NIH Consensus Statement on Breast Cancer Posted: 07-07-03 19:35pm
Each year, more than 180,000 women in the
United States are diagnosed with breast
cancer, the most common type of
noncutaneous cancer among women in this
country. If current breast cancer rates
remain constant, a woman born today has a
one in ten chance of developing breast
cancer.
Because of continuing research into new
treatment methods, women with invasive
breast cancer now have more treatment
options and a better chance of long-term
survival than ever before. The primary
treatment of localized breast cancer is
either breast-conserving surgery and
radiation or mastectomy with or without
breast reconstruction. Systemic adjuvant
therapies that are designed to eradicate
microscopic deposits of cancer cells that
may have spread or metastasized from the
primary breast cancer have been
demonstrated to increase a woman's chance
of long-term survival.
Systemic adjuvant therapies include
chemotherapy (anticancer drugs) and
hormone therapy. In addition to these
systemic therapies, radiotherapy is used
in selected cases as a local adjuvant
treatment to destroy breast cancer cells
that remain in the chest wall or regional
lymph nodes after mastectomy.
The rapid pace of discovery in this area
continues to expand the knowledge base
from which informed treatment decisions
can be made. The purpose of this
conference was to establish a consensus
regarding the use of adjuvant therapy for
invasive breast cancer and to communicate
that consensus to clinicians, patients,
and the general public. After reading
relevant literature and attending a day
and a half of presentations and audience
discussion, an independent, non-Federal
consensus development panel weighed the
scientific evidence and drafted a
statement that was presented to the
conference audience on the third day. The
consensus development panel's statement
addresses the following key questions:
Which factors should be used to select
systemic adjuvant therapy?
For which patients should adjuvant
hormonal therapy be recommended?
For which patients should adjuvant
chemotherapy be recommended? Which agents
should be used, and at what dose or
schedule?
For which patients should post-mastectomy
radiotherapy be recommended?
How do side effects and quality-of-life
issues factor into individual
decision-making about adjuvant therapy?
What are promising new research directions
for adjuvant therapy?
This conference was sponsored by the
National Cancer Institute and the NIH
Office of Medical Applications of
Research. The co-sponsors included the
National Institute of Nursing Research and
the NIH Office of Research on Women's
Health.
1. Which factors should be used to select
systemic adjuvant therapy?
The selection of systemic adjuvant therapy
is based on prognostic and predictive
factors. Prognostic factors are
measurements available at diagnosis or
time of surgery that, in the absence of
adjuvant therapy, are associated with
recurrence rate, death rate, or other
clinical outcome. Predictive factors are
measurements associated with the degree of
response to a specific therapy. For
example, a demonstration of hormone
receptors in tumor cells predicts the
response to hormonal therapy. Any factor
has the potential to be both prognostic
and predictive, and a factor's importance
depends on both the clinical endpoint and
on the method of treatment comparison.
Prognostic and predictive factors fall
into three categories: patient
characteristics that are independent of
the disease (such as age); disease
characteristics (such as tumor size and
histologic type); and biomarkers
(measurable parameters in tissues, cells,
or fluids), such as hormone receptor
status, progesterone receptor status, and
measures of cell turnover. Accepted
prognostic and predictive factors include
age, tumor size, axillary node status,
histological tumor type, standardized
pathologic grade, and hormonal-receptor
status.
The median age for the diagnosis of breast
cancer is between the ages of 60 and 65
years. Some younger women (particularly
under 35 years) have a more aggressive
form of the disease, characterized by
larger tumors of higher grade with
vascular invasion. Elderly women (over 70
years) with breast cancer frequently have
hormone receptor protein in their
malignant tissue, suggesting a more
indolent tumor pattern and a high
likelihood of response to hormonal
therapy.
Race appears to be a prognostic but not
predictive factor. In contrast to white
women, black breast cancer patients are
generally younger, often have larger
tumors at diagnosis, and a smaller
percentage have hormone receptors in their
tumor tissue. These factors contribute to
a poorer prognosis. In cases of similar
clinical presentation, however, adjuvant
treatment confers similar benefits to
black and white women. Research on the
benefits and risks of adjuvant therapy in
Hispanic, Asian, and Native American women
is needed.
