1610-P: On the Combined Effect of C-Reactive Protein (CRP) and Serum Amyloid Component P (SAP) on Mortality Risk in Type 2 Diabetes

Abstract

CRP and SAP are the two short, strongly homologous pentraxins produced in response to inflammation. Though their common contribution to innate immunity, they seem to differently affect atherosclerosis and related clinical outcomes. In the specific context of mortality rate i) CRP is a recognized risk biomarker; ii) data on SAP are sparse and conflicting; iii) no data are available on their possibly combined effect. Accordingly, the combined effect of CRP and SAP on mortality risk was investigated in the high-risk subset of patients with type 2 diabetes (T2D). Four cohorts of patients with T2D [i.e., Gargano Heart Study (GHS; n=358; follow-up (f-u)=5±3 years; 81 events); Gargano Mortality Study (n=650; f-u=11±4 years; 190 events); Foggia Mortality Study (n=530; f-u=7±3 years; 146 events) and Pisa Mortality Study (n=986; f-u=13±3 years; 230 events)] were analyzed by Cox proportional hazard models. In the pooled sample, with a total of 2,524 individuals experiencing 647 events, hs-CRP was positively [HR=1.53 (95% CI 1.41-1.66)] whereas SAP was negatively [HR=0.80 (95% CI 0.74-0.86)] associated with all-cause mortality. Similar results were observed on cardiovascular death in GHS: HR (95% CI) being 1.90 (1.48-2.44) and 0.78 (0.61-0.98) for hs-CRP and SAP, respectively. The whole sample was then stratified according to relatively low and high hs-CRP and SAP (< or > the median value), so to obtain four groups: low/high (1), low/low (2), high/high (3), and high/low (4) hs-CRP/SAP levels. As compared to group 1, group 2, 3 and 4 had HRs (95% CIs) of 1.25 (0.96-1.64), 1.80 (1.39-2.33) and 2.40 (1.81-3.17) for all-cause mortality (p for trend=1.1x10-11 or, in a model comprising study sample, age, sex, smoking habit, BMI, HbA1c, diabetes duration and all ongoing treatments, p=4.1x10-8). In conclusion, in patients with T2D, hs-CRP and SAP show a combined effect on all-cause death. Whether their simultaneous use may prove to be useful in predicting mortality in T2D needs further investigation. Disclosure M. Scarale: None. M. Copetti: None. M. Garofolo: None. L. Salvemini: None. S. De Csomo: None. O. Lamacchia: None. G. Penno: None. V. Trischitta: None. C. Menzaghi: None. Funding Italian Ministry of Health (RF-2013-02356459)