Brain SPECT Imaging in Dementia:

Brain SPECT Imaging in Dementia:

Alzheimer's Dementia:

Dementia affects 10% of people over the age of 60 years and Alzheimer's accounts for roughly 50% of these cases. Alzheimer's disease (AD) has a prevalence of 0.3% in patients aged 60-69 years, but increases to nearly 11% in 80-89 year olds [2]. The mental degeneration associated with Alzheimer's is insidious and progressive memory loss is the most important symptom [2]. Transient stabilization of cognitive and behavior function can be achieved with acetylcholinesterase inhibitor therapy [6].

Dementias produce deficits in perfusion, in part reflecting decreased metabolic needs. In Alzheimer's one classically sees bilateral decreased metabolism (PET imaging) and flow (SPECT imaging) in the temporal and parietal lobes with sparing of the primary motor, sensory, and visual cortices. The temporoparietal defects are noted in about 65% of Alzheimer's patients and are the most consistently recognizable sign of Alzheimer's, particularly when relatively symmetrical (although symmetric, the defects are not necessarily of the same magnitude and severity [2]). This pattern has a predictive value of over 80% for the diagnosis of Alzheimer's disease. A correlation has also been described between the severity of these defects, and the severity of the patient's dementia. Unilateral temporoparietal or isolated frontal defects can be found in up to 20% of Alzheimer's patients, and are more commonly seen early in the disease process. When the medial temporal lobes are particularly abnormal, the memory deficit is often more marked and reflects the functional importance of this region for memory. Frontal lobe abnormalities may also be seen in cases of advanced disease, but are less specific for Alzheimer's. The cerebellum, primary visual areas, and primary sensorimotor areas along the central sulcus remain relatively intact. Perfusion defects identified on SPECT images have been shown to correlate histologically to areas that contain large amounts of plaques and neurofibrillary tangles. In the later stages of the disease process, cortical atrophy itself contributes approximately 20% of the decrease in activity seen in the temporoparietal areas, possibly secondary to volume averaging.

Overall, Tc99m-HMPAO imaging has a sensitivity between 80-90% and a specificity between 65-87% for the diagnosis of Alzheimer's dementia. The negative predictive value of a normal study is approximately 80% (ie: about 20% of patients affected with Alzheimer's disease may have a normal CNS perfusion exam) [1,2]. In one study which compared SPECT exam findings with autopsy results, SPECT imaging had a sensitivity of 63%, a specificity of 82%, a positive predictive value of 81%, a negative predictive value of 65%, and an accuracy of 71% for the diagnosis of Alzheimer's (which was comparable to the clinical assessment for the disorder) [4]. This same study found that the greatest utility of SPECT imaging was in increasing the confidence of the clinical diagnosis for AD [4]. When SPECT imaging findings and clinical diagnosis for Alzheimer's disease are considered together, a positive SPECT interpretation increases the odds of having Alzheimer's by an additional factor of five [4]. SPECT imaging also holds potential for monitoring response to medical therapy [6]. Regional cerebral perfusion appears to remain stable in patients with stabilization of cognitive function while receiving acetylcholinesterase inhibitor therapy [6].

Other disorders to be considered in the differential of biparietal/temporal defects include: Parkinson's disease with dementia, bilateral parietal infarcts, multi-infarct dementia (typically asymmetric, and multiple small cortical defects), vertebral basilar insufficiency (produces bilateral occipital perfusion abnormalities which should be distinguished from the parietal abnormalities associated with Alzheimer's), hypoglycemia, and carbon monoxide poisoning. In a small percentage of patients, a combination of multi-infarct and Alzheimer's dementia may coexist (mixed dementia).

Parkinson's Disease:

There are four major dopaminergic pathways in the brain [16]. The largest of the four is the nigrostriatal pathway which contains about 80% of the brains dopamine and is composed of neurons that originate in the substantia nigra of the mid brain and terminate in the caudate and putamen- collectively termed the striatum [16]. If 60-70% of the nigrostriatal pathway cells are lost because of disease, the classic symptoms of parkinsonian motor dysfunction develop (resting tremor, rigidity, postural instability, and bradykinesia or akinesia [16]. Parkinsonian syndrome is an umbrella term for a group of neurologic disorders that occur due to nigrostriatal degeneration and include idiopathic Parkinson disease (comprises 75% of Parkinsonian syndrome cases), multisystem atrophy, progressive supranuclear palsy, corticobasilar degeneration, diffuse Lewy body disease, and vascular Parkinson disease [16].

