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Cellular Changes
Injury from ischemic stroke is the result of a complex series of cellular metabolic events that occur
rapidly after the interruption of nutrient blood flow to a region of the brain. The duration, severity, and
location of focal cerebral ischemia determine the extent of brain function and thus the severity of
stroke.
Shown is a summary of the cascade of cellular changes as ischemia progresses.
A neuron consists of a cell body, which contains a nucleus, and one or more extensions
protruding from the cell body. Dendrites receive nerve impulses from other neurons or from
sensory receptors. The axon carries the nerve impulses (action potential) away from the cell
body to another neuron or to an effector organ such as a muscle.
A stimulus affects the axon by changing the permeability of the axon to positive ions. The
influx of positive ions reduces the electrical potential across one segment of the membrane
(depolarization). The change in electrical potential in the first part of the axon triggers a
change in electrical potential in the adjacent segment of the axon such that the impulse
travels along the axon as a self-generating chain reaction.
At most synapses, arrival of the impulse at the presynaptic terminal leads to release of
neurotransmitter, which crosses the synapse to interact with receptors on the membrane of
the postsynaptic cell. This interaction opens ion-specific channels in the postsynaptic
membrane, changing the membranes permeability for positive ions.
The transient change in voltage induced by the action potential is determined by the
concentration of ions on either side of the cell membrane. Maintaining these ionic gradients
is an energy-consuming process that requires a constant supply of glucose and oxygen to
the neuron.
Glutamate further activates sodium and calcium ion channels in the neuron membrane.
As sodium and calcium ions rapidly accumulate within the cells, accompanied by an inflow of water,
cytotoxic edema causes rapid swelling of neurons and glia.
Activation of calcium channels results in further influx of calcium into the cell. One of the most
intensely studied calcium channels is the N-methyl-D aspartate (NMDA) channel.
Entry of calcium through the NMDA (and similar channels) can be devastating. First, attempts to get rid
of the excess calcium use up already scarce supplies of ATP. Second, excessive calcium influx causes
the disordered activation of a wide range of enzyme systems (proteases, lipases, and nucleases).
These enzymes and their metabolic products, such as oxygen free radicals, damage cell membranes,
genetic material, and structural proteins in the neurons, ultimately leading to cell death. This sequence
of events has been termed excitotoxicity because of the pivotal role of excitatory amino acids such as
glutamate.
Several agents are under investigation to block these steps.
tissue).
In the core zone, which is an area of severe ischemia (blood flow below 10% to 25%), the loss of
oxygen and glucose results in rapid depletion of energy stores. Severe ischemia can result in necrosis
of neurons and also of supporting cellular elements (glial cells) within the severely ischemic area.
Brain cells within the penumbra, a rim of mild to moderately ischemic tissue lying between tissue that
is normally perfused and the area in which infarction is evolving, may remain viable for several hours.
That is because the penumbral zone is supplied with blood by collateral arteries anastomosing with
branches of the occluded vascular tree (see inset). However, even cells in this region will die if
reperfusion is not established during the early hours since collateral circulation is inadequate to
maintain the neuronal demand for oxygen and glucose indefinitely.
In this example, the ischemic penumbra is shown as a rim of tissue surrounding the severely ischemic
core lying within the vascular territory of the pre-Rolandic branch of the left middle cerebral artery. The
Rolandic artery is occluded by a thromboembolus. The extent of the penumbra varies directly with the
number and patency of collateral arteries.
The penumbra is where pharmacologic interventions are most likely to be effective. However, it may
also be possible to salvage cells within the severely ischemic core zone. Although severe ischemia kills
selectively vulnerable neurons, glial cells may be spared if blood flow is restored early. Therefore,
timely recanalization of the occluded vessel should theoretically restore perfusion in both the
penumbra and in the severely ischemic core. Partial recanalization should markedly reduce the size of
the penumbra as well.
Edema Formation
Ischemic brain edema is a combination of two major types of edema: cytotoxic (cellular) and
vasogenic [Fishman RA. Cerebrospinal Fluid in Diseases in the Nervous System. 2nd Ed.
Philadelphia, PA: W.B. Saunders Co; 1992:103-155]. Cytotoxic edema evolves over minutes
to hours and may be reversible, while the vasogenic phase occurs over hours to days, and is
considered an irreversibly damaging process.
Cytotoxic edema is characterized by swelling of all the cellular elements of the brain
(shown). In the presence of acute cerebral ischemia, neurons, glia (indicated by astrocytes),
and endothelial cells swell within minutes of hypoxia due to failure of ATP-dependent ion
(sodium and calcium) transport. With the rapid accumulation of sodium within cells, water
follows to maintain osmotic equilibrium. Increased intracellular calcium activates
phospholipases and the release of arachidonic acid, leading to the release of oxygen-derived
free radicals and infarction.
Vasogenic edema (not shown) is characterized by an increase in extracellular fluid volume
due to increased permeability of brain capillary endothelial cells to macromolecular serum
proteins (e.g., albumin). Normally, the entry of plasma protein-containing fluid into the
extracellular space is limited by tight endothelial cell junctions, but in the presence of
massive injury, there is increased permeability of brain capillary endothelial cells to large
molecules. Vasogenic edema can displace the brain hemisphere and, when severe, lead to
cerebral herniation.
Acute hypoxia initially causes cytotoxic edema, followed within the next hours to days by the
development of vasogenic edema as infarction develops (Fishman, 1992). The delayed onset
of vasogenic edema suggests that time is needed for the defects in endothelial cell function
and permeability to develop.
http://www.strokecenter.org/professionals/brain-anatomy/cellular-injury-during-ischemia/edemaformation/
Brain ischemia
From Wikipedia, the free encyclopedia
Brain ischemia
CT scan slice of the brain showing a righthemispheric cerebral infarct (left side of image).
Specialty
neurology, cardiology
ICD-10
G45.9, I67.8
ICD-9-CM
435X,437X
MeSH
D002545
Brain ischemia (aka cerebral ischemia, cerebrovascular ischemia) is a condition in which there
is insufficient blood flow to the brain to meet metabolic demand.[1] This leads to poor oxygen supply
or cerebral hypoxia and thus to the death of brain tissue or cerebral infarction / ischemic stroke.[2] It is
a sub-type of stroke along with subarachnoid hemorrhage and intracerebral hemorrhage.[3]
Ischemia leads to alterations in brain metabolism, reduction in metabolic rates, and energy crisis. [4]
There are two types of ischemia: focal ischemia, which is confined to a specific region of the brain;
and global ischemia, which encompasses wide areas of brain tissue.
The main symptoms involve impairments in vision, body movement, andspeaking. The causes of
brain ischemia vary from sickle cell anemia tocongenital heart defects. Symptoms of brain ischemia
can include unconsciousness, blindness, problems with coordination, and weakness in the body.
Other effects that may result from brain ischemia are stroke,cardiorespiratory arrest, and irreversible
brain damage.
An interruption of blood flow to the brain for more than 10 seconds causes unconsciousness, and an
interruption in flow for more than a few minutes generally results in irreversible brain damage. [5] In
1974, Hossmann andZimmerman[disambiguation needed] demonstrated that ischemia induced inmammalian
brains for up to an hour can be at least partially recovered. Accordingly, this discovery raised the
possibility of intervening after brain ischemia before the damage becomes irreversible. [6]
Contents
[hide]
1 Classification
o
2 Symptoms
3 Causes
4 Pathophysiology
5 Treatment
6 Management
7 Research
8 References
9 Bibliography
10 Further reading
Classification[edit]
The broad term, "stroke" can be divided into three categories: brain ischemia, subarachnoid
hemorrhage and intracerebral hemorrhage. Brain ischemia can be further subdivided, by cause,
into thrombotic, embolic, and hypoperfusion.[3] Thrombotic and embolic are generally focal or
multifocal in nature while hypoperfusion affects the brain globally.
