Expression of 12-lipoxygenase as a biomarker for melanoma carcinogenesis

Expression of 12-lipoxygenase as a biomarker for melanoma carcinogenesis

12-Lipoxygenase (12-LOX), through its metabolite 12( )-hydroxyeicosatetraenoic acid [12( )-HETE], has been demonstrated to play a pivotal role in experimental melanoma invasion and metastasis, and 12-LOX expression may be important in early human melanoma carcinogenesis. We have studied the differen...

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Veröffentlicht in:Melanoma research 2002-09, Vol.12 (5), p.429-434
Hauptverfasser: Winer, I, Normolle, D P, Shureiqi, I, Sondak, V K, Johnson, T, Su, L, Brenner, D E
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Sprache:eng
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Arachidonate 12-Lipoxygenase - biosynthesis
Blood Platelets - enzymology
Humans
Image Processing, Computer-Assisted
Immunohistochemistry
Melanocytes - enzymology
Melanoma - diagnosis
Melanoma - enzymology
Nevus - enzymology
Precancerous Conditions
Skin Neoplasms - diagnosis
Skin Neoplasms - enzymology
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container_end_page 434
container_issue 5
container_start_page 429
container_title Melanoma research
container_volume 12
creator Winer, I
Normolle, D P
Shureiqi, I
Sondak, V K
Johnson, T
Su, L
Brenner, D E
description 12-Lipoxygenase (12-LOX), through its metabolite 12( )-hydroxyeicosatetraenoic acid [12( )-HETE], has been demonstrated to play a pivotal role in experimental melanoma invasion and metastasis, and 12-LOX expression may be important in early human melanoma carcinogenesis. We have studied the differences in 12-LOX protein expression during the progression of melanoma from human melanocytic cells to benign and dysplastic naevi to malignant metastatic disease. 12-LOX expression was determined in normal human skin melanocytes and in melanocytes found in compound naevi, dysplastic naevi and melanomas using a platelet-type 12-LOX antibody with a diaminobenzidine immunoperoxidase system detection system and was quantified using the analysis software NIH Image 1.62. Mean cellular pixel densities for 12-LOX staining ( = 50 cells/histological type) were unchanged in compound naevi ( = 0.14) and were increased in dysplastic naevi and melanomas compared with normal skin melanocytes ( = 0.03 and = 0.01, respectively). Similarly, melanomas had higher levels of expression compared with dysplastic naevi ( = 0.03). 12-LOX expression was significantly different between compound naevus and dysplastic naevus melanocytes ( = 0.01). These data suggest that 12-LOX may be an important novel marker for cancer progression within the melanoma system, and therefore could be a useful biomarker and therapeutic target for melanoma chemoprevention.
doi_str_mv 10.1097/00008390-200209000-00003
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We have studied the differences in 12-LOX protein expression during the progression of melanoma from human melanocytic cells to benign and dysplastic naevi to malignant metastatic disease. 12-LOX expression was determined in normal human skin melanocytes and in melanocytes found in compound naevi, dysplastic naevi and melanomas using a platelet-type 12-LOX antibody with a diaminobenzidine immunoperoxidase system detection system and was quantified using the analysis software NIH Image 1.62. Mean cellular pixel densities for 12-LOX staining ( = 50 cells/histological type) were unchanged in compound naevi ( = 0.14) and were increased in dysplastic naevi and melanomas compared with normal skin melanocytes ( = 0.03 and = 0.01, respectively). Similarly, melanomas had higher levels of expression compared with dysplastic naevi ( = 0.03). 12-LOX expression was significantly different between compound naevus and dysplastic naevus melanocytes ( = 0.01). 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We have studied the differences in 12-LOX protein expression during the progression of melanoma from human melanocytic cells to benign and dysplastic naevi to malignant metastatic disease. 12-LOX expression was determined in normal human skin melanocytes and in melanocytes found in compound naevi, dysplastic naevi and melanomas using a platelet-type 12-LOX antibody with a diaminobenzidine immunoperoxidase system detection system and was quantified using the analysis software NIH Image 1.62. Mean cellular pixel densities for 12-LOX staining ( = 50 cells/histological type) were unchanged in compound naevi ( = 0.14) and were increased in dysplastic naevi and melanomas compared with normal skin melanocytes ( = 0.03 and = 0.01, respectively). Similarly, melanomas had higher levels of expression compared with dysplastic naevi ( = 0.03). 12-LOX expression was significantly different between compound naevus and dysplastic naevus melanocytes ( = 0.01). 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subjects Arachidonate 12-Lipoxygenase - biosynthesis
Blood Platelets - enzymology
Humans
Image Processing, Computer-Assisted
Immunohistochemistry
Melanocytes - enzymology
Melanoma - diagnosis
Melanoma - enzymology
Nevus - enzymology
Precancerous Conditions
Skin Neoplasms - diagnosis
Skin Neoplasms - enzymology
title Expression of 12-lipoxygenase as a biomarker for melanoma carcinogenesis
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