Novel technologies (such as tissue and
expression microarrays and proteomics)
present exciting potential, but their
integration into clinical practice will
depend on the proper design and analysis
of clinical investigations. The same is
true for overexpression of HER-2/neu, p53
status, histologic evidence of vascular
invasion, and quantitative parameters of
angiogenesis. These have been extensively
studied clinically and biologically, but
do not have an established role in patient
management. For example, although
overexpression/amplification of HER-2/neu
is associated with an adverse outcome in
node-positive patients and may predict the
response to therapy, laboratory methods
and the reporting of results require
standardization before its predictive
performance can be established.
The development of immunohistochemical and
molecular methods to identify occult
cancer cells (i.e., micrometastases) in
histologically tumor-free axillary lymph
nodes or bone marrow has raised questions
as to whether such findings should alter
the clinical stage and become a further
indication for systemic adjuvant therapy.
At present, the clinical significance of
these findings remains uncertain, and they
require assessment in prospective clinical
trials before they directly alter patient
management.
It is essential that the value of
predictive and prognostic factors be
evaluated in well-designed clinical
studies that are based on standardized
protocols and have sufficient statistical
power. Because these standards are
infrequently met, very few new prognostic
or predictive factors have been validated
in the last 10 years, and future progress
will depend on greater attention to these
standards. Promising pilot studies should
be followed by a validation phase, during
which alternative assays for the biomarker
are evaluated in a head-to-head comparison
and prognostic/predictive value is
studied. Since no single study will have
sufficient power to properly evaluate
predictive value, results from these
trials should be combined.
2. For which patients should adjuvant
hormonal therapy be recommended?
The decision whether to recommend adjuvant
hormonal therapy should be based on the
presence of hormone receptors, as assessed
by immunohistochemical staining of breast
cancer tissue. If the available tissue is
insufficient to determine hormone receptor
status, it should be considered as being
positive, particularly in postmenopausal
women. The small subset of women whose
tumors lack hormone receptor protein but
contain progesterone receptor also appear
to benefit from hormonal therapy. The
presence or absence of HER-2/neu
overexpression should not influence the
decision to recommend hormonal therapy.
The goal of hormonal therapy is to prevent
breast cancer cells from receiving
stimulation from estrogen. Such
stimulation occurs primarily in tumors
that contain hormone receptor protein.
Estrogen deprivation can be achieved by
(a) blocking the receptor through the use
of drugs, such as tamoxifen; (b)
suppression of estrogen synthesis through
the administration of aromatase inhibitors
(e.g., anastrozole) in postmenopausal
women or LHRH agonists (e.g., goserelin)
in premenopausal women; or (c) destruction
of the ovaries through surgery or external
beam radiation therapy. The administration
of cytotoxic chemotherapy may indirectly
accomplish this same effect by damaging
estrogen-producing cells in the ovaries.
Adjuvant hormonal therapy should be
recommended to women whose breast tumors
contain hormone receptor protein,
regardless of age, menopausal status,
involvement of axillary lymph nodes, or
tumor size. While the likelihood of
benefit correlates with the amount of
hormone receptor protein in tumor cells,
patients with any extent of hormone
receptor in their tumor cells may still
benefit from hormonal therapy. Such
treatment has led to substantial
reductions in the likelihood of tumor
recurrence, second primary breast cancer,
and death persisting for at least 15 years
of followup. Possible exceptions to this
recommendation include premenopausal women
with tumors less than 10 mm in size who
wish to avoid the symptoms of estrogen
deprivation or elderly women with
similarly sized cancers who have a history
of venous thromboembolic episodes.
Tamoxifen is the most commonly used form
of hormonal therapy. Randomized trials and
a meta-analysis have shown that 5 years of
tamoxifen are superior to 1 to 2 years of
such treatment. Currently, there are no
convincing data that justify the use of
tamoxifen for longer than 5 years outside
the setting of a clinical trial. Although
tamoxifen has been associated with a
slight but definite increased risk of
endometrial cancer and venous
thromboembolism, the benefit of tamoxifen
treatment far outweighs its risks in the
majority of women. Neither transvaginal
ultrasonography nor endometrial biopsies
are indicated as screening maneuvers for
endometrial cancer in asymptomatic women
taking tamoxifen. Tamoxifen may be
combined with combination chemotherapy,
particularly in premenopausal women; such
combinations may further reduce the risk
of recurrence. There are no data to
support the use of raloxifene or aromatase
inhibitors as adjuvant hormonal therapy at
this time.
