Today, I will explain why I believe that ARC520, the chronic HBV drug candidate by Arrowhead Research, is particularly
well suited to exploit the unique potential of RNAi to deliver a functional
cure for many people suffering from chronic HBV. For the basic rationale of using RNAi gene silencing to treat HBV, the reader is referred to the previous blog entry.
ARC520 is Highly Potent
As illustrated in this week’s publication of preclinical
data on ARC520 (Wooddell et al. 2013), ARC520 promises to be a particularly potent example for therapeutic RNAi gene knockdown. 90% and more knockdowns were routinely
observed for all HBV proteins. What is more, the protein for which knockdown
is most important according to the underlying immune reactivation hypothesis, the Hepatitis B surface
Antigen (HBsAg), seems exceptionally susceptible to RNAi with multi-log gene knockdowns for this target. Equally important, the
masked melittin-like peptide component of DPC, expected to be dose
limiting, was very well tolerated at 10mg/kg in non-human primates, the highest
dose tested in the publication. Such an amount was considerably more than what was required for achieving
maximal knockdowns.
HBV is also an example for which the high knockdown potency of DPC
(and SNALP) sets it apart from other potential competing RNAi Therapeutics approaches for
HBV, including a GalNAc-siRNA conjugate-based one, which lack knockdown potencies adequate for such a
viral applications. At this moment, I do
not exclude Tekmira to become interested in HBV as well, especially with their
UsiRNAs and MV-RNAs which they probably consider to be free from the Alnylam-imposed
target restrictions.
ARC520 Fits into Current Standard of
Care
At the AsiaTides meeting in Tokyo that I have just attended
(btw, you’d be amazed how much serious RNAi Therapeutics development work is
going on in Japan, China, and South Korea), Dr. Lewis from Arrowhead Research
presented drug-drug interaction data for ARC520 and Entecavir, the current
standard of care Nuc for HBV. These interaction studies performed in mouse
models of HBV are important since ARC520 would initially likely be
used in combination with current standard of care (probably also
interferons). In fact, the distinct
mechanisms of actions of Nucs, interferons and RNAi Therapeutics would neatly
complement each other. Importantly,
ARC520 did not impair Entecavir-mediated suppression of viral replication nor did
Entecavir impair the 2-3 log-fold viral protein suppression by ARC520.
Moreover, the data which include 80% knockdown following a single
administration after 3 months in non-human primates (Factor VII
surrogate gene), clearly support once-monthly dosing. Given that ARC520 is not intended as a
chronic therapy, it should thus easily fit into current treatment regimes.
ARC520 May Be Foundation for HBV
Franchise
ARC520 is administered by intravenous infusion. In terms of dose escalation and achieving
maximal potency, this is positive since solubility and injection volume issues
do not apply. However, there is the obvious opportunity for Arrowhead to enhance the value of their HBV franchise by
developing a subcutaneously administered follow-on candidate, thus capitalizing
on their progress with the protease-sensitive DPCs. This would broaden the target population and
extend market exclusivities.
Risk-Reward
For a small biotech company like Arrowhead Research, the
enormity of the HBV opportunity also comes with its challenges. The complex course of chronic HBV and
probably also the various genotypes mean that clinical development will be
equally complex- and costly. I have followed
with horror the many billions Vertex Pharmaceuticals invested on developing
their HCV drug after the first exciting phase I proof-of-concept data were
reported. Ultimately, Vertex
shareholders that had invested before the phase I validation, only made a 3x
return taking on all the risk, and those that jumped onto the bandwagon after
the results did not see much appreciation after 6-7 more years, despite of the fact that clinically
pretty much everything went according to plan.
Part of the expense, however, was also driven by the fear of
the emerging competition in HCV leading to a capital intensification of
clinical development. Except for
competing RNAi Therapeutics candidates enabled by similarly potent
liver-directed knockdown technologies (perhaps SNALP), I do not see such
intense competition emerging for ARC520.
