Veru Inc. (VERU) CEO Mitchell Steiner on Q3 2022 Results – Earnings Call Transcript

Veru Inc. (NASDAQ:VERU) Q3 2022 Earnings Conference Call August 11, 2022 8:00 AM ET

Company Participants

Samuel Fisch – Executive Director, IR & Corporate Communications

Mitchell Steiner – Chairman, President & CEO

Michele Greco – CFO & Chief Administrative Officer

Gary Barnette – Chief Scientific Officer

Conference Call Participants

Brandon Folkes – Cantor Fitzgerald

Leland Gershell – Oppenheimer

Chris Howerton – Jefferies

Yi Chen – H.C. Wainwright

Operator

Good morning, ladies and gentlemen, and welcome to Veru Inc’s Investor Conference Call. All participants will be in listen-only mode. [Operator Instructions] After this morning’s discussion, there will be an opportunity to ask questions. Please note that this event is being recorded.

I would now like to turn the conference call over to Mr. Sam Fisch, Veru Inc’s, Executive Director of Investor Relations, and Corporate Communications. Please go ahead.

Samuel Fisch

Good morning. The statements made on this conference call may be forward-looking statements. Forward-looking statements may include but are not necessarily limited to, statements of the company’s plans, objectives, expectations or intentions regarding its business, operations, finances and development and product portfolio.

Such forward-looking statements are subject to known and unknown risks and uncertainties and our actual results may differ significantly from those projected, suggested or included in any forward-looking statements. Risks that may cause actual results or developments to differ materially are contained in our 10-Q and 10-K SEC filings, as well as in our press releases from time to time.

I’d now like to turn the conference call over to Dr. Mitchell Steiner, Veru Inc’s, Chairman, CEO and President.

Mitchell Steiner

Good morning. With me on this morning’s call are Dr. Gary Barnett, Chief Scientific Officer; Michele Greco, the Chief Financial Officer and CIO; Michael Purvis, Executive VP, General Counsel and Corporate Strategy; and Sam Fisch, Executive Director of Investor Relations and Corporate Communications. Thank you for joining our call. Veru is a biopharmaceutical company focused on developing novel medicines for COVID-19 and other viral and ARDS related diseases, and for the management of breast and prostate cancers.

The company has a commercial sexual health division called Urev, which includes two FDA approved products ENTADFI, a new treatment for benign prostatic hyperplasia and the FC2 female condom, internal condom for the dual protection against unplanned pregnancy and the transmission of sexually transmitted infections. The revenue from the sexual health division is being used to largely fund the clinical development of our late-stage drug candidate assets, which aim to address multi-billion dollar premium market opportunities.

This morning, we will provide an update on the COVID-19 Sabizabulin and clinical program and franchise, the clinical development of our oncology drug pipeline and the commercialization of our products. We will also provide financial highlights for our third quarter fiscal year 2022. First, I will update you on the status of our investigational drug candidate Sabizabulin for the treatment of hospitalized COVID-19 patients at high risk for ARDS.

We conducted a successful Phase III COVID-19 clinical trial, which was a double-blind multicenter, multinational randomized two to one placebo-controlled study evaluating daily oral 9 milligram dose of Sabizabulin for up to 21 days versus placebo in 204 hospitalized moderate to severe COVID-19 patients with high risk for ARDS and death. Both the placebo and Sabizabulin treated groups were allowed to receive standard of care which could include Dexamethasone, Remdesivir, anti-IL6 receptor antibodies and JAK inhibitors. Moderate to severe COVID-19 infection patients of those who were hospitalized and required supplemental oxygen with at least one comorbidity, non-invasive ventilation force oxygen or mechanical ventilation.

Furthermore, patients must have had a peripheral capillary oxygen saturation less than equal to 94% at room air and hospital admission. The goal was to select patients at high risk for progression to ARDS and death. The primary endpoint which of a portion of patients who die on study up to day 60, not to day 29, like the other Phase III clinical studies reported in the literature. Having a primary endpoint at day 60 allowed us to capture a more accurate and potentially greater number of deaths caused by COVID-19 infection.

Key secondary endpoints measured included the proportion of patients without respiratory failure, days in the ICU, days on mechanical ventilation, days in the hospital and viral load. The study was conducted in the U.S., Brazil, Argentina, Mexico, Colombia and Bulgaria and the COVID-19 infections in the study, due to both the Delta and Omicron variants.

On April 8, 2022, the Independent Data Monitoring Committee conducted a plan interim analysis in the first 150 subjects randomized in the Phase III COVID-19 study. After reviewing the unblinded clinical data, the independent data monitoring committee unanimously recommended that the Phase III study be halted early due to clear clinical efficacy benefit. The IDMC also remarked that no safety concerns were identified.

In this interim analysis, Sabizabulin treatment demonstrated a statistically significant 24.9 percentage point absolute reduction and a 55.2% relative reduction in all-cause mortality by day 60, which is the primary endpoint of the study with an odds ratio of 3.23, 95% confidence interval of 1.45 to 7.22 with a p-value equals 0.0042. The beneficial effects of Sabizabulin were observed starting as early as day three after dosing. And by day 15, statistically significant reductions and mortality were observed, the beneficial effects of Sabizabulin treatment of mortality were maintained to date 29, a standard time point for other studies that other studies have used as the efficacy endpoint, with a mortality rate of 35.2% for placebo compared with 16% for Sabizabulin, which is an absolute reduction of 19.2 percentage points and a relative reduction of 54.5%.

