Corcept Therapeutics Incorporated (NASDAQ:CORT) Q4 2023 Earnings Call Transcript

Corcept Therapeutics Incorporated (NASDAQ:CORT) Q4 2023 Earnings Call Transcript February 15, 2024

Corcept Therapeutics Incorporated beats earnings expectations. Reported EPS is $0.28, expectations were $0.25. Corcept Therapeutics Incorporated isn’t one of the 30 most popular stocks among hedge funds at the end of the third quarter (see the details here).

Operator: Welcome to the Corcept Therapeutics Conference Call. At this time, all participants are in a listen-only mode. After the speaker’s presentation, there will be a question-and-answer session. [Operator Instructions] Please be advised, today’s conference is being recorded. I would like to turn the call over Atabak Mokari. Please go ahead.

Atabak Mokari: Hello, everyone. Good afternoon and thank you for joining us. Today, we issued a press release announcing our financial results for the fourth quarter and providing a corporate update. A copy is available at corcept.com. Our complete financial results will be available when we file our Form 10-Q with the SEC. Today’s call is being recorded. A replay will be available at the Investors Past Events tab of our website. Statements during this call, other than statements of historical fact are forward-looking statements based on our plans and expectations that are subject to risks and uncertainties which may cause actual results to differ materially from those such statements expressed or implied. These forward-looking statements are described in today’s press release and the risks and uncertainties that may affect them are described in the press release and in our annual report on Form 10-K or our quarterly reports on Form 10-Q.

Please refer to those documents for additional information. We disclaim any intention or duty to update forward-looking statements. Our revenue in the fourth quarter of 2023 was $135.4 million, an increase of 31% compared to the fourth quarter of the prior year. We expect our revenue growth to continue and are reiterating 2024 revenue guidance of $600 million to $630 million, compared to 2023 revenue of $482.4 million. Net income was $31.4 million in the fourth quarter and $106.1 million for the full year of 2023. Our cash and investments at December 31 was $425.4 million. I will now turn the call over to Charlie Robb, our Chief Business Officer, to provide a legal update. Charlie?

Charlie Robb: Thanks, Atabak. In March 2018, we sued Teva Pharmaceuticals to prevent it from marketing a generic version of Korlym in violation of our patents. The case went to trial in federal district court in September of last year. On December 29, the court found that Teva’s generic product would not infringe the two patents we had asserted against it. We believe the court’s verdict is wrong and is based on a misunderstanding of the law. Accordingly, we are seeking its reversal by the Federal Circuit Court of Appeals. It is impossible to predict exactly how long the appeal will take. Briefing will be complete no later than May. Our opening brief is due March 09. Teva will have up to 40 days after we file to respond. Our reply brief, closing the briefing cycle, will be due no later than 21 days after that.

These documents will all be publicly available on the internet at the PACER website. With briefing complete, the timing of oral argument and issuance of an opinion are entirely up to the court. Based on past practice, it’s reasonable to expect oral argument in the fourth quarter of this year and a decision early in the first quarter of 2025. If we prevail, Teva would lose FDA approval of its product, at least until the expiration of our patents in 2037. We are eager to advance this appeal. As has always been the case, we strongly believe that our position is the correct one. We are confident that the Federal Circuit, with its deep expertise in this area of the law, will agree. I will now turn the call over to Joe Belanoff, our Chief Executive Officer.

Joe?

Joseph Belanoff: Thank you, Charlie. And thank you everyone for joining us this afternoon. Atabak highlighted our strong commercial performance and the revenue guidance we have set for 2024. A few weeks ago, I had the opportunity to meet with our endocrinology team at our National Field Meeting. The enthusiasm about our prospects in hypercortisolism was palpable. We have the opportunity to help many more patients with Cushing’s syndrome. We are reaching a tipping point of sorts, with the medical field increasingly understanding that hypercortisolism is far more prevalent than was previously assumed. Our ongoing Phase 4 CATALYST study will reinforce this emerging understanding, and I believe this study will be a landmark in guiding the future screening and accurate diagnosis of patients with Cushing’s syndrome.

