A combination therapy featuring the PCSK9 inhibitor alirocumab alongside statin treatment achieved dramatic cholesterol reductions in heart transplant recipients, according to results from the CAVIAR trial presented at the American Heart Association's Scientific Sessions 2025 and published simultaneously in Circulation.
The National Institutes of Health-funded study enrolled 114 adults within six months of heart transplantation to evaluate whether adding alirocumab to rosuvastatin could prevent cardiac allograft vasculopathy (CAV), a leading cause of death among transplant recipients that affects up to half of patients within 10 years.
Significant Cholesterol Reduction Achieved
After one year of treatment, participants receiving alirocumab experienced a remarkable drop in LDL cholesterol levels from 72.7 mg/dL at baseline to 31.5 mg/dL, representing a reduction of more than 50%. In contrast, the placebo group showed virtually no change, with levels remaining stable from 69.0 mg/dL to 69.2 mg/dL.
"Our study found treating patients who have had a heart transplant with a more aggressive cholesterol management regimen was safe and lowered their LDL-cholesterol levels significantly," said William F. Fearon, M.D., study author and professor of medicine at Stanford University School of Medicine.
Primary Endpoint Not Met Despite Safety Profile
Despite the substantial cholesterol reduction, the trial did not meet its primary endpoint for plaque progression. No significant difference in coronary artery plaque volume changes was observed between treatment arms (P = .86). Both groups experienced minimal plaque progression overall, and neither group reported major adverse events or notable safety concerns.
The study's design included participants randomized 1:1 to receive either 150 mg of alirocumab or placebo, both administered alongside rosuvastatin. All participants underwent screening procedures at enrollment and one year post-transplant to evaluate blood flow and plaque buildup in coronary arteries.
Clinical Context and Study Limitations
Fearon noted that participants in both arms had lower-than-expected baseline LDL cholesterol levels around 70 mg/dL. "This was lower than we anticipated and lower than previous studies had shown, and I think a reflection of the aggressive statin therapy that our participants received in the study," he explained.
Amanda R. Vest, director of the Cardiac Transplant Program at Tufts Medical Center, emphasized the multifactorial nature of CAV risk. "At the end of the day, the contributions towards development of CAV in our heart transplant patients from the traditional risk factors such as hyperlipidemia may be fairly modest," Vest said. "Although we want to optimize metabolic health to help our patients survive and thrive, maybe a simple lowering of LDL, at least in the short term, is not going to have a huge impact."
Future Research Directions
The researchers acknowledged that because plaque progression was less than expected in both groups and baseline LDL levels were already low in the rosuvastatin-only arm, the study's power to detect differences when adding alirocumab was reduced.
"These results support PCSK9 inhibitors for patients who have high LDL cholesterol levels in conjunction with statin therapy, however, we need more studies testing treatment with PCSK9 inhibitors with longer term follow-up with more participants to confirm if PCSK9s can reduce the development of cardiac allograft vasculopathy," Fearon stated.
The trial, conducted at Stanford Medical Center and Kaiser Permanente in Santa Clara, California, enrolled participants with a mean age of 58 years within eight weeks after heart transplantation, starting in 2019. Both Fearon and Vest highlighted the need for continued exploration of metabolic and inflammatory pathways in reducing post-transplant cardiovascular risk, including potential roles for glucagon-like peptide 1 receptor agonists.
