Expression of CD40, CD44, bcl‐2 antigens and rate of cell proliferation on fine needle aspirates from metastatic melanoma

Sviatoha, V.; Rundgren, Åke; Tani, Ednéia; Hansson, Johan; Kleina, Regina; Skoog, Lambert

doi:10.1046/j.1365-2303.2002.00376.x

Cited by 19 publications

(16 citation statements)

References 24 publications

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“…Over 1/3 of the examined melanotic and amelanotic melanoma were in S and G2/M phases which confirms the opinion that melanoma is a tumor with high proliferation rate [6,22]. But our observation that the amelantic form has more cells in S/G2/M phases than the melanotic one is of special importance because there are not such data in the melanoma literature although there is a common opinion that the amelanotic form is a more aggressive, rapidly growing melanoma form [16,23].…”

Section: Discussionsupporting

confidence: 77%

“…The results of other authors concerning the relationships between tumor growth and the ability of its cells to proliferate and undergo apoptosis are controversial; some authors showed that tumor growth depended mainly on cell proliferation [27], others indicated that both proliferation and apoptosis increased [28,29], that higher proliferation with decreased ability to undergo apoptosis supported tumor progression [29]. Observations of others that human melanoma cells have very low ability to undergo spontaneous apoptosis [30] and proliferating cells accounted for 20-40% of all cells [22] led them to the conclusion that the growth of human melanoma depends mainly on cell proliferative activity [31,32]. In contrast, our results may suggest that the expansive growth of the amelanotic melanoma line depends mainly on the decreased ability of cells in all cell cycle phases to undergo spontaneous apoptosis.…”

Section: Discussionmentioning

confidence: 99%

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Camptothecin-induced death of amelanotic and melanotic melanoma cells in different phases of cell cycle

Cichorek¹

2011

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Camptothecin and its analogues are used as S-phase specific antitumor drugs because of topoisomerase I inhibition providing cells to death by apoptosis. Our previous works documented that amelanotic hamster's melanoma is very sensitive to camptothecin. Because of the challenges in treating melanoma and S-phase specificity of camptothecin, we performed a study to search what melanoma cell cycle phases are susceptible to this substance.Melanotic (Ma) and amelanotic (Ab) lines of Bomirski hamster's melanoma were used. Camptothecin cytotoxicity was determined by TUNEL method and cell cycle analysis was done by DNA staining with propidium iodide.Camptothecin after short time killed amelanotic melanoma cells from S/G2/M phases but with extended time dying cells came from G0/G1. Melanotic melanoma had fewer cells in S/G2/M phases and 3-fold more of these cells spontaneously died in comparison to more aggressive amelanotic line. High susceptibility of amelanotic melanoma cells to camptothecin show that not only cells with proliferative activity were sensitive to this alkaloid but with extended time it killed cells from all cycle phases. High number of cells in S/G2/M phases and low rate of spontaneous death among amelanotic melanoma cells suggest that the expansive growth of this melanoma line depends mainly on the decreased ability to undergo spontaneous apoptosis. If the sensitivity of amelanotic melanoma is not only hamster's but also human melanoma feature, we can suspect that by choosing melanoma form for treatment with camptothecin we could improve effectiveness of this drug against melanoma.

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Section: Discussionsupporting

confidence: 77%

Section: Discussionmentioning

confidence: 99%

Camptothecin-induced death of amelanotic and melanotic melanoma cells in different phases of cell cycle

Cichorek¹

2011

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“…101,102,[104][105][106] CD40, a B cell marker that is also involved in tumor suppression, has increased expression in melanomas relative to nevi but has not been convincing as a prognostic marker. 107,108 van den Ord 109 studied CD26, an adenosine deaminase receptor, and found slightly increased staining in melanomas relative to benign nevi but no prognostic significance. There are conflicting reports of the expression of FAS and FASligand (tumor suppressor proteins of the tumor necrosis family) in melanomas and nevi and neither has been shown to be an independent prognostic factor.…”