For hormone receptor positive
premenopausal patients, alternative
strategies of hormonal therapy, which are
used far less frequently in the United
States, include ovarian ablation through
surgery, radiation therapy to the ovaries,
or chemical suppression of ovarian
function. Ovarian ablation appears to
produce a similar benefit to some
chemotherapy regimens. Combining ovarian
ablation with chemotherapy has not been
shown to provide an additional advantage
to date. The value of combining hormonal
therapies has not yet been adequately
explored.
Hormonal adjuvant therapy should not be
recommended to women whose breast cancers
do not express hormone receptor protein.
Randomized clinical trials have not yet
shown that such treatment substantially
reduces the likelihood of recurrence or,
in the case of tamoxifen, diminishes the
likelihood of contralateral breast
cancer.
3. For which patients should adjuvant
chemotherapy be recommended? Which agents
should be used, and at what dose or
schedule?
Over the past decade, data have emerged
that more clearly define the
subpopulations of women with localized
breast cancer for whom adjuvant
chemotherapy is indicated as a standard
component of treatment. Chemotherapy has
been shown to substantially improve the
long-term, relapse-free, and overall
survival in both premenopausal and
postmenopausal women up to age 70 years
with node-positive and node-negative
disease.
Randomized clinical trials have attempted
to define optimal chemotherapy regimens,
doses, and schedules in the adjuvant
treatment of breast cancer. These studies,
along with the results of overview
analyses, permit a number of conclusions
to be drawn.
The administration of polychemotherapy
(> 2 agents) is superior to single
agents. Four to six courses of treatment
(3 to 6 months) appear to provide optimal
benefit, with the administration of
additional courses adding to toxicity
without substantially improving overall
outcome. However, definitive data on the
benefits of more prolonged treatment are
lacking and future research is needed to
directly address this clinically relevant
issue.
Anthracyclines (such as doxorubicin and
epirubicin) have been used as components
of adjuvant polychemotherapy for breast
cancer. Available data indicate that
adjuvant chemotherapy regimens that
include an anthracycline result in a small
but statistically significant improvement
in survival compared to
nonanthracycline-containing programs.
There is no evidence for excessive cardiac
toxicity in women without significant
preexisting heart disease treated with
anthracyclines at the cumulative doses
utilized in standard adjuvant programs. In
clinical practice, the decision to use an
anthracycline in an individual patient
should take into consideration the
potential survival benefits versus
specific concern about additional
toxicity.
Randomized trials have demonstrated
threshold dose effects for two of the most
active chemotherapeutic agents,
doxorubicin (A) and cyclophosphamide (C).
These two drugs are frequently
administered together (AC) and appear to
result in a comparable survival outcome,
whether given preoperatively or
postoperatively. However, AC has not been
compared to
cyclophosphamide/doxorubicin/5-fluorouraci
l (CAF) or
cyclophosphamide/epirubicin/5-fluorouracil
(CEF). There is a need for future studies
to address the issue of defining the
optimal use of anthracycline-based
therapy.
There is currently no convincing evidence
to demonstrate that more dose-intensive
treatment regimens (e.g., high-dose
chemotherapy with peripheral stem cell
support) result in improved outcomes
compared to the administration of
polychemotherapy programs at standard dose
levels. Such stem cell-support treatment
strategies should not be offered outside
the setting of a randomized clinical
trial.
Taxanes (docetaxel, paclitaxel) have
recently been demonstrated to be among the
most active agents in the treatment of
metastatic breast cancer. As a result,
several studies have explored the clinical
utility of adding these drugs to standard
doxorubicin/cyclophosphamide treatment
programs in the adjuvant treatment of
node-positive, localized breast cancer.
Although a number of such trials have
completed accrual and others remain in
progress, currently available data are
inconclusive and do not permit definitive
recommendations regarding the impact of
taxanes on either relapse-free or overall
survival. There is no evidence to support
the use of taxanes in node-negative breast
cancer outside the setting of a clinical
trial.
Available data demonstrate that
chemotherapy and tamoxifen are additive in
their impact on survival when employed as
adjuvant treatment of breast cancer.
Therefore, most patients with hormone
receptor positive tumors who are receiving
chemotherapy should receive tamoxifen.
At the present time, there are no
convincing data to support the use of any
known biological factor in selecting a
specific adjuvant chemotherapy regimen in
breast cancer. Future prospective studies
are needed to determine if such factors in
an individual patient (e.g., HER-2/neu
overexpression) should influence the
choice of adjuvant cytotoxic therapy.
