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The COX-2 inhibitor meloxicam prevents pregnancy when administered as an emergency contraceptive to nonhuman primates

机译:作为非人类灵长类动物的紧急避孕药,COX-2抑制剂美洛昔康可预防妊娠

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Objective Cyclooxygenase-2 (COX-2) inhibitors reduce prostaglandin synthesis and disrupt essential reproductive processes. Ultrasound studies in women demonstrated that oral COX-2 inhibitors can delay or prevent follicle collapse associated with ovulation. The goal of this study was to determine if oral administration of a COX-2 inhibitor can inhibit reproductive function with sufficient efficacy to prevent pregnancy in primates. Study Design The COX-2 inhibitor meloxicam (or vehicle) was administered orally to proven fertile female cynomolgus macaques using one emergency contraceptive model and three monthly contraceptive models. In the emergency contraceptive model, females were bred with a proven fertile male once 2±1 days before ovulation, returned to the females' home cage, and then received 5 days of meloxicam treatment. In the monthly contraceptive models, females were cocaged for breeding with a proven fertile male for a total of 5 days beginning 2±1 days before ovulation. Animals received meloxicam treatment (1) cycle days 5-22, or (2) every day, or (3) each day of the 5-day breeding period. Female were then assessed for pregnancy. Results The pregnancy rate with meloxicam administration using the emergency contraception model was 6.5%, significantly lower than the pregnancy rate of 33.3% when vehicle without meloxicam was administered. Pregnancy rates with the three monthly contraceptive models (75%-100%) were not consistent with preventing pregnancy. Conclusions Oral COX-2 inhibitor administration can prevent pregnancy after a single instance of breeding in primates. While meloxicam may be ineffective for regular contraception, pharmacological inhibition of COX-2 may be an effective method of emergency contraception for women. Implications COX-2 inhibitors can interfere with ovulation, but the contraceptive efficacy of drugs of this class has not been directly tested. This study, conducted in nonhuman primates, is the first to suggest that a COX-2 inhibitor may be effective as an emergency contraceptive.
机译:目的环氧合酶2(COX-2)抑制剂可减少前列腺素的合成并破坏必要的生殖过程。妇女的超声研究表明,口服COX-2抑制剂可延迟或预防与排卵相关的卵泡塌陷。这项研究的目的是确定口服口服COX-2抑制剂是否能有效抑制生殖功能,以防止灵长类动物怀孕。研究设计使用一种紧急避孕模型和三个月度避孕模型,向经证实可育的雌性食蟹猕猴口服COX-2抑制剂美洛昔康(或媒介物)。在紧急避孕模型中,在排卵前2±1天将雌性与经过证实的可育雄性进行繁殖,然后放回雌性家笼中,然后接受美洛昔康治疗5天。在每月的避孕模型中,从排卵前2±1天开始,将雌性与经过证实的可育雄性共育5天。动物接受美洛昔康治疗(5天繁殖期的(1)周期第5-22天,或(2)每天,或(3)每天。然后对女性进行妊娠评估。结果使用紧急避孕模型服用美洛昔康的妊娠率为6.5%,明显低于未使用美洛昔康的媒介物的妊娠率为33.3%。三种月度避孕模型(75%-100%)的怀孕率与预防妊娠不一致。结论口服COX-2抑制剂可防止灵长类动物一次繁殖后怀孕。尽管美洛昔康对常规避孕无效,但COX-2的药理抑制作用可能是女性紧急避孕的有效方法。启示COX-2抑制剂可干扰排卵,但尚未直接测试此类药物的避孕功效。这项在非人类灵长类动物中进行的研究首次表明,COX-2抑制剂可作为紧急避孕药有效。

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