TY - JOUR
T1 - Global but not gonadotrope-specific disruption of bmal1 abolishes the luteinizing hormone surge without affecting ovulation
AU - Chu, Adrienne
AU - Zhu, Lei
AU - Blum, Ian D.
AU - Mai, Oliver
AU - Leliavski, Alexei
AU - Fahrenkrug, Jan
AU - Oster, Henrik
AU - Boehm, Ulrich
AU - Storch, Kai Florian
PY - 2013/8/1
Y1 - 2013/8/1
N2 - Although there is evidence for a circadian regulation of the preovulatory LH surge, the contributions of individual tissue clocks to this process remain unclear. We studied female mice deficient in the Bmal1 gene (Bmal1 -/-), which is essential for circadian clock function, and found that they lack the proestrous LH surge. However, spontaneous ovulation on the day of estrus was unaffected in these animals. Bmal1-/- females were also deficient in the proestrous FSH surge, which, like the LHsurge, is GnRH-dependent. In the absence of circadian or external timing cues, Bmal1 -/-females continued to cycle in constant darkness albeit with increased cycle length and time spent in estrus. Because pituitary gonadotropes are the source of circulating LH and FSH, we assessed hypophyseal circadian clock function and found that female pituitaries rhythmically express clock components throughout all cycle stages. To determine the role of the gonadotrope clock in the preovulatory LH and FSH surge process, we generated mice that specifically lack BMAL1 in gonadotropes (GBmal1KO). GBmal1KO females exhibited a modest elevation in both proestrous and baseline LH levels across all estrous stages. BMAL1 elimination from gonadotropes also led to increased variability in estrous cycle length, yet GBmal1KO animals were otherwise reproductively normal. Together our data suggest that the intrinsic clock in gonadotropes is dispensable for LH surge regulation but contributes to estrous cycle robustness. Thus, clocks in the suprachiasmatic nucleus or elsewhere must be involved in the generation of the LH surge, which, surprisingly, is not required for spontaneous ovulation.
AB - Although there is evidence for a circadian regulation of the preovulatory LH surge, the contributions of individual tissue clocks to this process remain unclear. We studied female mice deficient in the Bmal1 gene (Bmal1 -/-), which is essential for circadian clock function, and found that they lack the proestrous LH surge. However, spontaneous ovulation on the day of estrus was unaffected in these animals. Bmal1-/- females were also deficient in the proestrous FSH surge, which, like the LHsurge, is GnRH-dependent. In the absence of circadian or external timing cues, Bmal1 -/-females continued to cycle in constant darkness albeit with increased cycle length and time spent in estrus. Because pituitary gonadotropes are the source of circulating LH and FSH, we assessed hypophyseal circadian clock function and found that female pituitaries rhythmically express clock components throughout all cycle stages. To determine the role of the gonadotrope clock in the preovulatory LH and FSH surge process, we generated mice that specifically lack BMAL1 in gonadotropes (GBmal1KO). GBmal1KO females exhibited a modest elevation in both proestrous and baseline LH levels across all estrous stages. BMAL1 elimination from gonadotropes also led to increased variability in estrous cycle length, yet GBmal1KO animals were otherwise reproductively normal. Together our data suggest that the intrinsic clock in gonadotropes is dispensable for LH surge regulation but contributes to estrous cycle robustness. Thus, clocks in the suprachiasmatic nucleus or elsewhere must be involved in the generation of the LH surge, which, surprisingly, is not required for spontaneous ovulation.
UR - http://www.scopus.com/inward/record.url?scp=84880649647&partnerID=8YFLogxK
U2 - 10.1210/en.2013-1080
DO - 10.1210/en.2013-1080
M3 - Journal articles
C2 - 23736292
AN - SCOPUS:84880649647
SN - 0013-7227
VL - 154
SP - 2924
EP - 2935
JO - Endocrinology
JF - Endocrinology
IS - 8
ER -