Is there an association between thyroid function abnormalities and breast cancer?

Angelousi, Anna; Diamanti-Kandarakis, Evanthia; Zapanti, Evangelia; Nonni, Afroditi; Ktenas, Eftuxios; Mantzou, Aimilia; Kontzoglou, Konstantinos; Kouraklis, Grigorios

doi:10.1590/2359-3997000000191

ABSTRACT

Objective

The aim of this study was to evaluate the association between thyroid function abnormalities and breast cancer and, in particular, the prognostic markers of breast cancer..

Subjects and methods

Baseline levels of thyrotropin, free triiodothyronine, free thyroxine and thyroid autoantibodies were measured in 97 women with primary breast cancer, 27 women with benign breast disease, and 4 women with atypical ductal hyperplasia. Their baseline levels were compared with those in 48 healthy women with a normal mammography in the last 2 years.

Results

There were no significant associations between history of thyroid disease and breast cancer (p = 0.33). The mean baseline levels of triiodothyronine and thyrotropin did not differ significantly between the compared groups. The mean baseline levels of free thyroxine were found to be significantly higher in the breast cancer group, even after adjusting for thyroid replacement therapy. The presence of thyroid antibodies did not differ significantly between the compared groups. In a subgroup analysis, breast cancer cases with thyroid disease and particularly hypothyroidism had a significantly lower incidence of lymph node metastases compared with breast cancer cases without thyroid disease.

Conclusions

Our data confirmed the proliferative effect of thyroid hormones on breast cells, which had previously been shown in vitro. Additionally, thyroid disease and particularly hypothyroid function appeared to be associated with a lower incidence of lymph node metastases. Further studies to determine the prognostic role of thyroid hormones in breast cancer are warranted.

Breast cancer; hypothyroidism; hyperthyroidism; thyroid antibodies

INTRODUCTION

Thyroid hormones are involved in regulating mammalian development, cellular differentiation and metabolism (¹1. Ditsch N, Liebhardt S, Von Koch F, Lenhard M, Vogeser M, Spitzweg C, et al. Thyroid function in breast cancer patients. Anticancer Res. 2010; 30:1713-7.). High affinity binding sites for 3-3-5 triiodothyronine (T3) have been identified in nuclei isolated from human tumors, including those in breast cancer (BC), suggesting that thyroid hormones may play a role in the development of BC at the cellular level (²2. Lemaire M, Baugnet-Mahieu L. Nuclear thyroid hormone receptors in human cancer tissues. Anticancer Res. 1986;6:695-700.).

Recent studies in human breast cancer cells lines (MCF-7 and MDA-MB-231) have shown proliferative effects of thyroid hormones on breast tissue through the same signal cascade utilized by estrogens involving phosphoinositol 3-kinase (PI3K) and the mitogen-activated protein kinase (MAPK) (³3. Nogueira CR, Brentani MM. Triiodothyronine mimics the effects of estrogen in breast cancer cell lines. J Steroid Biochem Mol Biol. 1996;59:271-9.). In estrogen receptor positive (ER+) cell lines (MCF-7), T3 mimics estradiol via its binding to ER and induces the expression of progesterone receptor (PR) and growth factor-alpha (TGF-α) mRNAs (³3. Nogueira CR, Brentani MM. Triiodothyronine mimics the effects of estrogen in breast cancer cell lines. J Steroid Biochem Mol Biol. 1996;59:271-9.). In other human cell lines, T3 has been shown to have a mitogenic effect by increasing the expression of the epithelial growth factor receptor (EGF-r) gene (⁴4. Humes HD, Cieslinski DA, Johnson LB, Sanchez IO. Triiodothyronine enhances renal tubule cell replication by stimulating EGF receptor gene expression. Am J Physiol. 1992;262:540-5.). In mammary cells, T3 can also activate the estrogen response element (ERE) (⁵5. Hall LC, Salazar EP, Kane SR, Liu N. Effects of thyroid hormones on human breast cancer cell proliferation. J Steroid Biochem Mol Biol. 2008;109:57-66.), which is necessary for gene transcription and cell proliferation. Similarly, thyroxine (T4), much like estradiol, can activate the MAPK pathway and thus promote cell proliferation (⁶6. Tang HY, Lin HY, Zhang S, Davis FB, Davis PJ. Thyroid hormone causes mitogen-activated protein kinase-dependent phosphorylation of the nuclear estrogen receptor. Endocrinology. 2004;145:3265-72.). Additionally, thyroid stimulating hormone (TSH) has been shown to have a direct effect on mammary cells. Recently, TSH receptors have been identified in BC tissue with the use of RT-PCR and were correlated to a lower grade of BC (⁷7. Oh HJ, Chung JK, Kang JH, Kang WJ, Noh DY, Park IA, et al. The relationship between expression of the sodium/iodide symporter gene and the status of hormonal receptors in human breast cancer tissue. Cancer Res Treat. 2005;37:247-50.).

The potential correlation between thyroid disease and BC was based on the existence of common pathophysiological mechanisms in both glands. Thyroid hyperoxidase (TPO) and lactoperoxidase are immunologically similar enzymes that have been identified in both thyroid and breast tissue (⁸8. Turken O, NarIn Y, DemIrbas S, Onde ME, Sayan O, Kandemir EG, et al. Breast cancer in association with thyroid disorders. Breast Cancer Res. 2003;5:110-3.,⁹9. Giani C, Fierabracci P, Bonacci R, Gigliotti A, Campani D, De Negri F, et al. Relationship between breast cancer and thyroid disease: relevance of autoimmune thyroid disorders in breast malignancy. J Clin Endocrinol Metab. 1996;81:990-94.). Sodium-iodide symporter (NIS) (¹⁰10. Dohán O, Carrasco N. Advances in Na(+)/I(-) symporter (NIS) research in the thyroid and beyond. Mol Cell Endocrinol. 2003;213:59-70.) is an intrinsic plasma membrane glucoprotein of thyroid follicular cells that is also expressed physiologically in lactating breast tissue (¹¹11. Tazebay UH, Wapnir IL, Levy O, Dohan O, Zuckier LS, Zhao QH, et al. The mammary gland iodide transporter is expressed during lactation and in breast cancer. Nat Med. 2000;6:871-8.) as well as in BC in some cases (¹²12. Wapnir IL, van de Rijn M, Nowels K, Amenta PS, Walton K, Montgomery K, et al. Immunohistochemical profile of the sodium/iodide symporter in thyroid, breast, and other carcinomas using high density tissue microarrays and conventional sections. J Clin Endocrinol Metab. 2003;88:1880-8.,¹³13. Rudnicka L, Sińczak A, Szybiński P, Huszno B, Stachura J. Expression of the Na(+)/I(-) symporter in invasive ductal breast cancer. Folia Histochem Cytobiol. 2003;41:37-40.). Despite this pre-clinical evidence, there is a lack of robust clinical evidence on the association between BC and thyroid function abnormalities. The aim of this single-center case control study was to evaluate the association between thyroid function abnormalities and BC and, in particular, the prognostic markers of BC.

SUBJECTS AND METHODS

Patient characteristics

One hundred thirty-three women with mammographic abnormalities were evaluated in the 2^nd Surgical Department of the University of Athens (Greece) between June 2010 and March 2014; the women were evaluated before receiving any surgery or medical treatment (chemo and/or radiotherapy). All patients underwent fine needle aspiration of suspicious lesions followed by surgery. Three patients were excluded because of recurrence of known BC, and 2 patients were excluded because of a histological diagnosis of melanoma and sarcoma.