Catalyst is the largest clinical trial ever conducted to examine the prevalence of hypercortisolism in patients with difficult-to-treat type 2 diabetes. Its investigators are unquestionably the country’s top diabetologists. Today, we announced preliminary results from the first 700 patients enrolled. Those results showed a hypercortisolism prevalence rate of 24%, far higher than many in the medical community have believed to be the case in this population. This is a two-part study. The prevalence portion of catalyst continues to enrol patients. Those diagnosed with hypercortisolism can enrol in the treatment phase. The final results from the prevalence phase will be presented in a keynote session at the American Diabetes Association’s Annual Meeting in June.

The results of the CATALYST study will undoubtedly stimulate physicians to screen patients for hypercortisolism, and many more than are currently identified will be found. Corcept is well-positioned to help them. For more than a decade, we have invested in patient advocacy and education and patient support services that are all based on understanding the journey and needs of an individual diagnosed with hypercortisolism. Our team is proud of these programs, and we are prepared to help what we know will be a growing number of patients in the years to come. As the awareness and diagnosis of Cushing’s syndrome increases, we are working with a great sense of urgency to advance relacorilant. This sense of urgency comes from knowing that the compound has compelling efficacy without many of the significant side effects of Korlym.

All of our proprietary compounds, including relacorilant, modulate cortisol’s effects by binding to the glucocorticoid receptor, a receptor which is activated when cortisol levels are high. They do not bind to the progesterone receptor and, therefore, don’t cause some of Korlym ‘s most serious off-target effects. We are evaluating relacorilant for the treatment of hypercortisolism in two Phase 3 trials, GRACE and GRADIENT. We expect GRACE to serve as the basis for our NDA submission in Kuching syndrome and to build on relacorilant’s positive Phase 2 efficacy and safety data. Patients experience meaningful improvements in hypertension and glucose control, as well as the other signs of symptoms of Cushing’s syndrome in the Phase 2 study. Relacorilant did not cause progesterone-related side effects, including endometrial thickening or vaginal bleeding.

Relacorilant also did not cause drug-induced hypokalemia. Progesterone-related side effects and hypokalemia are leading causes of Korlym discontinuation. Relacorilant’s Phase 2 trial results were published in frontiers in endocrinology in July 2021. Our second Phase 3 trial in hypercortisolism, GRADIENT, is studying relacorilant’s effects in patients whose Cushing’s syndrome is caused by an adrenal adenoma or adrenal hyperplasia. Patients with this etiology of Cushing syndrome often experience a less rapid decline, but their health outcomes are poor, including a significantly higher risk of premature death. While we do not expect our NDA and Cushing syndrome to depend on efficacy data from GRADIENT, we do expect the study to provide valuable information about the treatment of an etiology of Cushing syndrome that affects many patients.

A biologist in a lab coat studying a culture of cells to find a cure for metabolic disorders.

It bears repeating that the first phase of our ongoing Phase 4 CATALYST study reinforces the findings from many smaller studies, indicating that hypercortisolism is far more prevalent than was previously assumed. The findings from CATALYST will be entirely relevant to relacorilant as it emerges. As I said, we are working with great urgency and we are on track to submit our relacorilant Cushing syndrome NDA in the second quarter. We are also studying relacorilant as a treatment for different types of cancer. Our most advanced oncology program is in platinum-resistant ovarian cancer, a lethal cancer with few useful treatment options. There is great enthusiasm among the investigators participating in our Phase 3 ROSELLA trial. Enrolment in the study will close shortly and data will be available by the end of this year.

The goal of ROSELLA is simply to replicate our positive Phase 2 ovarian cancer trial results. ROSELLA’s study design closely tracks our Phase 2 study with a planned enrolment of 360 women. Women enrolled in the study are randomized one-to- one to receive either relacorilant plus nab-Paclitaxel or nab-Paclitaxel alone. The primary endpoint is progression-free survival with overall survival of key secondary endpoint. We are conducting the study in collaboration with leading clinicians from the Gynecological Oncology Group, GOG, in the United States and the European Network of Gynecological Oncology Trials, NGOT Group in Europe. In our successful controlled Phase 2 trial, Relacorilant produced meaningful benefit to many women. While these women’s disease had progressed on two or more previous lines of treatment, including previous taxanes, Relacorilant appeared to resensitize their tumors to chemotherapy’s beneficial effects.

