Hey everyone, welcome to the Drive Podcast. I'm your host, Peter Attia. This podcast, my website, and my weekly newsletter, all focus on the goal of translating the science of longevity into something accessible for everyone. Our goal is to provide the best content in health and wellness, and we've established a great team of analysts to make this happen. It is
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get back much more than the price of the subscription. If you want to learn more about the benefits for our premium membership, head over to peteratia-md.com forward slash subscribe. My guess this week is Dr. Ted Schaeffer. Ted was a guest previously on episode 273 in October of 2023, and episode 39 all the way back in February of 2019. I wanted to have Ted back on to speak about one very specific topic, testosterone and prostate cancer, given
a recent study that came out since our last conversation. Given the interest in this topic that we see in our practice, in addition to all of the questions that are constantly coming at us through our site and social media, I figured it would be great to have Ted back on to speak about this. Throughout this podcast, we referenced the Traverse trial, and we talked about what the trial directly showed, in addition to what was not
entirely clear from the study. This is a study I've written about in the past, discussed some of its limitations. But really, the essence of our discussion today was understanding the role testosterone plays in prostate cancer initiation and propagation. And even though this is a topic I spend a lot of time reading about and discussing with experts, I came
away quite surprised with some of the insights from Ted. Given the ubiquity of testosterone replacement therapy today, this is an important topic for anybody who's ever considered it or anybody who cares about somebody who's ever considered it. Unfortunately, there is a lot of bad information out there when it comes to the role of testosterone and prostate cancer. Yet, fortunately, the literature actually provides a lot of evidence for testosterone
can be safely used and when it should not be used. Ted is an internationally recognized urologist and prostate cancer oncologist, author and speaker. He's the chair of the Department of Urology at the Feinberg School of Medicine and the urologist and chief at Northwestern Memorial Hospital. He's also the program director there as well. He is also co-author of one of the definitive textbooks in urology, Dr. Patrick Walsh's Guide to Surviving Prostate
Cancer. So without further delay, please enjoy this special episode with Ted Schaefer. Ted could be sitting down with you here. We're going to do something a little different, which is we're going to take a quicker drive than normal and really try to laser focus in on one topic. A topic that you and I spend a lot of time discussing internally, but through a number of back and forth emails, we decided this would actually make for a great
short podcast. Let's give folks a little bit of background as we jump right into this. So there was a study that was published a year ago called the Traverse Trial that set out to ask the question, does the use of exogenous testosterone increase the risk of ASEVD and I've written about that trial. We're not going to go into great detail with respect to its primary outcome of ASEVD. The short answer is it did not increase the risk of ASEVD.
And on some level, this was viewed as the answer to the question, testosterone, exogenous testosterone does not increase the risk of heart disease. But where you and I found ourselves discussing was more along a question of prostate cancer. So maybe tell folks a little bit about what we did and didn't learn with respect to prostate cancer from the Traverse study.