Our cohort consisted of 97 cases of primary BC, 27 cases of benign breast disease (BBD), primarily fibroadenomas and fibrocystic disease, and 4 cases of atypical ductal hyperplasia. Seventy-eight of the 97 cases with BC were diagnosed with ductal breast cancer; 75 cases (77.3%) were invasive ductal breast cancer, 3 (3.1%) were ductal in situ cancer (DCIS), and 19 (19.6%) were lobular infiltrating breast cancer. BC tumors were classified according to the Nottingham grading system and the American Joint Committee on Cancer stages. Fifty-nine (61%) of the 97 BC cases were grade I, 28 cases (29%) were grade II, and 10 cases (10%) were grade III. Three (3%) cases had stage 0 tumors (in situ), 44 (45.4%) had stage I, 29 (30%) had stage II, and 21 (21.6%) had stage III tumors. Seventy-five cases (77.6%) with primary BC showed positive ER and PR.

The control group consisted of 48 non-hospitalized healthy women who were recruited from the family members of the patients in the geriatric clinic of our hospital. All women were from the same geographical area as the cases, and they were required to have had a normal mammogram within the past 2 years.

Women (cases and controls) with a personal history of a previous cancer were excluded from the study. History of thyroid disease was retrieved from the patient’s medical records and/or patient history.

Written informed consent was obtained for each patient and control. The protocol of the study was reviewed and approved by the scientific board of the institutional research committee (Laiko hospital, University of Athens) and was in accordance with the international ethical standards (Declaration of Helsinski).

Laboratory measurements

Thyroid function tests were performed before surgery or treatment for breast cancer. TSH (normal range: 0.3-4.0 mU/L) was measured with the double enzyme radioimmunoassay (RIA) ‘sandwich’ method (TSH-DiaSorin – CTK-3 Kit, Italy). Free thyroxine (fT4) (normal range: 10-25 pmol/L) and free triiodothyronine (fT3) (normal range: 2.3-5.3 pg/mL) were measured in serum using the double enzyme radioimmunoassay ‘sandwich’ method (ThermoScientific kit, USA). Autoantibodies against thyroglobulin (Tg-Abs) (positivity > 10 mU/L) and thyroid peroxidase (TPO-Abs) (positivity > 50 mU/L) were measured with RIA (ThermoScientific kit, USA). All TSH, fT3, fT4, TPO-Abs and Tg-Abs measurements were performed in the biochemical laboratory of the ‘Laiko’ hospital in Athens, Greece. The TSH receptor antibodies (TRAK) (positivity > 2 U/L) were measured with the receptor radioassay (RRA) method (Thermo Fisher-BRAHMS 101.5 kit, Germany) in the endocrinology laboratory of Evgenidion hospital in Athens, Greece.

Immunohistochemistry

ER and PR expression were immunohistochemically detected with the commercially available ER (clone EP1) and PR antibodies (clone PgR636) (DAKO), according to ASCO recommendations (¹⁴14. Pathologists’ Guideline Recommendations for Immunohistochemical Testing of Estrogen and Progesterone Receptors in Breast Cancer. Breast Care. 2010;5:185-7.).

Statistical analysis

Continuous variables were initially evaluated with the Kolmogorov-Smirnov test. Variables with a normal distribution were evaluated using ANOVA. Variables without a normal distribution (values of fT3, fT4, TSH, TPO-Abs, Tg-Abs, and TRAK) were analyzed using the Kruskall-Wallis test. The categorical parameters were evaluated with Chi-Square test. The results were considered significant at p < 0.05 (95% CI). Cases with atypical ductal hyperplasia (n = 4) were excluded from the statistical analysis because of their small sample size. Statistical analyses were performed using SPSS software (version 20).

RESULTS

The clinical and epidemiological characteristics of the participants are summarized in Table 1. The 3 groups (controls, BC cases and BBD cases) differed significantly in mean age, age of menarche, menopausal status and alcohol use.

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Table 1
Epidemiological characteristics of the studied population

Association between history of thyroid disease and histopathological parameters of breast tissue

The overall frequency of self-reported thyroid disease was 32 of 97 (33%) BC cases, 8 of 27 (29.6%) BBD cases, 3 of 4 (75%) patients in the atypical ductal hyperplasia group and 22 of 48 (45.8%) controls. History of thyroid disease did not significantly differ between the compared groups (p = 0.33) (Table 2). Autoimmune thyroid disease (Hashimoto’s) and goiter were the most frequent thyroid diseases in the studied groups. Hashimoto’s disease was more frequent in the controls than in the BC cases, whereas goiter was more frequent in BC cases than in controls; however, a statistical analysis was not possible because of the small sample size.

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Table 2
Frequency of thyroid disorders and thyroid treatment in controls, BC and BBD cases

Twenty-one of the 97 patients in the BC group (22%), 7 of 27 in the BBD group (26%) and 7 of 47 (15%) in the control group reported levothyroxine treatment at the time of screening. The statistical analysis found no significant differences concerning levothyroxine treatment between the compared groups (p = 0.79). Three cases reported use of antithyroid drugs in the past, and one case reported treatment with iodide (I¹³¹).

Association between thyroid function tests and histopathological parameters of breast tissue

The mean baseline values of TSH were 2.37 ± 2.3, 2.07 ± 1.04, 1.88 ± 1.07 and 2.05 ± 1.6 mU/L in the BC, BBD, atypical ductal hyperplasia and controls groups, respectively. Abnormally high levels of TSH (> 4.0 mU/L) were recorded in 15.3% of the BC cases and in 5% of the BBD cases. None of the controls had abnormally high levels of TSH. Abnormally low levels of TSH (< 0.3 mU/L) were recorded in 2.6% of the BC cases and in 2% of the controls. None of the BBD patients had abnormally low levels of TSH. No significant association was found between the mean levels of TSH (p = 0.757) of the compared groups, although BC cases showed slightly higher mean levels of TSH than the other groups (Table 3).

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Table 3
Mean baseline levels of thyroid hormones (fT3, fT4) and of TSH in controls, BC and BBD cases

The mean baseline values of fT3 were 3.18 ± 0.74, 3.11 ± 0.83, 3.33 ± 0.37 and 3.47 ± 1.93 pg/mL in the BC, BBD, atypical ductal hyperplasia and controls groups, respectively. Abnormally low levels (< 2.3 pg/mL) of fT3 were recorded in 10% of the BC cases, 6% of the BBD cases and in 12% of the controls. Abnormally higher levels of fT3 (> 5.3 pg/mL) were recorded in only 2% of the controls. None of the cases (BC and BBD) had abnormally higher levels of fT3. No significant association was found between the compared groups’ mean values of fT3 (p = 0.622) (Table 3).

The mean baseline values of fT4 were 17.2 ± 3.28, 16.9 ± 3.29, 18.38 ± 2.8 and 15.5 ± 3.76 pmol/L in the BC, BBD, atypical ductal hyperplasia and control groups, respectively. All BC cases and controls had normal levels of fT4. The mean values of fT4 were significantly higher in the BC group than in the other groups (p = 0.035). This statistical significance, although attenuated (p = 0.055), remained present when patients with levothyroxine treatment were excluded.

Association between thyroid autoantibodies and histopathological parameters of breast tissue

The frequency of positive TPO-Abs was 21.4% in the BC group, 33.3% in the BBD group, and 18% in controls. Positive Tg-Abs were found in 65% of the cases in the BC group, 55.5% in the BBD group and 16.6% in the control group. The levels of TPO-Abs and Tg-Abs did not significantly differ between the compared groups (p = 0.43 for TPO-Abs and p = 1.00 for Tg-Abs) (Table 4). The tests for TRAK antibodies were negative for the whole study population (cases and controls) (positivity > 2 U/L). The mean values of TRAK did not differ significantly (p = 0.42) between the groups.