Despite the favorable impact of adjuvant
chemotherapy on long-term survival in
breast cancer, it is important to
determine whether there are specific
patient populations for whom it is
reasonable to avoid the administration of
cytotoxic chemotherapy. Unfortunately,
very limited information is available to
answer this important question. On the
basis of available data, it is accepted
practice to offer cytotoxic chemotherapy
to most women with lymph node metastases
or with primary breast cancers larger than
1 cm in diameter (both node-negative and
node-positive). For women with
node-negative cancers less than 1 cm in
diameter, the decision to consider
chemotherapy should be individualized.
Similarly, in patients with small,
node-negative breast cancers with
favorable histologic subtypes, such as
tubular and mucinous cancers,
retrospective data support long-term
survival following primary therapy without
the need for adjuvant chemotherapy.
There are limited data to define the
optimal use of adjuvant chemotherapy for
women more than 70 years of age. It is
likely that there is a survival benefit
associated with the administration of
chemotherapy in this patient population.
There is legitimate concern, however,
regarding the toxicity associated with
cytotoxic regimens in this population. In
addition, existing comorbid medical
conditions and mortality from noncancer
causes will influence the overall benefits
in this group of women. The decision to
treat women over the age of 70 with
adjuvant chemotherapy will need to
consider these factors. Increased
participation of women over 70 in
randomized clinical trials and studies
specifically addressing the value and
tolerance of adjuvant chemotherapy in
these women are urgently needed.
4. For which patients should
post-mastectomy radiotherapy be
recommended?
The standard of care for breast
conservation includes surgery followed by
breast radiotherapy. Before the advent of
effective adjuvant chemotherapy,
post-mastectomy radiotherapy was commonly
employed. Interest in this approach was
revived after several studies identified
patient subgroups with 20 to 40 percent
rates of locoregional recurrence after
mastectomy and chemotherapy. These
subgroups, which included women with four
or more positive lymph nodes or an
advanced primary tumor (a tumor of 5 cm or
greater or a tumor invading the skin or
adjacent musculature), were thought most
likely to benefit from a course of
post-mastectomy radiotherapy.
Recent randomized controlled trials have
demonstrated superior tumor control and
overall survival rates with the addition
of post-mastectomy radiotherapy. A recent
meta-analysis of more than 22,000 women
comparing adjuvant radiotherapy to no
radiotherapy reported an improvement in
locoregional tumor control rates from 70
percent to 90 percent. This resulted in a
significant improvement in the overall
survival rate and in the disease-specific
survival rate after a followup time of 20
years. These findings lend support to the
concept that improving locoregional tumor
control rates in breast cancer can lead to
an improvement in survival rates.
The potential benefits of post-mastectomy
radiotherapy must be weighed against both
the acute and long-term side effects of
this therapy. The same meta-analysis
documented an excess of non-breast cancer
deaths, the majority of which were
vascular in nature. These deaths were
probably related to the high radiotherapy
doses received by the heart and great
vessels through the use of outdated
radiotherapy techniques. Contemporary
radiotherapy delivery employing
image-based planning has substantially
reduced the radiotherapy dose received by
these structures. Although the duration of
followup of women treated with modern
techniques is more limited, preliminary
data show no apparent increase in vascular
deaths. Post-mastectomy radiotherapy,
however, is associated with an increased
risk of arm edema.
There is evidence that women with a high
risk of locoregional tumor recurrence
after mastectomy will benefit from
postoperative radiotherapy. This high-risk
group includes women with four or more
positive lymph nodes or an advanced
primary tumor. Post-mastectomy
radiotherapy must be coordinated with
adjuvant multiagent chemotherapy and/or
hormonal therapy. Radiotherapy should not
be delivered concurrently with
anthracycline chemotherapy and should be
delivered within the first 6 months
following mastectomy. In most
circumstances, combined modality adjuvant
therapy begins with several courses of
chemotherapy. Radiotherapy, as part of
such treatment programs, should be
delivered with modern techniques designed
to reduce the volume of heart and great
vessels receiving radiotherapy. At this
time, the role of post-mastectomy
radiotherapy for women with one to three
positive lymph nodes remains uncertain and
is being examined in a randomized clinical
trial.
5. How do side effects and quality-of-life
issues factor into individual
decision-making about adjuvant therapy?
Adjuvant therapy decisions are complicated
by marginal differences in treatment
results and risk-benefit profiles,
balancing acute effects with long-term
outcomes. Individual patients differ in
the value they place on these issues.
