Analysis of safety from a human clinical trial with pterostilbene

Daniel M Riche, Corey L McEwen, Krista D Riche, Justin J Sherman, Marion R Wofford, David Deschamp, Michael Griswold, Daniel M Riche, Corey L McEwen, Krista D Riche, Justin J Sherman, Marion R Wofford, David Deschamp, Michael Griswold

Abstract

Objectives. The purpose of this trial was to evaluate the safety of long-term pterostilbene administration in humans. Methodology. The trial was a prospective, randomized, double-blind placebo-controlled intervention trial enrolling patients with hypercholesterolemia (defined as a baseline total cholesterol ≥200 mg/dL and/or baseline low-density lipoprotein cholesterol ≥100 mg/dL). Eighty subjects were divided equally into one of four groups: (1) pterostilbene 125 mg twice daily, (2) pterostilbene 50 mg twice daily, (3) pterostilbene 50 mg + grape extract (GE) 100 mg twice daily, and (4) matching placebo twice daily for 6-8 weeks. Safety markers included biochemical and subjective measures. Linear mixed models were used to estimate primary safety measure treatment effects. Results. The majority of patients completed the trial (91.3%). The average age was 54 years. The majority of patients were females (71%) and Caucasians (70%). There were no adverse drug reactions (ADRs) on hepatic, renal, or glucose markers based on biochemical analysis. There were no statistically significant self-reported or major ADRs. Conclusion. Pterostilbene is generally safe for use in humans up to 250 mg/day.

Figures

Figure 1
Figure 1
Primary safety analysis. Interpretation: expected Changes in an Outcome (vertical axis) for any given level of baseline value (horizontal axis) across all four treatment groups. Adjusted for age, gender, and race.

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