Viking Therapeutics, Inc.
Q1 2021 Earnings Call Transcript

Published:

  • Operator:
    Welcome to the Viking Therapeutics’ 2021 First Quarter Financial Results Conference Call. At this time, all participants are in a listen-only mode. Following management’s prepared remarks, we will hold a Q&A session. As a reminder, this conference call is being recorded today, April 28, 2021. I would now like to turn the conference over to Viking’s Manager of Investor Relations, Stephanie Diaz. Please go ahead, Stephanie.
  • Stephanie Diaz:
    Hello and thank you all for participating in today’s call. Joining me today is Brian Lian, Viking’s President and CEO; and Greg Zante, Viking’s CFO.
  • Brian Lian:
    Thanks, Stephanie, and thanks to everyone listening on the webcast or by phone. Today we'll provide an overview of our first quarter 2021 financial results as well as an update on recent progress and developments with our pipeline programs and operations. During the first quarter, we continued to build on the progress made over the past year with both of our thyroid hormone beta receptor agonist programs. With our lead program VK2809 for the treatment of nonalcoholic steatohepatitis and fibrosis, we continued enrolling patients in our Phase 2b VOYAGE study and added new clinical sites in both the US and outside the US. During the first quarter, we also continued enrollment in a Phase 1 trial evaluating our second thyroid hormone beta receptor agonist VK0214 for the treatment of X-linked adrenoleukodystrophy or X-ALD. This trial is advancing well and we are nearing completion of this study's initial phase evaluating VK0214 in healthy volunteers. I'll provide additional detail on our development activities after we review our first quarter financial results. For that, I'll turn the call over to Greg Zante, Viking's CFO.
  • Greg Zante:
    Thanks Brian. In conjunction with my comments, I'd like to recommend that participants refer to Viking's Form 10-Q filing with the Securities and Exchange Commission, which we expect to file later today for additional details. I'll now go over our financial results for the quarter. Our research and development expenses for the three months ended March 31 2021 were $11.5 million, compared to $8.0 million for the same period in 2020. The increase was primarily due to increased expenses related to clinical studies, manufacturing for the company's drug candidates, salaries and benefits and stock-based compensation partially offset by decreased expenses related to preclinical studies.
  • Brian Lian:
    Thanks Greg. I'll now provide an update on the progress with our development programs beginning with our lead program VK2809. VK2809 is an orally available small molecule agonist of the thyroid hormone receptor that possesses selectivity for liver tissue as well as the beta receptor subtype. To date, the clinical studies have demonstrated compelling evidence supporting the potential of VK2809 in the treatment of multiple metabolic disorders, including NASH and fibrosis. Phase 1 studies in healthy volunteers, as well as in subjects with mild hypercholesterolemia have shown that treatment with VK2809 produces significant reductions in plasma lipids, including LDL cholesterol, triglycerides and atherogenic proteins. In addition, we previously completed a 12-week Phase 2 study in patients with non-alcoholic fatty liver disease, and hypercholesterolemia. This study successfully achieved its primary and secondary endpoint, with patients receiving VK2809 demonstrating highly statistically significant reductions in liver fat content, as well as improvements in LDL cholesterol. VK2809 also performed well on secondary measures demonstrating significant reductions in other plasma lipids such as triglycerides, apolipoprotein B, and lipoprotein A. Importantly, no serious adverse events were reported in this trial among patients receiving VK2809 or placebo. Initial data from this study as well as follow-up data have been highlighted in multiple oral presentations at key scientific meetings.
  • Operator:
    We will now begin the question-and-answer session. The first question will come from Steve Seedhouse of Raymond James.
  • Ryan Deschner:
    Hi, there. This is Ryan Deschner on for Steve Seedhouse. It might be a little early for this question, but in light of the recent FGF21 data in cirrhotic NASH. To what extent are you considering an F4 cirrhotic NASH study post Phase 2b data? And what data from the Phase 2b study would you be focusing on to aid in making that decision?
  • Brian Lian:
    Hi, Ryan, thanks for the question. At this point, we're not planning a cirrhotic NASH study. That would change of course depending on what the Phase 2b data look like. But it's not something that we're considering right now. I think we would base that decision on what the histology data look like on fibrosis after the 52-week treatment period. But at this point it's not in the works.
  • Ryan Deschner:
    Okay. Thank you. And one more quick question. I was wondering if you could give us any more detail on the structure and the size of the PoC study a proof-of-concept study in X-ALD.
  • Brian Lian:
    Yes. We haven't disclosed really the structure there. We will once the trial is initiated, but it will be a limited number of doses with a handful of patients in each dose and we'll get more detail when we initiate the study.
