High basal NF-κB activity in nonpigmented melanoma cells is associated with an enhanced sensitivity to vitamin D3 derivatives

Janjetovic, Zorica; Brożyna, Anna A.; Tuckey, Robert C.; Kim, T. K.; Nguyen, Minh N.; Jóźwicki, Wojciech; Pfeffer, Susan R.; Pfeffer, Lawrence M.; Slominski, Andrzej

doi:10.1038/bjc.2011.458

Cited by 80 publications

(121 citation statements)

References 36 publications

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“…Likewise, a similar effect was observed by other authors on colorectal cancer cells (Schwab et al, 2007) and prostate cancer cells (Krishnan & Feldman, 2010). Nevertheless, as opposing results have been also reported on the effects of Vit D on NF-kB expression levels (Bao et al, 2010;Janjetovic et al, 2011;Krishnan et al, 2007) further studies may better define the role of NF-kB in autophagy and, consequently, the potential therapeutic impact of Vit D in modulating this phenomenon in cancer cells.…”

Section: Vit D and Autophagymentioning

confidence: 53%

“…This phenomenon may results in an inhibition of IFN-g induced activation and potentiation of lysosomal activity of macrophages, recruitment of autophagic proteins, and, ultimately, may lead to a decrease of autophagy Wu and Sun (2011) NF-kB expression (?) Bao et al (2010), Krishnan and Feldman (2010), Tse et al (2010), andJanjetovic et al (2011) Induced expression of thioredoxin reductase 1 (TXNRD1) Swami et al (2003), Peehl et al (2004), Kovalenko et al (2010) Antioxidant defense and DNA repair Increased production of superoxide dismutase 1 and 2 (SOD1 and SOD2) in prostate epithelial cells (PECs) and in androgen-sensitive prostate cancer cells (LNCaP) Peehl et al (2004) and Lambert et al (2006) Increase of glucose-6-phosphate dehydrogenase (G6PDH) expression levels Zhang et al (2005), Bao et al (2008), and Kovalenko et al (2010) Induction of nuclear factor erythroid-derived 2-like 2 (NFE2L2) transcription factor that controls the gene expression of several enzymes of the antioxidants systems such as glutathione peroxidase (GPX) 3, heme oxygenase 1 (HMOX-1), and aldo-keto reductase 1C2(AKR1C2)…”

Section: Ink4dmentioning

confidence: 99%

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Vitamin D in cancer chemoprevention

Giammanco¹,

Majo²,

Guardia

et al. 2015

Pharmaceutical Biology

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Context: There is increasing evidence that Vitamin D (Vit D) and its metabolites, besides their well-known calcium-related functions, may also exert antiproliferative, pro-differentiating, and immune modulatory effects on tumor cells in vitro and may also delay tumor growth in vivo. Objective: The aim of this review is to provide fresh insight into the most recent advances on the role of Vit D and its analogues as chemopreventive drugs in cancer therapy. Methods: A systematic review of experimental and clinical studies on Vit D and cancer was undertaken by using the major electronic health database including ISI Web of Science, Medline, PubMed, Scopus and Google Scholar. Results and conclusion: Experimental and clinical observations suggest that Vit D and its analogues may be effective in preventing the malignant transformation and/or the progression of various types of human tumors including breast cancer, prostate cancer, colorectal cancer, and some hematological malignances. These findings suggest the possibility of the clinical use of these molecules as novel potential chemopreventive and anticancer agents.

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Section: Vit D and Autophagymentioning

confidence: 53%

Section: Ink4dmentioning

confidence: 99%

Vitamin D in cancer chemoprevention

Giammanco¹,

Majo²,

Guardia

et al. 2015

Pharmaceutical Biology

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“…Along with the primary products of CYP11A1 action on vitamin D3, 17,20(OH) 2 D3, 20,22(OH) 2 D3, and 20,23(OH) 2 D3, we have a unique set of derivatives all containing a 20-hydroxyl group plus one additional hydroxyl group at every position on the side chain, except C21 (note that C26 and C27 are equivalent). All of these 20-hydroxy derivatives have been shown to be biologically active (Zbytek et al, 2008;Janjetovic et al, 2009Janjetovic et al, , 2010Janjetovic et al, , 2011Li et al, 2010;Slominski et al, 2010Slominski et al, , 2011Slominski et al, , 2012aTang et al, 2010a;Tuckey et al, 2011;Kim et al, 2012;Lu et al, 2012;Wang et al, 2012). The low catalytic efficiency of CYP27B1 toward 20(OH)D3 is greatly enhanced when the second hydroxyl group is added toward the end of the side chain, as seen for 24,20(OH) 2 D3, 20,25(OH) 2 D3, and 20,26(OH) 2 D3.…”

