Sign in

Innate Pharma - Q3 2023

November 14, 2023

Transcript

Operator (participant)

Thank you for standing by, and welcome to the Innate Pharma third quarter 2023 financial results and business update. I would now like to welcome Henry Wheeler, VP, Investor Relations and Communications, to begin the call. Henry, over to you.

Henry Wheeler (VP of Investor Relations, Communications and Corporate Development)

Thank you very much. Good morning, good afternoon, and welcome, everyone. This morning, Innate issued a press release for our Q3 financial results and business update. We look forward to highlighting the progress made during the year to date, as well as addressing future goals and milestones. The press release and today's presentation are both available on the IR section of our website. On slide two, before we start, I'd like to remind you that we'll be making forward-looking statements regarding the financial outlook, in addition to regulatory and product plan development. These statements are subject to risks and uncertainties that may cause actual results to differ from those forecasted. On slide three, on today's call, we will be joined by Mondher Mahjoubi, our Chief Executive Officer. Then, we are pleased to welcome Sonia Quaratino, our new Chief Medical Officer, who will cover updates on lacutamab and monalizumab.

We'll then hand the call over to Yannis Morel, EVP of BD and Product Portfolio Strategy, who will then discuss our ANKET and ADC platform updates. We also have Frédéric Lombard, our CFO, on the line for Q&A. Mondher, I now hand the call over to you.

Mondher Mahjoubi (CEO)

Thank you, Henry. Good morning, good afternoon, everyone, and thank you for joining us on this call. Please move to slide four. Slide four is a reminder of our strategy. As an early clinical stage company, our business model centers around three key priorities, where we look to drive value from our early R&D efforts through later stage partnerships, where it makes sense to do so. Our ambition is to develop innovative drug candidates that contribute to transform cancer care through a strong pipeline of differentiated antibodies. Firstly, we look to create near-term value driven by our lead proprietary drug candidate, lacutamab, which is in clinical development for T-cell lymphoma, with updates coming at this ASH meeting, including final CTCL and early PTCL data.

As a reminder, our focus remains to leverage the value of our products as much as possible, which will further validate our science and offer capital that we can reinvest to advance our early R&D engine. We want to make sure that if we can gain valuable competencies via a partner agreement for lacutamab, we will consider that in our development plans for the product, as we look to later stage trials, as we have done in the past for other partnered assets. Second, we continue to fuel our pipeline and create longer-term value by leveraging our antibody engineering capabilities to develop innovative molecules with a primary focus on ANKET, our multi-specific NK cell engager proprietary platform. We are pleased to see continued progress, with Sanofi presenting various updates for the lead ANKET program, SAR443579, this year at ASCO, at ESMO, and also upcoming at ASH.

We also look to move our lead proprietary ANKET, IPH6501, towards phase 1 trial this year. Moreover, as we develop antibody targets for our ANKET platform, we recognize that some of these binders may be more suitable for antibody-drug conjugate therapeutics, and we announce some further updates in our ADC pipeline today. Last but not least, we are building a strong and sustainable foundation for our business with various partnerships across industry and academia. And here, our AstraZeneca partnership with monalizumab is progressing well in lung cancer. Before I hand over to Sonia, on slide five, you have a summary of our pipeline, which shows how we continue to translate our science into a robust portfolio of proprietary and partnered assets.

But it also illustrates how we are executing against our strategy with our lead proprietary assets, lacutamab, ANKET, and emerging ADCs, supported by partnered products with AstraZeneca, Sanofi, and Takeda from late to early stage development. We anticipate a series of potential clinical data readouts and catalysts in the upcoming couple of years as our R&D engine looks to leverage our scientific know-how to create sustainable business. I would like now to pass the call over to Sonia, who will review the progress made with our portfolio, starting with lacutamab, our most advanced proprietary asset. Sonia?