  • Ryan Deschner:
    Excellent. Thank you very much, Brian.
  • Brian Lian:
    Thanks, Ryan.
  • Operator:
    The next question is from Michael Morabito of Chardan Capital Markets.
  • Michael Morabito:
    Hi, team. Thanks for taking the call -- the questions. So I want to know the other studies that you've done for 2809 with the formulation in the hepatic impairment particularly. Should we expect to see that at medical meetings this year, either it's EASL or AASLD? And as a follow-on to the previous question the study in the hepatic impairment, do you think that that will lead to any additional clinical trials to expand the potential label of 2809?
  • Brian Lian:
    Hi, Michael, thanks for the question. No we're not planning to present those data at any upcoming conferences. It was really with the formulation studies they were really intended to develop a more commercial-friendly form and we have now great options with the soft gel and the tablet. With the hepatic impairment study that was just a requirement from FDA for everybody in NASH looking at -- trying to see if there are any safety risks or PK changes in patients with more severe hepatic impairment and we didn't see any. So we don't expect to have any limitations depending on -- or pending hepatic impairment. But we wouldn't be planning to present those at any of the upcoming conferences.
  • Michael Morabito:
    Okay. And just out of curiosity, you've mentioned the cash runway allows you to complete all of your planned studies. Does that runway include any additional studies that have not been mentioned or to move to initial studies what would be necessary from a capital perspective to say move into Phase 3 or advanced X-ALD into a Phase 2/3?
  • Brian Lian:
    Yeah, I can take that. The -- I think we've got enough runway to get through certainly a Phase 3 trial with X-ALD and well into if not fully through the biopsy endpoint in a Phase 3 trial with the VK2809.
  • Michael Morabito:
    Okay. Great. Excellent. Thank you very much.
  • Brian Lian:
    Thanks, Michael.
  • Operator:
    The next question comes from Matthew Luchini of BMO.
  • Unidentified Analyst:
    This is Jin on for Matthew. Congrats on the progress, and thanks for taking our questions. Two for me. So assuming that you guys choose to use a different formulation, following the formulation work like if you guys were to use a different formulation than what was used in VOYAGE trial? Is there any gating step before or moving on to Phase 3? And for VOYAGE data, what is your -- like what do you think you need to achieve to remain competitive in NASH? And I have a follow-up after that.
  • Brian Lian:
    Sure. Thanks, Jin. So the reason we did the study looking at different formulations. That's kind of the -- that was the study that we would plan to do sort of a bridging study to look at bioavailability differences that sort of thing. And so I think we've checked that box with -- what was the second question?
  • Unidentified Analyst:
    Is there a gating step for moving into Phase 3 regarding formulation? And what are -- what do you think you need to achieve in VOYAGE trial to remain competitive in NASH?
  • Brian Lian:
    Yeah. No, we think we've accomplished whatever gating step would be required with the formulation. We think the data that we've seen to date are pretty competitive. We think that's among the best, if not the best liver fat reduction from any oral agent. And so I think we're competitive. And if the Phase 2b data look remotely similar to the Phase 2a I think we would be competitive as an oral agent, particularly when you consider the profile with the broad effects on cardiovascular metrics LDL reduction triglyceride reduction, atherogenic protein improvements. All of those I think are very, very important in this population. And we don't have any pervasions in the negative direction on lipids that might cause polypharmacy to be considered right off the bat. So I think we're really, really competitive overall with the profile.
  • Unidentified Analyst:
    Okay. That's helpful. And my second question is, can we still expect data from Phase 1 SAD/MAD trial for 0214 first half this year? And for the PoC -- Phase 1b PoC trial if that were to start mid-year when can we expect the data?
  • Brian Lian:
    Yes. We've -- on prior calls we've talked about having some announcement describing the data in the first half. And I think we're still on track for that. With completion and announcement of data from the Phase 1b study it depends on how quickly that enrolls. It's difficult to project right now but we'll report the data as soon as it's available. I would anticipate that that's probably a 2022 event. But if we can do it sooner we'll report the data sooner.
  • Unidentified Analyst:
    Got you. thank you. I'll hop back into the queue.
  • Brian Lian:
    Thanks Jin.
  • Operator:
    The next question is from Derek Archila of Stifel.
  • Ben Porter:
    Hey. Thanks guys. This is Ben on for Derek. Thanks for taking my call. Two from us. Just building off that last question. Just on 214 in the Phase 1 study, have you thought any more about how do you present these data whether it's at your conference or just a PR of some sort? And then the second one from a modeling perspective, are there any qualitative comments you can share about kind of the OpEx ramp in 2021? Just in light of the 214 and 2809 studies on picking up? Thanks.
