Smilow Shares: Breast Cancer Awareness Month: Early-Stage Breast Cancer

Name: Smilow Shares: Breast Cancer Awareness Month: Early-Stage Breast Cancer
Uploaded: 2025-10-30T15:20:25.95Z
Duration: 51 min 26 s
Description: October 9, 2025 Moderated by: Rachel Greenup, MD, MPH Presentations by: Elizabeth Berger, MD, MS, FACS Mariya Rozenblit, MD Siba Haykal, MD, PhD, FRCS, FACS

October 30, 2025

October 9, 2025

Moderated by: Rachel Greenup, MD, MPH

Presentations by:

Elizabeth Berger, MD, MS, FACS

Mariya Rozenblit, MD

Siba Haykal, MD, PhD, FRCS, FACS

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ID: 13573
To Cite: DCA Citation Guide

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00:00Good evening, and welcome to
00:02the SmiloShares
00:03early stage breast cancer session
00:05entitled what patients and families
00:07should know.
00:08My name is doctor Rachel
00:10Greenup. I'm the chief of
00:11breast surgery
00:13at the SMILO in the
00:14department of surgery at the
00:16Yale School of Medicine. And
00:17tonight, we have three of
00:18our esteemed colleagues, doctor Elizabeth
00:20Berger,
00:21doctor Siba Haykel, and doctor
00:23Maria Rosenblatt.
00:24And we're gonna start with
00:26doctor Berger who's an assistant
00:27professor of surgery in the
00:29division of surgical oncology
00:31who will talking be talking
00:32to us about surgical updates
00:34and breast cancer.
00:35Doctor Berger, welcome.
00:40Thank you so much for
00:40that kind introduction, doctor Greenup.
00:42Let me share my screen.
00:49I get a thumbs up
00:51so everyone can see it?
00:52Great.
00:53So tonight, I I'm gonna
00:55spend about ten to fifteen
00:56minutes talking about some of
00:57the kind of updates of
00:58as far as surgical care
01:00in early stage breast cancer.
01:02And I appreciate the time,
01:03and, hopefully, we'll have time
01:04for questions,
01:05at the end if there
01:06are some.
01:07So the way we stage
01:09breast cancers in just kind
01:10of context as far as
01:11early stage goes is is
01:12multiple different ways. We think
01:13about how big the tumor
01:15size is, how how many
01:16lymph nodes may or may
01:17not be involved, and we
01:19essentially come up with a
01:20stage of breast cancer. And
01:21doctor Rosenblatt will probably get
01:22into this in more detail,
01:24but the biology of tumors
01:25now is so much more
01:26important than stage. But we
01:28still stage breast cancers based
01:29upon the staging,
01:31schema.
01:32And what we'll be talking
01:33about tonight is really this
01:35category of kind of stage
01:36zero, if you will, to
01:37stage two breast cancer is
01:38considered early stage.
01:40Stage zero breast cancer, kind
01:42of an enigma and doesn't
01:44make that much sense, but
01:45we really refer to what's
01:46called ductal carcinoma in situ
01:48as stage zero breast cancer.
01:50Or for a lot of
01:51my patients, when I say
01:52a precancerous process,
01:53it's in situ disease, meaning,
01:55you know, the abnormal cells
01:56are contained within the ducts.
01:58There's no invasion that we've
02:00identified.
02:01And so,
02:03you know, we really think
02:04that this is a precancerous
02:05lesion or stage
02:10We still think that we
02:11should take all of DCIS
02:12out. We should remove it
02:14surgically
02:15because we thought all DCIS
02:16became an invasive cancer at
02:18some point.
02:20Now what we know with
02:21ongoing clinical trials is maybe
02:23some DCIS
02:24never becomes invasive cancers,
02:26and we can actually safely
02:28observe or survey DCIS without
02:31actually having to remove it.
02:33So stay tuned.
02:34Hopefully, in maybe two thousand
02:35and thirty, we'll hear more
02:37about,
02:38stage zero or precancerous lesions
02:40such as DCIS
02:41being able to,
02:43stay in the breast, not
02:44have to be removed because
02:45of these ongoing clinical trials.
02:48So much of breast cancer
02:48care as I think everyone's
02:50call knows is really based
02:51upon really good clinical trial
02:53data, which is really exciting
02:54for all of us as
02:56providers and for patients.
02:58So if we're gonna talk
02:59about surgery for breast cancer,
03:00because surgery for breast cancer
03:02is is still important,
03:04we think about kind of
03:05where we've we've been and
03:06where we're going. So
03:08doctor Halsted used to perform
03:10what's called the radical mastectomy
03:11where we'd remove the chest,
03:13the the breast, the, pectoralis
03:16major and minor muscles.
03:17And now we know for
03:19breast cancer care that we
03:20can really preserve the breast.
03:22We can often do what's
03:23called lumpectomies where we do
03:25breast conservation and not remove
03:27the whole breast,
03:28and give patients similar, you
03:30know, the same outcomes from
03:31their cancer care.
03:37So and I recognize, but
03:39the the point the point
03:40of the slide is that,
03:42in the nineteen seventies, we
03:44started to ask these big
03:45questions for surgical care for
03:47breast cancer. And we realized
03:49that in the nineteen seventies,
03:50we didn't have to remove
03:52the whole breast,
03:53and we could do breast
03:54conservation with radiation.
03:56We then, if we pivoted
03:57towards the nineteen nineties, realized
03:59that we didn't have to
04:00do so much axillary surgery
04:02for early stage breast cancers.
04:04The z eleven trial was
04:06instrumental
04:06in allowing our patients to
04:08have less axillary surgery
04:10even if they had a
04:11few lymph nodes with cancer
04:12in it. And now fast
04:14forward to the, you know,
04:16kind of present time where
04:18we can do,
04:19maybe even less surgery for
04:20DCIS, and we just observe
04:22DCIS.
04:23So these are some of
04:24the really, important,
04:27practice changing trials for breast
04:28cancer care, especially in the
04:30early stage setting.
04:33We even may go as
04:34far as to say and,
04:35again, a little bit more
04:36in advanced, breast cancer settings,
04:38but we even may as
04:39go as to far as
04:40to say, if a woman
04:41gets chemotherapy before surgery and
04:44there's no cancer left in
04:45the breast, we may be
04:46even able to avoid surgery
04:48altogether.
04:49This is, I think, too
04:50early for prime time, not
04:51not ready yet,
04:53but something potentially down the
04:55pipe.
04:58So if we are gonna
04:58do surgery for early stage
05:00breast cancers,
05:01what are some of the
05:02updates? And I'll go through
05:03these in a kind of
05:04brief,
05:05review
05:06as far as thinking about,
05:08we do have noncancerous lesions
05:09that we often take out
05:10for breast,
05:11as breast surgeons. We do
05:12a lot of now more
05:13oncoplastic work, which I'll touch
05:15on, briefly.
