TFF Pharmaceuticals, Inc. (TFFP) Q1 2022 Earnings Call Transcript

TFF Pharmaceuticals, Inc. (TFFP 1.33%)
Q1 2022 Earnings Call
May 11, 2022, 4:30 p.m. ET

Contents:

• Prepared Remarks
• Questions and Answers
• Call Participants

Prepared Remarks:

Operator

Good day, and welcome to the TFF Pharmaceuticals, Inc. first quarter 2020 earnings conference call. [Operator instructions] Please note this event is being recorded. I would now like to turn the conference over to Corey Davis.

Please go ahead.

Glenn Mattes -- President and Chief Executive Officer

Thank you, Corey. Good afternoon, and thank you for joining us today to review the company's first quarter operations and recent highlights. During this call, I will provide an update on our overall progress then ask our chief financial officer, Kirk Coleman, to review our first quarter financials. Having announced our fourth quarter and year-end 2021 results, just a few weeks ago, we decided to provide a more focused formal commentary of our meaningful progress for this call.

This will leave more time for Q&A, and please note that Chris Cano, Dale Christensen, and Dr. Bill Williams are present on today's call and will participate in that session. TFF continued to build strong momentum in our pipeline and partnership activity in the first quarter of 2022. And this momentum carries over from our very successful fourth quarter, which saw numerous accomplishments, including the final data from the Phase 1b study of inhaled voriconazole powder in asthma patients and the initiation of our Phase 2 studies for both inhaled tacrolimus and voriconazole powders.

In addition, we began the Phase 1 inhaled niclosamide powder study in Canada to treat COVID-19. Advancement of our pipeline programs continued in the first quarter. TFF continues to progress with the inhaled voriconazole and tacrolimus inhaled powder Phase 2 programs. Both Phase 2 studies will produce interim analysis late in the third quarter of this year.

This is a key milestone event as these data will be shared with potential pharmaceutical company partners in a licensing process. That process has been initiated working with Torreya Partners to introduce the opportunity to invite interested companies to begin diligence. We have established a comprehensive data room and already have potential partners performing diligence as a result of inbound interest. TFF has also made voriconazole inhaled powder available on a limited compassionate use basis when requested by investigators.

We have received very positive feedback on the first of these patients on Monday. The treating physician shared results with us that supports the efficacy and safety target product profile for voriconazole inhaled powder. In general, this patient was considering only palliative care for his disease and now has reported outstanding efficacy and safety. Dr.

Dale Christensen will be happy to share more details should you have questions during the Q&A. TFF also advanced the inhaled niclosamide powder development program. After completing enrollment in the 40-patient Phase 1 study earlier in the quarter, in April, we announced positive safety and pharmacokinetic data showing that niclosamide inhalation powder was well tolerated with no serious adverse events across all subject cohorts. Importantly, the study also helped us identify what will be the optimal dosing level for the product in the Phase 2 program.

At the 6-milligram dose level, niclosamide inhalation powder is estimated to produce a concentration of 10 micromolar and the epithelial lining fluid in the lung, howling delivery as a dry powder, which would be considered highly potent with respect to inhibiting viral replication. A single administration of 6 milligrams of niclosamide inhalation powder to the lungs provide equal mean maximum drug concentration or Cmax in the blood as 100 milligrams delivered as a nebulized spray to the lungs and nasal cavity as demonstrated in a recent publication. Furthermore, the study's Safety Management Committee also expressed no questions or concerns about the safety and recommended the 6-milligram BID dosing as safe for progression into Phase 2 testing. Further highlighting the product's potency, in February, we announced the results from recently completed in vitro and viral replication assays, which shows the niclosamide inhalation powder completely inhibited viral replication of both the Delta and Omicron variants of SARS-CoV-2.

The results also show that our inhaled niclosamide demonstrated complete inhibition of Omicron replication and only one micromole compared to the Pfizer and Merck antivirals that each showed complete inhibition of Omicron at 2.5 micromolar. In our view, the high potency of inhaled niclosamide powder suggests that the product may have major advantages over oral delivery, including improved safety and tolerability. The program reflects the exact type of value we hope to create in every one of our collaborations which dramatically improved drug delivery so that an optimal amount of active molecule can be delivered while minimizing potential side effects to the patient. We continue to develop niclosamide inhalation powder in partnership with Union Therapeutics as a potential antiviral to treat COVID-19 and other respiratory viral diseases.

Union Therapeutics is now evaluating the data TFF has generated for niclosamide inhalation powder which will inform the decision on the option to assume responsibility to further develop the compound. New and disruptive technologies are often supported by a steady stream of basic research and development which over time leads to a significant body of scientific literature, and this is clearly the case with thin film freezing. At this year's RDD meeting, Dr. Bill Williams and his colleagues at the University of Texas at Austin presented five separate papers highlighting the versatility of thin film freezing technology.

