The penetration enhancement and the lipolytic effects of TAT–GKH, both in in vitro , ex vivo , and in vivo

It was demonstrated that the trans‐activating transcriptional activator (TAT) protein from HIV‐1 could enter cells when added to the surrounding media. TAT peptide chemically attached to various proteins was able to deliver these proteins to various cells and even at high levels in heart and spleen tissues in mice. In this study, the tri‐peptide GKH (glycine–lysine–histidine) derived from the parathyroid hormone, which is known as a lipolytic peptide, was attached to 9‐poly lysine (TAT) to be used as a cosmetic ingredient for eye‐bag care product. When glycerol is released, expressed as the extracellular glycerol concentration (the so‐called lipolysis index), TAT–GKH at 10 −5 m induces a maximal lipolytic effect of approximately 41.5% in epididymal adipocytes isolated from rats, compared with basal lipolysis. In a microdialysis study, TAT–GKH was perfused into epididymal adipose tissues of anaesthetized rats in increasing concentrations in a Ringer solution. The glycerol concentration in each dialysate was measured using an ultra‐sensitive radiometric method. The perfusion of TAT–GKH induced a lipolytic effect. A penetration study showed that TAT–GKH resulted in a sevenfold higher penetration into excised hairless mice skin than GKH. An in vivo study showed that a TAT–GKH containing emulsion had a better effect upon the relative volume reduction of eye bag after 28 days of application on 22 healthy female volunteers than the placebo. It was therefore concluded that TAT–GKH increased skin penetration, which resulted in enhanced lipolytic effects in in vitro, ex vivo and in volume reduction of eye‐bags in in vivo studies.