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首页> 外文期刊>The American Journal of Medicine >Gabapentin toxicity in patients with chronic kidney disease: a preventable cause of morbidity.
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Gabapentin toxicity in patients with chronic kidney disease: a preventable cause of morbidity.

机译:加巴喷丁对慢性肾脏病患者的毒性:可预防的发病原因。

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BACKGROUND: Gabapentin is frequently used as an analgesic in patients with chronic kidney disease. Although gabapentin is well known for its favorable pharmacokinetics, it is exclusively eliminated renally, and patients with chronic kidney disease are at risk for toxicity. Existing literature on such risk is lacking. METHODS: We examined the Mayo Clinic Rochester database from 1998 to 2007 in patients with serum gabapentin measurements and known medical outcomes. A total of 729 patients were stratified according to their estimated glomerular filtration rate: group I, 126 individuals with estimated glomerular filtration greater than 90 mL/min/1.72 mm(3); group II, 594 individuals with estimated glomerular filtration less than 90 mL/min/1.72 mm(3) without dialysis; group III, 9 individuals with chronic dialysis. RESULTS: Patients in groups II and III had higher serum gabapentin levels (8.39+/-0.32 microL/mL and 58.8+/-10.22 microL/mL, respectively) than in group I (5.52+/-0.32 microL/mL, P<.01). Toxicity occurred exclusively in groups II (5.56%) and III (77.8%); toxic manifestations were more severe in group III than in group II. Elderly individuals with multiple comorbidities were overrepresented in those with toxic manifestations. Gabapentin toxicity was suspected initially in only 41.5% of symptomatic cases. CONCLUSION: Gabapentin toxicity in patients with chronic kidney disease is underrecognized. Patients with chronic kidney disease often receive inappropriately high gabapentin dosage for their kidney function, occasioning overt toxicity; advanced age and comorbidity predispose these patients for toxicity. Heightened awareness of such preventable risk, amid the chronic kidney disease epidemic, would be cost-effective and improve healthcare quality.
机译:背景:加巴喷丁常用作慢性肾脏病患者的镇痛药。尽管加巴喷丁以其良好的药代动力学而闻名,但它仅在肾脏中被消除,患有慢性肾脏疾病的患者有毒性的危险。缺乏有关此类风险的现有文献。方法:我们检查了1998年至2007年间梅奥诊所罗切斯特(Mayo Clinic Rochester)数据库中有血清加巴喷丁测量值和已知医学结局的患者。根据估计的肾小球滤过率将总共729例患者分层:第一组,估计肾小球滤过率大于90 mL / min / 1.72 mm的126例患者(3);第二组,594名未透析患者的肾小球滤过率估计低于90 mL / min / 1.72 mm(3);第三组,有9例慢性透析患者。结果:第二和第三组患者的加巴喷丁血清水平(分别为8.39 +/- 0.32 microL / mL和58.8 +/- 10.22 microL / mL)高于第一组(5.52 +/- 0.32 microL / mL,P < .01)。毒性仅发生在第二组(5.56%)和第三组(77.8%);第三组的毒性表现比第二组更严重。具有多种合并症的老年人在具有中毒表现的人群中过多。最初仅在有症状的病例中怀疑加巴喷丁的毒性为41.5%。结论:加巴喷丁对慢性肾脏病患者的毒性作用尚不明确。患有慢性肾脏疾病的患者经常因肾功能不适当地服用高剂量的加巴喷丁,导致明显的毒性。高龄和合并症易使这些患者产生毒性。在慢性肾脏病流行中,提高对此类可预防风险的认识将具有成本效益,并改善医疗质量。

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