05:16We have some nipple sparing
05:17mastectomy updates as far as,
05:19nipple as far as sensation
05:21preservation
05:22and, potentially, you know, different
05:24options for reduction of lymphedema.
05:26So a lot of women
05:28will get diagnosed
05:30with these things called high
05:30risk lesions. They're not actually
05:31breast cancers, but sometimes,
05:34if they're in the breast
05:35and we remove it, we
05:36may find some underlying,
05:38essentially, precancer or DCIS diagnoses.
05:41So if a woman gets
05:42biopsy and has what's called
05:43atypical ductal hyperplasia,
05:45it is something that you
05:46wanna, consider seeing a breast
05:48surgeon for because it may
05:50be something we would talk
05:51to you you about removal
05:52of.
05:53Someone may get diagnosed with
05:54what's called LCIS or lobular
05:56carcinoma in situ, and it's
05:58alarming for patients and often
06:00get a a phone call
06:01from their primary doctor saying,
06:02you know, you have an
06:04carcinoma.
06:05But what we know about
06:06LCIS,
06:07that we actually don't need
06:08to take it out. It
06:09doesn't become a breast cancer,
06:11and it's something that we
06:12can watch,
06:13recognizing
06:14that it's a marker of
06:15risk. And then, you know,
06:17further things in the breast
06:18that can be diagnosed
06:20are the
06:21scars and papillomas.
06:23All
06:25some times,
06:26again, considering
06:29high risk lesions.
06:32Some we recommend,
06:34excision for, and some we
06:35don't recommend excision for.
06:38A lot of women ask,
06:39well, how are you gonna
06:40find who you're gonna be
06:41able to identify to get
06:42the the tumor out? And,
06:43unfortunately, that little biopsy clip
06:44get that gets left is
06:46not big enough for us
06:47as breast cancer surgeons to
06:48find on our own. So
06:50we need some help to
06:51be able to find that
06:52lesion, and it's always disappointing
06:53for the patient when we
06:54say we have to put
06:55in another thing into the
06:57breast before surgery, but it's
06:59very helpful for us, to
07:00be able to find accurately
07:01and pinpoint exactly where we
07:03need to go. So we
07:04used to use wires.
07:06And now,
07:07because of all the sometimes
07:09chaos that can happen with
07:10wires, sometimes we'll use what's
07:12called a tag or even
07:14a smaller device that goes
07:16into the breast a few
07:17days before surgery,
07:18and then often doesn't delay
07:20surgeries.
07:21A patient can get it,
07:22you know, a few days
07:23before on their own time,
07:25and it allows
07:27often
07:29to you know, a little
07:30bit, at different locations of
07:32the breast. Wires are still
07:33used. They're great technology.
07:35It's a very per, kind
07:36of surgeon preference and personal
07:38preference for the patient as
07:39well, but they're just different
07:41ways to, think about localization.
07:45Some women will come into
07:47our our
07:48clinic with, you know, these
07:49very large areas of, for
07:50instance, calcifications
07:52or even a large breast
07:53tumor,
07:55where, you know, we recommend
07:56surgery first.
07:58And sometimes, you know, there
07:59may be no other option
08:01but a mastectomy.
08:02But sometimes we have really
08:03nice options
08:04where we can do a
08:04very large resection and work
08:06very closely with our plastic
08:07surgeons, doctor Hakal and others,
08:09where we can do what's
08:10called an oncoplastic reduction. And
08:12so it allows us as
08:13breast cancer surgeons, even an
08:14early stage breast cancer, to
08:16take out a large piece
08:17of tissue,
08:18and really reduce or, you
08:20know, do what's called a
08:21mastopexy lift of the breast,
08:23and leave a woman with
08:24an amazing, reconstructive result,
08:27but still take out a
08:28fair amount of breast tissue
08:29and and get out the
08:30cancer safely.
08:32When we are taking
08:35out early stage cancers, we
08:37all kinda make sure that
08:38we get clear margins around
08:40the cancer. And I think
08:41this is can be a
08:42very confusing,
08:43for patients to understand.
08:45So when we think about
08:46clear margins,
08:48what essentially what we wanna
08:49do is we wanna take
08:50out, the cancer,
08:52and then we always want
08:53some healthy breast tissue
08:55around that cancer.
08:57And so, you know, unfortunately,
08:59when we have what's called
09:00a positive margin,
09:01what that means is is
09:02the what we hope is
09:04healthy breast tissue. Again, unfortunately,
09:06this is all microscopic
09:07disease.
09:08What we what a healthy
09:09breast tissue margin we we
09:11removed
09:12comes back underneath the microscope
09:13with some cancer on the
09:14edge of that margin. And
09:16that does often require us
09:18to go back to the
09:18operating room with the patient
09:19to take, again, a little
09:21bit more tissue.
09:22It doesn't mean that the
09:23cancer has spread all over
09:24the store. It doesn't mean
09:26that,
09:27you know, we missed something
09:29per se. Unfortunately,
09:30you know, we don't have,
09:32X-ray vision. If we did,
09:33that would be awesome.
09:35But since we don't, it's
09:36just a matter of where
09:37the pathologist, the doctors that
09:39look at things underneath the
09:40microscope, really have to examine
09:41that tissue to make sure
09:43that the cancer cells are
09:44clean of the edge.
09:47We also want cancer cells
09:48clean of the edge when
09:49we do DCIS,
09:51surgeries as well,
09:53and we always,
09:54kinda shoot for this idea
09:55of two millimeters from the
09:56edge of the piece of
09:57tissue when we take out
09:58margins.
10:01At Yale, the the study
10:03done to look at margins
10:05when we do remove breast
10:06tissue around,
10:08the the,
10:11cancer was done,
10:12by doctor Chagpar, who's no
10:14longer here at Yale, but
10:15she led this trial at
10:16Yale. And it was a
10:17really well done trial to
10:20show how we can take
10:21these,
10:22this healthy breast tissue around
10:24the cancer.
10:26As far as some of
10:27the mastectomy updates for early
10:28stage breast cancers, so when
10:30we think about mastectomies,
10:33there's multiple different ways to
10:34do mastectomies, multiple different types
10:36of reconstruction.
10:37And one of the ways
10:38now is what we can
10:39do is called a nipple
10:40sparing mastectomy.
10:42Yes, we know ducts do
10:44go into the nipple, and
10:45so sometimes there's fear that,
10:47you know, that may increase
10:48a woman's risk of developing
10:49a breast cancer if they
10:50have, for instance, the BRCA
10:52gene and want a prophylactic
10:53mastectomy.
10:54Or it may you know,
10:55there there may be some
10:56fear about risk of recurrence,
10:58if a patient has cancer
10:59and has a nipple sparing
11:00mastectomy.
11:01And a lot of really
11:02well done trials, you'll see
11:03doctor Greenup on this study,
11:05I should say.
11:07There's been a lot of
11:08work done in whether or
11:09not nipple sparing mastectomies are
11:11safe for our cancer patients
11:12in the early stage setting
11:13and in the prophylactic setting
11:15for our BRCA carrier patients.