Idiopathic parkinson disease is a progressive neurodegenerative disorder resulting from the progressive death of dopaminergic neurons in the nigrostriatal pathway [5]. It occurs in 1% of the population older than 55 years of age [7]. The median age at diagnosis is 60 years, although 5-10% of patients present before age 50 years, and the average duration of disease is 15 years from diagnosis to death [16]. Men are affected 1.5-2 times more frequently than women [16]. There has been a significant increase in incidence over the past 30 years, particularly in men over the age of 70 years [16].

Symptoms consist of rigidity, bradykinesia, difficulty in initiating and stopping movement, and a resting tremor [5]. Motor disturbances begin only after a loss of approximately 70-80% of striatal dopamine- thus, there is a long latent period which precedes the development of clinical symptoms [5]. Approximately 10% of patients affected with Parkinson's disease will develop dementia [2]. Generally, the perfusion pattern in these patients in non-specific and demonstrates either normal or mild global cortical deficits. A pattern of bilateral posterior parietal/temporal defects indistinguishable from Alzheimer's may be observed in patients with Parkinson's disease with dementia [2]. 

Other agents used for imaging Parkinsons include 123I-FP-CIT (which images dopamine transporter binding and presynapic dopaminergic degeneration of the nigrostriatal tract), 123I-IBZM (which images dopamine D2 receptors), and 123I-MIBG that can demonstrate pronounced cardiac sympathetic denervation in patients with Parkinsons disease (however, there is considerable overlap between Parkinsons and Atypical Parkinsons Disorder and low MIBG uptake alone does not necessarily indicate PD) [8].

123I-ioflupane:

The agent 123I-FP-CIT or 123I-ioflupane (N-w-fluoropropyl-2?-carbomethoxy-3?-(4-123I-iodophenyl) nortropane) is a molecular analog of cocaine that binds reversibly with high affinity to the dopamine transporter protein (DaT) [9,12]. DaT is a transmembrane protein in the presynaptic membrane of the dopaminergic synapse that transports dopamine from the synaptic cleft back into the presynaptic neuron [9]. Dopamine transporters function to clear and recycle dopamine from the synaptic cleft located in the putamen and caudate nucleus [13]. The agent can be used to demonstrate the location and concentration of dopamine transporters (DaTs) in the presynaptic terminals of striatal dopaminergic nerons [9,12]. The reduction of tracer binding is associated with the integrity of the nigrostriatal pathway- namely dopaminergic neuronal density and axonal dysfunction [17].

123I-ioflupane can aid in separation of patients with essential tremor from those with presynaptic Parkinsonian syndromes by identifying a presynaptic dopaminergic deficit [9]. DaT concentrations are lower in the striatum (particularly the putamen) in presynaptic Parkinsonian syndromes (even in early stage disease) and will be normal in patients with essential tremor, drug induced parkinsonism, and psychogenic parkinsonism [9,15]. DaT concentrations are also normal in patients with Alzheimers dementia, but are significantly reduced in patients with dementia with Lewy bodies [9], as well as in patients with progressive supranuclear palsey [15].

Ioflupane is an analog of cocaine. Medications that interfere with 123I-ioflupane binding should be discontinued for at least 5 half-lives [9]. Cocaine, amphetamines, and methylphenidate severely decrease 123I-ioflupane binding to DaT [9,16]. The CNS stimulants used for appetite supression ephedrine and phentermine may also decreased 123I-ioflupane binding [9,16]. Bupropion (used for smoking cessation), fentanyl, and some anesthetics (ketamine, phencyclidine, and isoflurane) may decrease 123I-ioflupane binding, as well [9,16]. Cholinesterase inhibitors and neuroleptics probably do not interfere significantly with binding [9].

Anti-Parkinson drugs in standard doses such as levodopa,  l-dihydroxyphenylalanine, dopamine agonists, monoamine oxidase B inhibitors, N-methy-D-aspartate receptor blockers, amantadine, and catechol-O-methyltransferase inhibitors in standard doses, do not interfere with binding to any significant degree and do not need to be stopped [9]. A caveat to this is that long term usage of levodopa can down-regulate the expression of DaT on the striatal presynaptic neurons [16].

Selective serotonin reuptake inhibitors used in anxiety and depression may increase binding to DaT somewhat, but should not interfere with exam interpretation [9,16]. It should be noted that certain medications - selegiline, sertraline, citalopram, and paroxetine can significantly affect the scan [13].

There is a normal decrease in DAT striatal binding of about 5-7% per decade, but this decrease is small in comparison with decreases caused by disease and normally should not interfere with exam interpretation [16].

