CNS Imaging

Question 1

Goal of brain imaging in NM?

Answer 1

Evaluate function - think of sz and ischemia, FDG brain for demential, cisternograms/shunt series etc.

Question 2

What 3 agents are commonly used in CNS nukes? How are they separated?

Answer 2

Extracted (can be used for parenchymal imaging - SPECT): HMPAO, ECD
NOT extracted (not used for parenchymal imaging): DTPA

Question 3

What property of HMPAO and ECD allow them to cross BBB? Why is this important? What do they accumulate proportional to?

Answer 3

Neutral and lipophilic - they accumulate in the brain and can be used with SPECT to look at brain blood flow which mimics metabolism. Accumulate in cortex proportional to blood flow (gray > white matter).

Question 4

What is the main difference between HMPAO and ECD?

Answer 4

HMPAO washout it fast. ECD washout is slow (more rapid clearance from blood pool with ECD).

Question 5

Where does uptake favor in HMPAO and ECD, respectively?

Answer 5

Frontal lobe, thalamus, cerebellum - HMPAO

Parietal and occipital lobes - ECD

Question 6

What property of DTPA allows it to stay in the blood?

Answer 6

Lipophobic - it stays in the blood or CSF if you put it there. Doesnt cross BBB.

Question 7

What is the advantage of DTPA over HMPAO and ECD?

Answer 7

It can be repeated without delay.

Question 8

What is the main utility for DTPA?

Answer 8

Shunt studies, NPH, brain death

Question 9

Why do NM studies for seizure? Findings?

Answer 9

To localize seizure focus. Will be hot during ictal state, and cold interictal. Plan for surgery.

Question 10

Describe properties of 201-Thallium. Decay type, half life, emissions.

Answer 10

Decay - electron capture
Half life - 3 days (73 hours)
Major emissions via characteristics x-rays of the daughter product Mercury 201 @ 69 kEV and 81 kEV
Usually given with chloride so it can be rapidly removed from blood

Question 11

How does thallium behave? What conditions increase uptake?

Answer 11

Like potassium - crosses membranes via Na+/K pump. Tumors and inflammatory conditions increase the uptake of the tracer. Need living cell to transport it (tissue viability)

Question 12

Normal distribution of 201-Thallium?

Answer 12

Thyroid, salivary glands, lung, heart, skeletal muscle, liver, spleen, bowel, kidneys, and bladder - muscle twitching is hot

Question 13

Positive or Negative in the following:

1) Toxoplasma infxn
2) Lymphoma
3) Kaposi Sarcoma (gallium?)
4) Tumor
5) Necrosis

Answer 13

1) Negative
2) Positive
3) Positive (gallium negative)
4) Positive
5) Negative

Question 14

What tracers are used for brain tumor SPECT?

Answer 14

201 Ti more commonly, and Sestamibi less commonly.

Question 15

Do inflammatory conditions show up with 201 Ti SPECT?

Answer 15

Yes, but not as intense as tumor. Higher tumor grade = higher activity.

Question 16

What is control for thallium study?

Answer 16

Scalp uptake. Abnormalities have greater uptake.

Question 17

Can you use Thallium in conjunction with HMPAO?

Answer 17

Yes.

Question 18

Thallium Hot, HMPAO cold - what is it?

Answer 18

Tumor

Question 19

Thallium cold, HMPAO cold - what is it?

Answer 19

Necrosis

Question 20

CNS Lymphoma, toxo, bacterial abscess, cryptococcus, and TB are positive with what tracer? CNS lymphoma is also positive with what other tracer? How does this help?

Answer 20

Gallium, Thallium. Thallium helps differentiate CNS lymphoma with Toxoplasmosis (toxo will be cold, CNS lymphoma will be hot)

Question 21

What do you look for in brain death imaging?

Answer 21

Absence of intracerebral perfusion

Question 22

What vessel must be identified with radiotracer otherwise study is repeated?

Answer 22

Common carotid

Question 23

Where will tracer stop in the setting of brain death?

Answer 23

Skull base

Question 24

What is the hot nose sign?

