Cytokeratin-18 is an essential component of the cytoskeleton of epithelial  cells (including hepatocytes). Serum concentrations of cytokeratin-18 (tissue  polypeptide-specific antigen [TPS]) are used as a marker of epithelial  neoplasms. Here, we investigated the potential interaction between alcohol and  obesity in relation to serum TPS concentrations.
 
 Alcohol consumption, body mass index, and components of  metabolic syndrome were measured in a random sample (n = 420) of the  adult population (aged 18 to 92 years, 45% men) from a single municipality.  Regular alcohol intake of >20 g/d (women) or >30 g/d (men) was considered  risky drinking. Serum TPS was measured with a commercial immunoassay.
 
 Risky drinking was associated with increased serum  concentrations of TPS, which was particularly evident among obese individuals.  Among individuals without risky drinking, TPS concentrations were similar for  all levels of body mass. Conversely, among risky drinkers, serum TPS  concentrations increased in parallel with body mass  (p = 0.002). The odds ratio of a high (>100 U/l) TPS  concentration for the combination of risky drinking and obesity was greater than  the additive effect of the 2 separate factors, after adjusting for age and sex.  A similar interaction was observed between risky drinking and abdominal  adiposity, a major component of the metabolic syndrome. Serum TPS concentrations  were correlated with markers of liver damage. Serum TPS was not superior to  standard markers (gamma-glutamyl transferase and red blood cell mean volume) for  the detection of risky drinking.
 There is a synergism between risky alcohol consumption  and common metabolic disorders (particularly obesity) in relation to serum  concentrations of cytokeratin-18 (TPS), which probably reflect liver  disease.
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Request Reprint E-Mail: arturo.gonzalez.quintela@usc.es

 
