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Clinical Trial Details — Status: Completed

Administrative data

NCT number NCT01563731
Other study ID # 27F201
Secondary ID
Status Completed
Phase Phase 4
First received
Last updated
Start date April 2013
Est. completion date March 31, 2021

Study information

Verified date February 2024
Source Istituto Auxologico Italiano
Contact n/a
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

Stroke is one of the major causes not only of mortality, but of disease burden worldwide, because of residual disability and cognitive decline. Although blood pressure lowering has been clearly shown to be the most effective means for primary and secondary prevention of stroke, the systolic blood pressure (SBP) levels to achieve by treatment in order to optimize prevention results are unknown, and whether SBP levels lower than those usually recommended are accompanied by further or reduced benefits is undecided yet. Likewise, while low-density lipoprotein cholesterol (LDL-C) lowering by statins has been shown to be associated with primary and secondary stroke prevention, whether more intense lowering is or is not of further benefit is unknown. The Stroke in Hypertension Optimal Treatment Trial (ESH-CHL-SHOT) is a factorial 3 x 2 arm, multicenter, randomized clinical trial designed to test the hypothesis that in elderly patients at high risk of recurrent stroke (previous recent stroke or TIA) antihypertensive treatment programs aimed at reducing SBP to the usually recommended values (< 145 to 135 mmHg), to a lower goal (< 135 to 125 mmHg) or to even lower values (< 125 mmHg) will result in progressively greater reductions in recurrent stroke, incidence of cardiovascular outcomes and cognitive decline. Parallely, the preventive efficacy of more and less intense LDL-C reductions will be tested on the same outcomes.


Description:

ESH-CHL-SHOT will randomize about 7500 participants aged > or = 65 years with SBP > or = 140 mmHg or antihypertensive therapy, who have presented a stroke or TIA, within 1 to 6 months before randomization. The trial will investigate 1. the effects of randomization to antihypertensive treatment of different intensities, aiming at three different SBP targets. SBP targets are < 145 to 135, < 135 to 125, < 125 mmHg, with approximate mean inter-target differences of 8 mmHg; 2. the effects of randomization to lipid lowering treatment of different intensity, aiming at two different LDL-C targets. Targets are 2.8 to 1.8 mmol/l (110 to 70 mg/dl) and < 1.8 mmol/l; 3. possible interactions between antihypertensive and lipid-lowering treatments. The primary hypothesis is that recurrent stroke rates will be 25% lower in the lowest vs intermediate SBP target group, 25% lower in the intermediate vs higher SBP target group, and 20% lower in the lower vs higher LDL-C target group. Sample size has been calculated to provide a 80% power with a significance of 5% after corrections for repetitive measurements on the assumption that stroke incidence will be 4% per year in the highest SBP target group. Participants will be recruited at approximately 250 clinics in Europe (2500 patients) and China (5000 patients) over a 2-year period, and will be followed up for an average of 4 years or until 925 recurrent strokes occur. Arms and assigned intervention 1. Antihypertensive treatment design and assigned treatment Participants will be randomly allocated to one of three different sitting SBP targets: 1. < 145 to 135 mmHg 2. < 135 to 125 mmHg 3. < 125 mmHg to be possibly achieved within 3 months and subsequently maintained within the target window. Investigators are free to choose the drugs (among those approved in each country) to be administered to individual patients. It is expected that patients already on antihypertensive therapy and with SBP at randomization not too far from target will be maintained on current therapy with suitable adjustments. Other patients (untreated or with SBP far from target) may follow a suggested treatment algorithm of progressive increase in number of compounds or doses. During follow-up visits drugs and/or doses will be modified if necessary to maintain patients within randomized target window. 2. Lipid-lowering treatment design and assigned treatment Participants will be randomly allocated to one of two different LDL-C targets: A) 2.8 to 1.8 mmol/l (110 to 70 mg/dl) B) < 1.8 mmol/l (< 70 mg/dl) to be possibly achieved within 3 months and subsequently maintained within the target window. Investigators are free to choose the statin (among those approved in each country) to be administered to individual patients. The initial statin dose should be chosen by the investigator according to LDL-C at randomization and the LDL-C target. The initial dose can be increased (to the maximum dose allowed in each country) or decreased until the LDL-C target is achieved possibly within 3 months, and further adjusted up or down at 6-month intervals in order to maintain LDL-C within the randomized target window.