Another risk for Arrowhead is that while the immune
reactivation hypothesis is attractive and supported by clinical data
correlating HBsAg seroconversion with preceding loss of HBsAg, the remaining
uncertainty may make ARC520 unsuitable for a small platform company to wager its
entire future on it. By contrast, a Big
Pharma may be willing to take on the risk if it agrees with the hypothesis simply
because the market opportunity is so large.
Witness how much capital is being spent on the amyloid hypothesis in
Alzheimer’s Disease or the good HDL-cholesterol hypothesis in cardiovascular disease.
Therefore, at the right time and for the right price, also
depending on factors such as clinical data, share price performance, and the
availability of non-dilutive funding opportunities, the HBV franchise should be
partnered. The issuance of the patentcovering the protease-sensitive DPCs which are amenable to subcutaneous
administration could be an important piece in this puzzle. After all, with manufacturing much less of an
issue with DPC 2.0, you don’t have much to sell unless you control the IP.
You lost your credibility, sir, when you endorsed Davis' work in San Antonio Spring '09- not that you were right or wrong about 'the science'- but, that you took an economic viewpoint or position.
ReplyDeleteIs this what you are doing now w/ regard to Arrowhead? With the same deceptive management? Can you make any objective referrals regarding either 'the science' Arrowhead picked up so cheaply or an objective explanation for why Roche would dump such 'great economic value'?
(We all have to make a living)
Great point, anonymous. As everyone will be quick to notice, Roche has never made 40 billion dollar mistakes in the past that could be indicative of the loss of future earnings...
ReplyDeleteDirk,
ReplyDeleteIt doesn't make much sense to me that Arrowhead would advance I.V version into the clinic if they already have a more potent SubQ version of ARC520. Tekmira delayed their Ebola program just to advance more potent formulation into clinic, which makes sense.
When they claim 99% of gene knockdown at 1 mg/kg of SubQ dose, it is not clear if it includes only SiRNA component or it includes both the component of the drug.
Agreed with the first post to some extent. No one is truly unbiased. Dirk has written some nice criticism of SRPT data, which has been adored by the whole angry mob including the great Feuerstein.
ReplyDeleteAt the end of the day, read as much as one can for both bull and bear thesis, then do you own homework to make your informed decision.
Looking past the immediate excitement of using RNAi such as arrowhead's IV, the long term treatment for diseases such as this, HBV and HIV will be a gene therapy.
ReplyDeleteIt is not that Roche didn't believe anymore in RNAi. Large pharmaceutical companies, pressured by patent expirations and declining sales, no longer had the patience to follow through in the development of this novel technology.
ReplyDeleteRoche just had to cut costs. And they wore in different fields. It is like on Wallstreet, if one guy is selling, the herd is doing the same! And most without thinking what they are doing. If Roche is out, I have to go out too! It is as simple as this. Innovation is done much better in small units!
RNAi is far from dead. As with monoclonal antibodies before it, biotechs will once again lead the way innovating and developing the technology. Look at other biotechs are working on next-generation technologies.
Commentators have noted RNAi is beautiful in concept; it is only a matter of time before we will see the beauty of its design.
Good science need some time. Most people loose patience after a few days of waiting...
Dirk,
ReplyDeleteYou say that ARC520 should not face lots of competition, but what do you think about Myrcludex B, a drug that blocks viral entry and is now in Phase I trials?
Myrcludex B seems to be closer to the existing nucleoside/nucleotide inhibitors in that it mainly aims at inhibiting viral spread/amplification. ARC520 by contrast aims at an immunological functional cure. I believe it is the latter that would really constitute a breakthrough in CHB.
ReplyDeleteI am in Ghana n i need a cure for hepatitis b virus
ReplyDeletethere is another drug by Gilead, GS9620 and one by Replicor called Rep9AC'. Thoughts on those?
ReplyDeleteGs96620 is just a copy of interferon..rep9ac Mabye need 10 yeares to exists..there no such thing as Na at this time..kuwait
ReplyDeleteThere is a great list of hepatitis B treatments at the Hepatitis Foundation's website. Here is the link: http://www.hepb.org/professionals/hbf_drug_watch.htm
ReplyDelete