Titan Pharmaceuticals, Inc. (TTNP) Q3 2017 Earnings Call Transcript
Published at 2017-11-09 18:52:05
Sunil Bhonsle - President and CEO Dr. Marc Rubin - Executive Chairman Dr. Kate Beebe - EVP and Chief Development Officer Brian Crowley - VP, Finance Jennifer Kiernan - IR
John Vandermosten - Zacks Scott Henry - Roth Capital
Thank you for holding and welcome to the Titan Pharmaceuticals Third Quarter 2017 Financial Results Conference Call. At this time, all participants are in a listen-only mode. There will be a question-and-answer session following today’s remarks. Please be advised that this call is being taped at the Company’s request and will be archived on the Company’s website starting later today. At this time, I would like to turn the conference over to Sunil Bhonsle, President and CEO of Titan Pharmaceuticals. Please go ahead.
Thank you, Amy, and thank you all for joining us. Welcome to the Titan Pharmaceuticals call to review financial and operational results for the third quarter of 2017 and recent business updates. Before we begin, I wanted to inform you that this morning, we filed our third quarter 2017 Form 10-Q with the SEC, and the press release issued this morning provides a summary of the results and it can also be found on our website titanpharm.com. Joining me on the call today from Titan are Dr. Marc Rubin, our Executive Chairman; Dr. Kate Beebe, our Executive Vice President and Chief Development Officer; and Brian Crowley, our Vice President of Finance. But before we provide an update on the Company and the summary financial results, Jennifer will review the required cautions regarding forward-looking statements. Jennifer, please?
Thank you, Sunil. I want to remind everyone that certain matters that will be discussed today other than historical information, may contain forward-looking statements within the meaning of Section 27A of the Securities Act of 1933 and Section 21E of the Securities Exchange Act of 1934. Such statements include, but are not limited to, any statements relating to our product development programs and any other statements that are not historical facts. Such statements involve risks and uncertainties that could negatively affect our business, operating results, financial condition and stock price. Factors that could cause actual results to differ materially from management’s current expectations include those risks and uncertainties relating to the commercialization of Probuphine; the regulatory approval process; the development, testing, production and marketing of our drug candidates; patent and intellectual property matters; and strategic agreements and relationships. We expressly disclaim any obligation or undertaking to release publicly any updates or revisions to any forward-looking statements contained herein to reflect any change in our expectations or any changes in events, conditions or circumstances on which any such statement is based, except as required by law. And now, back to you, Sunil.
Thank you, Jennifer. We will start the call with an overview from our Executive Chairman, Dr. Marc Rubin, followed by Dr. Kate Beebe who will provide an update on our product pipeline, and then Brian Crowley will summarize the financial results. I will close with a brief recap before opening the call for your questions. So, let’s get started. Marc? Dr. Marc Rubin: Thank you, Sunil, and thank you all for joining us today for a review of our business highlights for the quarter and an update on progress on our portfolio of products, based on our ProNeura long-term continuous drug delivery technology. I want to begin by addressing the decline in Probuphine revenue for the quarter. While we did certainly anticipate that the adoption of Probuphine for the year or so, post-launch would be a measured one, we were however very surprised and disappointed with the decline in its sales this quarter. Feedback from Braeburn as well as feedback from key opinion leaders indicates that patient access to Probuphine has been negatively impacted by issues related to the timing and level of reimbursement by third-party payers as well as requirements of the Risk Evaluation and Mitigation Strategy or REMS programs, as proscribed by the FDA. And as an example of the former issue, it can take weeks or even months for an insurance provider to approve coverage from the time of preauthorization claim is submitted. This kind of delay in receiving a much-needed and a potentially life-changing treatment is frustrating to both the patient as well as his or her health care provider, and it is especially disappointing in light of the ongoing national opioid epidemic. I do want to take a moment to address the changing landscape of treatment options for opioid use disorder. In the next several months, two companies have PDUFA dates for depot formulations of buprenorphine. Indivior is a company with monthly depot formulations and Braeburn with both weekly and monthly formulations, and both companies’ products received positive Advisory