Scafetta Tessa, Kovacs Orsolya, Milani Gregorio P, Bronz Gabriel, Lava Sebastiano A G, Betti Céline, Vanoni Federica, Bianchetti Mario G, Faré Pietro B, Camozzi Pietro
Family Medicine Institue, Faculty of Biomedical Sciences, Università della Svizzera Italiana, 6900 Lugano, Switzerland.
Department of Anesthesia, Hôpital du Valais, 1951 Sion, Switzerland.
J Clin Med. 2024 Sep 27;13(19):5781. doi: 10.3390/jcm13195781.
: Inborn errors of glutathione metabolism may cause high anion gap metabolic acidosis due to pyroglutamic acid accumulation. Since 1988, cases of this acidosis have been reported in individuals without these defects. : Given the poorly characterized predisposing factors, presentation, management, and prognosis of acquired pyroglutamic acidosis, we conducted a systematic review using the National Library of Medicine, Excerpta Medica, Web of Science, and Google Scholar databases. : A total of 131 cases were found. Most patients were females (79%), adults (92%) aged 51 years or older (66%) with pre-existing conditions (74%) such as undernutrition, alcohol-use disorder, or kidney disease, and had an ongoing infection (69%). The clinical features included diminished consciousness (60%), Kussmaul breathing (56%), and nausea or vomiting (27%). At least 92% of patients were on paracetamol therapy for >10 days at an appropriate dose, 32% on a β-lactamase-resistant penicillin, and 2.3% on vigabatrin. Besides severe anion gap acidosis, patients also presented with hypokalemia (24%) and kidney function deterioration (41%). Management involved discontinuing the offending drug (100%), bicarbonate (63%), acetylcysteine (42%), and acute kidney replacement therapy (18%). The fatality rate was 18%, which was higher without acetylcysteine (24%) compared to with it (11%). : Acquired pyroglutamic acidosis is a rare, potentially fatal metabolic derangement, which usually occurs after paracetamol use, frequently combined with a β-lactamase-resistant penicillin or vigabatrin. This condition predominantly affects adults, especially women with factors like undernutrition, alcohol-use disorder, or kidney disease, often during infection. Increased awareness of this rare condition is necessary.
谷胱甘肽代谢的先天性缺陷可能由于焦谷氨酸积累而导致高阴离子间隙代谢性酸中毒。自1988年以来,已有报道称无这些缺陷的个体也会出现这种酸中毒病例。鉴于获得性焦谷氨酸酸中毒的易感因素、临床表现、治疗及预后特征尚不明确,我们使用美国国立医学图书馆、医学文摘数据库、科学引文索引数据库及谷歌学术数据库进行了一项系统综述。共发现131例病例。大多数患者为女性(79%),成年人(92%),年龄在51岁及以上(66%),有基础疾病(74%),如营养不良、酒精使用障碍或肾脏疾病,且正在感染(69%)。临床特征包括意识减退(60%)、库斯莫尔呼吸(56%)以及恶心或呕吐(27%)。至少92%的患者接受对乙酰氨基酚治疗超过10天且剂量合适,32%的患者使用β-内酰胺酶耐药青霉素,2.3%的患者使用氨己烯酸。除严重阴离子间隙酸中毒外,患者还出现低钾血症(24%)和肾功能恶化(41%)。治疗措施包括停用致病药物(100%)、使用碳酸氢盐(63%)、乙酰半胱氨酸(42%)以及急性肾脏替代治疗(18%)。病死率为18%,未使用乙酰半胱氨酸时病死率(24%)高于使用时(11%)。获得性焦谷氨酸酸中毒是一种罕见的、潜在致命的代谢紊乱,通常发生在使用对乙酰氨基酚后,常与β-内酰胺酶耐药青霉素或氨己烯酸联合使用。这种情况主要影响成年人,尤其是有营养不良、酒精使用障碍或肾脏疾病等因素的女性,常在感染期间发生。有必要提高对这种罕见疾病的认识。