Sonia Quaratino (EVP and Chief Medical Officer)

Thank you, Mondher. On slide six, let me summarize the progress we are making with lacutamab, our anti-KIR3DL2 antibody. In T-cell lymphoma, we are pursuing a fast-to-market strategy for lacutamab in the niche indication of Sézary syndrome, where lacutamab was granted U.S. Fast Track Designation and E.U. PRIME designation in 2020. We have expanded past Sézary syndrome to mycosis fungoides, and we have seen encouraging preliminary data from our phase II trial in both diseases. For the Sézary syndrome, we announced early this month that final data is due at ASH next month, and we expect to have final data in-house for the mycosis fungoides later this year. Finally, we continue to enroll patients with refractory relapsed peripheral T-cell lymphoma in phase Ib with lacutamab monotherapy, and in a randomized phase II with lacutamab in combination with chemo, and some update will also be presented at ASH.

We announced earlier this month that the U.S. FDA placed lacutamab trial on a partial clinical hold due to one case of hemophagocytic lymphohistiocytosis in the TELLOMAK trial. We are currently undertaking efforts to address the FDA request and carried out an in-depth analysis of the HLH case, together with a steering committee with independent experts, which point to the fact that the case is related to the aggressive disease progression. On slide seven, we have the final efficacy data in Sézary syndrome that have been accepted for oral presentation at ASH.

The abstract details that in this heavily pretreated post-mogamulizumab patient pool, with a median number of six prior therapies, the global overall response rate was an encouraging 37.5%, as can be seen on the waterfall plot on the slide, and an overall response of 46.4% in skin and 48.2% in blood. We also observed a clinical benefit rate of 87.5% and the median progression-free survival of 8 months. It was very encouraging to see efficacy confirmed in the larger phase II trial in these late-line patients, together with a favorable safety profile. We look forward to sharing the full presentation at the ASH annual meeting in San Diego and sharing the data with the regulatory authorities. Next, I would like to update you on monalizumab, an asset we have licensed to AstraZeneca.

To remind you, monalizumab is an anti-NKG2A, which acts upon the checkpoint pathway to potentiate NK cells and activate tumor-infiltrating CD8 T-cells. On this slide, you can see an overview of the late-stage development plan for monalizumab in lung cancer. Building upon the data of the phase II COAST trial, AstraZeneca commenced PACIFIC-9, a phase III trial of durvalumab alone, or combined with monalizumab or oleclumab, an anti-CD73 antibody, as consolidation therapy for patients with unresectable stage III non-small cell lung cancer, who have not progressed after concurrent chemoradiation. The phase II COAST study had a similar study design to the PACIFIC-9. The result of an interim analysis after a median follow-up of 11.5 months were published in Journal of Clinical Oncology in 2022.

The results showed that the primary endpoint of confirmed overall response rate by investigator assessment was 35.5%, with durvalumab plus monalizumab, versus 17.9% with durvalumab alone. PFS was prolonged for durvalumab plus monalizumab versus durvalumab alone, with a hazard ratio of 0.42, and the 12-month PFS rate was 72.7% with durvalumab plus monalizumab versus 33.9% with durvalumab alone. The AstraZeneca-sponsored NEOCOAST-2 study is also underway in an earlier stage in lung cancer, evaluating monalizumab and durvalumab with chemo in the neoadjuvant setting. I will now hand over to Yannis to cover our ANKET and ADC platform.

Yannis Morel (EVP of Business Development and Portfolio Strategy)

Thank you, Sonia. On slide nine, I wanted to highlight our proprietary NK cell engager platform that we call ANKET. ANKET, standing for antibody-based NK cell engager therapeutics. ANKET is a versatile fit for purpose technology made of antibody building blocks that is creating a new class of multi-specific engager to induce synthetic immunity against cancer. This technology platform, which is leveraging our scientific expertise in the NK cell space, is an engine for us to create a series of drug candidates addressing multiple tumor targets. The backbone of the ANKET platform consists in the unique engagement of the activating NK cell receptors, NKp46 and CD16 on the NK cells, which allows for optimal harnessing of the NK cell functions. In addition, this mechanism can be further increased by the addition of the IL-2 variant, in order to induce NK cell proliferation.

