A study of transferrin and ferritin expression in tumor cells of patients with breast cancer

A study of transferrin and ferritin expression in tumor cells of patients with breast cancer

Aim: to study and to evaluate the clinical significance of the expression of iron-containing proteins ferritin and transferrin in tumor cells of patients with breast cancer (BC). Object and methods: the study included 143 patients with BC stage II–III. Methods: clinical, morphological and immunoh...

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Date:2014
Main Authors: Shepil, O.V., Lukyanova, N.Y., Chekhun, S.V., Polishchuk, L.Z., Antipova, S.V.
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Language:English
Published: Інститут експериментальної патології, онкології і радіобіології ім. Р.Є. Кавецького НАН України 2014
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Оригинальные исследования
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Cite this:A study of transferrin and ferritin expression in tumor cells of patients with breast cancer / O.V. Shepil, N.Y. Lukyanova, S.V. Chekhun, L.Z. Polishchuk, S.V. Antipova // Онкологія. — 2014. — Т. 16, № 2. — С. 108-112. — Бібліогр.: 35 назв. — англ.

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spelling nasplib_isofts_kiev_ua-123456789-1376242025-02-09T17:08:06Z A study of transferrin and ferritin expression in tumor cells of patients with breast cancer Дослідження експресії трансферину та феритину у пухлинних клітинах хворих на рак молочної залози Shepil, O.V. Lukyanova, N.Y. Chekhun, S.V. Polishchuk, L.Z. Antipova, S.V. Оригинальные исследования Aim: to study and to evaluate the clinical significance of the expression of iron-containing proteins ferritin and transferrin in tumor cells of patients with breast cancer (BC). Object and methods: the study included 143 patients with BC stage II–III. Methods: clinical, morphological and immunohistochemical, statistical. Results: it was shown that BC is characterized by intertumor heterogeneity of expression of transferrin and ferritin. The high degree of differentiation of BC correlates with the lack of expression of transferrin and ferritin. Positive expression of these proteins in the cells of primary tumors correlated with the development of metastases in regional lymphatic nodes. Correlation dependences between parameters of expression of transferrin and ferritin in tumor cells and overall survival in patients with BC have been determined. Conclusions: the expression of transferrin and ferritin may be individual predictive markers of clinical course and survival in patients with BC and one more molecular target for the development of new anticancer agents. Мета: вивчення експресії залізовмісних білків феритину (ФЕР) і трансферину (ТРФЕР) у пухлинних клітинах та оцінка її клінічного значення у хворих на рак молочної залози (РМЗ). Об’єкт і методи: у дослідження включено 143 пацієнток із РМЗ ІІ–ІІІ стадії. Методи дослідження: клінічні, морфологічний, імуногістохімічний, статистичний. Результати: показано, що РМЗ характеризується міжпухлинною гетерогенністю експресії ТРФЕР і ФЕР. Високий ступінь диференціювання РМЗ корелює з відсутністю експресії ТРФЕР і ФЕР. Позитивна експресія цих білків у клітинах первинної пухлини пов’язана з розвитком метастазів у регіонарних лімфатичних вузлах. Встановлено кореляційну залежність між експресією ТРФЕР та ФЕР у пухлинних клітинах і загальною виживаністю хворих на РМЗ. Висновки: експресія ТРФЕР і ФЕР може бути індивідуальним предиктивним маркером перебігу хвороби та виживаності пацієнток із РМЗ і ще однією молекулярною мішенню для розробки нових протипухлинних агентів. 2014 Article A study of transferrin and ferritin expression in tumor cells of patients with breast cancer / O.V. Shepil, N.Y. Lukyanova, S.V. Chekhun, L.Z. Polishchuk, S.V. Antipova // Онкологія. — 2014. — Т. 16, № 2. — С. 108-112. — Бібліогр.: 35 назв. — англ. https://nasplib.isofts.kiev.ua/handle/123456789/137624 en Онкологія application/pdf Інститут експериментальної патології, онкології і радіобіології ім. Р.Є. Кавецького НАН України
institution Digital Library of Periodicals of National Academy of Sciences of Ukraine
collection DSpace DC
language English
topic Оригинальные исследования
Оригинальные исследования
spellingShingle Оригинальные исследования
Оригинальные исследования
Shepil, O.V.
Lukyanova, N.Y.
Chekhun, S.V.
Polishchuk, L.Z.
Antipova, S.V.
