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Diabetes, Vol 40, Issue 1 44-51, Copyright © 1991 by American Diabetes Association
Age as independent determinant of glucose tolerance
H Shimokata, DC Muller, JL Fleg, J Sorkin, AW Ziemba and R Andres
Laboratory of Clinical Physiology, National Institute on Aging, National Institutes of Health, Baltimore, MD 21224.
It has been proposed that the decline in glucose tolerance with age is not
a primary aging effect but is secondary to a combination of other
age-associated characteristics, i.e., disease, medication, obesity, central
and upper-body fat deposition, and inactivity. To test this hypothesis, we
first eliminated from analysis the Baltimore Longitudinal Study of Aging
participants with identifiable diseases or medications known to influence
glucose tolerance. Seven hundred forty-three men and women, aged 17-92 yr,
remained for analysis. As indices of fatness, body mass index and percent
body fat were determined. As indices of body fat distribution, waist-hip
ratio and subscapular triceps skin-fold ratio were calculated. As indices
of fitness, physical activity level, determined by detailed questionnaire,
and maximum 02 consumption were calculated. We tested whether the effect of
age on glucose tolerance remains when data were adjusted for fatness,
fitness, and fat distribution; 2-h glucose values were 6.61, 6.78, and 7.83
mM for young (17-39 yr), middle-aged (40-59 yr), and old (60-92 yr) men and
6.22, 6.22, and 7.28 mM for the three groups of women, respectively. The
differences between the young and middle-aged groups were not significant,
but the old groups had significantly higher values than young or
middle-aged groups. Fatness, fitness, and fat distribution can account for
the decline in glucose tolerance from the young adult to the middle-aged
years. However, age remains a significant determinant of the further
decline in glucose tolerance of healthy old subjects.

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Copyright © 1991 by the American Diabetes Association.
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