Anavex Ny tråd juli 2024

deleted-user

Anavex Den nye analytiker rapport - kursmål 40,89 $!
( For de der ikke har FB )

Independent Investment Research - AUS
Virker som et seriøst analysefirma .

En rigtig fin og grundig gennemgang af casen.
Fint med nogle friske øjne, der måske kan holde Missling lidt mere til ilden, med kritiske spørgsmål med krav om svar, hvis de forsætte skal kunne dække selskabet.
Anavex burde tage imod denne ekstra mulige eksponering med kyshånd - det var jo netop det Missling udtrykte ved generalforsamling, at man gerne ville udbrede kendskabet til Anavex.
Tænker at allerede har været i direkte dialog med Anavex ved udformningen af analysen.

Flere positive udsagn i analysen:
"strong case for approval"

https://cdn.fbsbx.com/v/t59.2708-21/453669608_1075638987417664_6428007278213907997_n.pdf/AVXL-research-report.pdf?_nc_cat=106&ccb=1-7&_nc_sid=2b0e22&_nc_ohc=UEulsvPqJyQQ7kNvgEBnMdm&_nc_ht=cdn.fbsbx.com&oh=03_Q7cD1QHdTteiU0nc9KfNukpA6OX2ooXPmjlYWsfmzcq-dE2g4g&oe=66AC5F8E&dl=1

Kyed01

Jeg er ret sikker på at Anavex har betalt for den research rapport.

Man kan læse det med småt i begyndelsen og i slutningen af rapporten.

Intet overhovedet er negativt.

De kan selvfølgelig heller ikke skrive løgne historier og rapporten ser troværdig ud.

Side 30:
Corporate Research
Independent Investment Research has or may have, received a fee either
directly by a company itself or by a third party, to provide coverage
and/or corporate research (the "Fee"). Where a Fee has been received,
Independent Investment Research does not publish:
Buy / Hold / Sell recommendations for the security or managed
investment schemes.

deleted-user

Anavex 3. kvartalsrapport den 6. Aug kl. 14.30 DK-tid.

The live webcast of the conference call will be available on Anavex's website at www.anavex.com.

Anavex Life Sciences to Announce Fiscal 2024 Third Quarter Financial Results on Tuesday, August 6, 2024

Webcast and Conference Call To be Held Tuesday, August 6, 2024, 8:30 am ETNEW YORK, Aug. 01, 2024 (GLOBE NEWSWIRE) -- Anavex Life Sciences Corp. (“Anavex” or the “Company”) (Nasdaq: AVXL), a clinical-stage biopharmaceutical company developing differentiated therapeutics for the treatment of Alzheimer's disease, Parkinson's disease, schizophrenia, neurodevelopmental, neurodegenerative, and rare diseases, including Rett syndrome and other central nervous system (CNS) diseases, today announced that

Yahoo Finance (finance.yahoo.com)

Man skal nok ikke forvente større nyheder, men forhåbentlig lidt mere omkring div. tidshorisonter.
Gerne lidt skarpe spørgsmål fra analytikerne, inkl. nye IIR fra Australien.
Interessant med en australsk baseret analytiker, når Anavex jo har afholdt store dele af div. forsøg netop i Australien.

Vil nok først og fremmest forsøge at afkode, om ledelsen/Missling udtrykker ægte tilfredshed med de sidste resultater fra AD og troen på en endelig godkendelse.
Dette burde jo forhåbentlig være sidste Q-rapport før indsendelsen til EMA.

ProinvestorNEWS

Ugekommentaren med Anavex:

deleted-user

Anavex Lidt mere positiv omtale i "Alzheimer`s News Today"

Blarcamesine sustains benefits in early Alzheimer’s over year: Data

Experimental blarcamesine (Anavex 2-73) was able to slow cognitive and functional decline in early Alzheimer’s patients over a year, data show.

