OBJECTIVE

To investigate the association of normal fasting plasma glucose (FPG) and the risk for type 2 diabetes.

RESEARCH DESIGN AND METHODS

Data concerning 13,845 subjects, aged 40–69 years, who had their FPG measured at least three times between 1992 and 2008 were extracted from a database. Three FPG groups were defined (51–82, 83–90, and 91–99 mg/dL). A Cox proportional hazards analysis was applied to estimate the risk of incident diabetes adjusted for other risk factors.

RESULTS

During 108,061 person-years of follow-up (8,110 women and 5,735 men), 307 incident cases of type 2 diabetes were found. The final model demonstrated a hazard ratio of 2.03 (95% CI 1.18–3.50) for 91–99 mg/dL and 1.42 (0.42–4.74) for 83–90 mg/dL.

CONCLUSIONS

Our data suggest that FPG between 91 and 99 mg/dL is a strong independent predictor of type 2 diabetes and should be used to identify people to be further investigated and aided with preventive measures.

The prevalence of type 2 diabetes is increasing worldwide (1,2). Prediction methods are a matter of discussion (35). A recent study (6) showed an alteration of normal linear trajectories for fasting and postload plasma glucose concentrations and insulin sensitivity and secretion 3–6 years before diagnosis. Other studies (7,8) showed an increased risk of developing type 2 diabetes among normoglycemic subjects, particularly in those with a fasting plasma glucose (FPG) range of 91–99 mg/dL. Clear information regarding Mediterranean populations is lacking. We investigated whether the higher tertiles of within-normal-range FPG concentrations in a northern Italian population can help identify people at increased risk.

The Italian National Health Service facilitates health controls; on average, northern Italian individuals have one annual blood drawing with eight laboratory tests, including FPG. This induced us to use retrospective outpatient data of the Desio Hospital Laboratory to model an experimental population.

Selection criteria were basal FPG <100 mg/dL at inclusion; at least three additional FPG measurements between 1992 and 2008; and total, HDL, and LDL cholesterol and triglyceride measurements. Furthermore, they did not have any requests for glycated hemoglobin, a limit set to avoid inclusion of those with type 1 and type 2 diabetes.

A total of 13,845 people, aged 40–69 years (9), were considered. These subjects represented 17% of the corresponding stratum (82,000), which is 41% (equivalent to Milan province census data) of the general population (200,000) referring to our laboratory. Demographic and health status information collected through a questionnaire (from 1992 to 2008) was available for a random (one of four consecutive) subset of 3,593 outpatients. We diagnosed type 2 diabetes (study end point) after two FPG concentrations >125 mg/dL (10,11).

Blood samples, collected in lithium-heparin tubes, were analyzed by the enzymatic and colorimetric method (GOD-PAP) within 2 h. Analytical variability was within 2% (12). Data were stratified in groups according to three FPG concentration ranges (51–82, 83–90, and 91–99 mg/dL). Baseline characteristics (mean age, follow-up time, and lipids) across FPG groups were investigated.

The Cochrane-Armitage trend test was used to fit the median of each biomarker in the FPG group to estimate two-sided P values for trends of biomarkers across groups of FPG. A Cox proportional hazards analysis to estimate the hazard ratios and 95% CIs for the development of type 2 diabetes was applied; the values for age, then for triglycerides and total, HDL, and LDL cholesterol were subsequently added. The final Cox model applied to the subset group with health status information was adjusted for sex, age, triglycerides, total cholesterol, BMI, hypertension, family history of type 2 diabetes, smoking, and drinking habits. Statistical analyses were performed (SAS version 8.3; SAS Institute, Inc., Cary, NC).

Data from 8,110 women and 5,735 men with mean (±SD) ages at baseline of 53.8 ± 8.18 and 54.1 ± 8.24 years were observed for an average of 7.9 and 7.4 years (range 1–16 years), respectively. Triglycerides and LDL and total cholesterol increased across FPG groups in both sexes, whereas HDL cholesterol decreased only in women (Table 1).