The Traverse study really looked at men who were hypoganadil, who presented with some degree of symptoms, and then the idea was to replete the testosterone, bring it up to a eugonadile level. The bump that they had in the Traverse was pretty small, 140 nanograms per ml. So a tiny bump with bearing in mind about a 60 plus percent dropout rate at five years. So very few people were actually maintaining the protocols that they originally set out
to kind of do at the beginning of the study. With that in mind, the idea was does supplementation of someone's endogenous testosterone with exogenous testosterone increase one's risk for being diagnosed with prostate cancer? With the implication that this could address two potential concerns. One, exogenous T would fuel the progression of an pre-existing prostate cancer and or exogenous T would induce cancer de novo in somebody with a low T state when
you bring them into a higher testosterone state. So that's how they kind of took on the study. Now, as we talked about before, there's a lot of detail about who was enrolled in the study. So everybody was hypoganadil. And the mean PSA for individuals in Traverse in both arms was around.9. So this is a low risk group of men because we know PSA is the main way that we screened for prostate cancer. And in general, the higher ones PSA, the
higher ones risk would be a being diagnosed with prostate cancer. So these are men in their 60s on average. These are men with low testosterone on average. These are men with low PSAs on average. So a low risk group and you take them from a hypoganadil to barely eugenadil states. The bottom line for the trial and the secondary analysis pre-specified was that there were no more prostate cancers diagnosed in men on T replacement versus on placebo. The total
number of prostate cancers in Traverse that were detected was very low. I think it was 1T3. So incredibly low numbers of testosterone in a cohort of 50, 300 plus men. So the Oval Incidents of prostate cancer detected was quite low. The features of the individuals who had prostate cancer in Traverse were on average higher PSAs than the median. Again, the
median PSA on entry was around.9. So individuals who were diagnosed with prostate cancer had higher median PSAs and had higher shifts in their PSA while in the Traverse trial than those men that did not develop or were not diagnosed with prostate cancer. So what the study tells us is it's reassuring in many, many ways. Number one, men with low PSAs have a low risk of being diagnosed with prostate cancer. Number two, you can use PSA in generally similar
fashions when you're supplementing a man on exogenous testosterone. That is you can look at changes in the PSA. Most men in Traverse, their PSA did not change. It changed less than half a point over the course of the trial. And for those individuals whose PSA did go up, those were the men that were at risk for or were subsequently at higher risk for being identified as having or harboring a prostate cancer. Those would be the take home points from my perspective when
interpreting Traverse vis-a-vis the prostate cancer risk. There was a figure in the paper that showed the non-statistical significance in the difference between the incidence of prostate cancer in the groups. And even though, again, it never comes close to reaching statistical significance because in large part, I think the sample size is so low. So even if there was a
difference, it would be very hard to see. The incidence curves do diverge a little bit. And I think that's probably what was my first email to you was, hey Ted, is it possible that this was indeed increasing the incidence or recognition of prostate cancer? But the study wasn't long enough to see it. So it either wasn't long enough or wasn't large enough to see it. And if this had gone 10 years and or if it had 10 times the number of patients, we might have seen a difference. We don't know
the answer to that. We can't know the answer to that without doing it. But what were your thoughts on that line of inquiry? This is a large cohort of individuals. I felt like they're probably pretty limited data to suggest that levels of testosterone or supplementation of testosterone really are strong in correlated with the induction of or the precipitation of a preexisting
prostate cancer. So I personally felt as we had discussed that supplementation of individuals in a hypo-gonatal state to a eugenatal state is not going to increase their risk for the induction of or the propagation of a preexisting prostate cancer. That's based on the traversed trial which is a large cohort of men. But frankly, you're bringing somebody from a state that perhaps they have a low teeth to a more eugenatal state. And there's a couple of really interesting pieces of work
that help us understand what happens when a prostate grows. And one of the main growth components for a prostate are antigens either in the form of testosterone or dihydrotestosterone, which has a much higher finity for the energy receptor. And this really does two things. It causes growth and differentiation. And the sensitivity of prostate cancer cells to these growth hormones for them, antigens or DHT is different between a cancerous and a non-cancerous cell. There's
actually much higher densities of energy receptor within a benign prosthetic cell. And therefore, they're much more sensitive to supplementation of testosterone. With that in mind, most of the studies that have looked at supplementation of testosterone and eugenatal men have shown that they actually have
worsening more often than not of their BPH or urinary symptoms. And that's thought to be due to the greater sensitivity of benign cells to exogenous T, then actually the development or progression of a prostate cancer. So that's kind of traverse plus a couple of other smaller but consistent studies that have been published over the last two to three decades within the urology space. Now, the other point that we came and we began to talk about is this idea of the saturation theory.
So the energy receptor engages with testosterone. It engages with dihydrotestosterone. When that engagement occurs, it moves from the cytoplasm to the nucleus and binds to energy and response
of elements and you get production of energy-dependent genes and proteins down the road. Now, the idea behind the saturation theory is that once you reach a certain level of energy in a particular end organ, prostate, muscle, CNS, hair follicle, for example, once you reach a certain level, the receptor is fully saturated and anything above and beyond that level, you're going to get limited bang for your buck in terms of the kind of output from the receptor engaging the DNA.