From day 29 to day 60, the death rate increased by 9.9 percentage points in the placebo group and by only 4.2 percentage points in the Sabizabulin treated group, showing that the mortality benefit of Sabizabulin was still clinically evident. This efficacy is further supported by the consistency of the mortality benefit across subgroup analyses of the primary endpoint. Clinically meaningful reductions in deaths with Sabizabulin treatment compared to placebo was observed regardless of standard of care treatment received, baseline WHO Ordinal score, sex, age, baseline comorbidities, BMI or geographic location.

In the full overall final data set of 204 randomized patients, the all-cause mortality benefit was similar to the result observed in the interim efficacy analysis population with Sabizabulin treatment resulting in a 51.6% well reduction in deaths compared to placebo treatment. In both the interim analysis, efficacy and the overall 204 patient study groups, the key secondary efficacy endpoints demonstrated that Sabizabulin treatment resulted in a significant reduction in days in the ICU, days on mechanical ventilation, days in the hospital compared with placebo.

So, Sabizabulin had an acceptable safety profile, significantly fewer adverse and serious adverse events were reported for Sabizabulin compared to placebo. There were also fewer treatment discontinuations due to adverse events in the Sabizabulin group compared to placebo. The Phase III reported safety profiles suggest that Sabizabulin treatment may have resulted in fewer COVID-19 related morbidities, especially respiratory failure, pneumothorax, acute kidney injury, cardiac arrest, septic shock and hypertension.

The Phase III clinical trial interim efficacy and full study safety results were recently published the New England Journal of Medicine Evidence online on July 6, 2022. We’re now completing the final clinical study report for the overall study of 204 randomized subjects and we plan to submit a manuscript of full data set to a major peer reviewed medical journal soon. On May 10, we had a pre-emergency used authorization meeting with FDA to discuss the next steps, including the submission of an emergency use authorization application. We were told by FDA to submit the request for EUA.

On June 6, we submitted a request for EUA to FDA. As you know, there is no preset PDUFA date to have decision on a request for an EUA. We know FDA is actively reviewing the application. We have received and have responded to several requests for additional information to help their ongoing review. FDA has conducted a successful pre approval inspection of one of our manufacturing facilities. FDA has also already audited two U.S. clinical sites with no adverse findings and has scheduled audits of the clinical site in Bulgaria and one in Brazil, which should both be completed by the end of August. FDA has informed us that our request for an EUA application is a high priority.

Other major regulatory updates. On July 25, we announced that the United Kingdom’s Medicines and Healthcare Products Regulatory Agency, the MHRA, considers that the currently available safety and efficacy data will support an expedited review of the marketing authorization application with the company’s Sabizabulin treatment in the hospitalized COVID-19 patients and high risk for acute respiratory distress syndrome when the application is submitted.

On July 27, we announced that the European Medicines Agency, EMA, Emergency Task Force has informed the company that has initiated the review of Sabizabulin for the treatment of hospitalized COVID-19 patients and high risk acute respiratory distress syndrome. The emergency task force’s formal press release stated “the review will look at all available data, including data from a study involving hospitalized patients with moderate to severe COVID-19, who had high risk for acute respiratory distress syndrome and death. The results of this study, which is the New England Journal of Medicine Evidence publication would indicate that Sabizabulin treatment reduces the number of deaths in these patients compared with placebo.”

The review will assist the EU member states who may consider allowing use of the medicine before possible approval. The review is the first — this review is the first to be triggered under article 18 of the new EU regulation that expanded evolved EMA during public health emergencies, not only have we subsequently submitted an application, but we have also — we also had active discussions with the Emergency Task Force. We are also in various stages of discussion with regulatory agencies and other countries to obtain regulatory emergency or expedited authorization with Sabizabulin.

Furthermore, we have made great progress in our discussions for advanced purchase agreements with government officials outside the U.S. As with the commercial manufacturing status for Sabizabulin drug product, we have scaled up manufacturing processes and should be able to produce commercial drugs supply to address the anticipated drug needs following a potential FDA authorization in the U.S. and potential subsequent authorizations and approvals in other countries and territories.

With Sabizabulin in U. S. commercial update, we have hired Joel Batten, as Executive Vice President, the General Manager of Veru’s U.S. Infectious Disease Franchise effective May 23, 2022 and most recently Mr. Batten has been the head of the Respiratory Syncytial Virus, RSV franchise at Sobi North America, where he is responsible for Synagis business with revenue of approximately $600 million and a team of over 160 employees. Mr. Batten led strategy for the RSV franchise as well as market access, distribution and patient access services.

Prior to Sobi, he spent approximately 20 years in a number of positions of increasing responsibility in AstraZeneca / MedImmune and Sanofi Aventis in the various infectious disease franchises including commercial infrastructure build-out, sales management, marketing, public health sales, and government affairs. He has put the core U.S. Infectious Disease commercial leadership in place. We have contracts executed for the commercial launch teams, market access, medical affairs and distribution services for Sabizabulin. We are ready for the launch of Sabizabulin into hospitals and for granted emergency use authorization.

