[遗传性高结合胆红素血症患者 UGT1A1 基因突变谱与临床表型之间的相关性]。

Q3 Medicine
Q F Xiong, Y J Lu, L Zou, H Zhou, H Ren, X N Feng, Y F Yang
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Comparison of continaous veriable data with normal distribution using <i>t</i>-test. <b>Results:</b> 112 cases (male:female ratio 81:31, aged 9-70 years) had inherited hyperunconjugated bilirubinemia, with a total of 14 mutation sites identified, of which seven were confirmed mutations, and the frequency ranged from high to low: (TA)n accounted for 50%, c.211G>A (p.G71R) accounted for 49.10%, 1456T>G (p.Y486D) accounted for 16.96%, c.686C>A (p.R229W) accounted for 12.5%, 1091C>T (p.P364L) accounted for 8.04%, and c- 3279T>G accounted for 0.982%. Simultaneously, all patients had one to four mutations, of which only one mutation was the most common (55.36%), followed by two mutations (37.5%), and rare three and four mutations (5.36% and 1.78%). There was no statistical significance in total bilirubin (TBil) levels among the four groups (<i>F</i>=0.652, <i>P</i>=0.583). 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引用次数: 0

摘要

目的分析 UGT1A1 突变基因(包括增强子、启动子和 1-5 号外显子)的分布特征,进一步探讨遗传性高结合胆红素血症患者 UGT1A1 基因型与临床表型的相关性。研究方法回顾性分析2015年6月至2022年12月在南京市第二医院确诊的遗传性高结合胆红素血症患者。采用桑格测序法对所有患者的 UGT1A1 基因进行检测。对所有患者进行了全血细胞计数、肝功能和腹部影像学检查。使用χ(2)检验或Fisher百分位数检验比较分类变量数据。采用 t 检验比较正态分布的连续可变数据。结果112例(男女比例81:31,年龄9-70岁)遗传性高结合胆红素血症患者,共发现14个突变位点,其中7个为确证突变,突变频率由高到低依次为:(TA)n占50%,c.211G>A(p.G71R)占 49.10%,1456T>G(p.Y486D)占 16.96%,c.686C>A(p.R229W)占 12.5%,1091C>T(p.P364L)占 8.04%,c- 3279T>G占 0.982%。同时,所有患者都有一到四个突变,其中只有一个突变是最常见的(55.36%),其次是两个突变(37.5%),罕见的是三个和四个突变(5.36%和1.78%)。四组患者的总胆红素(TBil)水平无统计学意义(F=0.652,P=0.583)。在(TA)n和c.211G>A (p.G71R)中最常见的是一种突变,其中TA6/TA7(n=10)和TA7/TA7(n=14)突变对TBil有统计学意义(t=2.143,P=0.043)。c.211G>A(p.G71R)杂合子(9 个)和孤立突变(15 个)在 TBil 中无统计学意义(t=0.382,P=0.706)。GS组占75%,中间组占16.9%,CNS-Ⅱ组占8%。在 GS 组、中间组和 CNS-II 组中,突变 1(分别为 44 例、14 例和 4 例)和突变≥2(分别为 40 例、5 例和 5 例)之间的 TBil 在三组间具有统计学意义(F=270.992,Pχ(2)=3.317,P=0.19)。结论UGT1A1 基因突变位点的数量对遗传性高结合胆红素血症患者的 TBil 水平可能没有协同作用。TA7/TA7 突变并不罕见,TBil 水平相对较高。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
[Correlation between the mutation spectrum of the UGT1A1 gene and clinical phenotype in patients with inherited hyperunconjugated bilirubinemia].

Objective: To analyze the distribution characteristics of UGT1A1 mutant genes (including enhancers, promoters, and exons 1-5) and further explore the correlation between UGT1A1 genotype and clinical phenotypes in patients with inherited hyperunconjugated bilirubinemia. Methods: Patients diagnosed with hereditary hyperunconjugated bilirubinemia at Nanjing Second Hospital from June 2015 to December 2022 were retrospectively analyzed. The UGT1A1 gene was examined using Sanger sequencing in all patients. Complete blood count, liver function, and abdominal imaging examinations were performed. Comparison of categorical variable data using χ(2) testor Fisher percision tests. Comparison of continaous veriable data with normal distribution using t-test. Results: 112 cases (male:female ratio 81:31, aged 9-70 years) had inherited hyperunconjugated bilirubinemia, with a total of 14 mutation sites identified, of which seven were confirmed mutations, and the frequency ranged from high to low: (TA)n accounted for 50%, c.211G>A (p.G71R) accounted for 49.10%, 1456T>G (p.Y486D) accounted for 16.96%, c.686C>A (p.R229W) accounted for 12.5%, 1091C>T (p.P364L) accounted for 8.04%, and c- 3279T>G accounted for 0.982%. Simultaneously, all patients had one to four mutations, of which only one mutation was the most common (55.36%), followed by two mutations (37.5%), and rare three and four mutations (5.36% and 1.78%). There was no statistical significance in total bilirubin (TBil) levels among the four groups (F=0.652, P=0.583). One mutation was most common in (TA)n and c.211G>A (p.G71R), among which TA6/TA7 (n=10) and TA7/TA7 (n=14) mutations were statistically significant in TBil (t=2.143, P=0.043). The c.211G>A (p.G71R) heterozygous (n=9) and isolated (n=15) mutation had no statistical significance in TBil (t=0.382, P=0.706). The GS group accounted for 75%, the intermediate group accounted for 16.9%, and the CNS-Ⅱ group accounted for 8%. TBil was statistically significant among the three groups (F=270.992, P<0.001). There was no statistically significant difference (χ(2)=3.317, P=0.19) between mutation 1 (44 cases, 14 cases, and 4 cases, respectively) and mutations ≥ 2 (40 cases, 5 cases, and 5 cases, respectively) in the GS group, intermediate group, and CNS-II group. Conclusion: The number of UGT1A1 gene mutation sites may have no synergistic effect on TBil levels in patients with inherited hyperunconjugated bilirubinemia. TA7/TA7 mutations are not uncommon, and TBil levels are relatively high.

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中华肝脏病杂志
中华肝脏病杂志 Medicine-Medicine (all)
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