Symptoms[edit]
The symptoms of brain ischemia reflect the anatomical region undergoing blood and oxygen
deprivation. Ischemia within the arteries branching from the internal carotid artery may result in
symptoms such as blindness in one eye, weakness in one arm or leg, or weakness in one entire side
of the body. Ischemia within the arteries branching from the vertebral arteries in the back of the brain
may result in symptoms such as dizziness, vertigo, double vision, or weakness on both sides of the
body[citation needed]. Other symptoms include difficulty speaking, slurred speech, and the loss of
coordination.[9] The symptoms of brain ischemia range from mild to severe. Further, symptoms can
last from a few seconds to a few minutes or extended periods of time. If the brain becomes damaged
irreversibly and infarction occurs, the symptoms may be permanent.[10]
Similar to cerebral hypoxia, severe or prolonged brain ischemia will result in unconsciousness, brain
damage or death, mediated by the ischemic cascade.[11]
Multiple cerebral ischemic events may lead to subcortical ischemic depression, also known as
vascular depression. This condition is most commonly seen in elderly depressed patients. [citation
needed]
Late onset depression is increasingly seen as a distinct sub-type of depression, and can be
detected with an MRI.[12]
Causes[edit]
Brain ischemia has been linked to a variety of diseases or abnormalities. Individuals with sickle cell
anemia, compressed blood vessels, ventricular tachycardia, plaque buildup in the arteries, blood
clots, extremely low blood pressure as a result ofheart attack, and congenital heart defects have a
higher predisposition to brain ischemia in comparison their healthy counterparts.
Sickle cell anemia may cause brain ischemia associated with the irregularly shaped blood cells.
Sickle shaped blood cells clot more easily than normal blood cells, impeding blood flow to the brain.
Compression of blood vessels may also lead to brain ischemia, by blocking the arteries that carry
oxygen to the brain.Tumors are one cause of blood vessel compression.
Ventricular tachycardia represents a series of irregular heartbeats that may cause the heart to
completely shut down resulting in cessation of oxygen flow. Further, irregular heartbeats may result
in formation of blood clots, thus leading to oxygen deprivation to all organs.
Blockage of arteries due to plaque buildup may also result in ischemia. Even a small amount of
plaque build up can result in the narrowing of passageways, causing that area to become more
prone to blood clots.[citation needed] Large blood clots can also cause ischemia by blocking blood flow.
A heart attack can also cause brain ischemia due to the correlation that exists between heart attack
and low blood pressure. Extremely low blood pressure usually represents the inadequate
oxygenation of tissues. Untreated heart attacks may slow blood flow enough that blood may start to
clot and prevent the flow of blood to the brain or other major organs. Extremely low blood pressure
can also result from drug overdose and reactions to drugs. Therefore, brain ischemia can result from
events other than heart attacks.
Congenital heart defects may also cause brain ischemia due to the lack of appropriate artery
formation and connection. People with congenital heart defects may also be prone to blood clots.
Other pathological events that may result in brain ischemia include cardiorespiratory arrest, stroke,
and severe irreversible brain damage.
Recently, Moyamoya disease has also been identified as a potential cause for brain ischemia.
Moyamoya disease is an extremely rare cerebrovascular condition that limits blood circulation to the
brain, consequently leading to oxygen deprivation.[13]
Pathophysiology[edit]
During brain ischemia, the brain cannot perform aerobic metabolism due to the loss
of oxygen and substrate. The brain is not able to switch to anaerobic metabolism and because it
does not have any long term energy stored the levels ofadenosine triphosphate (ATP) drop rapidly
and approach zero within 4 minutes. In the absence of biochemical energy, cells begin to lose the
ability to maintain electrochemical gradients. Consequently, there is a massive influx of calcium into
thecytosol, a massive release of glutamate from synaptic vesicles, lipolysis, calpain activation, and
the arrest of protein synthesis.[14] Additionally, removal of metabolic wastes is slowed.[15] The
interruption of blood flow to the brain for ten seconds results in the immediate loss of consciousness.
The interruption of blood flow for twenty seconds results in the stopping of electrical activity.[5] An
area called a penumbra, may result, wherein neurons do not receive enough blood to communicate,
however do receive sufficient oxygenation to avoid cell death for a short period of time. [16]
Treatment[edit]
Alteplase (tpa) is an effective medication for acute ischemic stroke. When given within 3 hours,
treatment with tpa significantly improves the probability of a favourable outcome versus treatment
with placebo.
The outcome of brain ischemia is influenced by the quality of subsequent supportive care. Systemic
blood pressure (or slightly above) should be maintained so that cerebral blood flow is restored.
Also, hypoxaemia and hypercapnia should be avoided. Seizures can induce more damage;
accordingly, anticonvulsants should be prescribed and should a seizure occur, aggressive treatment
should be undertaken. Hyperglycaemia should also be avoided during brain ischemia.[17]
Management[edit]
When someone presents with an ischemic event, treatment of the underlying cause is critical for
prevention of further episodes.
Anticoagulation with warfarin or heparin may be used if the patient has atrial fibrillation.
Operative procedures such as carotid endarterectomy and carotid stenting may be performed if the
patient has a significant amount of plaque in the carotid arteries associated with the local ischemic
events.
Research[edit]
Therapeutic hypothermia has been attempted to improve results post brain ischemia[citation needed]. This
procedure was suggested to be beneficial based on its effects post cardiac arrest. Evidence
supporting the use of therapeutic hypothermia after brain ischemia, however, is limited.
A closely related disease to brain ischemia is brain hypoxia. Brain hypoxia is the condition in which
there is a decrease in the oxygen supply to the brain even in the presence of adequate blood flow. If
hypoxia lasts for long periods of time, coma,seizures, and even brain death may occur. Symptoms
of brain hypoxia are similar to ischemia and include inattentiveness, poor judgment, memory loss,
and a decrease in motor coordination.[18] Potential causes of brain hypoxia are suffocation,carbon
monoxide poisoning, severe anemia, and use of drugs such as cocaine and other amphetamines.
[9]
Other causes associated with brain hypoxia include drowning, strangling, choking, cardiac
arrest, head trauma, and complications during general anesthesia. Treatment strategies for brain
hypoxia vary depending on the original cause of injury.[18]
https://en.wikipedia.org/wiki/Brain_ischemia
What Is A Stroke?
Source: MedicineNet.com
Medical Author: Benjamin C. Wedro, MD, FAAEM
Medical Editor: William C. Shiel Jr., MD, FACP, FACR
Stroke: What is it?
A stroke, or cerebrovascular accident (CVA), occurs when blood supply to
part of the brain is disrupted, causing brain cells to die. When blood flow to
the brain is impaired, oxygen and glucose cannot be delivered to the brain.
Blood flow can be compromised by a variety of mechanisms.
Blockage of an artery
Narrowing of the small arteries within the brain can cause a so-called
lacunar stroke, (lacune=empty space). Blockage of a single arteriole can
affect a tiny area of brain causing that tissue to die (infarct).
Hardening of the arteries (atherosclerosis) leading to the brain. There are
four major blood vessels that supply the brain with blood. The anterior
circulation of the brain that controls most motor, activity, sensation, thought,
speech, and emotion is supplied by the carotid arteries. The posterior
circulation, which supplies the brainstem and the cerebellum, controlling the
automatic parts of brain function and coordination, is supplied by the
vertebrobasilar arteries.
If these arteries become narrow as a result of atherosclerosis, plaque or
cholesterol, debris can break off and float downstream, clogging the blood
supply to a part of the brain. As opposed to lacunar strokes, larger parts of
the brain can lose blood supply, and this may produce more symptoms than
a lacunar stroke.
Embolism to the brain from the heart. In situations in which blood clots form
within the heart, the potential exists for small clots to break off and travel
(embolize) to the arteries in the brain and cause a stroke.
Rupture of an artery (hemorrhage)
Cerebral hemorrhage (bleeding within the brain substance). The most
common reason to have bleeding within the brain is uncontrolled high blood
pressure. Other situations include aneurysms that leak or rupture or
arteriovenous malformations (AVM) in which there is an abnormal collection
of blood vessels that are fragile and can bleed.
What causes a stroke?
Blockage of an artery
The blockage of an artery in the brain by a clot (thrombosis) is the most
common cause of a stroke. The part of the brain that is supplied by the
clotted blood vessel is then deprived of blood and oxygen. As a result of the
deprived blood and oxygen, the cells of that part of the brain die. Typically, a
clot forms in a small blood vessel within the brain that has been previously
narrowed due to a variety of risk factors including:
high blood pressure (hypertension),
high cholesterol,
diabetes, and
smoking.