11:17And what we found from
11:18multiple trials now or studies,
11:21I guess, I should articulate,
11:22is that, it is a
11:23very, very safe procedure for
11:26women to have done. Not
11:27everyone will qualify for a
11:29nipple sparing for various reasons,
11:32but,
11:33you know, in the setting
11:34that it's it's, a reasonable
11:35operation for a patient, it's
11:37safe.
11:39Contralateral prophylactic mastectomy. So this
11:42is a whole another discussion
11:43about when a woman has
11:44an affected breast with breast
11:46cancer.
11:47What about removing the other
11:49breast? You know, there's a
11:50lot of discussion about whether
11:51breast cancer spreads from one
11:53breast to the other, and
11:54that's actually not the case.
11:55We know that breast cancers
11:56don't spread from the right
11:58breast, for instance, to the
11:59left breast, but we do
12:00know that a woman's at
12:01a higher risk of developing
12:03a contralateral cancer if they
12:04have a breast cancer in
12:05one of their breast.
12:07What we do know is
12:08that
12:09removing the contralateral breast does
12:11decrease that woman's risk of
12:13getting a breast cancer, but
12:14doesn't improve their survival from
12:16their actual cancer in their
12:17in their breast.
12:19It's something to consider. It's
12:20definitely a conversation to have
12:22with your surgeon.
12:24And, you know, some women
12:25elect to do it for
12:25a very personal reason, and
12:27some women don't. It's just
12:28something to always kind of
12:30think about.
12:32As far as nipple sin
12:34neurotization
12:35now, so,
12:36there is some
12:38data to suggest that we
12:40may be able to reneurotize
12:42or essentially give sensation to
12:44the mastectomy skin when we
12:46remove the breast. Oftentimes, we
12:48remove the breast, the skin
12:49is innervated or gets its
12:50sensation from the breast, And
12:52so the skin loses sensation.
12:54It becomes numb.
12:55And now, you know, there
12:57is some,
12:58ability
12:59to find these nerves along
13:01the the outside part of
13:03the breast,
13:04connect,
13:05what's called an allograph. So
13:06it's a cadaver nerve,
13:08and then so that also
13:10into nerves underneath the nipple
13:12to try to preserve some
13:13sensation.
13:15There's
13:16some data to suggest that
13:18it works and then some
13:19data to suggest that it's
13:20it's not perfect,
13:22and that it doesn't always
13:23work. And so, you know,
13:25I think this is, you
13:26know, kinda two weeks continued.
13:29You know, I think often
13:30it's worth a try, and
13:32then, you know, sometimes,
13:34you know, we'll just have
13:35to see what the data
13:36shows as far as long
13:37term outcomes,
13:38because it may not, hold
13:40true to for every woman.
13:44There's been a lot of
13:46changes in the way we
13:48think about removing lymph nodes
13:49underneath the armpit for early
13:50stage breast cancers, which is
13:52really exciting for patients.
13:54We used to have to
13:55remove all the lymph nodes
13:56underneath the armpit all the
13:57time, and it caused a
13:58lot of morbidity for our
14:00patients. And now what we
14:01know, we can really only
14:02have to remove a few
14:03lymph nodes off in called
14:05a sentinel lymph node biopsy
14:06and leave the the rest
14:08of the lymph nodes to
14:09avoid that really, you know,
14:10unfortunate risk of what's called
14:12lymphedema, the swelling of the
14:13arm.
14:14As I spoke, earlier on,
14:16the z eleven trial was
14:17the trial in the early
14:18two thousands that showed us
14:20that if a woman has
14:21only one or two positive
14:23lymph nodes at the time
14:24of surgery, we don't have
14:26to necessarily remove all the
14:27lymph nodes.
14:29Now we even know
14:31that with women who have
14:32early stage slow growing cancers,
14:35the hormone receptor positive breast
14:36cancers,
14:37we actually don't even have
14:38to remove lymph nodes at
14:40all. So we don't even
14:41have to do that sentinel
14:42lymph node biopsy.
14:44If a woman has small
14:45cancers, hormone receptor positive,
14:48two trials were done, kind
14:50of right near each other,
14:51one in Europe and one
14:53in the UK,
14:54that showed us that there
14:55was no difference in outcomes
14:56whether we actually remove lymph
14:58nodes at all.
15:00This was just a a
15:01little bit more detail on
15:02the sound trial that allowed
15:04us again to show if
15:05a woman has a normal
15:06axillary ultrasound before surgery, we
15:09do breast conservation.
15:11We don't have to remove
15:12lymph nodes. And this was
15:13the INSEMA trial in Europe,
15:15again, showing essentially the same
15:17results. As you can see,
15:18the surgical complications
15:20are real when we have
15:22to remove lymph nodes, and
15:24they did a really nice
15:24job demonstrating that when we
15:26omit removing lymph nodes, women
15:28have a lot less, surgical
15:30complications.
15:32We give neoadjuvant chemotherapy, meaning
15:34chemotherapy before surgery and sometimes
15:37still early stage breast cancers
15:38if they're more aggressive, like
15:39the triple negative setting and
15:41the HER2 positive setting.
15:42And now what we know
15:43is
15:44that if we remove lymph
15:46nodes after chemotherapy
15:49and there's no cancer left
15:50in any of them, we
15:52don't have to take out
15:52all that lymph nodes underneath
15:54the armpit.
15:55However, stay tuned because even
15:58now, when we have a
15:59few lymph nodes that still
16:00have cancer in it after
16:01chemotherapy,
16:02we may not need to
16:03take out all the rest
16:04of them, and we may
16:05be able to, offer the
16:07patient radiation alone. So these
16:09results are hopefully coming in
16:10the next four to five
16:11to ten years,
16:13but I think this will
16:13be practice changing patients
16:15as
16:16well.
16:19And doctor Hickall may get
16:20into this in a little
16:21bit more detail later, but
16:22we now know that if
16:23we do have to remove
16:24all the lymph nodes, even
16:25still for an early stage
16:26breast cancer, it can happen.
16:28We can do techniques now
16:29to hopefully avoid, the horrible
16:31complication of lymphedema,
16:33where we can connect a
16:35vein and a lymphatic, a
16:37little channel in the armpit.
16:38And, again, I ideally, allow
16:40our patients to suffer less
16:42from potential complications of lymphedema.
16:45There are ongoing clinical trials
16:47in this country looking at
16:48this very idea to hopefully
16:50have to show that there
16:52are good outcomes with it,
16:54but stay tuned as well.
16:56And I think that's all
16:57I have. Thank you so
16:58much for the time, and
16:59I'd love to take questions
17:00at the end.
17:01Thank you so much, doctor
17:03Berger. And we're gonna move
17:04on to our two additional
17:05speakers. We'll take questions at
17:07the end, and I'll be
17:08responding in real time in
17:09the chat.
17:11This is really meant to
17:12highlight our multidisciplinary
17:13team approach.
17:14Next up is doctor Siva
17:16Haykal, associate professor of plastic
17:18surgery and section chief of
17:20oncoplastic
17:21reconstruction.