Alzheimer's News Today (alzheimersnewstoday.com)

Lige en lille kommentar til Helges ellers udmærkede ugekommentar vedr. Anavex.
Her omtales Anavex`s AD forsøg, som et fase 2 forsøg, men det er faktiske et fase 2b/3 forsøg - dvs. har en størrelse og struktur/protokol, som fuldstændig svarer til et fase 3 forsøg.
Årsagen til benævnelsen fase 2b/3, mener jeg ligger oprindelige i at de 30 mg skulle udgøre fase 2b delen og 50 mg skulle udgøre fase 3 delen.

Det er også vigtigt at understrege, at det iflg. Anavex var EMA i november 2023, der efter at have set store dele af de data vi fik præsenterede den 28. Juli på AAIC, opfordrede Anavex til at ansøge om fuld markedsgodkendelse i hele EU.
EMA må således have accepteret forsøget som værende af en størrelse og kvalitet, svarende til et normalt fase 3 forsøg.
Anavex bekræftede igen, at ansøgningen indsendes i 2024.
Følges den normale proces fra EMA, bliver der allerede ca. 1 mdr. før den endelige indsendelse taget stilling til, om ansøgningen ønskes behandlet efter den acc. proces - dvs. 150 dage, mod standarden på 210 dage.
Dvs. Indsendes ansøgningen i nov. 2024, burde vi allerede i okt. få oplyst om det er den hurtige proces man ønsker. Dette sker ved en dialog mellem Anavex, CHMP rapportørene og EMA.
Sammenholdt med de gode præsenterede data, samt bivirkningsprofil og EMA´s tilskyndelse, vil jeg mene, at det mest oplagte ville være den hurtigst mulige proces!

Men ja - biotek er ikke for sarte sjæle - værdien af casen og kursudviklingen er ofte ikke sammenhængende.
Den reelle værdi af et biotekselskabet bliver også første reelt opgjort, når man først får en indtjening fra et godkendt produkt eller ved et opkøb af selskabet - indtil da er det stort set "fugle på taget", hvilket som Helge understreger også bør afspejles i investeringsprofilen!

Mine antal af "fugle på taget" er dog i Anavex`s tilfælde lige til den gode side.

Vedr. IIR - den nye analytiker, så er det tydligt, at Anavex har været med inde over - dette betyder dog især, at tingene som beskrevet skal være faktuelle.
IIR skal kunne stå inde for div. udsagn, hvis deres gennemgang af casen skal danne beslutningsgrundlag fra potentielle investorer, som bruger IIR, ellers ville selskabet nok ikke blive anset som seriøst fremadrettet.

Helge_LarsenPI-redaktør

Tak Tasso, Jeg er godt klar over at studiet er et fase 2b/3 studie, men fik ikke præciseret dette.

Lægemidler til sygdomme, hvor der ikke er effektive behandlinger tildeles ofte fast track/acc. proces og evt. godkendelse på baggrund af gode data i et fase 2b studie.

Helge_LarsenPI-redaktør

Anavex er ikke blandt "Key highlights" fra AAIC

"Alzheimer's advancements unveiled at AAIC

FirstWord's daily coverage of the Alzheimer's Association International Conference (AAIC) revealed the latest developments on the neurodegenerative disease. Key highlights included:

GLP-1 receptor agonists took their familiar place in the spotlight, with Novo Nordisk's liraglutide showing significant benefits in reducing cognitive decline and slowing brain volume loss. The findings offer positive readthrough for Novo's late-stage semaglutide studies in Alzheimer's disease, and add to preclinical findings showing that GLP-1s and other incretin mimetics lower brain insulin resistance, and that dual and triple agonists hold even greater promise

Unwilling to let Eli Lilly steal its hard-earned improved uptake for Leqembi (lecanemab-irmb), Eisai scientists presented data showing that long-term treatment with its Biogen-partnered anti-amyloid therapy provided better outcomes and relapse prevention than the finite dosing offered by Lilly's recently FDA-approved Kisunla (donanemab-azbt)

Among novel approaches touted at the meeting, two stood out most. Vigil Neuroscience's small-molecule TREM2 agonist VG-3927 - in an early-stage study and having garnered a $40-million investment from Sanofi in return for an exclusive option - seeks to boost amyloid clearance by activating the receptor. AC Immune's vaccine candidate, ACI-24.060 - on which a multibillion-dollar option agreement is focused - showed in vivo promise, demonstrating sustained antibody response against beta amyloid with efficacy comparable to that of Leqembi.