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Table 4
Frequency and mean baseline values of thyroid autoantibodies in the compared groups

Association between thyroid function and hormone dependent BC (ER and/or PR positivity)

Fifty-nine BC cases out of a total of 76 (77.6%) were found positive for estrogen and/or progesterone receptors through immunohistochemistry analysis (Table 5). Statistical analysis found no significant differences in the prevalence of history of thyroid disease between the hormone-dependent and hormone-independent BC cases (p = 0.47). Further analyses (not shown in Table 5) did not show any significant difference between hormone-dependent BC and positive thyroid autoantibodies (7 out of 25 hormone-dependent BC cases were positive for TPO-Abs, p = 0.15 and 6 of 11 hormone-dependent BC cases had positive Tg-Abs, p = 1.00) nor between the mean levels of thyroid hormones (p = 0.486 for TSH levels, p = 0.229 for fT3 levels and p = 0.15 for fT4 levels) and hormone-dependent BC.

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Table 5
Frequency of history of thyroid disease in the differenent T, N stages, the different grades (I, II, III) and the ER/PR positive BC

Association between thyroid disease and tumor size, nodal involvement or grading of BC

BC cases with a self-reported history of thyroid disease presented less frequently with lymph node infiltration (pN) than the BC cases without history of thyroid disease (p = 0.035) (Table 5). The frequency of primary hypothyroidism in BC cases with lymph node infiltration was 37.8% (2 patients with Hashimoto’s and 1 with primary hypothyroidism out of 8 cases) and was 47.6% (7 patients with Hashimoto’s and 3 with primary hypothyroidism out of 21 cases) in BC cases without lymph node infiltration.

BC cases with tumors with lymph node infiltration presented lower mean TSH levels and higher fT4 levels (mean value of TSH = 1.97 ± 1.4 mU/L, of fT3 = 3.37 ± 0.78 pg/mL and of fT4 = 17.68 ± 3.16 pmol/L) than the tumors without lymph node infiltration (mean value of TSH = 3.99 ± 1.0 mU/L, of fT3 = 3.09 ± 0.66 pg/mL and of fT4 = 16.33 ± 3.5 pmol/L), although there were no significant differences (p = 0.148 for TSH, p = 0.26 for fT3 and p = 0.113 for fT4). Due to the small sample of the T4 stage (n = 3), the corresponding statistical analyses were not performed.

The presence of positive thyroid autoantibodies was not significantly associated with the pT stage of BC (p = 0.31 for TPO-Ab and p = 1.0 for Tg-Ab), the pN stage of BC (p = 0.87 for TPO-Ab and p = 0.76 for Tg-Ab), nor the grade of BC (p = 0.803 for TPO-Ab and p = 0.348 for Tg-Ab (Table 5).

DISCUSSION

The present study showed that the mean baseline levels of fT4 were significantly higher in BC cases than in controls and patients with BBD. Additionally, history of thyroid disease was associated with a significantly lower frequency of lymph node metastases in BC cases. Recent data have shown that BC remains one of the most common cancers worldwide, with an estimated incidence of 464,000 new BC cases per 3.45 million new cases of cancer in Europe (¹⁵15. Ferlay J, Steliarova-Foucher E, Lortet-Tieulent J, Rosso S, Coebergh JW, Comber H, et al. Cancer incidence and mortality patterns in Europe: estimates for 40 countries in 2012. Eur J Cancer. 2013;49:1374-403.).

Previous studies are consistent with our results, showing no significant association between history of thyroid disease and histopathological characteristics of breast diseases (¹1. Ditsch N, Liebhardt S, Von Koch F, Lenhard M, Vogeser M, Spitzweg C, et al. Thyroid function in breast cancer patients. Anticancer Res. 2010; 30:1713-7.,¹⁶16. Michalaki V, Kondi-Pafiti A, Gennatas S, Antoniou A, Primetis H, Gennatas C. Breast cancer in association with thyroid disorders. J BUON. 2009;14:425-8.

17. Goldman MB, Monson RR, Maloof F. Cancer mortality in women with thyroid disease. Cancer Res. 1990;50:2283-9.

18. Kalache A, Vessey MP, McPherson K. Thyroid disease and breast cancer: findings in a large case-control study. Br J Surg. 1982;69:434-5.

19. Simon MS, Tang MT, Bernstein L, Norman SA, Weiss L, Burkman RT, et al. Do thyroid disorders increase the risk of breast cancer? Cancer Epidemiol Biomarkers Prev. 2002;11:1574-8.-²⁰20. Hoffman DA, McConahey WM, Brinton LA, Fraumeni JF Jr. Breast cancer in hypothyroid women using thyroid supplements. JAMA. 1984;251:616-19.). Nevertheless, other studies have demonstrated a higher (⁸8. Turken O, NarIn Y, DemIrbas S, Onde ME, Sayan O, Kandemir EG, et al. Breast cancer in association with thyroid disorders. Breast Cancer Res. 2003;5:110-3.,²¹21. Kuijpens JL, Nyklíctek I, Louwman MW, Weetman TA, Pop VJ, Coebergh JW. Hypothyroidism might be related to breast cancer in post-menopausal women. Thyroid. 2005;15:1253-9.,²²22. Muller I, Pinchera A, Fiore E, Belardi V, Rosellini V, Giustarini E. High prevalence of breast cancer in patients with benign thyroid diseases. J Endocrinol Invest. 2011;34:349-52.) or a lower incidence of thyroid disease in BC cases (²³23. Cristofanilli M, Yamamura Y, Kau SW, Bevers T, Strom S, Patangan M, et al. Thyroid hormone and breast carcinoma. Primary hypothyroidism is associated with a reduced incidence of primary breast carcinoma. Cancer. 2005;103:1122-8.). Hashimoto’s disease, with or without positive thyroid antibodies (TPO-Abs and Tg-Abs), has been shown to be associated with an increased risk of BC (⁸8. Turken O, NarIn Y, DemIrbas S, Onde ME, Sayan O, Kandemir EG, et al. Breast cancer in association with thyroid disorders. Breast Cancer Res. 2003;5:110-3.,⁹9. Giani C, Fierabracci P, Bonacci R, Gigliotti A, Campani D, De Negri F, et al. Relationship between breast cancer and thyroid disease: relevance of autoimmune thyroid disorders in breast malignancy. J Clin Endocrinol Metab. 1996;81:990-94.,²⁴24. Jiskra J, Barkmanova J, Limanova Z, Lánská V, Smutek D, Potlukova E, et al. Thyroid autoimmunity occurs more frequently in women with breast cancer compared to women with colorectal cancer and controls but it has no impact on relapse-free and overall survival. Oncol Rep. 2007;18:1603-11.

25. Giustarini E, Pinchera A, Fierabracci P, Roncella M, Fustaino L, Mammoli C, et al. Thyroid autoimmunity in patients with malignant and benign breast diseases before surgery. Eur J Endocrinol. 2006;154:645-9.

26. Hardefeldt PJ, Eslick GD, Edirimanne S. Benign thyroid disease is associated with breast cancer: a meta-analysis. Breast Cancer Res Treat. 2012;133:1169-77.-²⁷27. Smyth PP, Shering SG, Kilbane MT, Murray MJ, McDermott EW, Smith DF, et al. Serum thyroid peroxidase autoantibodies, thyroid volume, and outcome in breast carcinoma. J Clin Endocrinol Metab. 1998;83:2711-6.) and, according to some studies, with a better prognosis and increased disease-free survival in BC cases (¹⁶16. Michalaki V, Kondi-Pafiti A, Gennatas S, Antoniou A, Primetis H, Gennatas C. Breast cancer in association with thyroid disorders. J BUON. 2009;14:425-8.,²⁸28. Tosovic A, Becker C, Bondeson AG, Bondeson L, Ericsson UB, Malm J, et al. Prospectively measured thyroid hormones and thyroid peroxidase antibodies in relation to breast cancer risk. Int J Cancer. 2012;131:2126-33.). In our study, it seemed that Hashimoto’s disease was not associated with BC; however, the small sample size precluded any definitive conclusions.