Committee votes last week, as you probably know. If approved, these products should continue to shift to the current treatment paradigm away from daily oral therapy and towards longer duration procedure-oriented treatments. We believe that this dynamic should have a positive effect on the acceptance and uptake of Probuphine as patients enter the maintenance treatment stage. Opioid use disorder is a chronic neurobiological disease requiring ongoing treatment, often for years. And so, we strongly believe that patients can benefit from transitioning to Probuphine for maintenance treatment. And of course, we continue to believe in the long-term medical value of and the prospects for uptake of the product. In light of the current sales of Probuphine to-date, we do expect that we will need additional capital by the second half of 2018 in order to continue advancing our ProNeura development programs. We are evaluating alternatives and potential pathways available to us including ex-U.S. partnering opportunities for Probuphine, possible collaborations for one or more of our ProNeura programs and financing strategies. Importantly, I want to assure you that in addition to these alternatives that I just mentioned and in addition to our discussions with Braeburn and with treatment providers that are aimed at a fuller understanding of the impediments to the uptake of Probuphine, the Board is actively assessing all operative and strategic business options available that can increase shareholder value. We will keep you informed. I now want to turn the call over to Dr. Beebe to provide additional details on our development programs including our efforts to secure approval and partnerships for Probuphine in Europe as well as our ropinirole implant for Parkinson’s disease and our early stage programs for the prevention of opioid use relapse and overdoes, chronic pain, type 2 diabetes, hypothyroidism and the prevention of malaria as well as other chronic disease settings. Kate? Dr. Kate Beebe: Thank you, Marc, and hi, everyone. As you know our portfolio is based on our proprietary ProNeura technology, which is designed to provide long-term, continuous drug delivery for up to 12 months. We remain optimistic and committed to the prospects of ProNeura across a diverse range of chronic diseases. First, let me start with an update on Probuphine outside of the United States. While Braeburn holds commercialization rights to Probuphine in the U.S. and Canada, many of you know that we retain rights to Probuphine in Europe and other territories. Our initial focus for Probuphine outside of the U.S. is in Europe, which is the second largest market for Probuphine-based products with sales representing about 10% of the $2 billion plus U.S. market. This week, on Monday, November 6, we submitted our Marketing Authorization Application or MAA with the European Medicines Agency. We have also continued our discussions with the Irish rapporteur and British co-rapporteur countries, who will be leading the review of our MAA. And we received scientific advice and support from both agencies for application. At the same time, we have continued to meaningfully advance discussions with potential commercial and development partners for Probuphine in Europe and elsewhere. And lastly, in October 2017, Titan received a notice of allowance from the European Patent Office for a patent covering methods and use claims for treating opioid dependence with a subdermal implant containing buprenorphine. Upon issuance, this patent is expected to provide protection for Probuphine in Europe into 2023. Now, in addition, if approved by the EMA, Probuphine will receive 8 to 10 years of data exclusivity from the date of approval. This means that potential competitors would not be able to reference the Probuphine data as part of a generic development program. Now, turning to our ropinirole implant program for Parkinson’s disease. The ropinirole implant is designed for the long-term, continuous delivery of ropinirole HCL for the treatment of signs and symptoms of Parkinson’s disease like stiffness, tremors, muscle spasms and poor muscle control. Ropinirole is a dopamine agonist, currently available in daily or more frequently dosed oral formulations for both the treatment of Parkinson’s disease symptoms and restless leg syndrome. In October, we treated the first patient in our Phase 1/2 trial of the ropinirole implant, and this study is progressing. The primary objectives are to characterize the pharmacokinetic profile of the ropinirole implants, to evaluate their safety and tolerability and also to explore potential signals of efficacy using established disease-specific assessment scale. Patients on a stable dose of L-dopa plus oral ropinirole will have their oral ropinirole switched to ropinirole implants for three months of treatment in the study. Initial data from the first cohort of patients is expected in the first half of 2018 and the study completion is targeted for the end of next year. This quarter, we