2000
DOI: 10.1054/bjoc.1999.1076
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Expression of SCF splice variants in human melanocytes and melanoma cell lines: potential prognostic implications

Abstract: Summary Stem cell factor (SCF), the ligand for c-Kit, is known to regulate developmental and functional processes of haematopoietic stem cells, mast cells and melanocytes. Two different splice variants form predominantly soluble (sSCF or SCF-1) and in addition some membranebound SCF (mSCF or SCF-2). In order to explore the prognostic significance of these molecules in melanoma, total SCF, SCF splice variants and c-Kit expression were studied in normal skin melanocytes and in 11 different melanoma cell lines, u… Show more

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Cited by 27 publications
(19 citation statements)
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“…As tumor aggressiveness increased, a shift in alternative splicing towards the 'readthrough' transcript was noticed in tumor cells but not in near-by endothelial cells, suggesting modified control over the splicing factors leading to AChE-R production in malignant, as opposed to benign cells. Shifted splicing is often associated with tumorogenicity; for example, metastatic melanoma cell lines lose their ability to express stem cell factor (SCF)-2 but retain their ability to express its alternatively spliced SCF-1 variant (Welker et al, 2000). Also, the VEGF 121 variant, when over-expressed in breast carcinoma cells, increased angiogenicity and tumorogenicity more than other VEGF splice variants (Zhang et al, 2000).…”
Section: Tumor Versus Vascular Cellsmentioning
confidence: 99%
“…As tumor aggressiveness increased, a shift in alternative splicing towards the 'readthrough' transcript was noticed in tumor cells but not in near-by endothelial cells, suggesting modified control over the splicing factors leading to AChE-R production in malignant, as opposed to benign cells. Shifted splicing is often associated with tumorogenicity; for example, metastatic melanoma cell lines lose their ability to express stem cell factor (SCF)-2 but retain their ability to express its alternatively spliced SCF-1 variant (Welker et al, 2000). Also, the VEGF 121 variant, when over-expressed in breast carcinoma cells, increased angiogenicity and tumorogenicity more than other VEGF splice variants (Zhang et al, 2000).…”
Section: Tumor Versus Vascular Cellsmentioning
confidence: 99%
“…Simultaneous expression of c-kit and SCF has been reported in colon, gastric, and lung cancer cell lines, in which a growth/migrationstimulating autocrine loop has been demonstrated (Bellone et al, 1997;DiPaola et al, 1997;Hassan et al, 1998). On the other hand, in melanomas and in breast and thyroid carcinomas a loss of expression of these molecules, in comparison with normal melanocytes and mammary or thyroid epithelium, has been described (Moretti et al, 1999;Natali et al, 1992Natali et al, , 1995Welker et al, 2000). The introduction of a c-kit expression vector in melanoma and breast cancer cell lines caused growth inhibition (Huang et al, 1996;Nishida et al, 1996).…”
Section: Esposito Et Almentioning
confidence: 99%
“…Melanoma cells are known to express c-kit, PDGF-R and Abl (Worm et al, 1993;Montone et al, 1997;Welker et al, 2000;Potti et al, 2003;Shen et al, 2003). Moreover, based on experimental in vitro data gained from melanoma cell lines, autocrine growth loop mechanisms were postulated for the receptor -ligand interaction of PDGF-R and PDGF, as well as of Kit and stem cell factor (SCF) (Harsh et al, 1990;DiPaola et al, 1997).…”
mentioning
confidence: 99%