A study of transferrin and ferritin expression in tumor cells of patients with breast cancer
Онкологія
description Aim: to study and to evaluate the clinical significance of the expression of iron-containing proteins ferritin and transferrin in tumor cells of patients with breast cancer (BC). Object and methods: the study included 143 patients with BC stage II–III. Methods: clinical, morphological and immunohistochemical, statistical. Results: it was shown that BC is characterized by intertumor heterogeneity of expression of transferrin and ferritin. The high degree of differentiation of BC correlates with the lack of expression of transferrin and ferritin. Positive expression of these proteins in the cells of primary tumors correlated with the development of metastases in regional lymphatic nodes. Correlation dependences between parameters of expression of transferrin and ferritin in tumor cells and overall survival in patients with BC have been determined. Conclusions: the expression of transferrin and ferritin may be individual predictive markers of clinical course and survival in patients with BC and one more molecular target for the development of new anticancer agents.
format Article
author Shepil, O.V.
Lukyanova, N.Y.
Chekhun, S.V.
Polishchuk, L.Z.
Antipova, S.V.
author_facet Shepil, O.V.
Lukyanova, N.Y.
Chekhun, S.V.
Polishchuk, L.Z.
Antipova, S.V.
author_sort Shepil, O.V.
title A study of transferrin and ferritin expression in tumor cells of patients with breast cancer
title_short A study of transferrin and ferritin expression in tumor cells of patients with breast cancer
title_full A study of transferrin and ferritin expression in tumor cells of patients with breast cancer
title_fullStr A study of transferrin and ferritin expression in tumor cells of patients with breast cancer
title_full_unstemmed A study of transferrin and ferritin expression in tumor cells of patients with breast cancer
title_sort study of transferrin and ferritin expression in tumor cells of patients with breast cancer
publisher Інститут експериментальної патології, онкології і радіобіології ім. Р.Є. Кавецького НАН України
publishDate 2014
topic_facet Оригинальные исследования
url https://nasplib.isofts.kiev.ua/handle/123456789/137624
citation_txt A study of transferrin and ferritin expression in tumor cells of patients with breast cancer / O.V. Shepil, N.Y. Lukyanova, S.V. Chekhun, L.Z. Polishchuk, S.V. Antipova // Онкологія. — 2014. — Т. 16, № 2. — С. 108-112. — Бібліогр.: 35 назв. — англ.
series Онкологія
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fulltext ОНКОЛОГИЯ • Т. 16 • № 2 • 2014 ОРИГИНАЛЬНЫЕ ИССЛЕДОВАНИЯ 108 INTRODUCTION Ferritin (FER) and transferrin (TRFER) belong to the iron-containing proteins involved in many physiolo- gical and pathological processes. According to the data of literature, iron-containing proteins play the main role in control of iron homeostasis in organism as well as in such biological processes as development of tissues, functional activity of cells, angiogenesis, proliferation and regu lation of cellular cycle, etc. [1–4]. Expression of genes involved in iron metabolism, including genes of TRFER, FER and ferroportin, is regulated by iron reg- ulatory proteins 1/2 (IRP1/2) on the posttranscription- al level [5, 6]. Interest in study of the role of iron-con- taining proteins in cancer patients is conditioned by their role in regulation of iron metabolism in the pre sence of malignant neoplasm in organism [7, 8]. In series of stu- dies, connections between changes in le vel of iron-con- taining proteins and progression of tumor, as well as in- creased DNA synthesis in tumor cells (TC), expression of angiogenic factors (VEGF), reaction of cells to the ox- idative stress, have been showed [9–11]. According to the results of numerous studies, FER is a cytoplasmic protein playing key role in intracellular iron homeostasis. At the same time, it can locate in cell nuclei, including tumor nuclei. This protein has many functions, particularly protection of cells from oxidative stress, re- gulatory role in transcription processes, and preservation of iron in bioactive and non-toxic forms [12–14]. Syn- thesis of intracellular FER is controlled on transcrip- tional and translational levels by two ways — iron-de- pendent and iron-independent [14]. FER is also known as proinflammatory mediator, expression of which can by induced by