also announced that we are collaborating with Opiant Pharmaceuticals on a feasibility assessment of a ProNeura-based subcutaneous implant to administer an opioid antagonist for the prevention of opioid relapse and over dose. Currently, the only FDA approved opioid antagonist for relapse prevention is a monthly depot instruction of naltrexone. Our goal will be to develop a product with at least a six-month duration that would allow patients to be opioid-free for a longer period, providing a greater window for long-term recovery and most critically relapse and overdose prevention. Relapse and fatal overdose among those with opioid use disorder is significantly higher than any other type of drug addiction. For example, as many as 91% of those in recovery will experience a relapse, at least 59% of those who relapse do so within the first week of sobriety, while about 80% relapse within a month after discharging from a treatment or detox program. The risk of a fatal overdose is at its highest during a relapse. Now, we’re also evaluating the feasibility of several other product candidates across a variety of different chronic disease indications for potential inclusion in our portfolio. Early non-clinical testing is being conducted for the development of a Kappa opioid receptor implant for the treatment of chronic pain. If successfully developed and approved, this would offer a potential non-addictive opioid analgesic for the treatment of crime pain. We are also actively working on formulation optimization and early in vitro testing for liraglutide otherwise known as Victoza for adults of type 2 diabetes. Titan also presented data from a non-clinical study on the use of its ProNeura subdermal implant for the long-term sustained delivery of liothyronine or L-T3, during a poster session at the annual meeting of the American Thyroid Association. The ProNeura implants continuously released L-T3 dose dependently for more than six months, providing important initial in vivo information for the potential development as a treatment of hypothyroidism. In addition, Titan, Southwest Research Institute and the Walter Reed Army Institute of Research or WRAIR are collaborating to evaluate the ProNeura platform for long-term prevention of malaria. In November 2017, the WRAIR presented encouraging non-clinical data from this collaboration during a poster session at the annual meeting of the American Society of Tropical Medicine & Hygiene, demonstrating sustained release of anti-malarial drug atovaquone and protection from malaria for up to 12 weeks. This program is being fully funded and conducted by WRAIR. These early stage product candidates will be prioritized and pursued as resources allow. Our ProNeura continuous long-term drug delivery platform holds great promise for the treatment of select chronic diseases for which maintaining consistent levels of a medication in the blood over long periods of time may offer safety or other health benefits. We look forward to updating you on continued progress as we develop our portfolio of ProNeura-based product candidates. Now, I will turn the call over to Brian. Brian?
Thank you, Kate. The summary of the financial results was provided in our press release this morning and details are available in the Form 10-Q filed with the SEC. At this time, I’ll just highlight a few items. In the third quarter of 2017, we reported approximately $40,000 in license revenue from royalties earned on net sales of Probuphine by Braeburn, compared with approximately $26,000 in the third quarter of 2016. Research and development expenses for the third quarter of 2017 were approximately $2.7 million compared with approximately $1.6 million for the third quarter of 2016, an increase of approximately $1.1 million. The increase in R&D expenses was primarily associated with increases in external expenses related to the support of our ropinirole implant program and expenses on other ProNeura product development programs. General and administrative expenses for the third quarter of 2017 were approximately $1.4 million compared with approximately $1.1 million in the third quarter of 2016. The increase was primarily related to increases in non-cash stock compensation and employee-related expenses, fees and expenses related to Horizon loan and other expenses. Net loss applicable to common shareholders in the third quarter of 2017 was approximately $4.2 million, or approximately $0.20 per share compared with a net loss of approximately $2.6 million or approximately $0.12 per share in the same quarter in 2016. At September 30, 2017 we had cash and cash equivalents of approximately $11.7 million, which we believe is sufficient to fund our planned operations through August of 2018. We are evaluating potential funding options, including, but not limited to partnering opportunities for Probuphine outside of the U.S., collaborations for one or more of our ProNeura programs, and various financing strategies. Now, I’ll pass the call back to Sunil. Sunil?
