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Vol. 55, Issue 6, 1094-1100, June 1999
Department of Molecular Pharmacology, University of
Göttingen, Göttingen, Germany
The immunosuppressants cyclosporin A and FK506 (tacrolimus) can block
the phosphatase calcineurin, thereby inhibiting gene transcription
directed by the cyclic AMP (cAMP)- and calcium-responsive transcription
factor, cAMP response element (CRE)-binding protein, and its binding
site, CRE, in various cell lines. This action is a novel molecular
mechanism of cyclosporin A and FK506 action. Because inhibition of
CREB/CRE-directed transcription by cyclosporin A and FK506 has
previously been observed by using synthetic minienhancers, reporter
fusion genes were constructed to examine the effect of cyclosporin A
and FK506 on the transcriptional activity of CRE-containing natural
promoters. In transient transfection experiments, cyclosporin A and
FK506 inhibited the transcriptional activation by cAMP and the membrane
depolarization of three CRE-containing promoters. However, cyclosporin
A and FK506 failed to inhibit the activation by cAMP of another
promoter, the rat insulin I gene promoter. The lack of
cyclosporin A/FK506 sensitivity is not intrinsic to the insulin CRE
because cyclosporin A and FK506 inhibited the activation by cAMP of the
insulin CRE when isolated and used as a synthetic minienhancer.
Rather, cyclosporin A/FK506 resistance may be conferred by specific
promoter interactions because a mutational analysis of the insulin
promoter revealed that inside this promoter, CRE activity depends on an
adjacent control element. These data show that cyclosporin A and FK506
can inhibit CRE activity when the CRE resides in its natural promoter.
However, the cyclosporin A/FK506 sensitivity depends on the specific
promoter context. The results suggest that cyclosporin A and FK506 may
alter target tissue function through the regulation of a subset of
CRE-containing genes.
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