We recently presented scientific results from the Phase IIII Sabizabulin clinical program at the International Conference on Emerging Infectious Diseases in 2022 in August 8, in Atlanta, Georgia. The presenter was Dr. Michael Gordon, who is Chief Medical Officer at HonorHealth Research & Innovation Institute, Scottsdale, Arizona. So here we are COVID-19 Global cases, hospitalization and deaths on the rise again with an unexpected summer surge. The emergence of serious COVID-19 variants BA.4 and BA.5 have led to this new surge and these mutated strains have the ability to infect vaccinated patients.

The White House warrants that expect over 100 million new cases in the fall in winter. Over 1 million Americans have died from COVID-19. We must reduce the risk of death in COVID-19. Vaccines are not enough. Antivirals, PAXLOVID and Molnupiravir target the non-hospital general population, who’ve experienced less than five days of symptoms with a narrow therapeutic window of opportunity. PAXLOVID cannot prevent COVID-19 infections and is not effective in low risk population. Antivirals like Molnupiravir do not work in hospitalized minor to severe COVID-19 patients.

U.S. deaths in COVID-19 are now averaging 500 deaths a day and these patients are dying in the hospital. The death rate is unacceptable. It is clear that an effective and safe oral therapeutic to treat hospitalized, moderate to severe COVID-19 patients with high risk with ARDS that prevents deaths is desperately needed. We strongly believe that Sabizabulin with its dual anti-viral and anti-inflammatory properties can be that greatly needed oral therapy for hospitalized moderate to severe COVID-19 patients as the new standard of care.

We plan to initiate additional clinical studies to evaluate Sabizabulin treatment in other populations at risk for death from COVID-19 infection and as a treatment for other viruses that cause ARDS, including influenza A virus, which causes up to 52,000 deaths and 710,000 hospitalizations each year. And Respiratory Syncytial Virus, which causes 14,000 deaths and 177,000 hospitalizations each year in the U.S. These additional clinical studies that’s successful will allow us to expand Sabizabulin to other large serious infectious disease indications.

Some of these planned clinical trials include a Phase III randomized placebo controlled efficacy and safety study of Sabizabulin for the treatment of severe — for the treatment of COVID-19 hospitalized patients who are — who threes, which means they’re in the hospital at in trouble, but not on oxygen. And also the who falls without the avid presence of a comorbidity. And so that allows us to approach the other 50% of patients that are hospitalized. Phase III — the other trial is a Phase III randomized placebo controlled efficacy and safety study of Sabizabulin for the treatment of hospitalized patients with Acute Respiratory Distress Syndrome due to any viral illness.

I will now briefly discuss the progress of our oncology drug portfolio that’s focused on breast and prostate cancers. For patients with greater than equal to 40% AR expression, we are actively enrolling a global Phase III ARTEST registration clinical trial in approximately 210 patients who evaluate the enobosarm monotherapy for third-line treatment of AR positive, ER positive, HER2-negative metastatic breast cancer.

We’ve also moved the enobosarm monotherapy earlier in the treatment sequence into second line treatment setting for AR positive, ER positive, HER2-negative metastatic breast cancer. We are actively enrolling in a Phase III multicenter open label randomized active control registration ENABLAR-2 clinical study to evaluate the efficacy and safety of enobosarm and abemaciclib combination therapy versus an alternative estrogen blocking agent and subjects with AR positive, ER positive, HER2-negative metastatic breast cancer, who have failed first-line therapy with palbociclib, which is a CDK4s/6 inhibitor plus an estrogen blocking agent, who have greater than equal to 40% AR expression in their breast cancer tissue. Plan to enroll approximately 186 subjects in this Phase III clinical study.

We have a clinical trial collaboration and a supply agreement with Lilly for this ENABLAR-2 Phase III clinical study. Under the terms of the non-exclusive clinical trial collaboration and supply agreement, Veru is responsible for conducting the clinical trial, while Lilly is supplying and been a cycle for the study. Veru maintains full exclusive global rights to a enobosarm.

We’ve also made good progress in our prostate cancer program. Our first indication is evaluating Sabizabulin for third-line treatment of metastatic castration resistant prostate cancer in the Phase III VERACITY study. We have recently published in clinical cancer research, the clinical results of the positive Phase 1b/2 study of Sabizabulin in 80 men with metastatic castration resistant prostate cancer, who have progressed on at least one novel androgen receptor targeted agent.

A summary of the results published was that the maximum tolerated dose was not reached in the Phase 1b and the recommended Phase II dose was set at 63 milligrams a day. Most common adverse events, which is greater than 10% frequency at the 63 milligram oral daily dosing in the combined Phase 1b/2 data were predominantly grade 1 and 2 events, greater than three events included diarrhea at 7.4%, fatigue at 5.6% and alanine aminotransferase and the Aspartate aminotransferase elevations of 5.6% and 3.7% respectively.

Neurotoxicity and neutropenia were not observed. [indiscernible] clinical data in patients treated with greater than one continuous cycle of 63 milligram or higher, including an objective response rate in six of 29 or 20.7% of patients with measurable disease, which is one complete and five partial responses and 14 of the 48 or 29.2% of the patients had PSA declines.

