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Explanatory Note:
The following is a transcript of an analyst/investor conference call held by the senior
managements of Intercell AG and Iomai Corporation
on May 13, 2008 at 8:30 a.m. CET
Chaired by Mr Gerd Zettlmeissl, CEO of Intercel
(for which replay will be made available at www.intercell.com;
references in the transcript to pages of a presentation refer to the
roadshow presentation that was filed by Intercell with the SEC as
soliciting material under Rule 14a-12 on May 13, 2008)
***
Gerd Zettlmeissl
Good morning everybody,
this is Gerd Zettlmeissl speaking from Intercell. So its a relatively early
Q1 call of Intercell today, but the reason we have it so early is that we have a very important
news to tell you, in addition to our very nice Q1 news. Im here on the call with my colleagues
from the management board. Our Chief Financial Officer, Werner Lanthaler, our Chief Scientific
Officer, Alexander Von Gabain, and our Chief Operating Officer, Thomas Lingelbach. In addition I
would l like to welcome a special guest on this call, its Mr. Stan Erck, who is President and CEO
of Iomai Corporation, and he will also speak on this call at a later
point in time. The agenda
of the call is for us to give you an update on the financial and programme performance in the first
quarter, 2008. And then speak about the... the most imminent news; our acquisition of Iomai
Corporation, a vaccine company located in the Washington, D.C. area in the United States. If you
move to page four at this point I would like to hand over to Thomas just to give you, in the context
of the Q1 update, an overview of where we stand with our Japanese encephalitis regulatory
activities going forward. Thomas, please.
Thomas Lingelbach
Thank you, Gerd. Good morning everybody. Its a pleasure to update you on our progress on our JEV
to market programme, our leading programme right now. Everything so far is proceeding according to
plan and the most important topics we would like to update you with, with regard to the last
quarter, is that the FDA inspection as part of the US regulatory
approval process is now ongoing. And
there has been a discussion for quite a while as to whether or not we might need to have a product
advisory committee as part of the licensure process. FDA has waived this so called VRBPAC meeting
so theres no need for a critical product review at the FDA as part of this committee process. We
received, as part of the European licensure process, the Day 80 review, and we are well on track in
responding to those enquiries. The Australian PGA, and you might recollect at the last quarterly,
we were still discussing as to whether or not were going to get an accelerated approval process in
Australia. They have granted a priority review, which means that we
are going to get an action due date
by the end of the year. Our commercialization partner, Novartis, has submitted a licence
application for approval in Switzerland, so this is number four now, beside Europe, US and
Australia. And we have obtained excellent data in phase two trials in children, basically
confirming the immunogenicity and safety profile at even lower antigen content. With this short
update on JEV, I would like to hand back to Gerd to continue on the other programmes.
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Gert Zettlmeissl
The other programmes are also moving very nicely forward. We have a lot of progress in our vaccines
against hospital acquired infections. Dont forget the franchise where we have the only clinical
programmes in the whole industry going forward staphaureas and pseudomonas. We expect in phase two a result from the
staphaureas trial at the end of this year, early 2009, with our partner, Merck. The pseudomonas
vaccine is on track for starting phase two... three trials, also during this year, 2008. For the
pneumococcus programme, remember this is a new vaccine based on proteins only, with highly
conserved proteins protecting, essentially, against all 90 serotypes
of pneumococcus; really a great
innovation. This data is published in the journal of experimental medicine recently; it got a lot
of scientific benefit and recognition. And we are on track after having performed all preparatory
work and making materials to start the phase one, also in 2008. On our hepatitis C vaccine we have
seen breakthrough data in showing that the viral load can be reduced by T cell based therapeutic
vaccination, and we have seen a very good safety profile. The co-development we have here in this
programme, it is a 50/50 partnership with Novartis and is progressing very well. And we have
decided that we will include our strong adjuvant IC 31 into this vaccine to make the viral load
effect stronger; even stronger than we had before. The therapeutic approach has got also quite a
lot of recognition in the scientific and industry world. We just received on the last World Vaccine
Congress the best new therapeutic vaccine award, which obviously shows that this programme is a
highly regarded programme. In flu... you have seen in Q1 that we have seen good data for our phase
one, for our very first phase one trial. The programme is now ongoing with Novartis. We expect
further clinical trials to start in 2008 by Novartis also triggering, obviously, milestone
payments still this year. We have ended in the new collaboration for a breakthrough malaria
vaccine. We are working here again, with partners like in our pneumococcus programme and the
tuberculosis vaccine which is now in the broader industrial context
with Sanufi, is also moving very well with
further clinical trials. At this point, I would like to hand over to our Chief Financial Officer,
Werner Lanthaler, who will bring you all the news on numbers.
