一名患有鱼眼病和轻度表型的复合杂合子患者的 LCAT 基因新致病变体。

IF 3.6 3区 医学 Q2 PHARMACOLOGY & PHARMACY Journal of clinical lipidology Pub Date : 2024-10-02 DOI:10.1016/j.jacl.2024.09.013
Masaaki Miyata, Masayuki Kuroda, Junko Miyoshi, Mika Kirinashizawa, Rora Nagasawa, Misato Yamamoto, Yuichi Akasaki, Kensuke Utatsu, Yoshiro Maezawa, Koutaro Yokote, Mitsuru Ohishi
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引用次数: 0

摘要

背景和目的:低高密度脂蛋白胆固醇和角膜混浊与鱼眼病(FED)、家族性 LCAT 缺乏症(FLD)、载脂蛋白 A 缺乏症和丹吉尔病有关。鉴别诊断可通过临床和生化检验进行。测量 LCAT 活性是将 LCAT 基因变异引起的疾病(FED 和 FLD)与其他两种疾病区分开来的理想方法。然而,并非所有诊所都能做到这一点。在大多数 LCAT 基因变异的病例中,CE/TC 比值都低于参考范围,因此有人建议用 CE/TC 比值作为替代方法。我们报告了一例复合杂合子 FED,其 CE/TC 比值在参考范围内:方法:使用患者的血液样本进行 LCAT 活性测定和基因分析。通过体外表达检测对确定的 LCAT 基因变异进行了检查:结果:与正常血脂对照组相比,原发性患者的 LCAT α 活性约为 20%,而具有典型 FED 致变基因(p.Thr147Ile)的患者的 LCAT α 活性仅为 3%。我们发现了复合杂合变异体(c.101C>T/c.460A>G),这些变异体导致该患者的 LCAT 基因中出现 p.Pro34Leu/p.Asn154Asp 氨基酸残基置换。前一种变异先前已有报道,而后一种变异则是新发现的。体外表达试验表明,与野生型相比,p.Asn154Asp 变体的 LCAT α 活性明显降低,但与典型的 FED 致病变体(p.Pro34Leu 和 p.Thr147Ile)相比,其 LCAT α 活性保持得相对较好:这些结果表明,残余的20% LCAT α活性足以使CE/TC正常化,但不足以防止FED角膜混浊的发生。
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Novel pathogenic variant in the LCAT gene in a compound heterozygous patient with fish-eye disease and a mild phenotype.

Background and objective: Low HDL-cholesterol and corneal opacity are associated with fish-eye disease (FED), familial LCAT deficiency (FLD), ApoAI deficiency, and Tangier disease. The differential diagnosis is made by clinical and biochemical tests. Measuring the LCAT activity is the ideal way to distinguish conditions caused by LCAT gene variants (FED and FLD) from the other two diseases. However, this is not accessible from all clinics. The CE/TC ratio, which is below the reference range in most cases with LCAT gene variants, has been proposed as an alternative. We report a case of compound heterozygous FED with a CE/TC ratio within the reference range.

Methods: LCAT activity assays and genetic analyses were performed using patients' blood samples. Identified LCAT gene variants were examined by an in vitro expression assay.

Results: The proband showed approximately 20 % LCAT α-activity relative to the normolipidemic controls, whereas a patient with a typical FED-causing variant (p.Thr147Ile) showed only 3 % activity. We identified compound heterozygous variants (c.101C>T/c.460A>G) resulting in a p.Pro34Leu/p.Asn154Asp amino acid residue substitution in the LCAT gene of the proband. The former variant has been reported previously, but the latter was newly identified. An in vitro expression assay demonstrated that the LCAT α-activity of the p.Asn154Asp variant significantly decreased regarding the wild type, but it was relatively well preserved compared to the typical FED-causing variants (p.Pro34Leu and p.Thr147Ile).

Conclusion: These results suggest that the residual 20 % LCAT α-activity is sufficient to normalize CE/TC, but not sufficient to prevent the development of corneal opacity in FED.

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来源期刊
CiteScore
7.00
自引率
6.80%
发文量
209
审稿时长
49 days
期刊介绍: Because the scope of clinical lipidology is broad, the topics addressed by the Journal are equally diverse. Typical articles explore lipidology as it is practiced in the treatment setting, recent developments in pharmacological research, reports of treatment and trials, case studies, the impact of lifestyle modification, and similar academic material of interest to the practitioner. While preference is given to material of immediate practical concern, the science that underpins lipidology is forwarded by expert contributors so that evidence-based approaches to reducing cardiovascular and coronary heart disease can be made immediately available to our readers. Sections of the Journal will address pioneering studies and the clinicians who conduct them, case studies, ethical standards and conduct, professional guidance such as ATP and NCEP, editorial commentary, letters from readers, National Lipid Association (NLA) news and upcoming event information, as well as abstracts from the NLA annual scientific sessions and the scientific forums held by its chapters, when appropriate.
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