I.e. at a certain level giving additional levels of testosterone or having additional levels of T or DHT within that organ are not going to result in any worse or augmented effects. And so that we believe is true. There's a series of studies that have suggested that A, the saturation theory and thresholds for saturation of the endogen receptor exist. You can look at that within the prostate and that those levels of saturation of the
endogen receptor vary by the organ you're evaluating. So for example, it's thought and it's been modeled that the saturation of the endogen receptor levels of T that saturate AR within the prostate are probably around serum levels of 2 to 250 Ngm from milliliter, which is pretty low actually. Whereas in muscle, levels probably have to be much higher to get the anabolic effects from a steroid in muscle to promote muscle growth and muscle mass.
Heraphylicals are probably more similar to prostate. Why they have high densities of 5 alpha reductase and so they can convert T to DHT. There's also an effect on the central nervous system and cognitive function, et cetera, et cetera. So there's variation in terms of the effect of T on a variety of end organs and that variation in the effect of T on these end organs is probably
related to this idea of the saturation theory that is not unique to the endogen receptor. It's something that's pretty common within a variety of different receptor superfamilies, but certainly we think it exists within AR. And probably as again underscores the idea that supplementation of your serum testosterone levels to higher levels will have an end organ effect that's positive perhaps within muscle growth, but has pretty limited results in terms of its impact on the prostate
growth and initiation and propagation of prostate cancers. So Ted, let me make sure I understood that high level that made sense, but some of those examples and numbers are mind boggling to me. So you're saying if I heard you correctly that prostate tissue and hair follicles might reach saturation as low as 250 nanograms per desoleter of testosterone, which as you point out is very low.
That's a level that is probably at about the 10th percentile of the population for men over 18, suggesting that 90% of men walking around, even not taking testosterone replacement therapy, are already at levels of saturation for hair follicles and for prostate. You alluded to the fact that presumably for anabolic needs in the muscle, the saturation level would be much higher. So first of all, let me pause before I go on. Am I getting those numbers about right?
Yeah, and the way to think about it is in the prostate and in hair follicles, there's 5L for ductase. As soon as testosterone enters a prostate epithelial cell, it is immediately converted to DHT, which is about 10 times more potent than testosterone. So if you really wanted to kind of fiddle with the math, actually, if you didn't have DHT around, the saturation level that you would need for prostate, maximal saturation, you could argue would be 2500 nanograms per
desoleter. But the idea is that there's amplification of the effect of T by converting to DHT,
by about maybe 10X. So does that imply that on average, if a man is taking exogenous testosterone, let's say he started out at 300 nanograms per desoleter, which truthfully would still be considered hypogonatal, and he gets replaced to 800 nanograms per desoleter, would you not expect him to experience a BPH trajectory growth or hair loss or any of the things that might be associated with the increase that he's going to experience in both testosterone and DHT?
Yeah, I mean, most of the data on T supplementation within the prostate, you're going to see more of a precipitation of BPH symptoms. Again, we talked about the differential, and so there may be a little bit of a bump in terms of lower urinary tract symptomatology, but it's pretty subtle. And in fact, one of the biggest genes that uses or is antigen responsive is PSA. And most people, when you augment their testosterone, that's how they measured or estimated the saturation
to be between 200 and 250. Mokira did a nice study, he's a former drive guest. They estimated to be around there, and you can actually see that, because most people that you supplement from, let's say, three to 800, you're not going to see a big bump in their PSA. And so that would be the premise, whereas if someone's at three, they may have pretty limited muscle mass, and yet you bump them to 800, and you see a real nice impact.
So let's now talk about bringing it back to prostate cancer, a paper that you and I discussed, probably on your first appearance on the drive, which was that paper that came out in the New England Journal of Medicine back when we were residents. God, I really think this was probably
02 or 03. And it was at least for me not being a urologist, but still being someone that kind of at least read the New England Journal of Medicine, pretty remarkable in what it suggested, which was the lower a person's testosterone, the greater the risk of high grade prostate cancer.
