Analysis ofras mutations in human melanocytic lesions: activation of theras gene seems to be associated with the nodular type of human malignant melanoma

Jafari, Mehrdad; Papp, Thilo; Kirchner, Stephan; Diener, Ulrike; Henschler, D.; Burg, Günter; Schiffmann, Dietmar

doi:10.1007/bf01202725

Cited by 88 publications

(46 citation statements)

References 25 publications

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“…N-RAS is the most frequent RAS family member targeted in the melanocyte lineage, with activating mutations in as many as 56% of congenital nevi (Papp et al 1999), 33% of primary and 26% of metastatic melanoma samples (Demunter et al 2001). Activating N-RAS mutations have been correlated with nodular lesions and sun exposure (Jafari et al 1995;van Elsas et al 1996). Interestingly, N-RAS mutations are rarely found in dysplastic nevi (Albino et al 1989;Jafari et al 1995;Papp et al 1999), which may imply their distinct evolutionary path to melanoma.…”

Section: The Ras Family Of Proto-oncogenes: H-ras N-ras and K-rasmentioning

confidence: 99%

“…Activating N-RAS mutations have been correlated with nodular lesions and sun exposure (Jafari et al 1995;van Elsas et al 1996). Interestingly, N-RAS mutations are rarely found in dysplastic nevi (Albino et al 1989;Jafari et al 1995;Papp et al 1999), which may imply their distinct evolutionary path to melanoma. H-RAS activation has occasionally been detected in melanoma, albeit more commonly associated with Spitz nevi, based on amplification of its genomic locus on 11p and oncogenic point mutations (Bastian et al 2000).…”

Section: The Ras Family Of Proto-oncogenes: H-ras N-ras and K-rasmentioning

confidence: 99%

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Malignant melanoma: genetics and therapeutics in the genomic era

2006

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Cell for cell, probably no human cancer is as aggressive as melanoma. It is among a handful of cancers whose dimensions are reported in millimeters. Tumor thickness approaching 4 mm presents a high risk of metastasis, and a diagnosis of metastatic melanoma carries with it an abysmal median survival of 6-9 mo. What features of this malignancy account for such aggressive behavior? Is it the migratory history of its cell of origin or the programmed adaptation of its differentiated progeny to environmental stress, particularly ultraviolet radiation? While the answers to these questions are far from complete, major strides have been made in our understanding of the cellular, molecular, and genetic underpinnings of melanoma. More importantly, these discoveries carry profound implications for the development of therapies focused directly at the molecular engines driving melanoma, suggesting that we may have reached the brink of an unprecedented opportunity to translate basic science into clinical advances. In this review, we attempt to summarize our current understanding of the genetics and biology of this disease, drawing from expanding genomic information and lessons from development and genetically engineered mouse models. In addition, we look forward toward how these new insights will impact on therapeutic options for metastatic melanoma in the near future. The diseaseMelanomas most often arise within epidermal melanocytes of the skin, although they can also derive from noncutaneous melanocytes such as those lining the choroidal layer of the eye, GI and GU mucosal surfaces, or the meninges. Melanoma is also among the more common causes of "metastatic cancer of unknown primary," which may reflect either a propensity to arise in unexpected sites along the neural crest migratory route, or rapid growth of poorly differentiated lesions arising from indolent or unrecognized cutaneous primary lesions. Clinical staging for primary cutaneous melanoma employs measurements of thickness (in millimeters), presence of ulceration, penetration through cutaneous layers, mitotic rate, evidence of "in transit" metastasis, tumor spread to draining lymph nodes, and evidence of distant metastasis. Management issues in melanoma can be classified in terms of prevention, diagnosis, local disease management, and treatment of metastatic disease.In view of the epidemiological and emerging experimental evidence linking melanoma incidence to UV exposure and skin phototype, prevention and screening strategies represent key areas for reduction of disease incidence and severity. For most cutaneous melanomas in the so-called radial growth phase (e.g., thin melanomas), surgical removal affords curative treatment. In contrast, a significant fraction of patients diagnosed with intermediate-thickness (2-4 mm) cutaneous melanoma eventually succumb to recurrence at regional or distant sites.Critical biological questions facing the melanoma research community include: (1) What genetic and environmental factors contribute to and/or modulate risk of melanom...

