Good morning, ladies and gentlemen. Thank you for standing by, and welcome to the Agenus TIGIT Deal Conference Call and Webcast. Please note this event is being recorded and may be used in future Agenus promotional material. I would now like to turn the conference over to John Medina, Director of Investor Relations. John, please go ahead.
Thank you, Stacy, and thank you all for joining us today. Today's call is being webcast and will be available on our website for replay. Also, for today's announcement, we have a very short slide deck available for those of you that are logged in. And for those that are coming in for the replay, that will be posted to our website later today. I would also like to remind you that this call will include forward looking statements, including statements regarding our clinical development, regulatory and commercial plans and timelines as well as timelines for data release and partnership opportunities.
These statements are subject to risks and uncertainties and we refer you to our SEC filings for more details on these risks. As a reminder, this call is being recorded for audio broadcast. Joining me today are Doctor. Garo Armen, Chairman and Chief Executive Officer. And also joining us during the Q and A are Doctor.
Jennifer Buell, President and Chief Operating Officer Julie Zasander, Vice President and Head of Business Development and Alliance Management and Doctor. Steven O'Dea, our Chief Medical Officer. Now I'll turn the call over to Garo. Garo?
Thank you very much, John, and thank you all for joining us today on short notice. I'll make a few brief remarks on what has already been articulated in our press release. This is a global licensing transaction which covers our bispecific Fc enhanced anti TIGIT antibody AGEN-one thousand seventy seven. This molecule was designed and developed by our team. We believe it represents a major breakthrough in the way the immune system engages with TIGIT in combating cancer.
Under the agreement Bristol Myers Squibb will become for the development and commercialization of AGEN one thousand seventy seven worldwide. Agenus will receive a $200,000,000 upfront payment and up to $1,360,000,000 in future development, regulatory and commercial milestones. In addition, Agenus is entitled to receive tiered double digit royalties on net product sales. Agenus will retain options to conduct clinical studies under the development plan to conduct combination studies with certain other Agenus pipeline assets. We believe we also have the right to promote AGEN-one thousand hundred seventy seven in The U.
S. The agreement is subject to clearance under the Hart Scott Rodino Act of 1976. As mentioned in our previous communications, we expect to file an IND with the U. S. FDA for AGEN-one thousand seventy seven in the next rather in the current quarter.
BMS intends to advance the research and development of AGEN-one thousand seven and seventy seven in immuno oncology for high priority tumor indications including non small cell lung cancer. Now let me take a minute to reflect on what does this mean for Agenus. We certainly expect today's announced collaboration will provide the means and serve as a catalyst to propel us through significant value inflection points this year. These inflection points include advancing balstilimab to approval and launch, number one. Number two, advancing our AGEN1181 into trials designed for rapid approval in major cancer indications such as colon cancer where we expect to detect significant benefit in patients who are otherwise unresponsive to immunotherapy agents or any other agent for that matter.
Number three, we also intend to advance our cell therapy programs for COVID and cancer under the AgenTus banner. Like AGEN one thousand hundred seventy seven for the anti TIGIT class, we believe AGEN1181 has the potential to be transformative for the anti CTLA-four class. Both compounds, that is AGEN-one thousand seventy seven and AGEN1181, represent significant Agenus innovations and discoveries from start to finish. Both were born at Agenus starting from preclinical science, next, antibody discovery, after which in vitro and in vivo modeling followed by application of our innovations in cell line development and exceptional manufacturing. All of these are critically important Agenus competencies which have given rise to our unprecedented IO pipeline and our ability to balance our portfolio between partner assets such as AGEN1777 and unencumbered assets such as AGEN1181, which as I said earlier, we expect to develop and commercialize ourselves.
I would like to end with a few comments about our latest collaborator BMS. While the competitive process for AGEN1007 involves several major biopharma companies, BMS' pioneering record and innovative capabilities in immuno oncology truly stand out. We have had the opportunity to discuss rapid clinical development pathways and strategies with them and we believe that they are the best positioned to advance our TIGIT bispecific antibody as a potential breakthrough treatment for the benefit of cancer patients. Before I turn the call over to, the operator for instructions, I want to remind everyone once again that the Q and A part of this call will have Jen Buell, President and COO Julie Desander, VP and Head of Business Development and Alliance Management and our Chief Medical Officer, Doctor. Steven O'Dea available for any questions.
Operator, if you could provide instructions for the Q and A session.