17:22Tonight, she'll be talking about
17:24breast reconstruction
17:25and early stage breast cancer.
17:26Thank you, doctor Haykel.
17:28Thank you so much, doctor
17:29Greenup, and thank you, doctor
17:31Berger, for an amazing talk.
17:33I'll be sharing my screen.
17:42Please let me know if
17:43you can see it.
17:48Great. Thank you.
17:50Okay. Great. So we're gonna
17:51talk about breast reconstruction,
17:53and,
17:55I'm open to questions at
17:56the end. Hopefully, I can
17:57answer some of the questions
17:58by going through,
18:00some of the slides and
18:01some of the techniques where,
18:03breast,
18:04breast cancer surgeons are working
18:06in collaboration with reconstructive
18:09surgeons,
18:10in order to achieve a
18:11great outcome.
18:13So let's talk about breast
18:14reconstruction. So it can either
18:16be immediate, which is at
18:18the time of mastectomy,
18:19and we'll talk about lumpectomy
18:21as well, or it can
18:22be delayed, which is any
18:23day after the mastectomy.
18:26How do we determine the
18:28best options,
18:29and, how do we make
18:30a decision? So it has
18:32to do with patient preference,
18:34the need for postoperative treatments
18:36such as chemotherapy or radiation,
18:39whether we have donor sites,
18:40and I'll talk about what
18:41that means,
18:43other medical issues, and recovery
18:45time.
18:46So I'll first talk about
18:47oncoplastic
18:48reconstruction.
18:49So doctor Berger mentioned it
18:51a little bit, but oncoplastic
18:53reconstruction
18:54basically involves,
18:57rearranging breast tissue after a
18:59lumpectomy for breast cancer
19:01to achieve a better aesthetic
19:03result. So when a portion
19:04of the breast is removed,
19:06it can cause some dimples,
19:08some divots in the breast,
19:10and it can cause some
19:11asymmetry between the two breasts.
19:13So this is a great
19:15option for people who have
19:17large or very, what we
19:18call, tootic or saggy breasts.
19:21So a breast reduction is
19:22typically done on the other
19:24side as well,
19:26and or and or a
19:28breast lift.
19:31Now let's talk about implant
19:32based reconstruction.
19:34So there are some techniques
19:35that involve putting in an
19:37implant right away. So that's
19:39when we put an implant
19:41at the time of a
19:42mastectomy.
19:43It eliminates the need for
19:45what we call a tissue
19:46expander.
19:48It's a breast reconstruction
19:49that can be completed in
19:51one step,
19:52and people who are good
19:53candidates for this are really
19:55based on the breast size,
19:57the cancer size,
19:59and the type of mastectomy
20:01required.
20:02And frequently, it's done when,
20:05we try to keep the
20:06nipple areola.
20:07However, this is not the
20:09gold standard.
20:10It can lead to high
20:12revision rates.
20:14The gold standard for implant
20:16based reconstruction
20:17is what we call a
20:18two stage procedure.
20:20So in the first stage,
20:22we put either a tissue
20:23expander
20:24above or underneath the muscle
20:26and most commonly now above
20:28the muscle.
20:29This looks sort of like
20:30a balloon. It has,
20:32a magnetic port in it,
20:34and it's covered by the
20:35skin.
20:37And this requires
20:39filling of that,
20:40balloon
20:42in clinic every one to
20:43two weeks, and we fill
20:45it to the size that
20:46we're happy with or you're
20:47happy with.
20:48And it involves the second
20:50stage. So that means going
20:52back to the operating room,
20:54removing the expander, and putting
20:56in an implant.
20:57Because this is kinda what
20:59it looks like. Sometimes it's
21:00covered with a special type
21:02of mesh.
21:03And,
21:04in clinic, we use a
21:06mag we use a magnetic
21:08finder. We find the magnetic
21:10port, and we put a
21:11needle through the skin
21:13into the tissue expander, and
21:15we fill up that space.
21:16So, typically, we start filling
21:19about two to three weeks
21:20after surgery.
21:21The expansion process can take
21:23up to
21:36treatment as required.
21:39What are the advantages of
21:40implant based reconstruction?
21:42It's a quicker procedure.
21:44It's a shorter recovery time.
21:47You get to choose the
21:48size of your reconstruction.
21:50We're only operating on one
21:52side.
21:53The disadvantage is it can
21:54be more than one surgery.
21:56We can sometimes see and
21:58palpate the implant.
22:00If it's placed under the
22:01muscle, the muscle can cause
22:03animation.
22:04There's always a risk of
22:06infection.
22:07There's a risk of what
22:08we call capsular contracture, which
22:10is the body forming
22:12a capsule around the implant,
22:14which
22:15commonly happens. However, sometimes it
22:18can become
22:19hard and painful
22:21and can distort the implant.
22:23Implants can also rupture.
22:25Any radiation can lead to
22:27a higher failure rate, and
22:29there's a few things associated
22:31with implants that are less
22:33common and actually very rare,
22:35but we frequently
22:36talk about and you should
22:37discuss with your reconstructive surgeon,
22:40which are anaplastic large cell
22:41lymphoma and breast implant illness,
22:44which are related to safety,
22:46related to some types of
22:47implants,
22:48which are not always used,
22:51in all practices.
22:53Doctor Berger alluded to, sensation
22:55preservation.
22:58So this is frequently
23:00done when we can preserve
23:02the nipple
23:03and the areola,
23:04which can which is done
23:06in, some patients. Again, the
23:08tumor has to be far
23:09away enough from the nipple
23:11areola so that we can
23:12keep it.
23:13And then the breast have
23:14to has to already has
23:15a nice shape,
23:17to it so that we
23:18can preserve the nipple areola.
23:20So when that's done, we
23:21can do we can preserve
23:23sensation in two ways.
23:25One of them by connecting
23:27a nerve
23:28that comes off the shelf
23:30that has been processed,
23:32or we can take a
23:33nerve
23:34from the side of the
23:35breast that's not involved in
23:36the cancer
23:38and transfer it over to
23:39try to bring back sensation.
23:42Now the sensation is not
23:43like normal sensation.
23:45It's not erogenous
23:46sensation,
23:48but, we think with some
23:49studies that we can bring
23:51back sensation,
23:53better than not having this
23:54done at all.
23:56The other type of re
23:58re breast reconstruction is called
23:59autologous tissue reconstruction.
24:02Can you guys still hear
24:03me?
24:05Okay. Great. Sorry. I think
24:06you lost the signal.
24:08And that means using your
24:10own tissue. So that can
24:12come from different areas.
24:14So there it can come
24:15from the abdomen, the belly.
24:17That's called a deep flap.
24:18It can come from the
24:19thighs. That can is called
24:21the tug flap or the
24:22pad flap. It can come
24:24from the buttocks, the eye
24:26gap, or the s cap,
24:27or it can come from
24:28the back.
