Searching for genetic determinants for left ventricular non-compaction.

IF 2.9 2区 医学 Q2 RADIOLOGY, NUCLEAR MEDICINE & MEDICAL IMAGING Quantitative Imaging in Medicine and Surgery Pub Date : 2024-10-01 Epub Date: 2024-09-26 DOI:10.21037/qims-24-470
Michał Spałek, Aneta Kusińska, Jan Spałek, Zbigniew Siudak, Beata Wożakowska-Kapłon, Wioletta Adamus-Białek
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Abstract

Background: Left ventricular non-compaction (LVNC) is still a pathology around which there are numerous controversies regarding the criteria for its diagnosis, presentation, prognosis, and even classification into the appropriate group of diseases. So far, about 190 genes in which mutations may be associated with LVNC have been described, and in each of them, several to several dozen different loci have been discovered. We decided to analyze the frequency of single nucleotide variants (SNVs) in correlation to Petersen's criteria.

Methods: We retrospectively analyzed the results of cardiac magnetic resonance (CMR) studies. Twenty-three patients who met Petersen's criteria agreed to participate in the research and take blood samples for genetic testing. Next, we prospectively included 24 volunteers who did not meet Petersen's criteria. Petersen's criteria were complied with ratio of non-compacted to compacted myocardium (NC/C) ≥2.3. A total of 47 DNA samples were analyzed based on the selected regions of the following genes: β-myosin heavy chain (MYH7), α-cardiac actin (ACTC1), cardiac troponin T (TNNT2), myosin binding protein-C (MYBPC3), LIM-domain binding protein 3 (LBD3), and taffazin (TAZ).

Results: In total, 248 substitutions in exons and introns were obtained for all analyzed samples. No statistically significant differences were detected between the mentioned groups. No significant difference in either downward or upward trends in the number of substitutions in relation to the increasing trabeculation is observed. We indicated differences in the occurrence of the studied SNVs between groups, especially for rs8037241 (3'UTR region of ACTC1) and rs2675686 (LDB3), but they also did not show statistical significance. Although we did not find a significant correlation between the co-occurrence of individual mutations with LVNC, it is worth noting that the presence of one of the four mutations in the range rs8037241 (ACTC1 3'UTR), rs3729998 (TNNT2e. 12), and rs727503240 (MYH7e. 39) increases the risk of LVNC more than 4 times. An inverse association between the number of SNVs and the meeting the Petersen's criteria was demonstrated for studied LDB3 region and rs397516254 in exon 39 of the MYH7 gene.

Conclusions: To our knowledge, no studies have been published comparing the prevalence of selected SNVs in a group of healthy subjects and in a group meeting the Petersen criteria for LVNC. Among both completely healthy individuals who did not meet the Petersen criteria for LVNC as well as those with symptoms who met these criteria we found a similar incidence of SNVs in the ACTC1, TNNT2, LDB3 and MYH7 genes segments analyzed. Further studies are required to confirm or exclude "potentially protective" SNV in the 39th exon of MYH7 (rs397516254) and the role of co-occurrence of individual SNVs in rs8037241 (ACTC1 3'UTR), rs3729998 (TNNT2), and rs727503240 (MYH7) for the increase of the risk of LVNC.

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寻找左心室不充盈的遗传决定因素。
背景:左心室不充盈症(LVNC)仍然是一种病理现象,在其诊断标准、表现形式、预后,甚至将其归入相应的疾病类别等方面仍存在许多争议。迄今为止,约有 190 个基因的突变可能与 LVNC 有关,其中每个基因都发现了几个到几十个不同的位点。我们决定分析与彼得森标准相关的单核苷酸变异(SNV)的频率:我们对心脏磁共振(CMR)研究结果进行了回顾性分析。符合彼得森标准的 23 名患者同意参与研究并抽取血液样本进行基因检测。接下来,我们前瞻性地纳入了 24 名不符合彼得森标准的志愿者。彼得森标准为非压实心肌与压实心肌之比(NC/C)≥2.3。根据以下基因的选定区域分析了总共 47 份 DNA 样本:β-肌球蛋白重链(MYH7)、α-心脏肌动蛋白(ACTC1)、心肌肌钙蛋白 T(TNNT2)、肌球蛋白结合蛋白-C(MYBPC3)、LIM-domain 结合蛋白 3(LBD3)和 taffazin(TAZ):结果:所有分析样本的外显子和内含子共有 248 个替换。结果:所有分析样本的外显子和内含子共发生了 248 个置换。随着骨小梁的增大,替换数量的下降或上升趋势均无明显差异。我们发现研究的 SNV 在不同组间存在差异,尤其是 rs8037241(ACTC1 的 3'UTR 区域)和 rs2675686(LDB3),但它们也没有统计学意义。虽然我们没有发现单个突变的共同发生与LVNC之间存在显著相关性,但值得注意的是,在rs8037241(ACTC1 3'UTR)、rs3729998(TNNT2e.12)和rs727503240(MYH7e.在研究的LDB3区域和MYH7基因第39外显子中的rs397516254中,SNV的数量与满足彼得森标准之间呈反向关系:据我们所知,目前还没有任何研究对一组健康受试者和一组符合彼得森 LVNC 标准的受试者中选定 SNV 的发生率进行比较。在不符合 LVNC Petersen 标准的完全健康人群和符合这些标准的有症状人群中,我们发现在所分析的 ACTC1、TNNT2、LDB3 和 MYH7 基因片段中,SNV 的发生率相似。还需要进一步研究来确认或排除 MYH7 第 39 个外显子(rs397516254)中的 "潜在保护性 "SNV,以及 rs8037241(ACTC1 3'UTR)、rs3729998(TNNT2)和 rs727503240(MYH7)中的单个 SNV 共同出现对增加 LVNC 风险的作用。
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来源期刊
Quantitative Imaging in Medicine and Surgery
Quantitative Imaging in Medicine and Surgery Medicine-Radiology, Nuclear Medicine and Imaging
CiteScore
4.20
自引率
17.90%
发文量
252
期刊介绍: Information not localized
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