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骨转换状态:分类模型及临床意义。

Bone Turnover Status: Classification Model and Clinical Implications.

机构信息

Department of Geriatric Medicine, The Canberra Hospital, Canberra, ACT Health, Canberra, Australia.

Department of Orthopaedic Surgery, The Canberra Hospital, Canberra, ACT Health, Canberra, Australia.

出版信息

Int J Med Sci. 2018 Feb 1;15(4):323-338. doi: 10.7150/ijms.22747. eCollection 2018.

Abstract

To develop a practical model for classification bone turnover status and evaluate its clinical usefulness. Our classification of bone turnover status is based on internationally recommended biomarkers of both bone formation (N-terminal propeptide of type1 procollagen, P1NP) and bone resorption (beta C-terminal cross-linked telopeptide of type I collagen, bCTX), using the cutoffs proposed as therapeutic targets. The relationships between turnover subtypes and clinical characteristic were assessed in1223 hospitalised orthogeriatric patients (846 women, 377 men; mean age 78.1±9.50 years): 451(36.9%) subjects with hip fracture (HF), 396(32.4%) with other non-vertebral (non-HF) fractures (HF) and 376 (30.7%) patients without fractures. Six subtypes of bone turnover status were identified: 1 - normal turnover (P1NP>32 μg/L, bCTX≤0.250 μg/L and P1NP/bCTX>100.0[(median value]); 2- low bone formation (P1NP ≤32 μg/L), normal bone resorption (bCTX≤0.250 μg/L) and P1NP/bCTX>100.0 (subtype2A) or P1NP/bCTX<100.0 (subtype 2B); 3- low bone formation, high bone resorption (bCTX>0.250 μg/L) and P1NP/bCTX<100.0; 4- high bone turnover (both markers elevated ) and P1NP/bCTX>100.0 (subtype 4A) or P1NP/bCTX<100.0 (subtype 4B). Compared to subtypes 1 and 2A, subtype 2B was strongly associated with nonvertebral fractures (odds ratio [OR] 2.0), especially HF (OR 3.2), age>75 years and hyperparathyroidism. Hypoalbuminaemia and not using osteoporotic therapy were two independent indicators common for subtypes 3, 4A and 4B; these three subtypes were associated with in-hospital mortality. Subtype 3 was associated with fractures (OR 1.7, for HF OR 2.4), age>75 years, chronic heart failure (CHF), anaemia, and history of malignancy, and predicted post-operative myocardial injury, high inflammatory response and length of hospital stay (LOS) above10 days. Subtype 4A was associated with chronic kidney disease (CKD), anaemia, history of malignancy and walking aids use and predicted LOS>20 days, but was not discriminative for fractures. Subtype 4B was associated with fractures (OR 2.1, for HF OR 2.5), age>75 years, CKD and indicated risks of myocardial injury, high inflammatory response and LOS>10 days. We proposed a classification model of bone turnover status and demonstrated that in orthogeriatric patients altered subtypes are closely related to presence of nonvertebral fractures, comorbidities and poorer in-hospital outcomes. However, further research is needed to establish optimal cut points of various biomarkers and improve the classification model.

摘要

为了开发一种实用的骨转换状态分类模型并评估其临床实用性。我们的骨转换状态分类基于国际推荐的骨形成标志物(I 型前胶原 N 端前肽,P1NP)和骨吸收标志物(I 型胶原β C 端交联肽,bCTX),使用作为治疗目标提出的截断值。在 1223 名住院骨科老年患者中评估了转换亚型与临床特征的关系(846 名女性,377 名男性;平均年龄 78.1±9.50 岁):451 名(36.9%)髋部骨折(HF)患者,396 名(32.4%)非椎体(非-HF)骨折患者和 376 名(30.7%)无骨折患者。确定了六种骨转换状态亚型:1-正常转换(P1NP>32 μg/L,bCTX≤0.250 μg/L 和 P1NP/bCTX>100.0[中位数]);2-低骨形成(P1NP ≤32 μg/L),正常骨吸收(bCTX≤0.250 μg/L)和 P1NP/bCTX>100.0(亚型 2A)或 P1NP/bCTX<100.0(亚型 2B);3-低骨形成,高骨吸收(bCTX>0.250 μg/L)和 P1NP/bCTX<100.0;4-高骨转换(两种标志物均升高)和 P1NP/bCTX>100.0(亚型 4A)或 P1NP/bCTX<100.0(亚型 4B)。与亚型 1 和 2A 相比,亚型 2B 与非椎体骨折强烈相关(比值比[OR]2.0),尤其是 HF(OR 3.2)、年龄>75 岁和甲状旁腺功能亢进。低白蛋白血症和未使用骨质疏松症治疗是亚型 3、4A 和 4B 的两个共同独立指标;这三种亚型与住院死亡率相关。亚型 3与骨折(HF 的 OR 1.7,OR 2.4)、年龄>75 岁、慢性心力衰竭(CHF)、贫血、恶性肿瘤史有关,并预测术后心肌损伤、炎症反应高和住院时间(LOS)超过 10 天。亚型 4A 与慢性肾脏病(CKD)、贫血、恶性肿瘤史和使用助行器有关,并预测 LOS>20 天,但对骨折无鉴别力。亚型 4B 与骨折(HF 的 OR 2.1,OR 2.5)、年龄>75 岁、CKD 有关,并提示心肌损伤、炎症反应高和 LOS>10 天的风险。我们提出了一种骨转换状态分类模型,并表明在骨科老年患者中,改变的亚型与非椎体骨折、合并症和较差的住院结局密切相关。然而,需要进一步的研究来建立各种生物标志物的最佳截断值并改进分类模型。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/26c6/5835703/2299477a1fc5/ijmsv15p0323g001.jpg

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