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一名接受基于阿扎那韦/利托那韦的抗逆转录病毒治疗的HIV感染儿童急性发生库欣综合征。

Acute development of Cushing syndrome in an HIV-infected child on atazanavir/ritonavir based antiretroviral therapy.

作者信息

Dubrocq Gueorgui, Estrada Andrea, Kelly Shannon, Rakhmanina Natella

机构信息

Divisions of Infectious Diseases.

Divisions of Endocrinology and Diabetes.

出版信息

Endocrinol Diabetes Metab Case Rep. 2017 Oct 28;2017. doi: 10.1530/EDM-17-0076. eCollection 2017.

Abstract

UNLABELLED

An 11-year-old male with perinatally acquired human immune deficiency virus (HIV) infection on antiretroviral regimen, which included abacavir plus lamivudine (Epzicom), didanosine, ritonavir and atazanavir presented with bilateral axillary striae, increased appetite, fatigue, facial swelling and acute weight gain. Two months prior to presentation, the patient had received a diagnostic and therapeutic intra-articular triamcinolone injection in the knee for pain relief and subsequently became progressively swollen in the face, developed striae bilaterally at the axillae, experienced increased appetite, fatigue and an 8 pound weight gain. During the endocrine workup, suspicion for adrenal insufficiency prompted 24-h urine collection for free cortisol, which was found to be undetectable (below LLQ of 1.0 µg/L). This prompted further evaluation of the hypothalamic-pituitary axis (HPA) by standard dose adrenocorticotropic hormone (ACTH) stimulation test. A 250 µg cosyntropin stimulation test was performed and confirmed HPA axis suppression. Baseline cortisol level was <1 µg/dL and stimulated cortisol level at 30 min was 3.8 µg/dL. The patient was diagnosed with iatrogenic Cushing syndrome and suppression of HPA axis secondary to the drug interaction between ritonavir (RTV) and intra-articular triamcinolone injection. Following endocrine evaluation and workup, the patient was admitted for planned orthopaedic procedure including elective left hamstring lengthening, distal femoral osteotomy and patellar tendon advancement. Taking into consideration the diagnosis of iatrogenic Cushing syndrome, at the start of the surgical procedure, 100 mg IV stress dose of hydrocortisone followed by 50 mg hydrocortisone every 8 h for 24 h was administered. Stress dosing was discontinued 24 h after the procedure. Throughout the hospitalization and upon discharge, the patient continued his ART. From initial presentation, patient has remained clinically stable throughout surgery and postoperative period.

LEARNING POINTS

Drug-drug interaction between ritonavir and triamcinolone can cause Cushing syndrome.Although triamcinolone has a half-life of 3 h, an intra-articular injection may be systematically absorbed for 3 weeks after injection, and adrenal suppression may last as long as 30 days.Co-administration of ritonavir and corticosteroids may result in an increase of plasma levels of corticosteroids levels, as they are both eliminated by CYP3A metabolism, and this interaction has the potential to prolong the half-life of triamcinolone several fold.No specific guidelines are available for the management of iatrogenic Cushing syndrome secondary to ritonavir and corticosteroids.One treatment option includes replacing ritonavir with a non-protease inhibitor-based regimen.Initiating hydrocortisone replacement therapy to prevent an adrenal crisis is also an alternate option.

摘要

未标注

一名11岁男性,因围产期感染人类免疫缺陷病毒(HIV),正在接受抗逆转录病毒治疗,方案包括阿巴卡韦加拉米夫定(依非韦伦)、去羟肌苷、利托那韦和阿扎那韦,出现双侧腋窝条纹、食欲增加、疲劳、面部肿胀和急性体重增加。就诊前两个月,患者因疼痛接受了膝关节诊断性和治疗性关节内曲安奈德注射,随后面部逐渐肿胀,双侧腋窝出现条纹,食欲增加,感到疲劳,体重增加了8磅。在内分泌检查过程中,怀疑肾上腺功能不全促使进行24小时尿游离皮质醇收集,结果发现无法检测到(低于最低检测限1.0μg/L)。这促使通过标准剂量促肾上腺皮质激素(ACTH)刺激试验进一步评估下丘脑-垂体轴(HPA)。进行了250μg促肾上腺皮质激素刺激试验,证实HPA轴受抑制。基线皮质醇水平<1μg/dL,30分钟时刺激后的皮质醇水平为3.8μg/dL。患者被诊断为医源性库欣综合征,继发于利托那韦(RTV)与关节内曲安奈德注射之间的药物相互作用导致HPA轴抑制。经过内分泌评估和检查后,患者因计划中的骨科手术入院,包括择期左腘绳肌延长、股骨远端截骨术和髌腱推进术。考虑到医源性库欣综合征的诊断,在手术开始时,静脉注射100mg应激剂量的氢化可的松,随后每8小时注射50mg氢化可的松,持续24小时。手术后24小时停止应激给药。在整个住院期间及出院后,患者继续接受抗逆转录病毒治疗。从最初就诊起,患者在整个手术及术后期间临床情况一直保持稳定。

学习要点

利托那韦与曲安奈德之间的药物相互作用可导致库欣综合征。虽然曲安奈德半衰期为3小时,但关节内注射后可能会在3周内被系统吸收,肾上腺抑制可能持续长达30天。利托那韦与皮质类固醇联合使用可能会导致皮质类固醇血浆水平升高,因为它们都通过CYP3A代谢消除,这种相互作用有可能使曲安奈德的半衰期延长数倍。对于继发于利托那韦和皮质类固醇的医源性库欣综合征,尚无具体的管理指南。一种治疗选择包括用基于非蛋白酶抑制剂的方案替代利托那韦。启动氢化可的松替代疗法以预防肾上腺危象也是一种替代选择。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6229/5670321/092c8b89a0a2/edmcr-2017-170076-g001.jpg

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