Our data showed that the mean baseline levels of fT4 were significantly higher in BC cases compared with the other groups, which is consistent with other studies in the literature (¹1. Ditsch N, Liebhardt S, Von Koch F, Lenhard M, Vogeser M, Spitzweg C, et al. Thyroid function in breast cancer patients. Anticancer Res. 2010; 30:1713-7.,²⁹29. Takatani O, Okumoto T, Kosano H, Nishida M, Hiraide H, Tamakuma S. Relationship between the levels of serum thyroid hormones or estrogen status and the risk of breast cancer genesis in Japanese women. Cancer Res. 1989;49:3109-12.). This correlation was sustained after exclusion of patients with levothyroxine treatment. Recently, it was found that fT4 levels in women without known thyroid disease and levothyroxine treatment were positively associated with risk of breast cancer, particularly in women with a BMI > 25 (²⁸28. Tosovic A, Becker C, Bondeson AG, Bondeson L, Ericsson UB, Malm J, et al. Prospectively measured thyroid hormones and thyroid peroxidase antibodies in relation to breast cancer risk. Int J Cancer. 2012;131:2126-33.). However, hypothyroidism and low levels of fT4 (²¹21. Kuijpens JL, Nyklíctek I, Louwman MW, Weetman TA, Pop VJ, Coebergh JW. Hypothyroidism might be related to breast cancer in post-menopausal women. Thyroid. 2005;15:1253-9.) or only low levels of fT4 with normal TSH have also been shown to be related to an increased risk of BC risk in women (²⁹29. Takatani O, Okumoto T, Kosano H, Nishida M, Hiraide H, Tamakuma S. Relationship between the levels of serum thyroid hormones or estrogen status and the risk of breast cancer genesis in Japanese women. Cancer Res. 1989;49:3109-12.).

As with fT4 levels, there have been reports suggesting an association of higher (¹1. Ditsch N, Liebhardt S, Von Koch F, Lenhard M, Vogeser M, Spitzweg C, et al. Thyroid function in breast cancer patients. Anticancer Res. 2010; 30:1713-7.,³⁰30. Tosovic A, Bondeson AG, Bondeson L, Ericsson UB, Manjer J. Triiodothyronine levels in relation to mortality from breast cancer and all causes: a population-based prospective cohort study. Eur J Endocrinol. 2013;168:483-90.) or lower levels of fT3 with risk of BC (²⁹29. Takatani O, Okumoto T, Kosano H, Nishida M, Hiraide H, Tamakuma S. Relationship between the levels of serum thyroid hormones or estrogen status and the risk of breast cancer genesis in Japanese women. Cancer Res. 1989;49:3109-12.,³¹31. Perry M, Goldie DJ, Self M. Thyroid function in patients with breast cancer. Ann R Coll Surg Engl. 1978;60:290-3.,³²32. Rose DP, Davis TE. Plasma thyronine levels in carcinoma of the breast and colon. Arch Intern Med. 1981;141:1161-4.). Surprisingly, we found no significant association between the mean baseline levels of fT3 and BC. One possible explanation for this result could be the short half-life of fT3 compared to fT4, which makes fT3 a less reliable marker of thyroid function. Another potential reason could be the circadian rhythm and periodicity concerning TSH and fT3 levels in particular. This circadian variation is not as evident in fT4 levels (³³33. Russell W, Harrison RF, Smith N, Darzy K, Shalet S, Weetman AP, et al. Free triiodothyronine has a distinct circadian rhythm that is delayed but parallels thyrotropin levels. J Clin Endocrinol Metab. 2008;93:2300-6.).

The mean baseline levels of TSH were not found to be significantly different between groups. Although there have been data associating low baseline levels of TSH (< 0.5 mU/l) in patients without known thyroid disease or treatment with a significantly increased risk of lung and prostate cancer, this association in BC has not been clearly demonstrated (³⁴34. Hellevik AI, Asvold BO, Bjøro T, Romundstad PR, Nilsen TI, Vatten LJ. Thyroid function and cancer risk: a prospective population study. Cancer Epidemiol Biomarkers Prev. 2009;18:570-4.).

The association between positive thyroid autoantibodies and BC has been largely discussed in the literature (³⁵35. Sandhu MK, Brezden-Masley C, Lipscombe LL, Zagorski B, Booth GL. Autoimmune hypothyroidism and breast cancer in the elderly. Breast Cancer Res Treat. 2009;115:635-41.,³⁶36. Brinton LA, Hoffman DA, Hoover R, Fraumeni JF Jr. Relationship of thyroid disease and use of thyroid supplements to breast cancer risk. J Chronic Dis. 1984;37:877-93.). TPO-Abs are not thyroid-specific enzymes, and they can also be expressed in other tissues (²⁴24. Jiskra J, Barkmanova J, Limanova Z, Lánská V, Smutek D, Potlukova E, et al. Thyroid autoimmunity occurs more frequently in women with breast cancer compared to women with colorectal cancer and controls but it has no impact on relapse-free and overall survival. Oncol Rep. 2007;18:1603-11.). In particular, TPO mRNA and protein have been found to be weakly but clearly expressed in BC tissues, peri-tumor tissues and in fat depots, and although they lack their functional activity, they maintain their antigenic role and can trigger B lymphocytes (³⁷37. Muller I, Giani C, Zhang L, Grennan-Jones FA, Fiore E, Belardi V, et al. Does thyroid peroxidase provide an antigenic link between thyroid autoimmunity and breast cancer? Int J Cancer. 2014;134:1706-14.). Clinically, TPO-Abs have been associated with both an increased risk of BC (⁸8. Turken O, NarIn Y, DemIrbas S, Onde ME, Sayan O, Kandemir EG, et al. Breast cancer in association with thyroid disorders. Breast Cancer Res. 2003;5:110-3.,⁹9. Giani C, Fierabracci P, Bonacci R, Gigliotti A, Campani D, De Negri F, et al. Relationship between breast cancer and thyroid disease: relevance of autoimmune thyroid disorders in breast malignancy. J Clin Endocrinol Metab. 1996;81:990-94.,³⁸38. Fiore E, Giustarini E, Mammoli C, Fragomeni F, Campani D, Muller I, et al. Favorable predictive value of thyroid autoimmunity in high aggressive breast cancer. J Endocrinol Invest. 2007;30:734-8.) and a lower risk of BC; in some cases, TPO-Abs have even been associated with a lower frequency of distant metastases (³⁹39. Szychta P, Szychta W, Gesing A, Lewiński A, Karbownik-Lewińska M. TSH receptor antibodies have predictive value for breast cancer – Retrospective analysis. Thyroid Res. 2013;6:8.), a better outcome and better overall survival (27,38). Our data did not find an association between thyroid autoantibodies and risk of BC, which is consistent with a prospective study by Kuijpens and cols. (²¹21. Kuijpens JL, Nyklíctek I, Louwman MW, Weetman TA, Pop VJ, Coebergh JW. Hypothyroidism might be related to breast cancer in post-menopausal women. Thyroid. 2005;15:1253-9.).

