Genetic and Functional Analyses of Patients with Marked Hypo-High-Density Lipoprotein Cholesterolemia.

IF 3 2区 医学 Q2 PERIPHERAL VASCULAR DISEASE Journal of atherosclerosis and thrombosis Pub Date : 2024-09-01 Epub Date: 2024-03-28 DOI:10.5551/jat.64579
Yasuhisa Furuta, Yoshinori Osaki, Yoshimi Nakagawa, Song-Iee Han, Masaya Araki, Akito Shikama, Nami Ohuchi, Daichi Yamazaki, Erika Matsuda, Seitaro Nohara, Yuhei Mizunoe, Kenta Kainoh, Yasuhito Suehara, Hiroshi Ohno, Yoshinori Takeuchi, Takafumi Miyamoto, Yuki Murayama, Yoko Sugano, Hitoshi Iwasaki, Ken-Ichi Hirano, Masahiro Koseki, Shogo Nakano, Hiroaki Tokiwa, Motohiro Sekiya, Naoya Yahagi, Takashi Matsuzaka, Kiyotaka Nakamagoe, Yasushi Tomidokoro, Jun Mitsui, Shoji Tsuji, Hiroaki Suzuki, Hitoshi Shimano
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Abstract

Aim: This study aimed to analyze two cases of marked hypo-high-density lipoprotein (HDL) cholesterolemia to identify mutations in ATP-binding cassette transporter A1 (ABCA1) and elucidate the molecular mechanism by which these novel pathological mutations contribute to hypo-HDL cholesterolemia in Tangier disease.

Methods: Wild type and mutant expression plasmids containing a FLAG tag inserted at the C-terminus of the human ABCA1 gene were generated and transfected into HEK293T cells. ABCA1 protein expression and cholesterol efflux were evaluated via Western blotting and efflux assay. The difference in the rate of change in protein expression was evaluated when proteolytic and protein-producing systems were inhibited.

Results: In case 1, a 20-year-old woman presented with a chief complaint of gait disturbance. Her HDL-C level was only 6.2 mg/dL. Tangier disease was suspected because of muscle weakness, decreased nerve conduction velocity, and splenomegaly. Whole-exome analysis showed compound heterozygosity for a W484* nonsense mutation and S1343I missense mutation, which confirmed Tangier disease. Cholesterol efflux decreased by a mixture of W484* and S1343I mutations. The S1343I mutation decreased the protein production rate but increased the degradation rate, decreasing the protein levels. This patient also had Krabbe disease. The endogenous ABCA1 protein level of macrophage cell decreased by knocking down its internal galactocerebrosidase. Case 2, a 51-year-old woman who underwent tonsillectomy presented with peripheral neuropathy, corneal opacity, and HDL-C of 3.4 mg/dL. Whole-exome analysis revealed compound heterozygosity for R579* and R1572* nonsense mutations, which confirmed Tangier disease.

Conclusion: Case 1 is a new ABCA1 mutation with complex pathogenicity, namely, a W484*/S1343I compound heterozygote with marked hypo-HDL cholesterolemia. Analyses of the compound heterozygous mutations indicated that decreases in ABCA1 protein levels and cholesterol efflux activity caused by the novel S1343I mutation combined with loss of W484* protein activity could lead to marked hypo-HDL cholesterolemia. Galactocerebrosidase dysfunction could also be a potential confounding factor for ABCA1 protein function.

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明显低高密度脂蛋白胆固醇血症患者的基因和功能分析
目的:本研究旨在分析两例明显的低高密度脂蛋白胆固醇血症,以确定ATP结合盒转运体A1(ABCA1)的突变,并阐明这些新型病理突变导致丹吉尔病中低高密度脂蛋白胆固醇血症的分子机制:方法:生成野生型和突变型表达质粒,并将其转染到 HEK293T 细胞中,质粒含有插入人 ABCA1 基因 C 端的 FLAG 标记。ABCA1 蛋白表达和胆固醇外流通过 Western 印迹和外流检测进行评估。在蛋白水解和蛋白生成系统受到抑制时,对蛋白表达变化率的差异进行了评估:在病例 1 中,一名 20 岁的女性主诉步态障碍。她的高密度脂蛋白胆固醇水平仅为 6.2 毫克/分升。由于肌无力、神经传导速度下降和脾脏肿大,她被怀疑患有丹吉尔病。全外显子组分析显示,该患者存在W484*无义突变和S1343I错义突变的复合杂合子,这证实了丹吉尔病。W484*和S1343I混合突变导致胆固醇外流减少。S1343I 突变降低了蛋白质的生成率,但增加了降解率,从而降低了蛋白质水平。这名患者还患有克拉伯病。病例 2:51 岁女性,扁桃体切除术后出现周围神经病变、角膜混浊,HDL-C 为 3.4 mg/dL。全外显子组分析显示 R579* 和 R1572* 无义突变的复合杂合性,证实了丹吉尔病:病例 1 是一种具有复杂致病性的新型 ABCA1 突变,即 W484*/S1343I 复合杂合子,伴有明显的低密度脂蛋白胆固醇血症。对复合杂合子突变的分析表明,新型 S1343I 突变导致 ABCA1 蛋白水平和胆固醇外排活性下降,再加上 W484* 蛋白活性丧失,可导致明显的低密度脂蛋白胆固醇血症。半乳糖脑苷脂酶功能障碍也可能是影响 ABCA1 蛋白功能的潜在因素。
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来源期刊
CiteScore
6.60
自引率
15.90%
发文量
271
审稿时长
1 months
期刊介绍: JAT publishes articles focused on all aspects of research on atherosclerosis, vascular biology, thrombosis, lipid and metabolism.
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