Imaging Response Patterns in the Modern Era of Cancer Treatment, Dr. Lacey J. McIntosh (11-16-22)
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Today we are on our to welcome Dr. Lacey McIntosh
0:46
for a lecture on Imaging response patterns in
0:49
the modern era of cancer treatment, Dr. McIntosh currently
0:52
serves as the chief of the oncologic and
0:55
molecular Imaging division of the University of Massachusetts Medical
0:58
School.
1:00
She completed her Radiology residency at the University of Massachusetts Medical
1:03
School and a fellowship in cancer Imaging with
1:06
a focus on PET CT at Dana Farber,
1:09
Kansas cancer institute at Women's Hospital in
1:12
Boston.
1:14
Her interests are in clinical trial tumor assessment criteria Precision
1:17
oncology and novel PET
1:20
CT tracers at the end of the lecture join Dr.
1:23
McIntosh in a Q&A session where she will address questions
1:26
you may have on today's topic.
1:28
Please remember to use the Q&A feature to submit your
1:31
questions so we can get to as many as we can before our time is up
1:34
with that being said we are ready to begin. Today's
1:37
lecture Dr. McIntosh. Please take it from
1:40
here.
1:41
Hi everyone. Thank you for having me today and thank you
1:44
for registering for the conference very excited
1:47
to give this today and kind of
1:50
give some some of my perspective on how we
1:53
need to think about cancer Imaging, you know,
1:56
in today's modern era of kind of
1:59
new and exciting treatments. So that's what
2:02
we'll be talking about today.
2:07
It's just some disclosures. I do some clinical trial reading
2:10
and Consulting.
2:12
An outline of what we're going to cover today. We're going
2:15
to talk about Imaging assessment in general kind
2:18
of specifically looking at different response
2:21
criteria. You know how these
2:24
were created how these are used limitations and
2:27
using certain criteria and how
2:30
they've kind of changed over time. We're going
2:33
to review classes of drugs and have these
2:36
can result in different response patterns. We're
2:39
going to look at pitfalls and challenges associated
2:42
with you know, some of
2:45
the response criteria and some of
2:48
the newer treatments and then also talk a little bit about clinical
2:51
context.
2:54
So what I can say to start with imaging assessment
2:57
is that you know, what we
3:00
do in clinical trials is really kind of Highly regulated
3:03
and very specific which is
3:06
not necessarily equivalent to what we're doing in routine clinical
3:09
practice every day at the workstation, you know
3:12
in the clinical trial session setting it's
3:15
very specialized. We have Central readers who are all kind
3:18
of reading the same patients throughout the clinical trial blinded
3:21
to clinical data. We're prospectively
3:24
selecting Target lesions, and
3:27
we're kind of comparing them throughout the course of treatment to look
3:30
at how things have changed since the Baseline and
3:33
the nature which is where things look the best that kind
3:37
of assessment can be challenging in routine
3:40
clinical practice where you guys all
3:43
know as you know, either residents or practicing Radiologists that
3:46
we have lots of challenges where the baseline
3:49
or serial exams or not always available, especially if
3:53
you're working.
3:54
Kind of a larger Center where patients are sent to you, you know,
3:58
we are combining our objective measurements of
4:01
lesions and kind of subject assessment, you
4:04
know, we integrate clinical data into
4:08
our assessments tumor markers how
4:11
the patient's doing overall a lot
4:14
of times the information that we're trying to provide especially at
4:17
staging has to do with you know tnm staging
4:20
so, you know a t staging
4:23
of a lesion which is giving the largest measurement in any
4:26
Dimension maybe different than how we're
4:29
using recessed or clinical trial assessment, you
4:32
know an attractable way. So yeah,
4:36
these are not necessarily equivalent, but I think it's very important
4:39
to kind of understand how the
4:42
clinical trials are run and look at the different response assessment
4:45
criteria so that you can apply those principles into
4:48
your routine clinical practice and you know
4:51
kind of use the concepts as
4:54
you can in the setting that you have.
4:56
So I do want to share this resource. I have this as one of my home
4:59
pages that opens up anytime. I open up my browser, but
5:02
it's the cancer.gov NCI drug
5:06
dictionary and this is wonderful. You can type in any
5:09
drug you can use the the generic or the trade name
5:12
and it will pop up with just a short
5:15
paragraph on the mechanism of action and you know,
5:18
there's new drugs that come out all the time. So I use this
5:21
frequently to kind of understand what kind of drugs patients
5:24
are on because that can be really helpful in determining what
5:28
you expect to see for response patterns, which may
5:31
be atypical with some of these newer treatments.
5:35
So a big part of you know,
5:38
I think accurately staging or restaging
5:41
patients is knowing what to expect.
5:44
Right? So for patients
5:47
who are on traditional chemotherapies full of
5:50
fox anything Platinum based, you know,
5:53
the things that have been around for a long time when you
5:56
think about the mechanism of these drugs, these are
5:59
really cytotoxic and they're designed to kill cancer cells
6:02
are actually any kind of rapidly metabolizing cell,
6:05
which is why patients often lose their hair because hair
6:08
follicles cells are you know, regenerative frequently
6:11
turning over same thing
6:14
with sometimes in the skin and the bowel. So those
6:18
kind of you know are explaining the toxicity
6:21
is a little bit with targeted therapies,
6:24
which will go into more depth about,
6:27
you know, examples of these but these drugs
6:30
tend to be more cytostatic where they are designed
6:33
to actually help.
6:35
Cancer cell growth so, you know, they're inhibiting angiogenesis
6:38
or stopping the cell
6:41
cycle to inhibit proliferation things
6:44
like that. So, you know
6:47
for these assessment.
6:49
Criteria, you are not
6:52
necessarily looking for dramatic changes in size.
6:55
So we'll talk about that more but you know
6:58
and for you know therapy there's a couple
7:01
of different types passive inactive or the the way that
7:04
I like to category categorize these but when
7:07
you think about the mechanisms of
7:10
how these act you can kind of imagine how these might
7:13
manifest differently when the cancers are
7:16
responding to them. So in general for like
7:19
an outline, I like to think about, you know, when you're thinking about
7:22
traditional chemotherapy and these cytotoxic
7:25
treatments recess which is a size based
7:28
criteria, which we'll talk about in a second is you know,
7:31
the one that you're going to want to use here for the targeted
7:34
therapies, since you know size may not always
7:37
capture all of the response. There's
7:40
some other criteria like choice or mask that
7:43
we're gonna think about and you know
7:46
with immunotherapy we are all we're gonna be thinking about
7:49
all
7:49
Of these plus, you know some immune related response
7:52
criteria. So we're going to talk about all these in-depth but
7:55
you know, just an overview I think
7:58
you know, it's good to know what drugs patients are
8:01
on because then you kind of know what to expect. How should patients
8:04
be responding. How should their tumors be changing on
8:07
Imaging?
8:08
So I mentioned a couple but these
8:11
are kind of your traditional chemotherapy agents.
