Case report: malignant hypertension associated with catecholamine excess in a patient with Leigh syndrome.

IF 2.6 Q2 PERIPHERAL VASCULAR DISEASE
Ana Solis, Joshua Shimony, Marwan Shinawi, Kevin T Barton
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引用次数: 1

Abstract

Background: Leigh syndrome is a progressive neurodegenerative mitochondrial disorder caused by multiple genetic etiologies with multisystemic involvement that mostly affecting the central nervous system with high rate of premature mortality.

Case presentation: We present a 3-year, 10 month-old female patient with Leigh syndrome complicated by renal tubular acidosis, hypertension, gross motor delay, who presented with hypertensive emergency, persistent tachycardia, insomnia and irritability. Her previous genetic workup revealed a pathogenic variant in the MT-ND5 gene designated as m.13513G > A;p.Asp393Asn with a heteroplasmy of 69%. She presented acutely with malignant hypertension requiring intensive care unit admission. Her acute evaluation revealed elevated serum and urine catecholamines, without an identifiable catecholamine-secreting tumor. After extensive evaluation for secondary causes, she was ultimately found to have progression of her disease with new infarctions in her medulla, pons, and basal ganglia as the most likely etiology of her hypertension. She was discharged home with clonidine, amlodipine and atenolol for hypertension management. This report highlights the need to recognize possible autonomic dysfunction in mitochondrial disease and illustrates the challenges for accurate and prompt diagnosis and subsequent management of the associated manifestations. This association between catecholamine induced autonomic dysfunction and Leigh syndrome has been previously reported only once with MT-ND5 mutation.

Conclusions: Elevated catecholamines with malignant secondary hypertension may be unique to this specific mutation or may be a previously unrecognized feature of Leigh syndrome and other mitochondrial complex I deficient syndromes. As such, patients with Leigh syndrome who present with malignant hypertension should be treated without the need for extensive work-up for catecholamine-secreting tumors.

Abstract Image

病例报告:Leigh综合征患者伴儿茶酚胺过量的恶性高血压。
背景:Leigh综合征是一种进行性神经退行性线粒体疾病,由多种遗传病因引起,多系统受累,主要影响中枢神经系统,死亡率高。病例介绍:我们报告一位3岁10个月的Leigh综合征女性患者,合并肾小管酸中毒、高血压、大运动迟缓,表现为高血压急症、持续性心动过速、失眠和烦躁。她之前的遗传检查显示MT-ND5基因中有一种致病性变异,命名为m.13513G > a;p。Asp393Asn的异质性为69%。她急性表现为恶性高血压,需要重症监护病房入院。她的急性评估显示血清和尿儿茶酚胺升高,没有可识别的儿茶酚胺分泌肿瘤。在对继发原因进行广泛评估后,最终发现患者病情进展,髓质、桥脑桥和基底神经节出现新的梗死,这是最可能的高血压病因。出院时使用可乐定、氨氯地平和阿替洛尔治疗高血压。本报告强调了在线粒体疾病中识别可能的自主神经功能障碍的必要性,并说明了准确和及时诊断以及相关表现的后续管理的挑战。儿茶酚胺诱导的自主神经功能障碍与Leigh综合征之间的关联先前仅报道过一次MT-ND5突变。结论:恶性继发性高血压的儿茶酚胺升高可能是这种特定突变所特有的,也可能是Leigh综合征和其他线粒体复合物I缺陷综合征以前未被认识到的特征。因此,伴有恶性高血压的Leigh综合征患者应在治疗时不需要对分泌儿茶酚胺的肿瘤进行广泛检查。
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来源期刊
Clinical Hypertension
Clinical Hypertension PERIPHERAL VASCULAR DISEASE-
CiteScore
5.40
自引率
4.80%
发文量
34
审稿时长
6 weeks
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