Those who received relacorilant intermittently, the day before, the day of, and the day after they received nab-Paclitaxel exhibited statistically significant improvement in progression-free survival and duration of response compared to the group who received nab-Paclitaxel monotherapy. Women in the intermittent relacorilant group also lived longer than those in the comparator arm. 29% of the patients who took intermittent relacorilant were alive two years after study start, versus only 14% who took nab-Paclitaxel alone. The addition of relacorilant enhanced the effect of chemotherapy, likely by blunting cortisol’s anti-apoptotic effect. Just as important, the women who received relacorilant plus nab-Paclitaxel, experienced no additional side effect burden compared to those who took nab-Paclitaxel alone.

The results from this study were published in the Journal of Clinical Oncology in June 2023 with an accompanying editorial. Results have been featured in podium presentations in the 2021 and 2022 European Society for Medical Oncology ESMO meetings and the 2022 American Society of Clinical Oncology, ASCO annual meeting. Leading gynaecological oncologists have told us that relacorilant’s potential benefits, improved progression-free and overall survival without increased side effect burden, would constitute an important medical advance and that relacorilant plus nab-Paclitaxel has the potential to become a new standard of care in women with platinum-resistant ovarian cancer. A second mechanism by which cortisol modulation may prove useful is by blocking an important tumor growth pathway.

Cortisol stimulation is a major reason why patients with prostate cancer treated with the widely prescribed androgen receptor antagonist Enzalutamide eventually experience resurgent disease. Deprived of androgen stimulation, their tumor switched to cortisol activity to stimulate grip. Our hypothesis is that adding a cortisol modulator to androgen deprivation therapy will close this tumor escape route. Our collaborators at the University of Chicago are enrolling a randomized placebo-controlled Phase 2 trial of relacorilant plus Enzalutamide in patients with prostate cancer, before these patients have had an initial prostatectomy. A third cortisol modulation mechanism seeks to treat tumors by enhancing the body’s immune response. Cortisol suppresses the immune system, which may blunt the effectiveness of cancer therapies intended to stimulate the immune system.

Our hypothesis is that adding a cortisol modulator to immunotherapies such as checkpoint inhibitors may enhance the effectiveness of these therapies. We are conducting a Phase 1b trial of relacorilant plus the PD-1 checkpoint inhibitor Pembrolizumab in patients with advanced adrenal cancer whose tumors produce excess cortisol. Pembrolizumab is rarely effective as monotherapy in treating this form of adrenal cancer. While each of our compounds being evaluated in clinical studies selectively modulates cortisol activity, they are not identical and they produce distinct clinical effects. Some cross the blood-brain barrier, others do not. Some perform best in models of solid tumors, others are more potent in models of metabolic disease. Some appear to be tissue-specific, others have more global effects.

These diverse qualities allow us to study a wide variety of disorders using the best matched compounds. One of these compounds, dazucorilant, has shown great promise in animal models of ALS, improving motor performance and reducing neuroinflammation and muscular atrophy. As you know, ALS is a devastating disease with a very poor prognosis and limited options to help slow its progression. Our DAZALS trial is a randomized double-blind placebo-controlled Phase 2 trial of dazucorilant in patients with ALS. The primary endpoint is based on the ALS functional rating scale. The speed of enrolment in DAZALS exceeded our expectations. Enrolment will close shortly with data available by the end of this year. Finally, I’ll turn to our program in NASH, a serious liver disorder that afflicts millions of people in the United States.

Miricorilant has demonstrated compelling early evidence as a treatment for NASH. Our Phase 1b dose-finding study found that patients who received 100 milligrams of Miricorilant orally twice a week for 12 weeks experienced a 30% reduction in liver fat, with improvement in liver enzymes, markers of fibrosis and key metabolic and lipid measures, including Homa IR, serum triglycerides and LDL. Importantly, miricorilant was also very well tolerated with no apparent GI side effects. We look forward to building on these promising results in our MONARCH study, a randomized double-blind placebo-controlled Phase 2b trial, now actively enrolling patients with biopsy-confirmed NASH. The primary endpoint of the study is reduction of liver fat, with NASH resolution and fibrosis improvement as key secondary endpoints.

