Arrowhead Pharmaceuticals’ Proprietary Pulmonary TRiM™ Platform Achieves High Levels of Target Gene Knockdown and Long Duration of Effect
Arrowhead Pharmaceuticals (NASDAQ: ARWR) recently announced interim results from its ongoing Phase 1/2 study of ARO-RAGE, an RNA interference therapeutic aimed at treating inflammatory pulmonary diseases like asthma. The study reported a mean maximum reduction of 80% in serum soluble RAGE (sRAGE) levels after two doses, with some patients experiencing reductions of up to 90%. The pharmacologic effect lasted at least 6 weeks following the 92 mg dose. No serious adverse events were reported, indicating promising safety and tolerability. Data from the study will be further presented at the upcoming R&D Day on June 1, 2023. This represents a significant step for Arrowhead's therapeutic pipeline, showcasing the potential of its proprietary TRiM platform.
- Mean maximum reduction of sRAGE by 80% at the 92 mg dose, with some patients showing up to 90% reduction.
- Duration of pharmacologic effect lasted at least 6 weeks after the second dose.
- No serious adverse events reported, indicating promising safety and tolerability.
- None.
- Interim Results from Ongoing ARO-RAGE Phase 1/2 Study Demonstrate up to
- Further Data to be Presented at Upcoming R&D Day
Interim results from ARO-RAGE administration in Part 1 of the ongoing Phase 1/2 study in normal healthy volunteers include:
-
Reductions in soluble RAGE (sRAGE) as measured in serum after two doses on Day 1 and Day 29
-
Mean maximum reduction at 92 mg dose was
80% with a maximum reduction of90% -
Mean maximum reductions at 10 to 44 mg dose levels showed a dose response ranging from
31% to59%
-
Mean maximum reduction at 92 mg dose was
-
Duration of pharmacologic effect persisted for at least 6 weeks after the second administration of the 92 mg dose with further follow up ongoing
- Interim results for this cohort are only available through Day 71
-
Reductions in sRAGE as measured in bronchoalveolar lavage fluid (BALF) at Day 31 after a single dose
-
Mean reduction at 92 mg dose was
75% with a maximum reduction of92% -
Mean reductions at 10 to 44 mg doses ranged from
44% to52%
-
Mean reduction at 92 mg dose was
-
Reductions in serum sRAGE were also observed after a single dose
-
Mean maximum reduction at 92 mg dose was
56% with a maximum reduction of68% -
Mean maximum reductions at 10 to 44 mg dose levels showed a dose response and ranged from
23% to53%
-
Mean maximum reduction at 92 mg dose was
-
The pooled placebo groups experienced a mean sRAGE increase of
8% in BALF and a mean decrease of1% in serum -
Safety and tolerability
- Overall, no patterns of adverse changes in any clinical safety parameters
- No reported serious or severe adverse events
- No dropouts related to drug or related to adverse events
- These results include 4 of 5 escalating dose levels. Data are not yet available for single or multiple dose cohorts at 184 mg, the highest dose being tested
About the Phase 1/2 Study
ARORAGE-1001 (NCT05276570) is a Phase 1/2a, randomized, double-blinded, placebo-controlled study in normal healthy volunteers (NHV), Part 1, and patients with mild-to-moderate asthma, Part 2. The single ascending dose portion of the study includes 5 sequentially enrolled NHV cohorts with escalating single-dose levels. The multiple ascending dose portion of the study includes 5 NHV cohorts and 3 asthma patient cohorts. The objectives of the study include the assessment of safety and tolerability, pharmacokinetics, and pharmacodynamics of ARO-RAGE in NHVs and patients with asthma.
About RAGE
RAGE is implicated in the pathogenesis of numerous inflammatory diseases, including asthma. Reduction of RAGE expression via RNAi is designed to reduce the amount of RAGE protein expressed on pulmonary epithelial cells. Reduced RAGE expression in the pulmonary epithelium may result in reduction of RAGE-dependent inflammatory pathways, leading to decreased exacerbation frequency and improved airflow in patients with asthma
About
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