干扰素 α 作为伴有间质性肺炎的慢性活动性 EBV 病的抗病毒治疗 - 病例报告。
Interferon alpha as antiviral therapy in chronic active Epstein-Barr virus disease with interstitial pneumonia - case report.
机构信息
Department of Clinical Immunology and Immunotherapy, Medical University of Lublin, Chodzki 4a Street, 20-093, Lublin, Poland.
St. John's Cancer Centre, Jaczewskiego 7 Street, 20-090, Lublin, Poland.
出版信息
BMC Infect Dis. 2018 Apr 20;18(1):190. doi: 10.1186/s12879-018-3097-6.
BACKGROUND
Chronic active Epstein-Barr virus (EBV) disease (CAEBV) is defined as a severe, progressive lymphoproliferative disorder associated with active EBV infection persisting longer than 6 months and developing in patients without recognised immunodeficiency. Rarely, interstitial pneumonitis (IP) occurs as a serious complication in CAEBV patients. The standard therapeutic regimen for IP in CAEBV has not yet been defined. Although interferon alpha (IFN-alpha) is known to suppress viral DNA replication by affecting its basal promoter activation process, it is rarely used in CAEBV patients.
CASE PRESENTATION
A 22-year-old Caucasian woman, diagnosed with CAEBV 1.5 years earlier, was admitted to the Immunology Clinic due to a 4-week history of productive cough, fever and general weakness. Cultures of blood, urine and sputum were negative, but EBV DNA copies were found in the sputum, whole blood, isolated peripheral blood lymphocytes as well as in the blood plasma. Cytokine assessment in peripheral blood revealed the lack of IFN-alpha synthesis. Disseminated maculate infiltrative areas in both lungs were observed on a computed tomography (CT) chest scan. The patient was not qualified for the allogeneic hematopoietic stem cell transplantation (allo-HSCT) due to the risk of immunosuppression-related complications of infectious IP. Inhaled (1.5 million units 3 times a day) and subcutaneous (6 million units 3 times a week) IFN-alpha was implemented. To the best of our knowledge, this was the first documented use of inhaled IFN-alpha in a patient with CAEBV and concomitant IP. Patient's status has improved, and she was eventually qualified to allo-HSCT with reduced conditioning. Currently, the patient feels well, no EBV was detected and further regression of pulmonary changes was documented.
CONCLUSIONS
CAEBV should be considered in patients who present with interstitial lung infiltration and involvement of other organs. Although more promising results have been obtained with allo-HSCT, inhaled IFN-alpha may also be a therapeutic option in patients with CAEBV and a concomitant IP.
背景
慢性活动性 EBV 病毒(CAEBV)疾病定义为一种严重的、进行性的淋巴组织增生性疾病,与持续超过 6 个月的 EBV 感染有关,发生于无明确免疫缺陷的患者中。间质性肺炎(IP)作为 CAEBV 患者的一种严重并发症很少见。CAEBV 患者 IP 的标准治疗方案尚未确定。干扰素 alpha(IFN-α)通过影响其基本启动子激活过程来抑制病毒 DNA 复制,尽管如此,在 CAEBV 患者中也很少使用。
病例介绍
一名 22 岁的白人女性,1.5 年前被诊断为 CAEBV,因 4 周的咳嗽、发热和全身无力而被收入免疫科。血液、尿液和痰液培养均为阴性,但在痰液、全血、分离的外周血淋巴细胞和血浆中均发现 EBV DNA 拷贝。外周血细胞因子评估显示缺乏 IFN-α合成。胸部 CT 扫描显示双肺弥漫性斑片状浸润性阴影。由于感染性 IP 相关免疫抑制并发症的风险,该患者不适合进行异基因造血干细胞移植(allo-HSCT)。给予吸入(每天 3 次,每次 150 万单位)和皮下(每周 3 次,每次 600 万单位)IFN-α治疗。据我们所知,这是首例 CAEBV 合并 IP 患者使用吸入 IFN-α的病例。患者病情改善,随后符合 allo-HSCT 条件且预处理减少。目前,患者感觉良好,未检测到 EBV,进一步影像学显示肺部变化有所改善。
结论
对于出现间质肺浸润和其他器官受累的患者,应考虑 CAEBV。虽然 allo-HSCT 取得了更有前景的结果,但吸入 IFN-α也可能是 CAEBV 合并 IP 患者的一种治疗选择。
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