Werner Lanthaler
Thank you very much. I think its fair to say that our first quarter was strong. I would even go
that far and say it was unspectacularly strong, because there was no important message to be
reported on our financials in the first quarter, which is outside of any expectations. We have all
costs under control, we are fully on track to strongly increase our revenue base for this year, and
we are also fully on track to sustain profitability in 2008, despite the fact that we will also
discuss with you shortly, the acquisition that we announced today in the morning, which is an event
that followed Q1. We made a net loss of 4.6 million euros; which was planned given the fact that we
are fully running our operation towards market introduction of Japanese Encephalitis. That we are
fully running our full clinical pipeline at full speed. We increased our revenues to 8.6 million
euros in this quarter, which is a very nice step up from last year, which is mainly due to revenue
recognition from existing cooperations and deals. As you know, we control very nicely, our R&D
expenses with around ten million euros in the first quarter, which will also be the basis, more or
less, to go forward in the next quarters to come. There is a very comfortable cash position of 272
million euros on the bank, plus 40 million euros already committed forward payment
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without any conditions by
Novartis for this year, so we have around 300 million euros available at
this stage of the company, which could end up in a very strong, not only financial but also
strategic situation. With this, I think its also fair to say that we can finance the cash
component of our today announced acquisition comfortably from our existing financial reserves and we
are very happy that we can build Intercell and grow Intercell on such strong financial
fundamentals. What happened post Q1 is, as already mentioned, an acquisition and was a planned
acquisition as announced today, and I will basically bring you into this acquisition by stating our
mission again, which youll see on page number seven, which is accelerating innovation at this
point in time, for the whole vaccine industry by bringing the best technologies together and really
optimally financing innovation in this sector. What you can also see on page number eight, is that
we really distribute very nicely, over the quarter, our innovation optimal spending in R&D, and
also our balance with bringing in revenues. And never forget you have a company in front of you
that turned profitable without having the first product on the market. And you can imagine that by
bringing products on the market, which we will do with Japanese Encephalitis, already in 2008, in
Europe, in the US and in Australia. We think that we have a very, very good chance to really accelerate
our top line quite significantly, going forward. When you look at our... page number nine, you
basically see a setup also with an outlook of what you can expect
this year. We think that we will stay
profitable into 2008, despite the incurred costs, which are increasing due to the fact that we will
incorporate Iomai in due time when the deal is closed. You will see that we will increase our R&D
spending to really optimal into... invest in our R&D into innovation. You will see that we will
retain an extremely strong cash position by still having financed a strong component of this
acquisition out of that. And you will also see us growing our revenues by having just sales to the
US military in this year and by having also licensing and partner income in 2008.
With this I would like to guide you, on
page number 11, for the first time, into the deal structure
that we have entered into, by acquiring a US listed company called
Iomai Corporation. Its the
combination of the cash and the share consideration where we
tried to upfront, secure this deal also in
a sense that it will ultimately close in the very near future, by having aligned a part of the
shareholders already, to vote for this deal. You see us offering a share price of US$6.60 per share
of Iomai Corporation, which is a total consideration of around US$189, which represents US$122
million on current currency exchange rates, which is around 70 million in shares. New shares to be
issued from Intercell, two shareholders from Iomai that have already signed to accept a share
exchange from Iomai to Intercell, which will be a consideration of around US$119 million in cash
for the remaining shareholders. As already mentioned, we have more than 41 percent in share
exchange which we can do, and its a great honour and also a great pleasure for us that the
strategic rationale was so compelling that the shareholders of Iomai, who we addressed, to a large
extent were really more than willing to accept the share deal. We have aligned more than 50 percent
of voting agreements for this deal, and it is necessary to have more than 50 percent to get this
deal in the shareholders meeting of Iomai done. And we basically will finance the rest of the
acquisition through a cash merger between Intercell and the public shareholders in the United
States. From a closing perspective, we expect the deal to close in the third quarter, and we will
do everything to make this as fast as possible. Many of you will discuss, is this now a fixed
premium or a low premium, is it a high, but not such a high premium. And I think its a fair
discussion to have. Let me just reiterate that we think we did an excellent deal for Intercell for
our growth perspective, and for accelerating innovation. And prices are relative if you, for
example, look at the stock price of Iomai. When Iomai went public it was seven euros... US$7 sorry.
If you
4
look at the stock price of Iomai a year ago it was somewhere different. If you look at the stock
price of Iomai yesterday, it was also somewhere different. What has to be incorporated into this
valuation, is the strategic fit of this company to us, by bringing antigen, adjuvant and
delivery technology best in class together, and by adding late stage products into our pipeline where we
are certainly one of the best companies to industrialise late stage products into the market. With
this I hand back to Gerd.
Gerd Zettlmeissl
Indeed, as well as that, we are very proud to welcome the Iomai team on board. We have with Iomai
the best company developing needle free devices for application of
vaccines, a vaccine patch
developed over the years at Iomai. As well as that, valuation is relative. There is a very
important point to mention here, Iomai could really show a lot of breakthrough data during the last
couple of months, especially with the new and leading traveller diarrhoea vaccine, in addition with
a patch which is used in addition to pandemic inter pandemic flu vaccine. And from this we get as well, I
mentioned before, a very complimentary platform for our adjuvants, for our antigens we are
developing. And by that we are really convinced that we have here a very, very good strategic fit.
We obviously see opportunities from this technology, also moving forward with products. Intercell
has in development and also for general licencising possibilities, and we will come back to that in
more detail at a later point. At this point I would like to hand over to Stan Erck, President and
CEO of Iomai Corporation, to also give his view on the strategic fit of the deal. Stan, please.
