莱伯先天性黑蒙突变携带者的临床表型。
Clinical phenotypes in carriers of Leber congenital amaurosis mutations.
作者信息
Galvin Jennifer A, Fishman Gerald A, Stone Edwin M, Koenekoop Robert K
机构信息
Department of Ophthalmology and Visual Sciences, University of Illinois at Chicago, Chicago, Illinois 60612, USA.
出版信息
Ophthalmology. 2005 Feb;112(2):349-56. doi: 10.1016/j.ophtha.2004.08.023.
OBJECTIVE
To determine the clinical phenotypes in carriers with probable disease-causing sequence variations in 1 of 6 genes established to cause Leber congenital amaurosis (LCA).
DESIGN
Observational prospective comparative study.
PARTICIPANTS
Thirty carriers with various probable disease-causing sequence variations in 1 of 6 genes known to cause LCA.
METHODS
After the establishment of various disease-causing sequence variations in 37 (33.6%) of 110 patients with LCA, we examined a number of carriers who were either parents or offspring and who were willing to participate in our study. Evaluations included assessment of visual acuity, slit-lamp biomicroscopy, dilated fundus examination, and full-field electroretinogram (ERG) measurements.
MAIN OUTCOME MEASURES
Dilated fundus examination and full-field ERGs.
RESULTS
Of the 30 carriers with probable disease-causing sequence variations for LCA, 5 (16.7%) carriers had an AIPL1 variation, 4 (13.3%) CRB1, 0 (0%) CRX, 5 (16.7%) GUCY2D, 9 (30%) RPE65, and 7 (23.3%) carriers had a RPGRIP1 variation. Twenty-nine (96.7%) carriers had 20/20 or better visual acuity in their better seeing eye with correction. Drusenlike deposits were more selectively observed in carriers with mutations in the AIPL1, CRB1, RPE65, and RPGRIP1 genes, whereas mild peripheral chorioretinal atrophy was only observed in AIPL1 and RPE65 carriers. A reduced dark-adapted isolated rod ERG response and/or maximal combined cone and rod response was recorded in carriers with mutations in the AIPL1, GUCY2D, and RPGRIP1 genes. A reduced light-adapted ERG response to a single-flash and/or 32-Hz flicker was recorded in carriers with mutations in the AIPL1, CRB1, GUCY2D, and RPGRIP1 genes. Overall, our cohort of LCA carriers did not describe significant subjective visual difficulties, including nyctalopia and/or photosensitivity.
CONCLUSIONS
The variation of phenotypic expression in carriers among 5 LCA genotypes indicates that there is considerable phenotypic overlap. However, phenotypic trends were noted in carriers' fundus findings and ERG responses for each genetic subtype. Observations of phenotypic associations with specific disease-causing sequence variations in carriers have potential practical value for molecular screening strategies of patients with LCA.
目的
确定在已证实可导致莱伯先天性黑蒙(LCA)的6个基因中,携带可能致病序列变异的携带者的临床表型。
设计
观察性前瞻性比较研究。
参与者
30名携带者,他们在已知可导致LCA的6个基因中的1个基因上存在各种可能致病的序列变异。
方法
在110例LCA患者中的37例(33.6%)确定了各种致病序列变异后,我们检查了一些携带者,他们是父母或后代,并且愿意参与我们的研究。评估包括视力评估、裂隙灯生物显微镜检查、散瞳眼底检查和全视野视网膜电图(ERG)测量。
主要观察指标
散瞳眼底检查和全视野ERG。
结果
在30例携带可能导致LCA的致病序列变异的携带者中,5例(16.7%)携带者存在AIPL1变异,4例(13.3%)存在CRB1变异,0例(0%)存在CRX变异,5例(16.7%)存在GUCY2D变异,9例(30%)存在RPE65变异,7例(23.3%)携带者存在RPGRIP1变异。29例(96.7%)携带者矫正后较好眼的视力为20/20或更好。在携带AIPL1、CRB1、RPE65和RPGRIP1基因突变的携带者中更有选择性地观察到玻璃膜疣样沉积物,而仅在携带AIPL1和RPE65基因变异的携带者中观察到轻度周边脉络膜视网膜萎缩。在携带AIPL1、GUCY2D和RPGRIP1基因突变的携带者中记录到暗适应分离视杆细胞ERG反应和/或最大联合视锥和视杆细胞反应降低。在携带AIPL1、CRB1、GUCY2D和RPGRIP1基因突变的携带者中记录到对单次闪光和/或32赫兹闪烁光适应ERG反应降低。总体而言,我们的LCA携带者队列没有描述明显的主观视觉困难,包括夜盲和/或光敏性。
结论
5种LCA基因型携带者的表型表达存在差异,表明存在相当大的表型重叠。然而,在每个基因亚型的携带者眼底检查结果和ERG反应中注意到了表型趋势。观察携带者中与特定致病序列变异相关的表型对于LCA患者的分子筛查策略具有潜在的实用价值。
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