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Data driven attempt to create a clinical algorithm for identification of women with rheumatoid arthritis at high risk of osteoporosis

机译:数据驱动的尝试以创建一种临床算法来识别骨质疏松症高风险的类风湿关节炎妇女

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摘要

OBJECTIVES—To examine relations between osteoporosis and low bone mass and demographic and clinical variables in patients with rheumatoid arthritis (RA), in an attempt to develop a data driven clinical tool for identification of patients at high risk of osteoporosis.
METHODS—All patients were recruited from a county based register and were examined cross sectionally with a variety of clinical and health status measures as well as bone density measures (anteroposterior spine L2-4, total hip, and femoral neck). Associations between osteoporosis (T score ⩽−2.5SD) and low bone mass (T score ⩽−1SD), on the one hand, and demographic and clinical measures, on the other, were examined bivariately and by logistic regression analyses.
RESULTS—394 patients with a mean age of 54.8 years were examined. The percentages having osteoporosis/low bone mass were 16.8/45.8, 14.7/54.5 and 14.7/55.5 in spine L2-4, total hip, and femoral neck, respectively. Osteoporosis and low bone mass were bivariately related to age, body mass index (BMI), disease duration, disease process measures, presence of deformed joints, physical disability, current use of corticosteroids, and history of non-vertebral fracture. In multivariate analyses, age >60 years, low BMI, and current use of corticosteroids were consistently related to osteoporosis and to low bone mass at all sites. The presence of deformed joints was associated with osteoporosis at the total hip, and a history of previous non-vertebral fracture with osteoporosis at the femoral neck. The Modified Health Assessment Questionnaire (MHAQ) ⩾1.5 and non-vertebral fracture were also independently associated with low bone mass at the hip. The logistic regression analyses models could, however, only predict osteoporosis with a sensitivity of about 50-60% and a specificity of 80-90% at the various measurement sites, and low bone mass with a sensitivity and specificity of about 70%.
CONCLUSION—Consideration of demographic and disease markers may be of some help in predicting presence of osteoporosis or low bone mass, but a combination of markers cannot be used as a clinical tool with sufficient sensitivity and specificity for the identification of osteoporosis or low bone mass in patients with RA.

机译:目的—研究类风湿性关节炎(RA)患者的骨质疏松症和低骨量与人口统计学和临床​​变量之间的关系,以期开发一种数据驱动的临床工具来鉴定高骨质疏松症高危患者。
方法-所有患者均从县注册机构招募,并进行横断面检查,包括各种临床和健康状况测量以及骨密度测量(前后脊柱L2-4,全髋和股骨颈)。一方面,通过双因素和logistic回归分析研究了骨质疏松症(T评分⩽−2.5SD)与低骨量(T评分⩽−1SD)之间的关联,以及人口统计学和临床​​指标。结果—检查了394名平均年龄为54.8岁的患者。脊柱L2-4,全髋和股骨颈的骨质疏松/低骨质百分比分别为16.8 / 45.8、14.7 / 54.5和14.7 / 55.5。骨质疏松症和低骨量与年龄,体重指数(BMI),疾病持续时间,疾病过程措施,关节变形的存在,身体残疾,皮质类固醇的当前使用情况以及非椎骨骨折的历史密切相关。在多变量分析中,年龄> 60岁,BMI较低以及当前使用皮质类固醇与骨质疏松症以及所有部位的骨量低均相关。关节畸形的存在与整个髋部骨质疏松症有关,并且先前有股骨颈非椎体骨折伴骨质疏松症的病史。改良健康评估问卷(MHAQ)≥1.5和非椎骨骨折也与髋关节骨量低有关。但是,逻辑回归分析模型只能预测骨质疏松症,其在各个测量部位的敏感性约为50-60%,特异性为80-90%,而骨质疏松症的敏感性和特异性约为70%。 br />结论:考虑人口统计学和疾病标志物可能有助于预测骨质疏松或骨质疏松的存在,但不能将组合使用的标志物作为具有足够敏感性和特异性的临床工具来鉴定骨质疏松或骨质疏松RA患者的骨量。

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