Publication date: 20 March 2018
Source:Cell Reports, Volume 22, Issue 12
Author(s): Xu Zheng, Ali Beyzavi, Joanna Krakowiak, Nikit Patel, Ahmad S. Khalil, David Pincus
Clonal populations of cells exhibit cell-to-cell variation in the transcription of individual genes. In addition to this noise in gene expression, heterogeneity in the proteome and the proteostasis network expands the phenotypic diversity of a population. Heat shock factor 1 (Hsf1) regulates chaperone gene expression, thereby coupling transcriptional noise to proteostasis. Here we show that cell-to-cell variation in Hsf1 activity is an important determinant of phenotypic plasticity. Budding yeast cells with high Hsf1 activity were enriched for the ability to acquire resistance to an antifungal drug, and this enrichment depended on Hsp90, a known phenotypic capacitor and canonical Hsf1 target. We show that Hsf1 phosphorylation promotes cell-to-cell variation, and this variation, rather than absolute Hsf1 activity, promotes antifungal resistance. We propose that Hsf1 phosphorylation enables differential tuning of the proteostasis network in individual cells, allowing populations to access a range of phenotypic states.
Graphical abstract
Teaser
Zheng et al. reveal that the master transcriptional regulator of proteostasis, Hsf1, generates cell-to-cell variation in the expression of Hsp90 and other chaperones. This variation is driven by differential Hsf1 phosphorylation and results in the ability of yeast cells to acquire antifungal resistance, a hallmark of phenotypic plasticity.http://ift.tt/2uct3c8
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