So maybe for folks who don't remember that discussion, can you bring us back up to speed on that point and the findings of that paper, which I think are starting to make sense, by the way, in light of what we're talking about? So the main driver that people have always focused on, the dependent fuel for prostate cancer has always been postulated to be testosterone. And in a normal prostate cell, we talk about
these different thresholds. Obviously, when the gland undergoes mutations and prostate cancer is developed, some of the wiring is skewed and you can develop a cancer. Now, the initial study basically showed a correlation between grade and aggressiveness of prostate cancer with testosterone and PSA values, showing a lower PSA was associated with a higher grade prostate tumor.
And that concept was something that always intrigued me. And I think during the time we did our first podcast, which is in 2018 or so, I've been working on this again, studying that exact same concept and understanding, well, if a higher grade prostate cancer is a cancer that is less similar to a benign prosthetic gland, it's more dissimilar, it's more altered. What are the
factors that are associated with causing it to grow and causing it to be aggressive? And so we really did a very deep study to try to characterize not based on PSA values in grade, but actually on a much more comprehensive assessment of the engagement of the Andredin receptor with the ARE and the prostate cancer cell and the output of that engagement within a tumor. And so we developed a signature, anrogen receptor activity signature that basically looked at the end point of
anrogen receptor activity within a prostate cancer. And we found similar observations and similar findings. That is, the more aggressive a tumor was, the less it relied on or less output of a canonical AR engagement with its traditional receptors existed. And so that, again, underscores the observation that paper we talked about back in our first podcast. That is that cancers that are more aggressive are probably less reliant on the traditional growth and differentiation factors
that a prostate epithelial cell has in its normal microenvironment. And these tumors are much more aggressive than kind of AR high tumors. These tumors rely on different growth mechanisms to be aggressive. And they have different vulnerabilities in terms of sensitivity to agents that we may use when they present at later stages. So yeah, the initial observation was something that was always
at front of my mind. And we've done a lot of work in our lab to try to understand why those higher grade tumors are often found with lower PSA values and what the reasoning is and then what makes them look the way they are and act the way they do. So Ted, you referred to these canonical genes. I think you said there are nine of them that make up the ARA score. There are hundreds of genes that have canonical androgen responsive elements within them. We basically did a rank
ordering and identified the top 10 for reasons that are a little subtle. We kicked one of them out. But there are several different and there are many actually different androgen responsive signatures. You can look at ones from benign cells. You can look at ones from early cancers and you can look at ones from advanced cancers. And the fundamental principle
that there's this cohort of androgen responsive genes is pretty consistent. And if you look at them in any of these different stages in the benign cell signature, localized prostate cancer signature, antigen responsive or even in advanced disease, the same theme is true. That is the tumors that rely and have less of a signature that is less AR high like they are more aggressive.
Sorry, Ted. Just to make sure I understand something from the standpoint of the tool, this is something that you're doing post biopsy and or post prostitutectomy where you're looking at the actual patients genes and presumably you're finding mutated genes or you're finding snips that are known to be higher risk of a given set of genes. Yes, the analysis is based off of an affi 1.0 ST chip that basically looks at gene products presumably after the engagement of
the antivirceptor. Oh, I see. So you're doing an assay on the tissue to look at either mRNA or that's right. Something. Yeah, okay. Got it. It's an mRNA assay from a biopsy so you can actually characterize tumors up front from a biopsy or you can characterize tumors that have already been resected with surgery or frankly you could characterize a tumor from a metastatic location if you
really wanted to. It's an mRNA based assay looking at gene expression and the presumption is you could actually just look at an energy receptor gene expression within the tumors and we did and you see a similar story but as you know when you just say well we're going to take the nuclear hormone receptor and look at its 10 targets you're going to get an amplification of that particular signal.