  • Brian Lian:
    You want to take that Greg?
  • Greg Zante:
    Sure. The second part, I'd say from an OpEx standpoint we'll probably going to be in the 50% to 70% increase range from last year. Just to give you some perspective on that.
  • Ben Porter:
    Okay.
  • Brian Lian:
    And with the data presentation, we'll have to see the data first before we make that decision. So, I think minimally, we would plan for press release and potentially then present more detailed data at a conference in the future. But I think press release is the first step there.
  • Ben Porter:
    Okay, that’s it for us. Thanks guys.
  • Brian Lian:
    Thanks Ben.
  • Operator:
    The next question is from Andy Hsieh of William Blair.
  • Andy Hsieh:
    Thanks for taking the question. So, one, looking at the new slide deck, Brian, I think we have more information about the gene expression analysis on 2809. Just curious maybe you can describe for us the findings. And just curious is that like a new study that you've done or basically kind of just a presentation of a previous study -- preclinical study before?
  • Brian Lian:
    Yes. Hi Andy, that was updated data from a study that we presented at EASL I believe in 2017 or 2018, one of those EASL conferences, the gene expression the RNA sequencing data. And we thought it was interesting because generally you see improvement in genes associated with insulin sensitivity and lipid metabolism and a suppression of gene expression for those genes associated with fibrotic signaling. So, I think by themselves maybe they wouldn't be as exciting. But when you look at the histology from the same study, we see a 70% reduction in liver fat content and we saw a 50% reduction in fibrosis in that study. So, really nicely corroborates what was observed on the histologic assessments there.
  • Andy Hsieh:
    Got it, okay. That's helpful. Thanks Brian. Another thing is about kind of the vaccine rollout more and more percentage of the population are getting the vaccine. So, just curious about both the X-ALD healthy volunteer study and also the VOYAGE study. Is there any sort of washout period that the participants have to go through? And also from a behavioral perspective, are you seeing kind of an increase of patients being more open to participating in clinical trials just given the fact that these are -- they are more -- they're fully vaccinated?
  • Brian Lian:
    Yes. And it's an interesting question. I am not aware of any restrictions on vaccine timing and screening or enrollment. So, you have to assume that many of the patients in the studies both the healthy volunteer and the VOYAGE study have received their vaccinations. We've heard no comments or problems. And with regard to the second question, I think that we are seeing maybe a little bit better environment now than in the November through February time frame, but still very, very challenging when you think about the general hesitancy given that we're right coming off the back of the pandemic now, and I think people are generally still pretty cautious about everything.
  • Andy Hsieh:
    Okay. Yes, that's helpful. Thank you very much and thank you for answering all my questions.
  • Brian Lian:
    Thanks Andy.
  • Operator:
    The next question is from Jay Olson of Oppenheimer.
  • Jay Olson:
    Hey, thanks for taking my question. Now that you've identified the second half of 2021 is target time frame for completing enrollment of the VOYAGE study. Does that mean that we should expect to see the 12-week interim analysis of MRI-PDFF in the first part of 2022?
  • Brian Lian:
    Yes. Hey, Jay. So we've always said that once we announce completion of enrollment that we would probably have the data on that primary endpoint ready for announcement 16 to 20 weeks later. So it's hard to give a specific time frame to it, but once we announce completion that's what I would think about. You treat the last patient for 12 weeks. It's another four to eight weeks for data cleanup and get things ready to announce. And I think that adds up to 16 to 20 weeks, four to five months something like that, but that's about as specific as we've been so far.
  • Jay Olson:
    Okay. Thank you. And then I was just curious about any read across you expect from MAESTRO-NAFLD-1 study that's going to read out by the end of the year. And if you could share your thoughts with us on the potential to follow a similar registration strategy?
  • Brian Lian:
    Well, I think both agents are following a similar strategy for NASH, which is the only indication I think that's out there right now for fatty liver disease with a registration pathway. And as far as the read through, I think, the overall the compounds look fairly similar on liver fat. So, at least from what we've seen with the early data from that compound. So, I wouldn't necessarily expect much difference from what we've seen thus far.
  • Jay Olson:
    Would you consider conducting a study with similar design to MAESTRO-NAFLD-1?
  • Brian Lian:
    At this point, no, but that could change but not at this point. We know from our Phase 2a study that the drug is profoundly active in that population. So it's not clear at this point what a Phase 3 trial might -- what new information at Phase 3 trial might generate for us.