Leqembi comeback: Promising data and sales surge help offset EU setback

Though last week ended on a low note for Eisai and Biogen, with an EU regulatory panel recommending against Leqembi’s approval, the anti-amyloid monoclonal antibody for Alzheimer’s disease seems to be on an upward trajectory since then. Its aforementioned positive data from the open-label extension of the pivotal Clarity AD trial presented at AAIC may give it a leg up over Kisunla, and Biogen revealed in its consensus-beating second-quarter report that Leqembi also exceeded expectations and is gaining momentum after a lagging launch. The therapy rang up $40 million in global sales for the period, for its second consecutive quarter of growth.

Just a moment...

(firstwordpharma.com)

deleted-user

Anavex 100 % sammenfald med de 4 hovedsponsorer af AAIC!

Dette har vel intet med "Key highlights" at gøre???

Sponsorship Opportunities | AAIC | Alzheimer's Association

Elevate your brand and reach dementia industry professionals by sponsoring the Alzheimer's Association International Conference. Learn more now.

Sponsorship Opportunities | AAIC | Alzheimer's Association (aaic.alz.org)

Kyed01

Nej dem der betaler kommer i første række, det gælder isaer i USA, okay dette er i Canada.
2 danske firmaer som sponsorer, Novo Nordisk er en af Platinum sponsorerne.

Novo N kan vel købe Anavex uden at på sved på panden?

Vi vil acceptere 10 billioner$, tak.

Dog med et nuværende MC på ca 550mill$ er det ret usandsynligt ha-ha.

Kan jo også starte som partner?

Milito

Er det ikke amerikansk når det blev afholdt i Philadelphia? Eller får jeg blandet noget sammen.

Selv 2-3 milliarder dollars vil jeg acceptere.

Kyed01

Alzheimer's Association International Conference ' July 27-31, 2025 ' Toronto, Canada

Sponsorship Opportunities | AAIC | Alzheimer's Association

Elevate your brand and reach dementia industry professionals by sponsoring the Alzheimer's Association International Conference. Learn more now.

Sponsorship Opportunities | AAIC | Alzheimer's Association (aaic.alz.org)

Er det ikke den vi snakker om @Milito?

2-3 milliarder er ikke acceptabelt for mig, vil blive meget skuffet.

Milito

Korrekt at konferencen næste år er i Canada, mens netop afholdte AAIC 24 var i Philadelphia.

Kyed01

Ups, jeg er sgu vist ved a blive gammel og kunne bruge en daglig 2-73 pille.

TTTDK

Artikel i Medwatch:
Efter at Eisai præsenterede nye data fra studiet om brugen af lecanemab til patienter med Alzheimers sygdom, er der kommet skeptiske stemmer fra konkurrenter og forskningsmiljøet.
https://medwatch.dk/Medicinal___Biotek/article17325904.ece

Solsen

Lidt fra dagens cc.

Den megen debat omkring discontinuations og dizziness i fase 2b/3 blev belyst.

Anavex "tvang" optittrering af Blarcamesine hurtigt igennem og det har været medvirkende til det relativt store frafald pga dizziness. Pts troede de havde covid e.lign. og sprang derfor fra.

OLE forsøget har lært Anavex, at en langsom optittrering begrænser dizziness forekomsten og aftendosering har også hjulpet.

Anavex/Missling oplyste, at man har benyttet data fra alle pts i analysen. Der har været såettvivl om hvorvidt de har "snydt" med data idet der ikke var sammenfald i antallet af pts i de forskellige endpointmålinger. Men det skyldes, at ikke alle pts møder op til aftalte møder grundet covid etc. Det samme er tilfældet i "mabbernes" data.