Embolic stroke
Another type of stroke may occur when a blood clot or a piece of
atherosclerotic plaque (cholesterol and calcium deposits on the wall of the
inside of the heart or artery) breaks loose, travels through open arteries, and
lodges in an artery of the brain. When this happens, the flow of oxygen-rich
blood to the brain is blocked and a stroke occurs. This type of stroke is
referred to as an embolic stroke. For example, a blood clot might originally
form in the heart chamber as a result of an irregular heart rhythm, such as
occurs in atrial fibrillation. Usually, these clots remain attached to the inner
lining of the heart, but occasionally they can break off, travel through the
blood stream, form a plug (embolism) in a brain artery, and cause a stroke.
An embolism can also originate in a large artery (for example, the carotid
artery, a major artery in the neck that supplies blood to the brain) and then
travel downstream to clog a small artery within the brain.
Cerebral hemorrhage
A cerebral hemorrhage occurs when a blood vessel in the brain ruptures and
bleeds into the surrounding brain tissue. A cerebral hemorrhage (bleeding in
the brain) can cause a stroke by depriving blood and oxygen to parts of the
brain. Blood is also very irritating to the brain and can cause swelling of brain
tissue (cerebral edema). Edema and the accumulation of blood from a
cerebral hemorrhage increases pressure within the skull and causes further
damage by squeezing the brain against the bony skull.
Subarachnoid hemorrhage
In a subarachnoid hemorrhage, blood accumulates in the space beneath the
arachnoid membrane that lines the brain. The blood originates from an
abnormal blood vessel that leaks or ruptures. Often this is from an aneurysm
(an abnormal ballooning out of the wall of the vessel). Subarachnoid
hemorrhages usually cause a sudden, severe headache and stiff neck. If not
recognized and treated, major neurological consequences, such as coma,
and brain death will occur.
Vasculitis
Another rare cause of stroke is vasculitis, a condition in which the blood
vessels become inflamed.
Migraine headache
There appears to be a very slight increased occurrence of stroke in people
with migraine headache. The mechanism for migraine or vascular headaches
includes narrowing of the brain blood vessels. Some migraine headache
episodes can even mimic stroke with loss of function of one side of the body
or vision or speech problems. Usually, the symptoms resolve as the
headache resolves. What are the risk factors for stroke?
Overall, the most common risk factors for stroke are:
high blood pressure,
high cholesterol,
smoking,
diabetes and
increasing age.
Heart rhythm disturbances like atrial fibrillation, patent foramen ovale, and
heart valve disease can also be the cause.When strokes occur in younger
individuals (less than 50 years old), less common risk factors are considered
including illicit drugs, such as cocaine or amphetamines, ruptured
aneurysms, and inherited (genetic) predispositions to blood clotting. An
example of a genetic predisposition to stroke occurs in a rare condition called
homocystinuria, in which there are excessive levels of the chemical
homocystine in the body. Scientists are trying to determine whether the nonhereditary occurrence of high levels of homocystine at any age can
predispose to stroke. What is a transient ischemic attack (TIA)?
A transient ischemic attack (TIA) is a short-lived episode (less than 24 hours)
of temporary impairment to the brain that is caused by a loss of blood
supply. A TIA causes a loss of function in the area of the body that is
controlled by the portion of the brain affected. The loss of blood supply to the
brain is most often caused by a clot that spontaneously forms in a blood
vessel within the brain (thrombosis). However, it can also result from a clot
that forms elsewhere in the body, dislodges from that location, and travels to
lodge in an artery of the brain (emboli). A spasm and, rarely, a bleed are
other causes of a TIA. Many people refer to a TIA as a "mini-stroke."Some
TIAs develop slowly, while others develop rapidly. By definition, all TIAs
resolve within 24 hours. Strokes take longer to resolve than TIAs, and with
strokes, complete function may never return and reflect a more permanent
and serious problem. Although most TIAs often last only a few minutes, all
TIAs should be evaluated with the same urgency as a stroke in an effort to
prevent recurrences and/or strokes. TIAs can occur once, multiple times, or
precede a permanent stroke.
A transient ischemic attack should be considered an emergency because
there is no guarantee that the situation will resolve and function will return.
A TIA from a clot to the eye can cause temporary visual loss (amaurosis
fugax), which is often described as the sensation of a curtain coming down. A
TIA that involves the carotid artery (the largest blood vessel supplying the
brain) can produce problems with movement or sensation on one side of the
body, which is the side opposite to the actual blockage. An affected patient
may experience paralysis of the arm, leg, and face, all on one side. Double
vision, dizziness (vertigo), and loss of speech, understanding, and balance
can also be symptoms depending on what part of the brain is lacking blood
supply.
What is the impact of strokes?
In the United States, stroke is the third largest cause of death (behind heart
disease and all forms of cancer). The cost of strokes is not just measured in
the billions of dollars lost in work, hospitalization, and the care of survivors in
nursing homes. The major cost or impact of a stroke is the loss of
independence that occurs in 30% of the survivors. What was a self-sustaining
and enjoyable lifestyle may lose most of its quality after a stroke and other
family members can find themselves in a new role as caregivers.
What are stroke symptoms?
When brain cells are deprived of oxygen, they cease to perform their usual
tasks. The symptoms that follow a stroke depend on the area of the brain
that has been affected and the amount of brain tissue damage.Small strokes
may not cause any symptoms, but can still damage brain tissue. These
strokes that do not cause symptoms are referred to as silent strokes.
According to The U.S. National Institute of Neurological Disorders and Stroke
(NINDS), these are the five major signs of stroke:
1.Sudden numbness or weakness of the face, arm or leg, especially on one
side of the body. The loss of voluntary movement and/or sensation may be
complete or partial. There may also be an associated tingling sensation in
the affected area.
Although aspirin plays a major role in stroke prevention (see below), once
the symptoms of a stroke begin, it is generally recommended that additional
aspirin not be taken until the patient receives medical attention. If stroke is
of the bleeding type, aspirin could theoretically make matters worse.
Cincinnati Prehospital Stroke Scale (CPSS)
According to a study by the University of North Carolina, three commands
may be used to assess whether a person may be experiencing a stroke. Lay
In the acute stroke evaluation, many things will occur at the same time. As
the physician is taking the history and performing the physical examination,
nursing staff will begin monitoring the patient's vital signs, getting blood
tests, and performing an electrocardiogram (EKG or ECG). Part of the
physical examination that is becoming standardized is the use of a stroke
scale. There is a narrow time frame to intervene in an acute stroke with
medications to reverse the loss of blood supply to part of the brain. The
patient needs to be appropriately evaluated and stabilized before any clotbusting drugs can be potentially utilized.
Computerized tomography:
In order to help determine the cause of a suspected stroke, a special x-ray
test called a CT scan of the brain is often performed. A CT scan is used to
look for bleeding or masses within the brain, a much different situation than
stroke that is also treated differently.
MRI scan:
Magnetic resonance imaging (MRI) uses magnetic waves rather than x-rays
to image the brain. The MRI images are much more detailed than those from
CT, but this is not a first line test in stroke. While a CT scan may be
completed within a few minutes, an MRI may take more than an hour to
complete. An MRI may be performed later in the course of patient care if
finer details are required for further medical decision making. People with
certain medical devices (for example, pacemakers) or other metals within
their body, cannot be subjected to the powerful magnetic field of an MRI.
Other methods of MRI technology:
An MRI scan can also be used to specifically view the blood vessels noninvasively (without using tubes or injections), a procedure called an MRA
(magnetic resonance angiogram). Another MRI method called diffusion
weighted imaging (DWI) is being offered in some medical centers. This
technique can detect the area of abnormality minutes after the blood flow to
a part of the brain has ceased, whereas a conventional MRI may not detect a
stroke until up to six hours after it has started, and a CT scan sometimes
cannot detect it until it is 12 to 24 hours old. Again, this is not a first line test
in the evaluation of a stroke patient, when time is of the essence.
blood proteins that can increase the chance of stroke by thickening the blood
are measured. These tests are performed to identify treatable causes of a
stroke or to help prevent further injury. Screening blood tests looking for
potential infection, anemia, kidney function, and electrolyte abnormalities
may also be considered. What is the treatment of a stroke?