Stan Erck
Gerd, thank you. I think most of what I have to say has been said, but from Iomais point of view,
weve been looking for... weve been developing two products now on a platform that we think can be
broadly applied. And the two products are now entering into late stage phase twos and into phase
threes next year. We think... weve been looking for some time to find the best partner to help us
develop these programmes into licensure. Were certain that Intercell represents that partner and
we think it will allow us to advance, not only the programmes into phase three and licensure, but
the platform as well. And the product and cultural fit we found has been quite great, so were
looking forward to this.
Gerd Zettlmeissl
Thank you very much, Stan. On page 13 you will see the summary again, and a reminder on our
technologies, our antigen indentification platform, with our IC 31 platform and now a new, world leading
vaccine patch delivery platform, also in our hands. There is a lot of synergy we see for these
technologies, but most important we also have, through the acquisition, two late stage programmes
coming into the Intercell portfolio. One is a leading traveller diarrhoea vaccine patch, which Stan
just mentioned, is expected to start phase three trials in early 2009, with a market potential
which is certainly above half a billion euros. In addition to that, there is a patch pandemic flu
vaccine coming into the portfolio where, like in the case of traveller diarrhoea, Iomai has shown
very recently breakthrough clinical data. This vaccine, this pandemic flu vaccine is, at this point
in time, fully funded by the human health services in the United States. And here also a very fast
development is possible. In summary, for the whole Intercell portfolio, it means that we get an
even broader portfolio in the traveller franchise in total, in addition to our Japanese
Encephilitis
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vaccine. And we also really put the focus even more on late stage programmes and development. We
think from the learnings we had in our Japanese Encephilitis to market programme, especially from
all industrialisation aspects and late stage clinical trials, and regulatory aspects, there is
enormous synergy we can leverage and can transfer all these learnings now, all these positive
learnings to these late stage programmes, especially to the traveller diarrhoea vaccine patch
programme. In this next slide on page 15 you see an overview; many things have been said already.
Late stage products are coming to our portfolio with the traveller diarrhoea vaccine patch, with a
vaccine enhancement patch for pandemic flu. Now we are definitely, with this acquisition, the
leader in needle free vaccine patch technology, which is a need in the industry. We can, in the
future, really deliver vaccines as alternatives to injected vaccines, but we can also use the
enhancement patch as it has been used in the pandemic flu, to see whether we can, at this stage,
reduce those end number of contractions of existing vaccines out there in the market, including
childrens vaccines. The company has headquarters in Gaithersburg, Maryland in the United States
and it is about 110 additional employees who will join now Intercell. And the company has, as I
said before, in the last ten years has been working on this vaccine
patch and has brought it to a
real industrial standard now, and therefore for us it was really the right time to get it into
our portfolio. On page 17 you see a summary that we... the message here is that we have here,
really, a very nicely balanced portfolio of products going forward in our hands; with partner
products, with own products going forward. And this strengthens even more our portfolio in the
company, and we are looking forward really to move this aggressively forward. At this point I would
like to hand over to our Chief Scientific Officer, Alexander Von Gabain, who will bring you in more
detail into the traveller diarrhoea programme and the flu programme of Iomai.
Alexander Von Gabain
Thank you, Gerd. Good morning ladies and gentlemen. I should state this is also for the CFO a very
exciting moment to help to build a new company by integrating Iomai. I think if you go to page 18, I
just to described to you the need for a traveller diarrhoea vaccine. You all know its making a huge
problem, not only for the quality of life of travellers, it also has an enormous bearing that many
of the traveller diarrhoea has after you catch the disease, long term
seguallabe. I think there is,
actually, an estimated 55 million people of travellers who are going into the endemic areas, and I
think there is... I will show this on the next page on number 19,
extremely high incidence, so your
vacation or your business mission is basically ruined by catching this type of diarrhoea. If you
look at page 19 you see a compilation of how many travellers are really going into these endemic
areas. This is the very left column. The middle column shows you that
from the incidence of
traveller diarrhoea the major part is attributed to traveller diarrhoea, and I think if you
assess... if you basically split up within the segment of traveller diarrhoea, what are the causing
pathogens, the key culprit is etec, and then there are a couple of other minor bacteria and also a
couple of viruses. The vaccine as it has been designed and developed into phase two from our
colleagues from Iomai, I think, is designed to really hit traveller diarrhoea by being directed
against the key culprit, which is etec. And I think you are too kind to follow me to the next
page, which is page 20, you see the clinical results. I think if you go to the left side of the
chart you see a base line of antibodies against etec, and I think the two types of antibodies, the
so called IGG antibodies, and the IGA antibodies. These most important ones because the protect
the mucosal intestinal tissue against the colonisation of the bug. More important, if you look at
the right side you see the anti placebo control, I think you have the... as expected, a high
incidence 23 of about 110 of mild, strong and
6
very severe traveller diarrhoea, with also discomfort which is going together. I think you can see
that, in the clean group, which is in the right hand chart, on the left side, our colleagues only
observed three mild cases. Let me state that this is outstanding work. The key data is going to
