Elucidating the Mechanism of Absorption of Fast-Acting Insulin Aspart: The Role of Niacinamide

Jonas Kildegaard(Novo Nordisk (Denmark)), Stephen T. Buckley(Novo Nordisk (Denmark)), Rasmus Hjorth Nielsen(Novo Nordisk (Denmark)), Gro Klitgaard Povlsen(Novo Nordisk (Denmark)), Torben Seested(Novo Nordisk (Denmark)), Ulla Ribel(Novo Nordisk (Denmark)), Helle B. Olsen(Novo Nordisk (Denmark)), Svend Ludvigsen(Novo Nordisk (Denmark)), Claus Jeppesen(Novo Nordisk (Denmark)), Hanne H. F. Refsgaard(Novo Nordisk (Denmark)), Kristian Moss Bendtsen(Novo Nordisk (Denmark)), Niels Rode Kristensen(Novo Nordisk (Denmark)), Susanne Hostrup(Novo Nordisk (Denmark)), Jeppe Sturis(Novo Nordisk (Denmark))
Pharmaceutical Research
February 11, 2019
Cited by 77Open Access
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Abstract

PURPOSE: Fast-acting insulin aspart (faster aspart) is a novel formulation of insulin aspart containing two additional excipients: niacinamide, to increase early absorption, and L-arginine, to optimize stability. The aim of this study was to evaluate the impact of niacinamide on insulin aspart absorption and to investigate the mechanism of action underlying the accelerated absorption. METHODS: The impact of niacinamide was assessed in pharmacokinetic analyses in pigs and humans, small angle X-ray scattering experiments, trans-endothelial transport assays, vascular tension measurements, and subcutaneous blood flow imaging. RESULTS: Niacinamide increased the rate of early insulin aspart absorption in pigs, and pharmacokinetic modelling revealed this effect to be most pronounced up to ~30-40 min after injection in humans. Niacinamide increased the relative monomer fraction of insulin aspart by ~35%, and the apparent permeability of insulin aspart across an endothelial cell barrier by ~27%. Niacinamide also induced a concentration-dependent vasorelaxation of porcine arteries, and increased skin perfusion in pigs. CONCLUSION: Niacinamide mediates the acceleration of initial insulin aspart absorption, and the mechanism of action appears to be multifaceted. Niacinamide increases the initial abundance of insulin aspart monomers and transport of insulin aspart after subcutaneous administration, and also mediates a transient, local vasodilatory effect.


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