These data also support the differentiation of thin film freezing from other methods to create dry powder, particularly in biologics. In fact, one of the papers, which explores the use of machine learning algorithms to analyze how thin film freezing impacts aerosol delivery of dry powder therapies. It received a poster on the podium recognition. The research being conducted by Dr.

Williams and his colleagues to demonstrate the versatility of this unique innovation in pharmaceutical formulation development. And we look forward to highlighting additional research from our laboratories as they become available. Turning our attention to our collaboration activity. TFF announced a strategic partnership with the global CDMO Catalent during the first quarter.

The client base of over 1,000 companies, we are confident in the short-, mid-, and long-term productivity from this relationship. In particular, Catalent will introduce thin film freezing to a targeted list of potential licensing candidate. And with Catalent focused on biologics manufacturing provide a clear path forward in providing a source for product in this key arena. This matches very well the balance of TFF partnership portfolio.

I'm happy to report that TFF and Catalent have been working very well together to successfully launch the partnering effort, and I look forward to reporting multiple successes as we work together. During the quarter, we were also pleased to announce a second cooperative research and development agreement with the United States Army Medical Research Institute of Infectious Diseases and the Geneva Foundation. We consider our partnering activity in the government, defense, and other public-related sectors as a core area of focus for our business. And as applications of thin film freezing continue to expand, we anticipate that our public sector collaborations could provide a significant source of non-dilutive funding over time.

Speaking of non-dilutive funding, TFF continues to work to capitalize on the language in the omnibus budget legislation, which highlighted the opportunities created by thin film freezing. We are working through supportive groups to fully explore funding opportunities. Now looking at progress on other existing collaborations, TFF is continuing to work with PLUS Products who recently announced the transaction with Glass House. This transaction will build a highly competitive company in the cannabinoid space.

As this partnership is freshly minted, we are in discussions on a path forward on the TFF inhalation cannabinoid products that have been successfully tested with consumers. And finally, we are working with our development partners at Augmenta to identify next steps for Augmenta 3387, which has been identified as a highly potent monoclonal antibody to treat COVID-19 in preclinical animal models. In general, based on the robust pace of our ongoing partnership work and discussions, we remain highly confident that 2022 will see TFF Pharmaceuticals enter into meaningful monetized new collaborations while expanding many of our existing partnerships. The number of companies in our portfolio continues to grow and the work we are doing under open MTAs and statements of work continue to progress with successful scientific results and extreme purpose.

The first quarter also saw TFF Pharmaceuticals, bringing a wealth of new and diverse talent in the form of senior-level and board of director appointments. As the number of collaborations grow in our internal clinical programs advance, an appropriate level of investment is required to optimize such growth. The new colleagues added to TFF Pharmaceuticals reflects a company fast becoming stronger across all facets of our business. We believe these additions will lead to the expansion of existing collaborations, the forging of new and more strategic partnerships, and the advancement of multiple programs into late-stage testing, all of which will generate significant value for our shareholders.

And with that update, I will turn the call over to our chief financial officer, Kirk Coleman, for a review of the financials. Kirk?

Kirk Coleman -- Chief Financial Officer

Thank you, Glenn. For the three months ended March 31, 2022, research and development expenses for the company were $5.3 million, compared to $5.3 million for the same period in 2021. General and administrative expenses for the three months ended March 31, 2022 for the company were $3.2 million, compared to $2.6 million for the same period in 2021. The company reported a net loss for the three months ended March 31, 2022 of $8.4 million, compared to a net loss of $7.7 million for the same period in 2021.

Weighted average common shares outstanding basic and diluted for the three months ended March 31, 2022, were 25,371,781, compared with 23,140,607 for the same period in 2021. As of March 31, 2022, we had total assets of approximately $33.8 million and working capital of approximately $29.3 million. At the end of the first quarter, our liquidity included approximately $26.4 million of cash and cash equivalents. And with that, I'd like to turn the call back over to Glenn.

Glenn Mattes -- President and Chief Executive Officer

Thank you, Kirk. Since our last call only a few weeks ago, market conditions have clearly not improved. What hasn't changed is the pressing need for pharmaceutical companies to develop significantly improved drug formulations that could be more safely and efficiently delivered to patients. The work we are doing at TFF Pharmaceuticals to address this significant demand places our company in a unique and, in my view, quite enviable position.

From the research being conducted at the university benchtop all the way through to the progress we are demonstrating in the clinic and through our partnerships, the value being created by our thin film freezing technology continues to set new high watermarks quarter after quarter. Without question, we believe our technology represents a true breakthrough in formulation technology and one that the industry has been seeking for decades. As investors attempt to reconcile the latest short-term market conditions against TFF demonstrable progress, we can only provide our shareholders with the assurances that our company will continue to work diligently to maximize value across every facet of our business. This quarter, we did exactly that by signing a strategic collaboration agreement with Catalent, entering our second CRADA agreement with USAMRIID, and announcing positive data from yet another clinical-stage pipeline asset with inhaled niclosamide powder.