Der blev spurgt til om de vil bruge filingen omkring aktieudvidelse til noget. Missling sagde ikke i dag eller i morgen - kryptisk, men ikke nødvendigvis noget negativt. F.eks. vil vil nok ikke være utilfredse med en partneraftale med udstedelse af aktier til partneren.

Jeg blev lidt mere rolig omkring discontinuation raten og bivirkningen dizxiness om end jeg ikke har ligget søvnløs over det.

Det ligner til at det kører efter planen selv om det går langsomt.

OLE bliver rigtig spændende.

deleted-user

Anavex Udskrift 3. kvartalsrapport inkl. Q & A

Ikke meget nyt, men tingene kører som planlagt.

EMA har 100 % første prioritet med AD og indsendes i 2024!
Missling meldte klart ud om dette og at FDA og Asian og andre sundhedsmyndigheder må vente.
Anavex er et lille selskab og alle resurser bruges på EMA!

Meget plausibel forklaring på frafaldet af patienterne især titreringsperioden - Anavex havde jo en stram protokol at overholde.
Når først patienterne efter lidt svimmelhed mm. havde vænnet sig til Blarcamesine - ofte efter ganske få dage, så var der ingen problemer efterfølgende. - forståeligt, at nogle måske troede de havde fået COVID-19 og derfor stoppede.
Lægerne og Anavex så faktisk positivt på denne respons fra patienterne, da det indikerede en effekt i hjernen og den ønskede gennemtrængning af Blarcamesine gennem bold/hjerne-barrieren, som man gerne ville se.
Som Solsen nævner, synes der nu at være fuldstændig styr på dette og vil kunne minimere frafald i andre indikationer fremadrettet også.

Missling nævnte, at der har være god respons og skabt nye kontakter på AAIC - vi må se hvad det måske munder ud i?

Peer Review igen igen bekræftet publiceret i 2024!

RETT stadig på dagsorden, men synes at blive skubbet lidt i baggrunden for Fragile X, hvor de nu mener at have fundet fælles biomarkører, som er relativt nemt at eftervise som funktion af behandling med Blarcamesine. (elektrisk aktivitetsniveau i bestemte dele af hjernen)
Fragile X er ca. 6-7 gange mere udbredt som RETT og derfor også indtjeningsmæssig mere attraktiv.

Parkinson fase 2/3 forventes opstart igen igen i 2024!

Vi må se, men alt indikerer, at processen med AD og EMA kører helt på sporet - ingen røde lamper!

Anavex Life Sciences Corp. (AVXL) Q2 2024 Earnings Call Transcript
Aug. 06, 2024 12:19 PM ETAnavex Life Sciences Corp. (AVXL) Stock
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Anavex Life Sciences Corp. (NASDAQ:AVXL) Q2 2024 Earnings Conference Call August 6, 2024 8:30 AM ET

Company Participants

Clint Tomlinson - Investor Relations
Christopher Missling - President and CEO
Sandra Boenisch - Principal Financial Officer

Conference Call Participants

Tom Bishop - BI Research
Soumit Roy - Jones Research

Clint Tomlinson

Good morning, and welcome to the Anavex Life Sciences Fiscal 2024 Third Quarter Conference Call. My name is Clint Tomlinson, and I will be your host for today's call. At this time, all participants are in a listen-only mode. Later, we will conduct a question-and-answer session. [Operator Instructions]. Please note this conference is being recorded, and the call will be available for replay on Anavex's website at www.anavex.com.

With us today is Dr. Christopher Missling, President and Chief Executive Officer; and Sandra Boenisch, Principal Financial Officer.

Before we begin, please note that during this conference call, the company will make some projections and forward-looking statements. These statements are only predictions based on current information and expectations, and involve a number of risks and uncertainties. We encourage you to review the company's filings with the SEC. This includes without limitation, the company's forms 10-K and 10-Q, which identify the specific factors that may cause actual results or events to differ materially from those described in these forward-looking statements.