Recruitment information / eligibility

Status Completed
Enrollment 200
Est. completion date March 31, 2021
Est. primary completion date December 31, 2020
Accepts healthy volunteers No
Gender All
Age group 65 Years and older
Eligibility Inclusion Criteria: - Qualifying event: stroke or TIA 1 to 6 months previous to randomization. - All patients should have a CT scan or MRI (preferably MRI) at screening. The CT scan or MRI carried out at the time of the qualifying event, if available, is acceptable. Stroke will be defined as imaging evidence of a recent brain infarction (or haemorrhage) independently of duration of clinical symptoms, or as duration of clinical symptoms > 24 h even in absence of imaging evidence of lesion - TIA as clinical symptoms (involving limbs or speech) lasting < 24 h without imaging evidence of infarction. Enrolling units should avoid enrolling patients with TIA in a proportion greater than 25% of enrolled patients. The general coordinators in Milan and Beijing may decide stopping enrolment of TIA patients if their proportion is becoming greater than expected. - A haemorrhagic stroke (1 to 6 months previously) is also a qualifying event, but only for the BP-lowering component of the trial (see Exclusion criteria). - Age: 65 years and above. No fixed upper age limit is introduced, but frail patients aged above 80 years should not be enrolled. - Gender: either gender. - BP: Only hypertensive patients: untreated patients with SBP =140 mmHg; patients on antihypertensive treatment with any BP (but see exclusion criteria) - LDL-C: Patients without statin treatment with LDL-C > 2.8 mmol/l; patients on statin treatment with any LDL-C value (but see exclusion criteria) - Antiplatelet therapy: All patients should be under antiplatelet therapy (agents and doses chosen by the investigator according to accepted guidelines), unless contraindicated. Anticoagulant (instead of antiplatelet) therapy whenever indicated (e.g. atrial fibrillation). Exclusion Criteria: - Qualifying event: 1. Patients in unstable clinical conditions 2. Clinical disturbances caused by non-stroke pathology 3. patients with haemodynamically significant carotid stenosis or requiring carotid revascularization 4. haemorrhagic stroke is an exclusion criterion for the lipid lowering component of the trial; however, these patients should be randomized to the BP component, but considered in addition to the number of patients requested to each enrolling unit, in order not to decrease the power of the lipid-lowering component. - BP: - known secondary hypertension; - SBP >140 mmHg under three antihypertensive drugs at full doses (these patients are unlikely to achieve SBP < 125 mmHg, if so randomized); - orthostatic hypotension (SBP fall > 25 mmHg on standing); - LDL-C: - LDL-C >2.8 mmol/l under full dose of a statin (these patients are unlikely to achieve LDL-C targets). - LDL-C > 4.5 mmol/l under low dose of a statin or untreated (these patients are unlikely to achieve the lower LDL-C target). - Others: - Patients with a myocardial infarction (preceding or subsequent to the qualifying stroke or TIA) if their baseline LDL-C is < 1.8 mmol/l - Dementia - Severe disability (modified Rankin scale > 4) - Severe chronic renal failure defined as serum creatinine > 250 micromol/l - Hepatic disease as determined by either AST or ALT values > 2 times the upper limit of normal - History of hepatic encephalopathy, esophageal varices or portocaval shunt - History of gastrointestinal surgery or disorders which could interfere with drug absorption - Known allergy or contraindications to one of the drugs to be administered in the study - History of malignancy including leukaemia and lymphoma (but not basal cell skin cancer) within the last 5 years - History of clinically significant autoimmune disorders such as systemic lupus erythematosus - History of drug or alcohol abuse within the last 5 years - History of non-compliance to medical regimens and/or patients who are considered potentially unreliable - Inability or unwillingness to give free informed consent

Study Design


Intervention

Drug:
all approved antihypertensive drugs; all approved statins
All drugs to be used at doses capable of bringing SBP and LDL-C to targets; only doses approved in each country.

Locations

Country Name City State
Russian Federation Almazov Federal Heart, Blood and Endocrinology Centre Saint-Petersburg

Sponsors (3)

Lead Sponsor Collaborator
Istituto Auxologico Italiano Chinese Hypertension League, European Society of Hypertension

Country where clinical trial is conducted

Russian Federation, 

Outcome

Type Measure Description Time frame Safety issue
Primary Recurrent stroke Time to occurrence of (recurrent) stroke (fatal and non fatal) five years
Secondary Major cardiovascular (CV) events First major cardiovascular events, a composite of CV death, non fatal stroke, non fatal myocardial infarction, vascular intervention, hospitalized heart failure five years
Secondary Cognitive impairment and dementia Cognitive impairment (decline in Montreal Cognitive Assessment Test); Dementia (Disability Assessment for Dementia) five years
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