首页> 外文期刊>Journal of Oral and Maxillofacial Surgery >Oral bisphosphonate-induced osteonecrosis: risk factors, prediction of risk using serum CTX testing, prevention, and treatment.
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Oral bisphosphonate-induced osteonecrosis: risk factors, prediction of risk using serum CTX testing, prevention, and treatment.

机译:口服双膦酸盐引起的骨坏死:危险因素,使用血清CTX检测,预防和治疗的风险预测。

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摘要

PURPOSE: To assess the risk and time course of oral bisphosphonate-induced osteonecrosis of the jaws. MATERIALS AND METHODS: Detailed data from 30 consecutive cases were compared with 116 cases due to intravenous aminobisphosphonates. RESULTS: Results in part noted a higher incidence related to alendronate (Fosamax; Merck, Whitehouse Station, NJ), a 94.7% predilection for the posterior mandible, and a 50% occurrence spontaneously, with the remaining 50% resulting from an oral surgical procedure, mostly tooth removals. Just over 53% of patients were taking their oral bisphosphonate for osteopenia, 33.3% for documented osteoporosis, and 13.4% for steroid-induced osteoporosis related to 4 or more years of prednisone therapy for an autoimmune condition. There was a direct exponential relationship between the size of the exposed bone and the duration of oral bisphosphonate use. There was also a direct correlation between reports of pain and clinical evidence of infection. The morning fasting serum C-terminal telopeptide (CTX) test results were observed to correlate to the duration of oral bisphosphonate use and could indicate a recovery of bone remodeling with increased values if the oral bisphosphonate was discontinued. A stratification of relative risk was seen as CTX values less than 100 pg/mL representing high risk, CTX values between 100 pg/mL and 150 pg/mL representing moderate risk, and CTX values above 150 pg/mL representing minimal risk. The CTX values were noted to increase between 25.9 pg/mL to 26.4 pg/mL for each month of a drug holiday indicating a recovery of bone remodeling and a guideline as to when oral surgical procedures can be accomplished with the least risk. In addition, drug holidays associated with CTX values rising above the 150 pg/mL threshold were observed to correlate to either spontaneous bone healing or a complete healing response after an office-based debridement procedure. CONCLUSIONS: Oral bisphosphonate-induced osteonecrosis is a rare but real entity that is less frequent, less severe, more predictable, and more responsive to treatment than intravenous bisphosphonate-induced osteonecrosis. The morning fasting serum C-terminal telopeptide bone suppression marker is a useful tool for the clinician to assess risks and guide treatment decisions.
机译:目的:评估口服双膦酸酯引起的颌骨坏死的风险和时程。材料与方法:将连续30例的详细数据与116例由于静脉注射氨基双膦酸盐的患者进行比较。结果:部分结果表明,与阿仑膦酸盐相关的发生率较高(福萨麦斯;默克公司,怀特豪斯站,新泽西州),下颌骨后倾率为94.7%,自发发生率为50%,其余50%来自口腔外科手术,大部分是拔牙。超过53%的患者正在服用口服双膦酸盐治疗骨质减少,33.3%的已记录的骨质疏松症和13.4%的与泼尼松治疗4年或以上的自身免疫性疾病相关的类固醇诱导的骨质疏松症。裸露骨的大小与口服双膦酸盐的持续时间之间存在直接的指数关系。疼痛报告和感染的临床证据之间也有直接的相关性。观察到晨禁食血清C端端肽(CTX)的测试结果与口服双膦酸盐的使用时间相关,并且如果停用口服双膦酸盐,可能表明骨骼重塑的恢复值增加。相对风险分层显示,低于100 pg / mL的CTX值表示高风险,介于100 pg / mL和150 pg / mL的CTX值表示中度风险,高于150 pg / mL的CTX值表示最低风险。药物休假的每个月,CTX值会增加25.9 pg / mL至26.4 pg / mL,这表明骨重塑已恢复并且是何时可以以最低风险完成口腔外科手术的指南。此外,观察到与CTX值升高到150 pg / mL阈值以上相关的药物休假与基于办公室的清创手术后的自发性骨愈合或完整的愈合反应相关。结论:口服双膦酸酯引起的骨坏死是一种罕见但真实的实体,与静脉注射双膦酸酯引起的骨坏死相比,其频率更低,程度更轻,更可预测且对治疗的反应更强。早晨空腹血清C端端肽骨抑制标记物是临床医生评估风险和指导治疗决策的有用工具。

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