Most importantly, the Kaplan Meier median radiographic progression free survival was estimated to be 11.4 months with an end of 55 patients and we had durable responses lasting greater than 2.75 years. These data support ongoing Phase III VERACITY trials Sabizabulin in men with metastatic castration resistant prostate cancer. So we’re actively enrolling an open label randomized two to one multicenter Phase 3, VERACITY clinical study evaluating Sabizabulin 32 milligrams versus an alternative anti-receptor targeted agent for the treatment of chemotherapy naive man with metastatic castration resistant prostate cancer who have had tumor progression after previously receiving at least one androgen receptor targeted agent. The primary endpoint is radiographic progression free survival. Enrollment for the Phase 3 VERACITY clinical study is on track and we expect to enroll approximately 245 patients and 45 clinical centers in the U.S.

Our second clinical study in prostate cancer is evaluating VERU-100, the GNRH antagonist three month depot formulation in a Phase 2 dose finding clinical study for the treatment of hormone sensitive advanced prostate cancer. Although, this study is ongoing, the preliminary clinical data continues to be promising. As you can see, we have an exciting and treatment paradigm changing late clinical stage oncology portfolio of drug candidates making great progress in advanced breast and prostate cancers.

Veru has a commercial sexual health division called UREV, which includes two FDA approved products. FC2 for the dual protection against unplanned pregnancy and transmission of sexual transmitted infections, and the FDA approved ENTADFI to tadalafil and finasteride capsule and new treatment for benign prostatic hyperplasia, also known as BPH. We have built the infrastructure to allow broad market access to FC2 across the U. S. As a result FC2 is now available to multiple sales channels. We have partnered with fast growing, highly reputable telemedicine platform companies to bring our FC2 product to patients in the cost effective and highly convenient manner.

Our strategy to continue to drive FC2 sales is as follows: one, we will seek additional telemedicine internet pharmacy service partners. Two, we created and launched our own dedicated direct to patient telemedicine internet pharmacy services platform. This telemedicine platform is now up and running and is expected to be a new source of revenue. The website address is fc2condoms.com. Three, we’ve increased U.S. public sector sales by our new agreements with distribution partnerships with global protection as well as effects (ph).

We also have ENTADFI, an FDA approved new treatment for benign prostatic hyperplasia. The most common side effects of currently described BPH medicines of sexual adverse events, including impotence. ENTADFI has been shown to be faster and more effective for the treatment of benign prosthetic hyperplasia than finasteride alone without causing impotence.

I’m happy to report that we have officially launched ENTADFI and the product is available for pharmacies to dispense. We have partnered with GoodRx a U.S.-based digital resource for healthcare to reach their almost 20 million monthly visitors, which includes both consumers and healthcare providers to build awareness about ENTADFI. There are over 45 million prescriptions filled annually for drugs to treat BPH. We plan to augment our own marketing and sales efforts by seeking additional partners in the U.S. and ex U.S.

I will now turn the call over to Michele Greco, CFO and COO to discuss the financial highlights. Michele?

Michele Greco

Thank you, Dr. Steiner. As Dr. Steiner indicated, we have a lot of activity at Veru. Let’s start our highlights with the third quarter results for the three months ended June 30, 2022. Overall, net revenues were $9.6 million compared to $17.7 million in the prior year third quarter. The prescription business net revenue decrease from $13.5 million in the prior year third quarter to $6.7 million. The reduction is due to business challenges experienced by our telemedicine customers during the quarter, which resulted in a slowdown in orders during the current quarter.

Global public sector net revenues were $2.9 million compared to $4.2 million in the prior year third quarter. The decrease in sales in the global public sector during the third quarter is due to the timing of tenders. In the prior year, we sold 2.8 million units to Brazil for tenders which have ended and therefore did not repeat in the current year.

Gross profit was $7.1 million or 74% of net revenues compared to $13.9 million or 79% of net revenues in the prior year third quarter. The reduction in gross profit and gross margin is driven primarily by the reduction in sales in our U.S. FC2 prescription business.

Operating expenses for the quarter increased to $28.9 million compared to the prior year quarter of $16.7 million. The increase of $12.1 million is primarily due to research and development costs, which increased $6.9 million to $18.1 million compared to $11.2 million in the prior year quarter, and the increase in selling general and administrative expenses of $5.2 million from $5.6 million to $10.8 million in the current period.

The increase in research and development costs is due to the increased number of clinical trials. This quarter, we had four Phase III clinical trials and two Phase II clinical trials ongoing. While in the prior period, we had two Phase III clinical trials and two Phase II clinical trials ongoing. The increase in selling, general and administrative expenses is primarily due to the increase in headcount related to the preparations for the commercial launch of ENTADFI and Sabizabulin for COVID-19, resulting an increased compensation, increased stock compensation and increased sales and marketing expenses. The operating loss for the quarter was $21.8 million compared to $2.9 million in the prior year quarter.

Non-operating expenses were $234,000 compared to $2.7 million in the prior year third quarter, and primarily consisted of interest expense and changing the fair value of the derivative liabilities related to the synthetic royalty financing. For the quarter, we recorded a tax expense of $138,000 compared to a tax benefit of $2.9 million in the prior year third quarter.

The tax benefit recorded for the prior year quarter is primarily due to increased value of the UK net operating losses, due to an increase in the UK tax rates from 19% to 25%. The bottom line results for the third quarter of fiscal 2022 was a net loss of $22.2 million or $0.28 per diluted common share, compared to a net loss of $2.7 million or $0.03 per diluted common share in the prior year third quarter.

