The ALN-TTR02 phase II results have finally been announced. The results are consistent with the view that
ALN-TTR02 is a strong candidate for becoming RNAi’s first marketed drug. Having said that, the knockdown efficacy
results came short of what one could have expected based on the phase I and
non-human primate results and explain why the company has amended the protocol
to test increased dosing frequencies.
Non-human primate studies show cumulative dosing
Alnylam had long telegraphed the results for the phase II
studies. They stated that we should
expect the clinical results to be essentially the same as what they are seeing with
the drug in non-human primates. I
understand that non-human primates are an immensely insightful model system in
RNAi Therapeutics development. Still, making such strong suggestions just weeks before clinical data release seemed a bit odd in that it risked stealing its own thunder.
Anyhow, the non-human primate studies showed the peak and
the terminal knockdown (terminal knockdown defined as the knockdown just before
repeat dosing) increased with each additional dose administration. Whereas the peak/terminal knockdown in cycle 1
was ~85%/47% at 0.3mg/kg, they were ~90%/58% in cycle 2 and so on. This is what Alnylam refers to as with ‘cumulative’
efficacy.
Unfortunately, this was only partially repeated in humans.
Knockdown not as sustained with repeat dosing
The ALN-TTR02 phase II study represented the first opportunity to rigorously test gene knockdown of a SNALP-delivered RNAi Therapeutic following
repeat dosing. Whereas the phase I study
in healthy volunteers was a one-dose study, this phase II study was a 2-dose
repeat-administration trial in European patients with TTR amyloidosis (FAP
form). In both studies, target gene
knockdown could easily be determined by measuring TTR levels in the blood.
In my analysis of the data, I will stick with slide 10 of Alnylam’s slide set which seems to provide the clearest overview of the data. At the critical
0.3mg/kg dose level, the peak knockdown either remained +/- the same (~80à80% for
once-every-4-weeks) or showed evidence of cumulative activity (~80à88% for
once-every-3-weeks) when comparing the first with the second dose administration. While this looks
quite good, albeit somewhat less than what was observed in the phase I study, slide 5),
the downside surprise comes with the terminal knockdown values. Here, the knockdown for cycle one (day 28;
n=6) was around 75% with tight error bars, but dropped to 60% for cycle two (day
56; n=5) with much more considerable inter-patient variability. The same was observed for the 0.15mg/kg dose
level with ~53% and ~45% reductions after cycle one and two, respectively.
I have no idea where Alnylam is getting the 93% knockdown
from that is so prominently mentioned in the press release. Are they referring to a single patient that
achieved such knockdown?
Once-every-3-weeks to stay on top of competition
You can safely assume that reduced knockdown duration and the fact that the critical phosphorothioate antisense competitor
by ISIS/GSK has a ~70% knockdown have driven Alnylam’s decision to amend the
ongoing phase II study by including once-every-3-week regimens.
Data for the first such cohort was provided. As noted above, once-every-3-weeks showed evidence of cumulative peak knockdown activity thus staying on top of the antisense competition. It is a shame though that the data provided coincidentally ended on day 35, only a week
before the important repeat terminal knockdown point. It is thus not possible to tell whether
diminished terminal knockdown is also an issue for the once-every-3-week
regimen.
Safety findings largely related to route of
administration
Safety findings were only reported at the 0.3mg/kg level (4
events in 9 patients). The infusion-related
reaction and the 'nuisance' side effect of fever/chills are known for SNALP delivery, but do not appear to be prohibitive. Unfortunately, there was a serious adverse
event due to a misplacing of the infusion needle.
New to me is the finding of polyuria (peeing a lot).
Based on this profile, Alnylam will try to lower the amount
of immune suppression given with the drug. Immune suppression is given as a precaution to avoid hypersensitivity reactions seen with SNALP-enabled TKM-ApoB. It seems to me that in introducing
the once-every-3-week regimen, Alnylam wants to dial up the product profile by
lessening the burden of the immune suppression.
The future of ALN-TTR02
Given the high unmet medical need for FAP patients,
ALN-TTR02 should remain on track of making it to the market provided reduced TTR
levels indeed translate into a clinical benefit (a low risk at 80% knockdowns). Some additional warts, however, have been
added to the product profile and my main interest as to the future data will
be how efficacy and safety is maintained not after just two, but after 3,
4, 5 doses and so on.
It would also be good to find an explanation for the diminished knockdown
duration (e.g. some neutralizing antibodies or a peculiarity of TTR gene regulation?). Tekmira, the delivery partner which should receive a $5M milestone on the initiation of ALN-TTR02 phase III
studies at the end of this year, would be an important ally in answering this
question. This could therefore be an
important test of whether the two companies can put aside past differences.