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Section: The Ras Family Of Proto-oncogenes: H-ras N-ras and K-rasmentioning

confidence: 99%

Section: The Ras Family Of Proto-oncogenes: H-ras N-ras and K-rasmentioning

confidence: 99%

Malignant melanoma: genetics and therapeutics in the genomic era

2006

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“…Additional mutations were in codon 465 (exon 11). There is an inverse correlation between the occurrence of mutations in the BRAF gene and in the ras oncogene, which is activated in approximately 10-30% of human melanomas (Albino et al, 1989;Van't Veer et al, 1989;Jafari et al, 1995;Omholt et al, 2002). This suggests that the two proteins are in the same pathway of melanomagenesis.…”

Section: Introductionmentioning

confidence: 99%

Genomic alterations in spontaneous and carcinogen-induced murine melanoma cell lines

et al. 2004

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We have conducted an analysis of genetic alterations in spontaneous murine melanoma cell line B16F 0 and its two metastatic clones, B16F 1 and B16F 10 and the carcinogeninduced murine melanoma cell lines CM519, CM3205, and K1735. We found that unlike human melanomas, the murine melanoma cell lines did not have activating mutations in the Braf oncogene at exon 11 or 15. However, there were distinct patterns of alterations in the ras, Ink4a/Arf, and p53 genes in the two melanoma groups. In the spontaneous B16 melanoma cell lines, expression of p16Ink4a and p19 Arf tumor suppressor proteins was lost as a consequence of a large deletion spanning Ink4a/Arf exons 1a, 1b, and 2. In contrast, the carcinogen-induced melanoma cell lines expressed p16 Ink4a but had inactivating mutations in either p19Arf (K1735) or p53 (CM519 and CM3205). Inactivation of p19Arf or p53 in carcinogen-induced melanomas was accompanied by constitutive activation of mitogen-activated protein kinases (MAPKs) and/or mutation-associated activation of N-ras. These results indicate that genetic alterations in p16 Ink4a /p19Arf , p53 and ras-MAPK pathways can cooperate in the development of murine melanoma.

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“…In the case of RAS, activation can be mediated indirectly through di erent RTKs, such as EGFR, or through activating oncogenic mutations. Activating mutations in N-and H-RAS has been observed in close to 30% of a subset of melanoma, the nodular amelanotic type (Jafari et al, 1995). Although germline heterozygous mutations of PTEN do not confer a melanoma phenotype, they do lead to a cancer-prone state in the mouse (DiCristofano et al, 1998;Stambolic et al, 1998;Podsypanina et al, 1999).…”

Section: Rtk-ras-mapk Pathway In Pathogenesis Of Melanomasmentioning

confidence: 99%

“…With this hypothesis in mind, we speculated that the addition of oncogenic stimuli in an INK4a null setting may promote the transformation of these murine dermal melanocytes. The candidate oncogenic lesion considered early in the course of these studies was oncogenic RAS, based upon several lines of experimental evidence suggesting potent cooperative interaction between activated H-RAS V12G and INK4a/ARF de®ciency in cultured ®broblasts (Serrano et al, 1997), and the presence of activating N-and H-RAS mutations in human nodular melanoma (Jafari et al, 1995).…”

Section: Building a Mouse Model For Malignant Melanomamentioning

confidence: 99%

Modeling malignant melanoma in mice: pathogenesis and maintenance

Chin

1999

Oncogene

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Analysis ofras mutations in human melanocytic lesions: activation of theras gene seems to be associated with the nodular type of human malignant melanoma

Cited by 88 publications

References 25 publications

Malignant melanoma: genetics and therapeutics in the genomic era

Malignant melanoma: genetics and therapeutics in the genomic era

Genomic alterations in spontaneous and carcinogen-induced murine melanoma cell lines

Modeling malignant melanoma in mice: pathogenesis and maintenance

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