Section: Markers Of Tumor Cell Proliferationmentioning

confidence: 99%

Immunohistochemical characteristics of melanoma

et al. 2008

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Melanoma has a wide spectrum of histologic features which mimic epithelial, hematologic, mesenchymal, and neural tumors. Immunohistochemistry has been the primary tool to distinguish melanomas from these other tumors; it has also been studied for use as an adjunct to distinguish benign and malignant melanocytic tumors and to elucidate prognosis. Furthermore, there has been extensive effort to find a suitable marker to differentiate spindle cell and desmoplastic melanoma from other tumors. We have reviewed the literature investigating melanocytic differentiation markers, proliferation markers, immunomodulatory markers, signaling molecules, and nerve growth factors and receptors. Despite the proliferation of immunohistochemical markers, S‐100 remains the most sensitive marker for melanocytic lesions, while markers such as HMB‐45, MART‐1/Melan‐A, tyrosinase, and MITF demonstrate relatively good specificity but not as good sensitivity as S‐100. No marker has proven useful in distinguishing spindle cell and desmoplastic melanomas from other tumors. Ki67 remains the most useful adjunct in distinguishing benign from malignant melanocytic tumors. None of the markers reviewed has been shown conclusively to have prognostic value for melanocytic neoplasms.

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“…Studies report a wide range of frequencies of Bcl-2 expression (60%-96%), with inconsistent associations between Bcl-2 expression and clinical outcome. Some studies report that up-regulation of Bcl-2 correlates with advanced stage and poor prognosis (11)(12)(13), whereas others report that down-regulation of Bcl-2 is associated with disease progression, advanced stage, and poor prognosis (14 -19). It is important to note that other studies have shown that Bcl-2 expression does not change during tumor progression, with equivalent expression levels in melanoma and normal melanocytes (20 -22).…”

Section: Introductionmentioning

confidence: 99%

Automated Quantitative Analysis of Tissue Microarrays Reveals an Association between High Bcl-2 Expression and Improved Outcome in Melanoma

DiVito

Berger²,

Camp³

et al. 2004

Cancer Research

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The addition of B-cell lymphoma 2 (Bcl-2) antisense to dacarbazine in the treatment of metastatic melanoma demonstrates improved response rates and progression-free survival when compared with dacarbazine alone. Studies on small cohorts of melanoma patients have shown variability in Bcl-2 expression (60%-96% positive). We performed quantitative analysis of Bcl-2 expression in a large patient cohort to assess the association with outcome.Tissue microarrays containing intact melanoma specimens representing 402 patients (339 with associated survival data) were analyzed with our AQUA system for automated quantitative analysis. Automated, quantitative analysis uses S100 to define pixels as melanoma (tumor mask) within the array spot and measures intensity of Bcl-2 expression using a Cy5 conjugated antibody within the mask. A continuous index score is generated, which is directly proportional to the number of molecules per unit area. Scores were divided into quartiles and correlated with clinical variables.High Bcl-2 expression was associated with better outcome in the entire cohort and among metastatic specimens only (P ‫؍‬ 0.004 and P ‫؍‬ 0.015, respectively). Expression was higher in primary than in metastatic specimens (P < 0.0001). There was no association between Bcl-2 expression and Breslow depth or Clark level.The diverse results within the literature may be due to use of small cohorts or variability in staining technique. These results suggest studies are needed to evaluate the association between quantitative assessment of Bcl-2 expression and response to Bcl-2 targeting therapy toward the goal of improved response rates to these drugs.

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Expression of CD40, CD44, bcl‐2 antigens and rate of cell proliferation on fine needle aspirates from metastatic melanoma

Cited by 19 publications

References 24 publications

Camptothecin-induced death of amelanotic and melanotic melanoma cells in different phases of cell cycle

Camptothecin-induced death of amelanotic and melanotic melanoma cells in different phases of cell cycle

Immunohistochemical characteristics of melanoma

Automated Quantitative Analysis of Tissue Microarrays Reveals an Association between High Bcl-2 Expression and Improved Outcome in Melanoma

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