Section: Discussionmentioning

confidence: 99%

“…It has been documented that the CYP11A1-derived vitamin D3 analogs, 20(OH)D3 and 20,23(OH) 2 D3, display similar properties to 1,25(OH) 2 D3, such as inhibiting cell proliferation, promoting differentiation of keratinocytes and leukemia cells, and suppressing tumorigenicity of melanoma (Zbytek et al, 2008;Janjetovic et al, 2009Janjetovic et al, , 2011Li et al, 2010;Slominski et al, 2010Slominski et al, , 2012aTuckey et al, 2011;Kim et al, 2012;Lu et al, 2012;Wang et al, 2012).…”

Section: Downloaded Frommentioning

confidence: 99%

“…Via binding to the vitamin D receptor, these compounds can inhibit keratinocyte, melanoma, leukemia, breast, and liver cancer cell proliferation; promote differentiation; and display antiinflammatory activity by decreasing nuclear factor-ĸB activity (Zbytek et al, 2008;Janjetovic et al, 2009Janjetovic et al, , 2010Janjetovic et al, , 2011Li et al, 2010;Slominski et al, 2010Slominski et al, , 2011Slominski et al, , 2012aTang et al, 2010a;Tuckey et al, 2011;Kim et al, 2012;Lu et al, 2012;Wang et al, 2012). Importantly, all three of these derivatives lack calcemic activity in rodents, even at relatively high doses (Slominski et al, , 2013aWang et al, 2012).…”

Section: Introductionmentioning

confidence: 99%

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Hydroxylation of CYP11A1-Derived Products of Vitamin D3 Metabolism by Human and Mouse CYP27B1

et al. 2013

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CYP11A1 can hydroxylate vitamin D3 at carbons 17, 20, 22, and 23, producing a range of secosteroids which are biologically active with respect to their ability to inhibit proliferation and stimulate differentiation of various cell types, including cancer cells. As 1a-hydroxylation of the primary metabolite of CYP11A1 action, 20S-hydroxyvitamin D3 [20(OH)D3], greatly influences its properties, we examined the ability of both human and mouse CYP27B1 to 1a-hydroxylate six secosteroids generated by CYP11A1. Based on their k cat /K m values, all CYP11A1-derived metabolites are poor substrates for CYP27B1 from both species compared with 25-hydroxyvitamin D3. No hydroxylation of metabolites with a 17a-hydroxyl group was observed. 17a,20-Dihydroxyvitamin D3 acted as an inhibitor on human CYP27B1 but not the mouse enzyme. We also tested CYP27B1 activity on 20,24-, 20,25-, and 20,26-dihydroxyvitamin D3, which are products of CYP24A1 or CYP27A1 activity on 20(OH)D3. All three compounds were metabolized with higher catalytic efficiency (k cat /K m ) by both mouse and human CYP27B1 than 25-hydroxyvitamin D3. CYP27B1 action on these new dihydroxy derivatives was confirmed to be 1a-hydroxylation by mass spectrometry and nuclear magnetic resonance analyses. Both 1,20,25-and 1,20,26-trihydroxyvitamin D3 were tested for their ability to inhibit melanoma (SKMEL-188) colony formation, and were significantly more active than 20(OH)D3. This study shows that CYP11A1-derived secosteroids are 1a-hydroxylated by both human and mouse CYP27B1 with low catalytic efficiency, and that the presence of a 17a-hydroxyl group completely blocks 1a-hydroxylation. In contrast, the secondary metabolites produced by subsequent hydroxylation of 20(OH)D3 at C24, C25, or C26 are very good substrates for CYP27B1.

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