Examination:

The injection may contain up to 6% of free 123I [16]. Thyroid blocking using a single 400 mg dose of potassium perchlorate or a single dose of potassium iodide oral solution or Lugol's solution (equivalent to 100 mg of iodide) at least one hour prior to tracer injection may be considered, but even without blocking, the dose to the thyroid gland from the agent is low [9].

The dose is typically 5 mCi (185 MBq) given via a slow (20 second) IV infusion [9]. Patients do not need to be kept in a dim or quiet environment prior to injection [9]. Imaging is usually started 3-6 hours after tracer injection [9,16].

For imaging, the photopeak should be set for 159 keV +/- 10% and a high-resolution collimator should be used [9,16]. The field of view for imaging should include the brain and have the smallest possible circular rotational radius possible- typically 11-15 cm [9]. A 128 x 128 matrix is recommended for a pixel size of 3.5-4.5 mm [9]. Images can be acquired using a step-and-shoot mode with angle increments of 3 degrees or using a continuous rotation [9]. The number of seconds per head position is usually 30-40 seconds and a minimum of 1.5 million counts should be collected for optimal images [9,16]. However, this may be challenging in severely abnormal scans with minimal striatal activity [16].

Because 123I-ioflupane is excreted by the kidney, patients with severe renal impairment may have increased radiation exposure and altered  123I-ioflupane imges [9].

Exam findings:

The exam is particularly susceptible to motion artifacts [16]. The normal exam should demonstrate homogenenous, well-defined tracer uptake within the striata that should appear as two symmetric crescent or comma-shaped regions of focal activity corresponding to the paired caudate and putamen on transaxial images [9,16]. Mild asymmetry between left and right may occur in healthy individuals [16]. A normal exam would be expected in patients with essential tremor, dystonic tremor, drug-induced Parkinsonism, medication or drug induced tremor, most vascular PD, Alzheimers, psychogenic tremor, and in healthy individuals [16].

Abnormal striata will have reduced intensity on one or both sides, often shrinking to a circular or oval shape [9]. Other authors state that in Parkinson disease DAT imaging typically shows asymmetric reduction, predominantly in the striatum contralateral to the clinically most affected side [17]. Caudate and putaminal activity should be compared- generally the putamen, in particular the posterior putamen, is affected earlier and to a greater degree than the caudate in patients with Pakinsonism [13]. This may frequently be asymmetric, particularly in the early stages of disease, with a more pronounced loss in the striatum contralateral to the clinically affected limbs [16]. Abnormal studies typically fall into one of three appearances: asymmetric decreased putaminal activity (this produces a comma-shaped focus on one side and a period-shaped focus on the other side; absent putaminal activity, but preserved caudate activity (two period shaped foci of activity); or absence of putaminal activity and greatly reduced activity in one or both caudate nuclei [13,16].

There are a few pitfalls in exam interpretation- the most common is the "semicolon sign" secondary to forward head tilt [16]. This results in the caudate nuclei being seen on separate axial slices from the putamen and gives the false impression that DaT activity in the putamenis decreased or absent [16]. By scrolling up and down through the striata, it will be apparent that there is normal intense activity in these structures [16]. Another SPECT artifact is the "pinwheel sign" which arises from rotational head motion during exam acquisition [16]. The "kissing caudate sign" occurs when left and right caudate appear fused without an intervening gap- this occurs secondary to either patient motion or by using too large a radius for the SPECT exam [16].

Intense activity outside the brain included in the FOV can result in a scaling artifact [16]. If intense uptake in the salivary glands is included in the FOV, it can result in striatal activity being scaled down on reconstruction images [16]. Striatal activity may appear absent resulting in a false positive exam [16].

123I-ioflupane has been shown to have a sensitivity and specificity (exceeding 90%) and accuracy in differentiating between Parkinson disease and essential tremor [13,17]. Image quantification can improve diagnostic accuracy [15]. DAT imaging can lead to a change in diagnosis in 31-50% if patients and changes in management for 52-58% of patients [16]. However, about 11% of patients with Parkinsonian syndrome can have normal DAT imaging [16]. The patients have been shown to behave differently from subjects with classic PD in that they lack an appropriate response to medication [16]. They also show little or no progressive decline of motor function and their prognosis is more favorable [16].

Drug-induced Parkinson (DIP):

DIP may develop in individuals treated with dopamine receptor-blocking agents, such as neuroleptics and antiemetics, dopamine depleters, and calcium channel blockers [14]. DIP symptoms usually disappear within 2 months of discontinuation of the fofending drug [14]. DAT imaging is normal in patients with DIP because the condition occurs in the absence of presynaptic dopaminergic deficits [14].