Tissue plasminogen activator (TPA)
There is opportunity to use alteplase (TPA) as a clot-buster drug to dissolve
the blood clot that is causing the stroke. There is a narrow window of
opportunity to use this drug. The earlier that it is given, the better the result
and the less potential for the complication of bleeding into the brain.Present
American Heart Association guidelines recommend that if used, TPA must be
given within three hours after the onset of symptoms. Normally, TPA is
injected into a vein in he arm. The time frame for use can be extended to six
hours if it is dripped directly into the blood vessel that is blocked. This is
usually performed by an interventional radiologist, and not all hospitals have
access to this technology.For posterior circulation strokes that involve the
vertebrobasilar system, the time frame for treatment with TPA may be
extended even further to 18 hours.
Heparin and aspirin
Drugs to thin the blood (anticoagulation; for example, heparin) are also
sometimes used in treating stroke patients in the hopes of improving the
patient's recovery. It is unclear, however, whether the use of anticoagulation
improves the outcome from the current stroke or simply helps to prevent
subsequent strokes (see below). In certain patients, aspirin given after the
onset of a stroke does have a small, but measurable effect on recovery. The
treating doctor will determine the medications to be used based upon a
patient's specific needs.
Managing other Medical Problems
Blood pressure and cholesterol control are key to prevention of future stroke
events. In transient ischemic attacks, the patient may be discharged with
medications even if the blood pressure and cholesterol levels are acceptable.
In an acute stroke, blood pressure will be tightly controlled to prevent further
damage.In patients with diabetes, the blood sugar (glucose) level is often
elevated after a stroke. Controlling the glucose level in these patients may
minimize the size of a stroke. Finally, oxygen may administered to stroke
patients when necessary.
Rehabilitation
When a patient is no longer acutely ill after a stroke, the healthcare staff
focuses on maximizing the patient's functional abilities. This is most often
done in an inpatient rehabilitation hospital or in a special area of a general
hospital. Rehabilitation can also take place at a nursing facility. The
rehabilitation process can include some or all of the following:
1.speech therapy to relearn talking and swallowing;
4.family education to orient them in caring for their loved one at home and
the challenges they will face.
The goal is for the patient to resume as many, if not all, of their pre-stroke
activities and functions. Since a stroke involves the permanent loss of brain
cells, a total return to the patient's pre-stroke status is unfortunately, not a
realistic goal in many cases. When a stroke patient is ready to go home, a
nurse may come to the home for a period of time until the family is familiar
with caring for the patient and the procedures for giving various medications.
Physical therapy may continue at home. Eventually, the patient is usually left
at home with one or more caregivers, who now find their lives have changed
in major ways. Caring for the stroke patient at home may be easy or very
nearly impossible. At times, it becomes apparent that the patient must be
placed in a board and care home or a skilled nursing facility because
adequate care cannot be given at home despite the good intentions of the
family. What complications can occur after a stroke?
A stroke can become worse despite an early arrival at the hospital and
appropriate medical treatment. It is not unusual for a stroke and a heart
attack to occur at the same time or in very close proximity to each other.
During the acute illness, swallowing may be affected. The weakness that
affects the arm, leg, and side of the face can also impact the muscles of
swallowing. A stroke that causes slurred speech seems to predispose the
patient to abnormal swallowing mechanics. Should food and saliva enter the
trachea instead of the esophagus when eating or swallowing, pneumonia or a
lung infection can occur. Abnormal swallowing can also occur independently
of slurred speech.
Because a stroke often results in immobility, blood clots can develop in a leg
vein (deep vein thrombosis). This poses a risk for a clot to travel upwards to
and lodge in the lungs - a potentially life-threatening situation (pulmonary
embolism). There are a number of ways in which the treating physician can
help prevent these leg vein clots. Prolonged immobility can also lead to
pressure sores (a breakdown of the skin, called decubitus ulcers), which can
be prevented by frequent repositioning of the patient by the nurse or other
caretakers.
Stroke patients often have some problem with depression as part of the
recovery process, which needs to be recognized and treated.
The prognosis following a stroke is related to the severity of the stroke and
how much of the brain has been damaged. Some patients return to a nearnormal condition with minimal awkwardness or speech defects. Many stroke
patients are left with permanent problems such as hemiplegia (weakness on
one side of the body), aphasia (difficulty or the inability to speak), or
incontinence of the bowel and/or bladder.
A significant number of persons become unconscious and die following a
major stroke. If a stroke has been massive or devastating to a person's ability
to think or function, the family is left with some very difficult decisions. In
these cases, it is sometimes advisable to limit further medical intervention. It
is often appropriate for the doctor and the patient's family to discuss and
implement orders to not resuscitate the patient in the case of a cardiac
arrest, since the quality of life for the patient would be so poor. In many
cases, this decision is made somewhat easier if the patient has made such a
request when well. What can be done to prevent a stroke?
Risk factor reduction High blood pressure:
The possibility of suffering a stroke can be markedly decreased by controlling
the risk factors. The most important risk factor for stroke is high blood
pressure. When a person's blood pressure is persistently too high, roughly
greater than 130/85, the risk of a stroke increases in proportion to the degree
by which the blood pressure is elevated. Controlling blood pressure in the
normal range decreases the chances of a stroke.
Smoking:
Another important risk factor is cigarette or other tobacco use. Cigarettes
cause the carotid arteries to develop severe atherosclerosis, which can lead
to their closure and block the blood flow to the brain. Atherosclerosis in
general, including involvement of the arteries that supply blood to the heart,
is accelerated by smoking. So, when an individual smokes, the main question
becomes - which will occur first; a stroke, heart attack, or lung cancer?
Diabetes:
Another risk factor for developing a stroke is diabetes mellitus. Diabetes
causes the small vessels to close prematurely. When these blood vessels
close in the brain, small (lacunar) strokes may occur. Good control of blood
sugar is important in decreasing the risk of stroke in diabetic patients. An
elevated level of blood cholesterol is also a risk factor for a stroke due to the
eventual blockage of blood vessels (atherosclerosis). A healthy diet and
medications can help normalize an elevated blood cholesterol level.
Blood thinner/warfarin:
An irregular heart beat (atrial fibrillation in particular) is associated with an
increased risk of an embolic stroke, in which the blood clot travels from the
heart, through the bloodstream, and into the brain. Warfarin (Coumadin) is a
blood "thinner" that prevents the blood from clotting. This medication is
often used in patients with atrial fibrillation to decrease this risk. Warfarin is
also sometimes used to prevent the recurrence of a stroke in other
situations, such as with certain other heart conditions and conditions in
which the blood has a tendency to clot on its own (hypercoagulable states).
Patients taking warfarin need to have periodic blood checks to make sure
that their current dose is producing the desired effect. Patients on warfarin
also need to know that they are at increased risk for bleeding, either
externally or internally.
Aspirin and other antiplatelet therapy:
Many stroke patients who do not require warfarin can use another class of
medicines called "antiplatelet" drugs to reduce their risk of suffering another
stroke. These medicines reduce the tendency of the blood to clot (clog) in the
arteries. As a side effect, patients on these medicines usually have a higher
likelihood of bleeding, but this risk is less than when taking an anticoagulant
like warfarin. The most commonly prescribed first-choice antiplatelet agent
for preventing a stroke recurrence is aspirin. If the patient has an adverse
reaction to aspirin or has a stroke despite being on aspirin, newer antiplatelet
preparations can be used [clopidogrel (Plavix), dipyridamole (Persantine).
Carotid endarterectomy:
In many cases, a person may suffer a TIA or a stroke that is caused by the
narrowing or ulceration (sores) of the carotid arteries (the major arteries in
the neck that supply blood to the brain). If left untreated, patients with these
conditions have a high risk of experiencing a major stroke in the future. An
operation that cleans out the carotid artery and restores normal blood flow is
known as a carotid endarterectomy. This procedure has been shown to
markedly reduce the incidence of a subsequent stroke. In patients who have
a narrowed carotid artery, but no symptoms, this operation may be indicated
in order to prevent the occurrence of a first stroke. What is in the future for
stroke treatment?