Turning to the results for the nine months ended June 30, 2022. For the first nine months of fiscal 2022, total net revenues were $36.8 million compared to $45.6 million in the prior year period. Net revenues from the U.S. prescription business were $29.9 million compared to $32.9 million in the prior year period. Net revenues for the global public health sector business was $6.9 million compared to $11.8 million in the prior year period.

The reduction in the prescription net revenues is due to the business challenges experienced by our telemedicine customers in the third quarter. The decrease in sales in the global public sector during the period is due primarily to 9.7 million units sold to Brazil, and 2.8 million more units sold to South Africa in the prior year period for tenders, which have ended and therefore did not repeat in the current year.

Overall, gross profit was $30.1 million or 82% of net revenues compared to $35.6 million or 78% of net revenues in the prior year period. The increase in gross margin is due primarily to the mix and sales with the U.S. prescription business comprising a larger percentage of total net revenues. Operating expenses increased by $29.4 million to $68.6 million compared to the prior year period of $39.2 million. The increase is primarily driven by research and development costs, which increased by $19.3 million to $43.8 million from $24.4 million in the prior year period. The increase in research and development costs is due to the increased number of clinical trials, which I discussed previously.

Operating loss for the period was $38.6 million compared to an operating income of $14.8 million from the prior year period. The change of $53.4 million is primarily due to the gain on sale of PREBOOST of $18.4 million in the prior year period. The increase in research and development costs during the current year period and the reduction in net revenues and gross profit, which occurred during the third quarter.

Non-operating expenses were $4 million compared to $5.9 million in the prior year period and primarily consisted of interest expense and the change in the fair value of the derivative liabilities related to the synthetic royalty financing. For the nine month period, we recorded a tax expense of $225,000 compared to a tax benefit of $2.8 million in the prior year period. The company has net operating loss carry-forwards for U.S. federal tax purposes of $38.8 million with $29.7 million expiring in years through 2040 and $9.1 million, which can be carry-forward indefinitely.

Our UK subsidiary has net operating loss carry-forwards of $63.5 million which do not expire. The bottom line results for the first nine months of fiscal 2022 was a net loss of $42.8 million or $0.53 per diluted common share, compared to net income in the prior year period, which included the gain on sales PREBOOST of $11.7 million or $0.14 per alluded common share.

Turning to our balance sheet. As of June 30, 2022, our cash balance was $100.6 million and our accounts receivable were $8.3 million. Our net working capital was $100.6 million on June 30, 2022 compared to $136 million at September 30, 2021. During the nine months ended June 30, we used cash of $26.6 million for operating activities compared with $14.8 million used for operating activities in the prior period.

The expected future revenues from Sabizabulin for COVID-19, the continued revenue from sales in the U.S. FC2 prescription business and global public sector business coupled with the expected future revenue from the launch of ENTADFI and added to our strong balance sheet should continue to be the source of funds we use for commercial activities and to invest in our promising pharmaceutical clinical development programs as we continue to focus on developing novel medicines for COVID-19 in other viral and ARDS related diseases, and for the management of breast and prostate cancers.

Now I’d like to turn the call back to Dr. Steiner.

Mitchell Steiner

Thank you, Michele. In summary, we continue to advance our core deep late clinical stage, breast cancer and prostate cancer programs with three actively enrolling Phase III clinical studies and we have significant revenue generated more base sexual health business and have authorized, we expect to have substantial future revenue, Sabizabulin, 9 milligrams for hospitalized COVID-19 patients at risk ARDS.

Being opportunistic and successful in developing Sabizabulin to COVID-19 has led to the most eventful and transformative period in Veru’s history. We are preparing for the U.S. and global commercial launch of Sabizabulin and 9 milligrams for the treatment of hospitalized moderate to severe COVID-19 patients with high risk ARDS. As you can see from our balance sheet, we have the resources with these launch activities in the U.S. and global, if granted emergency use authorization. Again, we believe this will be an opportunity for significant near term revenue for Veru.

With that, I’ll now open the floor — the call to questions. Operator?

Question-and-Answer Session

Operator

Thank you. Ladies and gentlemen, at this time, we will begin the question-and-answer session. [Operator Instructions] Our first question comes from Brandon Folkes from Cantor Fitzgerald. Please go ahead.

Brandon Folkes

Hi. Thanks for taking my questions and congratulations on all the progress. Just from me, I guess, first up the multi-part question. Can you just elaborate on the order for these clinical sites and how typical of this is any sort of EUA approvals? Any indication at this stage that the two upcoming ex U.S. sites orders would be the last or do you believe the agency may look to continue to order additional facilities? And then within that, were these facilities picked randomly, granted the FDA, picked it, but if any commentary, or are there any data outlier that may have driven the selection of these orders?

Samuel Fisch

Okay. And make sure I understand the first question. So — say it again, it relates to clinical trials. Are you talking about the new additional ones?

Brandon Folkes

Yeah. The clinical sites. So the

Samuel Fisch

Clinical sites…

Brandon Folkes

Okay. Fine.

Samuel Fisch

Okay. No, your first question. So it always about clinical science.

Mitchell Steiner

Okay. My bad as they say. So, no, I don’t — so first of all, our expectation is that the FDA after they audit these two sites, there’s no indication that they’re going to be auditing additional sites. They’ve been pretty clear. As it relates to why they picked these sites. There is no indication at any particular site as an issue. This is done under GACP. We have an excellent CRO called World Clinical Trials, and the impression that we get is that the FDA is checking their boxes as they go through this very important review. And so, I see this as routine. I do have with me Dr. Gary Barnette, who is our Chief Scientific Officer and do you want to add comments to that?