publish in the lincet, and I think they have also passing peer review. Next page please. On page 21, you see what
this really means. Youve got basically a 75 reduction of moderate and severe travellers
diarrhoea, and I think 84 percent if you say the total reduction of severe traveller diarrhoea,
which is the one that is paralysing your situation. It may sound for you strange, if I tell you
that there is a 66 percent reduction of etec infection only. I think this is because the remaining
people also have another and a much milder form of etec, but this was still etec. Or you can put
this the other way, the only, I think, instances where etec was still involved were very
mild forms of, basically, etec diarrhoea. What is particularly fascinating about the outcome of
the phase two trial is that it has been shown and demonstrated in this trial, that also many of the
other bacteria and germs that cause traveller diarrhoea basically seems to be co-protected by this
vaccine. This can be scientifically explained by the fact that etec is, kind of, the front rider. So if you
prepare your body and raise immunity against etec, you also lower the incidence of the other
pathogens that cause the disease. So the vaccine has enormous potential, I think, to broadly
protect you against this unpleasant disease. You should not forget that this is an entire new
technology. The vaccine has not been applied by needles. It has applied by having the people two
times putting patches on their skin. The trial has shown that there are no side effects and I think
on the next page, on page number 22, you will see that the patch
device diarrhoeal disease can now smoothly move
forward. I think at the 2006/2007, I think we saw phase two efficacy
data came out, and I think we
are now in the stage of preparing phase three trial, which is in the year 2008, so we can still
start in the 2009. And I guess with data which we have in our hands, we are pretty confident
that the new combined companies can pave the way for a regulatory forward pass to get this vaccine
in 2010 and 2011, so the pivotal registration trials. So at the end of 2011 we hope that we have a
product to registration. So I think we should say that the data and everything which has been
prepared and evolved and developed by our colleagues at Iomai, are really impressive. And I think I
have talked to many experts in the field, who are in this field, who say this is the best data they
have ever seen in traveller diarrhoea. Next page on 23, it shows that the patch has other
applications. I think just very shortly, on a note, the patch
contains a protein, which is at the same
the etec antigen, but it is also kind of an adjuvant. So I think that that the ingene vaccine
of a vaccine are in the most essential form, as you can imagine. And if you take the very same
patch and you inject people and inject the both pandemic flu vaccine, and you put on top of it this
patch, I think, then you get an extreme adjuvantation, which Ill show you on the next page.
But first let me remind you there are many governmental supported attempts to get... in
preparation for pandemic flu to be moved forward. The only one which is registered is extremely
high doses vaccine, which only gives, I think, a protection of about 44% after two injections with
90 microgram of flu antigen, and I think this is the best what we have today on the table. I think
there is no other in preparation for a pandemic flu. There is no other vaccine, which has gathered
for a pandemic registration.
So if you move to page 24, we show you the data, which our colleagues at Iomai have achieved and
recently announced in using exactly the regimen, which I have described to you, namely you inject
the pandemic flu antigen, into the skin, in a usual vaccination setting, and then on top of it you
put on this patch for a couple of hours, and I think this application has shown that only after one
dose with 45 microgram of the adjuvant, 73% of the subjects are
basically raising titers against
the pandemic flu virus, which are
7
sufficient. We should say that the guideline of FDA in preparing people and I think products
against pandemic flu have clearly stated, if you achieve more of 70%, you have, so to say,
fulfilled the criteria that you are enabling humans to have a pandemic flu vaccine, which is
working with one shot, exactly what has been achieved in this trial, which has been concluded.
Just to get you into the loop, to get to a registration of a pandemic flu vaccine, you dont need a
phase three trial. It is sufficient to do an extended phase two trial, and I think if the data
come out as we expect, namely to reproduce what we have seen at this stage, we get a pandemic flu
registration, and this has enormous implications because this has a very high chance that the Iomai
technology, which is now, I think they have integrated into our
company, will have, the great
opportunity to be a provider of a pandemic flu vaccine, which is meeting the criteria to protect
you with one shot, and I think, which I did not mention to you, with two shots, it looks even
better, and it looks equally better good than the existing (?) that pandemic flu vaccine,
which I described to you in the previous page.
On page 25, I tried to conclude my part, and what you can see, ladies and gentlemen, for a CSO, it
is more and more difficult to, I think, coherently guide you through all our clinical programmes,
which has dramatically grown. So we have on the top line, the JEV, which is moving to
registration, now, in addition to traveller diarrhoea, we have, as Gerd told you, made nice
progress on staph aureus and pseudomonas and hepatitis C. Pandemic flu has came through a phase
one two trial, and is starting a phase two trial still this year. This has been now adding into
this pipeline. Also you should remember for the inter-pandemic, seasonal flu vaccine, we have made
nice progress with our adjuvant, and I think this is moving together with our partner, Novartis,
and also our tuberculosis vaccine, with SSI has found a nice harbour, by having Sanofi in the
boat, as a commercial developmental partner, and our pneumocaccal vaccine makes very nice progress
in moving forward still to a start in this year.
I dont go through all the other pipeline products, but you can see that if you now take all this
fantastic technologies we have, and Id just like you to follow to 26. It shows you from a, so to
say, immunological point of view, why patches are such an exciting tool for vaccine development.