8:15
you know, you can see there's like tons of different examples
8:18
here and how they act, you know
8:21
on different portions of like the cell or
8:24
the cell cycle, but the overall
8:27
you know, I think for Radiologists what's really important to know is
8:30
that these are cytotoxic and so these are designed
8:33
to kill cancer cells. Everything should get
8:36
smaller.
8:37
For targeted chemotherapy. This is
8:41
a little bit different you can see there's all you know variety of different
8:44
targets that we can design drugs for whether it's
8:47
you know, an endothelial growth factor
8:50
inhibitor or you know
8:53
parp Inhibitors. All of these drugs that
8:56
have Target these different regulations systems for
8:59
for cancer. And so I think
9:02
about these more as psychostatic and
9:05
so, you know size measuring size
9:08
alone is not always going to give you all the information that
9:11
you need.
9:13
Um, so one good hint that I like to you know,
9:16
give is that if anything ends in an IB,
9:19
you know synonyms seraphinib
9:22
imaginib. Those
9:25
are some common ones. Those are usually going to be in this targeted category
9:28
and they're usually tyrosine kinase
9:31
Inhibitors. So you can see again just
9:34
exhaustive list of all these different drugs for all
9:37
of these different targets that really the end goal is to
9:40
kind of slow down or stop cell proliferation and
9:43
angiogenesis.
9:45
So one thing that comes up with these is resistance
9:48
these drugs tend to work very
9:51
well at the beginning and then patients, you know can develop
9:54
resistance after a certain number of you know,
9:58
treatments or time on treatment and you
10:01
know, that may be due to mutations and drugs have
10:04
to get changed. But again kind of knowing just
10:07
broadly about how these drugs work
10:10
and what they should look like when they're being used.
10:14
So for Passive cancer immunotherapies, so
10:17
these terms are targeted but they're not the tyrosine kinase
10:20
Inhibitors. So really what we're talking about here is
10:23
kind of immune mediated but not actual T
10:26
Cell killings. So some good examples are
10:29
like bedesses you have which is avastin as
10:32
the trade name, which is a monoclonal antibody to to veg
10:35
F and then trust who's a
10:38
map is another one that's antique her two and retucks. The
10:41
map is commonly used philipomo, which is against the Monopoly antibody
10:45
against the cd-20 antigen. So these are going
10:48
to inhibit cancer cell growth by blocking receptor
10:51
sites and signaling proteins, and they basically
10:54
induce death by tagging these cancer cells
10:57
for removal by the immune system.
11:00
So I make this these distinctions between passive
11:03
and active cancer immunotherapy. This
11:06
is kind of the ones we just talked about here. And then you know,
11:10
the active is more T cell
11:13
mediated killing of the actual tumor cells. So
11:16
this is where we give drugs that
11:19
allow the immune system to actually recognize and kill
11:22
cancer cells. Usually we're
11:25
doing this by turning off mechanisms that cancer cells use
11:28
to evade detection and kind
11:31
of slow down the immune response. So I
11:34
love this graphic. I think it's really nice and clear
11:37
and explains kind of how these drugs work. So if
11:40
we're using the pd1 or PDL one
11:43
pathway, this is programmed death
11:46
is what PD stands for but normally what
11:49
we have is here's our tumor cell. Here's
11:52
our T cell and this interaction here between
11:55
the blue parts are is the pd1 and the
11:58
PDL one and basically this is
12:00
adaptive mechanism that the tumor cell has that's able to
12:03
shut off the T-cell it, you know, once this binding
12:06
occurs, it kind of makes the tumor cell invisible to the
12:09
T cell and it can just kind of go along doing, you know,
12:12
go along and its business doing whatever it wants when we
12:15
give patients these, you
12:18
know immune checkpoint inhibitor drugs, which are either targeted to
12:21
the PDL one or the pd1 side.
12:24
We block this this
12:27
Binding from occurring and we
12:30
allow the T Cell to see the tumor the
12:33
tumor cell and kill it as well. There's a
12:36
kind of a similar mechanism that happens over here
12:39
the graphic on the right between the Androgen presenting
12:42
cell and the T Cell
12:45
which allows it to kind of present it and so
12:48
similarly when we give these drugs. We not only enable The
12:51
Killing but we also enable the antigen presentation
12:54
which you know enhances the T Cell response.
12:57
So that's probably didn't expect this from a
13:00
radiology lecture, but it's really interesting and it's it's good
13:03
to know about because it helps you understand what you're
13:06
seeing on the Imaging and why it may be atypical.
13:10
Um, so in addition to the pd1 pdl1 pathway
13:13
ctla 4 is another pathway that
13:16
ax very similarly. If you block this interaction, you're
13:19
able to allow T cells to
13:22
kill tumor and also enhances the
13:25
antigen presentation.
13:29
So one of the side effects of this active cancer
13:32
immunotherapy is that we can get unwanted activation
13:35
of the immune system. And so there
13:38
can be a wide range of toxic effects. So it's just something
13:41
to kind of be aware of that. You don't want to mistake these findings for
13:44
progression.
13:46
So moving on to you know kind of an overview
13:49
of the different cancer response criteria. So these
13:52
are used when a patient has started out chemotherapy, you
13:55
know, whatever class we just talked about.
13:58
To be assessed at Baseline and then
14:01
at interval follow-ups and these may be
14:04
different depending on which clinical trial in clinical
14:07
practice patients are usually imaged every three months or
14:10
three to six months and you know that may space out
14:13
the longer out. They are from their diagnosis and depending on
14:16
what kind of treatment they've had. So generally they're
14:19
kind of classified. If you look in this left-hand column into
14:22
different response categories. So CR stands
14:25
for complete response PR stands for
14:28
partial response SD is stable disease and
14:31
PD is Progressive disease so you
14:34
can see these are just kind of a group of examples
14:37
recess one point
14:40
one is kind of the the new version
14:43
of the newest version of recessed and that's one of
14:46
the you know more commonly used response assessment
14:49
criteria, but if you look down the column and
14:52
you see, you know, kind of where how these descriptions
14:55
are, they're really only focused on size, right?
14:58
So a complete response would be a
15:01
disappearance of all lesions a partial response would be a 30%
15:04
decrease in the sum of longest Dimension and we'll
15:07
talk about kind of how this is done in a second.
15:10
Skip down to Progressive disease which
15:13
is a 20% or more increase in the sum of the
15:16
longest Dimensions or any new lesions and then
15:19
stable disease is kind of in between these two. So if
15:22
you are not meeting parcel response
15:26
and you're not meeting Progressive disease, so I think this is
15:29
kind of important to look at this distinction because you
15:32
may have like a little bit of response or
15:35
you may have a little bit of increase in size. But as long
15:38
as you're not meeting, you know that criteria of progression,
15:41
you know, that's actually considered stable.
