

Hypothyroidism in Pancreatic Cancer: Role of Exogenous Thyroid Hormone in Tumor Invasion—Preliminary Observations


Research Article
Hypothyroidism in Pancreatic Cancer:
Role of Exogenous Thyroid Hormone in Tumor
Invasion—Preliminary Observations

Konrad Sarosiek,1 Ankit V. Gandhi,1 Shivam Saxena,1 Christopher Y. Kang,1

Galina I. Chipitsyna,2 Charles J. Yeo,1 and Hwyda A. Arafat2

1Departments of Surgery, Jefferson Pancreatic, Biliary and Related Cancer Center, Thomas Jefferson University,
Philadelphia, PA 19107, USA
2Department of Biomedical Sciences, University of New England, Biddeford, ME 04005, USA

Correspondence should be addressed to Galina I. Chipitsyna; galina727@gmail.com

Received 5 October 2015; Revised 15 March 2016; Accepted 16 March 2016

Academic Editor: Noriyuki Koibuchi

Copyright © 2016 Konrad Sarosiek et al. This is an open access article distributed under the Creative Commons Attribution
License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly
cited.

According to the epidemiological studies, about 4.4% of American general elderly population has a pronounced hypothyroidism
and relies on thyroid hormone supplements daily. The prevalence of hypothyroidism in our patients with pancreatic cancer was
much higher, 14.1%. A retrospective analysis was performed on patients who underwent pancreaticoduodenectomy (Whipple
procedure) or distal pancreatectomy and splenectomy (DPS) at Thomas Jefferson University Hospital, Philadelphia, from 2005 to
2012. The diagnosis of hypothyroidism was correlated with clinicopathologic parameters including tumor stage, grade, and survival.
To further understand how thyroid hormone affects pancreatic cancer behavior, functional studies including wound-induced cell
migration, proliferation, and invasion were performed on pancreatic cancer cell lines, MiaPaCa-2 and AsPC-1. We found that
hypothyroid patients taking exogenous thyroid hormone were more than three times likely to have perineural invasion, and about
twice as likely to have higher T stage, nodal spread, and overall poorer prognostic stage (𝑃 < 0.05). Pancreatic cancer cell line
studies demonstrated that exogenous thyroid hormone treatment increased cell proliferation, migration, and invasion (𝑃 < 0.05).
We conclude that exogenous thyroid hormone may contribute to the progression of pancreatic cancer.

1. Introduction

Invasive pancreatic cancer is the fourth leading cause of can-
cer death in the United States. Most patients with pancreatic
cancer have a dismal prognosis and a median survival rate of
less than 6 months [1, 2]. At the time of diagnosis, the disease
is often discovered to be in its late stages, as more than 85%
of patients have tumors that have metastasized [2]. Currently,
surgery remains one of the few options to decrease pancreatic
cancer mortality. Despite many advances in cancer biology
over the past years, pancreatic cancer remains an elusive
disease process that requires further studies to understand
its molecular biology and investigate possible therapeutic
targets.

Thyroid hormones (T
3
and T

4
) are steroid hormones that

regulate body growth, brain maturation, and metabolism.
Although the major product of the thyroid is T

4
, most of

it is converted to more biologically active T
3
that binds

to nuclear thyroid receptors and modulates the expression
of proteins traditionally known to increase basal metabolic
rate and enhance growth [3]. Disorders of the thyroid that
result in either a deficiency or excess of thyroid hormones
are extremely common and can have various effects on the
human body. According to the NHANES national 1999–2002
survey, the prevalence of hypothyroidism in the general US
population was 3.7% [4]. Of note, the prevalence of thyroid
disorders increases with age (up to 4.4% for 60 years and

Hindawi Publishing Corporation
Journal of yroid Research
Volume 2016, Article ID 2454989, 7 pages
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2 Journal of Thyroid Research

older) and is consistent with females having higher rates of
hypothyroidism than men [5–8].

