Obesity Clinical Trial
Official title:
Evasion of Immune Editing by Circulating Tumour Cells in an Exercise Modifiable Mechanism Underlying Aggressive Behaviour in Obese Men With Prostate Cancer
Obesity, known to be associated with a pro-inflammatory, pro-thrombotic humoral milieu, confers a worse prognosis in prostate cancer (PrCa). Circulating tumour cells (CTCs) are identified in the blood in advanced cancer. Their quantitation provides prognostic information. "Cloaking" of CTCs by adherent platelets impedes natural killer (NK)-cell clearance of CTCs from the circulation, enhancing metastatic spread. NK-cell function in blood and in solid organs is quantitatively and qualitatively reduced in obesity. Platelet cloaking may be enhanced in obesity due to the pro-inflammatory, pro-thrombotic state, and may be a mechanism for worse cancer-specific outcomes in this group. Obesity and its biochemical effects may be influenced by lifestyle changes such as exercise. Physical activity reduces levels of systemic inflammatory mediators and so an aerobic exercise intervention may represent an accessible and cost-effective means of ameliorating the pro-inflammatory effects of obesity. The ExPeCT trial will determine if a prescribed exercise intervention can ameliorate the degree of platelet cloaking in obese and non-obese men with advanced prostate cancer.
The overarching hypothesis is that enhanced platelet cloaking of circulating tumour cells in
obese men with prostate cancer, due to increased systemic inflammation, is a mechanism
underlying worse prognosis of cancer in these patients.
The investigators aim to test the following four hypotheses, dividing the experimental and
analytical work into four separate projects.
1. Platelet cloaking of circulating PrCa tumour cells is more prominent in men with obesity
than without
2. Regular exercise can ameliorate platelet cloaking
3. The degree of platelet cloaking varies with levels of systemic and primary tumour
inflammation and coagulability
4. Expression of an obesity-associated lethality gene signature leads to variation in
platelet cloaking
For the first hypothesis, 200 men with metastatic PrCa will be recruited, and divided into
exposed and non-exposed groups based on body mass index (BMI >25). The objective will be to
enumerate CTCs and quantify the degree of platelet cloaking in exposed and non-exposed
groups, and to draw meaningful comparisons between the two.
For the second hypothesis, the objective will be to determine to what extent the number of
CTCs and the degree of platelet cloaking varies in exposed and non-exposed groups following a
supervised exercise intervention, and to compare this with a non-exercised comparison group.
The exercise intervention will prescribe moderate intensity aerobic exercise that will be
supervised once per week for 3 months and completed independently at home for a further 3
months. Patients will wear Polar heart rate monitors to monitor exercise prescription and
progression. Assessments including blood sampling and quality of life questionnaires will be
completed at baseline, 3 months and 6 months.
For the third hypothesis, the objective will be to build a serological, haematological and
immunological picture of the state of systemic inflammation and coagulability, and the degree
of inflammation within the prostate gland. Furthermore, the investigators intend to correlate
and compare these variables with the results of the first and second objectives, in order to
determine whether the number of CTCs and the degree of platelet cloaking varies with changes
in the inflammatory / coagulatory milieu.
For the fourth hypothesis, the objective will be to determine whether the expression profile
of a number of lethality-associated genes, known to be associated with PrCa progression,
coagulation and stem-cell like phenotype, correlates with the number of CTCs and the degree
of their cloaking by platelets.
CTC numbers and the degree of platelet cloaking will be common denominators which anchor
these four objectives together and enable comparison between them.
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