In conclusion, we are extremely optimistic about the future of Corcept. Our Cushing syndrome franchise is built on a solid foundation, a foundation that is supported by scientific, medical and commercial expertise that we have been strengthening and honing for over 20 years. Our strong commercial results reflect that physicians are more regularly screening for hypercortisolism and underscore our ability to support them as they manage this complex disease. We expect the findings from our CATALYST study to help physicians better identify and treat patients whose difficult-to-treat diabetes is caused by hypercortisolism, a population whose Cushing syndrome too frequently goes missed or undiagnosed. Relacorilant has demonstrated tremendous promise as a treatment for patients with Cushing Syndrome, and we are on track to submit our NDA in the second quarter.

Beyond Cushing Syndrome, our development programs are generating increasing evidence that cortisol modulation has the potential to treat a wide range of diseases. Ovarian cancer, prostate cancer, ALS, and NASH are current examples. We have a broad and active research portfolio of many proprietary selective cortisol modulators with potentially very different clinical attributes. We will continue to invest in understanding these attributes and their potential therapeutic applications, and we will advance the most promising compounds to the clinic. Over the course of this year, we expect data from our GRACE, GRADIENT and CATALYST studies in Cushing Syndrome, our pivotal RASELA trial in ovarian cancer, and our DASL study in ALS. This is an exciting time for Corcept.

I appreciate the efforts and dedication of our more than 350 employees who are working hard to achieve the ambitious goals we have set for ourselves. Before we take questions, I want to take a moment to introduce Roberto Vieira, who joined Corsept a few years ago. Roberto, as President of our oncology division, is responsible for the commercialization of relacorilant in platelet-resistant ovarian cancer and the expansion of our oncology footprint. You’ll have an opportunity to hear more from him over the course of 2024. Operator, let’s proceed now to questions.

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Q&A Session

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Operator: [Operator instructions] Our first question for the day will be coming from Matt Kaplan of Ladenburg. Your line is open.

Matt Kaplan: Hey, guys. Thanks for taking the question. Just wanted to start off first with your reiterating your guidance of $600 million to $630 million for 2024. Can you give us a little bit more color in terms of, I guess, given the court’s recent decision on the Teva case, why you’re still confident and why you’re reiterating the guidance that you had given before the court’s decision?

Joseph Belanoff: Just one small point, but good to hear from you, Matt. Our guidance came after the court’s decision, but we are reiterating it here. Sean Maduck, who is President of our Endocrinology Division, will take this question.

Sean Maduck: Matt, thank you for the question. Our revenue guidance will always consider all the information that we have and our best estimates going forward. Our range includes a multitude of factors, including a potential Teva launch and its impact. We have reiterated the range of $600 million to $630 million because we’re confident in our ability to both grow our own business and to defend our market share.

Joseph Belanoff: Then in terms of, I guess, maybe for Charlie, a legal update, you said that you remain confident in terms of being able to win the argument as you appeal the court’s decision. Can you give us some more color in terms of where you think the court erred in this decision and why you think you’ll be able to reverse it?

Charlie Robb: Yeah. Unfortunately, Matt, I really can’t share our legal deliberations as we work through. Obviously, I’ve given the matter a great deal of thought, but what I can say is what will really matter, will be available to everyone as the brief says we file it. I’m really going to have to let them speak for themselves and we’ll shortly be submitting our brief and you and everyone can take a look at it then and that’s really the most I can tell you at this point.

Matt Kaplan: Okay. Fair enough. And then I guess congrats on the initial results in the CATALYST study, 24% prevalence of hypercortisolism. That’s higher than, I guess, we had expected. How does this translate? Help us translate this into potential market size and numbers of patients given that result?