On slide 10, I wanted to share our enthusiasm for this platform. As you can see, our pipeline of ANKET molecule is significantly growing, with Sanofi having now licensed three molecules, with two of them in the clinic, and having an option on two other undisclosed targets. Also, our most advanced proprietary ANKET, IPH6501, which is targeting CD20 and is armed with an IL-2 variant, has cleared IND and is currently starting phase I. In addition, we have several proprietary pre-clinical programs against multiple targets. On the right panel, you can see the detailed mechanism of action of the ANKET molecules, which we have published in a couple of articles in high-impact journals. Our Nature Biotechnology paper, published in January this year, described the joint work with Sanofi on the CD123 NK cell engager, IPH6101, or SAR443579.

SAR443579 is a co-engaging NKp46 and CD16 on NK cells, and therefore triggers potent antigen-dependent killing of AML tumors, as well as production of key cytokine for the anti-tumor immune response, but without inducing the systemic cytokine release, which is a dose-limiting feature of the T-cell engagers. Moreover, we have shown in our Cell Reports Medicine paper that the incorporation of an IL-2 variant into an ANKET induce a preferential NK cell proliferation within the tumor microenvironment, increasing therefore the number of anti-tumor effector NK cells. On slide 11, you can see an overview of the clinical data presented this year at ASCO and ESMO, and also the abstract that has been accepted for presentation at this year's ASH meeting for the CD123 ANKET program, also named SAR443579.

In the ASH abstract, we were encouraged to see further single agent activity and safety for the SAR443579 in relapsed refractory AML patients. Additional complete responses were observed, with now five complete responses out of 15 patients treated at the 1 mg per kg dose levels. SAR443579 was well tolerated at dose up to 6 mg per kg, with no dose-limiting toxicity observed, and only two grade 1 CRS observed out of 43 patients. We look forward to the full presentation at ASH. In the ESMO update, two of the complete responders previously reported at ASCO remain in remission after eight point eight and 12.2 months after treatment, highlighting the durability of these responses. The FDA awarded SAR443579 Fast Track Designation in May, and Sanofi plans to evaluate further dose levels. We look forward to further updates from Sanofi in due course.

On slide 12, you can see a summary of our Sanofi alliance. In 2016, we signed an initial agreement for two ANKET molecules, up to worth up to EUR 400 million in milestones, among which we announced EUR 16 million to date. Both programs have progressed with SAR443579 and SAR514 now in phase I clinical trial. In December last year, we signed a further agreement whereby Sanofi licensed the IPH62 ANKET program, targeting B7-H3, a solid tumor target, with an option on two other undisclosed targets. Sanofi paid EUR 25 million upfront, with a EUR 1.35 billion in total milestone plus royalties. This now takes the total milestone package of our collaboration up to EUR 1.75 billion plus royalties. We look forward to working with Sanofi as we bring this new ANKET to the clinic. Slide 13 highlights our growing ADC pipeline.

As we continue to develop next generation therapeutics utilizing our antibody engineering platform, we find that for some tumor targets, we can generate antibodies more suited for ADC than for ANKET, especially when they show good internalizing properties. Our agreement with Takeda in the field is providing a validation to this research approach, and highlights our capability to generate differentiated ADC candidates. On slide 14, I wanted to give you some more details on our Nectin-4 targeted ADC, IPH45, as we prepare the IND. We have selected an antibody targeting a unique epitope, which is not competing with the one of enfortumab vedotin, or PADCEV, and we are using a Topo I payload with a stable and hydrophilic linker. These key scientific attributes for IPH45 translate into features that we have that have the potential to maximize the Nectin-4 opportunity across various solid tumors.