Answer 24

Secondary to perfusion through the external carotid to the maxillary branches - it cant be used to call brain death though because it is only a secondary sign

Question 25

Is SPECT used to dx stroke?

Answer 25

NO, but you can look at it

Question 26

Acute stroke is what on SPECT?

Answer 26

Cold

Question 27

Subacute stroke is what on SPECT?

Answer 27

Warm, from luxury perfusion (blood flow is more than dead cells need)

Question 28

Chronic stroke is what on SPECT?

Answer 28

Cold

Question 29

In ischemia, what medications are given to evaluate for cerebrovascular reserve? What is the result?

Answer 29

Acetazolamide (diamox) -> perfusion tracer. Image pre and post diamox; Areas already maxed on autoregulatory vasodilation are seen as hypointense (risk for ischemia), but areas that could benefit from revascularization will show worsening tracer uptake -> take to angio.

Question 30

What is diamox?

Answer 30

Acetazolamide

Question 31

Common indication for FDG brain PET?

Answer 31

Dementia imaging - because blood flow mimics metabolism HMPAO and ECD can also be used for dementia imaging

Question 32

What area of the brain will show activity on FDG PET for the following conditions?

1) Alzheimers
2) Multi-infarct dementia
3) Dementia with lewy bodies
4) Picks/Frontotemporal Dementia
5) Huntingtons

Answer 32

1) Low posterior temporoparietal cortical area (identical to parkinson’s, posterior cingulate gyrus is first abnormal area)
2) Scattered areas
3) Low in lateral occipital cortex with SPARING of the cingulate gyrus (cingulate island)
4) Low in frontal lobe
5) Low activity in caudate nucleus and putamen

Question 33

Condition with depressed blood flow and metabolism affecting the cerebellar hemisphere after a contralateral supratentorial insult?

Answer 33

Crossed Cerebellar Diaschisis

Question 34

Is there pathology in the cerebelum with Crossed Cerebellar Diaschisis? Why?

Answer 34

NO - briefly, corticopontine-cerebellar pathway is disrupted and is shut down, pathology is in the cerebral hemisphere but affects the contralateral cerebellar hemisphere due to above pathway

Question 35

What tracer is used for CSF imaging?

Answer 35

111 In DTPA

Question 36

Explain normal CSF imaging exam + timing.

Answer 36

T0 = LP
T2-4 hrs - ascends and reaches basal cisterns
T4-24 hrs - flows around sylvian fissues and interhemispheric cistern
T24 hrs - clear from basilar cisterns and be over the convexities

Question 37

What are some things that would be indicative of a negative CSF imaging exam?

Answer 37

1) tracer in lateral ventricles

2) failure to clear from the cisterns and localize over the convexities at 24 hours

Question 38

What do you look for on communicating hydrocephalus (NPH = Wet wobbly wacky)?

Answer 38

1) early entry (4-6 hours) of tracer into lateral ventricles
2) persistence of tracer in the lateral ventricle > 24 hours
3) delay in assent to the parasaggital region > 24 hours

Question 39

Can radionuclide cisternogram differentiate between communicating vs non-communicating hydrocephalus?

Answer 39

No - doesnt normally enter the ventricles

Question 40

Differentiate NPH and non-obstructive (communicating) hydrocephalus? Hint: clinical

Answer 40

High opening pressure on LP with NPH

Question 41

Most common sites (3) of CSF leak on cisternogram? Purpose of pledgets?

Answer 41

Between the cribiform plate and ethmoid sinus, from the sella turcica into the sphenoid sinus, and from the ridge of the sphenoid to the ear. Dont forget to image pledgets jammed into patient’s nose prior to exam (compare radiotracer in serum to pledgets and > 1.5 is positive)

Question 42

Radiotracer for shunt patency study?

Answer 42

Tc DTPA

Question 43

Normal shunt patency study vs abnormal?

Answer 43

Normal = radiotracer in peritoneum so distal end is patent, then manually occlude the distal limb to force into ventricles sp proximal end is patent
Abnormal = fails to reflux into ventricles or it does but doesn't clear so proximal obstruction, or delayed tracer into the peritoneum (> 10 min) may mean partial distal obstruction