Phase I Trial of Sequential Low-Dose 5-Aza-2′-Deoxycytidine Plus High-Dose Intravenous Bolus Interleukin-2 in Patients with Melanoma or Renal Cell Carcinoma

Gollob, Jared; Sciambi, Catherine J.; Peterson, Bercedis L.; Richmond, T.; Thoreson, M.; Moran, Kelly R.; Dressman, Holly K.; Jelı́nek, Jaroslav; Issa, Jean–Pierre J.

doi:10.1158/1078-0432.ccr-06-0883

Cited by 125 publications

(95 citation statements)

References 21 publications

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“…Recently, a phase I trial of low-dose 5-Aza-dC plus interleukin-2 was performed in patients with malignant melanoma (50). Among 16 patients, the response rate was 31% (50). Although global methylation was evaluated using repetitive sequences in this study, the methylation status of specific genes affected by 5-Aza-dC treatment were not examined.…”

Section: Discussionmentioning

confidence: 97%

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Methylation status of the SOCS3 gene in human malignant melanomas

Tokita

Maesawa²,

Kimura³

et al. 2007

Int J Oncol

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Abstract. The suppressors of cytokine signaling (SOCS) family inhibits not only Janus kinase (JAK)/signal transducers and activators of transcription (STAT) but also focal adhesion kinase (FAK) signaling pathways, and has tumor suppressor activity. Aberrant methylation in the promoter region of the SOCS3 gene frequently occurs in several types of human malignancy, and its transcriptional silencing is associated with malignant tumor behavior. In malignant melanomas, the expression and methylation status of the SOCS3 gene have not been elucidated. We therefore examined the methylation status and/or protein expression of the SOCS3 gene in 5 human malignant melanoma cell lines, 2 primary cultures of normal melanocytes, and surgically resected tumors (5 malignant melanomas and 2 melanocytic nevi). Four of the 5 melanoma cell lines and the 2 primary cultures of normal melanocytes expressed SOCS3 protein to various degrees, and only one melanoma cell line was negative. Expression of SOCS3 protein was inversely correlated with methylation status in the SOCS3 promoter region, and treatment with a demethylating agent (5-aza-2'-deoxycytidine) was able to induce expression of the protein in one melanoma cell line that was SOCS3-negative and another that was weakly positive. Three of the 5 primary malignant melanomas and one of the 2 melanocytic nevi showed aberrant methylation. These results suggest that inactivation of the SOCS3 gene by hypermethylation may be involved in the promotion of malignant behavior of melanomas.

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Section: Discussionmentioning

confidence: 97%

“…We expect that transcriptional silencing of the SOCS3 gene by aberrant methylation might contribute to resistance of malignant melanoma cells to IFN treatment. Recently, a phase I trial of low-dose 5-Aza-dC plus interleukin-2 was performed in patients with malignant melanoma (50). Among 16 patients, the response rate was 31% (50).…”

Section: Discussionmentioning

confidence: 99%

Methylation status of the SOCS3 gene in human malignant melanomas

Tokita

Maesawa²,

Kimura³

et al. 2007

Int J Oncol

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“…A daganatokban ezen enzimek gátlásával (DNMT-inhibitor például a decitabin, HDAC-inhibitor például a valproát) visszafordítható a tumorszuppresszor gének aberráns hipermetilációja, ami géncsendesítést okozott, ezáltal expressziójuk növekedésével újra el tudják látni a sejtosztódást fékező funkciójukat. A jövőben melanomás betegek is profi tál-hatnak ezen kutatások eredményeiből [34,35]. Emellett a cutan melanomák 60%-ában patológiásan működő PI3K/AKT/mTOR szignáltranszdukciós útvonal nemcsak a tumorszuppresszor PTEN által gátolható, hanem célzottan, AKT-inhibitorokkal (például perifosin) és mTOR-gátlókkal (például temsirolimus, everolimus) is.…”

Section: áBraunclassified

Genetic diversity and immunological characteristics of malignant melanoma: the therapeutic spectrum