15:44
So that's a point. I like to you know,
15:48
kind of highlight in terms of terminology. It's something
15:51
that I see where sometimes residents
15:54
or other Radiologists May document a
15:57
very slight increase in size of a finding, you know,
16:00
even in just you know millimeters, but if they put
16:03
in their impression like, you know progression of disease
16:06
that is actually not necessarily the right
16:09
use of that term
16:11
Um a more accurate or kind of better way to
16:14
describe that might be like a mild or a minimal increase
16:17
in size of you know, a particular finding or
16:20
very slight increase in tumor burden or things like
16:23
that. But I tend not to use the word progression unless it's
16:26
actually meeting this criteria, um,
16:29
you know, if there's new lesions or if there's actually like a 20% or
16:32
greater increase, so unless you're actually gonna like do that calculation or
16:35
it's very obvious. You need to be kind of careful about
16:38
your terminology.
16:40
So we kind of touched on recess, but you can see Choi which
16:43
we'll talk about a little bit talks about
16:46
size. But it also talks about attenuation revise Joy
16:50
very similar and then Mass criteria
16:53
also looks at attenuation immune response
16:57
criteria has some different thresholds and then has
17:00
some requirements for follow-up for confirmation, but
17:03
there's a lot of information on this slide, so don't
17:06
worry about about this. We're going to go through all of these things
17:09
together.
17:10
Um, there can be some types of diseases that
17:13
are very difficult to quantify, you know,
17:17
for instance peritoneal carcinomatosis. So
17:20
for a lot of these GYN or peritoneal base
17:23
tumors or you know, gi gi cancers
17:26
that have disseminated to the peritoneum. You can
17:29
imagine that when you have like military
17:32
Or sheet, like disease that it's very difficult to
17:35
measure that right and it's difficult to measure it in a reproducible
17:38
way. So there's some other
17:41
response assessment, you know such as the peritoneal cancer
17:44
index which is more kind of it's a way
17:47
to try and quantify this unquantifiable disease.
17:50
So you give scoring based
17:53
on how much tumor you see and where you see
17:56
it the whole, you know, the abdomen and pelvis or divided up into these segments,
17:59
so
18:01
Um, so recess 1.1 has evolved from
18:04
The Who criteria and then recess 1.0
18:07
which we don't really need to learn much about these because they're
18:10
not used anymore. But basically if you have measurable
18:13
disease you have to have at least one centimeter of
18:16
disease on CT and a non-notal lesion.
18:19
If your disease is within lymph nodes
18:22
and the they have to be a little bit bigger where
18:25
the short axis has to be at least 15 millimeters
18:28
to be considered a Target lesion, or at least
18:31
10 millimeters to 15 millimeters to be considered a non-target
18:34
lesion, and then we kind of
18:37
already talked about what the definition of progressive disease was, which
18:40
is you know, 20% is kind of the the threshold
18:43
there. So the way that we do this is we basically
18:46
look at a baseline exam and we can select up
18:49
to five lesions. You can have up to two in
18:52
any single organ and then you
18:55
basically just measure them in one dimension
18:58
and then you add all of those up.
19:01
And you come up with a number and then that number is kind of
19:04
calculated at each visit and you look at the differences and that's how
19:07
you classify patients into their different response assessment categories.
19:10
So
19:12
we kind of all disease needs to be documented. And
19:15
so, you know, you fill up your target slots,
19:18
you're up to five lesions and then everything else in excess
19:21
of that or that's not really measurable kind
19:24
of falls into this non-target lesion definition. So it's
19:27
kind of like you're following things and attractable measurable
19:30
way with the targets. And then with the non
19:33
targets is a little bit more qualitative where you're you know,
19:37
things like plural effusions or sides or peritoneal disease,
19:40
you're giving a little bit more of a subjective kind of
19:43
a little bit more leeway and determining is this
19:46
better. Is this worse? Is it about the same because it's
19:49
hard to measure right. So yeah,
19:52
that's pretty much it. I think we've
19:55
kind of reviewed all this stuff. So here's an example finally some
19:58
Radiology, right finally some Imaging. So this
20:01
is a patient who has colon cancer
20:05
with metastasis to the liver. And so these two top
20:08
images A and B are measured at the Baseline
20:11
so you can see you have
20:12
Two dominant lesions here. You're only allowed up
20:15
to to two per organ. And so if you take
20:18
4.6 centimeters, which is the longest access measurement.
20:22
Here and add it to your 5.4. Then
20:25
you get a 10 centimeters is
20:28
your sum of diameters at the Baseline so
20:31
images C. And I guess
20:34
also see it should be our measuring
20:38
3.3 centimeters and 2.7 centimeters. So
20:41
when we add those up we get six centimeters. So
20:44
how we would classify this using resist is
20:47
that we've had a you know greater than 30%
20:50
decrease in the sum of diameters. We have 40% here
20:53
that this would be a partial
20:56
response. So when when
20:59
your drug Works in a way
21:02
that lesions should decrease in size, this is a really really
21:05
good way to kind of classify how patients
21:08
have responded.
21:12
So limitations, we've touched on some of these already a
21:15
little bit. So non-measurable disease, we've all seen this
21:18
like peritoneal like taking or you
21:21
know, just kind of the linear like blanketing of
21:25
disease throughout the omentum and that's really hard to measure even
21:28
if you can measure it on one exam or you're going to be able to
21:31
measure it the same way on the next exam because you know,
21:34
it's kind of a mobile organ. It can be it can be really challenging. And so
21:37
when you are trying to designate a Target
21:40
lesion or something that's you know to be tracked over
21:43
a series of images or a series of time points, you
21:46
know, peritoneal disease may not be a good candidate for
21:49
that mesothelioma similar
21:52
thing. This doesn't grow in a spherical or mask
21:55
like fashion this kind of grows in
21:58
a more grind like morphology. And so, you know
22:02
when it's growing in that circumferential pattern, it's
22:05
how do you put a longest access measurement on this?
22:08
So we have some modifications where for musicalioma we
22:11
pick
22:12
Couple of places and we measure the width of it instead, but
22:15
that's another topic from today. But
22:18
some other limitations anybody who's read
22:21
lymphoma cases, you know that even when disease
22:24
has totally responded you can have residual soft tissue
22:27
or masses that persist after therapy. And if
22:30
you're using CT alone, it can be really hard to tell you know
22:34
has my patients disease gone away. I still
22:37
see lymph nodes are not as big as they used to be. Are they
22:40
still active cancer or is this treated disease which is
22:43
why pet, you know is really so important in lymphoma because you
22:47
can actually, you know, you kind of incorporate the
22:50
metabolic response as well as the
22:53
as well as the anatomic response.
22:56
So for targeted therapy, like we talked about this is you know
22:59
kind of accent a site of static way. And so really what's
23:02
happening at the cellular level is we are
23:05
stopping cell growth, right? And so if
23:08
we don't appreciate huge changes in size
23:11
in our tumors are we really capturing the
23:14
response that's going on there. We need to look
23:17
at more than size here.
23:19
So for things like just carcinomas other
23:22
soft tissues sarcomas, you know,
23:25
so certain tumors, but also, you know certain therapies. We really need
23:28
to look at density and kind of the inner character of the tumor.