cytokines; however, it can induce expres- sion of both proinflammatory and antiinflammatory cy- tokines and be immunosuppressant [15]. Another one iron-containing protein TRFER, which main function consists in transfer and deli very of iron to the cells, belongs to the markers of malig- nant tumor phenotype, since it is associated with proliferation of cells. It has been clearly demonstra- ted by example of cancer and neuroendocrine car- cinomas of pancreatic gland: the highest expression of TRFER was in proliferating cells of both primary tumors and metastases [16]. Number of TRFER re- ceptors (TfR1 and TfR2-alpha) in proliferating cells of hepatoma compared with cells in dormancy incre- ases up to 300 and 200%, respectively [17]. Using com- parative immunohistochemical (IHC) studies of ex- pression of markers in tumor and normal cells, it has been showed that level and distribution of TRFER re- ceptor in tumors of other genesis (colorectal cancer) changes depending on stage of tumor process and tu- mor differentiation grade: high expression of TRFER receptors in cells of highly differentiated forms of can- cer at sta ges A and B by Dukes and lack/low expression in cells of low differentiated carcinomas with metas- tases at stage C or D [18]. Biological role of TRFER at tumor growth is confirmed also in study, in which was sta ted that TRFER receptors can have different regulatory properties and differentially be expressed in proli ferating cells compared with those being in dormancy [19]. Although interest in iron-containing proteins and their role in TC homeostasis significantly increased in recent years, number of studies on FER and TRFER in TC of mammary gland is insufficient. Our previous in vitro studies have showed that the most essential disorders of homeostasis of endoge- nous iron and increased level of FER and TRFER ex- pression are detected in TC of human mammary gland of the most aggressive mesenchymal phenotype and in cells A STUDy Of TRANSfERRIN AND fERRITIN EXPRESSION IN TUMOR CELLS Of PATIENTS WITh bREAST CANCER Summary. Aim: to study and to evaluate the clinical significance of the expression of iron-containing proteins ferritin and transferrin in tumor cells of patients with breast cancer (BC). Object and methods: the study included 143 patients with BC stage II–III. Methods: clinical, morphological and immunohistochemical, sta- tistical. Results: it was shown that BC is characterized by intertumor heteroge- neity of expression of transferrin and ferritin. The high degree of differentiation of BC correlates with the lack of expression of transferrin and ferritin. Positive ex- pression of these proteins in the cells of primary tumors correlated with the deve- lopment of metastases in regional lymphatic nodes. Correlation dependences be- tween parameters of expression of transferrin and ferritin in tumor cells and over- all survival in patients with BC have been determined. Conclusions: the expression of transferrin and ferritin may be individual predictive markers of clinical course and survival in patients with BC and one more molecular target for the develop- ment of new anticancer agents. O.V. Shepil1,2 N.Y. Lukyanova2 S.V. Chekhun2 L.Z. Polishchuk2 S.V. Antipova3 1Lugansk Regional Clinical Oncology Dispensary, Lugansk 2R.E. Kavetsky Institute of Experimental Pathology, Oncology and Radiobiology of NAS of Ukraine, Kyiv 3Lugansk State Medical University, Lugansk, Ukraine Key words: breast cancer, transferrin, ferritin, prognosis. ОРИГИНАЛЬНЫЕ ИССЛЕДОВАНИЯ 109ОНКОЛОГИЯ • Т. 16 • № 2 • 2014 109 with phenotype of treatment resistance to the antitumor drugs of different mechanism of action [20, 21]. Also, we have determined connection between FER level in blood serum and tumor tissue and sensitivity to neoadju- vant the rapy in patients with breast cancer (BC) [22, 23]. However, to date there is no consensus of opinion con- cerning significance of presence of these proteins for prognosis of clinical course and survival of BC patients. Aim of the study was to investigate the expression of iron-containing proteins FER and TRFER in TC of BC patients and to evaluate their clinical significance. ObjECT AND METhODS Retrospective analysis of the results of examination, treatment and survival of 143 BC patients of II–III stage, who have been receiving inpatient treatment on the ba- sis of Lugansk Regional Clinical Oncology Dispensary during 