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POS1445 RETINOL BINDING PROTEIN 4 AS AN ACUTE PHASE REACTANT AND BIOMARKER IN PATIENTS WITH FAMILIAL MEDITERRANEAN FEVER AND AMYLOIDOSIS COMPARED TO INFECTIONS

医学 血清淀粉样蛋白A 淀粉样变性 家族性地中海热 急性期蛋白 转甲状腺素 内科学 血清淀粉样蛋白A C反应蛋白 淀粉样变性 胃肠病学 视黄醇结合蛋白 队列 生物标志物 淀粉样变性 淀粉样蛋白(真菌学) 免疫学
作者
Nevzat Koca,Rabia Deniz,M. Erdugan,Y. Yalçınkaya,Bahar Artım-Esen,M. L. Ocal,Murat İnanç,Ahmet Gül
出处
期刊:Annals of the Rheumatic Diseases [BMJ]
卷期号:80 (Suppl 1): 1006.2-1007
标识
DOI:10.1136/annrheumdis-2021-eular.3692
摘要

Background: Retinol binding protein 4 (RBP4) is a plasma retinol transporter that transports retinol from liver to periphery. RBP4 has been studied as a biomarker in metabolic and neoplastic conditions, however its association with inflammation is not clear. Serum amyloid A (SAA), another retinol binding protein, has been known as a sensitive biomarker of inflammation in familial Mediterranean fever (FMF) and other autoinflammatory disorders. C-reactive protein (CRP), erythrocyte sedimentation rate (ESR) and SAA are commonly used as acute phase reactants, but they are not successful in differentiating non-infectious inflammatory conditions from infections. Objectives: We aimed to evaluate the potential of serum RBP4 as a biomarker of acute phase response and to determine its performance in differentiation of inflammation of patients with FMF and AA amyloidosis from infections. Methods: A total of 169 participants in 5 groups, consisting of FMF (n = 60), FMF with AA amyloidosis (n = 58), non-FMF AA amyloidosis (n = 23), infections (n = 10, 3 pneumonia, 3 sepsis, 1 pyelonephritis, 1 fungal infection, 1 cellulitis, 1 disseminated zoster), and healthy controls (HC) (n = 18), were included and evaluated cross sectionally. Hemogram and serum CRP, ESR, SAA, ferritin, creatinine, AST, ALT, albumin levels were recorded from the patient charts. FMF and FMF + amyloidosis patients were evaluated during attack-free period. Serum RBP4 levels were investigated by ELISA (Elabscience, USA). Mean values and relative changes compared to healthy controls were evaluated for SAA, CRP, RBP4 levels in all groups. Results: Serum RBP4 level was found to be higher in FMF group compared to the patients with infection (p = 0.002) and HC (p <0.001) as well as in patients with amyloidosis. Compared to HC, 47%, 28% and 27% increase was observed in mean RBP4 levels in FMF, FMF + amyloidosis and non-FMF amyloidosis patients, despite no significant change in patients with infections. However, CRP and SAA elevations were much more prominent in patients with infections (58 and 134 times, respectively) compared to the patients with FMF (13 and 35 times, respectively), FMF + amyloidosis and non-FMF amyloidosis (Table 1). There was no significant difference in RBP4 levels between FMF, FMF-amyloidosis and non-FMF amyloidosis groups. CRP, ESR, ferritin and SAA levels were higher in the infection group compared to HCs. Table 1. Demographic features and laboratory findings of the participants Variables FMF (n=60) FMF- Amyloidosis (n=58) Non-FMF-AA Amyloidosis (n=23) Infection (n=10) Healthy control (n=18) Female/Male 46/14 33/25 8/15 3/7 8/10 Age (SD)* 38±13 (18-74) 43±11 (21-69) 53±13 65±15 33±9 Creatinine (mg/dL)* 0,8±0,2 1,7±1,7 2,0±1,6 1,7±1,0 0,7±0,2 Albumin(mg/dL)* 4,7±0,4 4,3±0,6 3,3±0,9 3,0±0,9 4,8±0,2 Ferritin (ng/mL)* 70±94 245±315 139±168 554±38 83±72 RBP4 (ng/mL)* 772±183 671±214 666±256 512±204 524±117 RBP4 (median ) 770 (434-1142) 653 (227-1259) 645 (331-1214) 487 (226-876) 498 (566-738) CRP (mg/L)* 16±47,1 12,8±32,8 25,7±36,4 69±36,8 1,2±1,2 SAA (mg/dL)* 10,3±31,4 5,0±13,9 7,1±14,1 40,2±18,5 0,3±0,1 ESR* 15±13 19±16 41±29 45±42 7±5 Relative RBP4 increase 1,47±0,35 1,28±0,41 1,27±0,49 0,98±0,39 Relative CRP increase 13,4±39,2 10,6±27,3 21,4±30,3 57,7±30,6 Relative SAA increase 34,5±104,8 16,0±45,7 23,7±47,1 133,9±61,7 *mean, RBP4 (Retinol Binding Protein 4), C-Reactive Protein (CRP), Erythrocyte Sedimentation Rate (ESR), Serum Amyloid A (SAA). Conclusion: This preliminary study showed that RBP4 levels may be increased about 1.5 times in FMF and to lesser extent in AA amyloidosis patients despite no significant change during acute phase response of different infections. Patients with infections show strong CRP and SAA response, and the differential response of RBP4 in FMF patients warrants further analysis in larger group of patients with different clinical characteristics. Disclosure of Interests: None declared

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