Angeli Simon I
Department of Otolaryngology, University of Miami Ear Institute, University of Miami Miller School of Medicine, Miami, Florida 33136, USA.
Laryngoscope. 2008 Nov;118(11):2014-23. doi: 10.1097/MLG.0b013e31817fb7ad.
OBJECTIVES/HYPOTHESIS: The aim of this study was to 1) determine the prevalence of DFNB1 in a cohort of children with prelingual nonsyndromic sensorineural hearing loss (HL), 2) study phenotype/genotype correlations, and 3) establish guidelines for genetic counseling of DFNB1.
Prospective cohort study.
A total of 119 unrelated children (107 sporadic and 12 familial cases) with prelingual nonsyndromic HL underwent mutational screening for DFNB1 in the noncoding and coding exons of GJB2, in addition to the del(GJB6-D13S1830) mutation of GJB6. Information regarding demographics, HL, developmental milestones, inner ear high resolution computed tomography, hearing habilitation, and associated phenotypic manifestations were collected in probands with biallelic pathogenic mutations.
The prevalence of DFNB1 in cases of prelingual nonsyndromic HL was 26% (25% in sporadic and 50% in familial cases). In regards to ethnicity, 19 probands were white and 12 probands of Hispanic ancestry had a mixed racial origin (black, Native-American, white). Greater allelic heterogeneity was shown with Hispanics of mixed descent exhibiting 10 of 12 GJB2 allelic variants, whereas whites had 4 of 10 allelic variants (Fisher exact test, P = .033); both ethnic groups had theGJB6 deletion. The frequency of deaf carriers of the most commonly found mutation (c.35delG) was 8% and higher than that of expected for the general population (Fisher exact test, P = .015). The hearing phenotype was variable in terms of degree of impairment (from mild to profound), onset, symmetry and progression, and there was no correlation with any specific genotype class. DFNB1 probands had normal gross motor development, and the frequency of computed tomography abnormalities of the inner ear was low at 8%. No other specific associated phenotypic manifestations were identified.
DFNB1 is the most common identifiable etiology of nonsyndromic prelingual deafness both in sporadic and familial cases in this cohort with ethnic diversity. The greater allelic variability observed in Hispanics and the high frequency of deaf probands carrying a single allelic variant of DFNB1 support extending the screening to noncoding regions of GJB2 and to the remaining DFNB1 locus. Most probands have a congenital HL that is stable, symmetrical and without associated manifestations, but the audiometric profile should not be the only criteria for offering mutational screening of DFNB1 because of the observed variability. These data can be applied to direct the clinical evaluation and effectively counsel families of children with DFNB1.
目的/假设:本研究的目的是:1)确定一组语前非综合征性感音神经性听力损失(HL)儿童中DFNB1的患病率;2)研究表型/基因型相关性;3)制定DFNB1遗传咨询指南。
前瞻性队列研究。
总共119名语前非综合征性HL的非亲缘儿童(107例散发病例和12例家族病例),除了对GJB6的del(GJB6-D13S1830)突变进行检测外,还对GJB2的非编码和编码外显子进行了DFNB1的突变筛查。收集了双等位基因致病性突变先证者的人口统计学、HL、发育里程碑、内耳高分辨率计算机断层扫描、听力康复及相关表型表现等信息。
语前非综合征性HL病例中DFNB1的患病率为26%(散发病例中为25%,家族病例中为50%)。在种族方面,19名先证者为白人,12名西班牙裔血统的先证者有混合种族背景(黑人﹑美洲原住民、白人)。混血西班牙裔显示出更大的等位基因异质性,12个GJB2等位基因变体中有10个,而白人10个等位基因变体中有4个(Fisher精确检验,P = 0.033);两个种族群体均存在GJB6缺失。最常见突变(c.35delG)的聋性携带者频率为8%,高于一般人群预期频率(Fisher精确检验,P = 0.015)。听力表型在损伤程度(从轻度到重度)、发病、对称性和进展方面存在差异,且与任何特定基因型类别均无相关性。DFNB1先证者的粗大运动发育正常,内耳计算机断层扫描异常频率较低,为8%。未发现其他特定的相关表型表现。
在这个具有种族多样性的队列中,DFNB1是散发病例和家族病例中语前非综合征性耳聋最常见的可识别病因。在西班牙裔中观察到的更大等位基因变异性以及携带DFNB1单等位基因变体的聋性先证者的高频率,支持将筛查扩展到GJB2的非编码区域和其余DFNB1基因座。大多数先证者患有先天性HL,其稳定、对称且无相关表现,但由于观察到的变异性,听力测定结果不应是进行DFNB1突变筛查的唯一标准。这些数据可用于指导临床评估并有效地为DFNB1患儿家庭提供咨询。