And we expect the steady cadence of pipeline progress and collaborative activity will continue throughout the year and beyond. I would like to thank all of the TFF employees and key consultants for their contributions to the company. I'd also like to thank the board and our shareholders for their support. And with that, I will turn the call back to the operator and open it up to questions.

Operator?

Questions & Answers:

Operator

Thank you. [Operator instructions] And the first question today will come from Jonathan Aschoff with ROTH Capital Partners. Please go ahead.

Jonathan Aschoff -- ROTH Capital Partners -- Analyst

Thank you, and congrats on the progress, guys. For one of your internal programs, can you provide any details about that TFF VORI compassionate use patients know how they did? And will you be treating any additional compassionate-use patients?

Glenn Mattes -- President and Chief Executive Officer

Yeah. Hi, Jonathan. This is Glenn. And to all of you that are asking questions, I will either answer the question or ask one of the members of the TFF team to respond to this question.

And actually, it's really appropriate because Dale has been the one that's been really working these programs personally, I would [Inaudible]. I'll ask Dale to answer the question.

Dale Christensen -- Director of Clinical Development

Thanks, Glenn, and thanks, Jonathan. So we received an update on this patient. The patient has now been treated for 11 weeks. This was a patient who had spent six months out of the last year prior to starting the compassionate use study in the hospital as an inpatient getting IV antibiotics and antifungals when tolerated.

The patient had experienced every side effect that could be imagined from antifungal therapies and was essentially ready to give up treatment and go home and they were discussing palliative care when the idea of treating them with the inhaled voriconazole came along. In the immediate aftermath, the patient has now been outpatient, taking the inhaled voriconazole for 11 weeks. He has seen stabilization. He had lost approximately 40% of his FEV1 lung function.

And in the 11 weeks, he's lost less than 3%. So it's stabilized on lung function. His forced vital capacity has increased over that time. And the patient is considered clinically stable for the first time in well over a year.

In addition to that, one of the things that we speak about with as the positive benefits of the inhaled voriconazole is minimization of drug-drug interactions. And this patient who was on tacrolimus to maintain his immunosuppression. This patient has not had to have a dose adjustment to his tacrolimus, which would have had -- if you had taken the oral voriconazole, there would have been major dose adjustments required to achieve levels because of those drug interactions. So all in all, the results from this one patient are exactly why I went into this business to improve people's lives because this person has truly benefited from this therapy.

Jonathan Aschoff -- ROTH Capital Partners -- Analyst

Thank you, Dale. So as you guys look at all the preclinical and the Phase 1 results with VORI and TAC, what are your key takeaways? And what do those takeaways signal about the probability of success in these ongoing pivotal Phase 2s?

Glenn Mattes -- President and Chief Executive Officer

Yeah. So thanks. So I think let me just add from a business perspective and Dale, I'd probably give you a minute or two to think about your response. So as you know, Jonathan, and I think most of you who know the company, with our data that we will glean from the Phase 2 trials leading up to probably the latter part of the third quarter, we think that will certainly be based upon the Phase 1s and based upon what we're seeing from the Phase 1b and now, albeit one compassionate-use patient and hopefully more.

We think that that will be the final piece of the puzzle to attract interested companies to bid on licensing the product. And we've engaged Torreya partners. I've worked with Torreya. They're a really outstanding firm.

They do this kind of work to place one or two assets in a company with meaningful economics. So certainly, from a business and revenue standpoint, this is a big piece of how we look at our capitalization. Now from a clinical perspective, I believe -- I've always believed that the probability of technical and regulatory success here was extremely high. Dale, maybe the perspective you can supply is in actuality, how has VORI and TAC performed against the clinical expectations you had? And whatever other comments you have, please feel free to add.

Dale Christensen -- Director of Clinical Development

Thanks, Glenn. So just as -- to take one step back, we selected the voriconazole, the TAC, and the niclosamide for the internal development programs because each of them is a validated drug best-in-class. In the case of tacrolimus, it's already used for 90% of lung transplant patients, but the problem is significant toxicity when delivered by oral because you have to put up -- push up the levels to get enough into the lung to be effective. Similar message with voriconazole.

In order to get enough into the lung where it can be effective, that comes along with systemic toxicities. And so in each of these cases, the premise has been can deliver the drug effectively to the lung, reduce the toxicity and avoid drug-drug interactions by direct topical delivery to the lung. And so all of the nonclinical and clinical data that we've generated to date fully support that premise. As I just mentioned, the patient that is on tacrolimus and went on inhaled voriconazole saw no need for dose adjustments, which -- that is one of the key premises of this that it will be easier for the patients and the physicians to use because there will be limited drug-drug interactions.