2005–2010, has been carried out. Stage of tumor process was determined according with the Internatio- nal clinical classification of tumors (TNM, 6th edition, 2002). Histological type of removed tumors was verified at morphological study of histological sections (staining with hematoxylin and eosin) according with the WHO International histological classification (2001). All pa- tients underwent adjuvant polychemotherapy (PCT) according with the standards of treatment approved in Ukraine by FAC or AC schemes with 21 day interval, number of PCT courses — 4–6. Postsurgical radiothe- rapy (RT) was carried out on gamma-therapeutic equip- ment «TERAGAM» (single focal dose 2 Gy, total focal dose 40 Gy) on the area of postsurgical scar, inguinal, parasternal and supraclavicular areas. For IHC study of FER and TRFER expression in TC, standard streptavidin-biotin-peroxidase me thod was applied. As primary were used antibodies speci fic to FER and TRFER (Abcam, USA). For visu alization of the results of reaction, reagent kit EnVision System, LSAB2 (Dako, Denmark) were used according with manufacturer’s recommendations; histological sec- tions were stained with Mayer hematoxylin. Evalua- tion of the results was carried out using optic micros- copy at magnification ×200. For evaluation of FER and TRFER expression, semi-quantitative method was applied. In each histological specimen, expression of markers in 1000 TC was analyzed determining quanti- ty of positive and negative cells in percentage and cal- culating level of expression of marker (high, moderate, strong). Strong positive expression of marker was con- sidered quantity of positive TC > 10% and strong/mo- derate expression of markers [24]. Statistical processing of the results of study was car- ried out using methods of variation statistics with use of program STATISTICA 6.0. For evaluation of signi- ficance of differences in expression of studied markers and other clinical-pathological parameters, χ2 was used. Evaluation of survival was carried out by Kaplan — Me ier me thod taking date of the beginning of treatment as re- ference point. Multivariate analysis was performed using Cox regression model and log-rank test. Correlation ana- lysis was carried out by calculation of Spearman corre- lation. Critical level of statistical significance was 0.05. RESULTS AND DISCUSSION General clinical characteristic of BC patients of II– III stage is given in Table 1. Age of patients varied from 25 to 76, mean age — 50.3 ± 4.3. The highest (27.1%) number of patients was in age interval 51–60. Most (61.5%) patients were in menopause. Part of BC patients of II stage has constituted 44.0%, III — 56.0%. Number of women with BC of IIa and IIb stages was almost equal and constituted 21.0 and 23.0%, respectively. Among pa- tients with III stage T3a (33.1%) was prevailed; stage T3b was detected in 22.9% of patients. In 22.4% of patients, no metastases in lymph nodes (LN) were detected, in 77.6% metastatic involvement of LN was diagnosed. Complex examination of patients (radiological, ultra- sound, laboratory), which was carried out before treat- ment, has not detected remote metastases. Morphologi- cal study of surgical material has showed that infiltrating duct cancer occurred more often (77.6%), than lobular cancer (22.4%); moderate tumor differentiation grade was determined in 42.6% of patients. Total number of tumors with positive TRFER and FER expression was the same in both groups and con- stituted 75 (52.4%) and 74 (51.4%), respectively. Here- after, TRFER and FER expression has been analyzed depending on such clinical features, as stage of disease, his- tological type of tumor and its differentiation grade, pre- sence/lack of metastases of cancer in regional LN, over- all survival (OS) of patients. No significant diffe rences in frequency of positive (+) tumors depending on stage and histological structure of BC was detected. In parti- cular, TRFER+ tumors were detected in 37 (58.7%) pa- tients with II stage and in 38 (60.3%) — with III stage; FER+ — in 33 (52.3%) and 41 (51.2%) patients corre- spondingly. TRFER+ were 57 (51.3%) samples of infil- trating duct cancer and 18 (56.25%) — infiltrating lobular cancer; FER+ — 58 (52.2%) and 16 (50%), respectively. In group of patients with high and moderate BC dif- ferentiation grade, number of tumors with positive ex- pression of TRFER and FER was lesser, than in