Plus Therapeutics, Inc. (PSTV) on Q2 2024 Results - Earnings Call Transcript

Operator: Good afternoon, ladies and gentlemen. Welcome to Plus’ Call. Before we begin, we want to advise you that over the course of the call, including any question-and-answer session, forward-looking statements will be made regarding events, trends, business prospects and financial performance which may affect Plus Therapeutics’ future operating results and financial position. All such statements are subject to risks and uncertainties, including the risks and uncertainties described under the Risk Factors section included in Plus Therapeutics’ Annual Report on Form 10-K and quarterly reports on Form 10-Q filed with the Securities and Exchange Commission from time to time. Plus Therapeutics advises you to review these risk factors in considering such statements. Plus Therapeutics assumes no responsibility to update or revise any forward-looking statements to reflect events, trends or circumstances after the date they are made. It is now my pleasure to turn the floor over to Dr. Marc Hedrick, Plus Therapeutics President and Chief Executive Officer. Sir, you may begin. Marc Hedrick: Thank you, Cherie, and good afternoon, everyone. Thank you once again for taking the time to join us today as we provide an overview of recent business highlights and discuss our Second Quarter 2024 Financial Results. Joining me on the call today is Mr. Andrew Sims, our Chief Financial Officer. I'll begin the call by reviewing our recent clinical and corporate progress in the second quarter, then turn the call over to Andrew, to review our financials and then we'll both come back on for Q&A. So let me begin with updates from the 2024 Society for Neuro-Oncology and combined American Society for Clinical Oncology CNS Metastases Conference, which met last week in Denver. At SNO/ASCO, Plus was quite busy. We had four presentations, sponsored a symposium on novel emerging diagnostics and therapeutics for leptomeningeal metastases, and participated in a panel discussion on the opportunity for emerging therapies for brain metastases alongside senior executives from Novartis and Pfizer. Two of our four presentations warrant highlighting on our call this afternoon, and the full data from those presentations and from the symposium will be available soon on our website. First of all, Dr. Andrew Brenner, the ReSPECT-LM trial Principal Investigator, presented an interim update on the trial through Cohort 4 and that's n=16 patients. This is the most significant update that we provided since the SNO 2023 presentation. His presentation showed that through Cohort 4, which is an administered dose of 44 millicuries rhenium obisbemeda was safe and well tolerated with no dose-limiting toxicities and the maximum tolerated dose had not been reached. Furthermore supporting the relative safety of the drug, thus far, the PK data demonstrated a high therapeutic window. Specifically, the mean absorbed radiation dose to the ventricles and cranial subarachnoid space was approximately 160 gray compared to only about 1 gray to the spleen. Also, a linear increase in absorbed dose to the regions of interest, specifically, the cranial subarachnoid space and cerebrospinal fluid was noted from Cohort 1 to no increase noted in the spleen, which was the critical organ. In terms of response data, circulating tumor cell data was not available through cohort, temporarily unavailable at that time, but it's now available and we are back up and using the test currently in Cohort 5. But recall that we observed a mean 53% reduction in CTC, circulating tumor cells in the CSF for the first three treated cohorts. That was observed out to 28 days post-treatment, but the CTC number came back up by 56 days post-treatment. Additional and significant response data through Cohort 5 is currently being reviewed and will be presented in detail at SNO in November, and I'll talk more about that in a moment. In terms of the median overall survival signal, again with 16 evaluable patients through Cohort 4, median overall survival was 12 months, with half the cohorts, that's eight out of the 16 treated patients remaining alive at the time of analysis. This is an increase from that, that was reported after Cohort 3 last November, which showed a median overall survival of 10 months. To put that data in perspective, LM is a devastating disease, I think, as most of you know, from both a morbidity and mortality perspective, with typical survival rates ranging from two to six months after diagnosis, depending on primary tumor type. So this emerging efficacy signal, though early, is very encouraging vis-à-vis the standard of care. There was also a second presentation at SNO/ASCO [Technical Difficulty] Dr. Priya Kumthekar, who reported the top line clinical results from our FORESEE trial. FORESEE evaluated the clinical utility of CNSide, our newly acquired novel CNS diagnostic on leptomeningeal metastases treatment decision making by physicians in 40 patients. The trial used a well described trial design that's used commonly in the diagnostic space. Specifically, she reported that FORESEE met its primary endpoint with CNSide influencing treatment decisions in over 90% of clinical decisions. That's [Technical Difficulty] clinical decision points evaluated, and that substantially exceeded the 20% level, which was the target for the