Cardiovascular Diseases Clinical Trial
Official title:
Novel Cancer Chemotherapeutics and the Vasculature: Endothelial Effects of VEGF Inhibition In Vivo in Man
Recent developments in chemotherapy, particularly VEGF-inhibitor (VEGFI) drugs, have markedly
improved the prognosis of patients with cancer. However, these drugs frequently cause high
blood pressure (hypertension) which can lead to heart attacks, heart failure and stroke and
can limit their use for cancer treatment.
Endothelin-1 is a hormone that causes blood vessels to tighten and may contribute to high
blood pressure associated with VEGFI drugs. Blocking the effects of endothelin-1 may
therefore reduce or prevent VEGFI-associated blood pressure changes, although this has never
been tested in humans.
Our long-term goal is to assess the protective effects of endothelin-1 blocker drugs in
patients treated with VEGFI. Before doing so, we must better explore whether VEGFIs cause
blood vessel narrowing and if endothelin-1 blockers prevent this. We will assess this in
healthy volunteers using a special technique called 'forearm plethysmography'. We will
examine the effect of VEGFI on blood flow and also the effect of simultaneous administration
of endothelin-1 blockers. These will be given at doses that produce local effects in the arm
without affecting the rest of the body.
These studies study will show whether endothelin-1 blockers may help treat VEGFI-associated
hypertension to enable more patients safely to receive vital cancer treatments.
Developments in chemotherapy have improved the prognosis for patients with cancer.1,2
Angiogenesis is essential for tumour growth and metastasis and vascular endothelial growth
factor (VEGF) is fundamental to this process.3,4 Chemotherapeutic VEGF inhibitor (VEGFI)
drugs have revolutionised therapy and improved the prognosis and survival of patients with
previously untreatable malignancies.1,2 Blood pressure elevation is a common complication
that occurs in up to 80% of patients treated with VEGFI and almost all patients have an
absolute increase in blood pressure, with 30-60% developing frank hypertension.1,5 Patients
are at risk of acute hypertensive complications, including stroke, acute coronary syndrome or
reversible leukoencephalopathy and the development of VEGFI-associated hypertension may
mandate the premature discontinuation of these important anti-cancer therapies. Those who
survive their cancer are at risk of developing end-organ damage leading to ischaemic heart
disease, heart failure, renal failure and stroke.1,5 Indeed, with substantially increased
cancer survivorship patients often survive long enough to allow cardiovascular morbidity to
take precedence over their initial cancer diagnosis.
Mechanisms contributing to the development of VEGFI-associated hypertension may include
endothelial dysfunction, capillary rarefaction and vascular remodelling.1,5 Endothelin-1
(ET-1) is a potent endogenous vasoconstrictor and is strongly implicated in the pathogenesis
of hypertension and endothelial dysfunction. 3,6,7 However, the effects of VEGFI on
endothelial function and the role of ET-1 in VEGFI-associated hypertension are incompletely
defined. Indeed, there is a paucity of information on mechanisms contributing to
VEGFI-induced hypertension and our study will address this key issue.
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