Few data exist regarding the role of Tg-Abs and TRAB in BC. Tg-Abs have been associated with different oncological diseases and have been found to be more prevalent in patients with BC (²³23. Cristofanilli M, Yamamura Y, Kau SW, Bevers T, Strom S, Patangan M, et al. Thyroid hormone and breast carcinoma. Primary hypothyroidism is associated with a reduced incidence of primary breast carcinoma. Cancer. 2005;103:1122-8.); however, they are not specific and may be influenced by different environmental factors (⁴⁰40. Dutton CM, Joba W, Spitzweg C, Heufelder AE, Bahn RS. Thyrotropin receptor expression in adrenal, kidney, and thymus. Thyroid. 1997;7:879-84.). Extrathyroidal expression of TSH receptor has also been demonstrated in cardiac muscle and adrenal and kidney tissue (⁴¹41. Ditsch N, Toth B, Himsl I, Lenhard M, Ochsenkühn R, Friese K, et al. Thyroid hormone receptor (TR)alpha and TRbeta expression in breast cancer. Histol Histopathol. 2013;28:227-37.) and was recently confirmed in BC tissue samples using RT-PCR (⁷7. Oh HJ, Chung JK, Kang JH, Kang WJ, Noh DY, Park IA, et al. The relationship between expression of the sodium/iodide symporter gene and the status of hormonal receptors in human breast cancer tissue. Cancer Res Treat. 2005;37:247-50.). In clinical studies, TRAB levels have been found to be significantly higher in BC cases, particularly in low-grade BC cases (⁷7. Oh HJ, Chung JK, Kang JH, Kang WJ, Noh DY, Park IA, et al. The relationship between expression of the sodium/iodide symporter gene and the status of hormonal receptors in human breast cancer tissue. Cancer Res Treat. 2005;37:247-50.), compared with healthy controls (⁴⁰40. Dutton CM, Joba W, Spitzweg C, Heufelder AE, Bahn RS. Thyrotropin receptor expression in adrenal, kidney, and thymus. Thyroid. 1997;7:879-84.) and BBD cases (¹1. Ditsch N, Liebhardt S, Von Koch F, Lenhard M, Vogeser M, Spitzweg C, et al. Thyroid function in breast cancer patients. Anticancer Res. 2010; 30:1713-7.).

The data in the literature associating thyroid function with prognostic markers of BC are scarce. In one study, BC cases with primary hypothyroidism showed a more indolent invasive breast cancer with less frequent lymph node metastases compared with euthyroid BC cases (²³23. Cristofanilli M, Yamamura Y, Kau SW, Bevers T, Strom S, Patangan M, et al. Thyroid hormone and breast carcinoma. Primary hypothyroidism is associated with a reduced incidence of primary breast carcinoma. Cancer. 2005;103:1122-8.). According to other data, TPO-Ab levels (²⁷27. Smyth PP, Shering SG, Kilbane MT, Murray MJ, McDermott EW, Smith DF, et al. Serum thyroid peroxidase autoantibodies, thyroid volume, and outcome in breast carcinoma. J Clin Endocrinol Metab. 1998;83:2711-6.) as well as the presence of nuclear TR-α receptors in breast cancer cells in vitro (²2. Lemaire M, Baugnet-Mahieu L. Nuclear thyroid hormone receptors in human cancer tissues. Anticancer Res. 1986;6:695-700.,⁴¹41. Ditsch N, Toth B, Himsl I, Lenhard M, Ochsenkühn R, Friese K, et al. Thyroid hormone receptor (TR)alpha and TRbeta expression in breast cancer. Histol Histopathol. 2013;28:227-37.) were inversely correlated with lymph nodes metastases. Our findings showed that a history of thyroid disease was significantly correlated with a lower incidence of lymph nodes (pN stage) metastases in BC cases. The frequency of primary hypothyroidism (mainly Hashimoto’s) was higher in BC cases with no lymph node involvement than in other thyroid diseases; however, the small sample size did not allow for a meaningful statistical analysis. We did not perform analyses for other prognostic markers such as Ki-67 and HER2 because of the limited data.

These data should be analyzed with caution because of the small size sample and because patients with known thyroid disease have more frequent access to hospital facilities and could thus be diagnosed with BC in earlier stages, which would explain the absence of lymph node metastases. Another limitation of this study was that patient’s history of thyroid disease and treatment was based on medical interviews and files, and this could have led to misclassifications in the diagnosis of thyroid disease.

In conclusion, our findings showed that a history of thyroid disease was not associated with risk of BC. However, a history of thyroid disease was associated with a significantly lower frequency of lymph node metastases, suggesting the potential for a better prognosis in these BC cases. The significantly higher mean baseline levels of fT4 in the BC cases compared with the other two groups may suggest a thyroid hormone pattern that is distinct from that of low T3 syndrome. Further studies to determine the prognostic role of thyroid hormones in BC are warranted, as the small number of cases in the present study precludes definitive conclusions.

Acknowledgments

we thank Maggie Meitzler and Valsamo Anagnostou for their assistance in writing this manuscript.