primary endpoint to show effectiveness. Moreover, the study also showed that CNSide helped identify actionable mutations in the CSF, such as HER2 amplification that influenced 24% of therapeutic selection decisions, that's 14 out of 55 clinical decision points evaluated. Importantly and related to the current state-of-the-art diagnostically that's found in major hospitals around the country, CNSide demonstrated more than twice the sensitivity in detecting tumor cells in the CSF compared to what is now the gold standard, which is cytology. Specifically, it showed a detection rate of tumor cells of 80% versus 29% for cytology. Also important, CNSide exhibited a very high specificity in that no tumor cells were detected in patients without leptomeningeal metastases. We were pleased to see this data and presented formally, and these FORESEE results highlighted and validate our previous high conviction that CNSide as a diagnostic and therapeutic selection and diagnostic therapeutic monitoring tool fulfills a critical clinical need in brain metastases that now has been shown to improve patient management and we believe will lead to better patient outcomes in the near future. Finally, in addition to our presentations at SNO/ASCO, we also reported important data at the 2024 Society for Nuclear Medicine and Molecular Imaging, known as SNMMI annual meeting in June 2024. The reported study used dosimetry data from the ReSPECT-LM clinical trial to evaluate the safety and potential for spinal cord toxicity of beta emitters or beta emission radioisotopes in the related physics and found that lower beta energy radionuclide such as rhenium 186 largely spare the spinal cord versus other beta radionucleotides that we studied. These findings further support the thesis that rhenium 186 is an ideal radionuclide for CNS cancers, hitting the therapeutic window delivering high therapeutic doses to the region of interest while minimizing toxicity. Now kind of moving on in terms of our leptomeningeal program broadly speaking, first of all therapeutically, the current Phase 1 single administration ReSPECT-LM dose escalation trial will continue dosing until the next DSMB meeting and at that time, we will determine if progressing to Cohort 6 is advisable. But thus far, as mentioned, a maximum tolerated dose has not been reached despite delivering up to a maximum of 66 millicuries to the CSF. In terms of upcoming data releases, a definitive trial update is planned for Society for Neuro-Oncology 2024 that will be held in Houston this November. To-date, we have dosed a total of 25 patients and also treated a subset of patients with multiple doses of rhenium obisbemeda under compassionate use and those patients have done really well. Also, the company has filed a new protocol under its open FDA IND to treat individual patients with a multiple dosing regime. This submission follows a positive FDA Type C meeting in Q2. Once formally approved with final agreement with the FDA, the company will share the details of that trial protocol. That trial is anticipated to begin enrolling later in 2024 at the current seven trial sites, with the number of new sites to be added in the interim. The leptomeningeal program continues to be significantly supported by an approximately $18 million product development award from CPRIT that covers approximately two-thirds of programmatic expenditures. Also, the company continues to be involved in active dialogue with CPRIT regarding program advancement and are actively seeking expanded ways to work with CPRIT that are mutually advantageous. In terms of our diagnostic LM program, we are in the process of expanding our CNSide diagnostic capabilities at a facility in Houston, Texas in specific, targeted, but strategic ways. First of all, we hired Dr. Greg Fuller, former Chief of Neuropathology at MD Anderson Cancer Center in Houston and an LM expert, to be the full time Medical Director of the CNSide lab and oversee lab operations and also help support our LM therapeutic objectives. We have also improved the lab quality assurance systems in our capabilities to steadily increase testing capabilities as anticipated for growing research use both from Plus’ growing trial number in LM, but also other trials that have contacted us with similar interest. In addition, we have applied for CLIA certification for CNSide as a laboratory developed test, and approval under CLIA is anticipated later in 2024. We anticipate providing further business updates on the CNSide diagnostic program later this year as developments warrant. Now I’d like to shift gears to our ReSPECT-GBM trial. As most of you know, this trial evaluates a single dose of rhenium obisbemeda in patients with recurrent glioblastoma and is funded mostly through the NIH. We continue to enroll both Phase 2 patients with recurrent GBM, and that’s for tumors that are less than or equal to 20 CCs and also enrolling patients in our Phase 1 now at Cohort 8 for patients with larger tumors. We anticipate three new active GBM convection enhanced delivery sites will be enrolling soon, and these should be able to transition to pivotal trial sites when the time warrants. Those are Ohio State University providing us a site in the Upper Midwest and North Shore Hospital, part of the Northwell, Lenox Hill network in the greater New York region. We are also evaluating other additional sites with