Due to the established effect of thyroid hormone on
growth and development, many have hypothesized a con-
nection between thyroid hormone and cancer. One of the
first reports linking these two comes from a 1976 article
that examines the relationship between supplemental thyroid
hormone intake and breast cancer. In a study with 5,000
female patients, it was calculated that the rate of breast cancer
in patients taking thyroid supplements for hypothyroidism
was 12.1% versus 6.2% in a control group [9]. Since then,
many studies have sparked a debate about a relationship
between hypothyroidism and malignancy. A search of the
literature reveals that hypothyroidism may be a risk factor for
respiratory, colon, breast, and liver cancer [10–14]. Cell line
experiments in breast and prostate cancer corroborate these
findings by demonstrating that treatment with T

3
enhances

cellular proliferation [15, 16].
In this study, a retrospective analysis was performed on

patients who underwent pancreaticoduodenectomy (Whip-
ple procedure) or distal pancreatectomy and splenectomy
(DPS) at Thomas Jefferson University Hospital, Philadel-
phia, from 2005 to 2012. The diagnosis of hypothyroidism
was correlated with clinicopathologic parameters including
tumor stage, grade, and survival. To further understand
how thyroid hormone affects pancreatic cancer behavior,
functional studies including wound-induced cell migration,
proliferation, and invasion were performed on pancreatic
cancer cell lines, MiaPaCa-2 and AsPC-1.

2. Materials and Methods

2.1. Data Collection. For this cross-sectional study, a database
search was conducted for patients who underwent pancreati-
coduodenectomy (Whipple procedure) or distal pancreatec-
tomy and splenectomy (DPS) at Thomas Jefferson University
Hospital, Philadelphia, PA, from 2005 to 2012. The eligibility
criteria consisted of patients with a diagnosis of invasive
pancreatic cancer confirmed by biopsy. Exclusion criteria
consisted of patients with a history of noninvasive, benign
pancreatic pathology or incomplete medical history. Data
collection included patient sex, age, body mass index (BMI),
medical history, medications, surgical information, survival,
tumor staging, and differentiation by hypothyroid status.
The TNM staging system as outlined by the American Joint
Committee on Cancer (AJCC) was used to define pancreatic
lesions. Patients were defined to be hypothyroid if they had a
positive medical hypothyroidism and were taking synthetic
or desiccated thyroid hormone. The Institutional Review
Board of Thomas Jefferson University Hospital, Philadelphia,
PA, approved this study.

MiaPaCa-2 (ATCC CRL-1420) and AsPC-1 (ATCC CRL-
1682) were purchased from ATCC. MTT cell growth, migra-
tion, and transwell invasion assays were performed as previ-
ously described [17].

2.2. Statistical Analyses. Descriptive statistics were calculated
on patient clinicopathological features. Differences in gender,

smoking status, venous-lymphatic invasion, perineural inva-
sion, T stage, N stage, prognostic stage, and differentiation
by hypothyroid status were determined by Chi-square test.
Differences in age and BMI were determined by unpaired Stu-
dent’s 𝑡-test. Survival analysis was performed using Kaplan-
Meier curves and Mantel-Cox log rank test, where survival
was defined as time between date of surgery and date of
death or of last follow-up. All functional experiments were
performed 3 to 5 times. Functional studies were analyzed
for statistical significance by Student’s 𝑡-test analysis, or two-
way ANOVA. Data are presented as mean ± SEM. All tests
of significance were two-sided with an alpha value of 0.05.
Analyses were performed with the assistance of a computer
program (Prism 6.0, GraphPad Software, Inc., La Jolla, CA).

3. Results

3.1. Patient Characteristics. An overview of the clinical
patient data is summarized in Table 1. Of 504 patients in the
database, 71 patients were found to be hypothyroid (of males,
7.7% and, of females, 20.8% were hypothyroid). As expected,
the hypothyroid group had a significantly greater proportion
of females than males (𝑃 < 0.001). The age of patients in the
hypothyroid group (67.8) was similar to the age of patients
in the euthyroid group (64.6). BMI was not significantly
different in the hypothyroid group when compared to the
euthyroid group (27.9 versus 26.3, resp.). Lastly, there was no
significant difference in smoking status between two groups.

3.2. Pancreatic Pathology. Pancreatic tissue specimens strat-
ified by pathology are shown in Table 2. Majority of the
biopsies (85%) were invasive ductal adenocarcinoma. Second
most common pathology was invasive IPMN (6%), followed
by endocrine, papillary, acinar cell, and mucinous cancers.