And we fully expect, and I think we're seeing that the drugs can reach efficacious concentrations. And so in all cases, the programs, as we've advanced, they're performing exactly as expected. And some of the results are -- it's hard to say better than we expected because we have high hopes, but they're performing very well. And we look forward to generation of the final data and seeing this truly benefit patients in the future.

Jonathan Aschoff -- ROTH Capital Partners -- Analyst

Thanks, Dale. Does Union -- they have a right to opt in and they have not yet made a decision on? Or is that included?

Glenn Mattes -- President and Chief Executive Officer

So as you know, Jonathan, we finished the Phase 1 trial. We've delivered all of the available information to them from those trials. There's still some data final tables case reports that we're sending. But in essence, they do have, we believe, enough information to begin their diligence.

In fact, we did get a list of diligence questions from them this morning. I went directly to Chris. We speak to them all the time. So I would say, certainly, their option deliberation period has commenced.

And you are correct, they have an option. And if they exercise that option, they will have the -- they will take over the development of niclosamide.

Jonathan Aschoff -- ROTH Capital Partners -- Analyst

And you said has commenced. It sounded a bit formal, so they have a formal time by which they have to say, yes.

Glenn Mattes -- President and Chief Executive Officer

I mean, as you go by the letter of the agreement, I think practically, it's commenced. I mean, there is a -- by the letter of the agreement, we have to have complete all the case report forms, but I believe they've had enough information that actually the option period. I mean, I don't think people should be doing an account down here for a rocket launch. But they are -- in my feeling and the company's feeling, the option period has begun.

Jonathan Aschoff -- ROTH Capital Partners -- Analyst

Thank you very much, and good luck with partnerships that results in some up-front, non-dilutive cash, hopefully sooner than later.

Glenn Mattes -- President and Chief Executive Officer

Very optimistic. Thank you.

Operator

Thank you. And the next question is from Daniel Carlson with TW Research. Please go ahead.

Daniel Carlson -- Tailwinds Research -- Analyst

Hey, Glenn. Thanks for taking my questions. First one is kind of a two-part one here. Just about the general market conditions, I'm wondering if you've noticed that progressing your deals has been impacted at all by this.

And then kind that leads to the second part is maybe you can update the status of the VORI and TAC out-licensing process and any timing around that?

Glenn Mattes -- President and Chief Executive Officer

Sure. Hey, Daniel, we have not noticed and obviously, we can't, but notice what's happening in the marketplace. But I'll ask Chris to confirm this or not. But I don't think that the market conditions have really slowed down any of the work that we're doing.

Look, so many of the partnerships and with that, I mean, the open MTAs and statements of work have been going off for some time with those companies that we believe are close to transacting. If anything, I would say some of the smaller companies. And there aren't many in the splits for us, where they're obviously now more acutely concerned about cash. I think that it does come up, but it also hasn't slowed down the pace of any of the work we're doing, hasn't slowed down any of the pace of the negotiations.

It hasn't changed any of the numbers that have been exchanged or what the asks are. Chris, do you feel any color to add to that?

Chris Cano -- Chief Operating Officer

Yeah, no. Thanks, Glenn, and thanks, Dan, for the question. I have not seen a slowdown in -- due to market conditions for engagement with collaboration partners. There hasn't been an impact to us.

Daniel Carlson -- Tailwinds Research -- Analyst

Yeah. If anything --

Chris Cano -- Chief Operating Officer

Do you want to talk -- go ahead.

Daniel Carlson -- Tailwinds Research -- Analyst

Go ahead. Go ahead, Chris.

Chris Cano -- Chief Operating Officer

I was going to say with the timing on the VORI and TAC, Dan. So right now, right, we're in the preparation process. So as Glenn mentioned earlier in his comments, the Phase 2 interim data is really a key milestone, right? So right now, we're doing -- from a process standpoint, we've done all of our work. We've engaged with Torreya.

They're representing us in this process. We've compiled all of the diligence materials in the data room. That data room is -- currently, we do have potential partners in the data room performing diligence right now. We've also assembled a comprehensive list of potential partners that will be reaching out.

And it's really all focused around delivery of the Phase 2 interim data.

Daniel Carlson -- Tailwinds Research -- Analyst

Got you. OK. Well --

Glenn Mattes -- President and Chief Executive Officer

Yeah. We'll take that and practical. I think -- I don't know how many -- we're trying to get away for the numbers, but the last couple of weeks, we've opened up a handful of new -- just in the last couple of weeks, new MTAs. And as I think about it, they're like mid-tier.