Gary Barnette

Yeah. This is generally a standard practice under NDA review where they go into these clinical sites and they pick the clinical sites, the review team selects the clinical sites for things like the number of patients that they put in the study and that kind of thing. So the two in the U.S. have been completed without any findings, adverse findings, the two outside. It does take a little longer for the FDA to schedule sites outside the United States for audit because of all the political things that have to go on with that. But we expect these sites to do very well in those audits. But as Mitch mentioned, do not believe that there’ll be any additional audit to clinical sites after these.

Brandon Folkes

Great. I appreciate the additional color. And then maybe just should you receive an EUA. How should we think about how quickly you can get the product into the hands of the hospitals?

Mitchell Steiner

Yeah. Great question. So we have done a lot of work. Thanks to the internal team and we quickly assembled a team, but it’s a robust team. And for things that we can’t do internally, i. e., bring — we brought in sort of the Chiefs. We’re contracting out with very reputable groups. One of the things that we’ve also done is, we’ve also signed up a very reputable and massive distribution wholesaler. And because that’s really — that’s the way the hospitals work.

That’s where you need to drop ship your product and that distributor is the one that gets it to all the hospitals and it’s very routinely done and very efficiently done. The one that we picked also is a big player with government contracts as well. And so it’s pretty robust. So with that said, if we get the EUA — when we get the EUA and we get the word, go, we believe it will be somewhere between nine days to 14 days that we will have the drug available with dispense in hospitals in the U.S.

Brandon Folkes

Thanks, Mitch. That’s very helpful and best of luck and congrats.

Mitchell Steiner

Great. Thank you.

Operator

The next question comes from Leland Gershell from Oppenheimer. Please go ahead.

Leland Gershell

Hi. Good morning, Mitch. Thanks for taking my questions. It must be very busy days here at Veru. Few questions from me. First, just again with respect to FDA activities heading into the EUA decision, you’d mentioned there had been an inspection of one of the manufacturing facilities. If you could just remind us how many others there may be and if there have been inspections scheduled for those and how critical those would be for the EUA because you already have one that’s been inspected, and I’ve got a couple more? Thanks.

Mitchell Steiner

Sure. So to answer your question, we have essentially — it’s really three buckets. So we have the API, which is manufactured by Olon Ricerca and they have a facility in Italy and in the U.S. Olon Ricerca has clearly been audited by the FDA on numerous occasions and this is the same API group that made — makes Molnupiravir for Merck. And so usually FDA doesn’t go back to a site that’s been recently inspected. They’re happy. And so this site, we do not believe, will be further inspected by FDA.

The second facility is CoreRx, which is the group that puts together the drug product (ph) and puts into capsules. That group was out of Clearwater, Florida and they have eight commercial products including our product ENTADFI, and so we know they’ve been recently audited and inspected, I should say, and they did great. And so we’re not expecting another audit — another inspection because they just been recently inspected. So we’re not expecting FDA to go to that group.

We have a packaging manufacturing facility called Athena in the U.S. and they have not been inspected by the FDA recently. And so the FDA chose that site to do a preapproval inspection. And as I mentioned in my comments, that went well. And so from a manufacturing standpoint, I think, it was set.

Leland Gershell

Okay, Great. And then with options for the most severe patients in the hospital at high risk with COVID-19 remaining limited, and given the compelling Phase III data, I want to ask as you have discussions with both private and public entities out there that would be interested in getting hold of [indiscernible] deal and can you comment on any interest in securing certain amounts upfront? could we see any ATAs event (ph) purchase agreements or any other such agreements to secure supplies of Sabizabulin and perhaps materializing for the EUA?

Mitchell Steiner

Yeah. So to answer the question, just so we’re clear, in the U.S. hospital-based COVID-19 products are handled differently than non-hospital based COVID-19 products or vaccines. So vaccines and drugs like PAXLOVID and Molnupiravir because it’s Part D, D as an dog, Medicare they’re handled by government purchases that are then, distributed by government, okay.

In the hospital setting, it’s much, much more efficient to work through the hospital system. So when you look at all of the hospital based EUA drugs, they’re managed by a DRG, a DRG payment to that, what they call an NCTAP, which is basically a new technology, COVID technology added payments to Medicare, and they have all other kinds of sweeteners to help hospitals deal with the complicated DRGs, complicated patients, COVID-19 patients, that obviously the DRG alone is not going to cover it. So they have additional sweeteners.

It seems to work. I mean, if you look at the Remdesivir, which is under the system last year, they brought in almost $4.56 billion in the system. And so I could see why mess with the distribution system. By the way, that’s part A as an alphabet. So that means the hospitals and there’s an important point that means that the hospitals have to seek reimbursement, not the company. So the company provides product to the wholesaler. When we do that, we book the sale, the wholesaler sells it into the hospital. the hospital gets their reimbursement for the DRG, not for the drug itself. And so once it leaves our hands and we can book it. So it’s very interesting system.

