Expression of leptin and its receptor in female breast cancer in relation with selected apoptotic markers.

Leptin and its receptor may be engaged in pathogenesis of breast cancer among various human tumors. In vitro investigations showed leptin-mediated escalation of estrogen synthesis and boosted activity of estrogen receptor ERalpha. Furthermore, leptin induced growth of malignant cells, counteracted a...

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Main Authors: Mariola Sulkowska, Luiza Kanczuga-Koda, Mariusz Koda, Katarzyna Jarzabek, Stanislaw Sulkowski
Format: Article
Language:English
Published: Via Medica 2008-04-01
Series:Folia Histochemica et Cytobiologica
Online Access:http://czasopisma.viamedica.pl/index.php/fhc/article/view/4483
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spelling doaj-514bbc123f5e4426a4a09239c55948c62020-11-24T23:40:12ZengVia MedicaFolia Histochemica et Cytobiologica0239-85081897-56312008-04-0145Suppl 118719110.2478/4483Expression of leptin and its receptor in female breast cancer in relation with selected apoptotic markers.Mariola SulkowskaLuiza Kanczuga-KodaMariusz KodaKatarzyna JarzabekStanislaw SulkowskiLeptin and its receptor may be engaged in pathogenesis of breast cancer among various human tumors. In vitro investigations showed leptin-mediated escalation of estrogen synthesis and boosted activity of estrogen receptor ERalpha. Furthermore, leptin induced growth of malignant cells, counteracted apoptosis and stimulated cell migration as well as overexpression of angiogenic factors and degrading enzymes that split network of intercellular matrix. On the other side, leptin has been reported to favor apoptosis, lately. Proapoptotic effect of leptin action was revealed in interstitial cells of bone marrow and adipocytes. Our past reports provide evidences for overexpression of leptin and its receptor in breast cancer in comparison with benign mammary lesions. In current study we aimed at assessment of eventual relationships between leptin, leptin receptor and selected protein regulators of apoptosis in breast cancer. We applied immunohistochemistry for leptin, leptin receptor, anti-apoptotic Bcl-2 and Bcl-xL as well as pro-apoptotic Bak and Bax expression assessment in 106 cases of human breast cancers. The immunoreaction was graded and statistically evaluated. Expression of leptin was positively correlated with Bcl-xL, Bak and Bax (p<0.001, r=0.614; p<0.001, r=0.518; p<0.001, r=0.511, respectively). Statistical significances were noted between expression of leptin receptor and Bcl-xL or Bax (p=0.011, r=0.210; p<0.001, r=0.313, respectively). No correlation was encountered between leptin and Bcl-2, either leptin receptor and Bcl-2 or leptin receptor and Bak. On the basis of obtained results, leptin system could interfere in balance among expressions of pro- and anti-apoptotic proteins and regulate cell turnover and--by means of it--facilitate breast cancer progression.http://czasopisma.viamedica.pl/index.php/fhc/article/view/4483
collection DOAJ
language English
format Article
sources DOAJ
author Mariola Sulkowska
Luiza Kanczuga-Koda
Mariusz Koda
Katarzyna Jarzabek
Stanislaw Sulkowski
spellingShingle Mariola Sulkowska
Luiza Kanczuga-Koda
Mariusz Koda
Katarzyna Jarzabek
Stanislaw Sulkowski
Expression of leptin and its receptor in female breast cancer in relation with selected apoptotic markers.
Folia Histochemica et Cytobiologica
author_facet Mariola Sulkowska
Luiza Kanczuga-Koda
Mariusz Koda
Katarzyna Jarzabek
Stanislaw Sulkowski
author_sort Mariola Sulkowska
title Expression of leptin and its receptor in female breast cancer in relation with selected apoptotic markers.
title_short Expression of leptin and its receptor in female breast cancer in relation with selected apoptotic markers.
title_full Expression of leptin and its receptor in female breast cancer in relation with selected apoptotic markers.
title_fullStr Expression of leptin and its receptor in female breast cancer in relation with selected apoptotic markers.
title_full_unstemmed Expression of leptin and its receptor in female breast cancer in relation with selected apoptotic markers.
title_sort expression of leptin and its receptor in female breast cancer in relation with selected apoptotic markers.
publisher Via Medica
series Folia Histochemica et Cytobiologica
issn 0239-8508
1897-5631
publishDate 2008-04-01
description Leptin and its receptor may be engaged in pathogenesis of breast cancer among various human tumors. In vitro investigations showed leptin-mediated escalation of estrogen synthesis and boosted activity of estrogen receptor ERalpha. Furthermore, leptin induced growth of malignant cells, counteracted apoptosis and stimulated cell migration as well as overexpression of angiogenic factors and degrading enzymes that split network of intercellular matrix. On the other side, leptin has been reported to favor apoptosis, lately. Proapoptotic effect of leptin action was revealed in interstitial cells of bone marrow and adipocytes. Our past reports provide evidences for overexpression of leptin and its receptor in breast cancer in comparison with benign mammary lesions. In current study we aimed at assessment of eventual relationships between leptin, leptin receptor and selected protein regulators of apoptosis in breast cancer. We applied immunohistochemistry for leptin, leptin receptor, anti-apoptotic Bcl-2 and Bcl-xL as well as pro-apoptotic Bak and Bax expression assessment in 106 cases of human breast cancers. The immunoreaction was graded and statistically evaluated. Expression of leptin was positively correlated with Bcl-xL, Bak and Bax (p<0.001, r=0.614; p<0.001, r=0.518; p<0.001, r=0.511, respectively). Statistical significances were noted between expression of leptin receptor and Bcl-xL or Bax (p=0.011, r=0.210; p<0.001, r=0.313, respectively). No correlation was encountered between leptin and Bcl-2, either leptin receptor and Bcl-2 or leptin receptor and Bak. On the basis of obtained results, leptin system could interfere in balance among expressions of pro- and anti-apoptotic proteins and regulate cell turnover and--by means of it--facilitate breast cancer progression.
url http://czasopisma.viamedica.pl/index.php/fhc/article/view/4483
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