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• 1. Bunn HF, Haney DN, Kamin S, Gabbay KH, Gallop PM. The biosynthesis of human hemoglobin A1c: Slow glycosylation of hemoglobin in vivo. J Clin Invest. 1976;57:16529. 2. John WG. Effect of Schiff base (labile fraction) on the measurement of glycated hemoglobin by affinity chromatography. Clin Chem. 1984; 30: 1111-2. 3. Goldstein DE, Peth SB, England JD, et al., Effects of acute changes in blood glucose on HbA1c. Diabetes. 1980; 29: 623-8. 4. The Diabetes Control and Complications Trial Research Group. The effect of intensive treatment of diabetes on the development and progression of long term complications in insulin dependent diabetes mellitus. N Eng J Med. 1993;329: 977 – 86.
• 5. Chandalia HB, Krishnaswamy PR. Glycated hemoglobin. Curr Scie. 2002; 83: 1522 – 32. 6. Kaiser P, Akerboom T, Molnar P, Reinauer H. Modified HPLC-Electrospray Ionization/ Mass Spectrometry Method for HbA1c Based on IFCC Reference Measurement Procedure. Clin Chem. 2008; 54:6 1018–22. 7. Bannon P, Joly JG, Lessard F, Lepage R. Comparison of three methods for the elimination of the labile fraction of the HbA1c. Clin Biochem. 1985; 18: 114 – 7. 8. Yatscoff RW, Tevaarwerk GJM, Clarson CL, Warnock LM. Interference of fetal hemoglobin and labile glycosylated hemoglobin with measurements of glycosylated hemoglobin. Clin Chem. 1983; 29: 543 – 5. 9. Corbe-Guillard E, Jaisson S, Pileire C, Gillery P. Labile hemoglobin A1c: unexpected indicator of preanalytical contraindications. Clin Chem. 2011; 57: 340-6.