We, who are in the arena of vaccines, we know all along that the most important first wave of
intermediate immune competent cells, which need to be trained, they are the upper layer of your
epidermis, and this patch device does something extremely elegant in a very reliable fashion. It
is taking off the upper layers of your epidermis without injuring your skin. And that makes this
area, which, so to say, has, I think, repaired the epidermis, the so-called antigen-presenting
cells, to infiltrate, and then you take the patch, and the patch is formulated for the time being
with the etec antigen, which I told you is also an adjuvant, but we are confident that you can
combine this also with our antigens, and with our adjuvants, or as a combo of, I think, the three
components we have now in this combined company on the table, and can repeat what our colleagues of
Iomai excitingly have been shown to induce strong immunicity.
On page 27, you see really how I think this patch vaccine technology, I think the (), is basically
functioning, and I think, how many applications you have, if you go to the left side, I think you
can see we have the TB vaccine, but we could also include, for example, our pneumo-coxi antigens
into such a patch, which will make it particularly suitable for a children vaccine, and there are
many other applications, which I think we will come back
8
to you next time, because we are designing a joint strategy. I think you could apply it also for
our hepatitis C vaccine, and others. On the right side, it has immediate consequences. I think it
will make us a pandemic flu, moving forward. I think we can consider a second-generation, one-shot
Japanese encephalitis vaccine, without changing, I think, doing exactly the same thing, which
has been done for the flu vaccine, and there are plans we are currently discussing in the new
company, which is created, I think to use also the patches to reduce the number of injections for
the usual childhood vaccines, and there are many other applications.
And I think this is a real good point to thank our colleagues at Iomai for their excellent work,
and I hand back, I think, the word to our Chairman and CEO, Gerd Zettlmeissl.
Gerd Zettlmeissl
Thank you very much, Alex.
The next
slides on page 28, 29 and 30 just summarise again what has been said.
A strong traveller
vaccine franchise with the addition of the traveller diarrhoea vaccine with a combined market
opportunity of above 750 million euros. A strong portfolio of vaccines in the flu arena, with our
IC 31 flu vaccine we are doing together with Novartis, and now the Iomai pandemic vaccine patch
moving forward, and last but not least, on page 30, as Alex now described, all the synergies we
have by applying our antigen and adjuvant technologies, together with the new delivery system in
the world class delivery system we just got through the acquisition of Iomai.
We have a plan, on page 31, for integration, which obviously shows you again also the timing, from
signing to closing, in the next two to three months. The companies
will operate on a joint steering
committee basis, and then after the closing, we will have a clear integration plan, for Iomai, and
just to bring our colleagues in the United States in the loop of the Intercell organisation, very
nicely and very smoothly.
Last but not least, on page 32, a summary again on our Japanese encephalitis to market. I will not
go again back into details. We discussed all that. The same for our staph aureus programme, on
page 33, going forward with Merck, and our pseudomonas programme, going forward, in our own
development is just for you a summary of all these activities, and I hand back to Werner to sum up
and to give you also an overview on the future milestones coming up.
Werner Lanthaler
Next, page 35 basically shows you that we have a strategy, and I would call it, its a, what do we
say, strategy, by growing and accelerating Intercell, going forward.
Page 36 shows you that our shareholders, and I can assure you that many of our shareholders are
very happy with what we are doing in regard also with accelerating the company, will change in a
sense that we will integrate also Iomai shareholders with issuing around 1.7 million new shares out
of Intercell, where all legal aspects are in place already for having the ability to do this. This
represents a dilution effect of less than 4%, and we think it is a justified dilution by the great
value that we get into this company. You will also see that with this acquisition we have a much
stronger footprint in the United
9
States, which is a key market for us when it comes to our product sales, going forward, and
therefore we are very happy to have now a strong presence in the United States as well.
And on the last page, we basically want to introduce you, and invite you to follow Intercell going
forward, because this is one step forward, with many more steps to create additional value for our
shareholders to come in the very near future. Watch out for our hospital-acquired franchise. This was
not touched upon too intensively now, because we will spend a very big part of our upcoming R&D day
on this, strongest franchise in hospital acquired infections in the next couple of days and weeks.
And especially watch out for the leverage that we will get out of our IC31 AIP technology and the
vaccine patch, going forward.
With this, I would like to invite you for all your questions, and I apologise that this time it was
a little longer conference call than usually on Q1 results. Thank you very much.
I want to hand back to the Operator, and ask you for your questions.
Questions and Answers
Peter Welford Lehman Brothers, London
Hi, its Peter Welford, from Lehman. A couple of questions, firstly on the Iomai acquisition and
the patch, travellers diarrhoea patch. I was wondering if you could talk a little bit about how
you think a moment about commercialising that product potentially, given that you talk about the
synergies, obviously, with the Japanese encephalitis vaccine for travellers? But Novartis
obviously has rights to the marketing for that, so I was wondering just how you thought about that?
And if you could also talk a little bit about the duration of effects that you...or if youve
looked at duration of effects with the patch, and so I guess how long you can be on holiday for?
How long your immunity lasts? And does the patch have to remain attached for that to be the case?
And then if you could just go on as well, to the potential phase three trial design? Does it have
to be carried out in endemic areas, and how many travellers are we talking about?
Gerd Zettlmeissl
Yeah. Peter, thank you for those questions. First, on your question on commercialisation.
