Hydroxymethylbilane Synthase Gene Mutation: The Hidden Driver of Abdominal Pain and Neurological Symptoms in Acute Intermittent Porphyria

Q4 Medicine Journal of Applied Hematology Pub Date : 2024-04-17 DOI:10.4103/joah.joah_19_24

Abeer F Zakariyah, Rahaf Alzahrani, I. Alhazmi, Alia Abotaleb, Mohammed Alasmari, A. Basendwah, Rasha Alsubaie, Muhammad Sohaib Khan, Leena Alnajjar, Sultan Altouri

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Abstract

Mutations in the hydroxymethylbilane synthase (HMBS) gene can lead to a deficiency of the HMBS enzyme, allowing porphyrins to accumulate to toxic levels in the liver and other organs, leading to acute intermittent porphyria (AIP). This case report describes the medical journey of a 20-year-old female, previously in good health, who experienced multiple hospitalizations and clinic visits due to severe abdominal pain episodes and remained undiagnosed for over 6 years. Despite the nonspecific nature of these symptoms, a suspicion of acute porphyria confirmed by genetic analysis revealed a splice pathogenic variant (c.826-2A>T) in the HMBS gene in a heterozygous state. As the disease progressed, the patient developed a series of complications, including hyponatremia, autonomic instability, and motor neuropathy, culminating in complete paralysis (quadriplegia) and respiratory failure. The case highlights the importance of early recognition and differential diagnoses in managing AIP, with genetic testing playing a crucial role in confirming the diagnosis.

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羟甲基比兰合成酶基因突变：急性间歇性卟啉症腹痛和神经症状的隐性驱动因素

羟甲基比兰合成酶（HMBS）基因突变可导致 HMBS 酶缺乏，使卟啉在肝脏和其他器官中积累到毒性水平，从而引发急性间歇性卟啉症（AIP）。本病例报告描述了一名 20 岁女性的就医经历，她以前身体健康，但因剧烈腹痛发作而多次住院和就诊，6 年多来一直未被确诊。尽管这些症状都是非特异性的，但通过基因分析发现，HMBS 基因中的一个剪接致病变体（c.826-2A>T）处于杂合状态，因此怀疑是急性卟啉症。随着病情的发展，患者出现了一系列并发症，包括低钠血症、自主神经不稳定和运动神经病变，最终导致全身瘫痪（四肢瘫痪）和呼吸衰竭。该病例强调了早期识别和鉴别诊断在治疗 AIP 中的重要性，而基因检测在确诊中起着至关重要的作用。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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