Proteome response at the edge of protein aggregation

Natalia Sanchez De Groot; Ricardo A. Gomes; Anna Villar-Pique; M. Madan Babu; Ana Varela Coelho; Salvador Ventura

doi:10.1098/rsob.140221

Proteome response at the edge of protein aggregation

Natalia Sanchez De Groot, Ricardo A. Gomes, Anna Villar-Pique, M. Madan Babu, Ana Varela Coelho, Salvador Ventura

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©2015 The Authors. Published. Proteins adopt defined structures and are crucial to most cellular functions. Their misfolding and aggregation is associated with numerous degenerative human disorders such as type II diabetes, Huntington's or Alzheimer's diseases. Here, we aim to understand why cells promote the formation of protein foci. Comparison of two amyloid-β-peptide variants, mostly insoluble but differently recruited by the cell (inclusion body versus diffused), reveals small differences in cell fitness and proteome response. We suggest that the levels of oxidative stress act as a sensor to trigger protein recruitment into foci. Our data support a common cytoplasmic response being able to discern and react to the specific properties of polypeptides.

Idioma original	Anglès
Número d’article	140221
Revista	Open Biology
Volum	5
Número	2
DOIs	https://doi.org/10.1098/rsob.140221
Estat de la publicació	Publicada - 1 de gen. 2015

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10.1098/rsob.140221

https://ddd.uab.cat/record/185258

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title = "Proteome response at the edge of protein aggregation",

abstract = "{\textcopyright}2015 The Authors. Published. Proteins adopt defined structures and are crucial to most cellular functions. Their misfolding and aggregation is associated with numerous degenerative human disorders such as type II diabetes, Huntington's or Alzheimer's diseases. Here, we aim to understand why cells promote the formation of protein foci. Comparison of two amyloid-β-peptide variants, mostly insoluble but differently recruited by the cell (inclusion body versus diffused), reveals small differences in cell fitness and proteome response. We suggest that the levels of oxidative stress act as a sensor to trigger protein recruitment into foci. Our data support a common cytoplasmic response being able to discern and react to the specific properties of polypeptides.",

keywords = "Amyloid- B-peptide, Oxidative stress, Protein misfolding, Proteomic response",

author = "{De Groot}, {Natalia Sanchez} and Gomes, {Ricardo A.} and Anna Villar-Pique and Babu, {M. Madan} and Coelho, {Ana Varela} and Salvador Ventura",

year = "2015",

month = jan,

day = "1",

doi = "10.1098/rsob.140221",

language = "English",

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T1 - Proteome response at the edge of protein aggregation

AU - De Groot, Natalia Sanchez

AU - Gomes, Ricardo A.

AU - Villar-Pique, Anna

AU - Babu, M. Madan

AU - Coelho, Ana Varela

AU - Ventura, Salvador

PY - 2015/1/1

Y1 - 2015/1/1

N2 - ©2015 The Authors. Published. Proteins adopt defined structures and are crucial to most cellular functions. Their misfolding and aggregation is associated with numerous degenerative human disorders such as type II diabetes, Huntington's or Alzheimer's diseases. Here, we aim to understand why cells promote the formation of protein foci. Comparison of two amyloid-β-peptide variants, mostly insoluble but differently recruited by the cell (inclusion body versus diffused), reveals small differences in cell fitness and proteome response. We suggest that the levels of oxidative stress act as a sensor to trigger protein recruitment into foci. Our data support a common cytoplasmic response being able to discern and react to the specific properties of polypeptides.

AB - ©2015 The Authors. Published. Proteins adopt defined structures and are crucial to most cellular functions. Their misfolding and aggregation is associated with numerous degenerative human disorders such as type II diabetes, Huntington's or Alzheimer's diseases. Here, we aim to understand why cells promote the formation of protein foci. Comparison of two amyloid-β-peptide variants, mostly insoluble but differently recruited by the cell (inclusion body versus diffused), reveals small differences in cell fitness and proteome response. We suggest that the levels of oxidative stress act as a sensor to trigger protein recruitment into foci. Our data support a common cytoplasmic response being able to discern and react to the specific properties of polypeptides.

KW - Amyloid- B-peptide

KW - Oxidative stress

KW - Protein misfolding

KW - Proteomic response

U2 - 10.1098/rsob.140221

DO - 10.1098/rsob.140221

M3 - Article

SN - 2046-2441

VL - 5

JO - Open Biology

JF - Open Biology

IS - 2

M1 - 140221

ER -

Proteome response at the edge of protein aggregation

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