23:32
Um, some drugs can cause an intraumeral Hemorrhage, you
23:35
know, which is actually part of the treatment
23:38
response and you can imagine that might cause some swelling
23:41
or growth of tumor that if
23:44
you're only looking at size you're going to miss classify that
23:47
you know as possibly an increase in
23:50
tumor burden or even progression if it's significant enough.
23:53
When we have long lesions
23:56
that respond showing cavitation, if
23:59
you're measuring the outer margin of
24:02
these lung lesions, it's probably not going
24:05
to significantly change overall, but you may have cavitation
24:08
and if you're using size only resist-based
24:11
measurements, you're not going to capture
24:14
that response, right? And then immunotherapy is
24:17
it's has its own sets of challenges, which we're really
24:20
kind of dive into later. So here's an example. This is
24:23
a patient metastatic colon cancer.
24:25
Sir, and says you mad or trade name is
24:28
avastin and this is the monoclonal antibody to vegf. So it's
24:31
very classic that you see cavitation in
24:34
response to this drug. But you know,
24:37
if you're looking at this knowledgeable and you measure this as seven
24:40
millimeters and then on your six week follow-up and measures one
24:43
point five you if you're only looking at size,
24:46
right you're gonna classify this as progression. This thing is
24:49
more than doubled in size. But in fact, this is a response.
24:52
So this is showing that recessed and
24:55
size based only is not always, you know, the right
24:58
thing to choose or not always reflective of
25:01
what's actually going on.
25:04
So this is particularly important for gist, you
25:07
know metastatic just to the
25:10
liver and if they've never been on any sort of tki and that
25:13
live it's very classic for these to have a mixoid
25:16
degeneration Hemorrhage necrosis as part of
25:19
their response patterns. And so while you may
25:22
not see significant changes in size or you may actually even see increase
25:25
in size you can you usually appreciate a
25:28
dramatic drop in density. Sometimes you
25:31
have lesions that like kind of up here
25:34
or become more well seen
25:37
and this may be due to
25:40
the fact that they were actually kind of a cult on the previous Imaging and
25:43
now you're seeing them because they're in a product. So this
25:46
is something important to be aware of because you don't want to misinterpret these
25:49
for Progressive disease whether you're calling an increase
25:52
and size of something that's existing or actual new
25:55
lesions. So if it's not
25:58
clear what's going on, which sometimes it's not special with like Hemorrhage
26:01
PET CT is another tool you
26:04
Use to kind of help figure out what's going on.
26:07
So here's a nice example, you know, we have
26:10
Baseline Imaging here up in
26:13
the top left and we've got a lesion that's 2.8
26:16
centimeters and illusion that is 1.7 centimeters. So
26:19
we add these up and this is 4.5. When we
26:22
look on the post treatment first follow-up time
26:25
Point. These lesions have gotten bigger right 3.9 centimeters
26:28
and 2.9 centimeters. So when we
26:32
add these up 6.8 we have a more than 50% or a
26:35
50% increase here. And so if we're using size
26:38
alone, you know, we would
26:41
we would say this drug isn't working. Right? This is like the cancer
26:44
is growing through the drug. That's what we mean when we say
26:47
progression.
26:48
Um, but when we look at these, you know,
26:51
Mr. Images of these same lesions, we can see that
26:54
these are T1 bright, you know
26:57
not having enhancement in these areas that this
27:00
is actually just intertumeral hemorage and we go
27:03
back and look at the CT if you can appreciate this area is so
27:06
much less dense than it was here. So what we're
27:09
seeing on the Baseline is like enhancing solid tissue. It
27:12
happens to be less enhancing than surrounding liver. This
27:15
is enhancing tissue on the follow-up that
27:18
we we actually have pockets of like not enhancing tissue, which
27:21
we know from the MR is into tubal Hemorrhage and so
27:24
the amount of actual like persistent enhancing
27:27
tissue is much less than it
27:30
was on the Baseline. So this is actually an excellent response to therapy.
27:34
Hugs, so this is an example of you know, how size
27:37
alone is not enough to characterize what's going on,
27:40
especially with certain tumors and especially with certain
27:43
drugs.
27:44
So as a result, you know
27:47
this criteria called the toy criteria was created. It's
27:50
been modified. But you know,
27:53
you can see that the definitions of how you classify a
27:56
patient's response or a little bit different right? So this
27:59
decrease in size of 10% So this is a
28:02
low earth threshold that was what was required for recess which
28:05
was 30% or a decrease
28:08
in tumor attenuation by 15% or
28:11
greater. And so
28:15
You know, we're looking at more than just partial response
28:18
which I mean sorry more than just size
28:21
which is really important. We also obviously have to have no new
28:24
lesions and no obvious progression of non-measurable disease. So
28:27
stable disease will
28:30
kind of skip because that basically is just something that doesn't fit PR or
28:33
PT, but for PD you have to have a size increase of
28:36
10% but all so it's
28:39
not, you know changing in attenuation that would
28:42
classify it as a PR. The other thing that
28:45
Joy highlights is these new intraumeral nodules or
28:48
increase in size that existing inch or
28:51
two moral nodules. You can imagine if you're looking at a very heterogeneous
28:54
lesion that has intraumeral nodules, you
28:57
know, if you've given overall size you're not
29:00
really going to be class.
29:02
Specifying these so here's an example of this where this patient
29:05
had been treated for metastatic gist and
29:08
their lesions were like very low density almost kind of like liquid
29:11
fluid looking and on a follow-up, you know,
29:14
the overall illusion definitely hasn't increased in size
29:17
is measuring exactly the same but we have these new
29:20
kind of enhancing soft tissue nodules
29:23
within the tumor. They're usually along the wall, you
29:26
know, that's where they tend to occur but
29:29
really important to look for these when you're reading follow-ups
29:32
on you know, patients with treated
29:35
disease or you know to follow these if patient
29:38
has these at the Baseline
29:40
So you can see a follow-up was done in these it
29:43
definitely all increase in size. And you know, if you're using
29:46
size assessment alone of the entire lesion, you
29:49
are going to miss all of this, right but when you're looking at
29:52
the character of the lesion, there's definitely progression and
29:55
increase in tumor burden here a pet
29:58
was done here which, you know kind of confirm that this is all active disease,
30:01
but we we know that right from the morphology and the
30:04
character of what's changing.
30:06
Um, so yeah, this has been you know,
30:10
modified and revised and everything but this the
30:14
newest criteria include what we talked about with
30:17
the decrease in size and the decrease in attenuation
30:20
or sometimes these do act like they're supposed to and they
30:23
just decrease in size. So they've kind of accounted for that as well.
30:29
Um, so here's some more limitations of recess.
30:32
This is a case of metastatic renal
30:35
cell carcinoma and this patient was on serafinib, which
30:38
is a tyrosineke is inhibitor. They ID gives you
30:41
that clue so it acts on a bunch of different targets here.