And our first question comes from Kelly Shai from Jefferies.
Hi, this is Hao calling in for Kelly Shi and congratulations and also thanks for taking my question. So my question is, are you expanding this FC enhanced franchise to other targets? And if so, what may be some of the targets that you are thinking about?
I don't think we can elaborate on all of the targets. But Jen, if you can take a crack at that question, that would be good.
Sure. Thanks for your question. What I will highlight, a molecule that is known to many of you is AGEN1181. And this is a next generation novel anti CTLA-four molecule. It also includes the Fc engineering that we've spoken about today related to our TIGIT molecule, AGEN1777.
We published these data in cancer cell and we'd be happy to share that with you. The molecule is advancing in clinical trials now actively and showing really interesting benefit across a host of tumors that we've shared with you at our last earnings call, including the molecules advancing in a Phase two study in patients with colorectal cancer. That's as much as we could talk about our Fc engineering and novel targets.
Thanks a lot and congratulations again.
Thank you.
Your next question comes from Mayank Mamtani from B. Riley Securities.
Good morning team. Congrats transaction and speaks volume to the quality of IO pipeline efforts you have underway. So maybe I have a few putting in context questions. So Garo, if you account for the upfront payment here and also some cash burn savings from an R and D standpoint that you had accounted for TIGIT, how should we think about your runway from here on out? Because that's an important question that we get asked by investors.
Could you maybe comment on that? Sure.
Mayank, as I said earlier, our key concentration areas will be the three that I outlined, which is advancing balstilimab to approval and commercialization. Very importantly as also Jen mentioned, advancing our eleven eighty one candidate very, very quickly to approval, in combination with balstilimab as well as along but particularly in combination with balstilimab because we have publicly elucidated that we've seen some very promising responses in these patients. We have not disclosed all of the responses received so far. But we're very, very driven by seeing that molecule to approval and commercialization. We do believe that that molecule perhaps in combination with belstilimab could be the basis for a blockbuster potential product particularly in cancers that we're not seeing much immunological advancement so far.
And of course, I made a very pointed statement in how we're going to take our cell therapy programs forward under the banner of AgenTus. So presumably if you interpret that under the banner of AgenTus, that will also impact our burn rate, in a favorable fashion. Now in terms of our burn, you know what our burn rate was for last year. I think going forward, we will manage our burn rate that about that number plus and minus some delta depending on the status of the programs and depending on our resources at any given point and our preferences of course. So, I don't expect to see major changes in our burn rate other than perhaps capital expenditures associated with putting up our new manufacturing facility which we will mitigate the burn by means of creative transactions So that too should not have a significant impact on overall burn.
Great. Thanks so much for that color. And then on the BMS, sort of how this fits in their IO portfolio, especially since they already have a TIGIT antibody. So could you maybe Jen, if you are able to comment on sort of how this kind of fits in their IOIO combination plans and obviously the landscape as a whole SC enhanced and SC competent and other aspects of engineering around this digit is also fast evolving. Could you just put in context some of the considerations that might have gone into
the deal? Let me just make a couple of comments and I'll turn it over to Jen. So it would be inappropriate for us to comment on BMS' specific plans. But suffice it to say that this deal has been the largest preclinical asset deal done in the last almost three years. So, that should answer part of your question, Mayank, in terms of why BMS may have decided to value this asset as highly as they have in spite of the fact that they have had their TIGIT antibody previously in spite of that.
Now, so notwithstanding any comments that we have made about BMS, or can't make about BMS because, we don't want to become presumptuous in, thinking for them. It's suffice it to say that we published, TIGIT data from our TIGIT bispecific that is very, very compelling. In fact we published data showing that our TIGIT bispecific is superior alone and even in combination with, other agents to any other TIGIT, that has been studied so far in preclinical models. So Jen, would you like to add to that?
Sure. I'll just a bit, Garo, I'll just say that we share certainly the excitement about the possibilities of this molecule. It's unique, it's differentiated, it provides what we believe to be potential for a superior blockade of tumor escape. And Bristol is very well positioned to create value given the complementarity of molecules in their portfolio.
Makes sense. And my final question, just quick one, on option to co promote, just curious if you do have also have an option get back into the core development aspects of the program before it gets commercialized. Like do you have an opt in right at a later stage development as part
of the deal?
I'll let Julie answer that question because she's the expert on the agreement.