First, in preclinical models, IPH45 has demonstrated a larger therapeutic index and a longer PK compared to enfortumab vedotin, which could improve the dosing regimen and aim at a better safety profile in patients. Second, as shown on the graph on the right, IPH45 shows strong antitumor efficacy in preclinical in vivo model resistance to enfortumab vedotin, suggesting that IPH45 could be active in patient refractory or relapsing after EV or other MMAE-based therapeutics. Last, the bystander effect of the topo I payload selected, together with the increased therapeutic index, suggests that IPH45 could address multiple tumor types across various Nectin-4 expression levels. Altogether, IPH45 has a unique profile with promising preclinical data that could translate into better patient outcomes across indications and lines of treatment. I will now turn to Mondher for a summary.

Mondher Mahjoubi (CEO)

Thanks, Yannis. Please move to slide 15, where we highlight the updates we are looking forward to at ASH in a few weeks' time in San Diego, where we will share the lacutamab updates, and Sanofi will present SAR443579 ANKET updates. We also plan to host a KOL call on site during the conference, and we look forward to further discussing the lacutamab data with you. So let me summarize now, and maybe if you move to slide 16, you are maybe familiar with this slide. We continue to work diligently to execute across all our strategic pillars, and we believe that we are laying the foundation to drive near and long-term value. Looking at our clinical program, we expect to achieve a number of milestones over the next two years.

As you've heard from Sonia, lacutamab phase II TELLOMAK, final Sézary syndrome and MF data is due at the end of this year, in addition to initial PTCL data. In parallel, we continue to develop our ANKET platform, further reinforced by our partnership with Sanofi, and we are very encouraged by the initial clinical data presented at congresses this year, and the IND clearance for our proprietary ANKET, which is progressing toward the clinic. We believe that this represents a natural evolution of our platform. Last but not least, for monalizumab, the lung cancer trials are underway, and we continue to advance the adenosine pathway agents in the clinic, where the phase two for IPH5201 in early lung cancer is underway. Let's move to the conclusion slide, please. As you can tell, we continue our exciting journey at Innate.

We look to build our business to create value for patients and stakeholders. In summary, we have positioned Innate Pharma for the future with our strategy and made meaningful progress across all three strategic pillars. With our R&D engine and antibody engineering expertise, our science is producing more candidates to progress to the clinic. So we are developing some alone, and some partnered. We have a focus on our NK cell engager platform, ANKET, as well as antibody-drug conjugates. But in parallel, our late-stage portfolio continues to advance, and as we look to maximize the late-stage portfolio assets of both lacutamab and monalizumab. Second, our partnership strategy continues to evolve, with the Takeda deal adding to those of AstraZeneca and Sanofi. Finally, we continue to carefully manage our resources, so we can continue our sustainable business and invest in progress in our pipeline.

I'm very pleased that we continue to have a strong cash position, with a runway into the second half of 2025. So collectively, we are driving value across our business and finally, advancing our goal to deliver innovative medicine to patients. We look forward to keeping you updated on our progress. That concludes our prepared remarks. We will now open the call to questions.

Operator (participant)

At this time, I'd like to remind everyone, in order to ask a question, press star then the number one on your telephone keypad. We'll pause for just a moment to compile any questions. Again, if you'd like to ask a question, please press star one on your telephone keypad now.

Henry Wheeler (VP of Investor Relations, Communications and Corporate Development)

Operator, can we, can we take the first question, please?

Operator (participant)

First question comes from the line of Daina Graybosch with Leerink Partners. Please go ahead.

Rabib Chaudhury (Equity Research Associate)

Hi, this is Rabib on for Dana. What is your view of SAR443579, or IPH6101 dosing profile to date? And how do you think that reads through to the ANKET platform more broadly? Thank you.

Mondher Mahjoubi (CEO)

Thank you. Probably Yannis is the best person here to answer the question about the dosing profile for 61, and beyond that, of course, the rest of our ANKET drug candidates.

