Adrenoceptors and breast cancer: Review article Roisman R., Klemm O., Raphaeli G., and Roisman I.
Dedicated to Mrs. Minka Klavins and Prof. Janis V. Klavins
Albert Einstein College of Medicine, New York, NY, USA
Correspondence to: Isaac Roisman, M.D., Dip. Surg., M. Surg., D.Sc. P.O.Box 45470, Haifa 31453, Israel
Tel.: (972-4)8388393, Fax: (972-4)8379503
Adrenoceptors and breast cancer: Review article Introduction
The incidence of breast cancer has increased greatly in Israel over the past decade. It is
estimated that in Israel in 2009 approximately 4800 new patients will suffer from
Despite recent advances in the diagnosis and treatment of breast cancer, this disease
continues to be a major cause of death. One of the biggest challenges in breast cancer
treatment is bone metastasis. Breast cancer cells are capable of migrating to the bone
marrow and utilizing the marrow microenvironment to remain quiescent. The
preprotachykinin-1 (PPT-I) gene encodes for the tachykinin peptides, which interact
with neurokinin (NK) receptors. Studies have correlated this interaction with breast
cancer cells integration into the bone marrow and breast cancer progression (1).
Environmental and psychological stresses have been shown to be associated with an
increased incidence of cancer in man and animals. Stress-induced neuron chemical
hormonal and immunological changes have been shown to influence tumor
development. Stress may promote mammary carcinogenesis by affecting the
neuroendocrine system and I or immune function. Neuroendocrine affects may involve
changes in adrenocortical steroids or opioid peptides which may exert their effects by
One of the risk factors for breast cancer is the increased amount of adipose tissue after
menopause which elevates estradiol production.
The adrenergic system plays a role in regulating energy balance through thermogensis
and lipid mobilization from brown or white adipose tissues (3).
The human fat cells are equipped with adrenergic receptors (adreno receptors) β1, β2
Physiology
The degree of affinity for adrenaline (epinephrine) is β2 > β1> β3 and the noradrenaline
(norephinephrine) it is β1 ≥ β2 > β3 (5).
Norepinephrine, epinephrine and dopamine are members of biogenic amines. They
share a common precursor - tyrosine. It is converted to L-dopa by tyrosine
hydroxylase and L-dopa is converted to dopamine by dopa decarboxylase. In the nerve
terminal dopamine is converted to norepinepherine.
If phenylethanol - N - methyl transferase (PNMT) is present norepinephrine is
methylated to epinephrine. Adrenergic neurons secrete norepinephrine because they
Adreno receptors may be activated by norepinephrine, which is released from
adrenergic neurons, or by epinephrine, which is secreted into the circulation by the
adrenal medulla. Among the sympathetic adrenoreceptors, receptor type is related to
In addition to their role as neurotransmitters and stress hormones, catecholamines play
a trophic role in the control of cell replication and differentiation in target cells that
express adrenergic receptors. In some cell lines, β -adrenergic stimulation elicits a
small, promotional effect on cell replication, whereas in others, stimulation of these
receptors and the consequent rise in intracellular cAMP levels inhibits mitosis. β -
adrenoreceptors on cancer cells, thus, recapitulate both the promotional and inhibitory
roles of these receptors in cell replication seen in the development of normal cells.
Location and mechanism of autonomic action
Vascular smooth muscle, skin, renal and splanchnic
gastrointestinal tract, bladder sphincter, iris, radial
Gastrointestinal tract wall, presynaptic adrenergic
Heart, salivary gland, adipose tissue, kidney
stimulation of adenylyl cyclase, increase cAMP
Va Vascular smooth muscle of skeletal muscle, GI wall,
The β -adrenergic agonist isoproterenol, stimulates mammary epithelial cell division
in vitro, as well as the development of end bud structures in the mammary gland of
ovary ectomized mice from which arise the mammary carcinoma induced by
administration of dimethylbenz (α) anthracene (DMBA). Specific β -adrenergic
receptors of the β2 subtype are present in epithelial cell membranes from lactating
The hormonal modulations of receptors which affect uterine contractility correlates
with the onset of psychological responses of the uterus such as contraction and
relaxation. In analogy with the uterus the regulation of the physiological status of the
mammary gland is achieved by modification of endocrine, autonomic and mechanical
factors during adolescence, the menstrual cycle, pregnancy parturition and lactation.
