Polypill for the prevention of major CV events in individuals with and without NASH

The PolyIran-Liver trial shows that treatment with polypill resulted in an insignificant reduction in major CV events among the randomized population and a significant reduction among subjects who consented. A similar reduction was observed in participants with and without NASH.

Polypill for prevention of cardiovascular diseases with focus on non-alcoholic steatohepatitis: the PolyIran-Liver trial
Literature - Merat S, Jafari E, Radmard AR et al., - Eur Heart J 2022, https://doi.org/10.1093/eurheartj/ehab919

Introduction and methods

Background

Individuals with fatty liver (non-alcoholic fatty liver disease) and especially those with non-alcoholic steatohepatitis (NASH) and elevated liver enzymes are at higher risk of CVD [1,2] and may benefit from primary prevention. However, these are not much data on primary or secondary prevention in individuals with increased liver enzyme levels [3].

This study was an extension of the PolyIran trial [4], a pragmatic cluster-randomized study in a rural population in Iran in which the effect of a four-component pill including aspirin, atorvastatin, hydrochlorothiazide and either enalapril or valsartan was investigated. Now, the effects of the same polypill on risk of major CV events were studied including participants with increased liver enzyme levels and individuals with fatty liver.

Methods

The PolyIran-Liver study is an open-label, individually randomized controlled trial. 2400 Participants ≥50 years from the Golestan cohort study who were resident of Gonbad city were randomized to receive polypill or no polypill. After randomization, participants were invited for participation and consent was obtained for those accepting (the Zelen design) [5]. Laboratory tests, ultrasonography and liver stiffness measurements were performed. Participants were identified as having presumed NAFLD (pNAFLD) and with elevated ALT levels participants were identified as presumed NASH (pNASH).

The polypill included 81 mg aspirin, 12.5 mg hydrochlorothiazide, 20 mg atorvastatin, and 40 mg valsartan.

Results were analyzed among the originally randomized population (n=2266) and among consenting participants who were eligible for polypill (n=1508).

Participants were visited every 6 months for 5 years.

Outcomes

Primary endpoint was the occurrence of major CV events (MCVE), a composite of fatal MI, sudden death, new-onset heart failure, coronary artery revascularization procedures, fatal and non-fatal stroke or hospitalization for an acute coronary event.

Main results

The randomized population

• MCVE occurred in 138 patients in the intervention group (11.0%) and in 137 in the control group (13.5%) (unadjusted RR 0.83, 95%CI: 0.66-1.03)

The consenting group

• After adjustment for smoking, baseline cholesterol and pre-existing CVD, treatment with the polypill reduced MCVE (adjusted RR 0.61, 95%CI: 0.44-0.83).
• There was also a lower risk of fatal MCVE, non-fatal MCVE and all-cause mortality in the intervention group compared to controls.

Subgroups

• In participants with pNASH, the RR of MCVE was less than half compared to those without pNASH (adjusted RR 0.35, 95%CI:0.17-0.74 vs. adjusted RR 0.73, 95%CI:0.49-1.00), but this difference was not significant.

Secondary outcomes

• In the consenting group, there was no difference between changes in ALT, AST and LSM from baseline to month 30 and 60 between study arms.
• In participants with pNASH, there was a greater reduction in ALT in the intervention group compared to controls at month 30 and 60.
• In the consenting intervention group, there was a significant reduction in SBP at month 30 and 60 compared to controls. In the intervention group, there were greater reduction in all lipid profiles from baseline to month 30 and 60.
• Incidence of adverse events was similar between the two arms. Frequency of adverse events decreased over time except for dyspepsia and cataract.

Conclusion

References

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