Yes. Thank you for the question. We do have a right for both co development as well as co funding in exchange for an increased royalty rate in The U. S.
Excellent. Thanks for taking my questions.
Your next question comes from Matt Phipps from William Blair.
Hi, thanks for taking my questions and congrats obviously, Garo, on really delivering on what you said you would come here this quarter. So good work, congrats and excited about this deal. I'm just wondering if you can give me any additional details on how the mechanics work of running a trial with seventeen seventy seven with wholly owned assets given there is quite a bit of overlap with some of your pipeline assets and then obviously things Bristol is likely to try in combination studies?
Sure, Matt. Thank you. Julie, would you elaborate on that point as well?
Sure. Yes, we do have the right to run combination studies with seventeen seventy seven with other agents in our pipeline subject to certain restrictions. Those restrictions have not been publicly disclosed.
Okay. I guess when you think about the potential of seventeen seventy seven, do you think it's really driving deeper responses in patients that you would expect there that maybe we would expect to respond to TIGIT antibodies, what we've seen so far as a PD L1 kind of high population? Or do you think it's really expanding the number of patients who would benefit? Obviously, there's the lower affinity CD16 patients, but maybe some other things as well given the bispecific aspect of the small field.
Sure, Matt. Now we haven't as you know, we haven't disclosed the other arm of the bispecific. So hence we have to be careful not to release too much in terms of what we think the bispecific does in this context because we don't want others to be able to guess what that additional arm is. So with that caveat, Jen, if you can carefully address perhaps a part of what Matt is asking.
Sure. So what I would just emphasize, and I'm going to have Stephen O'Dea say a few words about this, is given the mechanism and the preclinical data, which we have already publicly presented in some format, we do see that the way that this molecule has been designed shows features in which it may have the benefit as a monotherapy as well as in combination with other checkpoint modulating antibodies like PD-one. And I'll ask Stephen to say a few words.
Yes. Thanks, Jen. Thanks for the question. Yes, as Garo said, obviously, there two components of 1,177. One is the bispecific nature and then of course the Fc enhancement.
And as Garo and Jen have said, there is we haven't disclosed and will not at this time disclose the partner on the bispecific. In terms of the Fc enhancement, obviously, it's an important piece of our platform, and we believe it's a value added to these antibodies. The field of TIGIT, obviously, specific antibodies, there's multiple products out there both in Fc competent, Fc silence and now our Fc enhanced approach. I think what we can say from the clinic is TIGIT is an important target for immune cells and TIGIT shares both T cells and NK cells in terms of its expression. And so, what we have seen at least to date with the Fc confident molecules is that they have activity, it seems to be not as monotherapy particularly or in combination in PD-one resistant settings, but in this PD-one naive combination setting with high PDL expressing patients.
So it is a more narrow group right now where the strongest signal is appearing. And obviously, there's great opportunity with both mono specifics that have Fc engineering theoretically to add to that ability to benefit patients. And obviously, this bispecific has additional quality. So more data in multiple molecules forthcoming and we look forward to being part of that with this molecule with BMS.
Thanks, Steven. I guess one last question. Some recent data with a active Fc but not enhanced Fc TIGIT antibody from IKEAS, they looked at kind of depletion of some of these high expressing TIGIT T cells including regulatory and CD8, but then the CD8s kind of didn't recover soon after dosing. That a kind of phenomenon that you would expect to see with seventeen seventy seven or is there some other pharmacodynamic measures you'll be looking for?
I think we have to be careful in answering that question. I apologize, Matt, because I think we're moving in a direction that will reveal information, that may start the guessing game as to what the other arm is. So I apologize, but I think we'll refrain from answering that part of the question.
Gary, we've all been doing the guessing game here for a while, but I guess we'll have to wait a little bit longer. Thanks for taking my questions and congrats again.
Thank you.
And there are no further questions at this time.
Well, you very much, Stacy and everybody else for your time on this call. And as always, we're happy to entertain questions in your subsequent calls to us. And we also look forward to updating you with additional advances in our portfolio. As you know, while this is a single asset deal, it is representative of the fact that we've had a very robust and productive innovation engine at the company and AGEN 01/1977, is yet another very important example of what our innovation out of our own, research and multifunctional efforts has been able to produce. So thank you very much for your perseverance with our company and we look forward to again in our future dialogue.
This does conclude today's conference call. Thank you for your participation. You may now disconnect.