Description

The investigators will conduct a randomized controlled trial between April 2024 and April 2025 after the ethics committee of the faculty of medicine at Kafr el-Sheik University approves.

The investigators got written informed consent from all eligible patients or their first order of kin before randomization.

The study will be composed of 2 arms atorvastatin arm, which consisted of 300 patients who received 40 mg daily atorvastatin for 3 months, and the rosuvastatin arm consisted of 300 patients who received 20 mg rosuvastatin daily for 3 months, All the patients in the two groups received open-label aspirin at a loading dose of 75 to 300 mg and then 75 mg daily till the end of the 3 months. and open-label clopidogrel at a loading dose of 300 mg and then 75 mg daily till the end of the 3 months.

Study Procedures:

Every patient in our study will undergo:

Clinical workup: History, clinical assessment & NIHSS were recorded on admission, day 7, and the Modified Rankin Scale as a follow-up after one week and 3 months.

Detection of Risk Factors & Profiles:

Echocardiography& TOE: in indicated patients ECG Monitoring: daily ECG monitoring will be performed in indicated patients. - Carotid Duplex: carotid duplex in indicated patients.

4- ESR & Lipid Profile& liver functions: All will be tested routinely for all patients.

Imaging Follow-UP Non-contrast CT brain on admission Day 2 MRI: After 2 days of admission, all the patients in this study will have a brain MRI (stroke protocol; T1W, T2W, FLAIR, DWI, T2 Echo Gradient, MRA of all intra-cerebral vessels).

CT brain: Any patient with unexplained clinical deterioration at any time throughout his/her hospital stay will be urgently imaged by CT.

Primary End Point:

The primary efficacy outcome was the rate of new stroke at 90 days

• Secondary End Point: the secondary efficacy outcomes were to evaluate the rates of patients who achieved a significant reduction in NIHSS (decrease of four points or more) at the seventh day or discharge compared to baseline, the rates of a favorable outcome with (mRS = 0-2) after one week and after 90 days in a face-to-face interview in the outpatient clinic, rates of the composite of recurrent stroke, myocardial infarction, and death due to vascular events after 90 days of follow-up, while the secondary safety outcome was the rate of treatment-related acute liver injury assessed by ALT, AST test at 90 days, statin-induced myopathy assessed by CPK at 90 days and other adverse effects assessed by a follow-up questionnaire.

        the investigators excluded patients who had clinical seizures at the onset of their stroke,
        as well as those who had symptoms of any major organ failure, active malignancies, or an
        acute myocardial infarction within the previous six weeks, and those who were on warfarin,
        regular ticagrelor during the week before admission, or chemotherapy within the previous
        year.
        The investigators excluded patients with active peptic ulcers, GIT surgery, bleeding
        history within the last year, and those with a history of major surgery within the last
        three months.
        The investigators ruled out of our trial patients who had a known allergy to the study
        drugs and those with INR > 1.4 or P.T. >18 or blood glucose level < 50 or > 400 mg/DL or
        blood pressure < 90/60 or > 185/110 mmHg on admission or Platelets < 100,000.
        The investigators excluded pregnant and lactating patients and those with stroke due to
        venous thrombosis and stroke following cardiac arrest or profuse hypotension ineligible for
        our trial.
        The investigators excluded patients who were regular users of drugs that affect clopidogrel
        metabolism, such as ketoconazole, dihydropyridine calcium channel blockers, and rifampin.