Expression of the mast cell growth factor interleukin-3 in melanocytic lesions correlates with an increased number of mast cells in the perilesional stroma: Implications for melanoma progression Journal Article

  

Authors:	Reed, J. A.; Scott McNutt, N.; Bogdany, J. K.; Albino, A. P.
Article Title:	Expression of the mast cell growth factor interleukin-3 in melanocytic lesions correlates with an increased number of mast cells in the perilesional stroma: Implications for melanoma progression
Abstract:	The molecular events responsible for tumor progression in human cutaneous malignant melanoma remain unclear; however, critical to the process is the dysregulated proliferation of tumor cells and the development of new vascular channels which allow further growth and dissemination. Connective tissue mast cells (MC) have been implicated in tumor progression because they concentrate around tumors (including melanomas) prior to the formation of new blood vessels, and because they contain many chemical mediators, including basic fibroblast growth factor (bFGF), known to have mitogenic and angiogenic effects. Several MC chemotactic and mitogenic factors have been described including interleukin-3 (IL-3). In order to determine whether there is a differential expression of this MC chemotactic/mitogenic factor with tumor progression in vivo, we evaluated by immunohistochemistry 85 melanocytic lesions including primary invasive malignant melanoma (PIMM), melanoma in situ (MMIS), and ordinary intradermal benign melanocytic nevi (BMN) for expression of IL-3. Nucleic acid in situ hybridization also was used to evaluate the melanocytic lesions for IL-3-specific mRNA transcripts. Intracellular IL-3 protein was detected in 29/33 (88%) PIMM and 15/25 (60%) MMIS, but was not detected in any (0/27; 0%) BMN (p < 0.0001). IL-3-specific mRNA transcripts were present in 3/4 PIMM and 2/10 MMIS in which IL-3 protein was not identified, but were not detected in any BMN. IL-3 mRNA or protein was not detected in normal melanocytes present in the perilesional epidermis of any of the specimens studied. Immunohistochemistry also was used to confirm the presence of IL-3α-specific receptors on human cutaneous MC. As demonstrated by others, a significantly increased number of MC was present in the perilesional stroma of PIMM and MMIS vis a vis BMN (p < 0.0001). The results suggest that melanoma cells may attract MC in vivo by producing MC chemotactic/mitogenic factors such as IL-3. The recruitment of MC and the subsequent release of their potent mitogenic and angiogenic factors such as bFGF may thus represent a tumor-host interaction which favors tumor progression.
Keywords:	immunohistochemistry; human tissue; human cell; cell proliferation; melanoma; gene expression; skin neoplasms; epidermis; melanocyte; in situ hybridization; nevus, pigmented; rna, messenger; carcinoma in situ; stroma; cell count; neoplasm invasiveness; tumor growth; tumor vascularization; connective tissue; mast cell; mast cells; basic fibroblast growth factor; interleukin 3; interleukin-3; humans; human; article; interleukin 3 receptor; receptors, interleukin-3
Journal Title:	Journal of Cutaneous Pathology
Volume:	23
Issue:	6
ISSN:	0303-6987
Publisher:	John Wiley & Sons
Date Published:	1996-12-01
Start Page:	495
End Page:	505
Language:	English
DOI:	10.1111/j.1600-0560.1996.tb01441.x
PUBMED:	9001979
PROVIDER:	scopus
DOI/URL:	https://www.scopus.com/inward/record.uri?eid=2-s2.0-8044238369&doi=10.1111%2fj.1600-0560.1996.tb01441.x&partnerID=40&md5=3d9d378849e5ffb14369a341d78976f4
Notes:	Source: Scopus

https://synapse.mskcc.org/synapse/works/has_related_data_chk/119071