24:29So that's using,
24:30the patient's own tissues to
24:32create a breast mound. It
24:34avoids all the complications
24:36related to implants,
24:37and it's a pretty nice
24:38donor site. So let's talk
24:40about the options.
24:41The most common one is
24:43called the deep flap. That
24:45stands for deep inferior epigastric
24:47perforator flap. That just means
24:49the vessels that we actually
24:51use.
24:52So this is a cross
24:53section of the belly where
24:54we have skin and fat
24:56and the muscle.
24:58There's little vessels that are
24:59less than one millimeter in
25:01size that really penetrate through
25:03that muscle
25:04and give blood supply to
25:06the skin and the fat.
25:07So we get a CT
25:08scan of the belly first,
25:10and during the surgery,
25:12we find those little vessels.
25:14We follow them all the
25:15way down to the groin
25:16where they come from, where
25:17they become slightly larger, so
25:19about two to three millimeters.
25:21We disconnect them from that
25:23area,
25:24and we reconnect them in
25:25vessels underneath a small piece
25:27of rib.
25:29This is called microsurgery.
25:31We use loops and a
25:32microscope to do this, and
25:33it can be a long
25:34procedure.
25:36You end up with a
25:37scar from hip to hip
25:38and a scar around the
25:39belly button like a tummy
25:41tuck.
25:42Half of the belly is
25:44used for one side, half
25:45is used for the other
25:47side, and we create a
25:48breast out of it.
25:50We can also bring in
25:51a little nerve to try
25:53to bring back sensation
25:55and try to,
25:57you know, to create the
25:58sensation
25:59similar to what I talked
26:00about earlier.
26:02I'm sorry. I have a
26:03little child in the background.
26:05And we also have,
26:07however,
26:08it's, again, not like normal
26:10sensation,
26:12but we do know that
26:13with time, even without using
26:15a nerve graft, we can
26:16bring back since the, the
26:19nerves actually grow from the
26:20side,
26:21of the body to try
26:23to bring back sensation into
26:25the flap.
26:26One side takes about six
26:28hours.
26:29Two sides takes about ten
26:30hours.
26:31This admit patients have to
26:33admit be admitted for about
26:35two to three days. The
26:36first twenty four hours are
26:38the most important because we
26:39watch to make sure that
26:41everything is working okay.
26:43The advantages are that most
26:45of the reconstruction is done
26:46at the time of surgery.
26:48We're using your own tissues.
26:50It's lifelong. It's the best
26:52substitute for a natural looking
26:53breast.
26:54The benefits is a tummy
26:56tuck.
26:57However, it's a longer procedure.
26:59It's a longer recovery time.
27:01It's a separate donor site.
27:04It may require revision surgeries.
27:06There's a possibility of it
27:08not working, which is which
27:09doesn't happen very often.
27:11We can only use the
27:12belly once, and there's obviously
27:14more scars because we're operating
27:16in another area.
27:18Other areas that we can
27:19take it from is the
27:20buttocks,
27:21the thighs
27:23as well.
27:24Now let's talk about using
27:26implants with your own tissue.
27:28So that is a procedure
27:30where we can take,
27:31in cases, for example, of
27:33radiation,
27:34where we can take skin
27:36and fat and sometimes the
27:38muscle
27:39and swing it over to
27:40the breast
27:41along with a tissue expander
27:43of an or an implant,
27:45to recreate a breast.
27:48Now I also wanna talk
27:49about what we call aesthetic
27:51flat closure.
27:52So plastic surgeon can be
27:54involved in after mastectomies
27:56in patients who do not
27:57want reconstruction,
27:59but do not want redundant
28:01skin in that area. So
28:02we can do different techniques
28:04to try to make sure
28:05that we have scars,
28:08that look aesthetic
28:10and to make sure that
28:11there are no irregularities
28:13in the chest.
28:15Now the advantages of implant
28:17and autologous based reconstruction, which
28:18I mentioned earlier, is that
28:20it can be used in
28:21patients who had radiation,
28:23in patients who are too
28:25thin or have had a
28:26tummy tuck. The disadvantages
28:28is the disadvantages of an
28:29implant
28:30or using tissue from other
28:32part of the body.
28:34If we have to remove
28:35the nipple areola, then we
28:36can reconstruct the nipple areola,
28:39and that's usually done by
28:40either bunching up some tissue,
28:42kinda like origami, to make
28:43a nipple or an elevation
28:45out of it.
28:46And other techniques that we
28:47use are,
28:49tattooing.
28:50One of our APRNs will
28:52do that, and we have,
28:54they're involved in,
28:56clinical and operative care for
28:58breast, breast cancer patients.
29:00They're certified in tattoo art.
29:03Doctor Berger alluded to,
29:06a technique that we use
29:07for prevention.
29:09So one technique is called
29:11immediate lymphatic reconstruction,
29:13Most importantly, to prevent,
29:16to prevent lymphedema,
29:17it's the way that we
29:18actually remove the lymph nodes
29:20by making sure that we
29:22try to preserve the lymphatic
29:23vessels at the same time.
29:25But if all of the
29:27lymph nodes are removed and
29:28have to be removed,
29:30then what we can do
29:31is we can try to
29:32find those little lymph nodes
29:34again by using a microscope.
29:36Those are very, very small
29:38in size. They're less than
29:39one millimeter in size.
29:41And we find a vein
29:42of equal size, and we
29:44reroute them. We perform a
29:46bypass.
29:47The suture that we use
29:48to bring those together is
29:49actually finer than a hair,
29:51so you can imagine that
29:52that's very small.
29:54And we our goal is
29:56to hopefully prevent lymphedema.
29:59This adds about an hour
30:00to an hour and a
30:01half to the case, and
30:02we think by looking at
30:04studies that it has the
30:06ability to reduce the chances
30:07of lymphedema by about fifty
30:09percent.
30:10It doesn't necessarily mean that
30:12absolutely
30:13would not have lymphedema,
30:15but it definitely
30:16is,
30:17is worth, worth trying.
30:20Thank you very much for
30:21listening, and,
30:22I welcome any questions that
30:24may come at the end
30:25of this talk.
30:28Thank you very much, doctor
30:30Haykel.
30:31And, we'll move on to
30:32doctor Maria Rosenblatt.
30:34Doctor Rosenblatt is an assistant
30:36professor of medicine in the
30:37division of medical oncology,
30:40and she'll be talking with
30:41us this evening about updates
30:42in systemic therapy.
30:44Welcome, doctor Rosenblitt.
30:46Thank you so much.
30:49Okay. So I'm gonna be
30:50talking about systemic therapy for
30:52breast cancer.
30:55And as we've heard so
30:56far,
30:57really, the treatment of breast
30:59cancer is a multidisciplinary
31:00approach,
31:01and this involves the breast
31:03surgeon, the radiation oncologist, and
31:05the medical oncologist.
31:07And each part of the
31:09team has a slightly different
31:11goal. So the goal of
31:12the breast surgeon
31:13is to remove the known
31:14cancer,
31:15to obtain negative margins as
31:17we heard about, to evaluate
31:18the lymph nodes,
31:20and
31:21to remove involved lymph nodes.