The mammary gland, as other paired endocrine glands (adrenals, ovaries and testes),
High levels of β -adrenergic receptors are measured as palpable mammary tumors,
reaching a maximal concentration well before the actual increase in tumor mass. The
hormone sensitivity of the tumoral β -adrenergic receptor is further confirmed by the
high receptor concentration measured in progressing mammary tumors.
Stress effects may involve ACTH, glucocorticoids, catecholamines, prolactin, opioids
and immunosuppression, all factors crucially involved in tumor growth.
Catecholestrogens, their receptors, together with their catabolizing enzyme, catechol-
o-methyltransferease(COMT), are locally formed in both normal and neoplastic
mammary tissues. COMT levels are significantly increased in the cytosol of
malignant tumor cells than in the cytosol of benign tumor or normal cells (7).
Adrenoceptors and cancer
Recent studies in human cancer cell lines in animal models have shown that the
growth of adenocarcinomas of the lungs, pancreas and colon are under β -adrenergic
The expression of β -adrenergic receptors has been correlated with the over-
expression of the arachidonic acid-metabolizing enzymes cyclooxygenase-2 (COX-2)
and lipoxygenases (LOX) in adenocarcinomas of lungs, colon, prostate and pancreas.
Inhibitors of these enzymes have been identified as cancer preventive agents in animal
Many of breast adenocarcinomas over express COX-2 and / or LOX (13).
This may say that a subset of breast cancers may also be under β adrenergic control.
Studies have demonstrated that three estrogen-responsive and three non-estrogen
responsive human cell lines derived from breast adenocarcinoma show a reduction in
DNA synthesis in response to beta-blockers or inhibitors of the arachidonic acid-
Another study analysis by reverse transcription polymerase chain reaction (RT-PCR)
revealed expression of β 2-adrenergic receptors in all six breast cancer cell lines tested
(MDA-MB-361, ZR-75-l, MCF-7, MDA-MB-453, MDA-MB-468, MDA-MB-4355).
β 1 receptors were not found in two estrogen non-responsive cell lines (MDA-MB-
It was found that the second messenger cAMP may be a growth promoter for mouse,
rat and human mammary epithelioma (15, 16).
The effects of cAMP observed in malignant cells are involved in redifferentiation
amounting to renormalization of number of properties including morphology,
adhesive properties, lectin agglutination, cell movement and biochemical functions
A correlation between β adreno receptor (β -AR) stimulation and estrogen and
progesterone receptor functions was found in human breast cancer (18).
β 2-adrenergic stimulation induced cell proliferation in hormone-dependent human
breast cancer cell line (C6-5),but without involving the female steroid hormone
In C6-5 cells, the presence of functional β -AR's could be reasonable related to cell
proliferation when exposed to different concentrations of clenbuterol, a β 2-AR
agonist showed increased cell proliferation without involving significantly lower than
that induced by oestradiol β adreno receptor-mediated inhibition of DNA synthesis
was not shared by another cancer cell line, C6 rat glioma, that expresses a different β -
receptor subtype a lower levels whereas found that MDA-MB-231 cells express β 2-
receptors exclusively, C6 cell express primarily the β1 subtype (19).
In mammary tissue there are data that support a role of catecholamines in the control
of many cellular activities. Initial experiments indicate epinephrine sensitive
adenylate cyclase activities in 7, 12 - dimethylbenz (α) anthracene - induced
mammary carcinoma. Two groups have demonstrated the presence of β -adrenergic
receptors (β -AR) from mammary glands of lactating rats. β -adrenergic compounds
stimulated the enzyme leading to the generation of cAMP and its activation was
completely abolished by the β -AR blocking drug propranolol.
β -adrenergic - related increases in cAMP formation undoubtedly influence lactose
production by the acinar secretory end pieces. The initial response to β -AR is usually
an increase in adenylate cyclase activity resulting in an increased cellular cAMP
Among the epithelial, endocrine, and secretory cancer cell lines that express
adrenoreceptors, MDA-MB-231 human breast cancer cells exhibit comparatively high
concentrations. It is thus of critical interest that stimulation of these receptors leads to
immediate inhibition of DNA synthesis and, with prolonged exposure, reductions in
the total number of cancer cells: inhibition of DNA synthesis is a reliable predictor of
chemotherapeutic responses in breast cancer cells.