the intention of adding at least one site in the greater Southern California region. These sites, specifically OSU and North Shore Hospital, Lenox Hill are on track to enroll patients in 2024. Additional sites beyond those mentioned are also being investigated for activation to support a potential pivotal trial. We are working to complete enrollment by the end of 2024, but more likely to wind up completing enrollment in the first half of 2025. A faster timeline will be influenced to a significant degree by participation of these new sites. Our plan is to provide a substantial update on the Phase 1 and Phase 2 data this fall at the CNS or Congress of Neurological Surgeons annual meeting, which is in late September, early October in Houston, Texas, and this will be our first time to be on the podium presenting this data to the neurosurgical community. In addition, I’d like to briefly update you on our pediatric brain cancer program. We’ve previously announced that we received a U.S. Department of Defense award for $3 million to substantially support the Phase 1 trial for children with pediatric brain cancer, specifically pediatric high grade glioma and ependymoma. That award is in administrative phase and is anticipated to begin funding this September 2024. We are also on track to obtain IND approval for this trial and Lurie Children’s Hospital will be the initial clinical trial site. Finally, we are making good progress behind the scenes on a number of important business items, specifically building in redundancy and commercial readiness in our supply chain and enhancing our drug delivery capabilities, and we plan to make material public updates on those in the near future. And with that, I’ll now turn the call over to our Chief Financial Officer, Mr. Andrew Sims, who will review the financials. Andrew? Andrew Sims: Thank you, Marc. Good afternoon everyone. Please refer to our press release issued earlier today for a summary of our financial results for the second quarter ended June 30, 2024. The cash and investments balance was $8.4 million at June 30, 2024, compared to $8.6 million at December 31, 2023. The company recognized $2.9 million in grant revenue in the first half of 2024 compared to $2.3 million in the same period of 2023. This represents CPRIT’s share of the cost incurred for our rhenium obisbemeda development for the treatment of patients with LM. We expect 2024 grant revenue to be in the range of $6 million to $7 million. Total operating loss for the first half of 2024 was $7 million compared to $6.2 million in the same period of 2023. The increase is primarily due to increased spend related to the respect LM trial. Net loss for the first half of 2024 was $6.2 million, or $1.15 per share versus $6.3 million or $2.06 per share, for the same period the prior year. An update on our runway cash position and provide guidance on our grant funding for the remainder of 2024. There are two additional sources of cash to which Plus has access beyond the balance disclosed in cash on hand and liquid investments on our Q2 2024 balance sheet. First, and as a reminder, we announced in May that we closed a private placement financing of up to $19.25 million from new healthcare focused, institutional investors and company insiders, with a total of $7.25 million received at closing. In addition, there are up to $12 million of cash on exercise of the one and five year warrants. As a side note, at June 30, 2024, the warrants issued as part of this private placement were recorded as a liability on the balance sheet and as outlined in the subsequent events Footnote 14 the warrant form was amended eliminating the liability and henceforth these warrants will be accounted for under the equity accounting method. The second source of cash remains our anticipated ongoing funding through now three awarded grants. First, the CPRIT grant to support the ReSPECT-LM trial. As reported, we received the first of two expected amounts from CPRIT in 2024, the first in Q2 of $3.3 million. We remain on track to receive the next advance from CPRIT of $3.7 million in mid to late Q4 2024. An additional $3.7 million is expected from CPRIT in 2025. Second as reported on April 22, Plus has received an award recommendation from United States Department of Defense for $3 million to support the upcoming ReSPECT-PBC in September 2024 and materially cover the cost of the planned Phase 1 trial. Funding is received annually in advance and covers a three year period, i.e., approximately $1 million will be received under this grant in 2024. Third, Plus also continues to benefit from the NIH grant to support the ReSPECT-GBM Phase 1/2 trial. Although expected to be complete in 2024, it currently covers approximately 90% of the overall trial costs. We also continue to source other non-dilutive sources of grant capital and have applied for approximately $13 million in additional grant funding year-to-date. We will continue to only report on individual grants when they are awarded. In summary, this provides incremental access to cash of $22 million, $10 million from CPRIT and DoD, and $12 million from the exercise of A and B warrants from the May private placement. And now I’ll turn it back to you, Marc. Marc Hedrick: Great. Thanks a lot, Andrew. Before we move to Q&A, just let me take a moment to provide some specific guidance for key events and milestones that