31:23The radiation oncologist
31:25then tries to mop up
31:26any microscopic
31:28disease in the breast,
31:29and the regional lymph nodes,
31:31and this is usually done
31:33after surgery, so after a
31:35lumpectomy.
31:36And sometimes in special circumstances,
31:38it might be recommended after
31:39a mastectomy.
31:40And the goal of that
31:41treatment is to reduce local
31:43recurrence, so the risk of
31:45the breast cancer coming back
31:46in the same breast.
31:48As the medical oncologist, my
31:50goal is to really mop
31:51up any microscopic disease that
31:53might be anywhere else in
31:54the body. And my goal
31:56is to decrease the risk
31:58of what we call distant
31:59recurrence, so the risk that
32:00this cancer
32:01might come back in other
32:02parts of the body.
32:04And we call that, the
32:06risk of developing metastatic recurrence.
32:13Okay. So how do we
32:14decide,
32:15what kind of medical treatment
32:17to offer? And this is
32:18a really complex decision that
32:20we put a lot of
32:20thought into. And we heard
32:22a little bit from Doctor.
32:23Berger about stage. So we
32:25think about what size is
32:26the tumor, how many lymph
32:28nodes are involved,
32:30are we worried about any
32:31distant metastatic sites? And then
32:34we think about the patient
32:35in front of us. What
32:36is their age? What are
32:37their other medical problems?
32:39What is their life expectancy?
32:41What are their values?
32:43And then we also think
32:45about
32:46additional characteristics.
32:48So just as doctor Berger
32:49mentioned, it's not just about
32:50tumor size and lymph nodes,
32:52it's also about the molecular
32:53makeup of that tumor. So
32:55we know that,
32:57whether it's a hormone positive
32:58or HER2 positive or triple
33:00negative breast cancer,
33:02The type of breast cancer
33:03has a very different prognosis.
33:06We also think about grade,
33:07meaning how aggressive does this
33:09cancer look under the microscope,
33:11and we sometimes do special
33:13types of gene expression testing
33:15to try to help us
33:16figure out what is the
33:17risk of this cancer coming
33:18back.
33:20So in terms of the
33:21timing of the therapy, we
33:23think about it, in two
33:25large buckets, meaning adjuvant or
33:27neoadjuvant
33:28approach.
33:29When we talk about an
33:30adjuvant approach, that's when we
33:32have a discussion with the
33:33surgeon,
33:34and we come up with
33:35a plan that we recommend
33:37surgery first.
33:38After surgery,
33:40we think about whether
33:42the person would benefit from
33:43the addition of chemotherapy,
33:46if they have a HER2
33:47positive breast cancer, whether they
33:49need HER2 targeted therapy,
33:51and then if radiation is
33:53needed. And then if it's
33:54a hormone positive breast cancer,
33:56we would add on something
33:57called endocrine therapy at the
33:59end.
34:00Sometimes we prefer a neoadjuvant
34:02approach, and this is often
34:04when chemotherapy
34:06is recommended before surgery.
34:08And this is often done
34:09in larger tumors
34:11where there might be a
34:12lot of lymph nodes that
34:13we're hoping to shrink before
34:15surgery,
34:16or if it's a more
34:17aggressive cancer like a triple
34:19negative breast cancer or HER2
34:21positive breast cancer.
34:22And sometimes,
34:24we recommend
34:26systemic treatment first because how
34:28the tumor responds to the
34:29treatment can actually be very
34:31important information for us as
34:32medical oncologists.
34:35And when the patient gets
34:37to surgery,
34:38we are looking for something
34:39called a complete pathologic
34:41response. So if we did
34:42systemic therapy first
34:44and the whole tumor,
34:47was killed off by the
34:48therapy and it looks just
34:49like scar tissue under the
34:50microscope,
34:51prognostically, that's very important and
34:53predicts a very low risk
34:54of recurrence.
34:56The radiation,
34:57question is up to the
34:59radiation oncologist
35:00and really depends on,
35:02what type of surgery,
35:04was recommended.
35:05And then once again, if
35:06it's hormone positive, we would
35:08end,
35:08we would add on endocrine
35:10therapy at the end.
35:12So this is an example
35:13of an oncotype, but this
35:15is a test that we
35:16commonly send for hormone positive
35:18breast cancers.
35:19And what this does is
35:20it takes a small piece
35:21of tissue from the original
35:23breast tumor
35:24and sends it off to
35:25a special lab to look
35:26at a certain number of
35:27genes in the tumor itself
35:29that help to predict how
35:31aggressive that cancer is and
35:33what is the risk of
35:33the cancer coming back. And
35:35so what the report gives
35:37you is a number.
35:38And in general, anything above
35:40twenty five suggests that there's
35:42a benefit to chemotherapy,
35:44and it also gives you
35:45this number called distant recurrence
35:47risk at nine years. And
35:49so what that number tells
35:50you is over the next
35:52nine years,
35:53what is the risk of
35:54this cancer coming back in
35:56other parts of the body,
35:57so coming back as a
35:58metastatic breast cancer.
36:00And,
36:01if you take endocrine therapy,
36:04it gives you the the
36:05risk with the endocrine therapy.
36:08In general, we know that
36:09endocrine therapy reduces risk by
36:11about fifty percent. So if
36:13you don't take endocrine therapy,
36:15you can double that number.
36:17And then it also gives
36:18you the number for absolute
36:19chemotherapy
36:20benefit.
36:21And so often if it's
36:22a high oncotype,
36:24that absolute benefit is usually
36:25greater than fifteen percent, and
36:27that's when we'll be recommending
36:29chemotherapy.
36:32Here at Yale, we have
36:33developed several different pathways,
36:36to help standardize,
36:38the decision for when to
36:39send Oncotype.
36:41And so wherever you go
36:43as a patient across the
36:44Yale network,
36:45the different physicians will be
36:47following the same algorithm.
36:49And this can be really
36:50helpful because for some tumors
36:51that are very small, that
36:53have very low risk features,
36:54we often don't even have
36:56to send an oncotype.
36:57And then for some tumors
36:59that are very large and
37:00are very high risk and
37:01we know that that person
37:02needs chemotherapy,
37:04we often don't have to
37:05send oncotype either. And then
37:07sometimes there are these gray
37:08areas, and that's when these
37:09pathways can be really helpful.
37:11And if you're a physician
37:12and you're on the call,
37:14and you're
37:16looking for some guidance for
37:17when to send an oncotype,
37:19you can click the pathways
37:20tab in epic.
37:22And so this has been
37:23developed for both premenopausal
37:25and postmenopausal
37:26women with hormone positive breast
37:27cancer.
37:28And then in the adjuvant
37:30setting,
37:31where,
37:32somebody has already completed surgery,
37:35chemotherapy if they needed it,
37:37and radiation,
37:38We also think about ways
37:39that we can optimize what
37:41we call endocrine therapy. So
37:42we want to block estrogen
37:44in hormone positive breast cancer.