So the pursuit of the technology as an opportunity to reformulate or do formulation, it doesn't seem to be diminishing at all. And then just, in other words, most of our work is on NCEs, it's not on reformulation. So that also, I think, makes us a little bit more bulletproof. And look, I'm sorry to do this, I can't help but also say, look, you have to think of TFF as a platform technology company.

We're not a biotech company. Biotech companies have a 100% chance of spending money on studies. Our platform technology is going -- has value, and we'll bring in revenue. And I think that speaks a little bit to how we're being treated perhaps a little bit unfairly in the marketplace.

And look, I get it, but I just couldn't help us saying it. So sorry, I can't.

Daniel Carlson -- Tailwinds Research -- Analyst

No problem. That kind of segues nicely. So a question for Dr. Williams.

I'm just trying to if you could help me understand the significance of the data that he presented at that conference that that would be great.

Bill Williams -- Scientific Consultant

Yeah. Thanks, Dan, and hello to everyone. So the data at the RDD meeting, we had five presentations, and we were able to present on different applications of tacrolimus, voriconazole, some of our new work on biologics, the plasma DNA work. It was very well received.

And in fact, I was in several other presentations during the time. And now the thin film freezing platform is regularly referenced by other speakers in the same breath that they're talking about some of the competing technologies. And so that's really good. So that was the context of the presentations throughout that meeting.

Daniel Carlson -- Tailwinds Research -- Analyst

Great. Thank you. And then, Glenn, one last question for me, just kind of related to the Union and niclosamide. Maybe you can talk about the potential for niclosamide beyond COVID-19.

Glenn Mattes -- President and Chief Executive Officer

Sure. So I was just also [Inaudible] to the conference Bill referenced. Catalent made a presentation on their work and clearly a big chunk around TFF. That was really nice to see.

So we think there's a tremendous amount of potential for niclosamide. It's a potent antiviral. I'll have Dale speak about scientifically and clinically why. But to validate that, we are doing an extensive deep dive strategically into what those viral infections are that would pose the most opportunity.

We went into the exercise thinking perhaps RSV and VSV, but we're also broadening that horizon. We've engaged a group to work with there that is helping us with the analysis. We're looking at pricing. We're looking at the IP issues, if there are any, around what we would have.

We're talking to payers. So to sort of validate the scientific and clinical hypothesis, we're also doing a deep strategic dive to understand what's our best path forward. We'll have those data in the next two to four weeks to go along with Dale's working up what clinical trials might look like, costs for that. So we have a good understanding of not only important clinical significance might be, but what the business opportunity might be.

Now do we go out after this on our own? Well, right now, Union would have the options first for that. And we also think that these data will be helpful to Union to see help them deliberate their path forward and outcome.

Daniel Carlson -- Tailwinds Research -- Analyst

Great. Thanks, guys. I'll jump back in the queue.

Glenn Mattes -- President and Chief Executive Officer

OK. Oh, wait. Dale, do you want to add some clinical commentary on those as well?

Dale Christensen -- Director of Clinical Development

Yeah. So there is published information out there that has existed for a while, showing that niclosamide is broadly active agent against all coronaviruses with activity against the MERS coronavirus that came out in the Middle East area, as well as the original SARS coronavirus that emerged in the 2004 to 2007 time frame. And in addition to that, it has been published as a 2-nanomolar EC50 against RSV. And it was clinical eye so that's both RSA A and B type strain.

So it's a broad-acting antiviral against these respiratory viral pathogens that cause viral pneumonias. And so we think that there's a high degree of ultimately, the vision would be that a patient experiences a severe upper respiratory infection that could be viral. They call their doctor, and they get this. And it would be the amoxicillin of antiviral for respiratory infections.

Daniel Carlson -- Tailwinds Research -- Analyst

Got you. That's helpful. And maybe available for the next COVID-22 or whatever, so perfect. All right.

Thanks, guys. Appreciate it. 

Dale Christensen -- Director of Clinical Development

Thanks, Dan.

Operator

And our next question is from Mayank Mamtani with B. Riley Securities. Please go ahead.

Yuan Zhi -- B. Riley Securities -- Analyst

Hi, good afternoon. This is Zhi Yuan on for Mayank. Congrats on the quarter and all the new additions to the team. A quick question on the two internal programs first and then a quick follow-up.

Could you remind us of the enrollment targets for each of the trials? And then what the interim analysis looks like in terms of the endpoints on safety and efficacy that you plan to report?

Glenn Mattes -- President and Chief Executive Officer

Dale, we just -- we decided to disclose those, but you would know it's just -- if we have using [Inaudible].

