1,4-dihydroxy quininib activates ferroptosis pathways in metastatic uveal melanoma and reveals a novel prognostic biomarker signature

Tonelotto, Valentina; Costa-Garcia, Marcel; O’Reilly, Eve; Smith, Kaelin Francis; Slater, Kayleigh; Dillon, Eugene T.; Pendino, Marzia; Higgins, Catherine; Sist, Paola; Bosch, Rosa; Passamonti, Sabina; Piulats, Josep M.; Villanueva, Alberto; Tramer, Federica; Vanella, Luca; Carey, Michelle; Kennedy, Breandán N.

doi:10.1038/s41420-023-01773-8

Cell Death Discov.

2024

DOI: 10.1038/s41420-023-01773-8

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1,4-dihydroxy quininib activates ferroptosis pathways in metastatic uveal melanoma and reveals a novel prognostic biomarker signature

Valentina Tonelotto,

Marcel Costa-Garcia,

Eve O’Reilly

et al.

Abstract: Uveal melanoma (UM) is an ocular cancer, with propensity for lethal liver metastases. When metastatic UM (MUM) occurs, as few as 8% of patients survive beyond two years. Efficacious treatments for MUM are urgently needed. 1,4-dihydroxy quininib, a cysteinyl leukotriene receptor 1 (CysLT1) antagonist, alters UM cancer hallmarks in vitro, ex vivo and in vivo. Here, we investigated the 1,4-dihydroxy quininib mechanism of action and its translational potential in MUM. Proteomic profiling of OMM2.5 cells identified… Show more

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Cited by 4 publications

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Standardized lab-scale production of the recombinant fusion protein HUG for the nanoscale analysis of bilirubin

Sist,

Saeed,

Tramer

et al. 2024

MethodsX

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Standardized lab-scale production of the recombinant fusion protein HUG for the nanoscale analysis of bilirubin

Sist,

Saeed,

Tramer

et al. 2024

MethodsX

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Intracellular biliverdin dynamics during ferroptosis

Nakajima,

Nishizawa,

Chen

et al. 2024

The Journal of Biochemistry

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Ferroptosis is a cell death mechanism mediated by iron-dependent lipid peroxidation. Although ferroptosis has garnered attention as a cancer-suppressing mechanism, there are still limited markers available for identifying ferroptotic cells or assessing their sensitivity to ferroptosis. The study focused on biliverdin, an endogenous reducing substance in cells, and examined the dynamics of intracellular biliverdin during ferroptosis using a biliverdin-binding cyanobacteriochrome. It was found that intracellular biliverdin decreases during ferroptosis and that this decrease is specific to ferroptosis among different forms of cell death. Furthermore, the feasibility of predicting sensitivity to ferroptosis by measuring intracellular biliverdin was demonstrated using a ferroptosis model induced by the re-expression of the transcription factor BACH1. These findings provide further insight into ferroptosis research and are expected to contribute to the development of cancer therapies that exploit ferroptosis.

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The role of signaling pathways mediated by the GPCRs CysLTR1/2 in melanocyte proliferation and senescence

Huber,

Horioka-Duplix,

Chen

et al. 2024

Sci. Signal.

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In contrast with sun exposure–induced melanoma, rarer melanocytic tumors and neoplasms with low mutational burden present opportunities to study isolated signaling mechanisms. These include uveal melanoma and blue nevi, which are often driven by mutations within the G protein–coupled signaling cascade downstream of cysteinyl leukotriene receptor 2. Here, we review how the same mutations within this pathway drive the growth of melanocytes in one tissue but can inhibit the growth of those in another, exemplifying the role of the tissue environment in the delicate balance between uncontrolled cell growth and senescence.

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1,4-dihydroxy quininib activates ferroptosis pathways in metastatic uveal melanoma and reveals a novel prognostic biomarker signature

Cited by 4 publications

References 101 publications

Standardized lab-scale production of the recombinant fusion protein HUG for the nanoscale analysis of bilirubin

Standardized lab-scale production of the recombinant fusion protein HUG for the nanoscale analysis of bilirubin

Intracellular biliverdin dynamics during ferroptosis

The role of signaling pathways mediated by the GPCRs CysLTR1/2 in melanocyte proliferation and senescence

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