These factors may include, without limitation, risks inherent in the development and/or commercialization of potential products, uncertainty in the results of clinical trials or regulatory approvals, need and ability to obtain future capital, and maintenance of intellectual property rights.

And with that, I'd like to turn the call over to Dr. Missling.

Christopher Missling

Thank you, Clint, and good morning, everyone. Thank you for being with us today to review our most recently reported financial results and to provide our quarterly business update. We continue to meaningfully advance our differentiated precision medicine clinical program, highlighted by the recent presentation of comprehensive results from the Phase 2b/3 clinical trial, blarcamesine, ANAVEX2-73, which represented at the Alzheimer's Association International Conference AAIC, showing that oral, once daily blarcamesine significantly slowed clinical decline for early Alzheimer's disease, patients with good comparative safety profile and/or associated neuroimaging adverse events.

Full data from the blarcamesine study in Alzheimer's disease Phase 2b/3 placebo controlled clinical trial will be published in an upcoming peer-reviewed journal. The initiated process for submitting a Marketing Authorization application, MAA, to the European Medicine Agency, EMA, under the Centralized Procedure is underway with full regulatory submission of blarcamesine expected in Q4 of 2024.

The Marketing Authorization would allow direct market access throughout the European Union for oral blarcamesine for the treatment of Alzheimer's disease. There are an estimated 7 million people in Europe with Alzheimer's disease, a number expected to double by 2030, according to the European Brain Council.

Analysis of RNA sequencing RNA-seq, which would reveal which genes are actively transcribed or in other words expressed in Alzheimer's patients in comparison between placebo and blarcamesine of the placebo-controlled Phase 2b/3 blarcamesine trial in early Alzheimer's disease in underway. This data might have relevant value, since it may provide insight into Alzheimer's disease pathology and how cells function in the presence of placebo or in presence of blarcamesine, respectively. Interim data is expected in the second half of 2024.

In June we completed the last patient last visit in the ATTENTION-AD open-label extension 96-week trial. Interim data from this trial is expected in the second half of 2024. The reason AAIC 24 meeting resulted in constructive feedback coupled with enthusiasm around our Alzheimer's disease program strengthened by the recent addition of an experienced clinical team, which support Anavex future plans. Educational outreach to continue as work towards MAA submission and beyond.

We are also pleased to report that the clinical team continues to beat the planned timelines in the ongoing Phase 2 clinical trial of ANAVEX3-71 in schizophrenia patients. We have completed dosing of the first cohort and are nearing the completion of enrollment of the second cohort of schizophrenia patients in Part A of the trial.

In Parkinson disease, initiation of ANAVEX2-73 Phase 2b/3, an over six months trial, including biomarkers, which we believe may be key for understanding drug effect on Parkinson disease pathology and account for the recently changing context in the field of Alzheimer's disease of Parkinson disease is expected in the second half of 2024.

In Rett Syndrome, an educational presentation was provided at the 2024 IRSF Rett Syndrome Scientific Meeting, going from June 18 to June 19, 2024, which demonstrated the commitment of Anavex to the Rett syndrome community through direct engagement with patients and families. Positive and supportive feedback was received from families and investigators about the continued Anavex Rett syndrome program.

Regarding Fragile X, new disease-specific translatable, and objective biomarker data generated with ANAVEX2-73, supporting the initiation of the ANAVEX2-73 Phase 2/3 clinical trial was presented at the 19th NFXF International Fragile X Conference. Meeting with the NFXF leadership team strengthened Anavex relationship with community coupled with increased awareness of Anavex Fragile X syndrome program by engaging with patients and families in attendance.

We are also expecting the initiation of Anavex Phase 2/3 clinical trial in a new rare disease in the future. Finally, we are building medical affairs capabilities to expand education and physician support activities to ensure optimal medical impact, including continued clinical publications involving ANAVEX2-73 and ANAVEX3-71.

And now I would like to direct the call to Sandra Boenisch, Principal Financial Officer of Anavex, for a financial summary of the recently reported quarter.

