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Univariate and multivariate analyses of risk factors predisposing to auditory toxicity in patients receiving aminoglycosides.

机译:对接受氨基糖苷类药物的患者发生听觉毒性的危险因素进行单因素和多因素分析。

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摘要

Risk factors predisposing to auditory toxicity of aminoglycosides were analyzed from records of 187 patients enrolled in three prospective randomized trials comparing the toxicity of netilmicin, tobramycin, and amikacin. Patients were eligible if they received three or more days of therapy and at least two serial audiograms were available. The overall auditory toxicity rate was 9.6% (18 of 187). Auditory toxicity was detected in 4.4, 10.8, and 23.5% of patients given netilmicin, tobramycin, and amikacin, respectively (P = 0.05). In the univariate analysis, patients who developed auditory toxicity were significantly older (P = 0.01) and had a significantly higher (P = 0.04) percentage of trough levels of netilmicin or tobramycin above 2 mg/liter or amikacin above 5 mg/liter. In the final logistic regression model, only age was retained as independently influencing the development of auditory toxicity (P less than 0.00001). Conversely, factors that did not add significantly to the prediction of auditory toxicity were aminoglycoside serum levels, total aminoglycoside dose, duration of therapy, sex, peak temperature, presence of bacteremia, shock, liver cirrhosis, dehydration, previous otic pathology or renal failure, and development of renal toxicity. At least in certain populations, age is the most important predisposing factor for the development of auditory toxicity in patients receiving aminoglycosides.
机译:根据三项前瞻性随机试验的187名患者的记录,分析了氨基糖苷类听觉毒性的危险因素,比较了奈替米星,妥布霉素和阿米卡星的毒性。如果患者接受了三天或更多天的治疗并且至少有两张连续听力图可用,则他们是合格的。总体听觉毒性率为9.6%(187个中的18个)。分别接受奈替米星,妥布霉素和阿米卡星的患者分别有4.4、10.8和23.5%的患者发现听觉毒性(P = 0.05)。在单变量分析中,出现听觉毒性的患者年龄较大(P = 0.01),并且奈替米星或妥布霉素的谷值水平高于2 mg / L或阿米卡星的含量高于5 mg / L时显着更高(P = 0.04)。在最终的逻辑回归模型中,仅保留年龄,因为其独立影响听觉毒性的发展(P小于0.00001)。相反,没有明显增加听觉毒性预测的因素是氨基糖苷血清水平,总氨基糖苷剂量,治疗时间,性别,峰值温度,菌血症,休克,肝硬化,脱水,既往耳部病理学或肾衰竭,和肾毒性的发展。至少在某些人群中,年龄是接受氨基糖苷类药物的患者发生听觉毒性的最重要诱因。

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