Cardiovascular Risk Factor Clinical Trial
Official title:
Estudio clínico Fase III Para Evaluar la Eficacia terapéutica en Pacientes Mexicanos Con Dislipidemia Mediante el Uso vía Oral de L-Carnitina + Atorvastatina Comparado Con Atorvastatina
Clinical Trial Phase III, experimental, simple blind, randomized with two treatment groups,
multicentric, longitudinal, to evaluate the therapuetic efficacy to dislipydemias in mexican
adult population. This trial includes homogeneus populations that could be comparable by
their disease condition, biologic characteristics and sociodemographics characteristics.
2 Treatment groups: Experimental Group: Oral Administration of L-carnitine (1g) + Oral
Atorvastatin (20mg), every 24 hours for 6 months.
Active control group: Oral Administration of Atorvastatin 20mg every 24 hours for 6 months.
Sample Size: 120 subjects, females or males between 35 to 75 years old. Laboratory tests:
Hematic biometry, quimical blood components, electrocardiogram and pregnancy urinary test.
General objectives:
Evaluate the therapeutic efficacy in Mexican adults with dyslipidemia through the oral route
use of L-carnitine + atorvastatin in comparison with the use of Atorvastatin, after six
months of treatment.
Evaluate the safety of the medicines under study.
Hypothesis:
The combined use of L-carnitine + atorvastatin offers therapeutic superiority with respect to
the use of atorvastatin as treatment to reduce the percentage of C-LDL in patients with
dyslipidemia.
The combination of L-carnitine + atorvastatin shows fewer incidences in the presence of
adverse events attributable to the medicine in comparison to the use of atorvastatin as
mono-therapy, in the treatment of dyslipidemia patients.
Design:
Phase III clinical assay, experimental randomized with two treatment, multi-centered,
longitudinal, to evaluate the therapeutic efficacy in dyslipidemias of Mexican adults.
Material and Methods:
Sample Size 120 subjects will be included. Inclusion Criteria Mexicans between 35 and 75
years of age. Gender indistinct. Patient with abnormal lipid profile considered as serum
levels of C-LDL of 100mg/dl or greater obtained by laboratory parameters.
Not under pharmacologic treatment to handle their dyslipidemia or accepting to suspend their
current treatment and be evaluated for their inclusion in the next 3 weeks starting on the
day of the initial evaluation.
Women in fertile stage with a safe, hormonal-free family planning method. A safe planning
method includes surgical methods in women, intrauterine device that doesn't release
progestines and use of preservative in all their sexual relations.
Women in fertile stage who don't wish to become pregnant during their participation in the
study.
Post-menopause women or with hysterectomy history. Have a fixed and/or mobile telephone and
accept to receive calls from the site for study processes.
Grant their duly informed consent. Exclusion Criteria Subject lacking the mental capacity to
understand the processes which imply their participation in the study and thus,not capable of
granting their participation in a voluntary manner.
History of hypersensitivity to the medicines being studied. Daily intake of at least 240ml of
grape juice or sporadic ingestion of 1 liter. Potentially fertile women without a safe family
planning method, who wish to become pregnant during the study, are already pregnant or in
lactation period.
Having on Globorisk scale for Mexicans, or as an associated risk factor, a high
stratification for cardiovascular risk.
Basal laboratory values with elevation of ALT 1.5 times larger than the upper limit
considered normal according to international units.
Basal laboratory values with elevation of CPK not attributable to physical activity.
Subjects who are under anti-coagulant treatment, suffer from coagulation disorders, or any
circumstance which contraindicates the taking of a blood.
History of acute myocardial infarction, unstable angina, some confirmed coronopathy,
arrhythmias, congestive cardiac failure or cerebrovascular disease.
History of muscular conditions of the genetic type or of rhabdomyolysis in patient or first
degree relative.
History or diagnose of congenital hepatic disorders, chronic infection by hepatitis virus,
hepatitis with fatty liver, alcoholic hepatitis, primary biliary cirrhosis, primary
sclerosis, cholangitis or hepatic failure.
History or diagnose of congenital renal disorders, chronic renal failure, acute renal damage
or nephritic syndrome.
History of infection by Human Immunodeficiency Virus. History of Acute or Chronic
Pancreatitis. History of the following endocrine diseases: non-controlled Diabetes Mellitus,
lipodystrophy, thyroid disorders, Cushing Syndrome and/or Polycystic Ovary Syndrome.
Diseases which compromise immunity such as Systemic Lupus Erythematous, Rheumatoid Arthritis,
Antiphospholipid Antibodies Syndrome or Psoriasis.
Diseases by deposit such as Gaucher Disease, disease by glycogen deposit, Tay-Sachs juvenile
disease or Niemann Pick Disease.
Diagnose of Kawasaki Disease, Werner Syndrome, intermittent acute Porphyria, Idiopathic
Hyperkalemia or Klinefelter Syndrome.
Suffer from Idiopathic Hyperkalemia, Klinefelter Syndrome, Werner Syndrome, Kawasaki Disease
or Porphyria.
History of epilepsy. History or diagnose of alcoholism. Intake of more than 20g of alcohol
per day. User of marihuana. User of illegal drugs.
Intake of medicines with pharmacologic interaction which increase or decrease the efficacy of
L-Carnitine and/or atorvastatin or alter the lipids in blood such as:
Macrolide antibiotics: Erythromycin, Telithromycin and Clarithromycin. Azole anti-fungi:
Ketoconazole, Itraconazole, Fluconazole and Nefazodone. Quercetin, Amiodarone, Aprepitant,
Cimetidine, Ciprofloxacin, Cyclosporine, Diltiazem, Imatinib, Echinacea, Enoxacin,
Ergotamine, Metronidazole, Mifepristone, Tofisopam, Gestodene, Verapamil, Mibefradil,
Fluoxetine, Phenobarbital, Carbamazepine, Phenytoin, Rifampin, Modafinil, Glucocorticoids,
Felbamate, Rosiglitazone, Griseofulvin, Pioglitazone, Gemfibrozil, Clofibrate, Fenofibrate,
Niacin, Nefazodone, Cholestyramine, Colchicine, Colestipol, Primidone, Topiramate,
Troglitazone, Rifabutin, Digoxin, Thiazides, anabolic Steroids, Progestogens, Estrogens,
Danazol, Amiodarone, fibric Acid, docosahexaenoic acid, Isotretinoine, Immunosuppressives,
protease inhibitors of HIV or of the Hepatitis C Virus, Inhibitors of the co-transport of
sodium-glucose, Tamoxifen, Raloxifene, non-selective Beta blockers, biliary acid
sequestrants, asparginase, Sirolimus and Interferon.
Patients who have been diagnosed with terminal conditions. Patients with recent Cancer
diagnose or undergoing any type of therapy for same. Patients who have suffered skin cancer
not of the melanoma type and have been cured and haven't been on treatment for at least 1
year before the start of their participation in the study may enter.
Patients under lipid lowering treatment and who, because of their clinical condition aren't
candidates to the period of lavage or detoxification; or well reject same.
Been participating in another clinical trial or having concluded their participation in the
30 days previous to beginning their participation in this study.
Any other which, at the Investigator's criteria, puts at risk the safety of the participant
and/or interferes with the results of the study.
Medicine L-Carnitine, Atorvastatin Dose L-Carnitine 1 g + Atorvastatin 20 mg daily for 6
months and Atorvastatin 20 mg daily for 6 months
Efficacy criteria:
The efficacy of the combined treatment vs. atorvastatin in mono-therapy for dyslipidemia will
be compared, through evaluation of the variability of the biochemical parameters at the start
and end of the study.
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