Sandra Boenisch

Thank you, Christopher, and good morning to everyone. I'm pleased to share with you today our third quarter financial results for our 2024 fiscal year. Our cash position at June 30th was $138.8 million and we have no debt. During the quarter, we utilized cash and cash equivalents of $5.2 million in operating activities after taking into account changes in non-cash working capital accounts.

At our current cash utilization rate, we believe we have a cash runway of approximately four years. During our most recent quarter, general and administrative expenses were $2.9 million as compared to $2.8 million for the immediately preceding second quarter. Our research and development expenses for the quarter were $11.9 million as compared to $9.7 million for the immediately preceding second quarter.

And lastly, we reported a net loss of $12.2 million for the quarter, which is $0.14 per share.

Thank you. And now back to you, Christopher.

Christopher Missling

Thank you, Sandra. In summary, we remain dedicated to developing medicines for individuals suffering from brain disorders within neurodegenerative and neurodevelopmental disorders, which could further expand our differentiated precision medicine platform to deliver scalable treatments coupled with convenient oral dosing.

I would now like to turn the call back to Clint for Q&A.

Question-and-Answer Session

A - Clint Tomlinson

Thank you, Christopher. We'll now begin the Q&A session. [Operator Instructions]. And the first question comes from Tom Bishop, BI Research. Tom, you should be...

Tom Bishop

Hey. Can you hear me now?

Clint Tomlinson

Yep. Great. Thanks, Tom.

Tom Bishop

Okay. I had a couple of questions. What are your plans to meet with the FDA or regulators in Asia, which you also alluded to recently, as you did earlier with EMA and has a date been set for either or is there some sort of hold up or additional data you're waiting for?

Christopher Missling

Thank you for the question. There's no hold up. There's only the focus right now on the email submission, which takes a lot of resources. We have to submit and put together a package of many modules, which is -- can be so many pages and documents. So we focus on that. But the time will come, we don't know yet when to also meet regulatory bodies around the world, including the agency in this country as well.

Tom Bishop

Okay. With regards to the recent presentation at the AAIC of the Phase 2b/3 data, the question comes up with regard to varying number of patients included in different measures that the company presented. And I have assumed that you -- it's just simply due to the fact that you can't force patients in the trial to come in and take certain tests, especially more invasive ones, and that this explains it. But, of course, the dark side likes to claim cherry picking. So can you discuss this aspect and put the issue to rest as to whether you do anything with the data that's given?

Christopher Missling

May I understand better to talk about the number of patients, in each visit, schedule visits?

Tom Bishop

In the different things like Cog13 and whatever that you presented in to the AAIC. So the number of patients, some of these.

Christopher Missling

So it is a time point? Yes, so this is a -- there is no other way to explain it that every patient does not always present at the time point in question. He can skip. He can be impaired because of COVID and this trial was during COVID. It's very normal. You just have to then always account for when you have a data point, and that's exactly described in the presentation. And when you look up other papers from [indiscernible] from Lecanemab, Donanemab, they are exactly the same. Every number is different at every time point because they are not always the same amount of patients attending the visit. So that's a very common procedure.

Tom Bishop

But you use the data exactly as given to you by the biostatistical firm? And who was that?

Christopher Missling

Yes, of course. There is no other way than to take every available data point. There is no other way to do that other than that.

Tom Bishop

Okay. And I wanted to clear up or confirm for myself this the so called, the $150 million stock offering that the various news headlined, that was just a shelf offering to be used as needed opportunistically in the future. Correct?

Christopher Missling

So the company has been extremely cautious with, financing. We've been very conservative. While other companies spent ton of money, we've been very diligent on being very cautious with our fiscal responsible behavior. So what we did was just to make sure that one day in the future, when we do need more resources for market entry or other reasons that we have that in place. So it's not meant to be used today or tomorrow, but the opportunity could arise. But it was just to put in place something, so we have it in place for the future.

