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2 Patients with Cholangiocarcinoma

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So far we've spent quite a bit of time

0:02

talking about hepatocellular carcinomas

0:05

and LI-RADS, and I think that's appropriate.

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Because when you look at primary malignant

0:09

liver lesions, the vast majority of

0:12

them will be hepatocellular carcinomas.

0:15

Over the next case and the last few cases,

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I want to shift gears to talk about a

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few other malignant lesions that you can

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see in the liver, one of which is common,

0:25

while the other group are very, very

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common and arguably even more common.

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than hepatocellular carcinomas.

0:33

So we'll go on to these images.

0:34

We have two patients with the same diagnosis,

0:37

um, and we'll talk a little bit about

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diagnoses once I describe the findings.

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So neither of these patients has

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history of cirrhosis or chronic liver

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disease, but they have liver masses.

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First patient has a mass in the hepatic lobe.

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I'm just going to scroll through

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it to start with and then show

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you some sample snapshots of it.

0:57

So this is a T2-weighted image with fat

1:00

saturation, and we can see in the lateral left

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hepatic lobe, the signal is hyperintense,

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T2 hyperintense. This portion of the liver is

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abnormal, while the remaining portion of the

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liver over here has a relatively normal signal.

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And if we look with a very discerning eye, we

1:21

can see that amidst this area of abnormality,

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there are some bright tubular structures, and these

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are going to turn out to be dilated bile ducts.

1:29

So let's see what this looks like

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on our in and out-of-phase images.

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Here we have the T1 out-of-phase image.

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Here we have the T1 in-phase image.

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And if we actually look at the

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liver that's not diseased, i.e.,

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most of the right hepatic lobe,

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we can see that it actually loses signal

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on the out-of-phase image when you

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compare it to the in-phase image.

1:51

And both of these, of course,

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are being compared to the spleen over here.

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So it becomes as dark as the spleen,

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if not darker, on the out-of-phase

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image, while on the in-phase image

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it appears brighter than the spleen.

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So that tells us that a lot

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of this liver is steatotic.

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And as a result of that, it can trick

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our eye into thinking that maybe the

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out-of-phase and in-phase appearance

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of this lesion as well looks different.

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But if you actually look at it and measure

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region of interest over it, you'll see

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that the signal actually doesn't change

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between the out-of-phase and in-phase.

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It remains T1 hypointense, and this lesion

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does not contain any lipid within it.

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If we go to our T1 Fatsat pre-contrast

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images, again we can look at this lesion

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that's essentially replacing the lateral

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left hepatic lobe, and this has T1 hypointense

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signal before giving contrast.

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And after we have contrast,

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observe the enhancement pattern

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that we see with this lesion.

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So here we have a T1 fat-saturated

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post-contrast image.

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We've done this in the arterial phase,

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we have a portal venous phase here,

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and here's our equilibrium phase.

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Here's the lesion on each of these phases.

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And so far, when we've looked at lesions,

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and we've sort of classified them as

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hepatocellular carcinomas, we've looked for

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areas of arterial phase hyperenhancement.

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But if we look at this lesion, certainly, on the

3:14

arterial phase, there is enhancement within it.

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There is also enhancement on the

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portal venous phase, and there is also

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enhancement on the equilibrium phase.

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And if you sort of look at the way this is

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enhancing, it enhances more, or the most, on

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the equilibrium phase, followed by the portal

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venous phase, followed by the arterial phase.

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And you can just look at aspects of the lesion.

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Look at this aspect.

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It enhances a little bit.

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If it gets brighter over here,

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it gets even brighter over here.

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Look at this aspect.

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It enhances a little bit.

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It gets brighter over here, it gets

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even brighter on this sequence.

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So it's sort of heterogeneously

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enhancing, and that enhancement is

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sort of filling in as we go from the

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arterial phase to the equilibrium phase.

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In other words, it's brightest in the

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equilibrium phase when compared to either

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of the two other contrast-enhanced phases.