REFERENCES

¹
Ditsch N, Liebhardt S, Von Koch F, Lenhard M, Vogeser M, Spitzweg C, et al. Thyroid function in breast cancer patients. Anticancer Res. 2010; 30:1713-7.
²
Lemaire M, Baugnet-Mahieu L. Nuclear thyroid hormone receptors in human cancer tissues. Anticancer Res. 1986;6:695-700.
³
Nogueira CR, Brentani MM. Triiodothyronine mimics the effects of estrogen in breast cancer cell lines. J Steroid Biochem Mol Biol. 1996;59:271-9.
⁴
Humes HD, Cieslinski DA, Johnson LB, Sanchez IO. Triiodothyronine enhances renal tubule cell replication by stimulating EGF receptor gene expression. Am J Physiol. 1992;262:540-5.
⁵
Hall LC, Salazar EP, Kane SR, Liu N. Effects of thyroid hormones on human breast cancer cell proliferation. J Steroid Biochem Mol Biol. 2008;109:57-66.
⁶
Tang HY, Lin HY, Zhang S, Davis FB, Davis PJ. Thyroid hormone causes mitogen-activated protein kinase-dependent phosphorylation of the nuclear estrogen receptor. Endocrinology. 2004;145:3265-72.
⁷
Oh HJ, Chung JK, Kang JH, Kang WJ, Noh DY, Park IA, et al. The relationship between expression of the sodium/iodide symporter gene and the status of hormonal receptors in human breast cancer tissue. Cancer Res Treat. 2005;37:247-50.
⁸
Turken O, NarIn Y, DemIrbas S, Onde ME, Sayan O, Kandemir EG, et al. Breast cancer in association with thyroid disorders. Breast Cancer Res. 2003;5:110-3.
⁹
Giani C, Fierabracci P, Bonacci R, Gigliotti A, Campani D, De Negri F, et al. Relationship between breast cancer and thyroid disease: relevance of autoimmune thyroid disorders in breast malignancy. J Clin Endocrinol Metab. 1996;81:990-94.
¹⁰
Dohán O, Carrasco N. Advances in Na(+)/I(-) symporter (NIS) research in the thyroid and beyond. Mol Cell Endocrinol. 2003;213:59-70.
¹¹
Tazebay UH, Wapnir IL, Levy O, Dohan O, Zuckier LS, Zhao QH, et al. The mammary gland iodide transporter is expressed during lactation and in breast cancer. Nat Med. 2000;6:871-8.
¹²
Wapnir IL, van de Rijn M, Nowels K, Amenta PS, Walton K, Montgomery K, et al. Immunohistochemical profile of the sodium/iodide symporter in thyroid, breast, and other carcinomas using high density tissue microarrays and conventional sections. J Clin Endocrinol Metab. 2003;88:1880-8.
¹³
Rudnicka L, Sińczak A, Szybiński P, Huszno B, Stachura J. Expression of the Na(+)/I(-) symporter in invasive ductal breast cancer. Folia Histochem Cytobiol. 2003;41:37-40.
¹⁴
Pathologists’ Guideline Recommendations for Immunohistochemical Testing of Estrogen and Progesterone Receptors in Breast Cancer. Breast Care. 2010;5:185-7.
¹⁵
Ferlay J, Steliarova-Foucher E, Lortet-Tieulent J, Rosso S, Coebergh JW, Comber H, et al. Cancer incidence and mortality patterns in Europe: estimates for 40 countries in 2012. Eur J Cancer. 2013;49:1374-403.
¹⁶
Michalaki V, Kondi-Pafiti A, Gennatas S, Antoniou A, Primetis H, Gennatas C. Breast cancer in association with thyroid disorders. J BUON. 2009;14:425-8.
¹⁷
Goldman MB, Monson RR, Maloof F. Cancer mortality in women with thyroid disease. Cancer Res. 1990;50:2283-9.
¹⁸
Kalache A, Vessey MP, McPherson K. Thyroid disease and breast cancer: findings in a large case-control study. Br J Surg. 1982;69:434-5.
¹⁹
Simon MS, Tang MT, Bernstein L, Norman SA, Weiss L, Burkman RT, et al. Do thyroid disorders increase the risk of breast cancer? Cancer Epidemiol Biomarkers Prev. 2002;11:1574-8.
²⁰
Hoffman DA, McConahey WM, Brinton LA, Fraumeni JF Jr. Breast cancer in hypothyroid women using thyroid supplements. JAMA. 1984;251:616-19.
²¹
Kuijpens JL, Nyklíctek I, Louwman MW, Weetman TA, Pop VJ, Coebergh JW. Hypothyroidism might be related to breast cancer in post-menopausal women. Thyroid. 2005;15:1253-9.
²²
Muller I, Pinchera A, Fiore E, Belardi V, Rosellini V, Giustarini E. High prevalence of breast cancer in patients with benign thyroid diseases. J Endocrinol Invest. 2011;34:349-52.
²³
Cristofanilli M, Yamamura Y, Kau SW, Bevers T, Strom S, Patangan M, et al. Thyroid hormone and breast carcinoma. Primary hypothyroidism is associated with a reduced incidence of primary breast carcinoma. Cancer. 2005;103:1122-8.
²⁴
Jiskra J, Barkmanova J, Limanova Z, Lánská V, Smutek D, Potlukova E, et al. Thyroid autoimmunity occurs more frequently in women with breast cancer compared to women with colorectal cancer and controls but it has no impact on relapse-free and overall survival. Oncol Rep. 2007;18:1603-11.
²⁵
Giustarini E, Pinchera A, Fierabracci P, Roncella M, Fustaino L, Mammoli C, et al. Thyroid autoimmunity in patients with malignant and benign breast diseases before surgery. Eur J Endocrinol. 2006;154:645-9.
²⁶
Hardefeldt PJ, Eslick GD, Edirimanne S. Benign thyroid disease is associated with breast cancer: a meta-analysis. Breast Cancer Res Treat. 2012;133:1169-77.
²⁷
Smyth PP, Shering SG, Kilbane MT, Murray MJ, McDermott EW, Smith DF, et al. Serum thyroid peroxidase autoantibodies, thyroid volume, and outcome in breast carcinoma. J Clin Endocrinol Metab. 1998;83:2711-6.
²⁸
Tosovic A, Becker C, Bondeson AG, Bondeson L, Ericsson UB, Malm J, et al. Prospectively measured thyroid hormones and thyroid peroxidase antibodies in relation to breast cancer risk. Int J Cancer. 2012;131:2126-33.
²⁹
Takatani O, Okumoto T, Kosano H, Nishida M, Hiraide H, Tamakuma S. Relationship between the levels of serum thyroid hormones or estrogen status and the risk of breast cancer genesis in Japanese women. Cancer Res. 1989;49:3109-12.
³⁰
Tosovic A, Bondeson AG, Bondeson L, Ericsson UB, Manjer J. Triiodothyronine levels in relation to mortality from breast cancer and all causes: a population-based prospective cohort study. Eur J Endocrinol. 2013;168:483-90.
³¹
Perry M, Goldie DJ, Self M. Thyroid function in patients with breast cancer. Ann R Coll Surg Engl. 1978;60:290-3.
³²
Rose DP, Davis TE. Plasma thyronine levels in carcinoma of the breast and colon. Arch Intern Med. 1981;141:1161-4.
³³
Russell W, Harrison RF, Smith N, Darzy K, Shalet S, Weetman AP, et al. Free triiodothyronine has a distinct circadian rhythm that is delayed but parallels thyrotropin levels. J Clin Endocrinol Metab. 2008;93:2300-6.
³⁴
Hellevik AI, Asvold BO, Bjøro T, Romundstad PR, Nilsen TI, Vatten LJ. Thyroid function and cancer risk: a prospective population study. Cancer Epidemiol Biomarkers Prev. 2009;18:570-4.
³⁵
Sandhu MK, Brezden-Masley C, Lipscombe LL, Zagorski B, Booth GL. Autoimmune hypothyroidism and breast cancer in the elderly. Breast Cancer Res Treat. 2009;115:635-41.
³⁶
Brinton LA, Hoffman DA, Hoover R, Fraumeni JF Jr. Relationship of thyroid disease and use of thyroid supplements to breast cancer risk. J Chronic Dis. 1984;37:877-93.
³⁷
Muller I, Giani C, Zhang L, Grennan-Jones FA, Fiore E, Belardi V, et al. Does thyroid peroxidase provide an antigenic link between thyroid autoimmunity and breast cancer? Int J Cancer. 2014;134:1706-14.
³⁸
Fiore E, Giustarini E, Mammoli C, Fragomeni F, Campani D, Muller I, et al. Favorable predictive value of thyroid autoimmunity in high aggressive breast cancer. J Endocrinol Invest. 2007;30:734-8.
³⁹
Szychta P, Szychta W, Gesing A, Lewiński A, Karbownik-Lewińska M. TSH receptor antibodies have predictive value for breast cancer – Retrospective analysis. Thyroid Res. 2013;6:8.
⁴⁰
Dutton CM, Joba W, Spitzweg C, Heufelder AE, Bahn RS. Thyrotropin receptor expression in adrenal, kidney, and thymus. Thyroid. 1997;7:879-84.
⁴¹
Ditsch N, Toth B, Himsl I, Lenhard M, Ochsenkühn R, Friese K, et al. Thyroid hormone receptor (TR)alpha and TRbeta expression in breast cancer. Histol Histopathol. 2013;28:227-37.

Publication Dates

Publication in this collection
25 Aug 2016
Date of issue
Jan-Feb 2017

History

Received
15 July 2015
Accepted
26 Jan 2016

This is an Open Access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.

[1] ¹
Ditsch N, Liebhardt S, Von Koch F, Lenhard M, Vogeser M, Spitzweg C, et al. Thyroid function in breast cancer patients. Anticancer Res. 2010; 30:1713-7.

[2] ²
Lemaire M, Baugnet-Mahieu L. Nuclear thyroid hormone receptors in human cancer tissues. Anticancer Res. 1986;6:695-700.

[3] ³
Nogueira CR, Brentani MM. Triiodothyronine mimics the effects of estrogen in breast cancer cell lines. J Steroid Biochem Mol Biol. 1996;59:271-9.

[4] ⁴
Humes HD, Cieslinski DA, Johnson LB, Sanchez IO. Triiodothyronine enhances renal tubule cell replication by stimulating EGF receptor gene expression. Am J Physiol. 1992;262:540-5.

[5] ⁵
Hall LC, Salazar EP, Kane SR, Liu N. Effects of thyroid hormones on human breast cancer cell proliferation. J Steroid Biochem Mol Biol. 2008;109:57-66.

[6] ⁶
Tang HY, Lin HY, Zhang S, Davis FB, Davis PJ. Thyroid hormone causes mitogen-activated protein kinase-dependent phosphorylation of the nuclear estrogen receptor. Endocrinology. 2004;145:3265-72.

[7] ⁷
Oh HJ, Chung JK, Kang JH, Kang WJ, Noh DY, Park IA, et al. The relationship between expression of the sodium/iodide symporter gene and the status of hormonal receptors in human breast cancer tissue. Cancer Res Treat. 2005;37:247-50.

[8] ⁸
Turken O, NarIn Y, DemIrbas S, Onde ME, Sayan O, Kandemir EG, et al. Breast cancer in association with thyroid disorders. Breast Cancer Res. 2003;5:110-3.