patients with low differentiation grade (р < 0.05) (Table 2). Num- ber of tumors with positive expression of both markers turned out to be significantly higher (р < 0.05) in BC pa- tients with metastases in LN (Table 3). Results of correlation analysis are given in Table 4. No correlation between TRFER and FER expression and stage of BC and histological type of tumor has been determined. Also, it has been determined that TRFER/ FER negative expression correlates with high differen- tiation grade of tumors, and positive TRFER/FER ex- pression in primary tumor — with development of me- tastases in regional LN. No significant correlations be- tween TRFER and FER expression in samples of one tumor were detected (r = 0.10; p > 0.05) that points out at different ways of regulation of these proteins, which are quite complicated in TC, finally not determined and need further study [25]. ОНКОЛОГИЯ • Т. 16 • № 2 • 2014 ОРИГИНАЛЬНЫЕ ИССЛЕДОВАНИЯ 110 Table 1 General clinical characteristic of BC patients Index Number of patients n % Total number of patients 143 100 Menstrual cycle Preserved 55 38.5 Menopause 88 61.5 BC stage by TNM (category Т) ІІ (Т2) including Т2а Т2b 63 48 15 44.0 21.0 23.0 III (Т3) including Т3а Т3b 80 62 18 56.0 33.1 22.9 Metastases in regional LN (category N) N0 32 22.4 N1–3 111 77.6 Remote metastases (category М) М0 143 100.0 BC morphology Infiltrating duct cancer 111 77.6 Infiltrating lobular cancer 32 22.4 BC differentiation grade High 40 28.0 Moderate 61 42.6 Low 42 29.4 Methods of treatment Mastectomy by Madden + PCT 51 35.7 Mastectomy by Madden + PCT + RT 57 39.9 Mastectomy by Madden + RT 35 24.4 Table 2 Distribution of tumors by TRFER and FER expression depending on BC differentiation grade Differentiation grade Nu m be r o f t um or s wi th p os iti ve ex pr es si on o f T RF ER Nu m be r o f t um or s wi th n eg at iv e ex pr es si on o f T RF ER Nu m be r o f t um or s wi th p os iti ve ex pr es si on o f F ER Nu m be r o f t um or s wi th n eg at iv e ex pr es si on o f F ER n % n % n % n % High (n = 40/100.0%) 19 47.5 21 52.5 16 40.0 24 60.0 Moderate (n = 61/100.0%) 21 34.4 40 65.6 24 39.3 37 40.7 Low (n = 42/100.0%) 35 83.3 17 16.7 34 80.1 7 9.9 Total (n = 143/100.0%) 75 52.4 68 47.6 74 51.4 69 48.6 Using Kaplan — Meier method, 5-year OS of patients depending on TRFER and FER expression has been cal- culated. As data in Fig. 1 and 2 show, survival of BC pa- tients was higher at lack of TRFER and FER expression in remote tumors. Cox regression analysis conducted for determination of connections between TRFER and FER expression and OS rates of patients has showed that these proteins may be used as subsidiary predictive markers of BC prognosis (for TRFER β = −0.44; p < 0.05; for FER β = −0.29; p < 0.05). When analyzing obtained results and summarizing conducted study, one should mention that molecular and clinical aspects of changes in iron homeostasis in organism of patients and TC and their diagnostic va- lue are characterized by complexity of signal path- ways of expression of markers, which are connec ted with iron metabolism [25]. Significance of disorders of iron homeostasis for occurrence and progression of cancer diseases, including BC, is confirmed by data of numerous epidemiological and experimental stud- ies [1, 26–28]. Mechanisms of these disorders to date are not fully studied. There are data showing synergism of disorders of iron and estrogen metabolism at occur- rence of BC. In general, characteristic feature of TC is increased expression of proteins-importers and de- crease of level of proteins-exporters of iron [28]. Du- ring the process of carcinogenesis, excess of iron con- tributes to the formation of active oxy gen forms, which cause DNA damages. At the same time, estrogen can be additional substrate of these reactions due to attach- ment of hydroxyl group and formation of catechol es- trogen [28–30]. Compensatory protective mechanism, which contributes to the neutralization of free radi- cals and protection of DNA from damages caused by excess of iron, is increasing of FER level in TC. Di- sorders of estrogen metabolism on the background of excess of iron also cause stimulation of TRFER syn- thesis in TC of mammary gland. It is confirmed by ob- tained by us data and results of previous studies [22], which are the evidence of presence of increased level of FER and TRFER expression in more than 50% of studied