Charlie Robb: Yeah, Matt, I’ll take that question. I think it’s just really critical for people to understand that many people thought that the answer to that prevalence rate was going to be zero or zero to a couple of percent. Now, that wasn’t borne out by earlier evidence. There were many studies over the last decade that indicated in this group of patients, patients who have otherwise refractory diabetes, difficult to treat diabetes, that the results were substantial. There were substantial groups of patients with that, but no one had ever attempted as large a study in the way we did it prospectively or frankly with the level of investigators who actually participated in this study. So I don’t know exactly how that is going to reflect in what the final prevalence turns out to be, but what I can tell you is that it’s substantially higher than what has previously been assumed.

What’s been previously assumed, I’ll remind you, because we said it many times on this call, there were about 20,000 patients who had Cushing syndrome and about half of them were cured by split surgery. It’s very clear to us right now that the actual overall prevalence for Cushing syndrome is considerably higher than that.

Operator: Our next question is from Xinwen Yang [ph] of Canaccord. Your line is open.

Unidentified Analyst: Hi, team. Congrats on the results and thank you for taking the questions from us. So we understand that when a patient stops taking Korlym, the cortisol levels begin to rebound within four to five weeks and the randomized risk growth in the GRACE study is 12 weeks. So how confident are we that a statistical significant difference in the changes of blood pressure would be observed during that 12-week window?

Joseph Belanoff: I’m not sure I really understood the question and so please tell me if in the end I haven’t answered what you said, but I think the question had to do with for patients who were successfully treated with Korlym, how long does it take for stopping for when you stop Korlym for their effects of the Korlym effects to rebound? And now remember, we’re talking at this moment about Korlym, not relacorilant. Our experience was much quicker than I think what I heard you said. Usually within a couple of weeks, we actually see rebound for patients who stop taking Korlym, which frankly is a compelling reason for the high adherence rate we see with Korlym is that when they stop taking their medicine, they get pretty much worse pretty quickly.

We actually expect the same sort of timeline with relacorilant is that. Obviously, the study will give us the results for that, but we think that we have a more than substantial length of time in order to see the rebound effect that comes from not taking relacorilant in the upcoming study.

Operator: And our next question will be coming from David Amsellem of Piper Sandler. Your line is open.

David Amsellem: Hey, thanks. So, I just had a few. So, I wanted to come back to the generic of Korlym and I get your comments. I guess I just wanted to get more color on the barriers to generic adoption that you think are in place. In other words, the specialty hub that serves all of these high touch points that are related to Korlym. Is that something that ultimately proves to be a barrier to generics and can you just talk about those dynamics? That’s number one. And then secondly, you’re talking about filing. I’m sorry, filing in the second quarter on relacorilant, but you’re also going to have top line data in the second quarter. So, that’s kind of a tight turnaround. So, can you just talk about that and why you’re confident you can file it so quickly?

And then lastly, are you going to be running any additional trials on relacorilant to tease out long-term health benefits? Can you just talk about additional clinical work you might do to support that product? Thank you.

Joseph Belanoff: Okay. So, three different questions in three different areas, David. Thank you. The first one, I’m going to point to Sean to talk about how we run our endocrinology business. Go ahead, Sean.

Sean Maduck: Yeah. No, thank you for the question. And your question was specifically around sort of what we believe to be barriers to entry and I’ll just say that this is not your typical pharmaceutical market and supporting Korlym patients is far more than just filling a prescription. And automatic substitution does not happen at a Walgreens pharmacy till like you see in a lot of these cases. We have a very high touch, tightly controlled model. Every prescription that is written kicks off multiple high touch support initiatives to ensure that both the patient and the prescribing physician have the optimal experience.

Joseph Belanoff: And the only other thing I’d add here is that we spent over 12 years growing this business and we’ve done that through the development of a deep understanding of the market and by building very strong relationships with providers. Korlym is a very promotionally sensitive drug and we have all the pieces go through the initial part of the process of education of a physician through the filling of that prescription.

Sean Maduck: Charlie, would you take the question about the NDA, please?

Charlie Robb: Sure. Just a little background for those who don’t know this process as I’m sure David does. A new drug application, which is what we’re going to submit for relacorilant and Cushing’s syndrome in the second quarter, really is a substantial document. It’s a lot of work and so that’s why David’s asking a very good question. But I think what people also may not understand is that much of the information and analysis that you submit in the new drug application stems from work that is done years before the last patient leaves the pivotal study. So think of all of the preclinical research that’s done, all of the Phase 1 trials, the drug-drug interaction studies, the manufacturing development work. All this makes up a really substantial part of the NDA submission to the FDA and we’ve been working on that for almost a year now.