we’re looking towards through the remainder of 2024. As mentioned during the Congress of Neurological Surgeons, CNS and that’s in late September, early October, Dr. John Floyd, who’s the Chief of Neurosurgery at UTHSCSA, University of Texas Health Science Center in San Antonio, will be presenting an update on the recurrent GBM Phase 1 and Phase 2 trial and most recent results. At the Society for Neuro Oncology annual conference, which will be held in Houston, November 22 through 26 of this year we’ll have three presentations. The first is a substantial update, as I mentioned earlier, on the ReSPECT-LM trial. In addition, we have two CNSide diagnostic abstracts. The first is entitled CSF Tumor Cell Detection, Quantification and Biomarker assessment, and how it helps in the clinical management of breast cancer and non-small cell lung cancer in patients with leptomeningeal disease. The second, which actually deals with a very important emerging issue of genetic drift in LM patients, that is, where patients have a certain genetic component to their cancer that flips from their primary tumor to a metastases, for example in the CSF. And the title of that is The Oncogenetic Flip in Patients with Leptomeningeal Metastases, specifically the longitudinal detection in cerebrospinal fluid tumor cells counts, and what it reveals in terms of implications for the differential treatment of the LMD tumor. And so all three of those will be on again for snow in the November of timeframe this year. We also anticipate FDA approval on the respect LM Phase 1 multiple dose trial. So the IND for the Phase 1/2 study of rhenium obisbemeda for pediatric ependymoma and high-grade glioma patients is anticipated also later this year. So with those, Cherie, I'll turn it back over to you and we can have our Q&A session. Operator: Thank you. [Operator Instructions] And our first question will come from the line of Justin Walsh with Jones Trading. Your line is open. Justin Walsh: Hi, thanks for taking the question. I was wondering if you could provide some more context around the types of treatment decisions that are likely to be informed by CNSide. Obviously, therapy selection is one, but the 24% that informed therapy selection is lower than the 90% total decisions that were impacted? Marc Hedrick: Yes, it's a good question, Justin. So one of the key decisions is a, does the patient have the disease or not? And having a highly sensitive test like the circulating tumor cells. And we showed the comparative data with cytology from the 4C trial [ph] informs whether or not the patient requires treatment for LMD. And there have been a number of reports that we've received where patients have indeterminate clinical signs, indeterminate imaging, or maybe even supportive imaging consistent with LM disease, but their spinal fluid is negative. So that's a really – that's probably the most important decision, quite frankly. Do they have the disease or not? And even with the combination of clinical evaluation, MRI, and CTCs in cytology, that can often be a difficult decision to make. And generally what physicians are using now is they look to get two repeat CTC cell determinations and then make the decision if the patient does not have LM and doesn't require treatment. So that's kind of number one. Number two is, an assessment of the genetic drift issue, and we think that goes beyond just the HER2 issue, but into other actionable biomarkers that will dictate whether certain type of drug checkpoint inhibitor might be utilized in one kind of tumor versus the other. And that genetic drift goes both ways, from positive to negative in the leptomeningeal space, or the opposite. The other issue is whether it's potentially advantageous to stop treatment. For example, there are some case reports, certainly not significant series, but case reports where therapy can drive the number of circulating tumor cells down to zero, and then one can theoretically stop treatment, monitor patients that are doing well, and then reevaluate based on the ongoing CTC count going forward. So we're just beginning to open the envelope on what the data means, but there are at least, I think, three solid ways where decision making can be impacted by the clinician. Justin Walsh: Got it. Thanks. Quick follow up. It might be a little early, but I'm curious if you have any expectations with respect to timing once you get into the multi-dose LM portion of the trial? Marc Hedrick: Timing in terms of when it gets started or… Justin Walsh: Yes. And if you think there'll be relatively rapid enrollment? Or if it'll maybe be along the same pace as the single dose version. Just curious about your thoughts on that front. Marc Hedrick: Yes. Yes. So, thank you, Justin. So, yes, a couple of things. So the IND is open. I think we're optimistic that what we've currently negotiated with FDA will ultimately go through. So we'll hear back less than 30 days, and assuming that's the case, and in fact, we're already talking to sites and doing the activities you would do for site startup, there'll be a different protocol that's got to go through IRB review and budget and so forth. But because we have an open IND that's very similar, I think it ought to go pretty quickly. Our plan is to go back to the current seven sites that we're working with where this should also go more quickly. But we've also got a number of leading