Study design: Single-center, prospective, randomized, double-blind, placebo-controlled,
parallel-group clinical study.
Primary Outcome: To compare platelet aggregation in the dapagliflozin and placebo groups
by the Multiplate Analyzer® test (using ADP as an agonist) in hospitalized patients with
a diagnosis of AMI within seven days of evolution, using dual antiplatelet therapy with
acetylsalicylic acid (ASA) and an anti-platelet ADP, 48 ± 12 hours after starting
dapagliflozin/placebo treatment. Due to the rapid oral absorption of the medication,
reaching maximum plasma concentration after 2 hours and as its pharmacokinetics does not
change with food or other concomitant medications, our hypothesis is that there may be an
antiplatelet effect that can be detected early
Other exploratory analyses:
compare B-type natriuretic peptide (BNP) and troponin biomarkers between
dapagliflozin and placebo groups at 30 (± 5) days after randomization;
Correlation between levels of ultrasensitive C-reactive protein (us-CRP) and
platelet aggregability;
Compare hsCRP levels in dapagliflozin and placebo groups at 30 (± 5) days;
Compare the size of the AMI assessed by peak CK-MB mass and troponin in the
dapagliflozin and placebo groups;
Compare the behavior of glycemia in the dapagliflozin and placebo groups, taking
into account the following parameters: calculation of the glycemic mean (±SD) of
capillary blood glucose tests (remote laboratory tests) during 48 hours after
randomization; incidence of hypoglycemia (blood glucose below 70 mg/dl) and severe
hypoglycemia (glycemia below 40 mg/dl) during hospitalization; calculation of the
average insulin used during 48 hours after randomization;
Compare, in the dapagliflozin and placebo groups, the levels of creatinine, urea and
hematocrit analyzed immediately after randomization and before starting treatment,
and 30 (± 5) days after randomization;
Test of lipid transfer from artificial nanoemulsion to HDL in dapagliflozin and
placebo groups at inclusion and at 30 (± 5) days after randomization: EDTA plasma
samples in a volume of 200 μL will be incubated with 50 μL nanoemulsion artificial
in 3H-cholesteryl-esters and 14C-phospholipids or with free 14C-cholesterol and
3H-triglycerides. After 1h in agitation of the bath at 37 ºC, the precipitation
reagent consisting of 250 μL of the solution with 0.02% dextran sulfate (50,000 MW)
and 0.3 mol / L of MgCl2 will be added to the incubation, which will then be mixed
for 30 seconds and centrifuged for 10 min (3000g). Finally, 250 μL of the
supernatant is transferred to counting vials containing 5 μL of scintillation
solution (Packard BioScience, Groeningen, The Netherlands) and the radioactivity
measured with a Packard model TR 1600 liquid scintillation analyzer (Palo Alto, CA).
Blank plasma samples will be replaced by 200 μL of TRIS solution. The radioactive
transfer results from the nanoemulsion to HDL will be expressed as % of the total
incubated radioactivity found in the supernatant containing HDL.
Compare the diuresis obtained during 48 hours after randomization in the Coronary
Intensive Care Unit, in the dapagliflozin and placebo groups.
Compare, in the dapagliflozin and placebo groups, autonomic modulation, vascular
autonomic control and assessment of baroreflex control by means of a 10-minute
electrocardiogram, after inclusion and before the start of treatment, and 30 (± 5)
days after randomization .
Analyze the primary objective of the study in the following pre-specified subgroups:
obese (BMI ≥ 30 Kg/m2) and non-obese;
male and female sex;
elderly (≥ 65 years) and non-elderly;
smokers and non-smokers;
time since diagnosis of diabetes (≥ or < 10 years);
basal blood glucose ≥ 125 mg/dL and < 125 mg/dL;
glycated hemoglobin (HbA1c) ≤ 9.0% and > 9.0%;
use of clopidogrel or ticagrelor;
treatment performed for the acute coronary event: percutaneous coronary intervention
or clinical treatment;
ejection fraction ≤ 40% and > 40%.