Tom Bishop

Okay. And regarding Rett, is there a date to initiate another Rett trial? Or well, I'm not sure what was going on there?

Christopher Missling

So we have had very good feedback from the conference I mentioned, and there's no date yet. But we proceed as we stated to do a larger study, for Rett Syndrome as well.

Tom Bishop

Okay. And finally, with regards to Fragile X, was there a Phase 1? You mentioned going to a Phase 2b/3, I think and...

Christopher Missling

And Phase 1 was done with Blarcamesine with ANAVEX2-73 already, so we can start into a Phase 2 because of the Phase 1 was already done prior to this because of the drug was already tested in human healthy volunteers.

Tom Bishop

Okay. And, actually, I had one more. With regards to Schizophrenia, can you remind us a little more or explain the first cohort, the second cohort, Part A, is there a Part B? I mean, could you just run through that again?

Christopher Missling

Sure. So Part A is a signal ascending doses. So we test the tolerability of the patients for the first doses, lower dose and a higher dose subsequently and the second higher dose is now almost completed enrollment. And the Part B will be a longitudinal study run about, I think it's 28 days or so. So the drug will be given at the dose which will be considered the best tolerated dose, and we will then observe patients over a longer period of time.

Tom Bishop

So the second dose is the higher dose?

Christopher Missling

The second dose from Part A is the higher dose, and Part B will be the dose which we choose. Once it starts, and it would be a longer trial of 28 days or four weeks, basically.

Tom Bishop

All right. Thank you.

Christopher Missling

Thank you.

Clint Tomlinson

Thank you, Tom. Our next question comes from Soumit Roy at Jones Research.

Soumit Roy

Good morning everyone and thank you for taking the question. And also congrats on executing on multiple fronts. On the AAIC data, Alzheimer disease, could you give us a little color, make us understand on the dose dependency or a clear lack of dose dependency between 30 milligrams and 50 milligram? There was ADAS Cog was working a little better for the 50 milligram versus CDR-SB for the 30 milligram. And the discontinuation rate are, so what percent of the 50 milligram did you see had to scale back to 30 milligram because of adverse events in the open label extension?

Christopher Missling

So let me address the first question first. So the two arms are those groups, and we use the expression for that reason. When you read our description in the presentation, we talk about the dose groups, 30 milligram dose group or 50 milligram group. So since we allow titration to the best tolerated dose for those two arms as well as placebo, by the way, we basically realized that the end of the day, the target dose for most patients was relatively close to each other in those two arms. So while in the 50 milligram group, there were some with 50 milligram, there were also some with 30.

So it was a bit higher than the 30 milligram group, but not by much. So they're pretty much close, and that's why I also prespecified the two arms together against placebo in a predefined analysis. So that was the background. So we have seen prior to that a dose response curve in our Phase 2A. So there's no doubt about the dose response is confirmed. But what we now notice is that in this trial where we and that's coming to the second part of the question, where we noticed where we force patients to uptake trait to the target dose 50 very quickly within two weeks and then to three weeks, we noticed that didn't -- was very well received.

Some patients had some dizziness, and they wouldn't feel comfortable about it. So because they're not impaired patients, they're early Alzheimer, they felt saying maybe we have COVID. I don't want to continue this. It was during the time of COVID, of course, as well. So that's why we had some dropouts at the higher dose more than in the lower dose group.

So what we now realized when we did the open label study where we allowed a more, I would say, lenient and less stringent way of up titration in also allowing patients to take the drug at night time instead of in the morning, which we basically force patients to take during the trial early in the morning. So we noticed that there was much higher tolerance for either dose 30 or 50 as long as they were allowed to get used the drug for a longer period of time.

And we noticed that also in the Compassionate Use program with this extremely higher tolerance with allowing patients to titrate to 50 or 30 as long as they have enough time to do that and then taking also night time dosing. So we don't see the adverse events, we have seen in this trial because we basically forced them to titrate so quickly up to the target dose. And we also have to point out that it's actually a clearly manifestation of a manageable and addressable adverse event. It's not like, when you look at brain bleeding or brain swelling from the antibodies, which we don't have, that no matter how you take the drug, you always will have 30 or more percentage of patients with that very dangerous side effects of a drug of an antibody, which we don't have.