Currently, studies are being done on additional drugs that dissolve clots.
These drugs are administered either in the veins (like TPA) or directly into the
clogged artery. The goal of these studies is to determine which stroke
patients might benefit from this new and aggressive form of treatment.
New medications are also being tested that help slow the degeneration of
the nerve cells that are deprived of oxygen during a stroke. These drugs are
referred to as "neuroprotective" agents, an example of which is sipatrigine.
Another example is chlormethiazole, which works by modifying the
expression of genes within the brain. (Genes produce proteins that
determine an individual's makeup.)
Finally, stem cells, which have the potential to develop into a variety of
different organs, are being used to try to replace brain cells damaged by a
previous stroke. In many academic medical centers, some of these
experimental agents may be offered in the setting of a clinical trial. While
new therapies for the treatment of patients after a stroke are on the horizon,
they are not yet perfect and may not restore complete function to a stroke
victim. Stroke At A Glance
Stroke is the sudden death of brain cells due to lack of oxygen.
Clot-busting drugs like TPA can be used to reverse a stroke, but the time
frame for their use is very narrow. Patients need to present for care as soon
as possible so that TPA therapy can be considered.
Stroke facts
Although stroke is the fifth leading cause of death in America and a leading
cause of adult disability, many myths surround this disease. Test how much
you know about stroke today
MYTH
FACT
MYTH: Stroke recovery only happens for the first few months after a
stroke.
http://www.stroke.org/understand-stroke/what-stroke/stroke-facts
Right Brain
The effects of a stroke depend on several factors, including the location of the obstruction and how much brain tissue is affected.
However, because one side of the brain controls the opposite side of the body, a stroke affecting one side will result in neurological
complications on the side of the body it affects. For example, if the stroke occurs in the brain's right side, the left side of the body
(and the left side of the face) will be affected, which could produce any or all of the following:
Vision problems
Memory loss
Left Brain
If the stroke occurs in the left side of the brain, the right side of the body will be affected, producing some or all of the following:
Speech/language problems
Memory loss
Brain Stem
When stroke occurs in the brain stem, depending on the severity of the injury, it can affect both sides of the body and may leave
someone in a locked-in state. When a locked-in state occurs, the patient is generally unable to speak or achieve any movement
below the neck.
http://www.strokeassociation.org/STROKEORG/AboutStroke/EffectsofStrok
e/Effects-of-Stroke_UCM_308534_SubHomePage.jsp
How will the lost of blood supply be clinically manifested? (Clinical history
and physical examination, neurologic examination findings)
A P P R O X I M AT
E TIME TO
TYPE
Level-ofconsciousness
scale
Glasgow Coma Scale [a]
Stroke deficit
scales
Global
disability
scale
W E A K N E SS E
ADMINISTER
STREN GTH S
2 minutes
Simple,
valid,
reliable.
None
observed.
2 minutes
Brief,
reliable, can
be
administered
by nonLow
neurologists. sensitivity.
5 minutes
Brief, valid,
reliable.
Some useful
measures
omitted.
Good for
overall
assessment
of disability.
Walking is
the only
explicit
assessment
criterion.
Low
sensitivity.
5 minutes
Measures of
disability/acti
vities of daily
living (ADL)
Functional Independence
Measure
(FIM) [g]
Mental status
screening
Neurobehavioral
Cognition Status Exam (NCSE)
[i]
Widely used
for stroke.
Excellent
validity and
5-10 minutes reliability.
Low
sensitivity
for highlevel
functioning.
40 minutes
Widely used
for stroke.
Measures
mobility,
ADL,
cognition,
functional
Ceiling
communicati and floor
on.
effects.
10 minutes
Widely used
for
screening.
Several
functions
with
summed
score. May
misclassify
patients
with
aphasia.
10 minutes
Does not
distinguish
right from
left
hemisphere
. No
reliability
studies in
stroke.
Predicts gain No studies
in Barthel
of factorial
Index
structure.
scores.
Correlates
Unrelated to with
age.
education.
30-40
minutes
Extensively
evaluated
measure.
Good validity
and
reliability
for assessing
sensorimotor
function and
Considered
too complex
and timeconsuming
by many.
balance.
Balance
assessment
Mobility
assessment
Boston Diagnostic
Aphasia Examination [o]
Assessment of
speech and
Porch Index of
language
Communicative Ability (PICA)
functions
[p]
15 minutes
Good, brief
assessment
of
movement
and physical
mobility.
Reliability
assessed
only in
stable
patients.
Sensitivity
not tested.
5 minutes
Brief
assessment
of motor
function
of arm, leg,
and trunk.
Sensitivity
not tested.
10 minutes
Simple, well
established
with stroke
patients,
sensitive to
change.
None
observed.
5 minutes
Valid, brief,
reliable test
of physical
mobility.
Sensitivity
not tested.
1-4 hours
Widely used,
comprehensi
ve,
good
standardizati
on data,
sound
theoretical
rationale.
Time to
administer
long; half of
patients
cannot be
classified.
1/2-2 hours
Widely used,
comprehensi
ve,
careful test
development
and
standardizati
on.
Time to
administer
long.
Special
training
required to
administer.
Inadequate
sampling
of language
other than
one word
and single
sentences.
Western aphasia
Battery [q]
1-4 hours
Depression
scales
Time to
administer
long.
Aphasia
quotients
and
taxonomy
Widely used, of aphasia
comprehensi not well
ve.
validated.
Less useful
in elderly
and in
patients
with
aphasia or
neglect.Hig
Widely used, h
easily
rate of false
administered positives.
. Norms
Somatic
available.
items may
Good
not be due
with somatic to
symptoms.
depression.
Brief, easily
administered
, useful
in elderly,
effective for
screening in
stroke
population.
< 15
minutes
10 minutes
Brief, easy to
use with
elderly,
cognitively
impaired,
and those
with visual
or physical
problems
or low
Not
appropriate
for aphasic
patients.
High false
negative
rates in
minor
depression.
motivation.
Measures of
instrumental
ADL
Observer
rated;
frequently
used
in stroke
patients.
Multiple
differing
versions
compromise
interobserv
er reliability.
< 30
minutes
Measures
broad base
of
information
necessary
for
independent
5-10 minutes living.
Has not
been tested
in stroke
patients.
Developed
specifically
for stroke
patients;
assesses
broad array
of activities.
Sensitivity
and
interobserv
er reliability
not tested;
sensitivity
probably
limited.
Widely used
in stroke.
Computer
scoring
available.
Excellent
validity and
reliability.
Available in
multiple
languages.
Assessment
subjective;
sensitivity
not tested;
ceiling
and floor
effects.
Generic
health status
scale SF36 is
improved
version of
SF20. Brief,
can be self
administered
or
administered
by phone or
Possible
floor
effect in
seriously
ill patients
(especially
for physical
functioning)
, suggests
it should be
supplement
Frenchay Activities
Index [w]
10-15
minutes
Family
assessment
Health status/
quality of
life measures
10-15
minutes
interview.
Widely used
in the United
States.
Sickness Impact
Profile (SIP) [z]
20-30
minutes
ed by an
ADL scale
in stroke
patients.
Time to
administer
somewhat
long.
Evaluates
behavior
Comprehensi rather than
ve
subjective
and wellhealth;
evaluated.
needs
Broad range questions
of items
on wellreduces
being,
floor
happiness,
or ceiling
and
effects.
satisfaction.
http://www.strokecenter.org/professionals/strokediagnosis/stroke-assessment-scales-overview/
Stroke Syndromes
Ataxic Hemiparesis
Gerstmann Syndrome (Gerstmann Syndrome)
Middle Cerebral Artery - Inferior Division
Middle Aerebral Artery - Superior Division
Basilar Artery
Ataxic Hemiparesis
A N AT O M Y
VA S C U L A R
M A N I F E S T AT I O N
Contralateral
Contralateral
COMMENTS
Notes
Weakness usually more prominent in leg than arm; extensor plantar response; no facial involvement or
dysarthria. Other locations include thalamocapsular lesions, red nucleus, anterior cerebral artery
distribution. Also called homolateral ataxia and crural paresis.