In prostate or breast cancer cells stimulated by EGF or androgen or estradiol, small
peptides (6-10 amino acids) derived from ER or AR sequences involved in the
receptor interaction with Src, prevent AR/ER/Src association, Src/Erk pathway
stimulation, cyclin D1 expression and DNA synthesis. The peptide action is restricted
to cells expressing the steroid receptors and to signals mediated by these receptors.
Remarkably, the peptides do not modify. Although there has been no systematic
screening of breast cancer cell lines for β -adrenergic expression these receptors have
identified in both estrogen-dependent type and estrogen-independent type, including
C6-5, BF 20, T47-D, VHB-1 and MCF-7. Regardless of the ancillary mechanisms
involved in β -receptor — mediated inhibition of mitosis in MDA-MB-231 breast
cancer cells, the fact that inhibition does not disappear with receptor down regulation
and desensitization raises the possibility for therapeutic strategies employing receptor
agonists, alone or in combination with glucocorticoids and phosphodiesterase
Screening of human cancers for the presence of β -adrenoreceptors or other cAMP —
linked neurotransmitter receptors may establish new treatment strategies.
β -adrenergic receptors (β -AR's) were identified in CG-5breast cancer cells using a
radiometric assay. The total β -AR concentration was measured using the highly
potent β -adrenergic antagonist CGP 12 177, and the densities of β -AR subtypes were
discriminated in the presence of highly selective unlabelled ligands (CGP 207 12A
The second messenger cAMP was found to be a growth promoter for mouse, rat and
human mammary epithelioma and its levels are elevated in several breast carcinomas.
The effects of cAMP observed in malignant cells are often involved in
redifferentiation, amounting to apparent renormalization of a number of properties
including morphology, adhesive properties, lectin agglutination, cell movement and
biochemical functions. A correlation between β -AR stimulation and estrogen and
progesterone receptor functions was found in human breast cancer.
It was observed that β2-adrenergic stimulation induced cell proliferation in a
hormone-dependent human breast cancer cell line (CG-5),but without involving the
CG-5cells (mammary breast cell cancer cell line) contain measurable concentrations
of specific β AR's coupled to adenylate cyclase. The characteristics of these β -AR's,
identified by binding and competition assays, are those of β 1-AR and β2 -AR
subtypes. β 2-AR concentration is significantly higher than β 1-AR concentration in
CG-5cell membranes. Negligible concentrations of β -AR's were found in MCF-7
breast cancer cells from which CG-5cells are derived. In C6-5cells the presence of
functional β -AR's could be reasonably related to cell proliferation when exposed to
different concentrations of clenbuterol, a β 2-AR agonist, showed increased cell
proliferation without involving steroid hormone receptors.
Although the enhancement of CG-5cell growth was significantly lower than that
induced by estradiol the presence of functional β -AR’s (with the prevalence of the β
2-AR subtype) in tumor cell line suggests that β -adrenergic stimulation and resulting
cAMP production may be responsible for CG-5 cell proliferation.
Medroxyprogesterone acetate (MPA) is one of the most widely used compounds in
the endocrine therapy of advanced breast cancer in women. The mechanisms
underlying the antitumor activity of MPA are poorly understood. This steroid presents
a high affinity for progesterone (PgR) as well as for androgen (AR) and
glucocorticoid receptors (GR) in human mammary tumors.
The most easily explained effects of MPA are related to its glucocorticoid-like action.
Suppression of adrenal function by MPA is believed to be caused both by an
inhibitory action at the pituitary level and by direct inhibition of steroidogenesis.
In addition to ER and PgR, which are the most widely used markers of differentiated
endocrine functions in breast cancer; AR and GR (Glucocorticoid receptors) are
present in a substantial number of mammary tumors and established cell lines. The
ZR-75-1 human breast cancer cell line is an unusually appropriate system to study the
direct effect of MPA on cell growth. ZR-75-1 cells contain functional receptors for
estrogens, androgens, progestins and glucocorticoids. Progestins inhibit ZR-75-1 cell
proliferation exclusively in presence of estrogens and in absence of insulin.