3.3. Clinicopathological Parameters by Hypothyroid Status.
As shown in Table 3, there were no differences in survival
(Figure 1), venous-lymphatic invasion, and differentiation
between hypothyroid and euthyroid patients. Compared to
euthyroid patients, hypothyroid patients taking exogenous
thyroid hormone were more than three times likely to have
perineural invasion and about twice as likely to have a higher
T stage, nodal spread, and overall poorer prognostic stage.

3.4. T
3
Increases Cell Proliferation, Migration, and Invasion.

To evaluate whether T
3
was associated with cell viability,

MiaPaCa-2 cells were treated with T
3
(0–5000 nM) and

quantified via the MTT assay (Figure 2(a)). The addition of
T
3
significantly (𝑃 < 0.05) increased cell proliferation after

48 and 72 hours across all concentrations of T
3
. Additionally,

MiaPaCa-2 cells were treated with T
3
to evaluate its role

in cell migration (Figure 2(b)). T
3
significantly (𝑃 < 0.05)

increased cell migration at 48- and 72-hour time points at
1 and 10 nM of T

3
compared to the control. Lastly, the role

of exogenous thyroid hormone in invasion was evaluated via
transwell infiltration assay. Cells were treated with T

3
(0–

10 nM), and the extent of invasion was quantified via MTT
assay (Figure 2(c)). Adding T

3
significantly (𝑃 < 0.05)


Journal of Thyroid Research 3

Table 1: Clinical characteristics of patients.

Hypothyroid Euthyroid Total
(𝑛 = 71) (𝑛 = 433) (𝑛 = 504)

Male,𝑛 (%) 20 (28.2) 239 (55.2) 259 (51.4)
Female,𝑛 (%) 51 (71.8) 194 (44.8) 245 (48.6)
Age, mean (SD) 67.8 (12.6) 64.6 (12.1) 65.1 (12.2)
BMI, mean (SD) 27.9 (5.6) 26.3 (5.3) 26.5 (5.4)
Smoking status,𝑛 (%), yes 32 (53.3) 200 (54.9) 232 (54.7)
Smoking status,𝑛 (%), no 28 (46.7) 164 (45.1) 192 (45.3)

Table 2: Pancreatic tissue specimens stratified by pathology.

Pancreatic malignancy 𝑛 (%)
Invasive ductal adenocarcinoma 427 (84.7)
Invasive IPMN 31 (6.2)
Endocrine 22 (4.4)
Papillary 17 (3.4)
Acinar cell 4 (0.8)
Mucinous 3 (0.6)
All invasive pancreatic pathologies 504 (100)

increased cell invasion. Similar data (𝑃< 0.05) were obtained
for AsPC-1 cells (data not shown).

4. Discussion

The objective of this study was to evaluate the prevalence
of hypothyroidism and thyroid hormone supplementation
in patients with pancreatic cancer and to correlate hypothy-
roidism diagnosis with various clinicopathologic parame-
ters. Furthermore, functional studies were performed on
MiaPaCa-2 and AsPC-1 pancreatic cancer cell lines to study
how exogenous thyroid hormone influences cell behavior.
To our knowledge, this is the first study to suggest a higher
prevalence of thyroid hormone supplementation in patients
with pancreatic cancer and to demonstrate the proliferative
effects of T

3
in pancreatic cancer cell lines.

The association between hypothyroidism and neoplasia
remains controversial. Despite conflicting reports in the
literature, studies have shown that hypothyroidism may cor-
relate with many cancers including respiratory, colon, breast,
and liver cancer [10–14]. Some studies even suggest that a
diagnosis of hypothyroidism may result in poor response
to therapy in patients with breast cancer [18]. Other studies
argue that high levels of thyroid hormones induce cancer cell
proliferation while low levels slow disease progress [19]. A
number of prospective case-control studies have indicated
that subclinical hyperthyroidism increases risk of certain
solid tumors and that spontaneous hypothyroidism may
delay onset or reduce aggressiveness of cancers [20–22].
A controlled prospective trial of induced hypothyroidism
beneficially affected the course of glioblastoma [20].

In our study, the prevalence of patients with hypothy-
roidism treated with medication was 14.1% (7.7% in males,
20.8% in females). This percentage is much higher than the
prevalence of overt hypothyroidism reported in the elderly

Months elapsed

Su
rv

iv
al

 (%
)

0 20 40 60 80 100
0

50

100

Hypothyroid
Euthyroid

Figure 1: Kaplan-Meier curve comparing hypothyroid and euthy-
roid patients. There was no difference in survival.𝑃= 0.742.

