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Periodontitis increases vascular cyclooxygenase‐2: potential effect on vascular tone
Author(s) -
Mendes R. T.,
Sordi R.,
Olchanheski L. R.,
Machado W. M.,
Stanczyk C. P.,
Assreuy J.,
Santos F. A.,
Fernandes D.
Publication year - 2014
Publication title -
journal of periodontal research
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 1.31
H-Index - 83
eISSN - 1600-0765
pISSN - 0022-3484
DOI - 10.1111/jre.12083
Subject(s) - periodontitis , medicine , etoricoxib , cyclooxygenase , nitric oxide , inflammation , vasodilation , pathology , endocrinology , chemistry , biochemistry , enzyme
Background and objective It has been demonstrated that periodontitis induces a systemic inflammation, which may impair endothelial function. Cyclooxygenase‐2 ( COX ‐2) is an important enzyme in the inflammatory process and is responsible for prostacyclin production. We hypothesised that in periodontitis, an increase in vascular COX ‐2 expression may occur, which in turn may have a role in vascular homeostasis. Thus, we evaluated the vascular effects of COX ‐2 inhibition in an experimental rat model of periodontitis. Material and Methods Experimental periodontitis was induced in rats by placing a cotton ligature around the cervix of both sides of the mandibular first molars and maxillary second molars. Sham‐operated rats had the ligature removed immediately after the procedure. Mesenteric vessels were obtained for the study of COX ‐2 expression, and blood samples were collected for nitric oxide quantification. In another set of experiments, animals received etoricoxib (10 mg/kg/d, v.o.) or vehicle, and alveolar bone loss and cardiovascular parameters were evaluated. Results We observed an increase in COX ‐2 expression in mesenteric vessels harvested from animals with periodontitis, which was accompanied by a reduction in nitric oxide content. Etoricoxib treatment impaired the endothelium‐dependent reduction in blood pressure in rats with periodontitis. Conclusion Periodontitis increases vascular COX ‐2 expression, which is important in the maintenance of vascular homeostasis in this model. Despite the limitations of an animal study, these findings may have important implications regarding the safety of using selective COX ‐2 inhibitors in patients with periodontitis.

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