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Transcriptomic response of yeast cells to ATX1 deletion under different copper levels.

Published version
Peer-reviewed

Type

Article

Change log

Authors

Cankorur-Cetinkaya, Ayca 
Eraslan, Serpil 
Kirdar, Betul 

Abstract

BACKGROUND: Iron and copper homeostatic pathways are tightly linked since copper is required as a cofactor for high affinity iron transport. Atx1p plays an important role in the intracellular copper transport as a copper chaperone transferring copper from the transporters to Ccc2p for its subsequent insertion into Fet3p, which is required for high affinity iron transport. RESULTS: In this study, genome-wide transcriptional landscape of ATX1 deletants grown in media either lacking copper or having excess copper was investigated. ATX1 deletants were allowed to recover full respiratory capacity in the presence of excess copper in growth environment. The present study revealed that iron ion homeostasis was not significantly affected by the absence of ATX1 either at the transcriptional or metabolic levels, suggesting other possible roles for Atx1p in addition to its function as a chaperone in copper-dependent iron absorption. The analysis of the transcriptomic response of atx1∆/atx1∆ and its integration with the genetic interaction network highlighted for the first time, the possible role of ATX1 in cell cycle regulation, likewise its mammalian counterpart ATOX1, which was reported to play an important role in the copper-stimulated proliferation of non-small lung cancer cells. CONCLUSIONS: The present finding revealed the dispensability of Atx1p for the transfer of copper ions to Ccc2p and highlighted its possible role in the cell cycle regulation. The results also showed the potential of Saccharomyces cerevisiae as a model organism in studying the capacity of ATOX1 as a therapeutic target for lung cancer therapy.

Description

Keywords

Cell cycle regulation, Copper chaperon, Copper homeostasis, Copper transport, Menkes disease, Wilson disease, Yeast, Carrier Proteins, Cluster Analysis, Copper, Epistasis, Genetic, Fungal Proteins, Gene Deletion, Gene Expression Profiling, Gene Expression Regulation, Fungal, Gene Regulatory Networks, Transcription, Genetic, Transcriptome

Journal Title

BMC Genomics

Conference Name

Journal ISSN

1471-2164
1471-2164

Volume Title

17

Publisher

Springer Science and Business Media LLC
Sponsorship
The authors greatly acknowledge the Turkish State Planning Organization DPT09K120520, Bogazici University Research Fund through Project No 5562 and TUBITAK through Project No 110 M692 for the financial support provided for this research.