In late 2012, Arrowhead Research shocked the Oligonucleotide
Therapeutics world when it presented spectacularly potent and prolonged gene
knockdown data in non-human primates using a subcutaneously administered
single-molecule Dynamic Polymer Conjugate (DPC) formulation. This arguably represented the most elegant
delivery technology at the time.
Moreover, also due to its small, but not too small size (10-20nm) and
slight negative charge, it provided us with a glimpse into the future of systemic RNAi delivery for regulating genes beyond the liver.
It certainly got my
full attention and made me invest almost 100% of my stock portfolio back then.
Unfortunately, despite the validation in non-human primates
which suggested clinical readiness would not be far off, the subQ DPC technology
has seemingly struggled to reach clinical/commercial maturity. Not only
Arrowhead’s lead development candidate, ARC520 for HBV, but also its second development candidate,
ARC-AAT for AAT-related liver disease, was still based on the intravenously
administered two molecule DPC version.
Although the reasons for the delays were never really disclosed, a few
comments here and there made it seem very likely that chemistry and manufacturing
issues were behind the delay.
Back to the Future
Last week, Arrowhead Research finally published a paper
showing that single molecule DPC is still alive and kicking (Rozema et al.2015) and is progressing towards clinical application. In essence, the new single-molecule subQ DPC
prototype comprises of a membrane-active polymer which has been masked from
premature cytotoxic interactions by pegylation and cell-targeting ligands that
are added via protease-sensitive bonds;
as before, the highly modified/stabilized RNAi triggers are appended by
disulfide chemistry.
The DPC is made in a 4-step process followed by a
purification step to remove unwanted side-products and reactants. The latter step is apparently important when
going into primates.
The new old DPCs are thus distinguished from the intravenous
version not only in that it combines the RNAi trigger and endolysosomal release
polymer in a single molecule, but most importantly by the nature of its
triggered release mechanism. Whereas in
the former DPC generations triggered release was dependent on changes in pH such as they occur when a DPC is endosomally taken up, they are now responsive to the
presence of certain proteases in lysosomes.
pH-dependent formulations apparently suffered from instabilities
both in the body and during storage.
This was adequate for targeting genes in the liver because of the ready
access of macromolecules in the circulation to this organ following intravenous
administration, but not when the DPC first has to reach the circulation from
the subcutaneous space and when less well accessible target organs are the
ultimate destination.
Accordingly, non-liver single-molecule DPCs of the latest publication
had impressive circulation half-times of
the intact, protected molecule of 11 hours. Similarly, such DPCs are stable for at least a
year both in solution and when lyophilized.
The extra-hepatic
potential thus facilitated by increased stability now needs to be
demonstrated by finding suitable targeting ligands and I’m sure Arrowhead has
been busy working on that. It should be
noted that for target tissues where high concentrations comparable to the liver
are unlikely to be achieved following systemic delivery, the extra kick that
comes from an explicit release chemistry could provide a critical advantage
over competing approaches. These include
simple conjugates of the GalNAc-type and probably also self-delivering RNAi
trigger chemistries which incorporate ‘milder’ release chemistries (like lipid
tails).
Knockdown lasting for
weeks and months
The most impressive demonstration of the single molecule DPC
performance in the Rozema paper came from the primate studies. Here, a single administration of 0.5mg/kg 2’-O-methyl/F-modified
RNAi trigger led to a highly potent knockdown (peak knockdown >95%) of liver
expressed Factor VII with >80% knockdown of 2 and 4 months following
subcutaneous and intravenous administration, respectively.
Following the 2012 delays and some uncertainties around what
was really new and old in the recent publication, I am somewhat hesitant to declare that subQ DPC is now fully de-risked and ready-to-go.
In that regard, it would be helpful to learn more about the tox profile
of the new molecules and related to that which polymers will be eventually used
(e.g. 2-molecule with melittin-like peptide, a polyacrylate in the
publication).
Nevertheless, since Arrowhead has said that the new 2015
development candidate may be from the subQ line of DPCs (or if not going after
a extra-hepatic target) one would think that the most important challenges have
now been overcome.
10 comments:
Nothing coming next week with the ER. Nothing coming til after Obama gets his Fast Track Authority. We can just sit here and twiddle thumbs until then.
I think DPC is still not ready for SubQ delivery yet. Volume of injection seems to be too high. Higher injection volume can also create other problems like ISR. Does the SubQ need any premedication? Many questions remain to be answered.
Dirk wrong about manufacturing. ARWR is way ahead on MFR processes - look at their latest PR, where they said that they have learned much from their prior MFR experiences with ARC-520.
The reason for the slow progress of subQ (as I posted several times), is the long duration effect subQ has, versus DPC1 = 6+ months versus 2 months.
In preclinical design, they design the drug, test for 6 - 8 months, study the results, then redesign fore refinement. That's a year per development cycle, and why it took so long.
It was finally ready last year, 2 years after he read their 2012 paper on it, and that's when the work of starting a drug with it began, which we will see either this year or early next year.
Does the nine chimp trial revelation tell us that Novartis and Alnylam not know what they are doing when they gift Arrowhead their IP and targets?
Or does it suggest that data in hand at the time meant they could shift the next building block into place in anticipation of a Pharmasset type buyout?
I am of the latter view. Interested to hear the opinion of others. And whether any of the IP in use is inlicenced or not. And what a buyout would mean for the IP holders.
ARWR chimp trial is great news and clearly indicates they believe they are on to something momentous in medicine.
However market wise none of it will mean anything unless the shorts are satiated.
That may come only from the closing of the trade agreements with Asia/Japan and Europe.
Only then will you have success in the markets. Be that a buyout or any other transaction.
Modest as well.
I'll let you in on pro trick. Do it once ahead of good news, then point to it forever thereafter.
As well as what?
Maybe bullish on BLT now as well if short RGLS. Or if short RGLS then his largest never sell holding in ISIS must be short as well since they are a part of the RGLS JV with those nasty people he has told us about at ALNY.
Both of whom are about to lose their sector leader status if we listen to Dirk. And if not to RGLS then to whom?
I guess Dirk must know better than GS and JPM combined.
Short RGLS while PFE and MRK are still holding their cards and then tell everyone about it, when on another breath the message is don't come to my blog looking for charity!
You've blown your cover Dirk. Don't ever pursue a career in the BND.
Some interesting comments and detective work on InvestorVillage regarding the nine chimp trial.
Salient references from tufulipo regarding his bigger hand and grassy knoll comments. However, I am not sure if he is referring to the hand of government or the black hand. Am sure its not the invisible hand. Both were believed to be present on the grassy knoll that day. Even if they were embodied in just the one or so individual. And the black hand is easily found in stock markets.
And due to ARWR activities being based in Hong Kong/China and Australia, which government(s) is he referring to?
Dirk, what are your thoughts on PFE about to make a buy out?
Are you still short RGLS and long ISIS because of it?
Remember the update in the 2 molecule delivery model presented at TIDES last May?
Next Generation Dynamic PolyConjugate (DPC) for siRNA Delivery in vivo
http://files.shareholder.com/downloads/AMDA-2OTJP1/3957740268x0x759231/2007D6C8-93BB-4EB3-9C1F-54A6756642E7/TIDES_2014_Almeida.pdf
That, too, moved away from pH sensitivity.
Was that perhaps a step on the way to this newer generation single molecule model?
Linda
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