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Microsatellite analysis in cutaneous malignant melanoma

Authors :
Carmelo Urso
Umberto Maria Reali
Iacopo Sardi
Lorenzo Borgognoni
Marco Santucci
Alessandro Franchi
Daniela Massi
Augusto Giannini
Adriana Salvadori
Source :
Melanoma Research. 12:577-584
Publication Year :
2002
Publisher :
Ovid Technologies (Wolters Kluwer Health), 2002.

Abstract

The status and relevance of repetitive nucleotide sequences or microsatellite alterations in sporadic cutaneous melanoma has not been fully clarified. In this study we evaluated the presence of microsatellite alterations in a series of sporadic primary and metastatic melanomas in order to discover which genetic events may have a pathogenetic role in the development of this disease. Tumour samples were obtained from 21 patients with sporadic cutaneous melanoma, and from eight corresponding positive sentinel lymph nodes and one corresponding in-transit metastasis. In each specimen, selected neoplastic cells were procured by laser-assisted microdissection. Polymerase chain reaction-based microsatellite analysis was performed using a panel of 11 microsatellite markers, located at chromosome 2p, 4q, 9p, 16q, 17p and 21q. Overall, we found microsatellite alterations in five (23.8%) melanomas. Of these, one case showed alteration at marker D2S2182 and one at marker D17S261, whereas in another case alterations at three loci, D2S2182, D2S2291 and D9S171, were found. The fourth patient demonstrated an alteration at locus D9S171 both in the primary tumour and in the histologically positive sentinel lymph node. The fifth case was characterized by alterations at D2S2182 and at D17S250, whereas the corresponding in-transit metastasis showed the same alterations as the primary tumour and an additional alteration at IFN alpha. In conclusion, our study confirms previous observations that cutaneous melanomas demonstrate microsatellite alterations, although such instability occurs at a lower frequency than specific mismatch repair defects. Genetic analysis of metastatic lesions revealed that the same microsatellite alterations as in the primary tumour are seen, but additional genetic changes may develop during disease progression.

Details

ISSN :
09608931
Volume :
12
Database :
OpenAIRE
Journal :
Melanoma Research
Accession number :
edsair.doi.dedup.....1c7f6f15837089867d7fecc2bfa0f79e
Full Text :
https://doi.org/10.1097/00008390-200212000-00007