MPA further decreased the growth of ZR-75- 1 cells co-incubated with maximally
inhibitory concentrations of either 5 alpha-dihydrotestosterone ((DHT) or
dexamethasone (DEX) although at about 300-fold higher MPA concentrations with
DHT-treated than with DEX-treated ZR-75-1 cells, thus demonstrating a highly
predominant androgenic effect. The main action of MPA on ZR-75-1 human breast
cancer cell growth is due to its androgen receptor-mediated inhibitory action.
The majority of breast cancer are adenocarcinomas and many of them over express
cyclooxygenase - 2 (COX-2) (9) and/or lipoxygenases (LOX). This raises the
possibility that comparable to findings in adenocarcinomas of the lungs, pancreas,
colon and prostate, and a subset of breast cancer may also be under beta adrenergic
control. Studies have demonstrated that three estrogen-responsive and three non-
estrogen responsive human cell lines derived from breast adenocarcinomas
demonstrated a significant reduction in DNA synthesis in response to beta-blockers or
inhibitors of the arachidonic acid metabolizing enzymes COX-2 (9) and LOX-5.
Analysis by reverse transcription polymerase chain reaction (RT-PCR) revealed
expression of β2-adrenergic receptors in all six breast cancer cell tested (MDA-MB-
361, ZR-75-1, MCF-7, MDA-MB -453,MDA-MB-468, MDA-MB-435S) whereas β1
receptors were not found in two estrogen non-responsive cell lines (MDA-MB-435S,
Expression of mRNA that encodes a G-protein coupled inward by rectifying
potassium channel 1 (GIRK1) (7) has been shown in 40% breast cancer samples. This
expression of GIRK1 was associated with a more aggressive clinical behavior.
Previous studies indicated that the beta-adrenergic agonist isoproterenol stimulates
growth. GIRK currents have been shown to be increased in cells stimulated with the
beta-adrenergic agonist isoproterenol in rat atrial myocytes transferred with β1 or β2
receptors. Two po1ymorphisms in the β2 or β3 adrenergic receptors were found to be
correlated with decreased risk for breast cancer, suggesting an important role of this
receptor family in the genesis of breast cancer.
In C6-5 cells (16, 19) the presence of functional β -AR's could be reasonable related to
cell proliferation when exposed to different concentration of clenbuterol, a β 2-AR
agonist showed increased cell proliferation without involving significantly lower than
that induced by estradiol β adreno receptor-mediated inhibition of DNA synthesis
was not shared by another cancer cell line, C6 rat glioma, that expresses a different β -
receptor subtype a lower levels whereas (20) found that MOA-MB-23 1 cells express β
2-receptors exclusively, C6 cell express primarily the β1 subtype.
There is increasing evidence that describes a histamine role in normal and cancer cell
proliferation. To better understand the importance of histamine in breast cancer
development, the expression of histamine H3 (H3R) and H4 (H4R) receptors and their
association with proliferating cell nuclear antigen (PCNA), histidine decarboxylase
(HDC) and histamine content were explored in mammary biopsies. Additionally, we
investigated whether H3R and H4R were implicated in the biological responses
triggered by histamine in MDA-MB-231(20) breast cancer cells.
Centrally assess estrogen receptor (ER) and progesterone receptor (PgR) levels by
immunohistochemistry and investigate their predictive value for benefit of chemo-
endocrine compared with endocrine adjuvant therapy alone in two randomized
clinical trials for node-negative breast cancer.
Low levels of ER and PgR are predictive of the benefit of adding chemotherapy to
endocrine therapy. Low PgR may add further predictions among pre-and
perimenopausal but not postmenopausal patient whose tumors express ER.
The majority of all breast cancers are hormone responsive, traditionally defined by he
expression of oestogen receptor (ER) alpha and/or progesterone receptors. In contrast
to ERalpha, the clinical significance of the relatively recently identified ERbeta is still
ERalpha and ERbeta seem to be differentially associated to clinicopathological
parameters, and this would support the fact that they might have different functions in
In prostate or breast cancer cells stimulated by EGF or androgen or estradiol, small
peptides (6-10 amino acids) derived from ER or AR sequences involved in the
receptor interaction with Src, prevent AR/ER/Src association, Src/Erk pathway
stimulation, cyclin D1 expression and DNA synthesis. The peptide action is restricted
to cells expressing the steroid receptors and to signals mediated by these receptors.