Ex U.S. however, there is — I mean, in the ex U.S. there is definitely an advanced purchase agreement system where government, whether it’s hospital base and whether it’s out of the hospital, non-hospital base, they buy. And so as I said in my comments, we have been contacted and we have been in active discussions literally across the world with groups that are getting ready to understand the drug, to understand how much they want to purchase. And so we’re working through that, like I said, across the world.

What’s also interesting about that is starting to give us an indication a little bit about demand so that we can make sure that we’ve made enough for the world. We will have to allocate as we get into the next year, we will catch up. But one of the things that’s sort of an interesting wrinkle is that Europe, which has this expanded article 18, was a little bit of a surprise to us because we didn’t really know what the hell article 18 was. And article 18 turns out to be a very, very important article because in January 2022, the EMA recognized they needed something similar to an EUA.

And consequently, they allow the emergency task force to come up with a preliminary opinion that would allow and provide cover for the 31 member states of the EU to basically order directly from Veru. And that would mean a separate contract with each country that’s interested in buying the product, which as you know is a different strategy than if you were going to launch commercially in Europe, you typically pick certain countries to launch and that kind of stuff. So this is really different. And so that has been triggered and we’re in active discussions with the Emergency Task Force in EU. Same thing with MHRA.

And then we’re also been in discussions with other groups that have set up either expedited or provisional type processes. So it does feel different. I mean, this is — the world’s preparing for the emerging. They’re starting to see the summer surge. They’re concerned about the winter and the fall and the winter are coming up. Of example, in Korea, which is public information. Korea has said publicly in their newspapers, they were reviewing Sabizabulin. And Korea is a tenth largest economy. Korea is approaching the small country of 50 million people, who are starting to see about 100 –100,000 new cases of COVID-19 a day. Their hospitalization rates are going up and their death rates are going up and they’re very worried.

And when we speak to them, they’re always wearing masks. So they have — they kept their masks on. And so we are expecting — I think it’s fair to say, we are expecting APAs from multiple locations around the world, territories and countries. However, I think it’s clear to say that many of these APAs are going to be triggered by either the EUA authorization in the U.S., EMA authorization, Emergency Use Authorization and MHRA authorization. So they’re looking for cover in one of those three agencies.

So I think that’s clear. We have one offs with certain agencies that do their own work. I’m just getting the impression now having gone through this that they really look to the FDA and they look to EMA and they look to MHRA that used to be part of the EMA for guidance. And by any one of those three, it will open up to the 80% of the countries that are out there that are interested in getting the drug.

Leland Gershell

Great. With that Phase II having been in, up and running for some time probably may see data from that trial around this time. Just wondering if you could just share any thoughts or expectations as to when we may see data from that, that’s for the VERU-100? Thanks.

Mitchell Steiner

Yes. So VERU-100 continues to go well. The challenge there is, it turns out the reason nobody else has figured it out because it’s very complicated biologically. You have to — it turns out for GnRH antagonist that you give as a depo. You have to have a certain level to cause the castration and you have to have another blood level that maintains that castration. And the different and we’re asking a single injection to do both. And I’m happy to report we can do that. So now we’re just optimizing the dose and I feel very confident that this is going to be a very interesting product for prostate cancer because we know the agonists have their issues. And so we can have an antagonist that can go beyond one month.

And we have patients clearly beyond one month, approaching — we have some approach three months. So that’s why I said that my comments its promising, but we’re optimizing so that this way when we go to the 100 patients in the Phase III, every one of those patients will castrate immediately and maintain their castration for three months. So sit tight, I’ll be able to provide more clarity. I hope over the next few weeks.

Leland Gershell

Okay. Thanks for taking the questions.

Mitchell Steiner

Thank you.

Operator

The next question comes from Chris Howerton from Jefferies. Please go ahead.

Chris Howerton

Great. Thanks so much for taking the questions. I guess, two from me. One would be with respect to the kind of distribution and government assistance with respect to COVID-19 in the United States. I guess how should we be thinking about the status of the public health emergency? And what are some of the influences that we can expect in terms of the categorization of those things and the viability of path forward for the EUA and those reimbursement parameters that you discussed earlier, Mitch?

And then the second question that I have would be related to your capital strategy. Obviously, the female condom business has been excellent and certainly cash producing a little bit of a slowdown that we detect this quarter. So just wondering if you have any updates in terms of prioritization in terms of cash deployment given that observation?

Mitchell Steiner

Yes. All right. So let me answer the first question. So the first question is basically that’s great, you’ve got the sweeteners in, and the hospital setting it works for Remdesivir and other hospital based products. Essentially, what you have is a DRG that has an outlier payment, has 20% sweetener for COVID. And then on top of that, you have this NCTAP, which is a COVID added payment that is also provides more resources so that hospitals can get close to 75% plus covered and that’s wonderful. I’m glad we have that, but the question — and it works. And the question is what happens when the emergency goes away?

So first of all, the first fact is that these programs will stay in place until the end of that calendar year. So we’re going into this fall and the winter and we’re commercializing the product. The programs will stay in place until the end of that calendar year. If it turns out that the emergency gears are then pushed into the next year and we’ve been in this for 2.5 years and it just doesn’t feel like it’s going away and the death rate is pretty close to its been year one, year two. So it feels like it’ll continue, then that will mean if it goes into January of next year, then they’ll be required to pay until the end of January of 2023.

