Redox Regulation in Human Melanocytes and Melanoma

Meyskens, Frank L.; Farmer, Patrick J.; Fruehauf, John P.

doi:10.1034/j.1600-0749.2001.140303.x

Cited by 200 publications

(164 citation statements)

References 66 publications

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“…25 Consistently, expression of antioxidant enzymes is significantly elevated in melanoma tissue. 26 Whether DHCR24 is upregulated in melanoma cells by the same mechanisms and acts in concert with other antioxidant enzymes remains to be established. The pharmacologic agent U18666A is a hydrophobic amine that acts as an inhibitor of cholesterol biosynthesis by blocking DHCR24 activity as well as other enzymes of sterol biosynthesis, including oxidosqualene synthetase and D8-D7 sterol isomerase.…”

Section: Discussionmentioning

confidence: 99%

DHCR24 gene expression is upregulated in melanoma metastases and associated to resistance to oxidative stress‐induced apoptosis

Stasi

Vallacchi

Campi

et al. 2005

Intl Journal of Cancer

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The DHCR24 gene encoding for the 3β‐hydroxysterol Δ24‐reductase, an oxidoreductase involved in cholesterol biosynthesis, was isolated by subtractive hybridization as highly expressed in a short‐term melanoma cell line derived from a cutaneous metastases (S/M2) compared to that obtained from the autologous primary tumor (S/P). DHCR24 (alias seladin‐1, diminuto/dwarf1 homolog) has been reported to act as an antiapoptotic factor in neurons. Gene expression analysis by Northern blot confirmed that DHCR24 was 5‐fold upregulated in S/M2 compared to S/P cells. High levels of DHCR24 gene expression were detected in 13/25 melanoma metastases and in 1/7 primary melanomas by real‐time PCR, indicating that upregulation of this gene may occur in melanoma progression. In S/M2 cells, high DHCR24 gene expression associated with resistance to apoptosis triggered by oxidative stress induced by exposure to hydrogen peroxide. DHCR24 gene transfer was shown to protect melanoma cells from H2O2‐induced cytotoxicity. Although higher cholesterol levels were shown in S/M2 cells compared to S/P cells, DHCR24 gene transfer did not increase cholesterol content. To evaluate whether DHCR24 acts as an antiapoptotic factor in melanoma metastases, the cytotoxic effect of chemotherapeutic agents was tested in DHCR24 transfectants and in the presence of a DHCR24 inhibitor, U18666A. High DHCR24 gene expression in transfectants did not result in a higher resistance to cytotoxic agents; treatment with U18666A was cytotoxic in S/P cells with a lower DHCR24 content and showed additive cytotoxic effect only when associated with H2O2 and not with cysplatin or etoposide, indicating that the DHCR24 protective effect is exerted through an oxidative stress‐specific mechanism. © 2005 Wiley‐Liss, Inc.

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Section: Discussionmentioning

confidence: 99%

DHCR24 gene expression is upregulated in melanoma metastases and associated to resistance to oxidative stress‐induced apoptosis

Stasi

Vallacchi

Campi

et al. 2005

Intl Journal of Cancer

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“…Others have proposed that the establishment of the BRAF T1799A mutation occurs as a function of neighbouring UVinduced pyrimidine dimers (Thomas et al, 2006). According to another hypothesis, the BRAF mutation might be the result of UV-induced oxidation of melanin, resulting in the formation of reactive oxygen species and leading to increased DNA damage (Meyskens et al, 2001). As none of the above hypotheses has yet been proven, the mechanism-or mechanisms-underlying the acquisition of the BRAF T1799A mutation remains elusive.…”

Section: Braf Mutations and Uv Radiationmentioning

confidence: 99%

BRAFE600 in benign and malignant human tumours

et al. 2007

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Of the RAF family of protein kinases, BRAF is the only member to be frequently activated by mutation in cancer. A single amino acid substitution (V600E) accounts for the vast majority and results in constitutive activation of BRAF kinase function. Its expression is required to maintain the proliferative and oncogenic characteristics of BRAF E600 -expressing human tumour cells. Although BRAF E600 acts as an oncogene in the context of additional genetic lesions, in primary cells it appears to be associated rather with transient stimulation of proliferation. Eventually, BRAF E600 signalling triggers cell cycle arrest with the hallmarks of cellular senescence, as is illustrated by several recent studies in cultured cells, animal models and benign human lesions. In this review, we will discuss recent advances in our understanding of the role of BRAF E600 in benign and malignant human tumours and the implications for therapeutic intervention.

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“…Medical bibliography suggests that, among environmental factors, oxidative stress could play a prominent role (e.g. Chakraborty et al 1996;Meyskens et al 2001;Wittgen et al 2007). Oxidative stress is commonly defined as the imbalance between the production of reactive oxygen species (ROS) and the state of the antioxidant and repair machinery, with the balance tipped towards the former (Finkel & Holbrook 2000).…”

Section: Introductionmentioning

confidence: 99%

The expression of melanin-based plumage is separately modulated by exogenous oxidative stress and a melanocortin

2009

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Melanin-based traits involved in animal communication have been traditionally viewed as occurring under strict genetic control. However, it is generally accepted that both genetic and environmental factors influence melanin production. Medical studies suggest that, among environmental factors influencing melanization, oxidative stress could play a relevant role. On the other hand, genetic control would be exerted by the melanocortin system, and particularly by the alpha-melanocyte-stimulating hormone (a-MSH), which triggers the production of eumelanins (black pigments). To determine how the melanocortin system and an exogenous source of oxidative stress interact in the expression of melanin-based plumage, developing red-legged partridges (Alectoris rufa) were manipulated. Some partridges were injected with a-MSH, while other birds received a pro-oxidant molecule (diquat) in drinking water. Controls and birds receiving both treatments were also studied. Both a-MSH-and diquat-treated individuals presented larger eumelanin-based traits than controls, but a-MSHþdiquat-treated birds showed the largest traits, suggesting that oxidative stress and melanocortins promote additive but independent effects. Diquat also induced a decline in the level of a key intracellular antioxidant (glutathione), which is associated with high expression of eumelanin-based signals in other bird species. Some scenarios for the evolution of melanin-based traits in relation to oxidative stress are proposed.

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Redox Regulation in Human Melanocytes and Melanoma

Cited by 200 publications

References 66 publications

DHCR24 gene expression is upregulated in melanoma metastases and associated to resistance to oxidative stress‐induced apoptosis

DHCR24 gene expression is upregulated in melanoma metastases and associated to resistance to oxidative stress‐induced apoptosis

BRAFE600 in benign and malignant human tumours

The expression of melanin-based plumage is separately modulated by exogenous oxidative stress and a melanocortin

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