30:44
But what it does is it basically induces the cell
30:47
to disassemble itself and then
30:50
be cleared from the system. So when we
30:53
look at the Baseline here, you can see there's you know,
30:56
a few to multiple lesions in the
30:59
liver. This one has a nice hyper enhancing
31:02
kind of irregular thickened rim,
31:05
and then internally, there are probably some
31:08
cystic components but there's also some hypo enhancing
31:11
soft tissue as well when we
31:14
look on the image on the right that's labeled D.
31:17
This is a follow-up exam. And when you first look at this, right
31:20
probably what stands out to you is that looks like there's more
31:23
lesions and so oh no is this patient progressing through the
31:26
treatment? Is it not working? I see more lesions when I saw
31:29
Chord, it would be easy to miss classify this as Progressive disease,
31:32
right but when you actually look at the character of
31:35
the lesions that the dominant lesion in the left lobe no
31:38
longer has that enhancing a regular Rim. If you
31:41
look at the internal density, it's almost you know
31:44
certain the almost. The entire thing is kind of this liquid
31:47
fluid density. Now, they're you know, there is still some enhancing tissue
31:50
in the middle and maybe a septation but and when
31:53
you look at these other kind of newly apparent lesions,
31:56
they all are very low density. So what this
31:59
is actually showing us is that we have
32:02
a response in the tumors that we know about and we also
32:05
have a response in lesions that we're probably previously a
32:08
call there was more disease and we could even appreciate on the previous
32:11
exam. And so this is actually really excellent response to
32:14
therapy, but you can imagine that if
32:17
you're using recess or only thinking about size that
32:20
you're you're
32:21
Not going to come to that conclusion as
32:24
easily.
32:26
So Mass criteria is one that's specifically used
32:29
with metastatic renal cell carcinoma. And
32:32
so instead of using your crpr
32:35
SD and PD categorizations. They kind
32:38
of talk about these in a different way of a favorable or
32:41
unfavorable response, but,
32:44
you know similar to Choi they're looking at
32:47
You know, they're looking at size but they're also really looking
32:50
at character and you know attenuation of
32:53
lesions. So you don't have to know any
32:56
of these in depth. I mean, it's good to be familiar with
32:59
recess 1.1 but really
33:02
my intent and talking to about these
33:05
guys is to
33:08
You know kind of understand the concepts and just being
33:11
able to apply those at the workstation.
33:15
Um, so we kind of talked about this.
33:18
And so if you're using recessed, this is just
33:21
you know results from a study showing that less than
33:24
half of medicine renal cell patients could achieve an
33:27
objective response by recessed criteria. And so you
33:30
can imagine that if you are developing new drugs for metastatic
33:33
renal cell carcinoma, and your data
33:36
is showing that less than half of your patients can
33:39
achieve an objective response. Like that's not going to look like
33:42
your drug is working very well, right? And so that's kind of
33:45
why they come up with these alternative assessment patterns
33:48
to really kind of it's important to be
33:51
able to capture response. And so
33:54
that is you know, very very key for
33:57
the development of all of these different criteria is
34:00
to kind of find the best way to capture
34:03
response. So yeah,
34:07
I mean if you are calling something stable Disease by
34:10
recessed
34:12
You know you you may not be really capturing the
34:15
clinical benefit that they're getting from the particular drug.
34:21
All right. So for immune related response criteria, um,
34:24
these thresholds are a little bit different, right? So
34:27
CR is the same disappearance of all lesions PR
34:30
this requires a 50% or more
34:33
decreased in the bi-directional measurements. So this is measured into
34:36
Dimensions where as recess. It's
34:39
just one.
34:42
It's um, and then PD is
34:45
a 25% or greater increase in by
34:48
a directional measurements. These are a little bit, you know different from what
34:51
we were staying for but when we call PD,
34:54
especially early in treatment, we because
34:57
of this phenomenon of pseudo progression, which we're
35:00
going to talk about shortly. We need reassessment on an additional
35:03
scan which can be performed. No sooner than four
35:06
weeks.
35:07
So we'll talk about student progression in a second. But
35:10
we're going to review the immune checkpoint inhibitor
35:13
response patterns. So, you know,
35:16
there's like four patterns that are kind of recognized with
35:19
these drugs. Number one is really easy because it
35:22
is you know, what you expect to see when a
35:25
patient's on chemotherapy. So we see a decrease
35:28
in tumor size no evidence of new tumors, you know
35:31
after the completion of treatment and so kind
35:34
of any criteria that you use this is going to look like a response,
35:37
right? So either it shrinks or it
35:40
goes away what we expect to see so this is an example of
35:43
metastatic melanoma patient was on it the
35:46
limit and this is Baseline and 16 months.
35:49
So there's still some residual soft tissue here, but
35:52
you know, it's definitely increased by any measure of
35:55
response assessment. We're going to call this a response.
36:00
Um, so pattern number two is where you basically just
36:03
get like long-term stability. Sometimes you
36:07
get long-term stability and then an eventual response and sometimes
36:10
you just get long-term stability, so
36:15
This is an example of metastatic melanoma also on epilepsy
36:18
lab and this is at two four and
36:21
seven months after treatment completion. So really kind of
36:24
Not changing much.
36:27
So the third pattern is one of the
36:30
phenomenon that's described as pseudoprogression. And
36:33
so what we see here is that existing tumors
36:36
appear to increase early on
36:40
in treatment and then they're followed by an eventual decrease
36:43
and sometimes you know complete disappearance. And
36:46
so there's a lot of examples of
36:49
melanoma here because that's where these drugs were kind
36:52
of first introduced and most extensively studied. So you're
36:56
gonna see a lot of examples of melanoma here, but here we have,
36:59
you know, the subcutaneous knowledge will which on baseline
37:02
or sorry this is three weeks.
37:05
Four weeks seven weeks 13 months
37:09
and twenty. Sorry. The first one is the Baseline and
37:12
then three weeks four weeks seven weeks seven months 13 months
37:15
and 26 months, but you can see between the
37:18
first and second time Point. There's a significant increase
37:21
in size of this soft tissue. And so
37:24
if you are reading this by really
37:27
any criteria, there's no significant decrease in the density.
37:30
You're going to call this progression and say, oh no, this drug
37:33
isn't working a patient's cancer is growing while they're on the drug, but
37:36
you can see by the next time Point labeled C
37:39
that there's a little bit of a decrease in size, and
37:42
I don't know if you guys can appreciate it, but there's also a
37:45
decrease in density.
37:46
And then moving down to De andf, you
37:49
can see Progressive decreased in size
37:52
of this finding to where it's like almost not even seen anymore.
