STAT3 Mediates Nilotinib Response in KIT-Altered Melanoma: A Phase II Multicenter Trial of the French Skin Cancer Network

Delyon, Julie; Chevret, Sylvie; Jouary, Thomas; Dalac, S.; Dalle, S.; Guillot, B.; Arnault, Jean‐Philippe; Avril, Marie-Françoise; Bédane, Christophe; Bens, Guido; Pham‐Ledard, Anne; Mansard, Sandrine; Grange, Florent; Machet, L.; Meyer, Nicolas; Legoupil, Délphine; Saïag, Philippe; Idir, Zakia; Renault, Victor; Deleuze, Jean‐François; Hindié, Elif; Battistella, Maxime; Dumaz, Nicolas; Mourah, Samia; Lebbe, Célèste

doi:10.1016/j.jid.2017.07.839

Cited by 52 publications

(42 citation statements)

References 46 publications

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“…63 Five studies were conducted using this drug, in which all patients received orally nilotinib 400 mg twice a day. 56,[64][65][66][67] The most recent study was a phase II clinical trial conducted by the French Skin Cancer Network on 25 patients. 65 At 6 months after nilotinib initiation, only four patients were responsive to nilotinib (ORR: 16%, 90% CI: 5.6-33.0%), including one CR patient and three PR patients.…”

Section: Nilotinibmentioning

confidence: 99%

“…56,[64][65][66][67] The most recent study was a phase II clinical trial conducted by the French Skin Cancer Network on 25 patients. 65 At 6 months after nilotinib initiation, only four patients were responsive to nilotinib (ORR: 16%, 90% CI: 5.6-33.0%), including one CR patient and three PR patients. Out of the other 21 patients, six experienced progression and 15 died with an estimated PFS of 6.0 months and a median OS of 13.2 months (95% CI: 5.6-19.9 months).…”

Section: Nilotinibmentioning

confidence: 99%

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KIT and Melanoma: Biological Insights and Clinical Implications

2020

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OVERVIEW OF c-KIT AND ITS RTKs FAMILY c-KIT or CD117 is a member of class III transmembrane receptor tyrosine kinases (RTKs) along with platelet-derived growth factor receptors (PDGFRs), fms like tyrosine kinase 3 (FLT3)/ CD135, and macrophage colony stimulating factor receptors (M-CSFRs). It was discovered in 1987 as a cellular homologue of viral oncogene v-kit, which was isolated from a feline retro-virus. 1,2 A variety of cell types were identified to express c-KIT including hematopoietic cells, germ cells, gastrointestinal (GI) tract Cajal cells, melanoma cells, B cell progenitors, and mast cells. Wild-type c-KIT protein contains 976 amino acids (aa) divided into three main regions including an extracellular ligand-binding domain with 519 aa, a hydrophobic transmembrane domain with 23 aa, and an intracellular tail (Fig. 1). 3,4 The extracellular domain consists of five immunoglobulin-like domains D1-D5, in which D1-D3 is responsible for stem cell factor (SCF) binding while D4-D5 contains motif for receptor dimerization. The 433 aa cytoplasmic region includes a juxtamembrane domain and a tyrosine kinase domain with an insertion of approximately 80 residues. Most of phosphorylation sites on c-KIT are located at the juxta-membrane region, the kinase insertion domain, and the C-terminal tail. Human c-KIT is encoded by a proto-oncogene located on the chromosome 4 at position of q11-12. 5 This 90 kb gene is transcribed and translated into a core protein of 110 kDa, which is subsequently heterogeneously N-linked glycosylated, mainly in the extra

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Section: Nilotinibmentioning

confidence: 99%

Section: Nilotinibmentioning

confidence: 99%

KIT and Melanoma: Biological Insights and Clinical Implications

2020

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“…Treatment with KIT inhibitors resulted in a trend toward improved response in melanoma patients, with response rates of approximately 20%. Despite the clinical benefit achieved with KIT inhibition in select patients with melanoma harboring KIT mutations, most patients ultimately experience disease progression [9,10,11,12,13,14]. Immunotherapy has recently emerged as a promising treatment modality for cutaneous melanomas.…”

