Healthy Volunteers Clinical Trial
Official title:
Study of Biochemical Markers to Determine the Acetylsalicylic Acid Chemopreventive Effect Through Antiplatelet Action
This study in healthy volunteers is the first step in developing a collaborative research
program, which seeks to test the hypothesis that chemopreventive effect of acetylsalicylic
acid (ASA) on colon cancer is due predominantly to its antiplatelet effect.
The following features of the clinical evidence are consistent with the platelet-mediated
hypothesis:
1. The apparent saturability of the chemopreventive effect of ASA at low doses given once
daily, found in long-term analyses of cardiovascular and adenoma recurrence randomized
clinical trial, as well as in the vast majority of observational studies performed in
different settings and with different methodology. A remarkably similar saturability of
the cardioprotective effect of low dose ASA given once daily is explained by the
irreversible nature of cyclooxygenase (COX)-1 inactivation in platelets, and limited
capacity of human platelets for de novo protein synthesis.
2. Given the short half-life of ASA in the human circulation (approximately 20 min) and
the capacity of nucleated cells to resynthesize the acetylated COX-isozyme(s), it seems
unlikely that a nucleated target could be suppressed throughout the 24-h dosing
interval.
3. One of the cardiovascular randomized clinical trial (Thrombosis Prevention Trial) in
which the chemopreventive effect of ASA was detected on long-term follow-up, involved
the administration of a controlled-release formulation of ASA (75 mg) with negligible
systemic bioavailability.
4. Enhanced platelet activation and thromboxane (TX)A2 generation in vivo has been
demonstrated in patients with colorectal cancer and in Familial Adenomatous Polyposis
patients.
So, the main objective of this study is to assess the extent of acetylation at serine-529 of
platelet COX-1 after the 1st and 7th dose of low-doseof enteric-coated ASA 100 mg daily.
Changes of this novel biomarker of ASA action will be correlated to other known parameters
of ASA PK and PD: i) Tmax, Cmax and AUC of ASA and salicylate in the peripheral circulation
after oral dosing; ii) time to obtain the maximal antiplatelet effect by ASA and its
persistence throughout the dosing interval as assessed by measuring the inhibition of
platelet COX-1 activity in whole blood ex vivo, the inhibition of platelet aggregation in
whole blood ex vivo and the inhibition of the systemic generation of TXB2.
This study will be performed in healthy subjects, under fasting conditions, and it will
allow to acquire more information on the pharmacokinetics (PK) and pharmacodynamics (PD) of
low-dose enteric-coated ASA, and to characterize the variability (coefficient of variation),
accuracy and precision of a novel biomarker of ASA action, i.e., quantification of the
extent of COX-1 acetylation at serine-529, using a stable isotope dilution liquid
chromatography multiple reaction monitoring/mass spectrometry (LC-MS) technique. This
biomarker will be then used in another clinical study in the target population, i.e. FAP
patients, treated with low-dose ASA which that will be performed by Prof Angel Lanas
(University of Zaragoza, Spain).
Twenty four healthy volunteers recruited among the hospital and laboratory personnel will be
enrolled and treated with ASA (100 mg enteric-coated tablet per day, Adiro) for 1 week.
Blood samples will be collected at baseline (before treatment) and at 0.5, 1, 2, 3, 4, 5, 6,
7, 8, 10, 12 and 24 h after the first and the last dose of ASA to assess the extent of
inhibition of serum TXB2, as an index of platelet COX-1 activity, and plasma levels of ASA
and salicylate and the extent of COX-1 acetylation in circulating platelets. Moreover, the
investigators will assess the extent of inhibition of platelet aggregation in whole blood by
the PFA-100 system. Twenty four hours urine samples will be also collected to measure
11-dehydro-TXB2 (TX-M), an index of systemic TXA2 biosynthesis in vivo.
Healthy subjects will take their daily ASA under fasting conditions and will abstain from
the use of ASA and other NSAIDs for at least 2 weeks before enrolment.
All volunteers will be attended at the Clinical Research Unit of the University Hospital
Lozano Blesa.
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Endpoint Classification: Safety/Efficacy Study, Intervention Model: Single Group Assignment, Masking: Open Label, Primary Purpose: Prevention
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