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首页> 外文期刊>Journal of oncology pharmacy practice: official publication of the International Society of Oncology Pharmacy Practitioners >The management of prolonged, isolated hyperbilirubinemia following cytarabine-based chemotherapy for acute myeloid leukaemia.
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The management of prolonged, isolated hyperbilirubinemia following cytarabine-based chemotherapy for acute myeloid leukaemia.

机译:基于阿糖胞苷的急性髓细胞白血病化疗后长期隔离高胆红素血症的治疗。

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BACKGROUND: Patients diagnosed with Acute Myeloid Leukaemia (AML) often receive cytarabine-based chemotherapy as standard treatment. Cytarabine is usually given in combination with other agents such as idarubicin. Such treatments are known to cause hepatic dysfunction characterized by a combination of jaundice, hyperbilirubinemia and increases in liver enzymes. Isolated hyperbilirubinemia is rarely reported. It is often difficult to identify a causative agent for the hepatic dysfunction, as there are often complicating factors such as sepsis. AIM: To report a case of isolated hyperbilirubinemia in a patient treated with cytarabine-based chemotherapy for AML. CLINICAL DETAILS: After a diagnosis of AML the patient was admitted to hospital to receive induction chemotherapy consisting of high-dose cytarabine, idarubicin, and etoposide. All baseline laboratory results were normal, except the full blood evaluation that was consistent with AML. The chemotherapy was delivered over 7 days, and on the eighth day the patient had a bilirubin (BL) level of 27 micromol/L(normal range 522 micromol/L). All other liver function tests (LFT) were normal. This isolated hyperbilirubinemia remained for the rest of the patient's admission, peaking on day 26, with a level of 255 micromol/L. After a stay in the intensive care unit, the patient was discharged on day 45 with a bilirubin level of 33 micromol/L. All other LFT remained unremarkable. OUTCOME: The isolated hyperbilirubinemia resolved slowly and on day 68, when the patient was re-admitted for further dose-reduced cytarabine, the BL level was 21 micromol/L. The patient was successfully retreated with this lower dose regimen. CONCLUSION: Isolated hyperbilirubinemia is an uncommon presentation of cytarabine induced liver dysfunction. Resolution does occur but over a prolonged period. A lower dose of cytarabine for future treatment should be considered.
机译:背景:诊断为急性髓性白血病(AML)的患者通常接受基于阿糖胞苷的化疗作为标准治疗。阿糖胞苷通常与其他药物联用,例如伊达比星。已知这种治疗会引起肝功能障碍,其特征是黄疸,高胆红素血症和肝酶增加的组合。很少有孤立的高胆红素血症报道。由于通常存在诸如败血症之类的复杂因素,通常很难确定肝功能障碍的病因。目的:报道一例接受阿糖胞苷化疗的AML患者的单纯性高胆红素血症。临床细节:诊断为AML后,该患者入院接受诱导化疗,其中包括大剂量阿糖胞苷,伊达比星和依托泊苷。除与AML一致的全血评估外,所有基线实验室检查结果均正常。化疗进行了7天,第八天患者的胆红素(BL)水平为27微摩尔/升(正常范围为522微摩尔/升)。所有其他肝功能检查(LFT)均正常。其余的这种高胆红素血症在患者入院的其余时间内仍然存在,在第26天达到峰值,水平为255 micromol / L。留在重症监护室后,患者在第45天出院时胆红素水平为33 micromol / L。所有其他LFT仍然不显着。结果:孤立的高胆红素血症缓慢缓解,在第68天,当患者再次入院接受进一步剂量减少的阿糖胞苷治疗时,BL水平为21 micromol / L。使用该较低剂量方案成功治愈了患者。结论:孤立的高胆红素血症是阿糖胞苷引起的肝功能异常的罕见表现。解决方法确实会发生,但是会持续很长时间。应考虑使用较低剂量的阿糖胞苷用于将来的治疗。

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