Yannis Morel (EVP of Business Development and Portfolio Strategy)

Yeah, the data that have been presented by Sanofi up to date at the ASCO, but also more recently at the ESMO, show that the clinical responses were observed at the cohort where the maximum dose was 1 mg per kg. The ASH abstract also report additional response at 1 mg per kg, but not at higher doses. This suggests a potential bell-shaped effect on the drug. And like you can see in the abstract, more details on that should be presented at the ASH meeting. But if you look back at the ESMO presentation, there were blast reduction at all doses tested.

What it tells us is that we may, for, I mean, on a target per target basis, you know, because a multispecific engager is binding on one side to the tumor, but on the other side, on the NK cells, you may adapt the dose, in the phase I, from one target to the other. But, you know, it's not something that is unusual. There has been also some example recently, for example, with the tarlatamab from Amgen, where the 10 mg flat dose showed better results than the 100 mg flat dose in small cell lung cancer.

Mondher Mahjoubi (CEO)

Thank you, Yannis.

Operator (participant)

Our next question comes from the line of Yigal Nochomovitz with Citi. Please go ahead.

Carly Ackerina (Investment Relationship Officer)

Hi, team. This is Carly on for Yigal. Thanks for taking our questions. For lacutamab, we wanted to, to get your latest thinking on the next steps for CTCL. I think in the past, you've talked about the potential for the Sézary cohort to support an accelerated approval pathway. So just curious if that's still part of the plan, and then what different scenarios could look like for mycosis fungoides as well, in terms of future studies? Thank you.

Mondher Mahjoubi (CEO)

Yeah, I'm gonna take the question. So as you know, our aim is to pursue the development of lacutamab beyond the Sézary syndrome. The mycosis fungoides cohort in the TELLOMAK trial is a signal detection study because we didn't generate previously data outside Sézary syndrome. So this is, you know, the first prospective controlled phase II study to generate additional data outside Sézary. And of course, our main goal is to make sure that lacutamab gets to the patient who needs it as quickly as possible.

It's clear that in the Sézary syndrome, given, you know, the orphan drug designation or, of course, the fast-track designation, as well as the prime designation in Europe, there is a significant unmet medical need, especially in those patients who are, you know, progressing after two prior lines of therapy, especially after mogamulizumab. And clearly, the interim data that we are generating and about to present to ASH will be discussed with the FDA in terms of potential suitability for accelerated approval, and also the confirmatory phase three strategy, building, as I said, on the existing Fast Track and Orphan designation. As you know, our business model, of course, is clear.

Further development and registration of this asset is something we intend to progress via partnership, leveraging the capabilities and expertise of a partner in an area that we do not have existing capability of expertise. This will allow us to focus on our proprietary and innovative portfolio, and we will provide you updates as and when we can, and trust that you understand the sensitivity on any potential partnership prior to formal announcement. I also know that in our discussion with the FDA, we will certainly discuss about the confirmatory phase three trial, which of course will be including not only Sézary, but clearly other form of CTCL, in particular, mycosis fungoides.

Carly Ackerina (Investment Relationship Officer)

Okay, got it.

Mondher Mahjoubi (CEO)

I hope I answered your question.

Carly Ackerina (Investment Relationship Officer)

That's very helpful. And then-

Mondher Mahjoubi (CEO)

Okay.

Carly Ackerina (Investment Relationship Officer)

Yes, yes. Perfect. Thank you. And then just a follow-up question, maybe on the Nectin-4 ADC program. Seems like you think there's potentially an opportunity in the post-PADCEV setting here. Just wondering if you could talk a little bit more about early thoughts on the development strategy, and then just timelines for bringing that into the clinic. Thank you.