Indeed, you are completely correct we do the commercialisation of the Japanese Encephalitis vaccine in
most territories with Novartis. At this point in time we have not yet decided how to move forward
with a travellers diarrhoea patch commercialisation in the future, but obviously there could be a
likelihood always that there is an interest to go also with Novartis in this context, because
Novartis has been very strong in the past in commercialisation of traveller vaccines, but, as I
said before, no decisions yet, we see also the other opportunities.
Coming back to your question on the duration, of the immune response; from the current data, which
has been done by our colleagues of Iomai, we think that you have at least a couple of months of
protection after the second patch being given for the travellers diarrhoea, but there will be
obviously a long term follow up in the immunogenicity, and in the protection of the patch, if we are
moving forward in future trials.
10
And last, but not least, if it comes to the phase three trials, the phase three trials will be
using very much the design of the phase two trials, where people were vaccinated before they were
travelling into South America, and were then followed up for diarrhoea incident and for etec infection
incidents, so well use very much the design of the phase two, to do an extended study then in the
phase three. And we think that in the range of about 1,000, plus minus, should be enough to show
clear efficacy of the vaccine, going forward. In addition to that, you obviously have to do safety
trials, and lots and lots of consistency trials, in the future.
Okay, can I just quickly follow up? Have you done any...or have we got any data at all on the
patch? The patch itself, in terms of how well it remains attached? Any effect if the patch does
become removed? Any data at all on that in safety trials?
No, the patch is very stable.
It needs to stay at the moment for about six hours. But
it can even be, you know, take a shorter time in the future to keep the patch on, and we dont see
any problems with the application of the patch.
Great. Thank you.
Erica Whittaker Merrill Lynch, London
Hi there. Its Erica Whittaker from Merrill Lynch. Just another question about the travellers
diarrhoea patch. I mean, presumably it would address significantly more travellers, potentially
than the JE vaccine, but could you give us a comment on how youd expect a product like this to be
priced? And secondly, I was just wondering whether the acquisition process for Iomai, if there
were competing bidders, so to speak, and how comfortable you feel that the deal with be concluded?
Thank you very much, Erica, for the question. Gerd speaking. Ill take the first, and Werner
takes the second.
On the TD patch, youre absolutely right. We think that the market is significantly bigger as for
the Japanese encephalitis, because it also, you know, really addresses people going into other
areas than Southeast Asia, meaning South America, but also Africa, so its just broader
application. On the pricing, we think that a price somewhere for the vaccine in the range of 80 to
120 dollars per dose would be a reasonable price, but obviously these are things, which will be
defined in a later stage, when we are coming closer to registration. The second question I would
like to hand over to Werner.
Werner Lanthaler
Its always an exciting time between signing and closing, but I can just put the points forward to
you, what we think we have done optimally, in order to secure the deal. We have aligned and
convinced many of the existing shareholders of Iomai about the strategic rationale. We will do
everything to convince the market on the rationale of this deal, and I hope that this is the first
step to it. We want to do, and I think it is more important than many people think, everything to
do that the employees of Iomai think that this is the best combination that they want to work for,
because whoever wants to bid against us should lose the people, and we want to keep them.
11
Is it the right premium that we are paying? I think it is something, which is fair, as already
stated before. And with this we feel very secure. Okay. Could I just confirm from Gerd that the
pricing for the TD patch was 80 to 120 dollars per vaccination? Or per dose?
Gerd Zettlmeissl
No, this will be the idea per vaccination, essentially, we can think about in the future. Okay.
Thank you.
Linden Townson Goldman Sachs, London
Yes, this is Linden Townson from Goldman Sachs. Ive just got a quick question on one of the press
releases Ive seen on the Iomai website from April 3
rd
, where theyve signed a deal with
Merck and Co, looking at the immunostimulant patch. It says that theyve got first option to
negotiate an exclusive licence on that. I was just wondering where that stood now obviously youve
acquired the company?
Yeah. No, thank you very much for this question. The collaboration with Merck is just a product
specific collaboration, where essentially you see for the first time also interest in a big vaccine
company to use a patch in order to improve injectable vaccines, as it has been shown for the
pandemic flu vaccine. This is very much product specific, and these are indications, which we have
no interest, or any of our other partners have at this point interest in. We think that we can
broadly use the vaccine enhancement, or immunostimulant patch in different vaccines with different
partners, and this is one of the business opportunities we see coming out of this acquisition.
Okay. Thanks.
Khytai Thakrar MP Adv, Mumbai
Yeah. Hello. My question is regarding travellers diarrhoea vaccine patch. Using IC31 adjuvant
for the kind of second generation of TD patch, or, in future, so...?
Alex, would you like to answer this question, please?
Alexander Von Gabain
I...can you repeat the question? I could not really hear. Can you repeat it please?
Yeah. Will you use IC31 adjuvant? Its an Intercell for redesign all generation, second generation of
travellers diarrhoea vaccine patch, or so...?
