Absence of Pathogenic Mutations and Strong Association With HLA-DRB1*11:01 in Statin-Naïve Early-Onset Anti-HMGCR Necrotizing Myopathy.

IF 7.8 1区 医学 Q1 CLINICAL NEUROLOGY Neurology® Neuroimmunology & Neuroinflammation Pub Date : 2024-09-01 Epub Date: 2024-08-06 DOI:10.1212/NXI.0000000000200285
Laura Llansó, Alba Segarra-Casas, Cristina Domínguez-González, Edoardo Malfatti, Solange Kapetanovic, Benjamín Rodríguez-Santiago, Oscar de la Calle, Rosa Blanco, Amelia Dobrescu, Andrés Nascimento-Osorio, Andrés Paipa, Aurelio Hernandez-Lain, Cristina Jou, Anaís Mariscal, Laura González-Mera, Ana Arteche, Cinta Lleixà, Marta Caballero-Ávila, Álvaro Carbayo, Ana Vesperinas, Luis Querol, Eduard Gallardo, Montse Olivé
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Abstract

Background and objectives: Immune-mediated necrotizing myopathy (IMNM) caused by antibodies against 3-hydroxy-3-methylglutaryl coenzyme A reductase (HMGCR) is an inflammatory myopathy that has been epidemiologically correlated with previous statin exposure. We characterized in detail a series of 11 young statin-naïve patients experiencing a chronic disease course mimicking a limb-girdle muscular dystrophy. With the hypothesis that HMGCR upregulation may increase immunogenicity and trigger the production of autoantibodies, our aim was to expand pathophysiologic knowledge of this distinct phenotype.

Methods: Clinical and epidemiologic data, autoantibody titers, creatine kinase (CK) levels, response to treatment, muscle imaging, and muscle biopsies were assessed. HMGCR expression in patients' muscle was assessed by incubating sections of affected patients with purified anti-HMGCR+ serum. Whole-exome sequencing (WES) with a special focus on cholesterol biosynthesis-related genes and high-resolution human leukocyte antigen (HLA) typing were performed.

Results: Patients, aged 3-25 years and mostly female (90.9%), presented with subacute proximal weakness progressing over many years and high CK levels (>1,000 U/L). Diagnostic delay ranged from 3 to 27 years. WES did not reveal any pathogenic variants. HLA-DRB1*11:01 carrier frequency was 60%, a significantly higher proportion than in the control population. No upregulation or mislocalization of the enzyme in statin-exposed or statin-naïve anti-HMGCR+ patients was observed, compared with controls.

Discussion: WES of a cohort of patients with dystrophy-like anti-HMGCR IMNM did not reveal any common rare variants of any gene, including cholesterol biosynthesis-related genes. HLA analysis showed a strong association with HLA-DRB1*11:01, previously mostly described in statin-exposed adult patients; consequently, a common immunogenic predisposition should be suspected, irrespective of statin exposure. Moreover, we were unable to conclusively demonstrate muscle upregulation/mislocalization of HMGCR in IMNM, whether or not driven by statins.

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在他汀类药物无效的早发抗 HMGCR 坏死性肌病患者中不存在致病性突变,且与 HLA-DRB1*11:01 有密切关系。
背景和目的:由抗 3-羟基-3-甲基戊二酰辅酶 A 还原酶(HMGCR)抗体引起的免疫介导的坏死性肌病(IMNM)是一种炎症性肌病,从流行病学角度看,该病与既往接触过他汀类药物有关。我们详细描述了一系列 11 位年轻的他汀类药物无效患者的特征,他们的慢性病程模仿了肢腰肌营养不良症。我们的假设是,HMGCR上调可能会增加免疫原性并引发自身抗体的产生,因此我们的目的是扩大这一独特表型的病理生理学知识:对临床和流行病学数据、自身抗体滴度、肌酸激酶(CK)水平、治疗反应、肌肉成像和肌肉活检进行了评估。通过用纯化的抗HMGCR+血清培养受影响患者的切片,评估患者肌肉中HMGCR的表达。对胆固醇生物合成相关基因进行了全外显子组测序(WES),并进行了高分辨率人类白细胞抗原(HLA)分型:患者年龄为 3-25 岁,大部分为女性(90.9%),表现为持续多年的亚急性近端乏力和高 CK 水平(>1,000 U/L)。诊断延迟时间从 3 年到 27 年不等。WES 未发现任何致病变异。HLA-DRB1*11:01携带者的比例为60%,明显高于对照人群。与对照组相比,暴露于他汀类药物或他汀类药物无效的抗-HMGCR+患者体内的酶没有上调或错位:讨论:对一组肌营养不良型抗-HMGCR IMNM 患者进行的 WES 研究未发现任何基因(包括胆固醇生物合成相关基因)存在任何常见的罕见变异。HLA分析表明,该基因与HLA-DRB1*11:01有很强的相关性,而HLA-DRB1*11:01以前大多出现在他汀类药物暴露的成年患者中;因此,无论他汀类药物暴露与否,都应怀疑存在共同的免疫易感性。此外,我们无法确证 IMNM 中 HMGCR 的肌肉上调/异位,无论是否由他汀类药物引起。
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来源期刊
CiteScore
15.60
自引率
2.30%
发文量
219
审稿时长
8 weeks
期刊介绍: Neurology Neuroimmunology & Neuroinflammation is an official journal of the American Academy of Neurology. Neurology: Neuroimmunology & Neuroinflammation will be the premier peer-reviewed journal in neuroimmunology and neuroinflammation. This journal publishes rigorously peer-reviewed open-access reports of original research and in-depth reviews of topics in neuroimmunology & neuroinflammation, affecting the full range of neurologic diseases including (but not limited to) Alzheimer's disease, Parkinson's disease, ALS, tauopathy, and stroke; multiple sclerosis and NMO; inflammatory peripheral nerve and muscle disease, Guillain-Barré and myasthenia gravis; nervous system infection; paraneoplastic syndromes, noninfectious encephalitides and other antibody-mediated disorders; and psychiatric and neurodevelopmental disorders. Clinical trials, instructive case reports, and small case series will also be featured.
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