tumors of mammary gland. Table 3 Distribution of tumors by TRFER and FER expression depending on presence of BC metastases in regional LN Category N Nu m be r o f t um or s wi th p os iti ve ex pr es si on o f T RF ER Nu m be r o f t um or s wi th n eg at iv e ex pr es si on o f T RF ER Nu m be r o f t um or s wi th p os iti ve ex pr es si on o f F ER Nu m be r o f t um or s wi th n eg at iv e ex pr es si on o f F ER n % n % n % n % N0 (n = 32/100.0%) 9 28.1 23 71.9 11 34.4 21 65.6 N1–3 (n = 111/100.0%) 66 59.5 45 40.5 63 56.8 48 43.2 Total (n = 143/100.0%) 75 52.4 68 47.6 74 51.4 69 48.6 Table 4 Correlation of expression of studied molecular markers with clinical and morphological features of BC Correlation pairs Correlation coefficient Evaluation of correlation TRFER expression Stage of disease 0.09 No correlation between TRFER/FER expression and stage of diseaseFER expression −0.02 TRFER expression Histologi- cal type of BC 0.06 No correlation between TRFER/FER expression and histological type of tumor FER expression 0.07 TRFER expression Differenti- ation grade of BC −0.39* Negative TRFER/FER ex- pression correlates with high differentiation grade of tumor FER expression −0.33* TRFER expression Metasta- ses in regional LN 0.48* Positive TRFER/FER ex- pression in primary tumor correlates with develop- ment of metastases in re- gional LN FER expression 0.31* *Level of significance of correlation coefficient р < 0.05. ОРИГИНАЛЬНЫЕ ИССЛЕДОВАНИЯ 111ОНКОЛОГИЯ • Т. 16 • № 2 • 2014 111 0,00 20,00 40,00 60,00 80,00 100,00 0,00 10,00 20,00 30,00 40,00 50,00 60,00 TRFER– TRFER+ Pa tie nt s, % Time, months fig. 1. OS of BC patients calculated by Kaplan — Meier me- thod depending on TRFER expression in TC 0,00 20,00 40,00 60,00 80,00 100,00 0,00 10,00 20,00 30,00 40,00 50,00 60,00 FER– FER+ Pa tie nt s, % Time, months fig. 2. OS of BC patients calculated by Kaplan — Meier me- thod depending on FER expression in TC Lack of correlation between level of TRFER and FER expression in TC of examined patients and stage and morphological structure of BC, probably, is con- nected with presence of additional factors of regulation of stu died proteins on the level of other systems of iron meta bolism in organism. Data obtained concerning high level of TRFER and FER expression in tumors of low diffe rentiation grade is confirmation of participation of these malignant proteins in proliferation, growth and for- mation of stage of BC malignancy. This is evidenced by the results of our previous in vitro studies concerning in- crease of expression of iron-containing proteins already in the early stages of malignant transformation of cells of mammary gland and intensification of evidence of these di sorders in the process of acquisition by them of more aggressive mesenchymal phenotype [20, 31]. Determined existence of connections between expres- sion of studied proteins and development of metastases in regional LN and survival of BC patients coincides with data of literature and confirms significance of disorders of iron metabolism for progression and aggressiveness of clinical course of BC, as well as confirms fact of cancer ferrotoxici- ty [32]. For instance, significant expression of TRFER and FER in TC of BC patients has been determined — 92.2% of tumors were positive, at that expression of marker di- rectly correlated with cancer metastases in LN and malig- nancy of neoplasms [26]. Expression of TRFER (TfR1) and FER receptors in TC of patients with non-small cell lung carcinoma was determined in 88 and 62% of tumors correspondingly [27], but no correlation between indexes of expression of these markers in cells and their concen- tration in peripheral blood was determined. Significance of iron-containing proteins in cancer patients has been demonstrated also in other studies [18, 19]. Since iron-containing proteins participate in proli- feration of cells and progression of tumors and are con- nected with some biological features of tumor growth and clinical prognosis, they may be considered mole cular targets for antitumor drugs [9, 33]. Possibility of such approach to the treatment of cancer patients has been showed in some experimental studies [34, 35], as well as is has been confirmed by the results of our previous studies, which have showed significant increase of ex- pression of iron-containing proteins in resistant to anti- tumor drugs cells of BC in vitro and TC