So we thought we would have a broader array of cases to look at or a broader array of expression to look at if we developed a model that wasn't just a single gene in our case it was nine genes. Others have built ones that are 250 genes, 600 genes. We've tested them all. They all show the same and tell us the same story. So they tell us that within a prostate cancer agnostic of grade, agnostic of stage there are tumors that have signatures that are consistent with high
energy receptor output. Those would be like the way I explained to patients are those are weeds in your garden. They're really large above the surface but have very thin tiny roots. They're kind of differentiated. They're big and they're well differentiated but they're not aggressive and then there are tumors that have they don't look like a normal prostate gland at all
and they have signatures that reflect very low anderton receptor signaling. They have amplification of other signaling pathways, p10, mic, etc. And those are associated with a much more aggressive phenotype in terms of metastasis, in terms of progression, in terms of resistance to traditional therapies that we use for individuals who have prostate cancer.
These clear based approved studies, I mean if a patient is seeing a doctor who's not you or not one of the doctors that has one of these ARA assays and they undergo a biopsy, is it a given that they can get this type of analysis done? Yeah, they can. This is a clear approved assay. It is the collaboration that I undertook over 10 years ago with this company called Decifer and they are now owned by Vericite. And so you can do a Decifer assay. This is a mRNA-based assay that gives you
a single assessment of how aggressive your prostate cancer is. It's called a Decifer score. But in addition to doing that, which is looking at about 20 or 22 genes that are associated with aggressiveness in prostate cancer, we also kept all the data from the other 40 or so, 40,000 different spots on the AFI array. And then that's how we built this ARA signature. So you can actually get access to through your physician, what we call the grid signature. And within the grid, you can
actually look at the ARA activity of your individual tumor. You can kind of model whether or not the tumor is a more basal like a more luminal like tumor. And these features are important within localized prostate cancers, but are I think more important to understand the phenotype later on if the cancer were to progress in return, some of the vulnerabilities of the tumors. So let's talk a little bit about how you use this information with more standard decision making.
So let's just assume that a patient presents with either a high PSA or a significant enough change in PSA that it triggers an MRI. And let's say that that MRI shows a rad score that when combined with some other factor like the PSA or the PSA density creates enough suspicion for a biopsy. So you do the biopsy and we've talked in previous podcasts about what the Gleason score is. And let's say that biopsy returns something that is a Gleason 3 plus 3. So this is kind of a
watch and wait, correct? Yes. How does the finding of the ARA impact your decision making in the Gleason 3 plus 3 patient? Is it something where it changes the frequency with which you want to do surveillance or is there some other metric that changes in response to the genetic output or the transcription of those genes? For lower grade prostate cancers, ones that we would typically follow in surveillance, there are some outliers that are kind of more aggressive in terms of their
molecular features. But on average, those tumors are really benign looking from a transcriptomic molecular profiling level. So within the low grade tumors, you very rarely will see a tumor that is aggressive by the decipher score. It's about 7% of the time. So it's worth it to look if you really want to have a sense for, do you have an outlier tumor? Now, can you identify the outliers with normal surveillance tactics that we've discussed on prior podcasts? Yes, you can.
