Possible Involvement of Microglia Containing Cyclooxygenase‐1 in the Accumulation of Gonadotrophin‐Releasing Hormone in the Preoptic Area in Female Rats

Prostaglandins (PGs), especially PGE 2 , are involved in the hypothalamic control of gonadotrophin‐releasing hormone (GnRH) release, acting at least in part on the terminal of GnRH axons in the median eminence. The present study aimed: (i) to clarify the role of PG(s) in regulating GnRH cell function at the level of the perikarya in the preoptic area; (ii) to determine the cyclooxygenase (COX) isozyme responsible for producing PG(s) that regulates GnRH perikarya; and (iii) to identify cell types that contain the responsible COX isozyme in female rats. A surge of luteinising hormone (LH) secretion was induced by oestrogen and progesterone in ovariectomised rats. Treatment of the rat before the LH surge with indomethacin, a nonselective COX inhibitor, or NS‐398, a selective COX‐2 inhibitor, did not interfere with the surge. However, treatment with indomethacin or flurbiprofen, a selective COX‐1 inhibitor, significantly reduced the number of GnRH‐immunoreactive cells in the preoptic area at the time of peak LH secretion during the surge. NS‐398 did not affect the GnRH immunoreactivity. Double‐labelled immunofluorescent histochemistry revealed COX‐1 immunoreactivity in the vicinity of, but not within, GnRH containing neurones in the preoptic area. COX‐2 immunoreactivity was not found in the same area. The COX‐1 immunoreactivity was almost entirely localised in microglia in the preoptic area, but not in neurones or astrocytes. These results suggest that microglia in the preoptic area containing COX‐1 are responsible for producing PG(s), which, in turn, facilitates the accumulation of GnRH during the gonadotrophin surge in female rats.