Retrospective studies report that women
may be willing to undergo treatment for as
little as a 1 to 2 percent improvement in
the probability of survival. Clear
communication of benefits and risks is an
essential component in enabling as
informed a joint treatment decision as
possible. Absolute and relative benefits
and risks of therapy must be discussed
openly.
Acute, Long-Term and Late Medical Effects
of Adjuvant Therapy
Adjuvant Chemotherapy
Studies to date have documented a range of
acute and late side effects of adjuvant
chemotherapy that have the potential for
significantly affecting patients' quality
of life. Most acute side effects (e.g.,
nausea and vomiting, mucositis, hair loss,
neutropenia) occur in varying degrees in
the different chemotherapy regimens and
resolve after treatment completion. This
also seems to be true for psychological
distress. Several randomized studies have
found that the psychological distress
patients experience is greater during more
toxic adjuvant chemotherapy treatment,
resolving soon after treatment completion.
Similarly, 1 to 3 years after completing
treatment, the distress levels of cancer
survivors who had undergone any of the
different adjuvant chemoendocrine
therapies equal the levels of those who
had received no further adjuvant therapy.
The simultaneous combination of
chemotherapy plus tamoxifen is associated
with an increased risk of thromboembolism
when compared to tamoxifen alone.
Premature menopause, weight gain, and
fatigue are the most frequent long- and
short-term problems that have been
documented. Several small studies have
documented mild cognitive problems, such
as those in memory, with precise levels of
prevalence and severity yet to be
determined. There is also a very small
increase in the risk of treatment-related
second malignancies and cardiac disease.
Adjuvant Hormone Therapy: Tamoxifen and
Ovarian Ablation
Hot flashes and vaginal discharge have
been the most common side effects
attributed to tamoxifen. Tamoxifen is
associated with a small, increased risk of
endometrial cancer, pulmonary emboli, and
deep vein thrombosis, particularly for
women 50 years old or older. The benefits,
however, far outweigh the risks. Tamoxifen
has not been associated with an increase
in depression, weight gain, nausea and
vomiting, diarrhea, or problems in sexual
functioning.
As with adjuvant chemotherapy, ovarian
ablation is associated with the
development of premature menopause and its
associated symptoms including
osteoporosis.
Decision-making in Adjuvant Therapy for
Breast Cancer
Communication between patients and their
physicians is the primary vehicle through
which complex treatment decisions are
made. This communication will likely be
facilitated through the use of decision
aids, and well-designed patient
information materials about the medical
condition or procedure, treatment side
effects, probabilities associated with
health outcomes, and impact on quality of
life. Findings from current research
suggest that decision aids improve
patients' knowledge about treatment
options, reduce patients' anxiety about
treatment decisions and enhance their
comfort with treatment choices, and
stimulate patients to play a more active
role in joint decision-making with their
physicians.
6. What are promising new research
directions for adjuvant therapy?
During the past decade, major advances in
adjuvant treatment of breast cancer have
resulted from analyses of large
prospective randomized trials. In the
United States, however, fewer than 3
percent of cancer patients are entered in
clinical trials. To achieve continued
improvements in adjuvant treatment,
efforts should be made to improve patient
and physician participation in these
studies. A number of important questions
remain to be answered.
Randomized clinical trials should be
conducted to better define the risks and
benefits of continuing tamoxifen therapy
beyond 5 years. Studies are also needed to
expand experience with ovarian ablation,
to explore the value of combined hormonal
therapy, and to determine whether optimal
hormonal therapy is equivalent, superior,
or additive to chemotherapy in
premenopausal women whose tumors express
hormone receptor protein. The risks and
benefits of new, selective estrogen
receptor modulators (SERMs) and aromatase
inhibitors should also be examined in the
adjuvant setting.
Randomized clinical trials evaluating the
roles of high dose chemotherapy and
taxanes need to be completed to determine
whether these treatments have a role in
the standard management of breast cancer.
Additional studies are also needed to
determine the importance of variations in
the doses and schedules of the drugs used
in chemotherapy regimens that are
currently accepted as being standard. A
particular emphasis should be placed on
carefully designed studies to determine
the clinical and biological
characteristics that may more accurately
predict the effectiveness of specific
adjuvant treatments in individual
patients. As yet unproven treatments that
must be critically evaluated in
prospective trials in the adjuvant setting
include trastuzumab, bisphosphonates, and
newer chemotherapeutic and biologic
agents.
