A Familial Case Study Exploring Craniofacial, Velopharyngeal, and Speech Variations in Pierre Robin Sequence

Q4 Health Professions
Katelyn J. Kotlarek, J. Kotlarek, P. J. Reitnauer, Jamie L. Perry
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引用次数: 2

Abstract

Pierre Robin sequence (PRS) describes a pattern of features present in an individual initially caused by underdevelopment of the mandible in utero [1]. This can lead to other features such as glossoptosis, cleft palate, feeding and breathing difficulties, and failure to thrive [2]. The incidence reported varies from 1:8,500 to 1:14,000 live births [3]. PRS may occur in isolation, but it is part of an underlying disorder or syndrome in approximately 50% of cases [4]. It is most commonly associated with Stickler syndrome [5], being diagnosed in 18-35% of individuals with PRS [4,6,7]. Stickler syndrome is a connective tissue disorder that can be associated with distinctive craniofacial features, eye problems, hearing impairment, mitral valve prolapse, and various skeletal and joint findings [4,8]. However, Stickler syndrome demonstrates wide variability in features leading to delayed or missed diagnoses in milder cases, even among individuals in the same family [8-10]. Despite variable expressivity, Stickler syndrome is completely penetrant. Three types of Stickler syndrome have been described based on collections of represented features. A diagnosis of Stickler syndrome is made clinically. Consensus has not been achieved on diagnostic criteria. However, non-validated criteria have been established for type 1 Stickler syndrome, which includes the presence of features, family history, and known pathogenic variants in autosomal A descriptive, prospective case study design was used to describe craniofacial, velopharyngeal, and speech measures of three siblings with a family history of Stickler syndrome. Two of the siblings had Pierre Robin sequence and cleft palate. All participants underwent nasometry, perceptual resonance rating, speech sound analysis, and magnetic resonance imaging. The child with a history of compensatory articulation errors showed notable differences in velopharyngeal function and medical history, as well as craniofacial and velopharyngeal dimensions when compared to siblings without a history of these speech errors. Further analysis of velopharyngeal and speech measures should be performed using a larger sample size within this population.
皮埃尔·罗宾序列颅面、腭咽及言语变异的家族个案研究
Pierre Robin序列(PRS)描述了一种最初由子宫内下颌骨发育不全引起的个体特征模式[1]。这可能会导致其他特征,如舌下垂、腭裂、进食和呼吸困难以及发育不良[2]。报告的活产发生率从1:8500到1:14000不等[3]。PRS可能单独发生,但在大约50%的病例中,它是潜在疾病或综合征的一部分[4]。它最常见于Stickler综合征[5],18-35%的PRS患者被诊断为该综合征[4,6,7]。Stickler综合征是一种结缔组织疾病,可与独特的颅面特征、眼部问题、听力障碍、二尖瓣脱垂以及各种骨骼和关节表现有关[4,8]。然而,Stickler综合征表现出广泛的特征变异性,导致较轻病例的延迟或漏诊,即使在同一家族的个体中也是如此[8-10]。尽管表现力各不相同,但Stickler综合征是完全渗透性的。Stickler综合征的三种类型已经根据所代表的特征集合进行了描述。Stickler综合征的临床诊断。在诊断标准方面尚未达成共识。然而,1型Stickler综合征的标准尚未得到验证,其中包括常染色体中是否存在特征、家族史和已知致病性变异。采用描述性前瞻性病例研究设计来描述三个有Stickler综合症家族史的兄弟姐妹的颅面、腭咽和言语测量。其中两个兄弟姐妹患有Pierre Robin序列和腭裂。所有参与者都接受了鼻测量、感知共振评级、语音分析和磁共振成像。与没有这些言语错误史的兄弟姐妹相比,有代偿性发音错误史的儿童在腭咽功能、病史以及颅面和腭咽尺寸方面表现出显著差异。应在该人群中使用更大的样本量对腭咽和语音测量进行进一步分析。
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来源期刊
Clinical Archives of Communication Disorders
Clinical Archives of Communication Disorders Health Professions-Speech and Hearing
CiteScore
0.50
自引率
0.00%
发文量
9
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