瘢痕疙瘩、增生性疤痕和子宫肌瘤的发展:一项对黑人和非裔美国妇女的前瞻性超声研究

Christine R. Langton Ph. D. , Meghan Gerety B.A. , Quaker E. Harmon M.D., Ph. D. , Donna D. Baird Ph. D.
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引用次数: 0

摘要

目的探讨瘢痕疙瘩、增生性瘢痕与子宫肌瘤发病率及生长的关系。瘢痕疙瘩和肌瘤都是纤维增生性疾病,据报道黑人比白人更普遍,它们具有相似的纤维化组织结构,包括细胞外基质组成、基因表达和蛋白质谱。我们假设有瘢痕瘤病史的女性会有更大的子宫肌瘤发展。设计一项前瞻性社区队列研究(2010-2012年入组),在5年内进行4次研究访问,进行标准化超声检查,检测和测量直径≥0.5 cm的肌瘤,评估瘢痕疙瘩和增生性疤痕的病史,并更新协变量。设置底特律,密歇根州地区。患者:共有1610名女性,年龄23-35岁,自认为是黑人和/或非裔美国人,以前没有子宫肌瘤的临床诊断。暴露(s)瘢痕疙瘩(生长在原始损伤边缘以外的凸起疤痕)和肥厚性疤痕(生长在原始损伤范围内的凸起疤痕)。由于很难区分瘢痕疙瘩和肥厚性疤痕,我们分别研究了瘢痕疙瘩的历史、瘢痕疙瘩或肥厚性疤痕(任何异常疤痕)的历史以及它们与肌瘤发病率和生长的关系。主要结局指标:采用Cox比例风险回归评估肌瘤发生率(入组时无肌瘤超声检查后出现新肌瘤)。使用线性混合模型评估肌瘤生长。每18个月的日志量变化的估计值被转换为疤痕与无疤痕的估计百分比差异。根据随时间变化的人口统计学、生殖学和人体测量学因素对发病率和生长模型进行了调整。结果:在1230名无肌瘤的参与者中,199名(16%)报告曾患过瘢痕疙瘩,578名(47%)报告有瘢痕疙瘩或增生性疤痕,293名(24%)发生过突发性肌瘤。瘢痕疙瘩(校正风险比= 1.04;95%可信区间:0.77,1.40)和任何异常疤痕(校正风险比= 1.10;95%可信区间:0.88,1.38)与肌瘤发病率相关。结论(5)尽管分子相似,自我报告的瘢痕疙瘩和增生性疤痕与肌瘤的发展没有关联。未来的研究可能受益于皮肤科医生确认的瘢痕疙瘩或增生性疤痕的检查;然而,我们的数据表明,这两种类型的纤维化情况几乎没有共同的易感性。
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Keloids, hypertrophic scars, and uterine fibroid development: a prospective ultrasound study of Black and African American women

Objective

To examine the association between keloids, hypertrophic scars, and uterine fibroid incidence as well as growth. Both keloids and fibroids are fibroproliferative conditions that have been reported to be more prevalent among Blacks than Whites, and they share similar fibrotic tissue structures, including extracellular matrix composition, gene expression, and protein profiles. We hypothesized that women with a history of keloids would have greater uterine fibroid development.

Design

A prospective community cohort study (enrollment 2010–2012) with 4 study visits over 5 years to conduct standardized ultrasounds to detect and measure fibroids ≥0.5 cm in diameter, assess the history of keloid and hypertrophic scars, and update covariates.

Setting

Detroit, Michigan area.

Patients

A total of 1,610 self-identified Black and/or African American women aged 23–35 years at enrollment without a previous clinical diagnosis of fibroids.

Exposure(s)

Keloids (raised scars that grow beyond the margins of the original injury) and hypertrophic scars (raised scars that stay within the bounds of the original injury). Because of the difficulties in distinguishing keloids and hypertrophic scars, we separately examined the history of keloids and the history of either keloids or hypertrophic scars (any abnormal scarring) and their associations with fibroid incidence and growth.

Main Outcome Measure(s)

Fibroid incidence (new fibroid after a fibroid-free ultrasound at enrollment) was assessed using Cox proportional-hazards regression. Fibroid growth was assessed using linear mixed models. The estimates for the change in log volume per 18 months were converted to the estimated percentage difference in volume for scarring vs. no-scarring. Both incidence and growth models were adjusted for time-varying demographic, reproductive, and anthropometric factors.

Result(s)

Of the 1,230 fibroid-free participants, 199 (16%) reported ever having keloids, 578 (47%) reported keloids or hypertrophic scars, and 293 (24%) developed incident fibroids. Neither keloids (adjusted hazard ratio = 1.04; 95% confidence interval: 0.77, 1.40) nor any abnormal scarring (adjusted hazard ratio = 1.10; 95% confidence interval: 0.88, 1.38) were associated with fibroid incidence. Fibroid growth differed little by scarring status.

Conclusion(s)

Despite molecular similarities, self-reported keloid and hypertrophic scars did not show an association with fibroid development. Future research may benefit from the examination of dermatologist-confirmed keloids or hypertrophic scars; however, our data suggest little shared susceptibility for these 2 types of fibrotic conditions.

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来源期刊
F&S science
F&S science Endocrinology, Diabetes and Metabolism, Obstetrics, Gynecology and Women's Health, Urology
CiteScore
2.00
自引率
0.00%
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0
审稿时长
51 days
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