37:55
And so this is really rare
37:58
this only accounts and like three to ten percent of cases. But
38:01
what we postulate this is
38:04
due to is, you know, there's two mechanisms one is
38:08
that we have true continued growth during the
38:11
time that it takes to mount an immune response, right these drugs
38:14
take time to basically train the
38:17
immune system to kill so number one is
38:20
that it's actual tumor growth, but it's it's just
38:23
because the immune system hasn't kicked in yet. The second
38:26
thought is that you get
38:29
actual immune cell infiltration into tumors and
38:32
you know with or without a team and so you're you're
38:35
tumor may be actually like under attack
38:38
and swollen and undergoing like
38:42
cell death before it starts to actually
38:45
like turn around.
38:46
So we have like histopathologic confirmation
38:49
of both of these phenomena in these settings.
38:52
So it's something that you know, you have
38:55
to definitely keep in mind if you are looking early on
38:58
there's no specific set like
39:01
time criteria of when
39:04
pseudo progression can occur, but it's
39:07
most commonly seen I think in the first 12 to
39:10
15 weeks of treatment.
39:11
So if you are reading a cancer
39:14
case on a patient who you know is using an
39:17
immune checkpoint inhibitor. It's really
39:20
important to know when was that treatment started because if
39:23
you are in that first 15, you know
39:26
12 to 15 weeks and you've seen an increase in size. You
39:29
don't want to necessarily call it progression and take
39:32
a patient off a drug that might benefit for them. What you what you
39:35
need to say in those scenarios. Are we need another time
39:38
point we need to figure out where this is headed. Is this going
39:41
to continue to increase in size or we in one of these scenarios
39:44
where it's actually going to turn the corner and start responding. So
39:47
there are case reports that
39:50
show super progression occurring out as far as like 50 weeks. So
39:53
it's really, you know, like the drugs don't they don't
39:56
read the books. They don't necessarily follow the
39:59
guidelines, but you know, it's very important
40:02
to think about early on and that's why you know
40:05
that second time point is required to
40:08
kind of give confirmation.
40:11
Um, so here's another example. We've got
40:14
a patient with metastatic breast cancer. So pretreatment. You
40:17
can see she's got this long lesion on the right which by
40:20
time point B on week 12 again. We're
40:23
really early in treatment has definitely decreased in size
40:26
like nearly doubling right and then we go back at
40:29
week 20 and this thing has nicely decreased in
40:32
size both compared to the Baseline and the interim.
40:35
So this is a really nice example of super
40:38
progression for a patient on an anti-pedial One
40:41
agent on the graphic
40:44
below. This is a sorry a liver
40:47
lesion and a patient with metastatic lung cancer and you know
40:50
the middle graphic B on treatment week
40:53
seven like this thing has exploded right and it's not
40:56
like it's just decreased intensity by any response criteria
40:59
that you use Joy recess Mass. Whatever. This looks
41:02
like an increase in tumor, which very well
41:05
may be we may be kind of in that scenario where the drug
41:08
hasn't kicked in yet and we have
41:11
tumor growth and so on week 15
41:14
we can see that this is you know declared itself in the direction
41:17
of response and it's you know, definitely decreasing in
41:20
size. So again, this is an anti-pd-1
41:23
agent but this phenomenon of
41:26
student progression can be very very confusing because it looks exactly
41:29
like progression.
41:31
So here's another one. This is again metastatic. Melanoma.
41:34
You can see Progressive increase in size over the first three.
41:39
First three images on the top and then you can see it the first
41:42
one on the bottom row on the left. We have like
41:45
a significant drop in density followed by a decrease
41:48
in size.
41:51
Here's another metastatic. Melanoma on epilemon map
41:54
and you can see these soft tissue lesions in both thighs
41:57
actually with the arrowheads and on the middle time
42:00
Point definite decrease in size and
42:03
enhancement in number of nodules that area
42:06
that was previously kind of cystic and
42:09
necrotic is now kind of filling with soft tissue and
42:12
then time Point C like gone.
42:15
So these are
42:18
just some really really nice examples from the literature of pseudo
42:22
progression.
42:24
Here's another one Hodgkin's lymphoma on pembrolizumab.
42:27
And so even though the patient
42:30
in this case met criteria for Progressive disease,
42:33
their performance status was so good that they kept them
42:36
on the drug, but you can see from the myth images
42:39
on the top that this dominant.
42:42
That lesion in the mesentery in the right of our quadrome
42:45
mesentery has like, you know progressively increased up
42:48
until cycle 4 12 weeks and then at 24 weeks
42:51
is like magically gone. It's it's really
42:54
cool. Some of the disease in the chest had kind
42:57
of you know, gotten better. If you look in the left upper lobe these
43:00
findings had had gotten a little bit better. So one
43:03
question I get from clinicians a lot from oncologists is
43:06
how do you tell the difference between progression and pseudo progression
43:09
and the short answer is that we can't we
43:12
need more time points, right? We need the follow-up confirmation to
43:15
figure out which direction it's headed but something that
43:18
always makes me really think about pseudo progression
43:21
and you know, really kind of
43:24
lean that way is if there's a mixed response,
43:27
right? So if we have some disease that is getting better.
43:30
It makes me
43:33
wonder if you know, okay is someone
43:36
is some disease responding and some just has a lot had
43:39
long enough to actually start turning around yet. So
43:42
Short answer is you can't tell but I think about
43:45
it more when I see at least some of the disease responding.
43:51
Um, so the fourth pattern is where we don't
43:54
just see an increase in size of
43:57
disease that we know about but we actually see new
44:00
lesions. So this is an example metastatic melanoma
44:03
patients on epilepsy lab so you
44:06
can see this area of subcutaneous tissue in the left hip there's nothing going
44:09
on here. But on the follow-up at time point B,
44:12
we have a new or newly apparent soft
44:15
tissue nodule which then goes away
44:18
at you know, 24 weeks. And so what this
44:21
is thought to represent is that it may
44:24
not necessarily be like a new lesion, but it's kind of
44:27
blooming or blossoming of a site of micro metastatic
44:30
disease that we just couldn't resolve on on
44:33
our original Imaging because
44:36
it was just too small.
44:39
Here's a case of metastatic lung cancer on Pembroke and
44:42
Baseline three
44:45
months. They had a you know, a clear increase in
44:48
size of this right adrenal metastasis. Um,
44:51
but, you know, we were kind of in that first three month pattern. So
44:54
we said let's give it a little bit more time and at six months the lesion
44:57
is like pretty much gone just a tiny bit of warmth left
45:00
in that lateral limb.
45:03
Here's some examples. I just wanted to show you in other organs. We've
45:06
done a lot in like the liver and the lung and the subcutaneous tissues.
45:09
But here's one of the patient with metastatic
45:12
lung cancer and on immune
45:15
checkpoint inhibition and on week 8,
45:18
they have a new lytic lesion in the right iliac bone.