(4.4%) and is consistent with females having higher rates of
hypothyroidism than men [4–8].

Metastasis is one of the most significant predictors of
mortality in patients with pancreatic cancer. When com-
paring hypothyroid and euthyroid patients with pancreatic
cancer, hypothyroid patients on thyroid hormone supple-
mentation were found to have significantly (𝑃< 0.05) higher
rates of nodal spread and a T stage of T3 or higher, signifying
that the tumor has already extended beyond the walls of
the pancreas. It was not surprising that these patients were
more likely to have a poorer prognostic stage (OR 1.9). Inter-
estingly, patients on thyroid hormone supplementation also
had significantly higher rates of perineural invasion (OR 3.4).
Perineural invasion is a poorly understood process by which
cancer cells metastasize to nerves and their surrounding
neural sheaths [23]. Although metastatic spread via neural
invasion is often overlooked, PDAC has one of the highest
rates of perineural invasion when compared to other malig-
nancies, and it is a substantial cause of pain in pancreatic
cancer patients [24]. Despite these poor prognostic factors,
there was no significant difference in survival between
patients taking thyroid hormone supplementation compared
to patients who were not on medication. This might be due
to the limitations of this study. One of the limitations was
possible selection bias in the patient population. Because
surgery was reserved for patients with resectable disease
only, our study might not accurately capture patients with
advanced diseases. Another limitation was little information
available regarding the diagnosis of hypothyroidism. TSH
measurement was not used to diagnose or quantify the
degree of hypothyroidism. Similarly, the date and duration
of hypothyroidism and thyroid hormone implementation
were not available at the time of the surgery. Lastly, due to
difficulties in patient follow-up after hospital discharge, the
survival data were not the most current.

However, because all patients with hypothyroidism were
taking exogenous thyroid medication, one may hypothesize
that exogenous thyroid hormone may be responsible for


4 Journal of Thyroid Research

Table 3: Clinicopathologic parameters of hypothyroid and euthyroid patients with invasive PDA.

Hypothyroid Euthyroid OR [95% CI] 𝑃value
Median survival (months) 17.7 16.6 0.742
Venous-lymphatic invasion,𝑛 (%) 0.91 [0.52–1.58] 0.733

Yes 28 (48) 185 (51)
No 30 (52) 180 (49)

Perineural invasion,𝑛 (%) 3.38 [1.19–9.58] 0.012∗

Yes 62 (94) 335 (82)
No 4 (6) 73 (18)

T stage,𝑛 (%) 2.10 [1.00–4.37] 0.045∗

Low stage (T0–T2) 9 98
High stage (T3-T4) 61 317

Nodal status,𝑛 (%) 2.05 [1.12–3.75] 0.018∗

N0 15 (22) 157 (36)
N1 54 (78) 276 (64)

Prognostic stage,𝑛 (%) 1.89 [1.03–3.48] 0.037∗

Low stage (0–2A) 15 (22) 142 (34)
High stage (2B-3) 54 (78) 270 (66)

Differentiation,𝑛 (%) 0.612
Well 10 (14) 46 (12)
Moderate 44 (64) 242 (61)
Poor 15 (22) 105 (27)

Hypothyroid patients were found to have higher rates of perineural invasion, nodal spread, and advanced prognostic stage.∗𝑃< 0.05.

increasing growth and metabolism of pancreatic cancer cells,
thus responsible for promoting tumor invasion and spread
to nearby structures. Functional assays that were performed
demonstrated that treatment of MiaPaCa-2 and AsPC-1 cells
with physiologic concentrations of thyroid hormone caused
an increase in cell proliferation, migration, and invasion
at 48 h and 72 h. These results are consistent with studies
that demonstrate proliferative effect of T

3
in breast cancer,

prostate cancer, and hepatocellular carcinoma. It was also
shown that T

3
contributes to breast cancer cell prolifer-

ation through estrogen response elements mediated gene
expression, by promoting the effects of estrogens themselves
[15] or by upregulating TGF-𝛼 mRNA expression [25].
Murine glioma cell lines and human prostatic carcinoma
cells also revealed the increased proliferation in response to
physiological concentrations of both T

3
and T

4
[16, 26, 27].

