Targeting Ferroptosis As a Cell Death Pathway in Melanoma: From Molecular Mechanisms to Skin Cancer Treatment

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Targeting Ferroptosis As a Cell Death Pathway in Melanoma: From Molecular Mechanisms to Skin Cancer Treatment Publisher Pubmed

Manzari Tavakoli G^{1, 2} ; Mirzapour MH^{2, 3} ; Razi S^{2, 4, 5} ; Rezaei N^{5, 6, 7}

Show Affiliations

1. Department of Medicine, Tehran University of Medical Sciences (TUMS), Tehran, Iran
2. Cancer Immunology Project (CIP), Universal Scientific Education and Research Network (USERN), Tehran, Iran
3. School of Medicine, Isfahan University of Medical Sciences, Isfahan, Iran
4. School of Medicine, Iran University of Medical Sciences, Tehran, Iran
5. Research Center for Immunodeficiencies, Children's Medical Center, Tehran University of Medical Sciences, Tehran, Iran
6. Department of Immunology, School of Medicine, Tehran University of Medical Sciences, Tehran, Iran
7. Cancer Immunology Project (CIP), Universal Scientific Education and Research Network (USERN), Stockholm, Sweden

Source: International Immunopharmacology Published:2023

Abstract

Melanoma, the most aggressive form of human skin cancer, has been under investigation to reach the most efficient treatment. Surgical resection for early-diagnosed primary melanoma, targeted therapies, and immune checkpoint inhibitors for advanced/metastatic melanoma is the best clinical approach. Ferroptosis, a newly identified iron-dependent cell death pathway, which is morphologically and biochemically different from apoptosis and necrosis, has been reported to be involved in several cancers. Ferroptosis inducers could provide therapeutic options in case of resistance to conventional therapies for advanced/metastatic melanoma. Recently developed ferroptosis inducers, MEK and BRAF inhibitors, miRNAs such as miR-137 and miR-9, and novel strategies for targeting major histocompatibility complex (MHC) class II in melanoma can provide new opportunities for melanoma treatment. Combining ferroptosis inducers with targeted therapies or immune checkpoint inhibitors increases patient response rates. Here we review the mechanisms of ferroptosis and its environmental triggers. We also discuss the pathogenesis and current treatments of melanoma. Moreover, we aim to elucidate the relationship between ferroptosis and melanoma and ferroptosis implications to develop new therapeutic strategies against melanoma. © 2023 Elsevier B.V.

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Style	Citing Format
MLA	Manzari Tavakoli G, et al.. "Targeting Ferroptosis As a Cell Death Pathway in Melanoma: From Molecular Mechanisms to Skin Cancer Treatment." International Immunopharmacology, vol. 119, no. , 2023, pp. -.
APA	Manzari Tavakoli G, Mirzapour MH, Razi S, Rezaei N (2023). Targeting Ferroptosis As a Cell Death Pathway in Melanoma: From Molecular Mechanisms to Skin Cancer Treatment. International Immunopharmacology, 119(), -.
Chicago	Manzari Tavakoli G, Mirzapour MH, Razi S, Rezaei N. "Targeting Ferroptosis As a Cell Death Pathway in Melanoma: From Molecular Mechanisms to Skin Cancer Treatment." International Immunopharmacology 119, no. (2023): -.
Harvard	Manzari Tavakoli G et al. (2023) 'Targeting Ferroptosis As a Cell Death Pathway in Melanoma: From Molecular Mechanisms to Skin Cancer Treatment', International Immunopharmacology, 119(), pp. -.
Vancouver	Manzari Tavakoli G, Mirzapour MH, Razi S, Rezaei N. Targeting Ferroptosis As a Cell Death Pathway in Melanoma: From Molecular Mechanisms to Skin Cancer Treatment. International Immunopharmacology. 2023;119():-.
BibTex	@article{ author = {Manzari Tavakoli G and Mirzapour MH and Razi S and Rezaei N}, title = {Targeting Ferroptosis As a Cell Death Pathway in Melanoma: From Molecular Mechanisms to Skin Cancer Treatment}, journal = {International Immunopharmacology}, volume = {119}, number = {}, pages = {-}, year = {2023} }
RIS	TY - JOUR AU - Manzari Tavakoli G AU - Mirzapour MH AU - Razi S AU - Rezaei N TI - Targeting Ferroptosis As a Cell Death Pathway in Melanoma: From Molecular Mechanisms to Skin Cancer Treatment JO - International Immunopharmacology VL - 119 IS - SP - EP - PY - 2023 ER -

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