Ud. Dincer et al., The effect of diabetes on expression of beta(1)-, beta(2)-, and beta(3)-adrenoreceptor in rat hearts, DIABETES, 50(2), 2001, pp. 455-461
Diabetic hearts exhibit decreased responsiveness to stimulation by beta -ad
renoreceptor (beta -AR) agonists. This decrease in activity may be due to c
hanges in expression and/or signaling of beta -AR. Recently we showed that
right atrial strips from 14-week streptozotocin (STZ)induced diabetic rat h
earts exhibit decreased responsiveness to beta (1)-AR agonist stimulation,
but not to beta (2)-AR agonist. In the present study, we investigated the e
ffects of long-term diabetes on the expression of cardiac beta (1)-, beta (
2)-, and beta (3)-ARs and looked at whether these changes could be restored
with insulin treatment. Using reverse transcription-polymerase chain react
ion (RT-PCR), PAGE, and Western blot analysis, we found that beta (1)-AR mR
NA and protein levels decreased by 34.9 +/- 5.8 and 44.4 +/- 5.8%, respecti
vely, in 14 week-STZ-treated diabetic rat hearts when compared with age-mat
ched controls. On the other hand, mRNA levels encoding beta (2)- and beta (
3)-ARs increased by 72.5 +/- 16.6 and 97.3 +/- 26.1%, respectively. Althoug
h the latter translated into a proportional increase in beta (3)-AR protein
levels (100.0 +/- 17.0%), beta (2)-AR protein levels decreased to 82.6 +/-
1.1% of control. Insulin treatment for 2 weeks, after 12 weeks of untreate
d diabetes, partially restored beta (1)-AR mRNA and protein levels to 60.1
+/- 8.4 and 83.2 +/- 5.0%, respectively, of control. Although insulin treat
ment minimally attenuated the rise in mRNA levels encoding beta (2)- and be
ta (3)-ARs, the steady-state levels of these proteins returned to near cont
rol values. These data suggest that the decreased responsiveness of diabeti
c hearts to stimulation of beta -AR agonists may be due to a decrease in be
ta (1)-AR and an increase beta (3)-AR expression.