So for the lower grade tumors, understanding the molecular phenotypes for me personally is less important. But as the tumors become more aggressive, understanding the molecular characteristics that drive those tumors, I think is very important. We can't precisely say now that if you have a low AR output tumor, a tumor that perhaps is not as dependent on antigens to grow, we can't say at this point in time that that kind of tumor needs a more aggressive or different type of treatment
than a high AR tumor as the tumors get more aggressive. But there are a couple of radiation-based trials that are using the decipher score to molecular profile the tumors. And then actually, again, begin to answer that question as to, let's say, if you are an ARA low tumor and you have a high grade prostate cancer and you choose radiation, perhaps you shouldn't just get standard antigen suppression along with your radiation. But perhaps you should intensify that with a more
advanced newer agent like Enzo Ludamite, Appalutamite or Darulutamite. We have evidence from analyzing face retrials that if you're low ARA, you have a much enhanced sensitivity to this dual doublet-based therapy. So one could surmise that if you're somebody with a localized tumor that's of higher grade and you're going to have radiation, you'd want to know your ARA score, for example, because that may inform whether or not you should intensify your ADT or just get
standard ADT. Now, those studies are actually ongoing. They're fully accrued. The NRG is a radiation-based trial group and they've accrued individuals in these higher risk cohorts looking at their
genomics and then basically stratifying them in different therapies. We're going to know the results of those studies within the next two years and they'll be fascinating to understand, again, this idea of the real precision medicine within prostate cancer is here and how you deploy it and how you deploy it to enhance the outcomes for patients is actually around the forefront of understanding that. So lots to come, we just need to stay tuned for probably two more years
to get that information. Is it an oversimplification to say that an patient with a Gleason 3 plus 4, this is a cancer that needs to come out with a low ARA score? Is that a patient that should or should not be on androgen deprivation therapy? Is that a patient where you say we are much better off doing a surgical resection here than we are opting for radiation and androgen deprivation
therapy? Yeah, that's exactly right. So obviously radiation is biologically modifiable, surgery is extra patient so you're not going to really modify anything that you do with ADT
and surgery. So yeah, in my opinion if you can treat someone's localized prostate cancer and save them the morbidity from systemic hormonal therapy, that's a huge win for the patient and so that's exactly another way that you could use the ARA score or other scores that predict aggressiveness is to say, hey, if this is a low ARA tumor, let's do surgery because we can treat them successfully with surgery and avoid any exposure to total androgen suppression, which you know is incredibly
morbid for these individuals. Does radiation ever alter this head? In other words, is there any scenario by which radiation increases androgen sensitivity? No, but androgen deprivation increases radiation sensitivity. So it's used to augment the effect, androgen suppression induces DNA damage. So you're already making the cells vulnerable to further damage by kind of inducing some baseline DNA damage up front with androgen suppression, then you hit them with radiation as well
and the effect is synergistic. So Ted, let's kind of bring it back to testosterone replacement therapy. So we've just gone down the rabbit hole pretty deep on the molecular nature of prostate cancers and particularly the prostate cancers that are most lethal. So now let's talk about a patient who wants to receive testosterone. So presents in a hypogonatal state is symptomatic by all measures should benefit from TRT. What are the things that give you pause in that patient's clinical picture,
either PSA level, family history, prostate size, presence of BPH anything? How would you cancel that patient specifically around the risk of cancer? And are there any scenarios where in a cancer-free patient, you would advise against TRT? I would say I can't think of any scenarios where I really advise against TRT for somebody who is symptomatic. You know, there's so many other potential negative outcomes for a patient who has low T besides the possible development or
detection of a prostate cancer. So for me, if you're hypogonatal, I want to maintain your cardiovascular health. I want to maintain your bone health, your muscle mass, your cognitive function. So I want to make you eukonatal. For an individual who has prostate cancer, who has low T, it really comes down to how aggressive is their prostate cancer in terms of what it would advise them. So for somebody who has low grade prostate cancer, who's in surveillance, I'm doing surveillance to optimize
their total health. And so I want to maintain them in a eukonatal state. So if they're on T replacement and they get diagnosed with prostate cancer, it's low grade, I'll maintain them on T replacement. Let's just pause there for a second Ted. That's a remarkable statement. I'm sure there are many people that are missing what you just said because it really flies in the face of what
most doctors would believe. You're basically saying, if I've got a guy who's on TRT and his testosterone is humming along at 800 nanograms per desoleter and he's been on exogenous T for a couple of years, but in the course of something, whether it be a rising PSA, he gets a workup, he finds his way into my office. We ultimately do a biopsy after an MRI and find that he's got a Gleason 3 plus 3 and you're saying you're not going to tell like I he has to stop his testosterone.
Is that what I'm hearing you say? Yeah, there's no evidence that says exogenous T replacement causes acceleration or propagation of someone's prostate cancer. There's no evidence to suggest that. And as you know, what 30% of the population has a T that's 800 or higher depending on their age.