Section: Introductionmentioning

confidence: 99%

Atypical BRAF and NRAS Mutations in Mucosal Melanoma

Dumaz

Jouenne

Delyon

et al. 2019

Cancers

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Primary mucosal melanomas represent a minority of melanomas, but have a significantly worse prognosis than cutaneous melanomas. A better characterization of the molecular pathogenesis of this melanoma subtype could help us understand the risk factors associated with the development of mucosal melanomas and highlight therapeutic targets. Because the Mitogen-Activated Protein Kinase (MAPK) pathway plays such a significant role in melanoma development, we explore v-raf murine sarcoma viral oncogene homolog B (BRAF) and neuroblastoma RAS viral oncogene homolog (NRAS) mutations in mucosal melanoma and compare them to the mutation profiles in cutaneous melanoma and other tumors with BRAF and NRAS mutations. We show that in addition to being less frequent, BRAF and NRAS mutations are different in mucosal melanoma compared to cutaneous melanomas. Strikingly, the BRAF and NRAS mutation profiles in mucosal melanoma are closer to those found in cancers such as lung cancer, suggesting that mutations in mucosal melanoma could be linked to some genotoxic agents that remain to be identified. We also show that the atypical BRAF and NRAS mutations found in mucosal melanomas have particular effects on protein activities, which could be essential for the transformation of mucosal melanocytes.

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“…Several trials based on targeting with kinase inhibitors c-KIT showed consistent results, obtaining an ORR of 16-29% and a median OS of 12-13 months [7][8][9][10]. Other studies investigating nilotinib, a small molecule more potent than imatinib in inhibiting KIT, showed promising clinical activity [11,37,38]. The global, single-arm, phase II TEAM trial showed 26.2% ORR (all partial responses) and OS of 18 months [11].…”

Section: Kitmentioning

confidence: 80%

Molecular and Immune Biomarkers for Cutaneous Melanoma: Current Status and Future Prospects

Pilla

Alberti

Mauro

et al. 2020

Cancers

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Advances in the genomic, molecular and immunological make-up of melanoma allowed the development of novel targeted therapy and of immunotherapy, leading to changes in the paradigm of therapeutic interventions and improvement of patients’ overall survival. Nevertheless, the mechanisms regulating either the responsiveness or the resistance of melanoma patients to therapies are still mostly unknown. The development of either the combinations or of the sequential treatment of different agents has been investigated but without a strongly molecularly motivated rationale. The need for robust biomarkers to predict patients’ responsiveness to defined therapies and for their stratification is still unmet. Progress in immunological assays and genomic techniques as long as improvement in designing and performing studies monitoring the expression of these markers along with the evolution of the disease allowed to identify candidate biomarkers. However, none of them achieved a definitive role in predicting patients’ clinical outcomes. Along this line, the cross-talk of melanoma cells with tumor microenvironment plays an important role in the evolution of the disease and needs to be considered in light of the role of predictive biomarkers. The overview of the relationship between the molecular basis of melanoma and targeted therapies is provided in this review, highlighting the benefit for clinical responses and the limitations. Moreover, the role of different candidate biomarkers is described together with the technical approaches for their identification. The provided evidence shows that progress has been achieved in understanding the molecular basis of melanoma and in designing advanced therapeutic strategies. Nevertheless, the molecular determinants of melanoma and their role as biomarkers predicting patients’ responsiveness to therapies warrant further investigation with the vision of developing more effective precision medicine.

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STAT3 Mediates Nilotinib Response in KIT-Altered Melanoma: A Phase II Multicenter Trial of the French Skin Cancer Network

Cited by 52 publications

References 46 publications

KIT and Melanoma: Biological Insights and Clinical Implications

KIT and Melanoma: Biological Insights and Clinical Implications

Atypical BRAF and NRAS Mutations in Mucosal Melanoma

Molecular and Immune Biomarkers for Cutaneous Melanoma: Current Status and Future Prospects

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