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Training for treating open fractures in the austere setting.

机译:在严峻的环境中进行治疗开放性骨折的培训。

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NC, with renal failure secondary to bilateral dysplastic kidneys, received an LRD renal transplant (tx) at 17?months of age. Her early post-tx course was complicated by persistently elevated blood polyoma BK virus DNA loads. A protocol biopsy at six?months post-transplant revealed BKVAN. Blood viral loads did not respond to decreased immunosuppression or treatment with ciprofloxacin and leflunomide. Six?months post-tx, her serum creatinine began to rise and we sought experimental therapy to prevent the loss of her graft. At seven?months post-tx, with FDA approval under an eIND, the patient was started on a 36-wk course of treatment with the investigational drug. The patient is now more than 24?months after stopping treatment with CMX. BKV viral DNA loads remain at low, but still detectable levels. Urine viral loads have declined, but remain elevated. EBV DNA loads become undetectable. The patient's serum creatinine has declined back to a baseline of 0.5-0.7?mg/dL and has been stable for two?yr. Renal function was preserved in association with the use of CMX001 to treat BKV nephropathy in a young pediatric kidney transplant recipient. There were no serious adverse events associated with the use of CMX001. This novel medication may be of value in the treatment of BKVAN in pediatric renal transplant recipients.
机译:NC,伴有双侧发育不良性肾脏继发的肾衰竭,在17岁时接受了LRD肾移植(tx)。她的早期TX疗程因血液多瘤BK病毒DNA负荷持续升高而变得复杂。移植后六个月的活检表明BKVAN。血液病毒载量对降低的免疫抑制或用环丙沙星和来氟米特治疗无反应。放疗后六个月,她的血清肌酐开始升高,我们寻求实验治疗以防止其移植物丢失。发射后7个月,在eIND的FDA批准下,患者开始接受研究药物治疗的36周疗程。现在,患者停止使用CMX治疗已经超过24个月了。 BKV病毒DNA载量保持较低水平,但仍可检测到。尿液病毒载量有所下降,但仍保持较高水平。 EBV DNA负载变得不可检测。患者的血清肌酐已降至基线值0.5-0.7?mg / dL,并稳定了两年。结合使用CMX001治疗年轻的小儿肾脏移植受者的BKV肾病,可以保留肾脏功能。没有与使用CMX001相关的严重不良事件。这种新药在小儿肾移植受者的BKVAN治疗中可能有价值。

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