Interactive Transcript
0:00
Up until now,
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with respect to the evaluation of trauma
0:04
and degenerative diseases of the globe,
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we have relied on CT scanning.
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Now you may ask, "Why rely so heavily on CT scanning,
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particularly for diseases that also occur in children?"
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The problem with MRI scanning in globe
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pathology is that the eye moves.
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So it's very hard to have the patient fixate their gaze
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for 3-5 minutes during a typical MRI pulse
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sequence and not have motion artifact obscure subtle
0:33
abnormalities, such as anterior hyphemas
0:37
or small detachments of the globe.
0:40
In this situation,
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we are most concerned with the intracranial extension
0:45
of this patient's retinoblastoma.
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We've seen the CT scan and we saw the calcification.
0:51
Calcification is much better visualized
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on CT rather than MRI.
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This first pulse sequence that's being shown
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is the brain image, a FLAIR scan.
1:03
However, it nicely depicts the difference in the intensity
1:09
of the left globe compared to the right globe.
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The right globe has normal CSF intensity
1:17
in the vitreous.
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However, the left globe is bright in signal intensity
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on this FLAIR scan.
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We note that there are different components
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of the globe signal intensity.
1:34
There is the very high bright signal intensity,
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and then we have some intermediate
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signal intensity tissue.
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And to establish whether or not this represents
1:46
hemorrhage versus tumor will require gadolinium
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enhanced pulse sequences.
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We also note, in this case, that
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there appears to be a mass
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between the internal carotid arteries
2:00
in the suprachoroid
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portion of the internal carotid arteries in the
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suprasellar cistern. To evaluate this mass,
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we would prefer to have coronal images.
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These are the coronal T1-weighted scans
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through the orbits, as well as the brain.
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As we scroll through this,
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we'll initially look at the orbital imaging.
2:25
The orbital imaging demonstrates the absence of a lens
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on the left side, and the enlargement of the globe,
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with mixed signal intensity abnormality.
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Here we have slightly hyperintense
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area of T1-weighted signal.
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Here we have a mild hyperintense area of signal.
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And this should be CSF in signal intensity.
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So, both of these are abnormal.
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But there's different components within the abnormality.
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If we scroll more posteriorly,
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we see that we have marked enlargement of
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the left optic nerve sheath complex.
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The left optic nerve sheath complex
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is enlarged compared with the right, and this will
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extend posteriorly through the optic canal.
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Here we are scrolling posteriorly and we enter
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the optic canal. From the optic canal,
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we have the prechiasmal optic nerve segment.
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On the right, we have the normal optic nerve.
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On the left, you have an enlarged optic nerve.
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We then scroll more posteriorly.
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On this image,
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we see the pituitary gland as the slightly hyperintense
4:00
material between the cavernous carotid arteries.
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The cavernous carotid arteries
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show the signal void of flow.
4:08
However, above the pituitary gland, we find this mass.
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This is the intracranial extension of the retinoblastoma,
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coursing along the optic nerve
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to involve the optic chiasm.
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We can scroll more posteriorly and we arrive at
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the posterior margin of the optic chiasm.
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On this image,
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we see the third ventricle,
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inferior portion, and we see the posterior
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portion of the optic chiasm.
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However, there is a mass which is infiltrating the posterior
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portion of the optic chiasm,
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even to the base of the third ventricle.
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It is now at the point of entering the brain.
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This is better seen on the axial
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scans on T2 weighting.
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When we scroll through this
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sequence,
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we again see the abnormal mass
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in the suprasellar cistern.
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However,
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emanating posteriorly, we can see extension of the tumor
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into the brain substance itself.
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This is depicted as the brighter areas
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on the T2-weighted scan.
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And this tumor can track along the optic pathway into
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the optic radiations of the temporal lobe
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and even to the occipital lobe.
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Let's now look at the post-contrast fats suppressed
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T1-weighted scans.
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In this case,
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one can see the intracranial component of the tumor in
6:08
the suprasellar cistern and extending
6:11
through the optic canal.
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We also see a component that is in the
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cistern anterior to the midbrain.
6:22
These are seen along the surface of the midbrain and in
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the suprasellar cistern, as well as along the
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optic nerve in the orbit.
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Once again,
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it is important to make sure that one scrolls through
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and observes the signal intensity enhancement
6:44
characteristics of the contralateral globe
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to exclude bilateral retinoblastomas,
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which may occur in one third of patients.
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In those patients who have familial retinoblastoma
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and bilateral retinoblastoma,
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one may have what is called the trilateral retinoblastoma.
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In this case, you see a mass in the pineal region.
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The pineal gland is considered the
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"third eye", because you may have pineal blastomas in
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association with bilateral retinoblastomas
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in those patients who have hereditary retinoblastoma.
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This patient does not have that.
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However,
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on the axial post-gadolinium enhanced
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scans, through the pontine region,
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one sees an area of abnormal enhancement.
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This is on the right side,
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and this area of contrast enhancement
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represents subarachnoid seeding
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within the brain of retinoblastoma.
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In this case, along the root entry
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zone of the fifth cranial nerve.
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If one scrolls additionally through this case,
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it sheds light on the abnormality that was identified
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at the surface of the midbrain.
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This area of contrast enhancement is along the
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typical route of the third cranial nerve,
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leaving from the interpeduncular cistern
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and coursing towards the left eye.
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So this patient has subarachnoid seeding along the left
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third cranial nerve as well, as the right fifth cranial nerve,
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and therefore, has a very poor prognosis.
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