The longitudinal assessment of blood glucose levels and progression to diabetes is reported in Supplementary Table A1 and Supplementary Fig. A1.

During 108,061 person-years of follow-up, there were 307 incident cases of type 2 diabetes. Incidence was 1.9% for women and 2.7% for men. The incidence of type 2 diabetes increased across FPG groups from 0.75 and 0.58% in the 51–82 mg/dL category to 3.37 and 4.08% in the 91–99 mg/dL category, respectively, for women and men. In these groups, both women and men developed type 2 diabetes at a rate of 4.2 and 5.4 cases per 1,000 person-years, respectively.

Hazard ratios for type 2 diabetes adjusted only for age increased across groups of normal FPG, reaching 2.89 (95% CI 2.18–3.83) for women and 2.87 (2.03–4.04) for men in the highest FPG group. Additional adjustment for lipids did not significantly change risk. Men and women in the 91–99 mg/dL category showed the same hazard ratio (Table 1). The final model (not sex stratified), adjusted for recorded health status information, showed a hazard ratio of 2.03 (1.18–3.50) for the 91–99 mg/dL FPG category and 1.42 (0.42–4.74) for the 86–90 mg/dL category (Table 1).

During the follow-up of 13,845 apparently healthy Mediterranean adults, we found an increased risk of type 2 diabetes across FPG groups within normal range (10,11), suggesting that FPG between 91 and 99 mg/dL is a strong independent predictor of diabetes. This is in agreement with changes in glucose concentrations, insulin sensitivity, and secretion 3–6 years before the diagnosis (6). The increased risk (2.03) in the highest FPG group confirms that of 2.33 observed by Nichols et al. (8). The results indicate that elevated normal FPG may help select people at higher risk for future type 2 diabetes without the addition of strong independent risk factors, such as age, cholesterol, and triglycerides. Model adjustment for hypertension, BMI, and family history attenuates the hazard ratio (from 2.8 to 2.03).

The FPG range of 91–99 mg/dL can therefore be used to select those individuals to be subjected to further investigation with biomarkers of β-cell function, such as 1-h oral glucose tolerance test (OGTT) (5,13). In fact, a threefold decline in insulin sensitivity was demonstrated with increasing FPG levels from 70 to 125 mg/dL (14). The relationship between abnormal FPG and abnormal OGTT to the development of type 2 diabetes still remains an open question because some individuals develop abnormal FPG without developing abnormal OGTT and vice versa (15).

The incidence of diabetes in our study (2.7%) is higher than that in Tirosh et al. (7) (1.6%), perhaps because of the older population (mean age 54.1 vs. 32 years), yet is almost half of that (4.7%) described by Nichols et al. (8), who used less stringent criteria for diagnosis (only one FPG measurement >125 mg/dL with respect to our two) (10).

In conclusion, these results may help physicians to better identify those individuals who need further investigation and preventive measures. They can therefore support public health policy with an inexpensive tool for improving care and reducing costs of future treatment.

No potential conflicts of interest relevant to this article were reported.

P.B. conceived the plan of analysis, researched data, reviewed data analysis, and contributed to discussion. E.L.V. extracted data, performed data analysis, contributed to discussion, and drafted the manuscript. R.F. contributed to the review and revision of the manuscript. G.L. researched data and contributed to data analysis. S.S. and F.C. contributed to data research. P.M. conceived the plan of analysis, reviewed data analysis, contributed to discussion, and revised and approved the manuscript.