37:47And in addition to our
37:48estrogen blocking pills, we now
37:50have something called CDK four
37:52six inhibitors, and these are
37:54pills
37:54that actually inhibit the cell
37:56cycle. So if there's any
37:57microscopic
37:58cancer cells left over anywhere,
38:00it actually inhibits their growth
38:02and helps to kill them
38:03off, and we often give
38:04these in combination with estrogen
38:06blockers.
38:08And so this is often,
38:10saved for patients who have
38:12a high risk of recurrence,
38:14and so we've developed pathways
38:15here at Yale to help
38:16with that decision making as
38:18well.
38:19And oftentimes, it depends on
38:21the tumor size. So larger
38:22tumors,
38:24higher oncotypes,
38:26more lymph node involvement at
38:28the time of diagnosis.
38:31The other thing that we
38:32often think about as medical
38:34oncologist is whether somebody is
38:36eligible for clinical trials.
38:38And clinical trials are really
38:39important because it's a really
38:41great way to
38:43try to,
38:44optimize therapy for someone that
38:46we're seeing
38:47and either get a drug
38:49early,
38:50before it's on the market,
38:52or hopefully get, just a
38:54better approach to treatment.
38:56So one of the big
38:57questions currently in the field
38:58is, can we think about
39:00ways to
39:02chemotherapy
39:03in young women with hormone
39:05positive breast cancer?
39:06And the reason why this
39:07comes up is because,
39:09after doing this for many
39:11decades in breast cancer, we're
39:12not sure if it's really
39:14the chemotherapy
39:15drugs themselves
39:16that are showing benefit in
39:18this patient population
39:19or whether it's the chemotherapy
39:21putting these women into early
39:23menopause
39:23and whether it's actually the
39:25menopausal status,
39:26that is causing the benefit
39:28that we see.
39:29So there's currently a clinical
39:31trial being run by the
39:32NRG called BR009,
39:35and this is looking for
39:36young women who have
39:38oncotype below twenty five, which
39:40we generally think of as
39:42low risk,
39:43but they may have a
39:44positive lymph node and randomizing
39:47them to chemotherapy,
39:49which is the standard of
39:50care
39:51versus
39:52not doing chemotherapy, but really
39:54optimizing
39:55their estrogen blocking and putting
39:57them into early menopause.
39:59And so this is an
40:00important trial and something to
40:02think about,
40:03especially if if you are
40:04a young woman being diagnosed
40:06or you know somebody who's
40:07being diagnosed,
40:08because we're really starting to
40:10think that maybe it's not
40:12so much the chemotherapy,
40:13but the actual menopause status,
40:15that may be benefiting
40:18these young women.
40:20And then we also know
40:21that there's probably a subgroup
40:23of hormone positive breast cancers
40:25that are really high risk,
40:27high risk for coming back.
40:29And so how can we
40:30escalate and optimize treatment for
40:32those patients?
40:33And so there's a trial
40:34being run by Swag here
40:36at Yale called, two two
40:38zero six that is looking
40:39at something called mamaprint, which
40:41is very similar to Oncotype,
40:43but is a different assay
40:44looking at a different set
40:45of genes.
40:46And for patients who score
40:48in the in that really
40:49high risk category called high
40:51risk two or MP two,
40:53they're being randomized to adding
40:56immunotherapy
40:57to chemotherapy.
40:58In general,
40:59we don't think of hormone
41:01positive breast cancer,
41:03as a cancer that's very
41:04responsive to immunotherapy,
41:06But we think that there
41:07might be a subgroup of
41:08these very aggressive, fast growing
41:11hormone positive breast cancers that
41:12may benefit, and that's what
41:14that trial is looking at.
41:17We also wanna think about
41:18how can we tailor chemotherapy
41:20for triple negative breast cancer.
41:23And so there is a
41:24trial also out of SWOG
41:26that is looking at,
41:28patients with early stage triple
41:31negative breast cancer
41:32and randomizing
41:33to
41:35standard of care,
41:36chemotherapy,
41:38versus standard of care chemotherapy,
41:40but without the AC.
41:42And the AC drugs,
41:44often referred to as the
41:46red devil on the Internet,
41:48are the ones that have
41:49the most toxicity
41:50in terms of the chemotherapies
41:52that we use
41:53and also have a small
41:55but significant risk of potentially
41:57heart failure in the future.
41:59So we would like to
42:00avoid them as much as
42:01we can, And so we're
42:02hopeful that because triple negative
42:05tends to be more responsive
42:06to immunotherapy,
42:08we're hoping that this trial
42:09will show that we can
42:10avoid anthracyclines
42:12or AC in the future.
42:16And so the other thing
42:17that I think about, for
42:18hormone positive breast cancers in
42:20particular is how can we
42:22tailor our treatments
42:23to decrease the risk of
42:24late recurrence. So in general,
42:26most breast
42:27cancers, if they come back,
42:29they often come back in
42:30the first five years,
42:32but hormone positive breast cancers
42:34can come back late. So
42:35even as far as ten
42:37years out sometimes.
42:39And we don't really have
42:40a good way to detect
42:41them
42:42besides continuing to screen with
42:44our breast imaging with mammograms
42:46and ultrasounds.
42:47So this is, a trial
42:49called KEATS, that is now
42:50open at Yale and will
42:52be open across several different
42:54sites through the TBCRC.
42:56And this is looking at
42:57using a novel test called
42:59circulating tumor DNA,
43:02to see whether we can
43:03detect
43:04cancer coming back at just
43:06the microscopic
43:07level.
43:07And so for patients who
43:09are more than five years
43:10out from diagnosis with hormone
43:12positive breast cancer, who have
43:13completed all of their prior
43:15treatments,
43:17on this trial, they can
43:18get the ctDNA test, which
43:20is a blood test every
43:21three months.
43:23And if they end up
43:24coming back positive on this
43:26test
43:27and they don't have cancer
43:28yet on their scans,
43:30we're gonna be treating them
43:31with elocestrant,
43:32which is a pill.
43:33And it's one of these
43:35newer
43:36estrogen receptor degraders.
43:38So not just a blocker,
43:39but actually degrading the estrogen
43:41receptor.
43:42And we're hopeful that by,
43:45intervening
43:45at the microscopic
43:47state, we can prevent these
43:49cells from growing back into
43:50a tumor and growing back
43:52into a breast cancer recurrence.
43:55So thank you very much,
43:56and I hope that if
43:58you're a patient or a
43:59family member or a treating
44:01physician that you think about
44:02clinical trials or at least
44:04discuss clinical trials with your
44:06oncologist. Thank you.
44:08Thank you very much, doctor
44:10Rosenblatt.
44:12So we've answered many questions
44:14in the chat. This has
44:15been a fast and furious
44:16overview on updates in early
44:18stage breast cancer. We learned,
44:20surgical therapy from doctor Berger,
44:23options for reconstruction from doctor
44:25Hakal as well as updates
44:27and systemic therapy
44:28from doctor Rosenblit.
