生活在塞内加尔达喀尔郊区非流行区1例4岁儿童内脏利什曼病。

IF 1 Q4 INFECTIOUS DISEASES
Magatte Ndiaye, Dienaba Fafa Cissé, Aicha Djigal, Aminata Sow, Souléye Lélo, Fatoumata Ly, Isaac A Manga, Mame Ami Diouf, Doudou Sow, Oumar Gaye, Boubacar Camara, Babacar Faye
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引用次数: 0

摘要

内脏利什曼病(VL)是一种由利什曼属原虫引起的传染病。在非流行地区观察到散发病例,通常与有限的疫源地有关;因此,这种疾病很容易被忽视。此外,其他疾病具有类似的临床症状,这给临床医生做出准确的诊断和提供有效的治疗带来了困难。我们在塞内加尔Pikine的一名4岁儿童中发现内脏利什曼病。患者因出血、肿瘤和感染综合征被送入Pikine国立教学医院。入院时,患者表现为鼻出血和牙龈出血,耐受性差的严重贫血综合征,伴有39.5℃发热的全身炎症反应综合征,伴有11厘米肝肿大和12厘米IV型脾肿大的肿瘤综合征,以及非炎症性大多腺病。进行脊髓穿刺,GIEMSA染色后对样本进行直接显微镜检查,发现利什曼原虫的无梭体形式。用VL特异性引物(正向和反向)对骨髓抽吸提取的DNA进行PCR扩增,证实VL是引起感染的原因。给予甲氨苄胺锑酸盐(葡聚糖)治疗,临床症状缓解,3个月后进展良好,结果成功。结论。塞内加尔这一内脏利什曼病病例的诊断表明,除了血液系统恶性肿瘤外,还必须将该病与肿瘤综合征、出血性综合征和感染综合征结合起来考虑。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

A Case of Visceral Leishmaniasis in a 4-Year-Old Child Living in Nonendemic Area Located in Suburbs of Dakar, Senegal.

A Case of Visceral Leishmaniasis in a 4-Year-Old Child Living in Nonendemic Area Located in Suburbs of Dakar, Senegal.

Visceral leishmaniasis (VL) is an infectious disease caused by protozoa of the genus Leishmania. Sporadic cases are observed in nonendemic areas and often associated with limited foci; therefore, the disease is easily overlooked. In addition, other diseases have similar clinical symptoms, which make it difficult for clinicians to make an accurate diagnosis and to provide effective treatment. We identified visceral leishmaniasis in a 4-year-old child in Pikine, Senegal. The patient was admitted to the Pikine National Teaching Hospital for haemorrhagic, tumoral, and infectious syndromes. At admission, the patient presented with epistaxis and gingivorrhagia, a severe anaemic syndrome poorly tolerated, a systemic inflammatory response syndrome with fever at 39.5°C, a tumoral syndrome with 11 cm of hepatomegaly and 12 cm of type IV splenomegaly, and noninflammatory macropoly adenopathies. A spinal cord puncture was performed, and direct microscopy examination of the sample after GIEMSA staining revealed amastigote forms of Leishmania. The PCR amplification of extracted DNA from the bone marrow aspiration using specific primers for VL (forward and reverse) confirmed that VL was responsible for the infection. A treatment with meglumine antimoniate (Glucantime) was given and it gave a successful outcome with remission of clinical symptoms and favourable evolution with 3 months hindsight. Conclusion. This visceral leishmaniasis case diagnosis in Senegal has shown that, apart from haematological malignancies, this disease must be considered in combination with a tumor syndrome, haemorrhagic syndrome, and infectious syndrome.

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