Thank you, Brian. While we are disappointed at the low numbers for Probuphine in the third quarter, we continue to believe that Probuphine has an important role in the treatment of opioid use disorder. The clinicians we have spoken with continue to indicate a desire to treat patients with Probuphine. And while the numbers are small, the patients appear to like the benefits this product can provide. However, the restrictive REMS program together with inadequate reimbursement to patients and their doctors from insurance providers has hampered adoption of Probuphine. We are in dialogue with Braeburn to fully understand and address the issues limiting Probuphine sales and as needed, establish new strategies to help advance adoption of the product. We will also be closely monitoring the treatment landscape as new, extended release and depot injections become available in order to identify the best position for Probuphine in the marketplace. We’re also pleased to announce that we filed the MAA for Probuphine with the EMA on November 6. And we also received a notice of allowance on a patent that will offer protection for Probuphine in Europe through 2023. Now, simultaneously, we continue to advance our other ProNeura-based products with the belief that this long-term continuous drug delivery platform can have significant advantages over current daily dosed chronic disease treatments. During the third quarter, we treated the first patient in our Phase 1/2 trial of ropinirole for the treatment of the signs and symptoms of Parkinson’s disease. And we began a collaboration with Opiant Pharmaceuticals on a feasibility assessment of a subcutaneous implant using our ProNeura technology to administer an opioid antagonist for the prevention of opioid relapse and overdose. Additionally, we are continuing feasibility evaluation and non-clinical studies in the areas of chronic pain with the Kappa opioid receptor agonist and type 2 diabetes with the currently marketed product. Lastly, we reported encouraging non-clinical data from our programs in hypothyroidism and in the long-term prevention of malaria. So, while we work rapidly to get Probuphine back on track, we intend to pursue these additional programs based on priorities and of course resources. Although we can’t go into all the details right now, I want to assure you that the Board and management are looking at all options for maximizing the value of Titan, both from the product portfolio and other strategic considerations. We look forward to reporting continued progress as we move forward. This brings us to the end of our formal remarks. And now, Amy, if you’re ready, we are ready to take questions from the call participants.
[Operator Instructions] The first question is from John Vandermosten at Zacks.
Good afternoon, everyone. Just first wanted to get a sense of Braeburn’s ability to get done what needs to get done. I am thinking maybe a larger partner might have had relationships or some other skills or experience that might have helped them do a little better. And I am wondering if you can perhaps point to a few things that may be are missing that could be there for getting Probuphine, deeper penetration of the product?
Thanks, John. Certainly, our focus right now is to understand the nitty-gritty details of why Probuphine lost momentum. Clearly, there was momentum building in the second quarter. And when we saw the results for the third quarter, it was very disappointing to see that that momentum was not carried forward. Now, it’s been only a few days since we have learnt of this progress. And so, we have started digging, we have started talking with clinicians out in the field to understand what are the issues. We have of course spoken with Braeburn to understand how they see it, and this is going to continue for a few days. So, I cannot give you specific answers now except assuring you that we really are getting involved in the details to understand this and come up with strategies that will provide the correct -- getting Probuphine on the correct track. That is really our commitment and goal, and that’s what we are attempting to do. I am sure that benefits everyone including Braeburn, but we will look forward to seeing how best to progress this from here on.
And Mike took over as CEO back in June, and I was wondering if maybe he has changed the strategy up, and every time there is a change in strategy, maybe there is a little slowdown or something until the new approach takes over. I was wondering if that might be part of it.
John, I mean, it’s certainly Mike and our conservations with Mike when he came in, clearly had intended to support Probuphine just as it had been previously. And their commitment to that product he felt was strong. Of course, it’s the only product they are currently marketing. Our dialogue with Braeburn, which is periodic, they always indicated that they continue to support Probuphine. So, in that sense, that’s all I can point out that that’s what they have indicated. Clearly, at the same time, the momentum was lost. So, how and why that’s the key parts we want to find out and we will.
Okay. And then, the licensing agreement with Braeburn, are there certain minimums that have to be met, to maintain the license -- or once they have it, and they have it and they can do whatever they want with it?
The licensing agreement does not have minimums in it. It does require them to actively market and support the product similar to other products that they would. So, it has some things but not specific to minimum. So, these are typical of the licensing agreements for new products, and that’s how it is.
Okay. And then, Canada, I know that they sublicense that tonight, I believe. Have there been any sales in Canada yet?
It has not being approved in Canada yet. I believe it’s sometime next year, in mid next year or so is what the date seems to -- that I recall for approval in Canada.