[9] ⁹
Giani C, Fierabracci P, Bonacci R, Gigliotti A, Campani D, De Negri F, et al. Relationship between breast cancer and thyroid disease: relevance of autoimmune thyroid disorders in breast malignancy. J Clin Endocrinol Metab. 1996;81:990-94.

[10] ¹⁰
Dohán O, Carrasco N. Advances in Na(+)/I(-) symporter (NIS) research in the thyroid and beyond. Mol Cell Endocrinol. 2003;213:59-70.

[11] ¹¹
Tazebay UH, Wapnir IL, Levy O, Dohan O, Zuckier LS, Zhao QH, et al. The mammary gland iodide transporter is expressed during lactation and in breast cancer. Nat Med. 2000;6:871-8.

[12] ¹²
Wapnir IL, van de Rijn M, Nowels K, Amenta PS, Walton K, Montgomery K, et al. Immunohistochemical profile of the sodium/iodide symporter in thyroid, breast, and other carcinomas using high density tissue microarrays and conventional sections. J Clin Endocrinol Metab. 2003;88:1880-8.

[13] ¹³
Rudnicka L, Sińczak A, Szybiński P, Huszno B, Stachura J. Expression of the Na(+)/I(-) symporter in invasive ductal breast cancer. Folia Histochem Cytobiol. 2003;41:37-40.

[14] ¹⁴
Pathologists’ Guideline Recommendations for Immunohistochemical Testing of Estrogen and Progesterone Receptors in Breast Cancer. Breast Care. 2010;5:185-7.

[15] ¹⁵
Ferlay J, Steliarova-Foucher E, Lortet-Tieulent J, Rosso S, Coebergh JW, Comber H, et al. Cancer incidence and mortality patterns in Europe: estimates for 40 countries in 2012. Eur J Cancer. 2013;49:1374-403.

[16] ¹⁶
Michalaki V, Kondi-Pafiti A, Gennatas S, Antoniou A, Primetis H, Gennatas C. Breast cancer in association with thyroid disorders. J BUON. 2009;14:425-8.

[17] ¹⁷
Goldman MB, Monson RR, Maloof F. Cancer mortality in women with thyroid disease. Cancer Res. 1990;50:2283-9.

[18] ¹⁸
Kalache A, Vessey MP, McPherson K. Thyroid disease and breast cancer: findings in a large case-control study. Br J Surg. 1982;69:434-5.

[19] ¹⁹
Simon MS, Tang MT, Bernstein L, Norman SA, Weiss L, Burkman RT, et al. Do thyroid disorders increase the risk of breast cancer? Cancer Epidemiol Biomarkers Prev. 2002;11:1574-8.

[20] ²⁰
Hoffman DA, McConahey WM, Brinton LA, Fraumeni JF Jr. Breast cancer in hypothyroid women using thyroid supplements. JAMA. 1984;251:616-19.

[21] ²¹
Kuijpens JL, Nyklíctek I, Louwman MW, Weetman TA, Pop VJ, Coebergh JW. Hypothyroidism might be related to breast cancer in post-menopausal women. Thyroid. 2005;15:1253-9.

[22] ²²
Muller I, Pinchera A, Fiore E, Belardi V, Rosellini V, Giustarini E. High prevalence of breast cancer in patients with benign thyroid diseases. J Endocrinol Invest. 2011;34:349-52.

[23] ²³
Cristofanilli M, Yamamura Y, Kau SW, Bevers T, Strom S, Patangan M, et al. Thyroid hormone and breast carcinoma. Primary hypothyroidism is associated with a reduced incidence of primary breast carcinoma. Cancer. 2005;103:1122-8.

[24] ²⁴
Jiskra J, Barkmanova J, Limanova Z, Lánská V, Smutek D, Potlukova E, et al. Thyroid autoimmunity occurs more frequently in women with breast cancer compared to women with colorectal cancer and controls but it has no impact on relapse-free and overall survival. Oncol Rep. 2007;18:1603-11.

[25] ²⁵
Giustarini E, Pinchera A, Fierabracci P, Roncella M, Fustaino L, Mammoli C, et al. Thyroid autoimmunity in patients with malignant and benign breast diseases before surgery. Eur J Endocrinol. 2006;154:645-9.

[26] ²⁶
Hardefeldt PJ, Eslick GD, Edirimanne S. Benign thyroid disease is associated with breast cancer: a meta-analysis. Breast Cancer Res Treat. 2012;133:1169-77.

[27] ²⁷
Smyth PP, Shering SG, Kilbane MT, Murray MJ, McDermott EW, Smith DF, et al. Serum thyroid peroxidase autoantibodies, thyroid volume, and outcome in breast carcinoma. J Clin Endocrinol Metab. 1998;83:2711-6.

[28] ²⁸
Tosovic A, Becker C, Bondeson AG, Bondeson L, Ericsson UB, Malm J, et al. Prospectively measured thyroid hormones and thyroid peroxidase antibodies in relation to breast cancer risk. Int J Cancer. 2012;131:2126-33.

[29] ²⁹
Takatani O, Okumoto T, Kosano H, Nishida M, Hiraide H, Tamakuma S. Relationship between the levels of serum thyroid hormones or estrogen status and the risk of breast cancer genesis in Japanese women. Cancer Res. 1989;49:3109-12.

[30] ³⁰
Tosovic A, Bondeson AG, Bondeson L, Ericsson UB, Manjer J. Triiodothyronine levels in relation to mortality from breast cancer and all causes: a population-based prospective cohort study. Eur J Endocrinol. 2013;168:483-90.

[31] ³¹
Perry M, Goldie DJ, Self M. Thyroid function in patients with breast cancer. Ann R Coll Surg Engl. 1978;60:290-3.

[32] ³²
Rose DP, Davis TE. Plasma thyronine levels in carcinoma of the breast and colon. Arch Intern Med. 1981;141:1161-4.

[33] ³³
Russell W, Harrison RF, Smith N, Darzy K, Shalet S, Weetman AP, et al. Free triiodothyronine has a distinct circadian rhythm that is delayed but parallels thyrotropin levels. J Clin Endocrinol Metab. 2008;93:2300-6.

[34] ³⁴
Hellevik AI, Asvold BO, Bjøro T, Romundstad PR, Nilsen TI, Vatten LJ. Thyroid function and cancer risk: a prospective population study. Cancer Epidemiol Biomarkers Prev. 2009;18:570-4.

[35] ³⁵
Sandhu MK, Brezden-Masley C, Lipscombe LL, Zagorski B, Booth GL. Autoimmune hypothyroidism and breast cancer in the elderly. Breast Cancer Res Treat. 2009;115:635-41.

[36] ³⁶
Brinton LA, Hoffman DA, Hoover R, Fraumeni JF Jr. Relationship of thyroid disease and use of thyroid supplements to breast cancer risk. J Chronic Dis. 1984;37:877-93.

[37] ³⁷
Muller I, Giani C, Zhang L, Grennan-Jones FA, Fiore E, Belardi V, et al. Does thyroid peroxidase provide an antigenic link between thyroid autoimmunity and breast cancer? Int J Cancer. 2014;134:1706-14.

[38] ³⁸
Fiore E, Giustarini E, Mammoli C, Fragomeni F, Campani D, Muller I, et al. Favorable predictive value of thyroid autoimmunity in high aggressive breast cancer. J Endocrinol Invest. 2007;30:734-8.

[39] ³⁹
Szychta P, Szychta W, Gesing A, Lewiński A, Karbownik-Lewińska M. TSH receptor antibodies have predictive value for breast cancer – Retrospective analysis. Thyroid Res. 2013;6:8.

[40] ⁴⁰
Dutton CM, Joba W, Spitzweg C, Heufelder AE, Bahn RS. Thyrotropin receptor expression in adrenal, kidney, and thymus. Thyroid. 1997;7:879-84.