I guess...thank you for the question, now Ive got you acoustically. I dont think we will
necessarily use it for a second-generation diarrhoea vaccine, because the diarrhoea vaccine, as it
has been designed, has a good adjuvant, which is this etec antigen, and a good antigen, which is
this etec toxin. But I think you are addressing a very good question. We are pretty confident
that you could combine the patch with IC31 in many other indications
where we already have seen
very positive outcomes with IC31, and where we believe that the patch is a more rational design to
deliver the vaccine, but also further facilitating the immunogenicity by directly, so to say, applying
it to the skin, and this is one of the first things we are trying in the combined future R&D
pipeline.
12
Okay. Thank you.
Ann Marden JP Morgan, London
Hello. This is Ann Marden from JP Morgan in London. Can you guys hear me?
Werner Lanthaler
Sure.
Okay,
great. Well, congratulations on the deal. And just on your R&D
spend, could you talk about
how much your R&D spend will go up now, in 2009, when youre paying for the phase three trials for
the travellers vaccine, please? And then I also wanted to ask about whether or not you would be
looking at using this patch technology in paediatric vaccines?
Gerd Zettlmeissl
Yeah. Thank you very much, Ann, for the questions. For the first questions on the R&D spending,
we have a situation at the moment that obviously for our Japanese Encephalitis late stage
development those costs will be still carried in 2008, and then will go down in 2009, and we will then
replace these costs also, now focusing on the travellers diarrhoea patch, we think in the range of
about 20 to 30 million dollars additional costs, but there will
be also a shift going back
forwards, so this will not a 20 to 30 million overall increase for the Intercell R&D costs.
The second question, on the use of the patch in paediatric vaccines, you touch a very interesting
point here, because we really feel that this, especially this vaccine enhancement patch, or
immunostimulant patch, can be used in many vaccines, including paediatric vaccines, to reduce the
number of injections, to reduce the dose. It is definitely one of the applications, and the
interesting thing is with the pandemic flu data, our colleagues from Iomai for the first time have
clearly shown that this works, and this is from the proof of concept, and again we have seen for
the travellers diarrhoea vaccine a clear proof of concept that this was the right point for us to
now take it on board, for Intercell.
Right, okay. Thank you.
Erica Whittaker Merrill Lynch, London
Hi there again. Just wondering about manufacturing of Iomai for the TD patch. Could you give us
an idea of how happy you are with their manufacturing facility, what the capacity is, in terms of
patch production? And secondly, Ive just got a question about the fast track designation from the
TGA; what timeline then do you get for approval if you get fast track from the Australian
regulators for your JE vaccine?
Yes. Just take the first question; the second will be taken by Thomas. On the manufacturing, we
have been very comfortable. It was one of the drivers for us to make the decision, because there
is an existing GMP manufacturing facility for patches at Iomai, and owned by Iomai. This facility
is up and running to produce phase three clinical material for the different patches, namely for
travellers diarrhoea, and for flu. We think with this facility as it stands, and with some
certain adaptations, we can make in the range up about five to ten million, or this more to the
higher number, and in future with certain investments, can also increase that.
Concerning the second question on the Australian TGA acceleration, maybe Thomas can give us a short
answer?
13
Thomas Lingelbach
Okay. So, hello, Erica.
Hi.
On the TGA acceleration we have an action due date given by the Australian authorities, which is
December 2008.
Okay, thank you.
Khytai Thakrar
Yeah. Hi. Sorry, one question I forgot to ask, the question is for Werner. After this
acquisition, whats your current cash position, and will it increase your annual expense guidance
for 2008?
Werner Lanthaler
Our cash balance will remain above 200 million euros, comfortably. And our expenses with increase
in R&D, by taking up the Iomai operation, and I think here its conservative to assume that it will
be the same, at least the same, as Iomais spending at this stage. By the way, Iomai numbers will
be published today, in the morning, or tomorrow in the morning in
whatever time zone youre in. And for
2009 its largely depending on how the clinical trial programme is set up, but here Gerd gave the
guidance with a three-year maximum development for bringing the product from phase three to the
market. And 50 to 70 million clinical programme for TD. Euros.
Thank you.
Peter Welford Lehman Brothers, London
Hi, sorry about this. Just a follow up. Im just a bit confused after, because the point youve
just made, so should I understand then from the previous question that its 20 to 30 million
dollars additional R&D per year? 50 to 70 million euros in total, over three years? Is that how
we should understand it?
Gerd Zettlmeissl
Yeah, this is the total. The total is in the 20 to 30 million per year, going forward, heading up
to something in this range.
20, 30 million dollars per year, adding up to around 50 to 70 million euros?
Yes, exactly. And the reason for that is that, you know, the spending in the other programmes will
be relatively lower. The programmes, which are not travellers diarrhoea and all of the pandemic
flu programme, is funded by the HHS as we said before.
Thats great. Thanks [unclear].
14
Werner Lanthaler
One strategic remark to make is that we think, with all our sales forecasts, we feel relatively
comfortable to keep a profitable company, going forward, and to grow a profitable company, going
forward, despite the fact that we are bringing much more potent products to the market in the year
2011, 2012, from a market perspective.
Closing Comments
If there are no further questions, then I would really thank you very much. I would like to take
also the opportunity and invite you again to our R&D day in London on 14
th
May, and in
the United States on 21
st
May, because there we will have a little more time to
elaborate on another most important franchise of Intercell, which is the hospital-acquired
franchise, where we clearly see us as the leaders in the field as well as to the fields that we
touched upon right now.