EPONYM
Anton Syndome
A N AT O M Y
VA S C U L A R
M A N I F E S TAT I O N
Both
Both
Vertebral Artery
COMMENTS
MRI Compared to CT
This patients imaging studies show evolution of a left cerebral artery infarct on CT scan and
MRI.
Computed tomography of the head done 1/7/97 shows a hyperacute infarct, which is seen
only by the effacement of the cerebral sulci in the left parietal region and suggestion of loss
of grey/white distinction.
T2- weighted MRI scan shows no obvious signal abnormality.
Contrast-enhanced T1-weighted image shows slightly prominent intravascular contrast
enhancement within the branches of the left middle cerebral artery. Otherwise, the T1weighted images show no obvious abnormality.
One month later, on 2/7/97, the T2-weighted images show a typical wedge-shaped infarct in
the distribution of the left middle cerebral artery.
A contrast-enhanced T1-weighted image shows asymmetric intravascular contrast
enhancement. However, there is minimal parenchymal contrast enhancement of the wedgeshaped left middle cerebral artery infarct in the left parietal lobe.
Non-contrast computed tomography of the head shows a hypodense left middle cerebral
artery distribution infarct involving the left parietal lobe. Minimal contrast enhancement is
seen.
Lateral radiograph of the left carotid angiogram shows complete occlusion of the left internal
carotid artery with minimal collateral flow via external carotid branches.
Frontal radiograph of the left carotid angiogram shows complete occlusion of the left internal
carotid artery with minimal collateral flow via external carotid branches.
On 2/20/97, sagittal T1-weighted images show marked contrast enhancement of the left
parietal infarct following contrast administration. The images also show enhancement in the
occipital and temporal lobes.
Axial T2-weighted images now show minimal signal changes with linear T2-hypointensity in
the gyri in the left parietal lobe, indicating minimal hemorrhagic component, but most of the
signal changes of T2-weighted images have resolved. Note high signal in the cavernous
carotid artery on the lowest slice, indicative of carotid occlusion.
Cerebral Angiography
Cerebral angiography is an invasive test that involves the injection of contrast media into the carotid
artery by means of a catheter. Radiographs are taken as the dye works its way through the cerebral
circulation. Angiography may be utilized to identify bleeding aneurysms, vasospasm, and
arteriovenous malformations, and to differentiate embolism from large artery thrombosis [Adams HP,
et al, 1994. Mohr JP, 1992]. Cerebral angiography provides information on both arteries and veins, with
sequential images showing arterial, capillary, and venous phases.
The role of conventional angiography in the management of acute stroke is controversial. The test
itself is associated with a risk of stroke, since the catheter carrying the dye might dislodge plaque from
the carotid wall. In addition, patients may be allergic to the contrast dye, and the dye has been
associated with the development of renal failure, particularly when pre-existing kidney disease is
present. Presently, angiography is performed mainly in selected patients, especially those in whom
surgery (such as carotid endarterectomy or craniotomy for ruptured aneurysms or arteriovenous
malformations) is considered.
Conventional angiography has been replaced by magnetic resonance angiography (MRA) in some
patients with cerebrovascular disease [Bruno A, 1993]. A noninvasive test, MRA permits the
visualization of blood flow in vessels without the need for catheters or contrast agents. The technology
can yield information regarding collateral blood flow and is nearly as effective as conventional
angiography in estimating disease at the carotid bifurcation.
This left common carotid angiogram shows complete occlusion of the left middle cerebral artery distal
to the origin of the anterior temporal branch.
These are PET glucose metabolic images (shown on the right) compared with X-ray computed
tomography (shown on the left) of a patient with aphasia. The studies were performed at two months
and four years following left hemisphere cerebral hemorrhage. Note that for both time frames, the
extent of cerebral hypometabolism (less black) is much greater than the actual lesion or residual cavity
(at late time). These studies demonstrate that the functional abnormality demonstrated with PET
typically exceeds that seen with structural imaging techniques such as X-ray, CT, or MRI and is a more
representative depiction of the underlying functional state of the brain and the resultant abnormal
behaviors it produces. [Metter EJ, et al. Arch Neurol. 1980;47:1235-38.]
Brain Plasticity
Brain plasticity, also known as neuroplasticity, suggests that the location of a given function
in the brain (for example, speech) can move to another area of the brain. This transfer can
be activated by repetitive learning.
In the case of stroke, brain plasticity refers to healthy brain cells taking over the
functions of damaged brain cells.
This means that certain lost functions, such as speech and language, may
reemerge as the result of intensive rehabilitation.
http://www.speech-therapy-onvideo.com/brainplasticity.html
Figure 1. Blood supply of the brain. Each artery supplies a specific area of the brain. Some areas
are supplied by more than one artery.
What is a stroke?
Stroke is a sudden interruption of the blood supply to the brain. Most strokes are caused by an abrupt
blockage of an artery (ischemic stroke). Other strokes are caused by bleeding into brain tissue when a
blood vessel bursts (hemorrhagic stroke). The effects of a stroke depend on the severity and which area
of the brain is injured. Strokes may cause sudden weakness, loss of sensation, or difficulty with speaking,
seeing, or walking. Since different parts of the brain control different areas and functions, it is usually the
area immediately surrounding the stroke that is affected. Hemorrhagic strokes have a much higher death
rate than ischemic strokes.
Ischemic stroke - (most common - 83% of cases) is caused by a blockage of an artery from a blood clot
(thrombus) or from clogged blood vessels due to atherosclerosis (hardening of the arteries). In
atherosclerosis, cholesterol plaques are deposited within the walls of the arteries, narrowing the inside
diameter of the artery. As the artery narrows, less blood is able to pass to the brain and blood pressure
increases to meet the demands of the body. The normally smooth inner wall of the artery is now roughed
with plaque deposits causing blood cells to build up and form clots - called a thrombus (Fig. 2). Thrombus
build up usually occurs on large blood vessels of the neck and base of the brain.
Figure 2. An ischemic stroke is caused by a blocked artery to the brain either from the build-up of
plaques within the artery wall or from a clot.
Embolic stroke - is caused when a clot breaks off from the artery wall it becomes an embolus, which can
travel farther down the bloodstream to block a smaller artery. Emboli usually come from the heart, where
different diseases cause clot formation.
Hemorrhagic stroke - (less common - 17% of cases) is caused by rupture or leaking of an artery either
within or around the brain. It can occur when a weakened blood vessel ruptures releasing blood into the
space surrounding the brain - this is called a subarachnoid hemorrhage (SAH). It can be caused by a
ruptured aneurysm (Fig. 3), arteriovenous malformation (AVM), or head trauma.
Bleeding within the brain tissue itself is known as an intracerebral hemorrhage (ICH) and is primarily
caused by hypertension (Fig. 4). Hypertension is an elevation of blood pressure which may cause tiny
arteries to burst inside the brain.
Figure 4. A hemorrhagic stroke can be caused by rupture of tiny arteries within the brain tissue
(intracerebral hemorrhage). As blood collects, a hematoma or blood clot forms causing increased
pressure on the brain. Hypertension is the leading cause of ICH.
Sudden weakness or numbness of the face, arm or leg, usually on one side of the body
Who is affected?
Stroke is the third leading cause of death in the United States after diseases of the heart and all forms of
cancer. About 600,000 Americans have strokes each year. Someone has a stroke every 53 seconds.
Someone dies of a stroke every 3.3 minutes.
Risk factors you can't modify
Race - African Americans face twice the risk of stroke as the Caucasian population.
High blood pressure - the most dominant stroke risk factor and the easiest to modify is high
blood pressure, or hypertension. Have your blood pressure checked regularly and keep it
under control.
Weight - Being over-weight predisposes you to high cholesterol, high blood pressure and
diabetes, all of which increase stroke risk. If you are over weight, modify your diet and limit
your intake of fatty foods.
Diabetes - makes people susceptible to cardiovascular diseases, which can result in stroke. If
you have diabetes, keep it well controlled.
Prior stroke or TIA - increases your risk of having another stroke. Certain medications may
decrease stroke risk if taken regularly.
Heart disease - heart conditions, especially atrial fibrillation (an irregular heart beat), have a
greater stroke risk. Certain medications may decrease the risk if taken regularly.