Doma

Gulya

2015

Orvosi Hetilap

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A malignus melanoma pigmentsejtekből kiinduló, későn felfedezve igen agresszív, folyamatosan növekvő incidenciá-jú, bármely korosztályt érintő daganatos megbetegedés. Leggyakoribb formája meglévő hajlamosító tényezők (bőr-, szem-, hajszín, anyajegyek, pozitív családi anamnézis) talaján hozzáadódó környezeti faktorok (napégés) hatására a kültakarón, vagyis minden orvos számára könnyen vizsgálható helyen alakul ki. Sikeres kezelésének alapja továbbra is a korai diagnózis és műtéti eltávolítás. Áttétek jelentkezésekor a klasszikus, bár melanoma esetén csekély sikerrel kecsegtető kemo-és sugárterápia mellett, illetve helyett ma már új, molekuláris genetikai kutatásokon alapuló célzott terápiás szerek, valamint a gátolt tumorellenes immunválaszt a fék alól felszabadító immunterápiás gyógyszerek is rendelkezésre állnak. Az összefoglaló közleményben a szerzők régi és új ismereteket igyekeznek rendszerezni és terjeszteni, bármely, a téma iránt mélyebben érdeklődő gyógyító szakma képviselőjének átnyújtani. Orv. Hetil., 2015, 156(15), 583-591. Kulcsszavak: malignus melanoma, célzott terápia, jelátviteli útvonal, immunterápiaGenetic diversity and immunological characteristics of malignant melanoma: the therapeutic spectrum Malignant melanoma, originating from pigment cells, is a highly aggressive tumour affecting patients of any age group. Its incidence is rapidly growing. The most common form can be easily diagnosed by any physician. There are some well-known genetic (skin-, eye-, hair colour, naevi, melanoma in the personal/family history) and environmental (ultraviolet radiation) predisposing factors. Treatment is based on early diagnosis and excision. When metastasis occurs, the traditional chemo-and radiotherapy gives a low response rate. Recently some newly approved targeted therapies and immunomodulant drugs have become available. This review focuses on the classifi cation and novel therapeutic approaches of malignant melanoma to provide guidance to clinicians.

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“…However, injection of decitabine in nude mice carrying melanoma xenografts led to resensitization to interferon treatment (Reu et al, 2006). A phase I clinical trial of decitabine together with interleukin-2 in melanoma patients further showed an objective response in 31% of the patients (Gollob et al, 2006). Likewise, preclinical data also suggests that epigenetic therapy can induce radiosensitization and enhance current conventional treatment regimens (Munshi et al, 2005).…”

Section: Epigenetic Cancer Therapymentioning

confidence: 99%

Pharmaco-epigenomics: discovering therapeutic approaches and biomarkers for cancer therapy

2010

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An important feature of cancer is dysregulation of gene activity and gene expression, which is driven by a combination of acquired genetic and epigenetic alterations. Here, we will highlight how insights into the epigenetic processes underpinning tumor biology have led to the emerging field of cancer pharmaco-epigenomics. First, we will discuss how interference with the epigenetic machinery in cancer is leading to novel promising therapies, with several DNA methyltransferase and histone deacetylase inhibitors being approved for cancer treatment. Second, we will discuss how epigenetic markers in cancer may increasingly be used as complementary diagnostic tools, prognostic markers of disease progression, and predictive markers of treatment response. Although the anti-tumoral activities of epigenetic therapies have thus far been attributed to reactivation of silenced tumor-suppressor and/or apoptotic genes, they may also influence the tumor environment by directly affecting stromal cells. As an example, we will discuss how tumor-endothelial cells are regulated at the epigenetic level and are affected by methyltransferase and histone deacetylase inhibitors.

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Phase I Trial of Sequential Low-Dose 5-Aza-2′-Deoxycytidine Plus High-Dose Intravenous Bolus Interleukin-2 in Patients with Melanoma or Renal Cell Carcinoma

Cited by 125 publications

References 21 publications

Methylation status of the SOCS3 gene in human malignant melanomas

Methylation status of the SOCS3 gene in human malignant melanomas

Genetic diversity and immunological characteristics of malignant melanoma: the therapeutic spectrum

Pharmaco-epigenomics: discovering therapeutic approaches and biomarkers for cancer therapy

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