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Suprasellar Meningioma

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Let's look at this middle-aged female in her 40s

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with a history of pituitary adenoma and weight gain.

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I've got before you, Dr. Schupack,

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a Sagittal T1, non-contrast,

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an axial T2,

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and then the matching Sagittal T1 with contrast,

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which I'll scroll a little bit and allow our viewing

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audience to have a look at what we've got.

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I'll also scroll the T2 a little bit up and

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down so you can see what we've got there.

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And we do have an intermediate

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signal intensity abnormality,

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seemingly in the suprasellar region.

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And I'd like to ask you your thoughts on this case,

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since it already has a presumed diagnosis, right?

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Well,

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there is a presumed diagnosis and it's

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an important case clinically, right?

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Because as we talked about endocrine,

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there's some history that could be endocrine.

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So you give some thought to that.

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But also mass effects.

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So we have mass effect on the optic apparatus.

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So there's conceivable that at some point,

1:01

treatment, maybe surgical,

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is going to be considered, perhaps not now,

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depending on the patient's visual status,

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but it's going to be followed for that reason.

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So if you're thinking that there might be treatment,

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you've got to be pretty sure about the diagnosis.

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And this diagnosis of adenoma,

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I think I'm going to question that.

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And the reason I would say that there's a couple of

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things that we have discussed earlier on the earlier

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segments. The sella is not too big, you'd think?

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A big suprasellar mass. And also,

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I think we talked about this earlier,

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we're talking about parasellar structures.

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And so the tuberculum sellae is right here.

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And tuberculum sellae,

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remember we talked about skull-based lesions,

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meningiomas, they come in certain spots.

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They don't just show up anywhere, right?

1:48

They have certain spots.

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And the tuberculum sellae is

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a really good spot for it.

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So I think that's part of the diagnosis because you

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couldn't really work through this sella

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to get here anyway. So the question is,

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if the cella is not enlarged and you have a

2:00

suprasellar mass, is it something else?

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Well, here's another thought.

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It looks like there might even be a cleavage plane

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right there between it and the underlying

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pituitary fossa. Now,

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you can get meningioma lesions that

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arise from the tuberculum sellae,

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but you can also get them from the diaphragma sellae,

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directly from the diaphragm.

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You can also get them from the dural covering over

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the anterior clinoid processes we talked

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about in other vignettes. The big five.

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The big five,

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Kahuna Meningioma being number one when

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you get in the suprasellar region.

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But the others are meningioma, aneurysm,

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craniopharyngioma, and astrocytoma,

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a little bit different than if

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you were in the pituitary space,

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where you would be thinking about things like

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pituitary hyperplasia, hydrocephalus,

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craniopharyngioma, and then pilocytic astrocytoma.

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Which leads me to one other thought.

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You should be deciding in the audience

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if this lesion is intra or extra-axial.

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If it's intraaxial,

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you'd expect it to be coming from.

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Things like the optic chiasm right here or the

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hypothalamus or even the third ventricular region,

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but it's not. It's extra-axial.

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It's probably separate from pituitary gland.

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And it's got this sort of little point like it's

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growing flatly along the dural surface,

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almost like the dovetail sign that we see in the

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middle fossa when we have a middle fossa

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meningioma one along the petroclinoid ridge.

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Right? Now, another thing about it is you'd say,

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well, they did endocrine testing.

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Well, if that's abnormal, well,

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I could even imagine the proximity of the stalk

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if the prolactin was up a little bit.

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Now, if it's over 100,

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then you got to really think seriously about a

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secreting lesion. But let's say it's 40, 50.

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That could be extrinsic. Now, the other question is,

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since we're entertaining this

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diagnosis of meningioma,

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is there anything else we could marshal in support

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of that? One is the patient's a female.

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Let me make that a little bigger for you so

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everyone can see it. So the patient's a female,

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so they get meningiomas.

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They have hormone receptors,

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but also there's another meningioma.

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Okay, so the weight of the evidence,

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we're starting to get some support for that idea.

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And that's really important because they decided

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this was an adenoma and they're going to treat it

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at some point. Transphenoidal, wrong way to go.

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Right. The lesion,

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you're not going to be able to get to it.

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The lesion is not from there.

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That would be a mistake.

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Okay,

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so really critical differentiation

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to make for the clinician.

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And it turns out the prior diagnosis of pituitary

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adenoma was made by another radiologist at another

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institution. It wasn't pathologically proven,

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so it could lead you down the wrong path.

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Of course,

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you can get multiple meningiomas

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as part of a phakomatosis,

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either meningiomatosis or neurofibromatosis

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type two that wasn't present here.

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And then if we go back to the T two,

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just a few other takeaways to help support

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your diagnosis. Yes, it's true.

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Macroadenomas look like gray matter,

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but meningiomas look pretty close to gray matter,

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too.

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They can even be a little bit darker than

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gray matter. They're usually firm.

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You don't get a lot of cyst

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production in meningiomas.

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You do in suprasellar lesions like craniopharyngiomas.

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You can get them in macroadenomas,

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occasionally get some microcysts, and of course,

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meningiomas will calcify.

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That may be hard to see on MR, easier on CT,

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and they may produce a dural or skeletal reaction,

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which is not the case with a suprasellar

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craniopharyngioma or macroadenoma.

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So this was misdiagnosed by someone else.

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They missed this separation.

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They miss this linear growth pattern along

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the dura in the tuberculum sellae.

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This is suprasellar meningioma.

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Should we move on and do another one?

5:37

Yes, let's do it.

Report

Description

Faculty

Stephen J Pomeranz, MD

Chief Medical Officer, ProScan Imaging. Founder, MRI Online

ProScan Imaging

Tags

Sella

Neuroradiology

Neoplastic

MRI

Head and Neck

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