So it's within the normal distribution. Would I encourage someone to be higher than that? No. But if that's where they've titrated their dose to be, relieve their symptoms and so forth, I'm comfortable having the discussion with the patient and saying, okay, here's how you have a prostate cancer. I think we can monitor and follow it. And there's plenty of people out there that I monitor and follow their prostate cancers that have normally
produced T's that are over 800. In my mind, it's no different than anybody else who's within that normal distribution. It is a radical thing. If you just think about it, it's actually not that radical really at all. Yeah, when you frame it that way, which is if you have two people sitting in front of you, one of whom is supplementing to a level of 800, the other one is naturally at 800 and they show up with the same Gleason 3 plus 3 cancer. You're going to monitor both of them.
You wouldn't say to the guy who's on TRT, well, I have to take your prostate out as a result of this or make you stop the T. And remember, so in a normal prostate testosterone is a differentiation factor. It will differentiate a prosthetic cell towards a fully functional benign epithelial cell. So conceptually, when I think about it, okay, let's just say that high T is supplemented or endogenous.
This circle is back to the discussion at the very beginning. High T is associated with probably on average a more well differentiated tumor, not 100% of the time, but that's what it's actually doing biologically within the prostate gland. It's differentiating these cells. Now, of course, it's a cancer, so it's maybe a little bit more genomic, unstable than a benign cell, it's over,
but that's how it's working. Conversely, if you have a tumor that is in a low T environment, i.e. the original publications we talked about in any GM, way back or other anecdotal series, the tumors that develop in a low T environment, they're less dependent on antigens to grow. They often use other growth pathways to be aggressive, and actually, I think they're more worrisome because you don't exactly know how you're going to attack it or treat it
if it actually progresses. So full circle, low grade prostate cancer, guy comes in as T is 600, guy comes in, you're supplementing his T to 600. To me, you should follow them both carefully and in the same way. Now, when you have a tumor that is a prostate cancer that requires treatment, so gleecin 7, 437, 448, more serious stuff, how do you handle those? That's where you really come into differences. So if someone is leaning towards radiation, that's where those individuals
need to go on and they do go on aggressive, and urgent suppression. Take somebody, let's just say you're supplementing the 6 or 800, you're taking them and you're making them zero again. Most men become incredibly symptomatic when you take their T to zero. That's part of the radiation sensitization that you need to do to treat a higher grade prostate cancer with radiation. Those individual men, I really will talk to them and say, look, I think we should do surgery for
you. Why? We can maintain your testosterone. We may not run you at 800. We may bump you down to let's say 400, but that's just me being comfortable as we talked about with the saturation theory. We're probably fully saturated at any of those levels. We can treat you as surgery, and as long as your pathology is favorable after surgery, you can continue with your testosterone supplementation
so that you can maintain your full body health, frankly. And I think more radiation oncologists are hesitant to restart exogenous T in somebody after what, six months or two years of ADT with their radiation because just for the listener, when you do radiation, you're not removing all the prostate tissue. So if you have any residual benign tissue in your prostate after radiation, which you're going to have, and you give back T, you may cause a false positive in terms of a recurrence for
that particular patient's tumor. So for those individuals, yeah, radiation can actually be more harmful because you're not able to supplement back up someone's low T to their normal range afterward, which of course not only happens in the man who we talked about who was hypogonadil before their diagnosis or before their treatment, but frankly, only 50 to 60 percent of men will
actually recover normal levels of T after two years of hormonal suppression anyway. So you're really talking about inducing more hypogonadism in those men than you would have even before. So given how much better radiation therapy is today than 20 years ago, I mean, in many ways, radiation therapy and surgical therapy have improved in parallel fashions over 20 to 30 years. The morbidity of both of them has gone down so much. The efficacy of both have gone up so much.