Epidermal growth factor (EGF), transforming growth factor-alpha (TGFalpha),
amphiregulin (AREG), betacellulin (BTC), heparin-binding EGF-like growth factor
(HB-EGF),epiregulin (EREG) and neuregulins1-4 (NRG1-4) were quantified in 363
tumors by real-time reverse transcription-polymerase chain reaction using TaqMan
Paget's disease (PD) of the breast as well as the vulva is a rare condition, therefore
anti-hormonal therapy is not indicated. The high frequency of Her-2/neu and COX-2
overexpression, however, suggests that these molecules could be therapeutically
Epidemiological evidence indicates that the association between body weight and
breast cancer risk may differ across menopausal status as well as the estrogen receptor
(ER) and progesterone receptor (PR) tumor status.
The relation between body weight and breast cancer risk is critically dependent on the
tumor's ER/PR status and the woman's menopausal status. Body weith control is the
effective strategy for preventing ER+PR+ tumors after menopause.
ErbB3 transactivation can make tumor cells resistance to ErbB1/ErbB2 targeting
drugs. This urges for a reliable method to determine cel surface ErbB3 levels, but
their hands iodinated NRG1 beta is unstable and tends to underestimate the umber of
ErbB3 receptors in a radio-receptor assay.
Furthermore, they show by differential competition with unlabled NRG/YYDLL and
betacellulin that the number of ErbB3 and ErbB4 receptors can be quantified
separately on cultured human breast cancer cells.
Esterogen receptor (ER) antagonists have been widely used for breast cancer
treatment, but the efficacy and drug resistance remain to be clinical concerns. The
purpose of this study was to determine whether the extracts of coptis, an anti-
inflammatory herb, improve the anticancer efficacy of ER antagonists, Their results
showed that the combined treatment of ER antagonists and the crude extract of coptis
or its purified compound berberine conferred synergetic growth inhibitory effect on
MCF-7 cells (ER+), but not on MDA-MB-231 cells (R-). Similar results were
observed in the combined treatment of fulvestrant, a specific aromatase antagonist.
Analysis of the expression of breast cancer related genes indicated the EGFR, HER2,
bci-2, and COX-2 were significantly downregulated, while IFN-beta and p21 were
The negative association between he oestrogen receptor (ER) and the human
epidermal growth factor 2 (HER-2) in breast cancer travels in both directions. ER+
tumors are less likely HER-2+ and HER-2+ are less likely ER+. Studies the age-
related immunohistochemical (IHC) expression of ER, HER-2 in 2,227 tumors using
Estrogen receptors (ERs) are overexpressed in human breast cancers (BCs) and
associated with differentiated tumors and with a more favorable prognosis (22-34).
Paradoxically, ERs mediate the mitogenic action of estrogens in human BC cells and
the efficacy of antiestrogens in adjuvant therapy of primary tumors. The exact
mechanism underlying the ER protection against cancer progression to metastasis
remains to be investigated. They show that ERs decrease invasiveness of BC cells.
Detailed studies revealed that the unliganded and the E2-activated ERs decrease
cancer cell invasion in vitro through two distinct mechanisms. In the presence of
ligand, ERalpha inhibits invasion through a mechanism requiring the functional
ERalpha domains involved in the transcriptional activation of target genes.
Hormone receptors play important roles in breast cancer. The expression of hormone
receptors in breast cancer was investigated to evaluate the importance of hormone
receptors in the clinicopathology of breast cancer.