Dale Christensen -- Director of Clinical Development

Yeah. So we haven't disclosed the enrollment targets but I -- so I'll speak more to the interim analysis. Essentially, what we're -- both of the studies are open-label studies. As you can imagine, when you're doing a comparator between an oral and an inhaled therapy, and especially when the oral therapy can require dose adjustment to hit a target blood level, it is really difficult to think about how you blind that.

So we are using completely objective endpoints, things like overall survival dose requirements for dose adjustment discontinuation due to going on to salvage therapies, as well as things like in the case of voriconazole, chest CT scans, and looking at the cultures, to see if we're clearing the lungs of the fungus. And so all very clear objective endpoints, and therefore, we can do open label because the more objective your endpoints are, the more accepted in open-label type trial is because you don't have that kind of judgment involved in determining an endpoint. In the case of -- and so the interim analysis there will generate things like the differences between the oral and inhaled and treatment failures that require salvage therapy. The -- we'll also be looking at, as mentioned before, drug-drug interactions because many of the patients in this study are going to be on tacrolimus or other chemotherapy drugs that are interacting with CYP3A and therefore, would require drug-drug interaction monitoring.

And so it will be the proportion of patients that had to have their other concomitant medications adjusted due to the introduction of the voriconazole and overall safety and then overall kind of stabilization from a clinical perspective, how many achieved essentially clearance of the fungus from the lung, how many achieved reduction in chest CT scan infiltrates. So those are the things that will come out of the VORI trial. In the TAC trial, again, it's open label, and it's all one armed because these are -- the patients that are going into this study are all receiving oral tacrolimus but are experiencing significant kidney toxicity to the point that their physicians are contemplating either drug holidays or significantly reduced doses of voriconazole to try and spare the kidneys. So we will be looking at the stabilization of kidney function, can we see that we either stabilize, stop the increases in creatinine, or reduction in GFR.

Can -- and does it stabilize? Or can it even improve? And then from the efficacy standpoint, we are looking at several different markers using different biomarker techniques from endobronchial biopsies that can tell us if there's signs of acute rejection going on in the lung. So we'll be able to compare the continuation of effective immunosuppression and prevention of rejection in the lung along with stabilization of the kidney function.

Yuan Zhi -- B. Riley Securities -- Analyst

Excellent. Thanks for that extra color. That's really helpful. And looking forward to the analysis at the end of the third quarter.

Operator

Thank you. And the next question will be from Anthony Plogesma, a private investor. Please go ahead.

Unknown speaker

Hey, Glenn. Thanks for taking my call.

Glenn Mattes -- President and Chief Executive Officer

Yeah. Thank you.

Unknown speaker

I was wondering if you could give us the status on the Augmenta program and then followed up with any updates you could give on the UGA, ACOM and UPenn.

Glenn Mattes -- President and Chief Executive Officer

OK. I'll give you an over-the-top on the Augmenta program. And as you know, we have been really enjoying our work with Augmenta, very unique and innovative company. We've taken the 3387 molecule preclinical development.

We've looked at the potency in animal models against SARS-CoV-2 and its variants. And it's all been very successful. We've seen positive binding. We've seen positive neutralization.

The neutralization that we've seen in the Omicron variant and certainly not been at the same level that has been seen with the other variants. And this is a common theme, as you know, in what monoclonal antibodies have become in the overall armamentarium to treat COVID. We have a number of, I think, very creative ideas in terms of how to continue to develop Augmenta 3387. It is a bit of on the right turn from where we were headed.

I don't want to share those ideas. Because I think they're very unique, and we don't want to tip what we've come up with to the rest of the marketplace. We are working with one of our scientific advisory board members to help us craft that strategy. Dale, I don't know if you want to add anything to that, but we still believe in Augmenta, we still believe in the compound.

We think we have something that has clinical value. And we also believe that there's a need for monoclonals in treating COVID-19 today and tomorrow. Dale, I don't know if you want to add to that or not.

Dale Christensen -- Director of Clinical Development

Yeah. Thanks, Glenn. As Glenn pointed out, part of our commitment is to monitor ongoing and emerging variants as they occur and looking at the activity. So as we proceed, we are testing against various emerging variants and ensuring that it works.

And as you've seen with the Omicron variant, there's been, and especially with VA2 now, every commercial antibody that's already been given EUA either had the EUA removed or revoked. And so it's a difficult place right now for antibodies in the Omicron world. And so we're still assessing all of that activity.

Unknown speaker

OK. Thank you.

Glenn Mattes -- President and Chief Executive Officer

Can you say -- repeat your second question?

Unknown speaker

It was on if you could give any updates on what you're doing with UGA, UPenn, along those lines.

Glenn Mattes -- President and Chief Executive Officer

Sure, sure. Chris?

Chris Cano -- Chief Operating Officer

Yeah, sure. Thanks, Glenn. So on our academic collaborations, you had mentioned UGA, Albert Einstein, and UPenn. So I'll take them one at a time.