To learn your risk of experiencing a stroke in the next ten years take the Stroke Risk Assessment. Within
seconds you will receive a report of your stroke risk compared to the average stroke risk for Americans of
the same age and sex. The results are not meant to predict whether or not you will suffer a stroke, but to
assist you in assessing your risk of having a stroke. This assessment should accompany, not replace, a
routine physical examination by your family physician.
Angiogram is an invasive procedure in which a catheter is inserted into an artery and passed through the
blood vessels to the brain. Once the catheter is in place, contrast dye is injected into the bloodstream and
X-ray images are taken. This test is used to diagnose and determine the location of aneurysms and
AVMs.
Magnetic resonance imaging (MRI) scan is a noninvasive test that uses a magnetic field and
radiofrequency waves to give a detailed view of the soft tissues of your brain. An MRA (Magnetic
Resonance Angiogram) is the same non-invasive study, except it is also an angiogram, which means it
also examines the blood vessels, as well as the structures of the brain.
Angioplasty/stents
Carotid endarterectomy
received t-PA within 3 hours of onset of stroke symptoms were at least 33% more likely to recover from
their stroke with little or no disability after 3 months [2,3].
T-PA can also be delivered right at the clot site in a procedure called intra-arterial thrombolysis. In this
method the t-PA drug doesnt have to travel through your entire body before reaching the clot. A doctor
called a Neuro Interventionalist performs this procedure during an angiogram. A very small catheter is
inserted into an artery in your groin and guided through your bloodstream up to the brain where the clot is
located. The t-PA drug is then released to dissolve the clot. The doctor also pushes the catheter back and
forth through the clot to help break it up. Typically this treatment option is only available at specialized
stroke care centers.
Blood thinners
Anticoagulants, or blood thinners, such as warfarin and antiplatelet agents such as aspirin, ticlopidine,
diprydamole, or clopidogrel interfere with the blood's ability to clot and can play an important role in
preventing stroke.
Angioplasty
Angioplasty is used to open blood vessels narrowed or blocked by plaque build-up in atherosclerosis. A
Neuro Interventionalist performs the procedure during an angiogram. A catheter is inserted into an artery
in the groin and then passed through the blood vessels to the plaque build-up. The doctor guides the
catheter through the bloodstream while watching a fluoroscopy (a type of x-ray) monitor. Once positioned
correctly, a balloon is inflated to flatten the plaques against the wall and open the artery to restore blood
flow.
Carotid endarterectomy
Sometimes plaque build-up is too great to treat with angioplasty and the plaque must be removed through
surgery. A common area for build-up of plaques is at the common carotid arteries in the neck where the
internal and external carotid arteries branch. If the carotid artery is more than 70% blocked, a surgical
procedure called an endarterectomy may reduce your risk of stroke by 65% [4]. Through an incision in
your neck the carotid artery is opened and the plaque removed to restore blood flow.
Recovery
Each person's mental and physical deficits are unique. For example, someone who has a small stroke
may experience only minor deficits such as weakness of an arm or leg. On the other hand, someone who
has a larger stroke may be left paralyzed on one side or lose his/her ability to speak and process
language. Some of these deficits may disappear over time with healing and therapy. The recovery
process is long and may take weeks, months, or years to understand the level of deficits you incurred and
regain function. Rehabilitation professionals can help set up a treatment plan and help others understand
the stroke person's needs and help with daily living activities.
Aphasia is a total or partial loss of the ability to understand or use words. Caused by damage
to the brain's language center, some people quickly and completely recover from aphasia after
a stroke. Others may have permanent speech and language problems. Speech problems can
range from trouble finding words to being unable to speak. Some people have problems
understanding what others are saying or have trouble with reading, writing or math. In other
cases, someone with aphasia may have trouble talking but can understand what others say.
Apraxia is the inability to control your muscles making movement uncoordinated and jerky.
Dysarthria is a loss of control over muscles in the face and mouth. Their voice may sound
slurred, muffled, or hoarse. The mouth may droop on one side of face due to muscle
weakness. Exercises can strengthen these muscles.
Dysphagia is difficulty swallowing making eating and drinking a challenge and choking a
danger. Tongue and lip exercises can help regain control.
Hemiparesis is a weakness of muscles on one side of the body. Improving posture, range of
motion, and strength can help regain control.
Take your medication every day as directed. Your medication helps to thin your blood and
prevent clots.
2.
3.
4.
Quit smoking.
5.
Exercise regularly. Youll feel good about yourself, alleviate depression, and build muscle
strength.
6.
7.
Limit your use of alcohol. It can be risky to drink alcohol if you take certain medications. Talk to
your doctor.
8.
Talk about your feelings. Sudden mood swings and depression are common and lessen with
time. A support group or counselor can help you and your family.
Clinical trials
Clinical trials are research studies in which new treatmentsdrugs, diagnostics, procedures, and other
therapiesare tested in people to see if they are safe and effective. Research is always being conducted
to improve the standard of medical care. Information about current clinical trials, including eligibility,
protocol, and locations, are found on the Web. Studies can be sponsored by the National Institutes of
Health (see clinicaltrials.gov) as well as private industry and pharmaceutical companies
(see www.centerwatch.com).
http://www.mayfieldclinic.com/pe-stroke.htm#.VgmIaHFViko
Brain healing
From Wikipedia, the free encyclopedia
This article needs additional citations for verification. Please help improve this
article by adding citations to reliable sources. Unsourced material may be
challenged and removed. (October 2013)
Brain healing is the process that occurs after the brain has been damaged. If an individual survives
brain damage, the brain has a remarkable ability to adapt. When cells in the brain are damaged and
die, for instance by stroke, there will be no repair or scar formation for those cells. The brain tissue
will undergo liquefactive necrosis, and a rim of gliosis will form around the damaged area.
Contents
[hide]
1 Scar formation
3 Functional recovery
4 References
Scar formation[edit]
Apart from a small amount in the blood vessels, there are no fibroblasts in the brain. A scar is formed
by fibroblasts producing collagen to repair an area, which will later contract. If scars did form in the
brain, the contraction would cause even more damage.
Functional recovery[edit]
Brain injury will commonly be accompanied by acute swelling, which impairs function in brain tissue
that remains alive. Resolution of swelling is an important factor for the individual's function to
improve. The greatest factor in functional recovery after brain injury comes from the brain's ability to
learn, called neuroplasticity. After injury, neuroplasticity allows intact areas of the brain to adapt and
attempt to compensate for damaged parts of the brain. Although axons and theperipheral nervous
system in the developing brain can regenerate, they cannot in the adult brain. This is partly because
of factors produced by cells in the brain that inhibit this regeneration. Dendrites, however, will
develop from intact axons, as part of the neuroplasticity process. After severe brain injury,
improvement in function related to neuroplasticity is unlikely to occur without help from health
professionals skilled in rehabilitation. Recent studies have found collagen is extensively distributed
throughout the brain and may be essential in protecting the brain against degeneration such as that
in Alzheimers[1][2]
Following stroke, the neuronal circuitries that support cognitive and sensory-motor functions are lost
due to neuronal death and dysfunction. Still, over a 3 to 6 months period, stroke patients regain some
neurological functions, albeit a majority remain disabled to a significant degree (Duncan et al., 2000).
In man, recovery processes primarily engage ipsilateral brain regions, and if damage is severe,
contralateral brain areas are involved as well (Ward, 2005). Recovery of function following transient
MCAO in the rat is complex, but it is clear that the contralateral hemisphere is involved (Kim et al.,
2005, Biernaskie, et al., 2005).
Certain motor skills recover within a few days after the lesion, suggesting that for such rapid recovery
of neuronal function the unmasking or activation of silent pathways or silent synapses must be
considered (Metz et al., 2005). At the cellular level, adaptive changes in neuronal morphology (axonal
growth, dendritic arborization, and spine remodeling) are seen in the contralateral cortex (Schallert et
al., 2000). These most certainly involve recovery of spine function, since ischemia causes spine
collapse and actin aggregation (Hasbani et al., 2001; Gisselsson et al., 2005). Axonal outgrowth is
limited by growth-inhibitors such as Nogo A (Buchli and Schwab; 2005). This inhibition can be
overcome by Nogo A antibodies (Seymour at al., 2005) or by blocking peptides or mutations (Lee et
al., 2004). Intrathecal delivery of Nogo A antibody for one month, starting as late as seven days after
ischemia, dramatically enhances functional recovery after stroke (Seymour at al., 2005), and is
associated with increased sprouting of cortico-rubral projections. The contribution of the individual
hemispheres for the recovery process will be explored within this project.