To date, prospective trials of adjuvant
therapy have failed to include sufficient
numbers of women older than 70 years.
Studies need to be designed that will
determine the effectiveness of adjuvant
therapies in this group of women.
The role of post-mastectomy radiotherapy
in women with 1 to 3 positive lymph nodes
needs to be determined. Investigators
should continue to explore the importance
of risk factors for recurrence after
mastectomy to improve the selection of
patients who may benefit from adjuvant
radiotherapy. To maximize the possible
benefit of adjuvant radiotherapy, new
radiation techniques should be developed
that further reduce the radiation dose to
normal tissues, such as the heart and
lungs.
Although adjuvant therapy has been found
to produce significant improvements in
survival, the ability to predict the value
of these treatments in individual patients
is limited. The development of accurate
predictors of treatment efficacy would
permit better targeting of treatments,
improving efficacy and reducing the
morbidity and cost of treatment. It is
essential that the value of predictive and
prognostic factors be evaluated using
standardized protocols in well-designed
clinical studies with sufficient
statistical power to detect clinically
important differences. Successful
integration of new technologies, such as
tissue and expression microarrays and
proteomics, will depend on careful design
and analysis of clinical investigations.
The value of sentinel lymph node biopsy
and of sensitive assays for
micrometastatic disease in lymph nodes and
bone marrow should also be important
priorities for clinical research.
Quality-of-life and late-effect
evaluations should be judiciously
integrated into selected clinical trials
to better discern the acute and long-term
influence of treatment on patients and
their families. Interventions should be
sought that will reduce side effects and
improve quality of life. Decision aids and
other techniques should be developed and
evaluated for their ability to improve
patients' involvement and understanding of
treatment decisions.
Conclusions
During the past 10 years, substantial
progress has been made in the treatment of
invasive breast cancer. For the first
time, breast cancer mortality rates are
decreasing in the United States.
Refinements of adjuvant treatment have
contributed to this advance.
Generally accepted prognostic and
predictive factors include age, tumor
size, lymph node status, histological
tumor type, grade, mitotic rate, and
hormonal receptor status. Novel
technologies, such as tissue and
expression microarrays and proteomics,
hold exciting potential. Progress,
however, will depend on proper design and
analysis of clinical and pathological
investigations.
Decisions regarding adjuvant hormonal
therapy should be based on the presence of
hormone receptor protein in tumor tissues.
Adjuvant hormonal therapy should be
offered to women whose tumors express
hormone receptor protein. At present five
years of tamoxifen is standard adjuvant
hormone therapy; ovarian ablation
represents an alternative option for
selected premenopausal women. Adjuvant
hormonal therapy should not be recommended
to women whose tumors do not express
hormone receptor protein.
Because adjuvant polychemotherapy improves
survival, it should be recommended to the
majority of women with localized breast
cancer regardless of nodal, menopausal, or
hormone receptor status. The inclusion of
anthracyclines in adjuvant chemotherapy
regimens produces a small but
statistically significant improvement in
survival over nonanthracycline-containing
regimens.
Available data are currently inconclusive
regarding the use of taxanes in adjuvant
treatment of node-positive breast cancer.
The use of adjuvant dose-intensive
chemotherapy regimens in high-risk breast
cancer and of taxanes in node-negative
breast cancer should be restricted to
randomized trials. Ongoing studies
evaluating these treatment strategies
should be supported to determine if they
have a role in adjuvant treatment.
Studies to date have included few patients
older than 70 years. There is a critical
need for trials to evaluate the role of
adjuvant chemotherapy in these women.
There is evidence that women with a high
risk of locoregional tumor recurrence
after mastectomy benefit from
postoperative radiotherapy. This high-risk
group includes women with four or more
positive lymph nodes or an advanced
primary cancer. Currently, the role of
post-mastectomy radiotherapy for patients
with one to three positive lymph nodes
remains uncertain and should be tested in
a randomized controlled trial.
Individual patients differ in the
importance they place on the risks and
benefits of adjuvant treatments.
Quality-of-life needs to be evaluated in
selected randomized clinical trials to
examine the impact of the major acute and
long-term side effects of adjuvant
treatments, particularly premature
menopause, weight gain, mild memory loss,
and fatigue. Methods to support shared
decision-making between patients and their
physicians have been successful in trials;
they need to be tailored for diverse
populations and should be tested for
broader dissemination.
