Interactive Transcript
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This is an adolescent with a history
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of Von Hippel-Lindau syndrome,
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who's had several prior resections of
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cerebellar hemangioblastomas.
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We can see the encephalomalacia from the
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prior resection, this hypointense appearance
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on T2-weighted imaging, likely related to
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hemosiderin from the prior resection, and
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some degree of cerebellar volume loss.
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At the present time, we can see several
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enhancing lesions, which, given the
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history of Von Hippel-Lindau syndrome,
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likely represent small hemangioblastomas.
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Here's another lesion.
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Here are two additional lesions and
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another one in the inferior aspect
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of the left cerebellar hemisphere.
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Note that there is a lesion in the
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region of the obex, which is for
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some reason a common place for these.
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Hemangioblastomas do occur
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in Von Hippel-Lindau syndrome.
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There are other little enhancing areas.
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So some of which we have to
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look to see, are they a vessel?
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This looks like a vessel, but this is not.
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Given the setting of Von Hippel-Lindau
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syndrome, where we know there's a genetic
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predisposition for developing hemangioblastomas,
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every single one of these
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little enhancing areas is suspicious
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for an additional hemangioblastoma.
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These are multicentric lesions that can have
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multiple of them throughout the neural axis,
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in particular the cerebellum and in the spine.
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The prototypical hemangioblastoma that
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is described is a cystic lesion with an
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enhancing neural nodule that has some imaging
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similarities to a pilocytic astrocytoma.
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They very often can be a solid enhancing
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lesion, especially in the spine.
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Especially in the spine.
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They're very often just solid enhancing lesions.
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It's important to note that
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these lesions enhance because of
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the vascularity of the lesion.
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So they have a propensity to bleed.
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It is not just a regular solid tumor.
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These are highly vascular lesions.
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So it's important to be aware of that.
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Now, if we look
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the right globe, We've seen abnormality.
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Well, how do we make sense of it?
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Well, one of the things that can often help is
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an understanding is look at what you do know.
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So the left globe, we have the vitreous
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here, which is hyperintense in T2-weighted
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imaging, and it suppresses on FLAIR imaging.
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We have a normal morphology.
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In contrast, the right globe, we have several
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different components, including this area
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here, where it is intermediate hypointense
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signal on T2-weighted imaging without any
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appreciable suppression on FLAIR imaging.
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We have a crescentic area of T2 hyperintense
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signal that does appear to
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suppress on FLAIR imaging, and we have
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this hypointense interface here, and
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this likely is a susceptibility artifact.
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And so this is an appearance that
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is seen with intravitreous silicone
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injection seen after vitrectomy.
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So this patient with Von Hippel-Lindau
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syndrome had a right orbital lesion.
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These orbital lesions typically are
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evaluated with things such as fluorescein
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angiography and optical coherence
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tomography, which are performed by
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ophthalmologists, often retina specialists.
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And so the primary evaluation is typically
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not from a radiologic perspective.
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However, this is the post-treatment appearance
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after a vitrectomy of the right globe.
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So it's important to be aware of that, and
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it's important to look at the globes in
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patients with suspected Von Hippel-Lindau
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syndrome to see if we can see some potential
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enhancing component, which may result in
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accelerated visits to the ophthalmologist.
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But ophthalmology surveillance is, with
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dilated fundoscopic exams, is one of
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the key follow-up recommendations for
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patients with Von Hippel-Lindau syndrome.
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So this patient has multifocal multicentric
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cerebellar hemangioblastomas in the setting
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of several previously resected cerebellar
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hemangioblastomas, as well as prior right-sided
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detrectomy for a right-sided ocular lesion.
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