  • Jay Olson:
    Okay. Got it. Thank you, Brian.
  • Brian Lian:
    Thanks Jay.
  • Operator:
    Next question comes from Scott Henry of ROTH Capital.
  • Scott Henry:
    Thank you and good afternoon. First for clarification, I just want to make sure I heard this correctly. Do you expect operating expenses to be up 50% to 70% in 2021 from 2020?
  • Greg Zante:
    Hey, there. I think Scott it's probably 50% closer to range. I mean, we were at about 43% last year and I had expected to go up and it's really all driven by our external spending related to our trials here.
  • Scott Henry:
    Okay. Perfect. Thank you for clarifying that. And then perhaps on a big picture type of question. When we think about VK2809 and potential partnership interest. Would you expect that to increase perhaps just after the 12-week data or do you think partners would be interested in also seeing the 12-month dosing data as you start to prepare for a Phase 3 program?
  • Brian Lian:
    Hi, Scott. Yes, it's a great question, and it's unclear, I mean, we know that some are very interested in the histology endpoints and confirmation that the mechanism is effective in this disease. But we also know that there is a lot of interest in our 12-week data from the ongoing study ahead of the second biopsy read. So I don't know it's always hard to predict partnering activities. But we do think there's a fair amount of interest in both of those time points.
  • Scott Henry:
    Okay, great. Thank you for the color.
  • Brian Lian:
    Thanks Scott.
  • Operator:
    The next question comes from Mayank Mamtani of B. Riley FBR.
  • Sahil Kazmi:
    Hi, good afternoon. This is Sahil Kazmi on for Mayank. Congrats on the progress and thanks for taking our questions.. Maybe starting first on 2809. Just a quick one on enrollment dynamics, could you talk to how you see it sort of shaking out by the end of the year in terms of US versus EU site split and then also F1 to F3 patients? And then just regarding the secondary endpoint of change in histology at 12 months, can you talk to some of the underlying assumptions? Is this something that's powered to show statistical significance?
  • Brian Lian:
    Yes. So we haven't disclosed the statistical assumptions there as far as the histology changes. We think we're adequately powered to show a benefit on NASH resolution. And as far as the enrollment contributions right now we feel that likely it's going to be a US heavy enrollment distribution relative to ex-US, but that could change. It just seems like Europe is a little bit behind the US with the emergence from the pandemic. As far as the breakout of fibrosis enrolled thus far, we really haven't talked about what we've seen on the demographics at this point. But we've said we can allow up to 25% F1s as long as they have another risk factor like diabetes obesity hypertension something like that that predisposes them to metabolic syndrome. But we haven't given breakouts on what we're seeing live.
  • Sahil Kazmi:
    Got it. That's helpful. And maybe as a brief follow-up could you provide any color on how you think the placebo effect or rather the effect size may be modulated in the context of the ongoing pandemic?
  • Brian Lian:
    Well the placebo effects the way we've always thought about it as on both NASH resolution and fibrosis. It seems to be in the mid-teens to low 20% range and that's been fairly consistent across most of these histology readouts. I don't -- I wouldn't expect the pandemic to really impact that significantly one way or another their histology reads. So, I wouldn't expect anything from COVID to really have an impact there.
  • Sahil Kazmi:
    Okay great. And then maybe just a brief one on 0214, I appreciate that you're going to disclose a bit more of the study details once we get closer to that Phase 1b. But if you could provide some qualitative color on is there going to be any background treatment allowed for these patients? And how you might use the study to enrich the patient population in the future? And then what you anticipate might be sort of the treatment window required to see a meaningful clinical benefit? Thank you.
  • Brian Lian:
    Sure. Well there's nothing approved right now for these individuals. So we don't really think that there's much need to control on the background therapies. We would expect the registration endpoints to be a little bit longer term 12 to 24 months focused on function. But that's based on prior Phase 2 and 2/3 studies that have been completed probably going to be focused on gate. But as far as enriching the population we'll have to see what the Phase 1b data look like before we discuss what the ideal target population is for Phase 3.
  • Sahil Kazmi:
    Great. Thanks a lot for taking our question. Congratulations on the project.
  • Brian Lian:
    Thanks a lot.
  • Operator:
    And this concludes our question-and-answer session. I would now like to turn the conference back over to Stephanie Diaz for any closing remarks.
  • Stephanie Diaz:
    Thank you again for your participation and continued support of Viking Therapeutics. We look forward to updating you again in the coming months. Thank you.
  • Operator:
    Thank you. The conference has now concluded. Thank you all for attending today's presentation. You may now disconnect your lines. Have a great day.

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