1.
Shaw
JE
,
Sicree
RA
,
Zimmet
PZ
.
Global estimates of the prevalence of diabetes for 2010 and 2030
.
Diabetes Res Clin Pract
2010
;
87
:
4
14
[PubMed]
2.
Wild
S
,
Roglic
G
,
Green
A
,
Sicree
R
,
King
H
.
Global prevalence of diabetes: estimates for the year 2000 and projections for 2030
.
Diabetes Care
2004
;
27
:
1047
1053
[PubMed]
3.
Wilson
PWF
,
Meigs
JB
,
Sullivan
L
,
Fox
CS
,
Nathan
DM
,
D’Agostino
RB
 Sr
.
Prediction of incident diabetes mellitus in middle-aged adults: the Framingham Offspring Study
.
Arch Intern Med
2007
;
167
:
1068
1074
[PubMed]
4.
Abdul-Ghani
MA
,
Williams
K
,
DeFronzo
RA
,
Stern
M
.
What is the best predictor of future type 2 diabetes?
Diabetes Care
2007
;
30
:
1544
1548
[PubMed]
5.
Abdul-Ghani
MA
,
Lyssenko
V
,
Tuomi
T
,
DeFronzo
RA
,
Groop
L
.
Fasting versus postload plasma glucose concentration and the risk for future type 2 diabetes: results from the Botnia Study
.
Diabetes Care
2009
;
32
:
281
286
[PubMed]
6.
Tabák
AG
,
Jokela
M
,
Akbaraly
TN
,
Brunner
EJ
,
Kivimäki
M
,
Witte
DR
.
Trajectories of glycaemia, insulin sensitivity, and insulin secretion before diagnosis of type 2 diabetes: an analysis from the Whitehall II study
.
Lancet
2009
;
373
:
2215
2221
[PubMed]
7.
Tirosh
A
,
Shai
I
,
Tekes-Manova
D
, et al
;
Israeli Diabetes Research Group
.
Normal fasting plasma glucose levels and type 2 diabetes in young men
.
N Engl J Med
2005
;
353
:
1454
1462
[PubMed]
8.
Nichols
GA
,
Hillier
TA
,
Brown
JB
.
Normal fasting plasma glucose and risk of type 2 diabetes diagnosis
.
Am J Med
2008
;
121
:
519
524
[PubMed]
9.
Bonora
E
,
Kiechl
S
,
Willeit
J
, et al
;
Bruneck Study
.
Population-based incidence rates and risk factors for type 2 diabetes in white individuals: the Bruneck Study
.
Diabetes
2004
;
53
:
1782
1789
[PubMed]
10.
Genuth
S
,
Alberti
KG
,
Bennett
P
, et al
;
Expert Committee on the Diagnosis and Classification of Diabetes Mellitus
.
Follow-up report on the diagnosis of diabetes mellitus
.
Diabetes Care
2003
;
26
:
3160
3167
[PubMed]
11.
American Diabetes Association
.
Standards of medical care in diabetes: 2007
.
Diabetes Care
2007
;
30
(
Suppl. 1
):
S4
S41
[PubMed]
12.
Sacks
DB
,
Bruns
DE
,
Goldstein
DE
,
Maclaren
NK
,
McDonald
JM
,
Parrott
M
.
Guidelines and recommendations for laboratory analysis in the diagnosis and management of diabetes mellitus
.
Clin Chem
2002
;
48
:
436
472
[PubMed]
13.
Abdul-Ghani
MA
,
DeFronzo
RA
.
Plasma glucose concentration and prediction of future risk of type 2 diabetes
.
Diabetes Care
2009
;
32
(
Suppl. 2
):
S194
S198
[PubMed]
14.
Dagogo-Jack
S
,
Askari
H
,
Tykodi
G
.
Glucoregulatory physiology in subjects with low-normal, high-normal, or impaired fasting glucose
.
J Clin Endocrinol Metab
2009
;
94
:
2031
2036
[PubMed]
15.
Meigs
JB
,
Muller
DC
,
Nathan
DM
,
Blake
DR
,
Andres
R
;
Baltimore Longitudinal Study of Aging
.
The natural history of progression from normal glucose tolerance to type 2 diabetes in the Baltimore Longitudinal Study of Aging
.
Diabetes
2003
;
52
:
1475
1484
[PubMed]
Readers may use this article as long as the work is properly cited, the use is educational and not for profit, and the work is not altered. See http://creativecommons.org/licenses/by-nc-nd/3.0/ for details.

Supplementary data