of BC patients resistant to neoadjuvant chemotherapy [21, 22]. Thus, results of carried out study and data of liter- ature show that iron ions and iron-containing proteins play important role in metabolism of normal and neo- plastic cells, can be individual markers of predictive prog- nosis of survi val of BC patients. Data obtained can be the basis for deve lopment of new diagnostic criteria and im- provement of exi sting schemes of antitumor treatment taking into account indexes of TRFER and FER in TC of mammary gland. CONCLUSIONS 1. BC is characterized by intertumor heterogene- ity of TRFER and FER expression. Part of tumors with strong positive TRFER and FER expression has consti- tuted 52.4 і 51.4%, respectively. 2. No correlation between TRFER and FER expres- sion, on the one hand, and stage of disease and histolo- gical BC type, on the other hand, has been determined. 3. High differentiation grade of BC correlates (p < 0.05) with lack of TRFER and FER expression. 4. Positive TRFER and FER expression in cells of pri- mary tumor of mammary gland correlates with develop- ment of metastases in regional LN. 5. Prognostic value of TRFER and FER expression in TC of mammary gland for the evaluation of OS of pa- tients has been determined. TRFER and FER expression can be individual predictive marker of survival of BC pa- tients and one more molecular target for the development of new antitumor agents. REfERENCES 1. Knovich MA, Storey JA, lan g, et al. Ferritin for the clini- cian. Blood Rev 2009; 23 (3): 95–104. 2. Arosio P, Ingrassia r, cavadini P. Ferritins: a family of mo- lecules for iron storage, antioxidation and more. Biochim Biophys Acta 2009; 1790 (7): 589–99. 3. holmes-hampton gP, chakrabarti M, cockrell Al, et al. Changing iron content of the mouse brain during development. Metallomics 2012; (8): 761–70. 4. Saletta f, rahmanto yS, Siafakas Ar, richardson Dr. Cel- lular iron depletion and the mechanisms involved in the iron-de- pendent regulation of the growth arrest and DNA damage family of genes. J Biol Chem 2011; 286: 35396–406. ОНКОЛОГИЯ • Т. 16 • № 2 • 2014 ОРИГИНАЛЬНЫЕ ИССЛЕДОВАНИЯ 112 5. Torti fM, Torti SV. Regulation of ferritin genes and protein. Blood 2002; 99: 3505–16. 6. Styś A, galy b, Starzyński rr, et al. Iron regulatory protein 1 outcompetes iron regulatory protein 2 in Regulating Cellular Iron Homeostasis in Response to Nitric Oxide. Blood 2013; 122: 885–89. 7. callens c, coulonS, Naudin J, et al. Targeting iron homeosta- sis induces cellular differentiation and synergizes with diffe rentiating agents in acute myeloid leukemia. J Exp Med 2010; 207 (4): 731–50. 8. Torti SV, Torti fM. Ironing out cancer. Cancer Res 2011; 71 (5): 1511–4. 9. Eckard J, Dai J, wu J, et al. Effects of cellular iron deficien- cy on theformation of vascular endothelial growth factorand angio- genesis. Cancer Cell Internat 2010; 10: 28. 10. летягин вП, Тупицын нн, артамонова ев. Рецептор трасферина (CD71) на клетках рака молочной железы. Мол Мед 2007; (1): 16–21. 11. ермилова вд, Тупицын нн, артамонова ев и др. Новые иммунологические маркеры (СD71, LU-BCRU-G7), взаимосвязанные с прогнозом рака молочной железы. Совр Онкол 2001; (4): 161–163. 12. Alkhateeb AA, connor Jr. Nuclear ferritin: A new role for ferritin in cell biology. Biochim Biophys Acta 2010; 1800 (8): 793–7. 13. wang w, Knovich MA, coffman lg, et al. Serum ferritin: past, present and future. Biochim Biophys Acta 2010; 1800: 760–9. 14. Orino K, watanabe K. Molecular, physiological and clini cal aspects of the iron storage protein ferritin. Vet J 2008; 178 (2): 191– 201 (http://www.ncbi.nlm.nih.gov/pubmed/17764995)/ 15. rosário c, Zandman-goddard g, Meyron-holtz Eg, et al. The Hyperferritinemic Syndrome: macrophage activation syndrome, Still’s disease, septic shock and catastrophic antiphospholipid syn- drome. BMC Med 2013; 11: 185. 16. ryschich E, huszty g, Knaebel hP, et al. Transferrin recep- tor is a marker of malignant phenotype in human pancreatic can- cer and in neuroendocrine carcinoma of the pancreas. Eur J Can- cer 2004; 40 (9): 1418–22. 17. lee Aw, Oates PS, Trinder D. Effects of cell proliferation on the uptake of transferrin-bound iron by human hepatoma cells. Hepatology 2003; 38 (4): 967–77. 18. Prutki M, Poljak-blazi M, Jakopovic M, et al. Altered iron metabolism, transferrinreceptor 1 and ferritinin patients with co- lon cancer. Cancer Lett 2006; 238 (2): 188–96. 