sites that want to participate. So that'll be an important part of the plan. So I think, as mentioned, we'll get the trial up and running later this year. Some sites will be before other sites, obviously. So that's number one. In terms of how long it would take to enroll? The Phase 1 single administration was plagued by a couple of things. Number one, it had a Part A and a Part B. The FDA was very [Audio Dip] the amounts in terms of the administered dose of radiation that we were giving and wanted a formal stopping point. And we had to go back, as you'll recall, to move forward to the second half of that trial, which we're now in. Plus we had intracohort DSMB decisions that we could roll very quickly, but then we had to wait for 90 days from the first patient and 30 days from the last patient before we go back to DSMB. So bottom line is, I think we'll be getting data a lot more quickly from this. What's currently contemplated is, we're dialing in multiple doses for these patients without going back to the FDA. So I think the data will accumulate quickly, both in terms of number of patients and longitudinal data on a variety of endpoints within four individuals [Audio Dip]. Once we – my preference is to wait till once we have the final feedback from the FDA, which we anticipate shortly, and then we'll make all that public and then put out some guidance about timing. Justin Walsh: Great. Thanks for taking the question. Marc Hedrick: Thanks, Justin. Operator: Thank you. [Operator Instructions] And that will come from the line of Sean Lee with H.C. Wainwright. Your line is open. Sean Lee: Good afternoon, guys, and congrats on the clinical progress this quarter. My first question is on the CNSide assay, so my understanding is that, correct me if I'm wrong, but all the tech transfer has been completed and you're now just setting up the test to be manufactured and marketed. So, I was wondering, what are the next steps that you have to do before you can start selling the tests to the market, or at least to the clinical sites? Marc Hedrick: Hey, Sean, thanks for the question. Yes. Let me kind of review where we are and the plan going forward. So what we've done is, we've acquired all the IP hard assets, knowhow SOPs and technology-related information, plus customer information. Remember this test was commercial for a couple years and was growing at about a 30% year-over-year rate, with about 200 individual customers at the time the test became unavailable prior to our acquiring it. So we transferred the technology, I think back in Q1 of this year, got the test up and running, reimplemented it in our Cohort 5, as mentioned and we're now. We're now performing the test within our trial. In the background, what we've done is we have hired a Medical Director. We are actually manufacturing ourselves some of the chips that the test is done on, the microfluidic chips. We're now manufacturing those. Those were a gating item in terms of expanding the testing. We're now manufacturing those. So those are no longer a critical supply element. And so now it's really scaling the test. Now we can scale the test effectively for our multiple dose trial. We're going to be testing, doing many more tests on patients longitudinally because they're getting multiple doses. And that's going to require pretty significant ramp up in testing throughput. And so now we're kind of positioned well to accommodate that from a QA perspective. And as I mentioned, Dr. Fuller's on board will be the Medical Director. So in the background, we are doing a significant amount of commercial evaluation to determine what the magnitude of the commercial opportunity for this test, and then what's the required investment. That analysis is going well. Thus far it looks very positive, but I think before we kind of commit, we want to have a full and well thought through plan and be ready to execute on that before we say too much more. But I will say that's going well, and those we'll be talking about that relatively soon as we finalize that plan. Sean Lee: Great. Thanks for that. My second question is on the LM studies. Now that you have a multi dose study in the works, does it still make much sense to continue the single-dose study, especially to higher dose cohort? Or would you be switching your focus mainly to the multi dose study going forward? Marc Hedrick: It's a really good question, and here's how I would respond to that. The FDA, both in our GBM trial and related to this LM trial, they're very interested to getting to a maximum tolerated dose. They've made that very clear. So, I think we're committed to understand where the level of toxicity lies. So, and I think we're close, quite honestly. I think what kind of, what we see from the safety signals in Cohort 5 kind of lead us to believe that we're probably pretty close, if not, there but as I mentioned, we have not officially reached an MTD at this point, but we'll continue that until we get to the formal stopping point or we get to a maximal feasible dose. So we're not there yet. Secondly, I think we wanted, we think long term, based on what we see in the single administration trial and specifically that small group of patients that have had multiple doses, they're doing quite well. We believe we can get with this disease, but it likely will require multiple doses. So we wanted to get that multiple dose trial going