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Alternative-Site Blood Glucose Measurement at the Abdomen

¹ Department of Internal Medicine, Martini Hospital, Groningen, the Netherlands
² Pharmacy, State University, Groningen, the Netherlands

Alternative sites for self-monitoring of blood glucose (SMBG) (e.g., forearm, abdomen, calf, or thigh) are currently being introduced in clinical practice (1). However, blood glucose (BG) concentrations by these methods may differ from those by traditional fingertip pricking (2–4). In an elegant study, Jungheim and Koschinski (3) demonstrated that BG measurements, at the forearm by three commercially available devices, showed a less steep increase after an oral glucose load and a delayed decline after insulin administration. In addition, Ellison et al. (4) showed similar findings, which were less adequately followed at the forearm after a standardized meal.

Given the patients’ preference for alternative-site SMBG, an appreciation mainly based on the avoidance of painful fingertip pricking (1), clinical application will certainly ensue and, thereby, will introduce a new problem, i.e., what glucose value is actually measured and how does this relate to reference values?

We compared capillary BG taken at the fingertip (Glucotrend; Roche Diagnostics, Mannheim, Germany) and the abdominal wall (Freestyle; Disentronic, S’ulzbach, Switzerland) in 12 healthy nondiabetic males (age 25 ± 11 years [mean ± SD], BMI 23.7 ± 3.5 kg/m²). The participants arrived at the outpatient clinic after an overnight fast. They were clamped on their fasting BG by a varying glucose infusion and received an intravenous insulin infusion of 30 mU · kg^-1 · h^-1. After 60 min, the glucose infusion was stopped and BG was allowed to drop to near hypoglycemic levels. Then, after BG was increased by intravenously administered glucose (20% by weight, 0.15 x body weight x 12 [ml]), which was intended to increase BG 12 mmol/l above the actual BG level, the glucose infusion rate was increased. BG was measured every 5 min at the abdomen and fingertip. This was done every minute for 15 min after the sudden increase in BG. The agreement in fingertip and abdominal BG measurements during the gradual decrement and the sudden increment in BG levels was evaluated by repeated measurement ANOVA. Abdominal BG measurement adequately followed the decline in BG measured at the fingertip (see figure). In contrast, abdominal BG concentrations were 10–18% lower than fingertip BG the first 15 min after the rise in BG (P < 0.01, see figure).

Our finding that an increase in BG was less well followed by abdominal BG measurements supports the contention of Jungheim and Kochinsky (3) that alternative-site SMBG differs from classic finger pricking. It illustrates the existence of tissue-specific differences in glucose kinetics, and we previously noted that distribution effects may play a role in abdominal BG measurements (6,7). Obviously, compartment-dependent glucose characteristics should be taken into account with alternative-site SMBG. One solution is adjustment of glucose values generated from alternative sampling sites (forearm, abdomen, thigh, or calf) to arterial or nearby fingertip capillary values, known as the golden reference, and this was actually done in the report of Jungheim and Koschinski (3). Another approach could be that BG measurements are interpreted according to the site-specific characteristics. For instance, hypoglycemic episodes were more protracted in abdominal subcutaneous adipose tissue (8), suggesting that clinically relevant tissue glucopenia may be overlooked by conventional BG measurements. This illustrates that alternative sites may be preferable as they may better reflect tissue glucose homeostasis. Therefore, we challenge the view that fingertip capillary BG is the only reference in denoting BG excursions. We are entering a new era of BG monitoring with the first available glucose sensors that will provide us with a wealth of data on previously unavailable BG excursions, but at the same time confront us with compartment-specific differences in BG concentrations from traditional fingertip pricking.

View larger version (22K): [in this window] [in a new window]   Figure 1— Fingertip and abdominally measured capillary blood glucose concentrations after a gradual decline and sudden increase in blood glucose level. *P < 0.01.

Address correspondence to Department of Internal Medicine, Martini Hospital, PO Box 30033, 9700 RM Groningen, The Netherlands. E-mail: k.hoogenberg{at}mzh.nl.

References

1. Fineberg SE, Bergenstal RM, Bernstein RM, Laffel LM, Schwartz SL: Use of an automated device for alternative site blood glucose monitoring. Diabetes Care 24:1217–1220, 2001[Abstract/Free Full Text]
   
2. Koschinsky T, Jungheim K: Risky delay of hypoglycemia detection by glucose monitoring at the arm (Letter). Diabetes Care 24:1303–1304, 2001[Free Full Text]
   
3. Jungheim K, Koschinsky T: Glucose monitoring at the arm: risky delays of hypoglycemia and hyperglycemia detection. Diabetes Care 25:956–960, 2002[Abstract/Free Full Text]
   
4. Ellison JM, Stegmann JM, Colner SL, Michael RH, Sharma MK, Ervin KR, Horwitz DL: Rapid changes in postprandial blood glucose produce concentration differences at finger, forearm, and thigh sampling sites. Diabetes Care 25:961–964, 2002[Abstract/Free Full Text]
   
5. Jungheim K, Wientjes KJ, Heinemann L, Lodwig V, Koschinsky T, Schoonen AJ: Glucose Monitoring Study Group: subcutaneous continuous glucose monitoring: feasibility of a new microdialysis-based glucose sensor system (Letter). Diabetes Care 24:1696–1697, 2001[Free Full Text]
   
6. Wientjes KJ, Schoonen AJ: Determination of time delay between blood and interstitial adipose tissue glucose concentration change by microdialysis in healthy volunteers. Int J Artif Organs 24:884–889, 2001[Medline]
   
7. Hullegie LM, Lutgers HL, Dullaart RP, Sluiter WJ, Wientjes KJ, Schoonen AJ, Hoogenberg K: Effects of glucose and insulin levels on adipose tissue glucose measurement by microdialysis probes retained for three weeks in type 1 diabetic patients. Neth J Med 57:13–19, 2000[Medline]
   
8. Moberg E, Hagstrom-Toft E, Arner P, Bolinder J: Protracted glucose fall in subcutaneous adipose tissue and skeletal muscle compared with blood during insulin-induced hypoglycaemia. Diabetologia 40:1320–1326, 1997[Medline]
   

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This Article Extract Full Text (PDF) Purchase Article View Shopping Cart Alert me when this article is cited Alert me if a correction is posted Services Email this article to a friend Similar articles in this journal Similar articles in PubMed Alert me to new issues of the journal Download to citation manager Request Permissions Citing Articles Citing Articles via Google Scholar Google Scholar Articles by van der Valk, P. R. Articles by Hoogenberg, K. Search for Related Content PubMed PubMed Citation Articles by van der Valk, P. R. Articles by Hoogenberg, K. Social Bookmarking                What's this?