Clinical Case of X-Linked Lymphoproliferative Syndrome Burdened with Hemophagocytic Lymphohistiocytosis and Crohn's Disease

Pediatric pharmacology Pub Date : 2023-02-28 DOI:10.15690/pf.v20i1.2522

Ekaterina S. Matros, Alena I. Karitskaya

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Abstract

Background. X-linked lymphoproliferative (XLP) syndrome is hereditary disease with the incidence of 1-3 per 1 million born boys. This clinical case demonstrates a rare picture of XLP type 2 manifestation without prior Epstein-Barr virus.Clinical case description. Boy D., 15 years old, was admitted to Morozovskaya Children's City Hospital with complaints on fever, abdominal pain, loose stools, weight loss. The past medical history included hemophagocytic syndrome (remission) and acute erythema nodosum. We have performed several studies: abdominal ultrasound (hepatomegaly, dynamic changes in the intestine: parts of the small intestine were enlarged and walls were thickened, mass peristalsis, walls of transverse colon and descending colon are thickened up to 5 mm, mesenteric lymphadenopathy), rectosigmoidoscopy (high-activity ulcerative proctosigmoiditis corresponds to Crohn's disease), biochemical and clinical blood tests (active hemophagocytic syndrome), coagulogram (secondary hypocoagulation), myelogram (no data on hemoblastosis or aplastic condition). Virological blood tests (CMV, EBV, HHV-VI): negative. Laboratory and instrumental tests have revealed recurrence of hemophagocytic syndrome and Crohn's disease. The child was consulted by rheumatologist, hematologist, gastroenterologist, geneticist, neurologist, and clinical pharmacologist. The primary immune deficiency disease was suspected in this patient due to his medical history. Molecular genetic study was performed (deletion including the XIAP gene was revealed) and the diagnosis of primary immune deficiency was verified: X-linked lymphoproliferative syndrome type 2. Thus, allogeneic haematopoietic stem cell transplantation (HSCT) was performed.Conclusion. XLP diagnosis and management require multidisciplinary approach. The early diagnosis is crucial due to the high risk of secondary complications development that can significantly worsen the disease's prognosis. Allogeneic HSCT is the only effective treatment for the disease.

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嗜血球性淋巴组织细胞增多症伴克罗恩病的x连锁淋巴细胞增生性综合征临床分析

背景。x连锁淋巴细胞增生性(XLP)综合征是一种遗传性疾病，发病率为1-3 / 100万出生男孩。本病例为罕见的无eb病毒的XLP 2型表现。临床病例描述。男孩D, 15岁，因发烧、腹痛、便稀、体重减轻被送入莫罗佐夫斯卡亚儿童城市医院。既往病史包括噬血细胞综合征(缓解期)和急性结节性红斑。我们做了几项研究:腹部超声(肝肿大，肠道动态变化;小肠部分肿大，肠壁增厚，肿块性蠕动，横结肠和降结肠壁增厚达5mm，肠系膜淋巴结病，直肠乙状结肠镜检查(高活性溃疡性乙状结肠炎对应克罗恩病)，生化和临床血液检查(活动性噬血细胞综合征)，凝血图(继发性低凝)，骨髓图(无造血增生或再生状况)。病毒学血检(巨细胞病毒、EBV、HHV-VI):阴性。实验室和仪器检查显示噬血细胞综合征和克罗恩病复发。风湿病学家、血液病学家、胃肠病学家、遗传学家、神经科医生和临床药理学家咨询了该儿童。根据患者的病史，怀疑为原发性免疫缺乏症。进行分子遗传学研究(发现包括XIAP基因缺失)，证实原发性免疫缺陷的诊断:x连锁淋巴细胞增生性综合征2型。因此，进行同种异体造血干细胞移植(HSCT)是可行的。XLP的诊断和管理需要多学科的方法。早期诊断是至关重要的，因为继发性并发症发展的高风险，可显着恶化疾病的预后。同种异体造血干细胞移植是治疗该疾病的唯一有效方法。

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Pediatric pharmacology

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