Is the bigger issue for you in helping a patient whose cancer is really amenable to either or? So we're not talking about patients that present with metastatic disease where there's a very clear direction they need to go in. And we're not talking about patients who are in a surveillance pattern. We're talking about that three plus four who could go either way, or sometimes the four plus four is your primary point of differentiation more around the androgen deprivation therapy than
it is the morbidity differences between surgery and radiation. In other words, do you feel that those kind of cancel each other out now given that both have come such a long way? I mean, they've definitely improved substantially. I think you put the whole picture together, but for sure it's at the top of the list in terms of the discussion as can we save this individual from systemic suppression of their testosterone levels, which have profound impacts on how they feel.
So for me, that's a critical component of the discussion. There's other subtle things about urinary function, sexual function, life expectancy, and so forth that we put into the equation, but it's definitely at the forefront of our mind. And that's why there's three ongoing NRG trials that really are looking at intensification and de-intensification of androgen suppression in these higher grade prostate cases that are treated with radiation in a way to expose fewer men potentially to
androgen suppression. Because we may find that there are tumors that look like an eight, but are actually on the inside not so aggressive and they don't need androgen suppression for as long or as aggressively as we previously thought. Ted, was there ever an adjuvant study that was done? I'll back up and explain why I'm asking this
question. The experience for breast cancer is completely different. So in breast cancer, when a woman has an ER positive breast cancer, even if it is completely amenable to surgical resection and it is removed, there is no evidence that the cancer has spread. She is still going to be placed on an adjuvant regimen of antiestrogen therapy. And just as the man who is placed on antianrogen therapy is going to experience pretty bad side effects. So to do the women who are placed
on antiestrogen therapy. So they are at a dramatic increase for osteoporosis. They go through basically menopause. And for many of these women, they're quite young and this can be quite morbid. Now the data suggests that that therapy does reduce the incidence of a recurrence, though it's not clear that it translates to a survival benefit. So there's a little bit of controversy there, although within that community, it doesn't seem very controversial. Most
oncologists I speak with are pretty adamant that that therapy be used. And again, they can point to the clinical trials that demonstrate a reduction in recurrence of cancer. Are there such trials that have been done in prostate cancer? Was there a day when status post radical prostate ectomy men were still put on antigen deprivation therapy as an adjuvant to basically see if that prevented recurrence? One of the big benefits that we have in the prostate cancer spaces,
we have this exquisitely sensitive biomarker, the PSA. So PSA was first described as a way to measure the efficacy of your treatment after you received it. So breast does not have that biomarker. So that's the big difference. And that's when people begin to try to compare as equals, as apples and apples, outcomes with breast and prostate, that analogy follows far short. Because for five years on average, I'm not an expert at impressed. They're on suppression. We don't do
that in prostate. So we can measure exquisitely if they have a recurrence. We're much more conservative about adjuvant therapy because we have this incredibly sensitive biomarker that detects whether or not there's a recurrence. So frankly, 100, 200 cells, you'll pick up something that low levels. And so we have ways to more aggressively deploy early salvage therapies. Yeah. So instead of just taking this bazooka approach, you can be a sniper.
That's right. So we have that luxury. And I think it's one of the great benefits in the prostate cancer space. Yeah. And so I think the hope here is if you're listening to this and you're a woman contemplating, you know, God, what if I develop estrogen dependent breast cancer? It's like, hopefully we see the acceleration of liquid biopsies that are going to be amenable to, again, looking at cell-free DNA as a way to monitor for recurrence so that breast cancer can take a page
out of the prostate cancer playbook and do more targeted therapy. And then basically, you would like to only have to give an origin deprivation to the women who need it and not to probably the 90 percent of women who don't. That's right. That's where all those cell-free DNA-based biomarker assays are really spectacular. And they're the newer ones are really look impressive for almost all cancers, but prostate where we just don't need necessarily to give that lily much more to be honest with you.
Well, Ted, this was great. I know this is a different format for us, but I wanted to give it a try. So I figured no better topic to do a mini drive than something is pointed as the specific role of testosterone and antigen receptors in prostate cancer. So Ted, thank you for taking time between cases today to sit down. Yeah, thanks for having me, Peter. Thank you for listening to this week's episode of The Drive. It's extremely important to me to provide all of this content without relying
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