Yannis Morel (EVP of Business Development and Portfolio Strategy)

Yes, indeed, by actually switching the class of payload and going after a topo I inhibitor, we are seeing some pretty good efficacy in preclinical models after PADCEV, and in, I mean, in models that are resistant to PADCEV. And what is also encouraging for this approach is that there are some reports in the literature showing that patients who are relapsing or to PADCEV are not losing the expression of the antigen. So the antigen is still there, but it's more a mechanism of resistance against the payload that is developing within these patients. So this is clearly one path that we at some point would like to explore in our clinical development plan.

But it's not only the only one, as the Nectin-4 can be also expressed in several other solid tumors that are so far showing pretty limited activity with the PADCEV, and this leveraging the wider and larger therapeutic index of our compound. And in terms of timing, yeah, we are actively working to file an IND next year with this one.

Henry Wheeler (VP of Investor Relations, Communications and Corporate Development)

Thank you.

Carly Ackerina (Investment Relationship Officer)

Thank you for answering the question.

Operator (participant)

Again, as a reminder, the floor is now open for your questions. To ask a question at this time, please press star one on your telephone keypad. Our next question comes from Arthur He with HC Wainwright. Please go ahead.

Speaker 8

Hey, everyone, this is Arthur Ong for Arcade. Thanks for taking my question. So I just wonder for the 579 data at the ASH, could you give us more color on the safety side, especially for that grade fouce case, grade 4 neutropenia? Could you give us more color on that?

Mondher Mahjoubi (CEO)

So I'm not sure I'm getting the question right. So far, actually, based on the abstract, the safety profile of 579 or IPH6101 was reported as favorable. There were one grade 4 neutropenia, but we don't have details more than what is in the abstract, so clearly something to ask when the data will be presented at ASH in a couple of days. But a reminder, those are heavily pre-treated patient, median number of prior line of therapy. Most of the patient received venetoclax. A significant number went through stem cell transplantation, and this is, of course, interesting to better understand the reason of this grade 4 neutropenia, whether it is disease related or drug related.

Speaker 8

Thanks for that. My second question is, I'm just curious, when you are evaluating different binder which is suitable for the ANKET or versus the ADC platform, what kind of a criteria or selection preference for each side? Just curious from your perspective. Thanks.

Mondher Mahjoubi (CEO)

I'm gonna hand over to Yannis to give you a more detailed answer, but as we explained in the past, of course, some of the binders are more suitable for ANKET. The ones that internalize actually are by design favorable candidates for the ADC. But Yannis can give you more color on our thinking on how we select those binders.

Yannis Morel (EVP of Business Development and Portfolio Strategy)

Yes, it's but it's obviously a target-by-target discussion, because you know that some targets do have this property to internalize and some do not. And depending on the structure, this property of the target, the structure, and the ability to generate binders that are hitting the target at different epitope, we can generate binder that are rather staying at the cell surface and are pretty good candidate for ANKET molecule, and other that do internalize, and this we are screening that in vitro with pretty classical methods that are widely used by people developing ADCs. And we are checking the ability to induce the direct killing based on the expression level of the target.

So there are also many more parameters that we are taking into account, like the medical need, the development path, and the potential opportunity for this molecule. But in terms of antibody characteristics, this is really one we are using in one of our early filters.

Speaker 8

Oh, thanks. Thanks for taking my question.

Operator (participant)

Our next question comes from the line of Liisa Bayko, with Evercore ISI. Please go ahead.

Jamie Easton (Senior Managing Director and Head of Communications & External Affairs)

Hi, this is Jamie in for Liisa. Thanks for taking our questions. So, I have two questions. So one is, maybe I've missed it in the prepared remarks, but can you give us an update on your clinical hold for lacutamab? And then my second question is for your PTCL update at ASH. What will be an appropriate benchmark for this data? Thank you.

Mondher Mahjoubi (CEO)

Okay. The first question is about lacutamab clinical hold, you said? I think, and, probably it's time-

Jamie Easton (Senior Managing Director and Head of Communications & External Affairs)

Yes

Mondher Mahjoubi (CEO)

and the opportunity for Sonia to provide an update on the partial clinical hold for lacutamab. And then I'll take the question on PTCL. Sonia?

