Mitotic rate and S-phase fraction as prognostic factors in stage I cutaneous malignant melanoma

Karjalainen, Jari; Eskelinen, Matti; Nordling, Stig; Lipponen, P; Alhava, Esko; Kosma, Veli‐Matti

doi:10.1038/bjc.1998.318

Cited by 34 publications

(23 citation statements)

References 40 publications

(54 reference statements)

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“…Results (mean and s.e.m.) are presented as a percentage of the total cells adhering after incubation with media alone Proliferation of abnormal melanocytes/melanoma cells is important for early tumour development and subsequent tumour progression, and the rate of proliferation (as measured by the mitotic index, S phase fraction, and percentage Ki67 positivity) is recognized as an important prognostic factor in this neoplasm (Moretti et al, 1990;Ramsay et al, 1995;Karjalainen et al, 1998). Previous research has shown that aMSH (and aMSH analogues) can suppress melanoma cell proliferation (Legros et al, 1981;Jiang et al, 1995;Smalley and Eisen, 2000), but our results demonstrate an aMSH-induced reduction in proliferation in the wild type MC1R transfected cell lines, whereas this decrease in cell numbers was not observed in the variant MC1R transfected melanoma cells.…”

Section: Discussionmentioning

confidence: 99%

Human melanocortin 1 receptor (MC1R) gene variants alter melanoma cell growth and adhesion to extracellular matrix

Robinson

Healy

2002

Oncogene

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Pigmentation is a significant determinant of individual susceptibility to cutaneous melanoma, with fair skinned subjects at highest risk of developing this neoplasm. Melanocortin 1 receptor (MC1R) gene variants alter pigment synthesis in vivo, and are causally associated with red hair and fair skin in humans. MC1R variants are more frequent in subjects with melanoma, and increase the risk of developing this tumour in sporadic and familial cases. MC1R variants may predispose to melanoma as a result of alterations in skin pigmentation (which affords less protection against incident ultraviolet radiation). However, melanoma cells synthesize and release alpha-melanocyte stimulating hormone (aMSH, the ligand for MC1R), therefore MC1R variants could alter the autocrine effects of aMSH on melanoma cell behaviour, thereby affecting early melanoma development and progression via non-pigmentary mechanisms. B16G4F melanoma cells, which are functionally null at Mc1r, were stably transfected with wild type and variant (Arg151Cys, Arg160Trp, and Asp294His) human MC1R. At similar MC1 receptor numbers per cell, aMSH increased intracellular cAMP in wild type MC1R transfected melanoma cells, but the cAMP response was compromised in the variant MC1R transfected clones. In growth inhibition experiments, aMSH significantly reduced growth of wild type MC1R transfected cells, but had no effect on cells transfected with variant MC1R. In addition, binding to fibronectin was significantly reduced by aMSH in the wild type transfectants whereas this was not observed in the variant transfected clones; binding to laminin was not affected by aMSH in this cell line. These results provide evidence for differences in melanoma cell behaviour secondary to MC1R variants, and suggest an alternative non-pigmentary mechanism whereby MC1R variants could modify melanoma susceptibility or progression.

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Section: Discussionmentioning

confidence: 99%

Human melanocortin 1 receptor (MC1R) gene variants alter melanoma cell growth and adhesion to extracellular matrix

Robinson

Healy

2002

Oncogene

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“…115 J AM ACAD DERMATOL VOLUME 52,NUMBER 5 tumor-infiltrating lymphocytes). For example, tumor thickness and mitotic rate reflect the degree of cellular proliferation, a process representing the balance between cell birth (eg, growth fraction [139][140][141][142] and cell death (apoptosis) influenced by cell-cycle regulatory proteins (eg, loss p16 INK4a and apoptotic regulatory proteins 143,144 [eg, loss of apoptotic protease activating factor-1 145,146 ]). Tumor thickness is also influenced by the degree to which tumor cells can invade the dermis and maintain an adequate blood supply, processes governed by proteolytic enzymes (eg, matrix metalloproteinase [MMP]-2 expression [Gelatinase A]), 147 intercellular adhesion molecules (eg, gain of N-cadherin expression and loss of E-cadherin expression), and angiogenic growth factors/angiogenesis (eg, expression of VEGF).…”

Section: Potential Prognostic Molecular Markers In Primary Cutaneous mentioning

confidence: 99%

Molecular diagnostics in melanoma

Carlson

Ross

Slominski

et al. 2005

Journal of the American Academy of Dermatology

132

106

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“…98 Mitotic rate and S-phase fraction proved to correlate independently with survivorship in one multivariate analysis. 99 Lymph node status and the sentinel lymph node biopsy Survival from melanoma drops progressively from 90% at 10 years for Stage I to 10% at 10 years for Stage IV disease. The major independent variable predicting survivorship in thick (ie 44.0 mm in depth) melanoma is the presence or absence of micrometastatic disease in the sentinel lymph node.…”

Section: Ulcerationmentioning

confidence: 99%

Prognosticators of melanoma, the melanoma report, and the sentinel lymph node

2006

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Since the 1960s, the clinical characteristics of melanoma, its histopathology and its biological basis have been the subject of intense study at pigmented lesion clinics in North America, Europe, and Australia. More recently, the immense database of the Melanoma Committee of the American Joint Committee on Cancer (AJCC) has been exploited through complex mathematical models to measure the impact of various histologic features of primary melanomas and of sentinel lymph node deposits and to correlate these parameters with patient survival. The wealth of modern information available to pathologists and clinicians has become of vital interest to the prognostication of the individual patient with melanoma. The purpose of this review is to bring to the attention of anatomic pathologists the essential characteristics of the pathology report for primary cutaneous melanoma in the modern era.

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Mitotic rate and S-phase fraction as prognostic factors in stage I cutaneous malignant melanoma

Cited by 34 publications

References 40 publications

Human melanocortin 1 receptor (MC1R) gene variants alter melanoma cell growth and adhesion to extracellular matrix

Human melanocortin 1 receptor (MC1R) gene variants alter melanoma cell growth and adhesion to extracellular matrix

Molecular diagnostics in melanoma

Prognosticators of melanoma, the melanoma report, and the sentinel lymph node

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