123I-MIBG in Parkinsons disease:

Reduction of MIBG uptake in the heart (cardiac sympathetic denervation) is considered a specific finding for idiopathic Parkinson's disease without autonomic failure and can be used to differentiate it from other Parkinsonian syndromes [10]. The pathobiologic mechanism appears to be neurodegenerative, associated with alpha-syniclein accumulation in the autonomic cardiac plexus [11]. However, other authors indicated that there is considerable overlap between Parkinsons and Atypical Parkinsons Disorder and low MIBG uptake alone does not necessarily indicate PD [8]. Although sympathetic function appears globally reduced on planar MIBG imaging, 11C Hydroxyephedrine PET imaging suggests the denervation to be segmental, involving the proximal lateral LV wall most severely, and with relative sparing of the anterior and proximal septal walls [11].

Multi-infarct Dementia:

Multi-infarct dementia (MID) is characterized clinically by multiple cerebral infarcts that occur sporadically and produce a step-wise deterioration in intellectual function. MID is the second most common cause of dementia in the elderly [2]. HMPAO findings that suggest the diagnosis include multiple, bilateral, and randomly distributed cortical perfusion defects that follow vascular territories. The basal ganglia, motor, and sensory cortices may also be involved (spared in Alzheimer's).

Ischemic brain disease refers to dementia secondary to ischemia without evidence of frank infarction. The Diamox challenge test can be used to identify areas of perfusion abnormality in these patients as their baseline exam is often normal.

HIV:

AIDS dementia complex (ADC) can be seen in up to 11 to 65% of HIV patients. Multiple areas (small and large) of decreased perfusion are identified in the cortical and subcortical regions, often producing a patchy distribution of the tracer. Basal ganglia involvement is also common. The number of defects identified does not necessarily correlate with the severity of the patients' symptoms or clinical findings. The perfusion pattern may improve with therapy (AZT, Calcium channel blockers). SPECT imaging has about a 90% sensitivity in the detection of ADC. The MRI findings in these patients range from normal, to atrophy, to multiple focal white matter signal abnormalities.

Scintigraphic findings similar to ADC have also been described in cocaine polysubstance drug abusers, Lyme disease, and chronic fatigue syndrome. In polysubstance drug abusers the defects are felt to be related to the vasospastic actions of cocaine. Although improvement can be seen following abstention or treatment with buprenorphine, many of the defects are permanent. A recent study [3] suggested that the improvement in perfusion was related primarily to treatment with buprenorphine, was dose dependent, and again worsened upon removal of the drug.

Patients with vasculitis secondary to Lyme disease may demonstrate SPECT findings indistinguishable from ADC, including basal ganglia involvement. The scan will improve in these patients following successful antibiotic therapy.
 

Pick's Disease (Frontal lobe dementia):

A rare frontal dementia characterized by bilateral cerebral degeneration with atrophy affecting the frontal or temporal lobes and involving both gray and white matter [2]. Symptoms usually include the gradual onset of confusion with respect to place and time, anomia, slowness of comprehension, loss of tact, and changes in personality and behavior [2]. SPECT images demonstrate bilateral, diffuse decreased frontal lobe perfusion extending to the cingulate gyrus [2].

Progressive supranuclear palsy:

PSP is characterized by parkinsonism with bradykinesia and rigidity, postural instability, and a pseudobulbar syndrome with dysarthria and dysphagia [13]. The key feature of PSP is supranuclear palsy of vertical gaze (although this may be absent at disease onsset) [13]. In contrast to Parkinson disease, PSP manifests as a symmetric rather than asymmetric-rigid syndrome [13]. PSP also initially targets the trunk and neck, rather than the limbs, causing early postural and gait instability with falls [13]. The condition will also produce decreased activity within the frontal lobes. FDG PET reveals decreased glucose metabolism in the basal ganglia, midbrain, and mindline frontal lobes- in particular, the anterior cingulate gyrus [13]. There is no cortical deposition of amyloid on amyloid PET imaging [13]. 123I-ioflupane demonstrates reduced striatal dopaminergic activity with variable patterns that may be symmetric or asymmetric and may affect the putamen or caudate nucleus [13].

Huntingtons disease:

Huntingtons disease is an autosomal dominant, degenerative movement disorder characterized by chorea, dementia, and psychiatric symptoms [2]. Brain SPECT imaging will demonstrate decreased or absent tracer uptake in the caudate or basal ganglia [2]. The defects are usually bilateral, but are not necessarily symmetric [2].

Korsakoff's Syndrome:

Seen in alcohol abusers, it is due to thiamine deficiency. Perfusion defects tend to involve the posterior cortical regions predominantly.

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