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痛经女性基于症状的表型:一项潜在类别分析

Symptoms-Based Phenotypes Among Women With Dysmenorrhea: A Latent Class Analysis.

作者信息

Chen Chen X, Ofner Susan, Bakoyannis Giorgos, Kwekkeboom Kristine L, Carpenter Janet S

机构信息

1 Indiana University, Indianapolis, IN, USA.

2 University of Wisconsin-Madison, WI, USA.

出版信息

West J Nurs Res. 2018 Oct;40(10):1452-1468. doi: 10.1177/0193945917731778. Epub 2017 Sep 15.

DOI:10.1177/0193945917731778
PMID:28914180
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5832523/
Abstract

Dysmenorrhea is highly prevalent and may increase women's risk for developing other chronic pain conditions. Although it is highly variable, symptom-based dysmenorrhea phenotypes have not been identified. The aims of the study were to identify symptom-based dysmenorrhea phenotypes and examine their relationships with demographic and clinical characteristics. In a cross-sectional study, 762 women with dysmenorrhea rated severity of 14 dysmenorrhea-related symptoms. Using latent class analysis, we identified three distinctive phenotypes. Women in the "mild localized pain" phenotype ( n = 202, 26.51%) had mild abdominal cramps and dull abdominal pain/discomfort. Women in the "severe localized pain" phenotype ( n = 412, 54.07%) had severe abdominal cramps. Women in the "multiple severe symptoms" phenotype ( n = 148, 19.42%) had severe pain at multiple locations and multiple gastrointestinal symptoms. Race, ethnicity, age, and comorbid chronic pain conditions were significantly associated with phenotypes. Identification of these symptom-based phenotypes provides a foundation for research examining genotype-phenotype associations, etiologic mechanisms, and/or variability in treatment responses.

摘要

痛经非常普遍,可能会增加女性患其他慢性疼痛疾病的风险。尽管痛经症状差异很大,但基于症状的痛经表型尚未得到明确。本研究的目的是确定基于症状的痛经表型,并研究它们与人口统计学和临床特征之间的关系。在一项横断面研究中,762名痛经女性对14种与痛经相关的症状的严重程度进行了评分。通过潜在类别分析,我们确定了三种不同的表型。“轻度局部疼痛”表型的女性(n = 202,26.51%)有轻度腹部绞痛和腹部隐痛/不适。“重度局部疼痛”表型的女性(n = 412,54.07%)有严重腹部绞痛。“多种严重症状”表型的女性(n = 148,19.42%)在多个部位有严重疼痛和多种胃肠道症状。种族、民族、年龄和合并的慢性疼痛疾病与表型显著相关。识别这些基于症状的表型为研究基因型-表型关联、病因机制和/或治疗反应的变异性提供了基础。

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