So we're working with Dr. Kartik Chandran at Albert Einstein, right? We've successfully completed our vitro testing of our dry powder. And we're in the process of conducting a large in vivo study with their VSV for COVID. We're performing an efficacy study in hamsters.

And this study is being done and performed in collaboration with the researchers at USAMRIID and the Geneva Foundation. So very excited about the work we're doing with Dr. Chandran. In collaboration with Dr.

Ted Ross at UGA. So we've prepared dry powder versions of their universal influenza vaccine. That's the one that has AddaVax as an adjuvant. And so we've completed in vitro testing and in vivo testing in both mice and ferrous on our dry powder vaccines, right? And that allowed us to confirm that our dry powder preparation maintain the immunogenicity and efficacy.

Our dry powder performed very well. So we're in discussions with UGA and MIG on clearly defining next steps on advancing our TFF dry powder version of their universal influenza vaccine and how into the clinic. For UPenn, our collaboration with Dr. Drew Weissman, we've completed our initial mRNA formulation work.

We've identified our lead optimal formulations. We finalized our protocols for animal testing, and we're preparing to deliver our TFF dry powder samples to Dr. Weissman so that they can commence these animal studies in the very near future. So we continue to push very hard on all of our academic collaborations.

Unknown speaker

Excellent. Thank you.

Operator

Thank you. And the next question will be from Richard Deutsch with National Securities. Please go ahead.

Richard Deutsch -- National Securities -- Analyst

Yes. Thank you for taking my call. And there's almost too broad landscape to have to get into one call. I sympathize with people trying to get specific.

So I'm going to just ask one question and come back and if you have enough time to get to a couple of them. But you did just announce another major commercial partner which is Aptar, which -- if people don't know them, they're on the New York Stock Exchange. And even on this market conditions, they're $6.8 billion major corporation. It's been in business commercially successful.

Can you tell us a little bit about what this partnership means? And how have they decided to move forward and what their milestones? And what they're looking to do over the next six to 12 months?

Glenn Mattes -- President and Chief Executive Officer

First of all, thank you, Richard, for noticing that. We did put out a new corporate presentation and I guess, Richard doing his diligence notice that I went out on a commensurate with the press release. I'll have Chris gets all the credit for this one. So as he does, frankly, for all the transactions.

So I'll have him give you the details there.

Chris Cano -- Chief Operating Officer

Great. Thanks, Richard. So really excited about our partnership with Aptar. This is a new initiative.

So the concept is formulating our TFF dry powder for use in an intranasal device. So TFF working with Aptar and using their proprietary intranasal device. So we're running some initial experiments and if these initial experiments proved successful, we believe that our TFF dry powder brings unique attributes, right, for nasal administration. And this is not only for vaccines but also for therapeutics.

So depending on the compound and the disease states, this could be very advantageous for both patients and prescribers. So the way that it's structured is many of the Aptar customers are looking for dry powder intranasal delivery, right? And at TFF, we're fielding very similar inquiries from our partners, can you deliver intranasally. So the concept is marrying our respective technologies. The TFF dry powder technology with the Aptar proprietary device and then we can drive our collaboration to address each of our respective customers' needs.

So again, as I mentioned, it really depends on the compound and the disease state where dry powder intranasal spray could be very advantageous for delivery of vaccines and therapeutics. So it's really proof of concept. We're doing some experimental work right now. So I look forward to sharing the progress as we continue down this road with that trial.

So thanks for the question.

Glenn Mattes -- President and Chief Executive Officer

It also really is synergistic with the Catalent partnership. We, as a team, have the opportunity to visit just a couple of weeks ago, their site in Boston, which is an inhalation site and they're doing nasal work as well. So we anticipate that we're going to get a lot more opportunities to work in the intranasal space. And the Aptar relationship could not come at a better time.

So this is all coming together quite nicely. operator, next questioner, please.

Operator

Sure. Next question is from Ted Ketterer with TK Associates. Please go ahead.

Ted Ketterer -- TK Associates -- Analyst

Hi, guys.

Glenn Mattes -- President and Chief Executive Officer

Hi, Ted.

Ted Ketterer -- TK Associates -- Analyst

Glenn, to be very candid, the elephant in the room is your balance sheet and what three quarters of cash. And so far, there's no progress in terms of any incoming revenue. My question is, are we going to get diluted at $2 a share? Or are you guys -- is it something going to happen that's going to put your balance sheet in a position where the people who scale the market for companies that are going to run out of cash shorter than depressive stock. The rest of what you're doing is fabulous, but the fact of the matter is, OK, there are companies that's got about $8 million a quarter in expenses.

And you're adding -- it sounds like you're adding expenses with three new people and five new partners. Can you comment?