Diabetics and non-diabetics
Onset of symptoms ≤ 72 hours and > 72 hours
Study plan: Eligible patients will be enrolled within the first seven days of symptom
onset. After signing the Informed Consent Form, laboratory tests will be collected, as
previously specified in the methodology. Subsequently, patients will be randomized to use
dapagliflozin or placebo in a double-blind manner. Randomization will be performed using
the Graphipad® program, with distribution of numbered vials containing the study
medication (dapagliflozin 10 mg tablets or placebo-equivalent), randomly between the two
groups. All patients must be using dual antiplatelet therapy and the results will be
stratified by the type of treatment performed for AMI. Study medication, once initiated,
will be maintained until the final platelet assessment, scheduled for 30 days, is
performed. The other medications, including other oral antidiabetics and insulin, will be
used according to the institution's routines, except for prohibited medications, as
stated in the exclusion criteria. After the end of the study, the sealed envelopes will
be opened to identify the blinding codes.
Glycemic control: According to institutional routines, the cut-off value of 140 mg/dL
will be used in two sequential capillary blood glucose levels as the threshold for
starting treatment with subcutaneous insulin. Patients whose diabetes control is not
adequate, as evidenced by a capillary blood glucose value maintained greater than 250
mg/dL, will receive the intravenous insulin protocol, also in accordance with the
institutional routines (summary below).The HbA1c target will be of < 7.5%.
Inclusion criteria:
Men and women aged ≥ 18 years (women of childbearing age must have a negative
pregnancy test)
In routine use of dual antiplatelet therapy with ASA plus an ADP receptor
antagonist, according to institutional routines;
Acute myocardial infarction, with or without ST-segment elevation (STEMI/NSTEMI)
defined according to the 4th Universal Definition of Acute Myocardial Infarction,
with up to 7 days of evolution from the onset of symptoms;
Signature of the Free and Informed Consent Term.
Exclusion criteria:
Current or recent (within 24 months) treatment with pioglitazone and/or use of
pioglitazone for a total of 2 years or more during a lifetime at any time;
Current or recent (within 12 months) treatment with rosiglitazone;
Chronic use (>15 consecutive days) of any SGLT2 inhibitor at the time of
hospitalization;
Chronic use (>30 consecutive days) with an oral steroid at a dose equivalent to
prednisolone ≥10 mg (eg, betamethasone ≥1.2 mg, dexamethasone ≥1.5 mg,
hydrocortisone ≥40 mg) per day;
systolic BP > 180 or diastolic BP > 100 mmHg at randomization;
Diagnosis of Type 1 diabetes mellitus, MODY (maturity onset diabetes of the Young)
or diabetes mellitus secondary to diverse endocrinopathy, pancreatic resection,
medication, pancreas neoplasia or chronic pancreatitis;
History of bladder cancer or history of radiation therapy to the lower abdomen or
pelvis at any time;
History of any other malignancy within 5 years (with the exception of skin cancers
successfully treated non-melanoma);
Chronic cystitis and/or recurrent urinary tract infections (3 or more in the last
year);
Any condition that, in the opinion of the Investigator, may render the research
participant unfit to complete the study, including, but not limited to,
cardiovascular disease (KILLIP > 2, modified Forester > IIa,recurrent ventricular
arrhythmias) or non cardiovascular (eg, active malignancy other than basal cell
carcinoma, cirrhosis, chronic lung disease, severe autoimmune disease);
Pregnancy or lactation;
Active participation in another clinical trial
Patients with septic shock or severe glycemic decompensation requiring the use of IV
insulin at the time of randomization;
TGP/ALT(Alanine Amino Transferase) >3x the upper limit of normality (ULN) or total
bilirubin >2.5 x ULN;
Estimated glomerular filtration rate (GFR) < 45 ml/min/1.73m² , calculated by MDRD,
or kidney transplant;
Known thrombophilias or thrombocytosis;
Blood dyscrasias or any disorder that causes hemolysis, previously known;
Hematological abnormality (Hb ≤ 11g/dL or > 17g/dL, leukocytes ≤ 4500/mm³ or
>11000/mm³, platelet count <150,000/mm³ or > 450,000/mm³)
Casuistry: To calculate the sample size, the following assumptions were taken into
account consideration :
Aggregability of 482.61 ± 231.82 (area under the curve AUC) in a previous study of
patients with ACS using dual antiaggregation therapy with AAS and clopidogrel;
estimated difference of 33% less in the dapagliflozin group (323.35 ± 231.82 AUC);
alpha of 0.05 and statistical power of 80%. Based on this information, the sample
size was calculated at 70 patients, and in order to compensate for any follow-up
losses, 80 patients (40 in each group) will be included in this project.