44:31I think the last thing
44:32we'd love to share with
44:33our attendees is that we
44:35do make decisions as a
44:36multi disciplinary cancer team. So
44:38patients that
44:39come to any site across
44:41the Yale Smilow network
44:43will meet with a medical
44:45oncologist,
44:46surgeon, radiation oncologist, and plastic
44:48surgeon,
44:49and we work as a
44:50cohesive united team in patients
44:52care.
44:53I think there's one last
44:55question in the chat, doctor
44:56Rosenblatt, about a lobular
44:59carcinoma with an oncotype
45:01of thirty four
45:02and,
45:03some concern about how estrogen
45:05gene expression,
45:08being borderline positive
45:10and how that
45:12information
45:13influences your recommendations for systemic
45:16therapy.
45:22That's a great question. So
45:24Oncotype
45:25was really designed to
45:27answer the question of, is
45:29there benefit to chemotherapy
45:31or not?
45:32And it really wasn't designed
45:34to
45:36kind of investigate
45:38how hormone
45:39positive a breast cancer is.
45:41So we still do rely
45:42on
45:43looking at the tumor under
45:45the microscope, and that would
45:46be a discussion with your
45:49team, including the pathologist
45:51in terms of how,
45:53how much estrogen positivity you're
45:55seeing in that case.
45:57In general,
45:58even for borderline
46:00positive
46:01cases,
46:02it looks like in this
46:03case, it was
46:05ninety percent is what I'm
46:06understanding
46:07from
46:08the report.
46:10We would go ahead and
46:11treat that as an estrogen,
46:14hormone positive breast cancer.
46:16There are borderline cases where
46:18the estrogen positivity is very
46:20low, and that becomes just
46:21a very complex discussion with
46:23your medical oncologist.
46:24And in that case, they
46:26might
46:27tailor the chemotherapy
46:28and offer you a slightly
46:29different chemotherapy
46:31if it's borderline.
46:33Thank you very much. There's
46:35another question about
46:38what we recommend for young
46:39women who are
46:42thinking about future pregnancy
46:44and have an estrogen positive
46:46tumor. Unfortunately,
46:48the positive trial, which was
46:50run out of Dana Farber
46:51but included multiple institutions
46:53across the country and the
46:55world,
46:56did look at young women.
46:57They were forty two or
46:59younger who
47:00were treated for hormone receptor
47:02positive breast cancer and received
47:04between eighteen and thirty months
47:06of anti estrogen therapy or
47:08hormone,
47:10endocrine therapy to target their
47:12breast cancer. They went on
47:13to take a break for
47:14pregnancy and
47:16potential breastfeeding, and their pregnancy
47:18success was very good
47:21as well as the risk
47:22of a recurrence
47:23was similar to the women
47:25who did not go ahead
47:26with pregnancy. So the data
47:27we currently have
47:29is showing great promise
47:32that it's safe for select
47:33women with hormone receptor positive
47:36breast cancers to take a
47:38break for pregnancy and,
47:40future,
47:41breastfeeding.
47:42And this is certainly something
47:44you should discuss with your
47:46oncology team. It's important that
47:48you're at a right stage
47:49of your cancer treatment and
47:51that we can monitor you
47:52as well as possible during
47:54and after pregnancy.
47:57There's another question about,
48:00a recent article on spike
48:02proteins
48:03and the aggressive new cancers.
48:05Doctor Rosenblatt, I'd I'd defer
48:07to you if you're able
48:08to answer this question.
48:11I don't see this question
48:12about the spike proteins.
48:15It says, any comment on
48:17the recent article on spike
48:18protein and aggressive new cancers?
48:22I'm not exactly sure what
48:24this article is referring to.
48:26There is a lot of
48:27research out there trying to
48:29figure out,
48:30better ways of predicting aggressiveness
48:33and recurrence, so that's probably
48:34what that's referring to.
48:37It's nothing that has reached,
48:38you know, standard of care
48:40yet. It hasn't entered mainstream
48:42practice.
48:43But, yeah, I I look
48:44forward to reading more about
48:45it.
48:46Okay.
48:47And then there's another question
48:49about tracking recurrences
48:51and HER2 positive versus
48:53hormone receptor
48:54positive HER2 negative cancers.
48:57I'll dive in very quickly
48:58as a surgeon. I think
49:00locally, we're examining your skin.
49:02We're looking at any changes.
49:04There can be there was
49:06another comment and question in
49:08the chat. There can be
49:09ongoing changes in the breast
49:10tissue
49:11after surgery, reconstruction, and radiation
49:14for even a couple years,
49:15but most cancer patients should
49:17be under surveillance with their
49:18oncology team.
49:20We decide to survey people
49:22for a distant recurrence in
49:24the setting of of symptoms
49:26or abnormal labs, and doctor
49:27Rosenblitz really an expert in
49:29ctDNA.
49:30So I'll, turn that over
49:32to her.
49:34Yeah. So the main surveillance
49:36mechanism, like we mentioned, is
49:38physical exam and then breast
49:40imaging.
49:42In breast cancer, we have
49:43not seen any benefit
49:44from PET scans or CAT
49:46scans, and so we don't
49:47do them because
49:49the risk of the radiation
49:50from the scans actually outweighs
49:52any any benefit in terms
49:54of finding a recurrence.
49:56And we don't have good
49:57blood tests either. There are
49:59blood tests out there called
50:00tumor markers and we use
50:01them for metastatic breast cancer
50:03all the time, But for
50:04early stage breast cancer, they've
50:06been shown to have what's
50:08called low sensitivity and low
50:09specificity. So they can be
50:11negative and there can still
50:12be a cancer and they
50:13can be positive and there
50:14could be no cancer. So
50:16they're not very helpful to
50:17us. And that's why we're
50:18trying to develop this new
50:19blood test called circulating tumor
50:21DNA.
50:22Right now, we're looking at
50:23it just in the research
50:25setting because we don't know
50:27yet how helpful this test
50:28is, and we don't have
50:30a treatment option. We need
50:31to investigate what treatment we
50:33can give if that test
50:34is positive.
50:35So there are trials going
50:36on for that for both
50:37hormone positive and HER2 positive
50:39and triple negative breast cancer.
50:41So if you're really interested,
50:43please look out for those
50:44trials.
50:45They're in very early stages,
50:47but we'll probably see more
50:48of those clinical trials in
50:50the next couple of years.
50:54Alright. Well, thank you to
50:55my esteemed colleagues,
50:57for joining us tonight and
50:58sharing your knowledge, and thank
51:00you to all the attendees
51:01for joining us for this
51:02Milo shares. We,
51:04encourage you to attend our
51:06future sessions in the month
51:07of October, which as many
51:09of you know is breast
51:10cancer awareness month. And please
51:12reach out,
51:14to any member of our
51:15program if you or family
51:17or friends need to be
51:18seen.
51:19We wish you all well,
51:21and
51:21thank you again for joining.