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Hypertension and stroke


Learning objectives

  • Learning
  • Understand
  • Integrate
  • Reflect

Introduction

Hypertension is a major risk factor for cardiovascular events, including ischaemic stroke and haemorrhagic stroke. Hypertension is the single most important modifiable risk factor for stroke. It is a contributing factor in over 70% of strokes. It promotes the formation of atheroma in large and medium sized vessels e.g. carotids and aortic arch. It also damages small end arteries. It may cause LV dysfunction and atrial fibrillation. The benefits of treatment are most significant in those younger than 60.

Blood pressure is measured as the level of pressure when the heart is contracting (Systolic blood pressure) and when the heart is relaxed and filling with blood (Diastolic blood pressure). These pressure levels change continually as part of everyday life. The British Hypertension Society Guidelines recommend that the diagnosis and treatment of hypertension should be based on an average of at least two readings after 5 minutes at rest in the seated position. There is no absolute level that defines BP. NICE recommends that lowering raised blood pressure decreases the risk of stroke, coronary events, heart failure, and renal impairment.

Risk factor

Hypertension is a significant and treatable risk factor for both Ischaemic and Haemorrhagic stroke. It is estimated that 25% or more of strokes may be due to hypertension and this increases to 60-70% when discussing haemorrhagic stroke. It is by far the main risk factor for most causes of Spontaneous Intracerebral Haemorrhage. Those at most risk are those who are non-compliant with therapy, those with hypertension at a young age < 55. Smoking also adds to risk. It is important to remember that hypertension is a chronic illness and prior to presentation has almost always been present for years, perhaps undiagnosed due to a lack of screening opportunities. In those in whom it has been diagnosed treatment may have been suboptimal and many patients, especially the young have difficulty taking antihypertensive therapies for a variety of reasons.

Chronic exposure of small arterioles to hypertension leads to lipohyalinolysis to the small penetrating arteries (i.e. Lenticulostriate from the middle cerebral artery, paramedian pontine perforators from the Basilar artery) in the brain predominantly supplying white matter. These vessels often come off abruptly from much larger vessels at right angles and it suggested that these vessels are exposed to higher than expected pressures than would be seen if there was a normal gradated step down in vessel calibre and so are more prone to ongoing damage. There is much overlap with the topic of Small vessel disease.

Vascular changes include obstruction to vessels which causes the typical lacunar stroke clinical syndrome with corresponding imaging or microaneurysms also called Charcot-Bouchard aneurysms may be apparent and they can rupture causing bleeding. The same areas of the brain affected by hypertensive lacunar strokes are also blighted by hypertensive bleeds. The typical areas are the basal ganglia, thalamus, cerebellum and the ventral pons. With time those with hypertensive changes have significant periventricular changes with hypodensity or bleeds.

Hypertension also plays a role in general atherosclerosis and is a cause of heart disease and left ventricular hypertrophy which can precipitate atrial fibrillation.

BP and Stroke
Imaging
Blood Pressure Variability

Blood pressure is a dynamic physiological measurement that can fluctuate by minute, hour and day and that this variability in itself is a risk factor for stroke distinct from the simple absolute measurement of DBP or SBP. Short and long term BP variability is associated with cardiac, vascular and renal disease. The suggestion is that treatment should focus on both lowering BP but also reducing its variability. Notably ß blockers have the poorest effect on blood-pressure variation.

Blood Pressure in the Acute Stroke

Cerebral autoregulation which closely controls cerebral blood flow across a wide variety of systemic blood pressure is altered in the acute stroke setting. Generally, despite there being a number of large clinical trials and systematic reviews, there is no clear guide for BP following acute ischaemic stroke. There is evidence that BP should be lowered rapidly in patients with ICH. THis is very much based on the Interact trial. This did not show a significant reduction in death or severe disability, but an ordinal analysis of modified Rankin scores showed improved functional outcomes with intensive lowering of blood pressure to a target of SBP < 140 mmHg.

Management

There is evidence that Lowering BP reduces the risk of stroke and the more the BP is lowered, the more effective it is. The PROGRESS trial showed that treatment to lower blood pressure in people who have had a stroke or TIA reduces the risk of further stroke.