T
3
also promotes cell proliferation and invasion in human

hepatoma cell lines in cooperation with TGF-𝛽 [28, 29].
Thyroid hormones enhance the development of gastric cancer
in rats by stimulating the proliferation of gastric cancer
cells [14, 30]. Additionally, thyroid hormones act as growth
factors in both papillary and follicular human thyroid cancer
cell lines [31]. It was shown that both T

3
and T

4
caused

proliferation of malignant glioma U-87 MG cells through
PI3-kinase, Src kinase, and ERK1/2 signaling cascades [32].
T
3
and T

4
promote both tumor cell division and angiogene-

sis by activating mitogen-activated protein kinase (MAPK)
via binding to a hormone receptor on the 𝛼v𝛽3 integrin,
overexpressed on many human myelomas and other cancer
cells [33, 34]. Other in vitro studies of thyroid hormones
action in cancer cells implicated many molecular targets,

including TGF-𝛽, hyperphosphorylation of Rb, and MAP
kinase pathways [15, 16, 26, 35, 36]. Thyroid hormones have
also been shown to promote angiogenesis in cancer cells by
upregulating HIF-1𝛼 [35, 37].

5. Conclusions

This study demonstrates that there may be an association
between thyroid hormone supplementation and pancreatic
cancer invasion. Although the use of exogenous thyroid
hormone may not necessarily be involved in the initial insult
responsible for tumorigenesis, it may contribute to the pro-
gression of preexisting tumor. Increased perineural invasion,
higher T stage, nodal spread, and advanced prognostic stage
in hypothyroid patients may be due to enhanced metabolism
of malignant cells via thyroid hormone supplementation. The
proliferative effects of T

3
on MiaPaCa-2 and AsPC-1 cells

support this hypothesis.
We propose that spontaneous hypothyroidism might

develop in cancer patients as a protection mechanism against
tumor progress/spread, but thyroid hormone supplementa-
tion might abolish this action. Clinical studies have shown
[38] that interventional lowering of serum-free T

4
may be

associated with extended survival in patients with some
terminal cancers, and compassionate medical induction of
hypothyroxinemia could be considered for patients with
advanced cancers to whom other avenues of treatment are
closed [38]. Thus, accumulating clinical evidence may justify
new, broadly based controlled studies in cancer patients to
determine the possible contribution of thyroid hormone to
tumor behavior. Insights into molecular mechanism of this


Journal of Thyroid Research 5

∗

∗ ∗

∗
∗

0 1 10 100 1000 5000

0.6

0.4

0.2

0.0

R
el

at
iv

e 
ce

ll 
pr

ol
ife

ra
tio

n

24 h
48 h

72 h

T
3

concentration (nM)

(a)

Time (hours)

M
ig

ra
tio

n 
di

st
an

ce

0

50

100

150

200

∗

∗

0 nM
1 nM

10 nM

0 24 48 72

(b)

R
el

at
iv

e 
ce

ll 
in

va
si

on

0.0

0.5

1.0

1.5

2.0

∗∗

0 1 10

T
3

concentration (nM)

(c)

Figure 2: Effects of exogenous thyroid hormone treatment on PDAC cells proliferation, migration, and invasion (𝑃< 0.05). (a) Proliferation
assay of MiaPaCa-2 cells incubated with T

3
. Proliferation was increased at all concentrations after 48 and 72 hours. ∗𝑃< 0.05. (b) Migration

assay of MiaPaCa-2 cells incubated with T
3
. Cell migration was increased after 48 and 72 hours. ∗𝑃< 0.05. (c) Transwell infiltration assay of

MiaPaCa-2 cells incubated with T
3
. Cell invasion was increased by 1 and 10 nM T

3
. ∗𝑃< 0.05.

process might uncover possible targets which would allow
thyroid hormone supplementation without promoting cancer
progression.

Competing Interests

All named authors have no financial interests in respect of
this work and its publication or other interests that might be
perceived to influence the results and/or discussion reported
in this paper.

Acknowledgments

Authors acknowledge research support and funding they
have received from the Department of Surgery, Thomas
Jefferson University Hospital, Philadelphia, PA, and Depart-
ment of Biomedical Sciences, University of New England,
Biddeford, ME, relevant to the work described.

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