quickly at our cohort 2 dose. And that data thus far, from a single administration perspective has looked very promising. And you've seen that data and we've now presented that multiple times. So that's up and running. So I think that. So the next step, really, I know it's a long answer, but look at the Phase 1 data, understand it, look at the response data, discuss with FDA, get the multiple dose study up and running, and then we'll make a decision about whether or not we want to take a single administration dose into a Phase 2/3 pivotal, as envisioned in our CPRIT Grant, for example. That was the initial clinical plan. That may still be the right thing to do. That may accelerate things but provide a bit more risk or we might wait for the data related to multiple doses. But if we look like it's potentially safe and effective with a single administration, then we have to really seriously consider whether or not we where we want to take that to a pivotal or not. It'll be an interesting discussion, but that'll be a good problem to have. Sean Lee: Thanks for that. That's very helpful. My last question is on the GBM study. I think in the prepared remarks, you mentioned that the grant for the GBM studies will be coming to an end towards the end of this year. I was wondering whether we can expect any more data updates from that later this year as well? Thanks. Marc Hedrick: Yes. So with respect to the GBM trial. So as mentioned, we'll do a meaningful update on the Phase 1 progress and the Phase 2 progress at the CNS, the Congress for Neurosurgeons, which will be in late September and into early October in Houston this year. So that'll be the next update. And the goal is to get enrollment completed this year, as mentioned. I think that's going to be difficult. We've got two new sites that are in the final stages of onboarding right now. If those can contribute substantially, we've got a chance at getting that trial enrolled by the end of the year. If not we think it will be in the first half of next year, and then at that point, we'll evaluate the data. We've continued to have good safety signals and very interesting efficacy signals related to standard of care. If we continue to see that, then I think based on our previous discussions with the FDA, we have a pretty good idea what a pivotal trial design would look like, and we'll be ready to pull the trigger on that. Sean Lee: Great. That's all I have. Thanks again for taking my questions. Marc Hedrick: Thank you, Sean. Operator: Thank you. [Operator Instructions] And that will come from the line of Edward Woo with Ascendiant Capital. Your line is open. Edward Woo: Yes. Congratulations on all the progress, and congratulations on lining up additional potential grant funding. I was wondering, is there any seasonality to the grant funding? Are they issued all in certain times of the year? And have you noticed any change in the funding’s that's out there? Has it been more or less or been about the same? Thank you. Marc Hedrick: Hey, Ed. Yes, no, thanks for the question. It's definitely seasonal in this regard, and I'll take CPRIT, for example. CPRIT has historically had two times of the year where they accept grants, and so it takes about six months to go through that funding cycle. So if you submit a proposal and let's say July or August, in that timeframe, it takes about six months to go through the review process to get a decision for funding and then get the administrative award mechanics finalized so you can receive funding. So it's seasonal and that we're responding to their granting calendar. And our experience with the NIH is similar, but oftentimes it's more sporadic, where they have requests for proposals, specifically our DoD proposal that we responded to in RFP, as I recall. And that's more of a one off situation. So there's some peculiarities that can be seasonal, but also can be sporadic and affecting the timing. As mentioned, I think we've developed a really good relationship working with CPRIT. We know of companies that have up to at least three grants per company. We also know that CPRIT will fund up to $20 million through Phase 2. So I think there's, you know, that's been a nice relationship, and that that capital has been very important to us. And so I think that's what we'll continue to try to work with them closely, as well as look at some of these more sporadic alternatives to continue to leverage that non-dilutive capital and minimize the dilution to shareholders. Edward Woo: Great. Well, thanks for answering my questions, and I wish you guys good luck. Marc Hedrick: Thank you. Andrew Sims: Thanks, Ed. Operator: Thank you. I'm showing no further questions in the queue at this time. I would now like to turn the call back over to Dr. Marc Hedrick for any closing remarks. Marc Hedrick: Thank you, Cherie. And we thank everyone, our analysts and shareholders and investors, for listening to this call. And also want to thank our patients, talking to two of them next week in Texas, who trust us to give them this investigational treatment. And thank you to all our employees who worked so hard to make it happen. We wish everyone a nice evening. Thank you. Operator: This concludes today's program. Thank you all for participating. You may now disconnect.
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Recent Market Movements Highlight Notable Stock Performances