Okay. And then, just the last question is on R&D expense. As we’ve continued with the development programs, it’s come up a little bit, and I guess we should expect similar level to continue through the fourth quarter and on -- into next year?
To some extent, the third quarter included the start-up of parts of the ropinirole study, but also some of the expenses associated with filing the MAA that we just did in the beginning of November. So, preparation of these things took some extra expenses. We, of course, are very conscious of now the cash position we are in as well and what potentially we may see as revenues from Probuphine. So, we will look to contain our expenses within manageable levels. Key part, of course, is the ongoing clinical study for ropinirole, which we intend to pursue. And we will keep things in mind with other programs to make sure we stay within our budget. So, I would expect the fourth quarter research and development expense to be probably a little less than the third quarter, but not by a lot.
Sure, John. Thank you very much.
The next question is from Scott Henry of Roth Capital.
Thank you and good afternoon.
Hey, Scott. Glad you could join in.
Certainly. As you kind of survey the landscape to try to get a sense of what’s happening with Probuphine, what kind of feedback have you received from physicians? Is there a general -- is it demand not the issue and it’s more of the execution of getting reimbursement or just any feedback that you’re getting that you find interesting?
I mean, certainly, we have spoken with a handful of clinicians out in the field. We haven’t such -- not a large group yet. We are doing this and continuing to do this. What we do see is that patients who are treated like this product, that’s what they have indicated, they have indicated that patients that they believe would benefit and when they talk to them about it, they get a favorable response. So, it’s good from that standpoint, at least in the small numbers, positive feedback about the patients is very good. What frustrates the physicians is the length of time it takes to get the approvals. They give us examples where it goes from few weeks to few months. And they -- maintaining patient’s enthusiasm to switch to this treatment is not so simple when it takes that long. And so, these are the frustrations that the physicians talk about. How best to address that clearly has to also do with the insurance systems, and this should be addressed and will be addressed.
If I could just task another question. With regards to monetization of some of the pipeline products. So, the ex-U.S. rights, what sort of time table would you expect? I mean, obviously, you don’t know for certain, but do you think you could monetize something in the next six months or just any color you could provide?
Sure. I mean, obviously the progress along we have been pursuing Probuphine in Europe and the potential for establishing a partnership for that and we certainly hope that over -- in the next six months period that that is in place. Clearly, submitting the MAA is a major milestone. It starts a clock ticking in terms of acceptance, approval and all these things that come down the road. So, that is certainly something we are very eager and keen and interested in pursuing as rapidly as we can. Outside of that, you know we are collaborating in the early assessment with Opiant Pharmaceuticals with a antagonist implant for treating opioid disorder. And that the early assessment results from both the technical side which we are pursuing and the commercial evaluation that Opiant is doing will be available in the first half of next year. And I certainly hope that that will be a successful result that can lead into a potential program as well that has value, and shows substantial value added to Titan. So, those certainly are the early ones we have and obviously the WRAIR, the Walter Reed program going on, and we look for funding for that from the government. And if that’s available, that would be very meaningful. And we will look at other avenues including what NIH can provide for say the collaboration with Opiant and others.
The next question is from John Vandermosten at Zacks.
I just had a follow-up. Is there any way that the Opiant collaboration might get ahead of the ropinirole or T3 programs at all, just because it maybe has lot more focus or partner is eager to push it along?
That’s certainly a very timely program. It has -- there is a lot of potential to the epidemic opioid crisis right now. And funding for something like that, if it is made available by the NIH, it can certainly speed up that program tremendously. So, it’s our hope that that will be the case. But, it’s a meaningful program and is looked at that way by the medical community as well as NIH.
This concludes our question-and-answer session. Now, I’d like to turn the conference back over to Bhonsle for closing remarks.
Thank you, Amy. Thank you everyone for participating in this call today. I know, it’s not an easy one at times, but trust us, we are trying to accomplish a lot during this coming quarter and we will attempt to get Probuphine back on track. As always, we appreciate your ongoing support and we will provide periodic updates as we move forward. So, thanks everyone. Have a good day.
This conference is now concluded. Thank you for attending today’s presentation. You may now disconnect.