Thank you very much, and lets hope for all the best for all of us. Thank you.
Gerd Zettlmeissl
Thank you. Bye-bye.
Alexander Von Gabain
Bye-bye.
Additional Information and Where to Find It:
In connection with the proposed transaction, Iomai Corporation will be filing a proxy statement for
its stockholders and other documents regarding the proposed transaction with the Securities and
Exchange Commission (SEC). BEFORE MAKING ANY VOTING OR INVESTMENT DECISION, IOMAI STOCKHOLDERS AND
INVESTORS ARE URGED TO READ THE PROXY STATEMENT AND OTHER RELEVANT MATERIALS CAREFULLY IN THEIR
ENTIRETY WHEN THEY BECOME AVAILABLE BECAUSE THE DOCUMENTS WILL CONTAIN IMPORTANT INFORMATION ABOUT
THE PROPOSED TRANSACTION AND IOMAI. Investors and stockholders may obtain copies of the proxy
statement and other relevant documents filed with the SEC by Iomai free of charge at the SECs web
site at www.sec.gov. In addition, investors and stockholders may obtain copies of the proxy
statement and other relevant documents filed with the SEC by Iomai (when they are available) by
going to Iomais Investor Relations page on its corporate website at www.iomai.com.
Iomai and its directors, executive officers and other members of management may be deemed to be
participants in the solicitation of proxies from Iomais stockholders with respect to the proposed
transaction. Information regarding Iomais executive officers and directors, and their beneficial
ownership of Iomais common stock as of March 26, 2008 is available in Iomais proxy statement for
its 2008 Annual Meeting of Stockholders, which was filed with the SEC on April 4, 2008. Other
information regarding the interests of such
15
potential participants in the proxy solicitation will be contained in the proxy statement and other
relevant materials to be filed with the SEC when they become available.
Forward Looking Statements for Intercell AG:
This communication expressly or implicitly contains certain advance statements concerning Intercell
AG and its business. Such statements involve certain known and unknown risks, uncertainties and
other factors which could cause the actual results, financial condition, performance or
achievements of Intercell AG to be materially different from any future results, performance or
achievements expressed or implied by such advance statements. Intercell AG is providing this
communication as of this date and does not update any advance statements contained herein as a
result of new information, future events or otherwise.
Forward Looking Statements for Iomai Corporation:
Some matters discussed in this press release constitute forward-looking statements that involve
known and unknown risks and uncertainties that could cause actual results to differ materially from
those expressed or implied by the forward-looking statements. Such forward-looking statements
include statements about the anticipated acquisition of Iomai by Intercell and timing of and
potential benefits of the anticipated acquisition; the potential synergies between the combination
of Iomai and Intercells product technologies; expectations regarding the timing of clinical trials
and product development; the ability of Iomais adjuvant patches to provide protective immune
responses; the significance of clinical results described in this press release; expectations that
the clinical trial data from a clinical trial will be sufficient to proceed with future clinical
trials; estimates of potential markets for Iomais product candidates; the potential for Iomais
product candidates to be lower cost or more effective for specific patient populations;
expectations that the characteristics of Iomais adjuvant patch for pandemic influenza would make
the product ideal for stockpile and rapid distribution; expectations that TCI technology will
enhance the efficacy of or replace or be an alternative to current injected vaccines, expectations
that TCI technology can facilitate development of a broad range of vaccine products; and
expectations for further collaboration with Merck & Co., Inc. or any other potential
collaborations. These statements are subject to risks and uncertainties that could cause actual
results to differ materially from those projected in these forward-looking statements. Applicable
risks and uncertainties include, among others, that the proposed acquisition does not close or that
the companies may be required to modify aspects of the transaction to achieve regulatory approval;
that prior to the closing of the acquisition, Iomais business suffers due to uncertainty; that the
companies are unable to successfully execute their integration strategies, or achieve planned
synergies; that future clinical trials may not replicate results seen in the trials described in
this press release; that the U.S. Food and Drug Administration or other regulatory authorities may
not concur with Iomais analysis of the trial results described in this press release; that Iomai
may not be able to enroll sufficient numbers of subjects in future clinical trials; that Iomai may
be unable to obtain the regulatory approvals or financing necessary to conduct additional clinical
trials; that competitors may develop products that are safer, more effective, or more convenient to
use; that future clinical results may not support regulatory approval to commercialize Iomais
product candidates, which will depend on the outcome of additional clinical trials and analysis by
regulatory authorities of data Iomai submits; that development costs may exceed expectations; that
Iomai may fail to adequately protect its intellectual property or may be determined to infringe on
the intellectual property of others; and the risks identified under the heading Risk Factors in
our Annual Report on
Form 10-K
for the year ended December 31, 2007 and filed with the Securities
and Exchange Commission. Iomai cautions investors and others not to place undue reliance on the
forward-looking statements contained in this press release. These statements speak only as of the
date of this document and we undertake no obligation to update or revise the statements. You are
encouraged to read Iomais filings for a discussion of these and other risks and uncertainties
which are filed with the U.S. Securities and Exchange Commission and are available at
http://www.sec.gov.
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