19. Daniels Tr, Delgado T, rodriguez JA, et al. Thetransfer- rin receptor part I: Biology and targeting with cytotoxic antibodies for the treatment of cancer. Clin Immunol 2006; 121 (2): 144–58. 20. Shpyleva SI, Tryndyak VP, Kovalchuk O, et al. Role of fer- ritin alterations in human breast cancer cells. Breast Cancer Res Treat 2011; 126 (1): 63–71. 21. chekhun Vf, lukyanova Ny, burlaka ар, et al. Iron metabolism disturbances in the MCF-7 human breast cancer cells with acquired re- sistance to doxorubicin and cisplatin. Int J Oncol 2013; 43 (5): 1481–6. 22. антіпова св, Шепіль Ов, лук’янова ню, Чехун вФ. Зв’язок рівня феритину в сироватці крові та пухлинній тканині з чутливістю до неоад’ювантної хіміотерапії у хворих на рак молочної залози. Онкология 2013; 15 (3): 204–9. 23. Чехун вФ, Шепіль Ов, лук’янова ню та ін. Cпосіб прогнозування чутливості до неоад’ювантної терапії у хворих на рак молочної залози. Патент № 84044 від 10.10.2013. Опубл. Бюл. № 19/2013. 24. gahlawat S, Marwah N, Singh S. Immunohistochemi- cal localization of Transferrin in breast lesions. Internet J Pathol 2008; 8(2). 25. Evstatiev r, gasche c. Iron sensing and signaling. Gut 2012; 61: 933–952. 26. Agarwal PK, Mehrotra A, chandra T, Singh K. Immuno- histochemical localization of transferring in human breast cancer tissue. Indian J Pathol Microbiol 2000; 43 (4): 441–7. 27. Kukulj S, Jaganjac M, boranic M, et al. Altered iron meta- bolism, inflammation, transferring receptors, and ferritin expression in non-small-cell lung cancer. Med Oncol 2010; 27 (2): 268–77. 28. Marques O, Martins da Silva b, Porto g, lopes c. Iron homeostasis in breast cancer. Cancer Letters 2014; 347 (1): 1–14. 29. Moore Ab, Shannon J, chen c, et al. Dietary and stored iron as predictors of breast cancer risk: a nested case-control study in Shangai. Int J Cancer 2009; 125: 1110–7. 30. cozzi A, corsi b, levi S, et al. Overexpression of wild type and mutated human ferritin H-chain in HeLa cells: in vivo role of ferritin ferroxidase activity. J Biol Chem 2000; 275: 25122–9. 31. Чехун вФ. Создание новых лекарственных форм на основе нанокомпозитных материалов для решения совр еменных про блем онкологии. Наносистеми, наноматеріали, нанотехнології 2011; 9 (1): 261–74. 32. Toyokuni S. Role of iron in carcinogenesis: Cancer as a fer- rotoxic disease. Cancer Sci 2009; 100: 9–16. 33. whitnall M, howard J, Ponka P, richardson Dr. A class of iron chelators with a wide spectrum of potent antitumor acti- vity that overcome resresistance to chemotherapeutics. Proc Natl Acad Sci USA 2006; 103 (40): 14901–6. 34. Kwok Jc, richardson Dr. Anthracyclines Induce Accu- mulation of iron in ferritin in myocardial and neoplastic cells: in- hibition of the ferritin iron mobilization pathway. Mol Pharmacol 2003; 63 (40): 849–61. 35. Koshkaryev A, Piroyan A, Torchilin VP. Increased apoptosis in cancer cells in vitro and in vivo by ceramides in transferrin-modi- fied liposomes. Cancer Biol Ther 2012; 13 (1): 50–60. ДОСЛІДЖЕННЯ ЕКСПРЕСІї ТРАНСФЕРИНУ ТА ФЕРИТИНУ У ПУхЛИННИх КЛІТИНАх хВОРИх НА РАК МОЛОЧНОї ЗАЛОЗИ O.В. Шепіль, Н.Ю. Лук’янова, С.В. Чехун, Л.З. Поліщук, C.В. Антіпова резюме. Мета: вивчення експресії залізовмісних білків феритину (ФЕР) і трансферину (ТРФЕР) у пухлинних клітинах та оцінка її клінічного значен- ня у хворих на рак молочної залози (РМЗ). Об’єкт і методи: у дослідження включено 143 пацієнток із РМЗ ІІ–ІІІ стадії. Методи дослідження: клі- нічні, морфологічний, імуногістохімічний, статис- тичний. Результати: показано, що РМЗ характе- ризується міжпухлинною гетерогенністю експресії ТРФЕР і ФЕР. Високий ступінь диференціюван- ня РМЗ корелює з відсутністю експресії ТРФЕР і ФЕР. Позитивна експресія цих білків у клітинах первинної пухлини пов’язана з розвитком мета- стазів у регіонарних лімфатичних вузлах. Вста- новлено кореляційну залежність між експресією ТРФЕР та ФЕР у пухлинних клітинах і загальною виживаністю хворих на РМЗ. Висновки: експресія ТРФЕР і ФЕР може бути індивідуальним предик- тивним маркером перебігу хвороби та виживанос- ті пацієнток із РМЗ і ще однією молекулярною мі- шенню для розробки нових протипухлинних агентів. Ключові слова: рак молочної залози, трансферин, феритин, прогноз. correspondence: Lukyanova N.Y. 45 Vasylkivska str., Kyiv 03022 R.E. Kavetsky Institute of Experimental Pathology, Oncology and Radiobiology of NAS of Ukraine Received: 25.03.2014

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