Androgen receptor (AR), estrogen receptor (ER) and progesterone receptor (PR)
expression characteristics were evaluated using immunohistochemistry stain,
comparing patient age, tumor size and axillary lymph node status for 23 pure
mucinous and 105 non-mucinous infiltrating ductal carcinomas in the human female
Findings revealed that mucinous carcinoma samples from the breast show distinct
clinicopathologic and hormone receptor expression features compared to non-
There is increasing evidence that describes a histamine role in normal and cancer cell
proliferations. To better understand the importance of histamine in breast cancer
development, the expression of histamine H3 (H3R) nad H4 (H4R) receptors and their
association with proliferating cell nuclear antigen (PCNA), histidine decarboxylase
(HDC) and histamine content were explored in mammary biopsies. Additionally, we
investigated whether H3R and H4R were implicated in the biological MDA-MB-231
β -adrenergic receptors (β -AR's) were identified in C6-5breast cancer cells using a
radiometric assay. The total β -AR concentration was measured using the highly
potent β -adrenergic antagonist CGP 12 177, and the densities of β -AR subtypes were
discriminated in the presence of highly selective unlabelled ligands (CGP 20712A and
The second messenger cAMP was found to be a growth promoter for mouse, rat and
human mammary epithelioma and its levels are elevated in several breast carcinomas.
It was observed that β 2-adrenergic stimulation induced cell proliferation in a hormone
dependent human breast cancer cell line (CG-5),but without involving the female
steroid hormone receptor system. CG-5 cells (mammary breast cell cancer cell line)
contain measurable concentrations of specific β AR's coupled to adenylate cyclase.
The characteristics of these β -AR's, identified by binding and competition assays, are
those of β 1-AR and β 2-AR subtypes. β 2-AR concentration is significantly higher
than β 1-AR concentration in CG-5 cell membranes. Negligible concentrations of β –
AR's were found in MCF-7 breast cancer cells from which CG-5 cells are derived.
Although the enhancement of CG-5cell growth was significantly lower than that
induced by estradiol the presence of functional β -AR’s (with the prevalence of the β2-
subtype AR) in tumor cell line suggests that β -adrenergic stimulation and resulting
cAMP production may be responsible for CG-S cell proliferation.
Medroxyprogesterone acetate (MPA) is one of the most widely used compounds in
the endocrine therapy of advanced breast cancer in women.
The mechanisms underlying the antitumor activity of MPA are poorly understood.
This steroid presents a high affinity for progesterone (PgR) as well as for androgen
(AR) and glucocorticoid receptors (GR) in human mammary tumors.
The most easily explained effects of MPA are related to its glucocorticoid-like action.
Suppression of adrenal function by MPA is believed to be caused both by an
inhibitory action at the pituitary level and by direct inhibition of steroidogenesis.
In addition to ER and PgR, which are the most widely used markers of differentiated
endocrine functions in breast cancer; AR and GR are present in a substantial number
of mammary tumors and established cell lines. The ZR-75-1 human breast cancer cell
line is an unusually appropriate system to study the direct effect of MPA on cell
growth. ZR-75-1 cells contain functional receptors for estrogens, androgens
progestins and glucocorticoids. Progestins inhibit ZR-75- 1 cell proliferation
exclusively in presence of estrogens and in absence of insulin.
MPA further decreased the growth of ZR-75-1 cells co-incubated with maximally
inhibitory concentrations of either 5 alpha-dihydrotestosterone (DHT) or
dexamethasone (DEX) at about 300-fold higher MPA concentrations with DHT-
treated than with DEX-treated ZR-75- 1 cells, thus demonstrating a highly
predominant androgenic effect. The main action of MPA on ZR-75-1 human breast
cancer cell growth is due to its androgen receptor-mediated inhibitory action.
In normal and malignant mammary tissues there are data supporting a role for
catecholeamines in the control of many cellular activities. The presence of functional
β-AR's in human mammary cell lines has been described. All six breast cell lines
express either GIRK2 or GIRK4 indicating that functional GIRK potassium channels
are possible in these cancer cell lines. The direct control of cell proliferation shown in
vitro could eventually open new avenues for adjuvant therapies in the treatment of
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The 500-mg Invirase tablets are beige and im-printed with “ROCHE” on one side and “SQV 500” on the other side. Also known as: Ro 31-8959, saquinavir mesylate, SQV Patient assistance. Roche offers a patient assistance program for Background and description. This drug is a protease inhibitor those who qualify. For more information call 800.282.7780. man u fac tured by F. H
¿El cigarrillo electrónico es un método seguro para dejar de fumar? El cigarril o electrónico es un dispositivo que se ofrece como alternativa al cigarril o tradicional. Tiene el tamaño y aspecto de un cigarril o, funciona a batería y a través de calor vaporiza nicotina. Tiene pequeños cartuchos con concentraciones variables de nicotina y también con sabores diferentes, que pued