Twice-yearly inclisiran reduces LDL in ASCVD, FH
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Inclisiran, an investigational cholesterol-lowering therapy, reduced LDL in high-risk patients with atherosclerotic CVD and in those with heterozygous familial hypercholesterolemia, or FH, according to data from the ORION-10 and ORION-9 trials, respectively.
“Inclisiran is a small interfering double-stranded RNA which harnesses natural process of RNA interferences in the liver,” Frederick J. Raal, MBBCh, PhD, FCP(SA), FRCPC, MRCP, professor at University of the Witwatersrand, Johannesburg, said during the presentation.
ORION-10
In this phase 3 trial, twice-yearly injections of inclisiran sodium 300 mg (The Medicines Company) resulted in placebo-adjusted LDL reductions of 58% at 17 months (P < .0001) and time-averaged placebo-adjusted LDL reductions of 56% from month 3 to 18 (P < .0001), R. Scott Wright, MD, professor of medicine and consultant in cardiology at Mayo Clinic in Rochester, said during the presentation.
“Inclisiran potentially offers a novel new treatment for LDL,” Wright said. “Assuming FDA approval, twice-yearly administration coincides with typical twice-year patient visits with health care providers.”
The new data also demonstrate safety, with a profile similar to placebo. The proportion of patients who experienced at least one serious treatment-emergent adverse event was 26.3% in the inclisiran group vs. 22.4% in the placebo group. The incidences of all-cause death (1.4% vs. 1.5%) and new, worsening or recurrent malignancies (3.3% vs. 3.3%) were similar between the inclisiran and placebo groups. There were also no adverse changes in laboratory markers.
Events including reaction, erythema, rash, pruritus and hypersensitivity occurred in 2.6% of patients assigned inclisiran. Events were predominantly mild and none were persistent, Wright said. Halfway through the trial, the injection switched from a vial and syringe to a prefilled syringe; this resulted in numerically lower injection-site pain, he said.
ORION-10 enrolled 1,561 patients with ASCVD and elevated LDL despite maximum tolerated doses of LDL-lowering therapies. Each patient received inclisiran 300 mg administered as a subcutaneous injection initially, again at 3 months and then every 6 months thereafter. Most patients in this study were taking inclisiran or placebo in addition to existing lipid-lowering therapy with a maximally tolerated statin, with or without ezetimibe.
ORION-9
Researchers analyzed data from 482 patients with heterozygous FH who were diagnosed by phenotype or genotype with an LDL greater than 100 mg/dL on a low-fat diet and maximally tolerated statin doses.
Patients were assigned 300 mg of inclisiran subcutaneously every 6 months (n = 242; median age, 56 years; 46% men; baseline LDL, 155 mg/dL) or placebo (n = 240; median age, 56 years; 48% men; baseline LDL, 151 mg/dL) for 18 months. Both treatments were on top of maximally tolerated statins.
A genetic subanalysis of 432 patients was also conducted, during which next-generation sequencing was performed. LDL receptor variants were identified and classified.
The primary effectiveness endpoint was the percent of LDL change vs. placebo at 510 days and an average between 90 and 540 days. Secondary effectiveness endpoints included LDL change over time and changes in PCSK9 and other lipids. Safety and tolerability endpoints were defined as treatment-emergent adverse events and laboratory parameters.
Patients assigned inclisiran had highly significant reductions in LDL compared with placebo at 510 days (difference = –50%; P < .0001) and in a time-averaged analysis between 90 and 540 days (difference = –45%; P < .0001). Robust responses were seen in all genotypes.
“The reduction in those that were found to have an LDL variant was very similar to those with an ApoB variant,” Raal said during the presentation. “Interestingly, the patients that had two variants also had a robust reduction in LDL cholesterol. The single patients with a PCSK9 gain-of-function mutation had a greater than 90% reduction in LDL cholesterol, which is in keeping with the mechanism of action of inclisiran.”
The safety profile of inclisiran was similar to placebo except for adverse events at the injection site, which occurred in 13.3% of patients assigned inclisiran vs. 0% in those assigned placebo. Injection-site reactions were often minor or moderate. There was no evidence of liver, kidney, muscle or platelet toxicity and no difference in serious adverse events in the inclisiran group vs. the placebo group.
“Inclisiran shows potential to address the unmet need of high-risk FH patients,” Raal said during the presentation. – by Katie Kalvaitis and Darlene Dobkowski
- References:
- Raal FJ, et al. Late Breaking Science VI: New Frontiers in Lipid Therapy.
- Wright RS, et al. Late Breaking Science I. Outside the Box: New Approaches to CVD Risk Reduction.
Disclosures: The trials were sponsored by The Medicines Company. Raal reports he received honoraria from Amgen, Sanofi/Regeneron and The Medicines Company. Wright reports he receives honoraria from Boehringer Ingelheim and research support from AstraZeneca and The Medicines Company.