45:21
So that's kind of
45:24
confusing right but we're at week eight. So we don't really
45:27
know what to make of it follow up week 17 we can
45:30
see that this thing is getting sclerotic which you know
45:33
indicates that there's an interval healing and
45:36
this thing is responding. We also have
45:39
a lymph node here in the right and the right
45:42
external iliac station, which was like totally totally
45:45
normal pretreatment resolves by
45:48
week 12. This is a patient with metastatic melanoma. And
45:51
then this one here on the bottom see I
45:54
think this is the same patient, but they had like
45:57
new lyric lesion in this lumbar vertebral body
46:00
and right transfers process which then
46:03
You know become sclerotic by week 23, so I
46:06
think you know in most cases patients aren't
46:09
being imaged this early in treatment. These are
46:12
from kind of clinical trials and early development week
46:15
eight is very early to image most people wait
46:18
three months for the first Imaging time point but sometimes
46:21
patients come into the ER sometimes they're sick
46:24
they get Imaging early for whatever reason so really
46:27
important to have this on your radar and to also
46:30
think about at that first time point of three months
46:33
when you see changes because we don't really know which way they're headed
46:36
yet.
46:37
So how do we know what's actually going on? So history
46:40
is really really important and you guys
46:43
know that's always a struggle to kind of get and
46:46
depending on how good of
46:49
a functioning electronic medical record you have
46:52
it may be easy to get or it may not but you
46:55
know things that I always want to know when I'm
46:58
reading a cancer patients Imaging who's undergoing treatment
47:01
is you know, what treatment is the patient on and then
47:04
I kind of know what response patterns I'm
47:07
expecting to see right if they're on cytotoxic treatment.
47:11
Every like traditional chemotherapy everything should get better. There's a
47:14
really no circumstance in which anything can get worse
47:17
and a response be happening.
47:20
If they're on immune checkpoint inhibitor, that's a totally different story. Right
47:23
things can look a little bit worse before they get better. Also if
47:27
I know they're on a targeted therapy or a tki I
47:30
really need to focus on the character of the tumors as
47:33
well as the size.
47:35
So how long have they been on it? You know this
47:38
is really important for the immune checkpoint of hippers. Like we talked about with
47:41
considering student progression. Um and which
47:44
comparison to use as a new Baseline. So these cancer
47:47
treatment regimens can be really complicated patients
47:50
can go through multiple lines of therapy. And
47:53
so in order to give the clinician the information
47:56
that they need you need to know. When was this new treatment started
47:59
because if you just pick a study that's like two years old that may
48:02
be from two treatments, you know regimens previously
48:05
like you need to kind of go through the medical record
48:08
figure out when was this drug started and this is
48:11
actually something to be really challenging because sometimes with insurance approval
48:14
or if a patients getting on a trial their Baseline
48:17
Imaging or what you think is their Baseline may
48:20
not actually line up when with when there's treatment
48:23
was started. And so sometimes you see changes but
48:26
you say the CT was done two months before the
48:29
patient started their treatment. I don't know if this growth that
48:32
occurred was actually prior to starting
48:34
Therapy and now disease is stable or is
48:37
it actually just growing through, you know, whatever treatment they're
48:40
on so knowing kind of where your
48:43
Imaging lines up with your treatment
48:46
is really important.
48:48
And so if you see a parent worsening of
48:51
disease while patients are on immune checkpoint Inhibitors, you
48:54
know, you really need to think about
48:57
student progression and you need follow-up Imaging
49:00
before you can really make a decision.
49:04
So yeah, just to kind of recap you
49:07
don't need to know the specifics if you know, I think it's good
49:10
to be familiar with recess because it's the most commonly when
49:13
used one but it's just
49:16
I think conceptually nice to know about these different
49:19
response assessment criteria. So size, you
49:22
know recess really only considers size
49:25
toy and mask kind of consider size and
49:28
morphology, you know and immune
49:31
response related response criteria. Think about
49:36
You know all of those things, but also, you know may require
49:39
some additional time points, especially early on.
49:42
So again, knowing what
49:45
to expect so know what drugs the patients are on and you
49:48
know kind of know which Concepts to use for looking for response.
49:53
Um, so just some pitfalls. We only have a few minutes left,
49:56
but one thing I want to point out are these sarcoid
49:59
like reactions so particularly with the
50:02
immune checkpoint Inhibitors, you can kind of you can
50:05
get this overdrive of the immune system. And
50:08
so it's very common to see things like thyroiditis colitis patients
50:11
get rashes. We don't usually appreciate those on
50:14
Imaging but pneumonitis. These are really kind of important things
50:17
and so you don't want to miss classify those as Progressive disease
50:20
and you also want the clinicians to know
50:23
because in rare cases and humanitis can be fatal patients
50:26
may be very symptomatic. So it's good to have on your
50:29
radar but I'll show you one example, we have this patient with
50:32
a left axillary melanoma and
50:35
she underwent treatment where you can see that the the
50:38
lesion went away, but she actually showed up with a right axillary
50:41
lymph node hot on pet and her follow-up exam.
50:44
So this ended up getting a biopsy and
50:47
it showed you know changes consistent with sarcoidosis
50:50
not casing illness.
50:53
Um, so she went on for her next follow-up time point and she
50:56
had kind of a more classic presentation of what we see with these
50:59
sarcoid-like reactions, which is usually kind of media style and Hyler
51:02
activated lymph nodes, but you
51:05
can see it on CT too. Obviously they get big
51:07
Here's a case of kind
51:10
of like a mild pneumonitis after this patient
51:13
had metastatic lung cancer, which was on pembrolizing lab.
51:17
So you can see these changes here in the right upper
51:20
lobe left lower lobe patient was stopped
51:23
on their therapy and
51:26
given steroids and you can see that it went away.
51:29
So really important thing to put on the clinicians radar.
51:32
They want to know kind of what it looks like how much of the long
51:35
it's involving. You can see kind of more minor changes here and here as
51:38
well.
51:40
But yeah, those are kind of important to not mistake for
51:43
for PD. So take home points know
51:46
your cancer know how it behaves we didn't talk much about that because
51:49
that's more of like a staging thing and today's really focused on
51:52
like restaging but know the treatment the class
51:55
of drug how long they've been
51:58
on it what the side effects are like be careful
52:01
about terminology, you know progression really
52:04
refers to a specific set of criteria. So
52:07
if you're if you're saying that make sure that's what it really means because
52:10
what the clinician sees when they see progression is
52:13
this drug is not working and we need to change it.
52:17
So understand limitations and size only assessment and
52:21
use all of your tools get all
52:24
the information you can out of the medical record sometimes additional
52:27
findings like, you know, tumor markers can be
52:30
really helpful to not sway you but confirm,
52:33
you know what you're thinking and then
52:37
lastly student progression is rare. You can
52:40
suggest it up front but it's only kind of confirmed retrospectively
52:43
when you have your follow-up time
52:46
points, but there are lots of patients on these drugs
52:49
every day at every hospital. So this isn't just
52:52
something you need to know how to make Center Community Hospitals use
52:55
these drugs all the time.
52:56
So that's all we have time for. Thank
52:59
you everyone for logging in and I'm
53:02
going to check out.
53:06
Let's see the Q&A box here.
53:10
So, let's see. How do you see the clinical impact of AI
53:13
on ecologic monitoring real world
53:16
application like volumetric data, not just radionomics and
53:19
academic like markers that need extensive validation.