  • Plus Therapeutics, Inc. (NASDAQ:PSTV) saw a 177.57% increase in stock price, likely due to FDA's conditional acceptance of REYOBIQ™.
  • Impact BioMedical Inc. (NYSE American:IBO) experienced a 170.06% surge, possibly reflecting investor optimism from its participation in The Microcap Conference 2025.
  • SAG Holdings Ltd (NASDAQ:SAG) had a 67.41% rise in stock price following the successful closing of its initial public offering.

In recent market movements, several companies have shown significant price changes, capturing the attention of investors and market analysts alike. Among these, Plus Therapeutics, Inc. (NASDAQ:PSTV), Impact BioMedical Inc. (NYSE American:IBO), Rain Enhancement Technologies Holdco, Inc. (RAINW), Osisko Development Corp. Warrant expiring 5/27/2027 (ODVWZ), and SAG Holdings Ltd (NASDAQ:SAG) stand out due to their notable performance.

Plus Therapeutics, Inc. (NASDAQ:PSTV) experienced a remarkable surge, with its price jumping by 177.57% to $1.4184. This biotechnology firm focuses on developing treatments for cancer and other diseases. The significant price movement could be attributed to the U.S. Food and Drug Administration's conditional acceptance of the proprietary name REYOBIQ™ for its lead drug candidate, as highlighted by the company. This development is a positive step in the clinical investigation for Leptomeningeal Metastases and Recurrent Glioblastoma.

Impact BioMedical Inc. (IBO) also saw a substantial increase, with its stock price rising by 170.06% to $1.4313. The company engages in the discovery and development of specialty biopharmaceuticals and consumer healthcare products. The surge might reflect investor optimism about the company's participation in The Microcap Conference 2025, where CEO Frank D. Heuszel will present. This event is a key gathering for growth-focused companies and investors.

Rain Enhancement Technologies Holdco, Inc. (RAINW) witnessed an 83.03% increase in its stock price to $0.11. Although specific catalysts for this increase are not provided, such movements often result from positive news about technological advancements or successful pilot projects. The company focuses on ionization rainfall generation technology, which could be gaining attention for its innovative approach.

SAG Holdings Ltd (NASDAQ:SAG) experienced a 67.41% increase in its stock price to $1.13. This movement could be related to the successful closing of its initial public offering, raising $7 million through the sale of 875,000 ordinary shares at $8.00 per share. The company distributes automotive and industrial spare parts, and this financial boost may indicate strong growth prospects.

These companies, spanning diverse industries from biotechnology to gold development and automotive spare parts distribution, have shown impressive market performances. Their recent gains could be attributed to a variety of factors, including successful clinical trials, technological advancements, favorable market conditions, strategic partnerships, or financial growth. Investors and analysts will likely keep a close eye on these companies for further developments that could influence their stock prices.

Plus Therapeutics, Inc. (NASDAQ:PSTV) Sees Surge After FDA Orphan Drug Designation

  • Plus Therapeutics, Inc. (NASDAQ:PSTV) stock surged by 311.4% following the FDA's Orphan Drug Designation for its lead radiotherapeutic candidate.
  • The FDA's designation provides benefits like seven years of market exclusivity, tax credits, and fee exemptions, crucial for addressing the unmet medical need for treating leptomeningeal metastases.
  • Despite financial challenges, including a negative price-to-earnings (P/E) ratio of -0.96 and a current ratio of 0.44, the recent FDA designation offers a promising outlook for PSTV's future.

