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患有 H 综合征、心源性休克、多器官浸润和手指缺血的患者。

Patient with H syndrome, cardiogenic shock, multiorgan infiltration, and digital ischemia.

机构信息

Paediatric Department, Hospital Universitario Son Espases, Carretera de Valldemosa, 79, 07120, Palma, Spain.

Dermatology Department, Hospital Universitario Son Espases, Palma, Spain.

出版信息

Pediatr Rheumatol Online J. 2021 Jun 30;19(1):104. doi: 10.1186/s12969-021-00586-2.

Abstract

BACKGROUND

H syndrome (HS) is a rare autoinflammatory disease caused by a mutation in the solute carrier family 29, member 3 (SCL29A3) gene. It has a variable clinical presentation and little phenotype-genotype correlation. The pathognomonic sign of HS is cutaneous hyperpigmentation located mainly in the inner thighs and often accompanied by other systemic manifestations. Improvement after tocilizumab treatment has been reported in a few patients with HS. We report the first patient with HS who presented cardiogenic shock, multiorgan infiltration, and digital ischemia.

CASE PRESENTATION

8-year-old boy born to consanguineous parents of Moroccan origin who was admitted to the intensive care unit during the Coronavirus Disease-2019 (COVID-19) pandemic with tachypnoea, tachycardia, and oliguria. Echocardiography showed dilated cardiomyopathy and severe systolic dysfunction compatible with cardiogenic shock. Additionally, he presented with multiple organ dysfunction syndrome. SARS-CoV-2 polymerase chain reaction (PCR) and antibody detection by chromatographic immunoassay were negative. A previously ordered gene panel for pre-existing sensorineural hearing loss showed a pathological mutation in the SCL29A3 gene compatible with H syndrome. Computed tomography scan revealed extensive alveolar infiltrates in the lungs and multiple poor defined hypodense lesions in liver, spleen, and kidneys; adenopathy; and cardiomegaly with left ventricle subendocardial nodules. Invasive mechanical ventilation, broad antibiotic and antifungal coverage showed no significant response. Therefore, Tocilizumab as compassionate use together with pulsed intravenous methylprednisolone was initiated. Improvement was impressive leading to normalization of inflammation markers, liver and kidney function, and stabilising heart function. Two weeks later, he was discharged and has been clinically well since then on two weekly administration of Tocilizumab.

CONCLUSIONS

We report the most severe disease course produced by HS described so far in the literature. Our patient's manifestations included uncommon, new complications such as acute heart failure with severe systolic dysfunction, multi-organ cell infiltrate, and digital ischemia. Most of the clinical symptoms of our patient could have been explained by SARS-CoV-2, demonstrating the importance of a detailed differential diagnosis to ensure optimal treatment. Although the mechanism of autoinflammation of HS remains uncertain, the good response of our patient to Tocilizumab makes a case for the important role of IL-6 in this syndrome and for considering Tocilizumab as a first-line treatment, at least in severely affected patients.

摘要

背景

H 综合征(HS)是一种罕见的自身炎症性疾病,由溶质载体家族 29 成员 3(SCL29A3)基因突变引起。它的临床表现多变,表型与基因型相关性小。HS 的特征性标志是位于大腿内侧的皮肤色素沉着,常伴有其他全身表现。已有报道称托珠单抗治疗后少数 HS 患者病情改善。我们报告首例 HS 患者,其表现为心源性休克、多器官浸润和手指缺血。

病例介绍

8 岁男孩,父母为摩洛哥裔近亲结婚,因呼吸急促、心动过速和少尿在 COVID-19 大流行期间入住重症监护病房。超声心动图显示扩张型心肌病和严重收缩功能障碍,符合心源性休克。此外,他还出现了多器官功能障碍综合征。SARS-CoV-2 聚合酶链反应(PCR)和色谱免疫分析法检测抗体均为阴性。先前为筛查先前存在的感音神经性听力损失而进行的基因面板检查显示 SCL29A3 基因存在病理性突变,符合 H 综合征。计算机断层扫描显示肺部广泛肺泡浸润,肝脏、脾脏和肾脏多个定义不清的低密病灶;腺病;以及左心室心内膜下结节引起的心增大。广谱抗生素和抗真菌治疗联合侵入性机械通气无明显效果。因此,开始同情使用托珠单抗联合脉冲静脉内甲基泼尼松龙。病情显著改善,炎症标志物、肝肾功能和心脏功能稳定。两周后,他出院,此后一直病情稳定,每两周接受一次托珠单抗治疗。

结论

我们报告了迄今为止文献中描述的最严重的 HS 病程。我们患者的表现包括不常见的新并发症,如急性心力衰竭伴严重收缩功能障碍、多器官细胞浸润和手指缺血。我们患者的大多数临床症状都可以用 SARS-CoV-2 来解释,这表明进行详细的鉴别诊断以确保最佳治疗非常重要。尽管 HS 自身炎症的机制尚不清楚,但我们患者对托珠单抗的良好反应表明 IL-6 在该综合征中起重要作用,并表明托珠单抗至少在病情严重的患者中可作为一线治疗。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6c1b/8247137/0a1983a6f7df/12969_2021_586_Fig1_HTML.jpg

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