[41] ⁴¹
Ditsch N, Toth B, Himsl I, Lenhard M, Ochsenkühn R, Friese K, et al. Thyroid hormone receptor (TR)alpha and TRbeta expression in breast cancer. Histol Histopathol. 2013;28:227-37.

Groups/Epidemiological data	Controls	BC	BBD	Atypical hyperplasia	Statistical significance (p)
Total number	48	97	27	4
Age (mean ± SD)	54.27 ± 12.84	64.02 ± 14.11	52.07 ± 16.93	60.31 ± 13.86	p < 0.05¹
BMI (kg/m²)	27.02 ± 7.53	28.00 ± 7.09	25.60 ± 5.30	27.42 ± 0.00	p = 0.226¹
Age of menarche (mean ± SD)	13.43 ± 1.55	11.85 ± 3.07	12.26 ± 3.09	12.39 ± 2.75	p = 0.002¹
Menopausal status
Premenopausal (%)	17/48 (35%)	18/90 (20%)	13/24 (54%)	2/4	p = 0.044¹ (between pre and post-menopausal)
Postmenopausal (%)	30/48 (62.5%)	68/90 (76%)	10/24 (42%)	2/4
Perimenopausal (%)	1/48 (2%)	4/90 (4%)	1/24 (4%)	0
History of pregnancy
Yes (%)	37/48 (78%)	80/91 (88%)	17/24 (71%)	¾	p = 0.44¹
No (%)	11/48 (22%)	11/91 (12%)	7/24 (29%)	¼	p = 0.44¹
Parity
1-2	34/37 (92%)	65/78 (83%)	10/17 (65%)
> 3	3/37 (8%)	15/78 (17%)	4/17 (35%)
Age of 1^st birth
< 20	6	8	4	0	p = 0.46¹
21-30	11	25	6	0
> 31	10	21	2	0
Use of contraceptives
Yes (%)	4/39 (10%)	8/79 (10%)	5/16 (31%)	0/2	p = 0.11¹
No (%)	35/39 (90%)	71/79 (90%)	11/16 (69%)	2/2	p = 0.11¹
Smoking
Yes (%)	12/48 (25%)	22/88 (25%)	6/25 (24%)	¼	p = 1.0¹
No (%)	36/48 (75%)	66/88 (75%)	19/25 (76%)	¾	p = 1.0¹
Alcohol
Yes (%)	1/48 (2%)	5/83 (6%)	5/24 (21%)	0/4	p = 0.025¹
No (%)	47/48 (98%)	78/83 (94%)	19/24 (79%)	4/4	p = 0.025¹
1^st degree family history of BC
Yes	7/48 (15%)	14/93 (15%)	4/24 (16.6)	¼	p = 0.95¹
No	41/48 (85%)	79/93 (85%)	20/24 (83.3)	¾	p = 0.95¹

Groups/Frequency of thyroid disorder and treatment	Controls	BC	BBD	Atypical hyperplasia	Statistical significance (p)
History of thyroid disorders
Yes (%)	22/48 (46%)	32/97 (33%)	8/27 (30%)	3/4	p = 0.33¹
No (%)	26/48 (54%)	62/97 (64%)	17/27 (63%)	1/4
No data	0	3/97 (3%)	2/27 (7%)	0
Type of thyroid disorder
Hashimoto (%)	7/22 (32%)	9/32 (28%)	3/8 (37.5%)	0	nd²
Primary hypothyroidism (other causes) (%)	0	4/32 (12.5%)	0	2
Hyperthyroidism (%)	4/22 (18%)	4/32 (13%)	0	0
Goiter (%)	2/22 (9%)	9/32 (28%)	5/8 (62.5%)	1
Nodules (%)	9/22 (40%)	5/32 (16%)	0	0
No data	0	1/32 (3%)	0	0
Treatment
Yes (substitution, antithyroid drugs)	7/47 (15%)*	21/97 (22%) 3/97 (3%)	7/27 (26%)	3/4	p = 0.79¹
No	40/47 (85%)	73/97 (75%)	20/27 (74%)	1/4

Groups/Mean values ± SD, (n)	Controls	BC	BBD	Atypical hyperplasia	Statistical significance (p)
TSH (0,3-4,0 mU/L)	2.05 ± 1.57 (n = 42)	2.37 ± 2.30 (n = 78)	2.07 ± 1.03 (n = 20)	1.88 ± 1.90 (n = 4)	p = 0.757¹
fT3 (2,3-5,3 pg/mL)	3.47 ± 1.93 (n = 41)	3.20 ± 0.74 (n = 69)	3.11 ± 0.83 (n = 16)	3.33 ± 0.37 (n = 3)	p = 0.622¹
fT4 (10-25 pmol/L)	15.50 ± 3.76 (n = 41)	17.20 ± 3.30 (n = 67)	16.97 ± 3.29 (n = 16)	18.38 ± 2.80 (n = 4)	p = 0.035¹

Groups/Frequency and mean values ± SD, (n)	Controls	BC	BBD	Atypical hyperplasia	Statistical significance
TPO-Abs

Μean values ± SD (n)	149.50 ± 495.54 (n = 39)	312 ± 810 (n = 42)	520 ± 1089 (n = 12)	20 ± 26.54 (n = 2)	p = 0.6¹
Negative (< 50 mU/L)	32/39 (82%)	33/42 (78.5)	8/12 (66.6%)	2/2	p = 0.43¹
Positive (> 50 mU/L)	7/39 (18%)	9/42 (21.4%)	4/12 (33.3%)	0/2	p = 0.43¹

Tg-Abs

Mean values ± SD (n)	28.48 ± 64 (n = 12)	132 ± 238 (n = 17)	17.41 ± 14.65 (n = 9)	nd	p = 0.07¹
Negative (< 10 mU/L)	10/12 (83%)	6/17 (35%)	4/9 (44.4%)	nd	p = 1.00
Positive (> 10 mU/L)	2/12 (16.6%)	11/17 (64.7%)	5/9 (55.5%)	nd	p = 1.00

TRAK

Mean values ± SD (n)	0.71 ± 0.23 (n = 41)	0.64 ± 0.12 (n = 20)	0.66 ± 0.20 (n = 3)	nd	p = 0.42¹
Negative (> 2 U/L)	41/41	20/20	3/3	nd
Positive (< 2 U/L)	0	0	0	nd

Thyroid disease/Prognostic factors of BC	History of thyroid disease		Statistical significance (p)

	Yes	No
TNM stage
pT1	14 (14.4%)	27 (28%)	p = 0.805*
pT2	12 (12.4%)	24 (25%)
pT3	4 (4%)	8 (8.2%)
pT4	1 (1%)	2 (2%)
pT+	8 (23.5%)	26 (76.5%)	p = 0.034
pT-	21 (46.6%)	24 (53.3%)
Grade
I	2 (25%)	6 (75%)	p = 0.83
II	17 (33%)	35 (66%)
III	7 (22%)	18 (78%)
Hormone-sensitivity
ER +/PR +	20 (34%)	39 (66%)	p = 0.47
ER -/PR-	5 (33.5%)	10 (66.6%)

Brasil

Brasil

Is there an association between thyroid function abnormalities and breast cancer?

ABSTRACT

Objective

Subjects and methods

Results

Conclusions

INTRODUCTION

SUBJECTS AND METHODS

Patient characteristics

Laboratory measurements

Immunohistochemistry

Statistical analysis

RESULTS

Association between history of thyroid disease and histopathological parameters of breast tissue

Association between thyroid function tests and histopathological parameters of breast tissue

Association between thyroid autoantibodies and histopathological parameters of breast tissue

Association between thyroid function and hormone dependent BC (ER and/or PR positivity)

Association between thyroid disease and tumor size, nodal involvement or grading of BC

DISCUSSION

Acknowledgments

REFERENCES

Publication Dates

History