But in our case, the adverse event of dizziness is a manageable one because it just depended on the titration schedule, and that can be flexible, changed. And that's what we now will, of course, do in the future. So that's the answer to your question. And also, needless to say that we are also acknowledging that, and we've heard that from physicians that the dizziness sign again, not all patients had that. We also have to put this in perspective, that it's a sign that shows penetration in the brain and shows that some thing's happening in the brain.

Also, one last point I'd like to make that this dizziness lasted really relatively short for those patient who had it was sometimes between seven to 11 days in the average. So it's a very -- and a mild form of dizziness. So it's a very easy to address situation, but it shows up in this trial because again, we forced patients to go to these high doses very quickly, and we learned the lesson that we can avoid that.

Soumit Roy

That is really helpful color. So last question is, when should we expect the open label 96 week data? Is it CTAD or more towards the end of the year? And should we expect after that data, you would approach the FDA with the entire packet submitted to European Authority plus this open level? Or if you can provide any details there?

Christopher Missling

Yes, so let us first put together, data together. But once we have it, we will make the decision. But all your suggestions could be a valid recommendations.

Soumit Roy

Thank you, and congratulations again on the progress.

Christopher Missling

Thank you. Appreciate it.

Clint Tomlinson

That's all the questions for now, Dr. Missling.

Christopher Missling

Thank you. So in closing, we continue to focus on execution and commercial readiness as we advance our therapeutic pipeline to potentially improve patients' lives living with these devastating conditions. Thank you very much.

Clint Tomlinson

Thank you, ladies and gentlemen. This concludes today's conference call. We appreciate your participation, and you can now disconnect.

TTTDK

Ikke meget nyt, men deres AD case er bekræftet med deres AAIC præsentation, hvor hullerne ift. forskel i antal af patienter nu også er forklaret.
Det kunne havde været rar at sp blev fordoblet lige efter AAIC lol.
Men... EMA submission rykker tættere og tættere på. Intet er ændret i min stambeholdning af Anavex.

TDT123

Oven på regnskabet, er det kommer en købsanbefaling med et target på 15$ AI artikel, med efterfølgende gennemgang af JT...

deleted-user

Anavex HC Wainwright bibeholder kursmål 40 $ i dag.

Just a moment...

(www.tipranks.com)

HC Wainwright forventer en EMA godkendelse (2025 ?) og efterfølgende markedsføring i 2026.
Ved en godkendelse i hele EU og salg til potentielle 7 mill. AD patienter - uden reel konkurrence, så virker kursmål 40 $ meget lavt sat, hvis de er af den overbevisning.
Vi skal selvfølgelig passerer de 40 $ på vej op i løbet af 2025, hvis HC Wainwright mener at Blarcamesine kommer på markedet i 2026 - tror dog, at Blarcamesine kommer på markedet i slutningen af 2025.

deleted-user

Anavex Lidt mere omtale i Neurology Live.

Attention Required! | Cloudflare

(www.neurologylive.com)

Ikke noget nyt, men det skader ikke at udbrede de rigtig gode resultater - det almene kendskab til Anavex og Blarcamesine er stadig minimal.
Hvis Biogen eller en af de andre BPer havde haft disse resultater, ville de have været på landsdækkende tv og fået stor omtale på div. medier. Anavexs tid skal nok komme, når først EMA modtager og efterfølgende accepterer ansøgningen for AD i EU og højst sandsynlig godkender Blarcamesine i sidste ende!

Ideen med Novo Nordisk (forslået længere oppe i tråden), som en evt. kommende partner/ejer virker på mange måder tiltalende. Blarcamesine på dygtige danske hænder.
For mit vedkommende ville det på en måde også slutte ringen for mig, da Novo Nordisk var det allerførste biotekselskab, jeg investerede i for nu en hel del år siden.