The reason they do that is there are other programs that you can transition into like instead of NCTAP, this is called NTAP. So NTAP has been in place and again its new technology added payment. And NTAP will only work if you have a full approval. So we will be doing full approval through an NDA. So obviously, we will be doing it after the EUA, is having a meeting with FDA for a pre-NDA meeting, and the pre-NDA meeting will allow us to find out what are some of the additional information we need for labeling, et cetera., that will allow us to go from an Emergency Use Authorization to a full approval and the full approval will then allow us to trigger the NTAP in some of those payments. So there is a strategy to allow us to continue to see robust reimbursement.

As it relates to the capital strategy, yes, we saw a slowdown in FC2. It reminded us why it’s important for us not to be reliant on customers and that’s why we created our own direct-to-consumer portal. I think it was a timely move on our part because it takes time, and it’s in and it’s working. It feels good because we’re seeing revenue coming in from that portal and it allows us to be in control of our own destiny as it relates to getting capital. And so in addition to full expectation based on our communications with our customers that the whole telemedicine group across the board got hit as people have transitioned from staying at home to going back out and going back home probably at some point. But it’s being — it’s turning around and we’re expecting fourth quarter to be better and next year to be even better.

With that said, anything had happened, but that’s the signals that we’re seeing and our own portal allows us to have control. And ENTADFI is completely new revenue. And as I’ve said in my comments, we are in discussions with a large telemedicine group that can help us with that and plus, we’re moving very, very actively to GoodRx and market access. And this is an easy one to sell. If you talk to urologists about ENTADFI, which is a combination of erectile dysfunction medicine, in a medicine that shrinks the prostate. But it shrinks prostate faster and more effectively than finasteride alone. They get it and I think this will be again another source of revenue.

With that said, the reason we still have $100 million in the bank and we raised that money almost 18 months, 20 months ago, is because we’ve been able to match our spend with the money we bring in. And so we know the levers to pull. And so we would do the same thing So we’re not waiting for revenue to catch up. We’re going to — we’re managing our business so that we can be efficient in clinical trial recruitment and getting to commercialization. But again, as you mentioned, we have to prioritize.

So at this point now, we’re focused highly on Enobosarm in a second-line setting, and a third-line setting. We have the VERACITY study going, it’s Phase III recruiting. And VERU-100 is one of those that is just such an established market that once we can get there that can be a nice cash count. And in the meantime, if the emergency use authorization is granted and we get resources when we drop ship product to the distributor. And we’re not worrying about reimbursement because that’s not what we do.

It’s not like Part D where you wait for the prescription to be filled. In this situation, once it goes into the wholesaler, we can get the money, then there is a real opportunity to see significant revenue within two weeks or so from the time we get to the EUA, which means that we’ll have the capital that can continue the new Phase III studies for COVID-19 and to maintain our business and to become profitable.

So we still have the fundamental company in place. We have a core oncology business that’s doing great. We have the resources to match the spend and even with the extra spend, as you heard from Michele, getting ready with the COVID-19 infectious disease franchise. We’ve done very well to have those resources ready to go and we didn’t have to do a raise in dilute. So I think we’ve done a good job managing our finances.

Chris Howerton

I would agree. Thank you so much, Mitch for the — taking the questions and congratulations.

Mitchell Steiner

Thank you.

Operator

[Operator Instructions] Our next question comes from Yi Chen from H. C. Wainwright. Please go ahead.

Yi Chen

Thank you for taking my question. Just to clarify, has the UK MHRA already started reviewing package for Sabizabulin?

Mitchell Steiner

To clarify, when we do first, the way the process works, is you have to meet with their COVID-19 task force. So we have to submit the materials to begin that process. And so when we met with them, as we said in the press release, they were so excited about the medicine that the entire task force basically said, you submit because there’s a process in MHRA, you submit and we’re going to support it for expedited review and they’re the only ones do that. And however, you have to submit.

And so what we were waiting for before we submit to the U.K. is the entire data set for all 204 patients, which we’ve now received. And so as we speak now, the application is being prepared for submission and then they can start the clock. Once they start the clock, and again, the clock is unclear at this point, but once we have more clarity, I’ll be able to share that with you, but that’s in place.

Yi Chen

So the UK MHRA’s review process and EMA’s review process are completely independent from FDA’s EUA review process, correct? They will now wait for FDA’s decision to affect their own decision, right?

Mitchell Steiner

Yeah. So if you look at the Emergency Use Authorizations for Molnupiravir, it turned out that MHRA approved — had the emergency use authorization done before U.S. So they are very independent. And so just to be very clear, MHRA is independent. EMA, independent. FDA is independent. And if any one of those three organizations authorize Sabizabulin and about 80% of the countries in the world will take that as a trigger to authorize in their country.

Yi Chen

Got it. Thank you.

Operator

Ladies and gentlemen, this concludes our question-and-answer session. I’d like to turn the conference call back over to Dr. Mitchell Steiner for any closing remarks.

Mitchell Steiner

Thank you. I appreciate you joining us on today’s call. I look forward to updating you all on our progress in our next investors call. Thank you.

Operator

The digital replay of the conference call will be available beginning approximately noon Eastern Time today, August 11, by dialing 1-877-344-7529 in the U.S. and 1-412-317-0088 internationally. You’ll be prompted to enter the replay access code, which will be 1902173. Please record your name and company when joining. The conference call is now concluded. Thank you for attending today’s discussion.