Plus Therapeutics, Inc. (NASDAQ:PSTV) is a clinical-stage pharmaceutical company focused on developing innovative treatments for rare diseases. The company is set to release its quarterly earnings on March 11, 2025, with Wall Street estimating an earnings per share of -$0.51 and projected revenue of approximately $1.19 million. Despite these figures, recent developments have significantly impacted PSTV's stock performance.

On March 6, PSTV's stock price surged by 311.4% following the FDA's Orphan Drug Designation for its lead radiotherapeutic candidate, rhenium (186Re) obisbemeda. This drug targets leptomeningeal metastases in lung cancer patients, a rare and challenging condition. The FDA's designation provides benefits like seven years of market exclusivity, tax credits, and fee exemptions, as highlighted by the FDA.

The Orphan Drug Designation is crucial for Plus Therapeutics as it addresses the unmet medical need for treating leptomeningeal metastases. This condition involves the spread of cancer to the cerebrospinal fluid, posing significant treatment challenges. The designation, along with a previously granted Fast Track designation, marks a significant milestone for the company, as emphasized by Mike Rosol, Ph.D., the Chief Development Officer.

Despite the positive news, PSTV faces financial challenges. The company has a negative price-to-earnings (P/E) ratio of -0.96, indicating a lack of profitability. The price-to-sales ratio is 2.17, suggesting investors pay $2.17 for every dollar of sales. Additionally, the enterprise value to sales ratio is 2.68, providing insight into the company's valuation relative to its revenue.

PSTV's financial metrics also highlight potential liquidity concerns. The current ratio is 0.44, indicating the company may struggle to cover short-term liabilities with its short-term assets. The negative debt-to-equity ratio of -0.66 suggests a unique capital structure or financial strategy. Despite these challenges, the recent FDA designation offers a promising outlook for the company's future.

Plus Therapeutics, Inc. Gears Up for Q1 2024 Earnings Release

  • PSTV is set to release its EPS estimate of -$0.25 and expected revenue of approximately $1.69 million for the quarter.
  • Previous quarter performance showcased revenue of $1.31 million and a gross profit of $1.13 million.
  • Significant improvement in EPS from -$0.84 to an estimated -$0.25, indicating a potential positive financial trajectory.

Plus Therapeutics, Inc. (NASDAQ:PSTV), a clinical-stage pharmaceutical company, is gearing up to share its quarterly earnings on Thursday, May 16, 2024, after the market closes. Specializing in the development of targeted radiotherapeutics for central nervous system cancers, PSTV's financial performance is closely watched by investors and analysts alike. The anticipation builds around the earnings per share (EPS) forecasted at -$0.25 and expected revenue of approximately $1.69 million for the quarter.

The upcoming earnings report follows a period where PSTV reported revenue of $1.31 million with a gross profit of $1.13 million. This financial snapshot indicates a company that, despite its challenges, is managing to generate revenue and maintain a certain level of gross profit. The cost of revenue standing at $182,000 for the same period further highlights the company's ability to control its production or service delivery costs, an essential factor for its financial health.

However, PSTV's financial journey is not without its hurdles. The company faced a significant net income loss of -$3.81 million and an operating income loss of -$3.86 million. These figures point to the challenges PSTV encounters in balancing its operational costs against its revenue. The reported EBITDA (Earnings Before Interest, Taxes, Depreciation, and Amortization) of -$3.68 million further underscores the financial strains the company is experiencing, reflecting broader operational challenges beyond mere net income figures.

Moreover, the earnings per share (EPS) for the quarter was reported at -$0.84, a critical metric for investors as it provides a direct insight into the company's profitability on a per-share basis. This figure is particularly significant when compared to the upcoming earnings forecast, which estimates the EPS to be -$0.25. The improvement in EPS, if realized, could signal a positive shift in PSTV's financial trajectory, offering a glimmer of hope for stakeholders looking for signs of recovery and growth.

As PSTV prepares to unveil its first quarter financial results for 2024, the management team plans to host a conference call and webcast to discuss the outcomes and provide updates on the company's operations. This event is not only a platform for financial disclosures but also an opportunity for PSTV to articulate its strategic direction and operational updates, offering a comprehensive view of its path forward in the competitive pharmaceutical landscape.