Breast Cancer Clinical Trial
Official title:
A Phase III Multicentre Double Blind Randomised Trial of Celecoxib Versus Placebo in Primary Breast Cancer Patients
It has been found that the chemical changes that take place in a patient's body during the
development of inflammation may provide an environment which stimulates cancer cells. One
step in the development of inflammation is the production of certain chemical substances
which are important in the formation and spread of tumours. These are called prostaglandins.
Cyclo-oxygenase II (COX-2) is an enzyme (a substance that speeds up chemical changes in the
body) involved in the production of these prostaglandins and although it is not usually
present in most tissues it is made at the sites of inflammation. Celecoxib is a selective
Non-Steroidal Anti Inflammatory Drug (NSAID) which works by blocking the action of the COX-2
enzyme, leading to a decrease in the production of prostaglandins and a reduction in
inflammation.
The purpose of this study is therefore to find out if celecoxib can be used after breast
cancer treatment (chemotherapy and/ or radiotherapy) to reduce inflammation and thus reduce
the ability of new tumours to grow and survive.
2590 women with primary breast cancer will be recruited in this study from several locations
in the United Kingdom and Germany. Eligible patients will be randomly allocated a treatment
group, which can be celecoxib or placebo. Both treatments are taken orally (celecoxib 400mg
daily, placebo 2 tablets daily) for a total of 2 years. In addition, hormone receptor
positive patients will receive endocrine treatment as per local practice. Patients will
prematurely discontinue treatment with celecoxib/placebo if disease progression is confirmed
or if patients experience unacceptable toxicity.
Patients will be seen every 6 months for the first 3 years and then off treatment follow-up
is carried out annually. Participating patients will also be given the option to take part in
the pathology sub-study by donating a sample of the tumour tissue collected at the time of
the primary surgery.
It has long been recognised that there is an association between chronic immune activation
and cancer but the mechanisms behind this observation are not fully understood. The
inflammatory process may provide an environment for development of malignant disease, with
mediators of inflammatory response such as the cyclo-oxygenases playing an important role and
providing a target for therapeutic intervention.
Prostaglandins (PGs) are synthesised from phospholipids by the action of phospholipase A2 and
cyclo-oxygenases. Cyclo-oxygenase (COX) -1 differs from COX-2 in that the latter is inducible
and its expression is induced by a large range of oncogenes and growth factors. Celecoxib is
a selective COX-2 inhibitor that does not cause the effects of COX-1 inhibition, namely
gastrointestinal ulceration.
The key regulatory step in this process is the enzymatic conversion of fatty acids to PGG2
and PGH2 by COX. PGH2 is subsequently converted to one of several structurally related PGs
including PGE2, PGD2, PGF2, and thromboxane A2 (TxA2), by the activity of specific PG
synthases. PGs have important functions in every organ system and regulate a variety of
physiological functions such as immunity, maintenance of vascular integrity and bone
metabolism. COX-2 is not normally expressed in most tissues, but is induced by a wide
spectrum of growth factors and pro-inflammatory cytokines in specific pathophysiological
conditions. The expression of COX-2 is highly induced in cells transformed with the oncogene
v-src or treated with phorbol esters.
Several studies have suggested an association between non-steroidal anti-inflammatory drug
(NSAID) consumption and decreased breast cancer risk.
Elevated COX expression in breast cancer was suggested some time ago by the finding of
elevated PG production in breast tumours.
There is pharmacological and genetic evidence to indicate that a significant component of the
anticancer property of NSAIDs is due to their ability to inhibit the COX-2 enzyme.
This phase III randomised study assesses the impact on disease free survival and overall
survival of the Cox-2 inhibitor Celecoxib as maintenance therapy following surgery and
chemotherapy in the treatment of primary breast cancer.
2590 women with primary breast cancer will be recruited in this study from several locations
in the United Kingdom and Germany.
Prior to randomization all patients should have completed at least 4 cycles of (neo) adjuvant
chemotherapy. Patients who satisfy all the eligibility criteria for the study will be
informed and consented to join the study. The Local Investigator will then contact the ICCG
randomization centre to randomize the patient by fax or by telephone.
1. Assessments required pre-randomisation
- Complete history and physical examination (within 4 weeks before randomisation)
- Haematology (Hb, WBC or ANC, platelets) & Biochemistry [serum bilirubin,
creatinine, alkaline phosphatase] (within 4 weeks before randomisation)
- Mammogram, Chest X-ray, liver ultrasound, bone scan (at a maximum 00 months prior
to diagnosis of breast cancer). In case of clinical symptoms metastatic disease has
to be excluded before randomisation by the appropriate investigations
- Collection of tissue blocks for the central tumour banks at Glasgow Royal Infirmary
(for sites managed by ICCG) land Studienzentrale in Frankfurt (for sites managed by
GBG)
2. Treatment
Treatment must begin within 14 working days after randomisation and within 12 weeks of
day 1 of the last cycle of adjuvant chemotherapy. Radiotherapy should be given according
to local policy (concomitant trial treatment and radiotherapy is permitted). Patients
will be randomised 2: 1 (in favour of celecoxib) to receive:
Two Placebo capsules twice daily with food or Two Celecoxib 200mg capsules twice daily
(800mg per day) with food The duration of celecoxib/placebo treatment is 2 years. In
addition all postmenopausal ER + and/or PgR+ postmenopausal patients will receive
exemestane (25mg daily) for 5 years. The start of the treatment will be at same time as
starting celecoxib or placebo.
3. Routine Follow up Visits During the course of the trial all patients will be followed up
every 3 months in the first year, every 6 months in !years 2 and 3 and annually from
year 4 onwards.
Follow up Assessments
- Clinical examination and history
- Haematology & biochemistry
- Metastatic screen -additional tests/investigations (eg. Bone/liver scan etc) are at
the investigators discretion if clinically indicated.
- Serious Adverse Events
4. Follow up upon relapse Any relapse requires treatment to be stopped and patients should
have the minimum tests carried out as described in section (c) above.
Relapse is categorized as ipsilateral breast or axillary nodal relapse [loco regional]
distant relapse (including supraclavicular nodes) [distant] and contralateral breast disease
(malignant) [2nd primary]. In the event of tumor recurrence the relevant recurrence form
should be completed and the trials office notified within 4 weeks.
All patients will be followed up long term irrespective o whether they have been withdrawn
from treatment prematurely.
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