeast quality and performance during beer fermentation? Telini, Bianca de Paula Proteostase Levedura cervejeira Transcriptoma Ethanol stress Beer fermentation Inter-organellar communication |
| title_short |
Does inter-organellar proteostasis impact yeast quality and performance during beer fermentation? |
| title_full |
Does inter-organellar proteostasis impact yeast quality and performance during beer fermentation? |
| title_fullStr |
Does inter-organellar proteostasis impact yeast quality and performance during beer fermentation? |
| title_full_unstemmed |
Does inter-organellar proteostasis impact yeast quality and performance during beer fermentation? |
| title_sort |
Does inter-organellar proteostasis impact yeast quality and performance during beer fermentation? |
| author |
Telini, Bianca de Paula |
| author_facet |
Telini, Bianca de Paula Menoncin, Marcelo Bonatto, Diego |
| author_role |
author |
| author2 |
Menoncin, Marcelo Bonatto, Diego |
| author2_role |
author author |
| dc.contributor.author.fl_str_mv |
Telini, Bianca de Paula Menoncin, Marcelo Bonatto, Diego |
| dc.subject.por.fl_str_mv |
Proteostase Levedura cervejeira Transcriptoma |
| topic |
Proteostase Levedura cervejeira Transcriptoma Ethanol stress Beer fermentation Inter-organellar communication |
| dc.subject.eng.fl_str_mv |
Ethanol stress Beer fermentation Inter-organellar communication |
| description |
During beer production, yeast generate ethanol that is exported to the extracellular environment where it accumulates. Depending on the initial carbohydrate concentration in the wort, the amount of yeast biomass inoculated, the fermentation temperature, and the yeast attenuation capacity, a high concentration of ethanol can be achieved in beer. The increase in ethanol concentration as a consequence of the fermentation of high gravity (HG) or very high gravity (VHG) worts promotes deleterious pleiotropic effects on the yeast cells. Moderate concentrations of ethanol (5% v/v) change the enzymatic kinetics of proteins and affect biological processes, such as the cell cycle and metabolism, impacting the reuse of yeast for subsequent fermentation. However, high concentrations of ethanol (> 5% v/v) dramatically alter protein structure, leading to unfolded proteins as well as amorphous protein aggregates. It is noteworthy that the effects of elevated ethanol concentrations generated during beer fermentation resemble those of heat shock stress, with similar responses observed in both situations, such as the activation of proteostasis and protein quality control mechanisms in different cell compartments, including endoplasmic reticulum (ER), mitochondria, and cytosol. Despite the extensive published molecular and biochemical data regarding the roles of proteostasis in different organelles of yeast cells, little is known about how this mechanism impacts beer fermentation and how different proteostasis mechanisms found in ER, mitochondria, and cytosol communicate with each other during ethanol/fermentative stress. Supporting this integrative view, transcriptome data analysis was applied using publicly available information for a lager yeast strain grown under beer production conditions. The transcriptome data indicated upregulation of genes that encode chaperones, co chaperones, unfolded protein response elements in ER and mitochondria, ubiquitin ligases, proteasome components, N-glycosylation quality control pathway proteins, and components of processing bodies (p-bodies) and stress granules (SGs) during lager beer fermentation. Thus, the main purpose of this hypothesis and theory manuscript is to provide a concise picture of how inter-organellar proteostasis mechanisms are connected with one another and with biological processes that may modulate the viability and/or vitality of yeast populations during HG/VHG beer fermentation and serial repitching. |
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2020 |
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2020 |
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2024-03-28T06:23:32Z |
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Frontiers in Genetics. Lausanne. Vol. 11 (Jan. 2020), e2, 15 p. |
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