Cell genesis in neurogenic zones is stimulated following stroke (Arvidsson et al., 2002; Parent et al.,
2002). Neuroblasts are continuously generated up to 4 month after injury, providing a pool of cells
that potentially can develop into mature neurons (Thored et al., 2005). Neurogenesis is depressed by
inflammation occurring during recovery after stroke (Jakubs et al., 2007). Neuronal, glial, and
endothelial progenitor cells support plasticity of surviving neurons by releasing growth factors, or
providing cellular components (Zhang et al., 2005; Lu et al., 2003). In addition, angiogenesis is
prominent and may enhance vascularization of the surviving penumbra area as well as stimulating
neurogenesis (Busch et al., 2003).
http://www.europeanstrokenetwork.eu/index.php?
option=com_content&view=article&id=38&Itemid=47
The brain may recruit parallel pathways and networks that perform
similar functions. For example a part of the brain that controls shoulder
movement may start to take over movement of the hand muscles.
For the most part we are an adaptable species and will naturally seek
out behavioral strategies to compensate for what we have lost. For example,
as we become more forgetful we may make more lists.
WHAT REHAB DOES ACCOMPLISH
The key is to look at the various mechanisms of recovery and to figure out
how rehabilitation can positively influence each one. The recovery process
clearly has a component of natural biological recovery, for we know that
people will improve to some degree without rehabilitation. Like school,
rehabilitation brings to the table new learning and exercises that take people
to a higher functional level. Children who never go to school learn some skills
while those with education develop
much more sophisticated skills.
We have learned that exercise is more
than just strengthening and keeping
muscles moving. Experimental
evidence suggests that active functional
therapies can recruit and open up new
pathways in the brain. In one study a
group of normal people were taught to
play a one handed piano exercise for five days, while another group was
never shown the exercise. Brain activity was measured at the beginning of
the study and five days later. Increased brain activity could be measured over
the part of the brain that controlled the hand in those patients who performed
the five days of exercises as compared to those who did not.
Much more elaborate experiments have been performed in primates. A
discrete stroke was created by closing off small vessels in the brain that
resulted in weakness of one of the monkeys hands. One half of the monkeys
received exercises with food rewards while the other half did not. The half that
received therapy improved more rapidly, but more importantly, these studies
suggested that the brain was truly plastic. The part of the brain that
previously controlled shoulder movement had now taken over movement of
the hand. The brain had reorganized itself and done so more efficiently in
those who received monkey therapy. Research like this supports the notion
that therapies can facilitate the opening of new pathways and turn on brain
cells that previously were not primarily responsible for the movement of a
particular part of the body.
Another study reported that animals placed in
an enriched environment after a brain injury
did better. They were given more toys and
activity. Repetitive use of an extremity
enhanced recovery, as did increased cage size,
companions, stimulation and increased
activities. Physiological studies suggested that those animal receiving rehab
were better able to reorganize the structures in their brains. Rehab made a
difference!
These types of studies raise some interesting questions. Should we primarily
teach patients how to compensate for their deficits or should we focus our
strategies on paralyzed muscles for prolonged periods of time? How long will
it take to open up a new pathway and what is the best way to do it? If we
bypass the usual movement patterns and substitute new methods of
movement will we prevent the opening of parallel or collateral pathways?
How long do you have to work with a paralyzed muscle to turn on a collateral
network or neuron and can it be done routinely in humans?
In our current health care environment we may never know the answers to
many of these questions, for we are asked to discharge a patient from
rehabilitation as soon as possible. Clearly therapy should not go on for years,
but it may be that we are writing off some patients too soon and sacrificing
some potential gains.
the brain and the patients function improves. The problems with this
approach are many. The clinical benefit is modest and the amount of fetal
tissue available is limited. New methods of acquiring stem cells that are less
controversial will greatly enhance future research.
GENETICALLY ENGINEERED TRANSPLANTS. The controversy over the
use of fetal cells led to the use of genetically engineered cells. Neural cells
lines have been developed from human tumor lines by treating the tumor cells
so that they will no longer divide and one does not have to worry about
causing cancer. When transplanted into the Central Nervous System they
send out axons and acquire other
characteristics of neurons.
Within this group of cells are embryonic
precursor cells. These cells have the potential
to become a variety of different cells when
exposed to trophic growth factors. One of the
problems is how to guide the regenerating
axons into the right place. In frogs and rats
there appear to be guidance cues in the local environment where the cells
are implanted that instruct the axons and neurons on how to make the right
connection. It was cells like these that were used in the first human motor
neuron transplant.
http://www.richardsenelick.com/articles/rewiring-brains-rehabilitation-plasticity-andtransplants
Table of Contents
Know Stroke
What is a stroke?
Stroke Symptoms
Call 911
o
STROKE PREVENTION
o
Know Stroke
Each year in the United States, there are approximately 795,000
strokes. Stroke is the fourth leading cause of death in the country.
And stroke causes more serious long-term disabilities than any other
disease. Nearly three-quarters of all strokes occur in people over the
age of 65 and the risk of having a stroke more than doubles each
decade after the age of 55.
For African Americans, stroke is more common and more deadly even in young and middle-aged adults - than for any ethnic or other
racial group in the United States.
Learning about stroke can help you act in time to save a co-worker, friend, or relative. And making changes in your lifestyle
can help you prevent stroke.
What is a stroke?
A stroke is serious - just like a heart attack. A stroke is sometimes called a "brain attack."
Most often, stroke occurs when blood flow to the brain stops because it is blocked by a clot.
The brain cells in the immediate area begin to die because they stop getting the oxygen
and nutrients they need to function.
Stroke Symptoms
top
Call 911
If you believe you are having a stroke - or someone you know is having a stroke - call 911 immediately.
If you have high blood pressure, work with your doctor to get it under control. Many people do not realize they have
high blood pressure, which usually produces no symptoms but is a major risk factor for heart disease and stroke.
Managing your high blood pressure is the most important thing you can do to avoid stroke.
If you have diabetes, learn how to manage it. As with high blood pressure, diabetes usually causes no symptoms
but it increases the chance of stroke.
If you are overweight, start maintaining a healthy diet and exercising regularly.
STROKE PREVENTION
Eat right
Exercise
Don't smoke
Prepared by:
Office of Communications and Public Liaison
National Institute of Neurological Disorders and Stroke
National Institutes of Health
Bethesda, MD 20892
NINDS health-related material is provided for information purposes only and does not necessarily represent
endorsement by or an official position of the National Institute of Neurological Disorders and Stroke or any
other Federal agency. Advice on the treatment or care of an individual patient should be obtained through
consultation with a physician who has examined that patient or is familiar with that patient's medical history.
All NINDS-prepared information is in the public domain and may be freely copied. Credit to the NINDS or the
NIH is appreciated.
Last updated June 18, 2013
http://www.ninds.nih.gov/disorders/stroke/stroke_needtoknow.htm#URGENT
Nurses play a pivotal role in all phases of care of the stroke patient. The 2 phases of stroke care:
(1) The emergency or hyperacute care phase,2,3 which includes the prehospital setting and the
emergency department (ED), and (2) the acute care phase, which includes critical care units,
intermediate care units, stroke units, and general medical units. Nurses are often responsible for
the coordination of care throughout the continuum. 49 Coordinated care of the patient results in
improved outcomes, decreased lengths of stay, and decreased costs.10
Stroke is a complex disease that requires the efforts and skills of all members of the
multidisciplinary team. In developing this comprehensive overview, the writing panel applied the
rules of evidence and formulation of strength of evidence (recommendations) used by other AHA
writing groups11 (Table 1). We also cross-reference other AHA guidelines as appropriate.
http://stroke.ahajournals.org/content/40/8/2911.full