Preventative Trials
HOPE study Effects of an ACEI, Ramipril on Cardiovascular Events in high risk patients. Ramipril significantly reduces the rates of death, myocardial infarction, and stroke in a broad range of high-risk patients who are not known to have a low ejection fraction or heart failure. (N Engl J Med 2000;342:145-53.)
PROGRESS study Randomised trial of a perindopril-based blood-pressure-lowering regimen among 6105 individuals with previous stroke or transient ischaemic attack This blood-pressure-lowering regimen reduced the risk of stroke among both hypertensive and non-hypertensive individuals with a history of stroke or transient ischaemic attack. Combination therapy with perindopril and indapamide produced larger blood pressure reductions and larger risk reductions than did single drug therapy with perindopril alone. Lancet. 2001 Sep 29;358(9287):1033-41.
PRoFESS Study: Yusuf S et al Telmisartan to Prevent Recurrent Stroke and Cardiovascular Events Therapy with telmisartan initiated soon after an ischemic stroke and continued for 2.5 years did not significantly lower the rate of recurrent stroke, major cardiovas- cular events, or diabetes. (N=20,332) N Engl J Med 2008;359:1225-37
ASCOT-BPLA: Blood Pressure-Lowering Arm of the Anglo-Scandinavian Cardiac Outcomes Trial The amlodipine-based regimen prevented more major cardiovascular events and induced less diabetes than the atenolol-based regimen On the basis of previous trial evidence, these effects might not be entirely explained by better control of blood pressure, and this issue is addressed in the accompanying article. Nevertheless, the results have implications with respect to optimum combinations of antihypertensive agents. Lancet September 2005, Vol. 366 Issue: Number 9489 p907-913
Guidelines

NICE have very straightforward guidance. Those with a blood pressure > 140/90 mmHg or higher with TIA or stroke should be treated.

Lifestyle changes
  • Sodium restriction
  • Exercise
  • Weight loss
  • Alcohol restriction
  • Stop smoking
Management acutely

There is no one size fits all acute regimens, so stroke physicians have some latitude for treatment in the acute scenario for ischaemic stroke. Outside the acute thrombolysis or hypertensive emergencies pathway I aim for a SBP of < 220mmg or ideally < 200 mmHg. Personally, if patient can take oral agents I start with those and may consider Amlodipine 5 mg PO or Ramipril 2.5 mg acutely. Note there is not always a need to give medication. The patient may be in pain, be in urinary retention (easy to miss) or distressed and calm reassurance may do wonders. Set some treatment goals such as to lower BP by 10-20% acutely over several hours. In extreme cases or when oral cannot be given or for thrombolysis patients IV Labetalol 10-20 mg bolus may be useful. For haemorrhage there is evidence to lower to SBP of 140 mmHg and again IV Labetalol may be useful. Several lw dose agents may be needed.

Cause of high BP acutely
  • pain e.g. a fractured hip in a dysphasic patient
  • Acute urinary retention
  • Acute alcohol withdrawal
  • Acute mental stress
  • White coat hypertension
  • Pheochromocytoma
Patients under 55 years:
  • Step 1: ACE inhibitor; if not tolerated, offer an angiotensin-II receptor antagonist. If both ACE inhibitors and angiotensin-II receptor antagonists are contra-indicated or not tolerated, consider a beta-blocker; beta-blockers, especially when combined with a thiazide diuretic, should be avoided for the routine treatment of uncomplicated hypertension in patients with diabetes or at high risk of developing diabetes
  • Step 2: ACE inhibitor or angiotensin-II receptor antagonist in combination with a calcium-channel blocker. If a calcium-channel blocker is not tolerated or if there is evidence of, or a high risk of, heart failure, give a thiazide-related diuretic (e.g. chlortalidone or indapamide). If a beta-blocker was given at Step 1, add a calcium channel blocker in preference to a thiazide-related diuretic (see Step 1)
  • Step 3: ACE inhibitor or angiotensin-II receptor antagonist in combination with a calcium-channel blocker and a thiazide-related diuretic
  • Step 4 (resistant hypertension): Consider seeking specialist advice
  • Add low-dose spironolactone [unlicensed indication], or use high-dose thiazide related diuretic if plasma-potassium concentration above 4.5 mmol/litre
  • Monitor renal function and electrolytes

    If additional diuretic therapy is contra-indicated, ineffective, or not tolerated, consider an alpha-blocker or a beta-blocker

Patients over 55 years, and patients of any age who are of African or Caribbean family origin:
  • Step 1: Calcium-channel blocker; if not tolerated or if there is evidence of, or a high risk of, heart failure, give a thiazide-related diuretic (e.g. chlortalidone or indapamide)
  • Step 2: Calcium-channel blocker or thiazide-related diuretic in combination with an ACE inhibitor or angiotensin-II receptor antagonist (an angiotensin-II receptor antagonist in combination with a calcium-channel blocker is preferred in patients of African or Caribbean family origin)
  • Steps 3 and 4: Treat as for patients under 55 years. Cardiovascular risk reduction.
Additional
  • Aspirin reduces the risk of cardiovascular events and myocardial infarction. Unduly high blood pressure must be controlled before aspirin is given. Unless contra-indicated, aspirin is recommended for all patients with established cardiovascular disease. Use of aspirin in primary prevention, in those with or without diabetes, is of unproven benefit. For the role of aspirin in the prevention of stroke in patients with atrial fibrillation, see Arrhythmias.
  • Statins are also of benefit in cardiovascular disease or in those who are at high risk of developing cardiovascular disease.
References

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