Sonia Quaratino (EVP and Chief Medical Officer)

Certainly. As mentioned before, the FDA placed the partial clinical hold due to one case of HLH that was reported in one subject. We, of course, intend to lift the partial hold as soon as possible, once the FDA requests have all been satisfied. However, this clinical hold or partial hold does not impact the TELLOMAK timelines, because the recruitment in both mycosis fungoides and Sézary have been completed, and the final data are imminent. And for the PTCL, we have also recruited the, let's say, first cohort of patients, and we are making an interim analysis of the data.

I have to remind that this HLH case that has been highlighted in the TELLOMAK trial is indeed related to a transformation of the Sézary into a large cell lymphoma. As you probably know, HLH is commonly reported as a complication of cutaneous T-cell lymphoma.

Mondher Mahjoubi (CEO)

Thank you, Sonia. So for the second question, so let me first maybe go back a few years ago when we finished phase I. At the time, we didn't have data outside Sézary syndrome. Most, if not all the patients included in the phase I program had Sézary syndrome. And of course, the obvious question, we are excited, and we are still excited by the signal we've seen in Sézary patients, but the main question was to see whether there is activity outside Sézary. And the logic next step was to go in cutaneous T-cell lymphoma outside Sézary and test the drug in mycosis fungoides. That was the priority number two, and that's what we will be communicating at the end of the year. As we said, we are on track to have the final data in-house in mycosis fungoides.

From the data published, the interim data published last year and updated even recently this year, we are confident that the signal is present actually when KIR3DL2 is expressed. And that hence the potential for lacutamab to be used in the treatment of peripheral T-cell lymphoma. I remind you that almost half of the patients with PTCL do express KIR3DL2. We are running two trials in the difficult-to-treat relapse refractory setting. One is a company-sponsored trial. It's mainly a safety phase Ib trial that we are conducting, and for which we will present an update in a couple of weeks at ASH. And the second trial is an investigator-sponsored trial performed in collaboration with the LYSA group, and it's a combination trial.

I think the combination strategy, in particular in the relapsed refractory, is something very important. We are, of course, excited by the preclinical data that we have generated, and that will be published at ASH, as I said, in a couple of weeks. We remain optimistic about the potential to run combination trials in the relapsed refractory setting, but also in first line. The plan, of course, is to expand the development of lacutamab in peripheral T-cell lymphoma beyond the difficult-to-treat relapse refractory, but that's the first step.

Jamie Easton (Senior Managing Director and Head of Communications & External Affairs)

Got it. Thank you.

Operator (participant)

There are no further questions at this time. I would now like to turn the call over to Mondher Mahjoubi for closing remarks.

Mondher Mahjoubi (CEO)

Oh, thank you. As a closing concluding remark, I would say, we are very encouraged by the robust outcomes of lacutamab in heavily pretreated patient with Sézary syndrome. Discussions with the FDA will enable us to evaluate the potential for accelerated approval and to firm up Phase III plans. We are, of course, in ongoing dialogue with potential partners that can realize the full potential of the drug for patient with T-cell lymphoma, both cutaneous and peripheral T-cell lymphoma. Second message, we are making great progress with our early-stage pipeline. Pleased to see the progress of IPH6101 or SAR443579 in AML, with an update at the upcoming ASH.

Pleased to announce that we have cleared the IND for IPH6501, and we are waiting for the start of the phase I this year. Finally, as you've heard from Yannis, excited by our differentiated anti-Nectin-4 ADC with the topo I payload, which is moving toward IND next year. Last but not least, sufficient cash to fund operation into H2 next year, with, as of end of September, EUR 122 million. 2025, sorry. Yeah, fund cash in H2 2025. Thank you very much.

Operator (participant)

I would like to thank our speakers for today's presentation, and thank you all for joining us. This now concludes today's call, and you may now disconnect.