Increased blood glycohemoglobin A1c levels lead to overestimation of arterial oxygen saturation by pulse oximetry in patients with type 2 diabetes

Glycohemoglobin is produced via a non-enzymatic reaction between the free aldehyde group of glucose or other sugars and the unprotonated form of free amino groups of hemoglobin[1]. Glycosylated hemoglobin A1c (HbAlc) is a stable minor hemoglobin variant separated by charge that is composed primarily but variably of glycohemoglobin. A clinical relationship between blood concentration of HbAlc and status of glycemic control has been elucidated[2], and elevated HbAlc levels represent increased risk of coronary artery disease and poor outcome in diabetic patients[3‐5]. Previous studies have shown that glycosylation alters the structure and function of hemoglobin[6, 7] and tends to shift the oxygen dissociation curve to the left, leading to an increase in hemoglobin-oxygen affinity and a reduction in oxygen delivery to tissues[6, 8, 9]. Pulse oximetry is widely used as a noninvasive tool for continuous monitoring of artery oxygen saturation (SaO₂)[10, 11], but pulse oximeter oxygen saturation (SpO₂) may overestimate arterial blood gases-determined SaO₂ in acute sickle chest syndrome and severe sepsis[12, 13]. So far, its accuracy for titrating fractional inspired oxygen in type 2 diabetic patients with mechanical ventilation or oxygen therapy remains unclear. Given that chronic hyperglycemia accelerates the accumulation of advanced glycation end products (AGE) in the skin collagen[14], which poses specific autofluorescence feature, may emit light by absorbing specific wavelengths light[15], and interfere with the accuracy of pulse oximetry, it is pertinent to examine if elevated blood HbAlc concentrations could result in an overestimation of SaO₂ by SpO₂ with finger probes particularly for type 2 diabetic patients with poor glycemic control.

The present study is the first to demonstrate that despite similar levels of red blood cell 2, 3-DPG, PO₂, PCO₂, pH and body temperature, type 2 diabetic patients with HbA1c > 7% had higher SaO₂ (the mean difference was 1.1%) and bias (1.83 ±0.55%) compared with those with HbA1c ≤ 7%, suggesting that elevated blood HbAlc levels led to an overestimation of SaO₂ by pulse oximetry.

Hypoxemia denotes a condition that is characterized by low oxygen content or percent saturation of hemoglobin with oxygen[13]. Arterial blood gases have been traditionally used to assess the status of oxygenation and to adjust fractional inspired oxygen in patients receiving mechanical ventilation or oxygen therapy[20]. Currently, noninvasive continuous monitoring of SaO₂ with SpO₂ has become the standard care for patients with critical conditions[13, 21], to decrease the likelihood of hypoxemia[22‐25] and to wean mechanical ventilation[10, 11, 26]. In the present study, when comparisons were performed at identical PO₂, SaO₂ was higher in type 2 diabetic patients with HbA1c > 7%, which is likely due to an increased hemoglobin-oxygen affinity. Our results are in line with previous findings that higher blood concentrations of HbA1c significantly reduce oxygen dissociation velocity[27]. Although the exact mechanism remains not fully understood, it may be, at least partly, explained by glycation of multiple ß-chain sites of hemoglobin A molecule, accompanied by increasing -chain glycation at high glycohemoglobin concentrations[28, 29].

The major finding of this study is that in type 2 diabetic patients with poor glycemic control, pulse oximetry overestimated arterial blood gases-determined SaO₂ by a mean of 2.7% when compared with those with HbA1c ≤ 7%. Previous studies showed that older women have higher HbA1c than men, even after controlling for body mass index[30], and accumulation of AGE in human skin collagen is age-dependent[31]. However, both gender distribution and age did not significantly differ between the two groups in the present study, suggesting that the difference between SpO₂ and SaO₂ may be mainly related to HbA1c levels as higher HbA1c levels were associated with great differences (Pearson’s r = 0.307, p < 0.01).

Our findings may be of important clinical relevance. First, falsely high SpO₂ could cause under-diagnosis of hypoxemia in type 2 diabetic patients. Second, because a greater SpO₂ was required to achieve the same arterial blood gases-determined PO₂ for diabetic patients with HbA1c >7% compared with those with HbA1c ≤ 7%, care should be taken in adjusting oxygen supply during mechanical ventilation or oxygen therapy. The reason for a higher SpO₂ than SaO₂ may be partly explained by an extensive accumulation of AGE in the skin collagen in patients with poor glycemic control[14], interfering with transdermal absorption of the specific wavelength light by hemoglobin with finger probes[12, 32]. These observations support a notion that the causes of high bias does include skin effect[33, 34], and when SaO₂ needs to be determined with a high degree of accuracy, arterial blood gases are recommended in type 2 diabetic patients with poor glycemic control.

Elevated blood HbA1c concentrations lead to an overestimation of SaO₂ by SpO₂, suggesting that arterial blood gas analysis may be needed for type 2 diabetic patients with poor glycemic control during the treatment of hypoxemia.