So the reason we’ll be able to submit this so quickly is that a great deal of the work will be complete before the last patient leaves the great study and we will be ready therefore to file really promptly after that. That’s why we’re confident. Thank you, Charlie and Bill Guyer, who’s our Chief Development Officer, will answer the question about relacorilant and longer-term use.

William Guyer: Yeah, long-term data. So thank you for that question. So there’s a study that’s actually ongoing that we don’t talk about much, and it’s a long-term extension trial and so that is a study that is taking patients from our Phase 2 trial, they can roll into the long-term extension trial. GRACE and GRADIENT, when they completed those trials, they can roll into that long-term extension trial. At this point in time, we have patients out six years in that long-term extension trial. We’re going to continue that study throughout to continue to provide long-term data on the safety and efficacy of relacorilant patients with Cushing syndrome.

Joseph Belanoff: Thank you, Bill. Next question, please.

Operator: And our next question will be coming from Swayampakula Ramakanth of H.C. Wainwright. Your line is open.

Swayampakula Ramakanth: Thank you. This is R.K. from H.C. Wainwright. I have a few questions, so I’m going to kind of ask, if you don’t mind, one at a time. The first one is on the guidance itself. So you’re kind of guiding, if I take the midpoint, you’re guiding for like 27% increase from where we are now and then in ’23, you grew about 20%. So I’m just trying to understand the tremendous growth that you’re expecting from where you are now. So what is included in that? How much of that is price increase and in terms of market growth itself, where do you see that market growth coming from because in the fourth quarter, we didn’t see that jump — that quite rate compared to Q3.

Joseph Belanoff: I’m not, R.K., I think I got the question a little bit difficult to hear. Sounded as if what you were asking was you’d like to know what are the components of the growth that we see currently in the market and where we think it’s going in the future. So I think that’s about right. Now, it’s not let us know, but I’ll turn that over to Sean.

Sean Maduck: Yeah, no, thank you for the question. In terms of, I guess, the range I mentioned earlier, it takes in a multitude of factors and the biggest, obviously, right now is that we have more positions prescribing Korlym and more patients being prescribed from each position. Over the last year and growth that we see continuing, we’ve added new patients from both existing and new prescribers throughout the country and we’re really pleased with the result we’ve seen, been driven by improved field execution and we’re starting to see early returns from some of the investments that we’ve made, both on the salesforce side and on the disease education side. And one of the areas of growth on our business has been on the salesforce expansion.

I wanted to update you on that in terms of where that team’s at. Now we’re currently at about 70 clinical specialists and we’re continuing to add clinical specialists throughout the country. Our target right now is 100 and we’re unlikely to stop there and we’ll continue to add top talent as we find it throughout the country, but we believe that that expansion is going to also help drive growth.

Joseph Belanoff: Let me just sum that up for you, RK. More doctors prescribing and more patients from each doctor, it’s a trend which really got very strong towards the end of last year and we’re seeing it continue as we speak.

Swayampakula Ramakanth: Is there a price increase included in this?

Joseph Belanoff: Sorry, I couldn’t hear the question.

Sean Maduck: Is there a price increase included in this? There’s not an additional price increase included in the range for this year. We took a price increase on January 01 of this year, 9.49%. We realized about 6.5% of that, but there was no other price increase included in that number.

Swayampakula Ramakanth: Okay. And then on the diabetes population itself, I’m trying to understand a little bit more about how the catalyst data is going to help you out. So to start off, in terms of the percent of population, the diabetes population who are considered difficult to treat, can you give us a number? What percentage of the diabetes population is considered that? And then do you need to do, how do you plan to include that into your label? Is this going to be, do you need to file something or how does it work?

Joseph Belanoff: Yeah. So I think the answer, I think the first question you were asking, RK, was what percentage are difficult to treat diabetics and that’s specifically defined in the protocol, patients who have hemoglobin A1Cs despite having multiple treatments and optimal care. So those patients have been on all of the modern medicine. We’ve been told by our expert, the diabetologists.