53:24
So
53:25
yeah, I mean, I think these response assessment
53:28
criteria have been developed as a way
53:31
for us to track lesions, you know
53:34
their conventionally done in one or two
53:37
dimensions on axial slices. And this
53:40
is a you know, a difference of how things are done at the workstation
53:43
versus like, you know at a clinical trial Reading Center.
53:46
Those aren't always as necessarily as
53:49
reflective as like, you know, T stage or things
53:52
like that. So it's it's really kind of a reproducible way
53:55
to track something. And so I think AI can
53:58
definitely enhance that um, some clinical
54:01
trials do like to use volumetric assessment
54:04
and you know, they
54:07
Sometimes we'll look at recess 1.1 but then they'll
54:10
also create additional criteria to look at
54:13
and follow and see how those line up and you know, that's sometimes how
54:16
new response that response assessment are validated or
54:19
kind of created is they're done
54:22
in parallel with older older systems. So I
54:26
think you know practically the way
54:29
that we do it to be able to read lots of patients over lots
54:32
of time points is in a way that's simple but I think that
54:35
can certainly be enhanced by by AI, you
54:38
know as well as metric assessments, maybe more kind
54:41
of comprehensive and reflective then just,
54:44
you know, unilateral or by dimensional measurements which
54:47
have been designed more for practicality.
54:51
All right and suspected pseudo progression
54:54
in which time do we say next CT to
54:57
exclude City progressions? It's a great question. So I think
55:00
the guidelines tell us to not do it sooner than
55:03
four weeks because if you do it standard
55:06
four weeks, you're likely to just see the same thing and be in the same position so
55:09
I often will
55:13
say in my fall of recommendations no sooner than
55:16
four weeks, but in conversations with with clinicians,
55:19
they usually like to just give it
55:22
one more cycle of treatment. And so if they
55:25
are particularly worried about a patient
55:28
because the one thing that you have to kind of keep in
55:31
mind in addition to student progression is hyper progression,
55:34
which we didn't really talk about today, but that's like we're patients
55:37
just hyper progress on a particular drug and
55:40
you want to catch that sooner rather than later. So, you
55:43
know, if a patient is out there three months follow-up appointment
55:46
and it looks like there's you know worsening of
55:50
disease and we don't know if it's
55:51
Aggression or suited progression? Sometimes they
55:54
say I'm surprised that the Imaging looks like this because the
55:57
patient is doing great. They feel so much better. Their symptoms are
56:00
improved. They're doing more than you know,
56:03
we say well maybe this is super progression. Why don't you
56:06
give it another cycle? And so they'll actually wait like three months before they do another
56:09
scan. But if they're like, you know, the patients
56:12
deteriorating like they're not doing very well, they feel horrible. Um,
56:16
then, you know, they may image closer to like
56:19
four six or eight weeks from from that time point
56:22
so I think
56:24
You know, the the guidance is no less than four weeks,
56:27
but I think how far you go out kind of really depends
56:30
on the clinical picture of the patient, which unfortunately we
56:33
don't really usually know and that's kind of up to the clinician to
56:36
the side.
56:37
Okay, next question what might be the
56:40
clues to stop a drug or biologic therapy During the period of
56:43
time when pseudo progression is possible. Well, maybe
56:46
the clues.
56:48
To stop during the time.
56:50
Yeah, so this one we've kind of talked about that.
56:54
You know, if if you are suspecting a
56:57
hyper progression and that's not something that we suspect radiologically
57:00
we just are more objective in
57:03
that, you know things look worse things look better. Um,
57:06
but you know, if I get the clinical information not a
57:09
patient is like doing very poorly then, you
57:12
know, then I think more about hyper progression
57:15
and that's really when the drug should be stopped. You know,
57:19
and it sometimes it can be hard to tell like are they having
57:22
are they doing poorly because their disease
57:25
is continuing to grow and they are hyper progressing
57:28
and their cancer is making them
57:31
feel poorly or are they feeling poorly
57:34
because they're having toxicities and side effects from the drugs
57:37
and one interesting point.
57:40
Is that patients who develop these
57:43
toxicities they actually tend to respond. And
57:46
so if you see somebody that's developing thyroiditis
57:49
or pneumonitis or they have like rashes
57:52
that may actually tell you
57:55
that the drug is working very well and that they are going to be somebody
57:58
who responds so I think that's
58:01
a little bit we have to rely on our clinical colleagues to
58:04
kind of kind of tell us, you know,
58:07
if they're feeling poorly what do we think? It's
58:10
what do we think it's due to, you know, in addition
58:13
to us being able to detect those other talks to cities.
58:17
Um, okay next one.
58:21
So recessed is absolutely approved by oncology, or
58:24
is it instill in trial or research state? So recess
58:27
1.1 is definitely established. It came
58:30
out several years ago and that's being routinely
58:33
used in clinical trials. That's it's used
58:36
in research, but rhesus one point one is
58:39
like absolutely validated.
58:42
Um, all right, somebody said can you discuss the features of
58:45
Legato criteria? I would love to that's like a whole
58:48
separate a whole separate topic. That's
58:51
really a Lugano is an assessment criteria that is used
58:55
in lymphoma. And there are
58:58
pet features that you look at versus CT
59:01
features. And that depends is
59:04
your lymphoma fdg Avid, then we use the pet
59:07
criteria or is your lymphoma not fdg, then
59:10
we use CT based criteria, but there are some
59:13
similarities where you pick certain Target lesions
59:16
and you follow them over time. Those are
59:19
assess a little bit differently measure long and short access
59:22
you multiply them by each other and then you come up with, you know,
59:25
some of perpendicular products which are
59:29
then compared and the thresholds for how you categorize patients
59:32
response are a little
59:35
bit different than racist one point one, but the using the
59:39
pet we kind of talk about
59:41
Little criteria, which is a five-point Scale
59:44
based, you know relative to background
59:47
tissues relative to liver and we kind of classify the
59:50
metabolic behavior of lymphoma and
59:53
look at assessment response assessment based
59:56
on improvements or worsening in SUVs. So
60:00
that's like the two minute the two-minute version of
60:03
it, but it's it's kind of totally separate than
60:06
the ones we talked about today the ones we talked about today are really
60:09
for solid tumors and don't really address lymphoma.
60:14
I think
60:16
That is all we have. So yeah all
60:19
we have time for at least. Thank you guys for having
60:22
me and yeah, it's a
60:25
great platform to to be able to share these lectures and
60:30
I am happy to be here.
60:32
Dr. McIntosh, thank you so much for your lecture today and thanks
60:35
to all for your participation in our new conference.
60:38
A reminder that you can access the recording of today's conference
60:41
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60:46
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60:49
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60:58
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60:59
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61:08
have a great day.
61:09
Thanks everybody.
Lacey McIntosh, MPH, DO
Director, Oncologic Imaging; Assistant Professor, Radiology
University of Massachusetts Medical School / Memorial Health Care
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