首页> 外文期刊>DMW: Deutsche Medizinische Wochenschrift >Severe oral mucositis in a patient with HIV infection [Schwere orale Mukositis bei einem Patienten mit HIV-Infektion]
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Severe oral mucositis in a patient with HIV infection [Schwere orale Mukositis bei einem Patienten mit HIV-Infektion]

机译:HIV感染患者的严重口腔粘膜炎[HIV感染患者的严重口腔粘膜炎]

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History and clinical findings: A 50-year-old man with HIV infection (first diagnosed > 20 years ago) presented at our hospital with fulminant oral mucositis. Antiretroviral therapy (tenofovir, emtricitabine, raltegravir) had been started 2 months ago. Previously he had no opportunistic infections and no other pre-existing illnesses. He had not travelled outside Europe but stayed in Spain for several weeks during summer. Investigations: Physical examination revealed swelling of the lips and severe ulcerative mucositis of the gums and pharynx. The patient complained of painful swallowing. The blood-chemistry showed no abnormalities. The microscopical analysis of a smear and a biopsy of the buccal mucosa revealed amastigotes of leishmania. By means of PCR technique, Leishmania donovani complex was specified. Treatment and course: The patient was treated with liposomal amphotericin B (1 mg/kg) for 21 days. Because of the immunosuppression he was put on maintenance therapy afterwards (liposomal amphotericin B every 3 weeks). However, 4 months later there was a clinical relapse of the mucositis and a new cultural and PCR detection of leishmania in a buccal biopsy. After another course of 21 days with liposomal amphotericin B (3 mg/kg) and miltefosine (150 mg/d), the mucositis subsided. Therapy with liposomal amphotericin B (3 mg/kg single dose every 3 weeks) has since been maintained. The antiretroviral therapy was changed meanwhile to lamivudin, abacavir and raltegravir because of kidney failure with elevated urea and creatinine. The patient has been clinically stable ever since without any other HIV-related problems. The latest CD4 count was 456/l and the HIV load 340 copies/ml. Conclusion: Leishmaniasis is a severe infection in HIV-positive patients. Clinical manifestations can be atypical in immunosuppressed patients and the treatment is complicated with HIV coinfection. This is also due to a lifelong persistence of the parasite with potential reactivation especially in patients with suppressed CD4 cells. Therefore maintenance therapy after standard therapy of leishmaniasis is mandatory at least for a CD4 count below 350/l. Especially in HIV patients with a leishmaniasis relapse lifelong maintenance therapy should be considered.
机译:病史和临床发现:一名50岁的HIV感染者(首次确诊> 20年前)在我们医院出现了暴发性口腔粘膜炎。抗逆转录病毒疗法(替诺福韦,恩曲他滨,raltegravir)已于2个月前开始使用。以前,他没有机会感染,也没有其他先前存在的疾病。在夏季,他没有去过欧洲,但在西班牙呆了几个星期。研究:体格检查发现嘴唇肿胀,牙龈和咽部严重溃疡性黏膜炎。病人抱怨吞咽疼痛。血液化学没有显示异常。颊粘膜涂片和活检的显微镜分析显示利什曼原虫的变形虫。通过PCR技术,确定了利什曼原虫donovani复合物。治疗和疗程:该患者接受脂质体两性霉素B(1 mg / kg)治疗21天。由于免疫抑制作用,他随后接受了维持治疗(脂质体两性霉素B每3周一次)。然而,四个月后,口腔粘膜炎临床复发,并在颊活检中进行了新的利什曼原虫培养和PCR检测。用脂质体两性霉素B(3 mg / kg)和米替福辛(150 mg / d)进行21天的疗程后,粘膜炎消退。此后一直保持使用脂质体两性霉素B的疗法(每3周3毫克/千克单剂量)。同时由于肾功能衰竭伴尿素和肌酐升高,抗逆转录病毒疗法改为拉米夫定,阿巴卡韦和拉格列韦。从此患者就一直保持临床稳定,没有任何其他与HIV相关的问题。最新的CD4计数为456 / l,HIV载量为340拷贝/ ml。结论:利什曼病是HIV阳性患者的严重感染。在免疫抑制的患者中临床表现可能是非典型的,并且治疗与HIV合并感染并存。这也归因于该寄生虫的终生持久性,并具有潜在的重新激活作用,尤其是在CD4细胞被抑制的患者中。因此,对于至少低于350 / l的CD4计数,在利什曼病的标准治疗后必须进行维持治疗。特别是在患有利什曼病的艾滋病毒患者中,应考虑终身维持治疗。

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