绝经前妇女黄体生成素可刺激子宫平滑肌瘤的发展。

Donna D Baird, James S Kesner, David B Dunson
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引用次数: 31

摘要

目的:人绒毛膜促性腺激素(hCG)对子宫平滑肌和子宫平滑肌瘤组织有体外增殖作用。我们假设黄体生成素(LH)会通过激活LH/hCG受体而产生同样的效果,因此,基础LH水平较高的绝经前妇女更容易患平滑肌瘤。方法:随机选择35 ~ 49岁的预付费健康计划妇女进行盆腔超声平滑肌瘤筛查。在月经周期的前5天或最后5天收集尿液样本,通过免疫荧光法分析LH,并校正肌酐浓度(n = 523)。采用Logistic回归和贝叶斯分析来评估LH与平滑肌瘤存在和大小的关系,调整年龄和其他危险因素。结果:LH水平较高的女性患平滑肌瘤的可能性更大(与较低水平的女性相比,第二和第三阶段的校正优势比分别为1.7和2.0;95%置信区间分别为1.0 ~ 2.7和1.2 ~ 3.4)。对于大的平滑肌瘤,这种关联更强。设计用于单独估计LH对肿瘤发生和肿瘤生长影响的贝叶斯分析显示,LH显著加速了肿瘤发生,但几乎没有证据表明LH对肿瘤生长有影响。年龄是平滑肌瘤的独立危险因素,但在logistic模型中纳入LH并不影响年龄。结论:正如假设的那样,LH较高的女性更容易患平滑肌瘤,但这并不能解释在围绝经期平滑肌瘤的年龄相关增加。确定黄体生成素是致病的还是易感性的标志还需要进一步的研究。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Luteinizing hormone in premenopausal women may stimulate uterine leiomyomata development.

Objective: Human chorionic gonadotropin (hCG) has proliferative effects on uterine smooth muscle and leiomyoma tissue in vitro. We hypothesized that luteinizing hormone (LH) would have the same effect by activating the LH/hCG receptor, and it would follow that premenopausal women with higher basal LH levels would be more likely to have leiomyomata.

Methods: Randomly selected women, aged 35 to 49 years, from a prepaid health plan were screened for leiomyomata with pelvic ultrasound. Urine samples collected during the first or last 5 days of the menstrual cycle were analyzed for LH by immunofluorometric assay, and concentrations were corrected for creatinine (n = 523). Logistic regression and Bayes analyses were used to evaluate the association of LH with presence and size of leiomyomata, adjusting for age, and other risk factors.

Results: Women with higher LH were more likely to have leiomyomata (adjusted odds ratios for second and third tertiles were 1.7 and 2.0 compared with lower tertile; 95% confidence intervals, 1.0 to 2.7 and 1.2 to 3.4, respectively). The association was stronger for large leiomyomata. Bayes analyses designed to estimate LH effects on tumor onset separately from tumor growth showed significantly accelerated tumor onset but little evidence of effects on tumor growth. Age, an independent risk factor for leiomyomata, was not affected by inclusion of LH in the logistic models.

Conclusions: As hypothesized, women with higher LH were more likely to have leiomyomata, but this did not explain the age-related increase in leiomyomata during perimenopausal ages. Determining whether LH is causal or a marker for susceptibility will require further research.

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