Glenn Mattes -- President and Chief Executive Officer

OK. Well, Ted, just to correct you, we capitalized through to the mid part of next year, almost through August. So we have more than nine months. We believe we are very well capitalized.

You know our business model. And I'll leave it at that. We're well capitalized. We manage our budgets extremely well.

And I have nothing else to say than that. We've talked about our business model repeatedly. I said on this call that we are extremely optimistic about our ability to close transactions with meaningful revenue.

Operator

Thank you, sir. And the next question will be from Leo Saraceno with Waushacum Capital. Please go ahead.

Leo Saraceno -- Waushacum Capital -- Analyst

Hi, Glenn. I got a question regarding your open MTAs. Would you be able to break down what percentage of the MTAs are biologics versus vaccines, mRNA, mAbs, etc., along those lines?

Glenn Mattes -- President and Chief Executive Officer

OK. I'm going to put my friend, Chris Cano, on the spot here. That, he knows, but he may not know offhand. So Chris, if you could try out, please do.

Chris Cano -- Chief Operating Officer

Sure. Thanks, Leo. Thanks for the question. So if I take a look at all of our ongoing collaborations, right, in our different MTAs, we have a tremendous focus on biologics.

So we're -- of all of our different NTAs, over 87% of them are really focused on biologics. And as Glenn had mentioned earlier, all of these biologics are NCEs, right, to our partner or to the originator of the technology. So if I had to -- what I can share with you, Leo, is more of these collaboration projects, right? We're focused on biologics over 87%. Well, of that 65% of these projects are oral inhalation, right, as the primary route of administration of our dry powder versus 30% of our projects, which are more of a stable dry powder for reconstitution and injection as the route of administration.

We have a couple of other projects which have alternate routes of administration. But by and large, there are a large number of projects that overlap. So we're working with partners on a dry powder vaccine. And the second project with that partner is an oral inhalation and now with our new Aptar engagement and arrangement.

Based on demand, we're now looking at intranasal delivery of our dry powder. So hopefully, that addresses your question, Leo, and gives you a little context of where our focus is and where our MTAs are.

Leo Saraceno -- Waushacum Capital -- Analyst

Great. Great, Chris. That's very helpful. Thanks.

Glenn Mattes -- President and Chief Executive Officer

We probably have time for one more question. Is there any --

Operator

Yes. Then our final question will be a follow-up from Richard Deutsch with National Securities. Please go ahead.

Richard Deutsch -- National Securities -- Analyst

Yes. Thank you again for -- you did mention in your presentation that you had interacted with Glass House, which has finally purchased PLUS Products. And can you give us a little bit more of an update on how soon we might see a decision on commercialization? And I just want to -- just make one comment about Ted's question about running out of money. Obviously, your business plan has monetization of TAC, VORI, niclosamide, the cannabis products, government programs themselves evolve into higher and higher levels of product development and thus inventory purchase, those alone would be enough to start a separate company.

So I just wanted to throw that in as Ted's comments seem to be out of line with the reality of what you've done, putting all of these products into final stage over the last year or two.

Glenn Mattes -- President and Chief Executive Officer

Yeah. Thanks for the comment, Richard, and other opportunities, clearly. Specifically, we have what we believe, first and foremost, Richard, our go-to-market assets, our formulations. And I have to really -- again, I said this call after call, PLUS has been a remarkable partner to us in helping us develop these go-to-market assets.

They've helped us test them in the marketplace. Congratulations to PLUS for culminating their restructuring with Glass House. The feedback I have from the PLUS management is that Glass House is interested, certainly. But we have -- in all this time, we have contingencies in place to get our compounds to the marketplace as quickly as possible.

Everyone we've talked to is very impressed with our compounds. And as I said, we will hopefully, do this through Glass House. But it's not we have contingencies. So we are excited about the opportunities here.

And our goal is to get the first commercial sale as quickly as possible, realizing look at the PLUS situation didn't help witjyou know, I make myself quite available to you. So if you have any questions at any time, you can contact me or Corey, and we'll answer your questions. I hope you all stay well, and thank you. Enjoy your evening.

Operator

[Operator signoff]

Duration: 58 minutes

Call participants:

Glenn Mattes -- President and Chief Executive Officer

Kirk Coleman -- Chief Financial Officer

Jonathan Aschoff -- ROTH Capital Partners -- Analyst

Dale Christensen -- Director of Clinical Development

Daniel Carlson -- Tailwinds Research -- Analyst

Chris Cano -- Chief Operating Officer

Bill Williams -- Scientific Consultant

Yuan Zhi -- B. Riley Securities -- Analyst

Unknown speaker

Richard Deutsch -- National Securities -- Analyst

Ted Ketterer -- TK Associates -- Analyst

Leo Saraceno -- Waushacum Capital -- Analyst

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