Proteomics

Dataset Information

0

Quantitative proteomics of HT-1080 cells exposed to single-atom engineered graphene derivatives versus copper ionophore elesclomol and glutathione peroxidase 4 inhibitor RSL3


ABSTRACT: This dataset presents a comparative proteomic analysis of the human fibrosarcoma cell line HT-1080 in response to treatment with nitrogen-doped graphene acid (NGA) and the single atom engineered derivatives, NGA-Fe3+ and NGA-Cu2+. To further investigate the role of metal-induced cell death pathways, cells were exposed to elesclomol, a well-known copper ionophore, and RSL3, a ferroptosis activating compound. The main objective was to characterize the proteomic alterations associated with single atom engineered NGA to elucidate potential mechanisms of action. We also examined the effects of elesclomol and RSL3 to provide reference datasets for copper-induced cytotoxicity (aka cuproptosis) and ferroptosis, respectively. This dataset provides insights into the cellular responses triggered by NGA and its derivatives and how these materials impinge on regulated cell death pathways.

INSTRUMENT(S):

ORGANISM(S): Homo Sapiens (human)

TISSUE(S): Ht-1080 Cell

SUBMITTER: Massimiliano Gaetani  

LAB HEAD: Massimiliano Gaetani

PROVIDER: PXD067483 | Pride | 2026-02-02

REPOSITORIES: Pride

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Publications

Copper ionophore elicits calpain-dependent paraptosis coincident with proteotoxic stress.

Sae-Fung Apiwit A   Fadeel Bengt B  

Cell communication and signaling : CCS 20251212 1


Copper is essential to all living organisms. However, too much copper is deleterious, and cellular copper content is therefore subject to tight control. Excess copper was recently found to perturb a set of metabolic enzymes in mitochondria, leading to the aggregation of these proteins and the demise of the cell. However, our understanding of the mechanism of copper-dependent cell death remains incomplete. Here, we report that copper ionophore (elesclomol)-induced cell death is calpain-dependent,  ...[more]

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