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英国生物库 26558 名参与者中 ABCA4 p.Asn1868lle 基因型对视网膜结构影响的分析

An Analysis of the Effect of ABCA4 p.Asn1868Ile Genotypes on Retinal Structure in 26,558 Participants in the UK Biobank.

机构信息

Institute of Ophthalmology, University College London, London, United Kingdom.

NIHR Biomedical Research Centre at Moorfields Eye Hospital NHS Foundation Trust and the UCL Institute of Ophthalmology, London, United Kingdom.

出版信息

Invest Ophthalmol Vis Sci. 2023 Jun 1;64(7):31. doi: 10.1167/iovs.64.7.31.

Abstract

PURPOSE

To determine whether the ABCA4 retinopathy-associated variant p.Asn1868Ile (c.5603A>T) is associated with retinal structure or subclinical disease among the general population.

METHODS

UK Biobank participants of European ancestry with available spectral-domain optical coherence tomography (OCT) passing quality control metrics and exome sequencing data were included. Regression analyses using both linear and recessive models tested for the association between the p.Asn1868Ile variant and total retinal thickness, clinically relevant segmented layer thicknesses, and visual acuity. Further regression analyses were performed with automated quality control metrics to determine if the p.Asn1868Ile variant is associated with poor quality or abnormal scans.

RESULTS

Retinal layer segmentation and sequencing data for the p.Asn1868Ile variant were available for 26,558 participants, following exclusions. We identified no significant association between the p.Asn1868Ile variant and retinal thickness, any of the segmented layers, or visual acuity. There was also no significant difference for homozygous p.Asn1868Ile when tested under the assumption of a recessive model. No association was identified for any of the quality control metrics, and a χ2 test showed that participants with the p.Asn1868Ile variant were not more likely to be excluded during quality control due to poor quality scans (P = 0.56).

CONCLUSIONS

The p.Asn1868Ile variant does not appear to affect the retinal structure or have pathogenic or subclinical effects on its own within the general population. The variant is likely to require other specific cis- or trans-acting modifying factors to cause ABCA4 retinopathy.

摘要

目的

确定 ABCA4 相关性视网膜炎相关变异 p.Asn1868Ile(c.5603A>T)是否与一般人群中的视网膜结构或亚临床疾病有关。

方法

纳入了具有可用光谱域光学相干断层扫描(OCT)通过质量控制指标和外显子组测序数据的英国生物银行欧洲血统参与者。使用线性和隐性模型的回归分析测试了 p.Asn1868Ile 变体与总视网膜厚度、临床相关分段层厚度和视力之间的关联。进一步的回归分析使用自动质量控制指标进行,以确定 p.Asn1868Ile 变体是否与质量差或异常扫描有关。

结果

排除后,共有 26558 名参与者可获得 p.Asn1868Ile 变体的视网膜层分段和测序数据。我们没有发现 p.Asn1868Ile 变体与视网膜厚度、任何分段层或视力之间存在显著关联。在隐性模型下测试时,杂合子 p.Asn1868Ile 也没有显著差异。没有发现任何质量控制指标存在关联,卡方检验显示,由于扫描质量差,携带 p.Asn1868Ile 变体的参与者在质量控制过程中被排除的可能性没有差异(P=0.56)。

结论

p.Asn1868Ile 变体似乎不会影响视网膜结构,也不会在一般人群中对其自身产生致病或亚临床影响。该变体可能需要其他特定的顺式或反式作用修饰因子才能引起 ABCA4 相关性视网膜炎。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/599b/10291893/2751f0863a58/iovs-64-7-31-f001.jpg

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