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The other thing to look for in this patient

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is, you know, I mentioned this patient does not

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have a history of cirrhosis, should not have,

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therefore, a nodule or liver contour, and yet.

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If we look at aspects of the liver

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contour, certainly along the right

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aspect, it looks pretty smooth.

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And most of the liver that's not diseased looks

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pretty smooth, but look what happens here.

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Diseased liver has capsular

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retraction associated with it.

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Tumor has a desmoplastic response, a fibrotic

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response that's pulling the liver towards it.

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You can see it over here as well.

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So that's our first patient.

4:31

I want you to show you the second patient

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and we'll sort of summarize the findings and

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talk a little bit about what this lesion is.

4:36

Okay.

4:36

Thank you.

4:37

So this is our second patient, no history

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of cirrhosis, has a liver lesion that

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is certainly involving the medial aspect

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of the left hepatic lobe and involving

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probably segment 5 over here as well.

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We can see this lesion.

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This is on our T2-weighted sequence.

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It has hyperintense signal

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on the T2-weighted images.

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It's not fluid bright, but certainly

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looks intermediate signal, um, and very

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similar to the spleen, if anything.

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If you look at the border of the liver, it

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looks very, very smooth here, and if you

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go down, there is this capsular retraction,

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again, seen associated with this lesion.

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I'm not going to show you

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the in and out of phase.

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This lesion did not contain fat.

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But what I will show you is

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the post contrast images.

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And in the post contrast images, we

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see a pattern that is very similar

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to the case that we just saw.

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So this is T1 Fatsat, post contrast

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arterial phase, portal venous phase.

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Equilibrium phase, and we can see that

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there is a very heterogeneous enhancement,

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and the brightest amount of enhancement

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is seen in the equilibrium phase.

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See how much this area fills

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in as compared to this.

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So if we were to summarize this, uh, lesion,

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either lesion that we've seen in either

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of these, uh, two cases, we certainly

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have, you know, a variably sized lesion.

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It has intermediate to hyperintense T2 signal.

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There is no fat within this lesion.

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It is associated with capsular retraction.

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When we give contrast, it has sort of centripetal

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enhancement that's most on the delayed images.

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Also, in the first case that I showed you, it

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was associated with biliary ductal dilatation.

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So when we see these findings, it is quite

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characteristic of cholangiocarcinoma.

6:25

Thank you.

6:25

Now cholangiocarcinoma sort of comes

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in different flavors and we can, uh,

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qualify it by describing its location.

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So if we draw sort of a, a liver, mini

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liver over here, and these are the

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bile ducts, cholangiocarcinomas can be

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seen in the extrahepatic biliary tree,

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so over here, so that's extrahepatic.

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Oftentimes they're seen at the bifurcation

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of the right and left bile ducts over

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here, so that's what we call perihilar.

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Tumors, also known as Klatskin tumors,

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or they can be sort of intraductal.

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And these are also known as

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peripheral cholangiocarcinomas.

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Intraductal peripheral cholangiocarcinoma,

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which is just what this is.

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And these tumors can also look

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in a variety of different ways.

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The cases that I presented here are

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mass-forming in their shape, but they

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can also be quite infiltrative and

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just form along the ducts themselves.

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Or they can manifest as polypoid

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masses inside the ducts.

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But often times we see them when

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they're intraductal or peripherally

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located, we see them as mass-forming.

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And the key finding is that they have this

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capsular retraction, they're desmoplastic

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tumors, and this, uh, centripetal enhancement,

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and most evident on delayed phase images.

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And if we are suspecting a

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cholangiocarcinoma, we often do ten

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minute delayed post-contrast images.

7:50

Thank you very much.

7:51

Because that's when the

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enhancement will be most apparent.

Report

Faculty

Mahan Mathur, MD

Associate Professor, Division of Body Imaging; Vice Chair of Education, Dept of Radiology and Biomedical Imaging

Yale School of Medicine

Tags

Neoplastic

MRI

Liver

Gastrointestinal (GI)

Body

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