Swayampakula Ramakanth: No, that doesn’t give percentage. That just defines who is considered that, but what percentage of population is that?

Joseph Belanoff: I’m getting there. The percentage of the population that, of diabetic population that’s considered to be in that group, difficult to treat diabetics is about a quarter.

Swayampakula Ramakanth: Okay. Thanks.

Joseph Belanoff: And the second question, Sean?

Sean Maduck:

35.05 [ph] :

Operator: And we have a follow-up question from David Amsellem of Piper Sandler.

David Amsellem: Yeah, just a follow-up. So to the extent that the two other generic, Sun and Hikma, enter the market later this year, does that change how you think about your sales expectations or does your $600 million to $630 million contemplate three generic entrants by the second half of this year? Thank you.

Joseph Belanoff: Our guidance includes all those scenarios. And I just want to state that we’ve been thinking about this for a long time and we’ve been prepared for this possibility since 2020. We have a plan in place and we will continue to revise that plan as we receive new market intelligence and as I said before, we’re continuing to invest in our Korlym business and we’re confident in our ability to both grow and protect the share that we have. But yes, all of those scenarios are included.

Operator: And our next question will be coming from Joon Lee of Truist. Your line is open.

Joon Lee: Thanks for the update, and for taking our questions. So 24% of the quarter of 30 million diabetics in the U.S. is an attractive opportunity, but with the Phase 3 grades not having hyperglycemia as an endpoint spelled out, represent a headwind to utilization of melacorlin in diabetics. Or do you think the data from the GRADIENT could be supported there? And also with the orphan pricing of Korlym or relacorilant be prohibited in the utilization and I have a follow up.

Joseph Belanoff: Yeah, Joon, I’m very glad that you asked the first question because it really gives us an opportunity to really clarify what the situation is. Bill, could you please take that one?

William Guyer: So yeah, for the GRACE trial, we have a primary endpoint blood pressure control and a secondary endpoint of glycemic control and so what we do is we have a hierarchy. When we meet our blood pressure control, we plan to then have that as our primary endpoint and therefore, we then move in that hierarchy to glucose control and we expect to meet both of those endpoints and we expect to have a robust response to both hypertension and diabetes control, as well as other comorbidities and based upon meeting all those endpoints, we expect a broad indication for miricorilant.

Joseph Belanoff: I think that’s really an important thing. I’m just going to emphasize that I don’t have anything different to say than Bill said. I want to just underscore that. Our anticipated label for relacorilant is to treat Cushing syndrome. There are many variables that we’re measuring in that and in the hierarchy, hypertension is at the top of the list, but glucose intolerance is on that list, as are many other endpoints that describe Cushing syndrome. It’s probably 20 different endpoints, because Cushing syndrome is a syndrome caused by excess cortisol activity. Cortisol goes everywhere in the body. And many things go wrong when people have Cushing syndrome. Now, you asked a really interesting question about price as we go forward and that’s — that really is something that we really have to think about, as the market enlarges and enlarges and enlarges and we don’t know, as someone I asked, I answered to an earlier question, exactly what the market size is, but we will certainly take all those things into account as we go forward.

One thing I want to just emphasize at this point is that we have not seen a single bit of influence yet from the catalyst information, not a patient. So it’ll be very interesting to see where that goes over time.

Joon Lee: All right, looking forward to the full data. And on generic, are you seeing any impact to Korlym since Teva was generic launch six, eight weeks ago and have you or do you plan to institute any new sales strategy in response to generic launch? Thank you.

Joseph Belanoff: I’m going to give you back to Sean for that question.

Sean Maduck: Yeah, no, June, thanks for the question. There has been no impact to our business since Teva announced its launch. We have seen no evidence of generic Mifepristone in the marketplace and we’re monitoring daily. And to your second question, I’m not going to go into any specifics, but again, we’ve been prepared. We have a plan in place and more to follow.

Operator: Thank you. There are no further questions in the queue.

Atabak Mokari: All right. Well, thank you, everybody. And look forward to three months.

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