Department of Health Professions, Manchester Metropolitan University, Manchester, UK.
Int J Lang Commun Disord. 2012 Jan-Feb;47(1):106-11. doi: 10.1111/j.1460-6984.2011.00072.x. Epub 2011 Jun 20.
Mutations of mitochondrial DNA (mtDNA) cause a broad spectrum of clinical phenotypes. Anecdotal evidence suggests that voice and swallow problems are a common feature of these diseases.
To characterize accurately the prevalence and severity of voice and swallow problems in a large cohort of patients with mitochondrial disease.
METHODS & PROCEDURES: Patients with proven mitochondrial disease were sent validated questionnaires to assess both voice and swallow function. The presence of voice and swallow symptoms was correlated with other clinical features of mitochondrial disease in affected patients.
OUTCOMES & RESULTS: From the original 177 patients contacted, 98 swallowing status questionnaires and 96 Voice Handicap Index questionnaires were returned, response rates of 55% and 54%, respectively. Swallow: 48% of patients reported more difficulties with swallowing than control participants. Patients with single mtDNA deletions were most likely to report problems (65.2%), with patients with an m.8344A>G point mutation least likely (33.3%). All genotypes had a mean severity score in excess of the normal range, the highest mean score being found in the single large-scale mtDNA deletion group (10.12), the lowest in the m.3243A>G group (5.56) Voice; 48% of patients reported some difficulty with voice. Patients with single large-scale deletions showed the highest prevalence (65.2%), patients with the m.3243A>G mutation the lowest (33%). The most severe voice difficulties were reported by patients with an m.8344A>G point mutation. Patients with an m.3243A>G point mutation had the mildest and lowest incidence of voice problems. All genotypes scored outside of the normal range expected on the VHI overall (≥11.5 in control trials). Patients with an m.8344A>G point mutation reported a significantly higher degree of physical voice handicap than m.3243A>G patients (13.13 versus 4.40, p = 0.02). In patients with either single or multiple mtDNA deletions the likely pathophysiological mechanism is of proximal muscle weakness, whereas in patients with the m.8344A>G mutation cerebellar ataxia is the likely cause.
CONCLUSIONS & IMPLICATIONS: Dysphagia and dysarthria have been identified as symptoms in previous research, however the prevalence and pathophysiology of these symptoms have not been explored. This paper indicates that voice and swallow problems are a common, though predominantly mild feature of mitochondrial disease and that there is a core group of pathophysiological symptoms linked to the presence of voice and swallowing problems. This paper recommends early referral to speech and language therapists to identify emerging dysphonia and dysphagia and to provide appropriate intervention.
线粒体 DNA(mtDNA)突变导致广泛的临床表型。有传闻证据表明,声音和吞咽问题是这些疾病的常见特征。
准确描述大量线粒体疾病患者中声音和吞咽问题的患病率和严重程度。
将经过验证的问卷寄给已确诊的线粒体疾病患者,以评估他们的声音和吞咽功能。在受影响的患者中,将声音和吞咽症状的存在与线粒体疾病的其他临床特征相关联。
在最初联系的 177 名患者中,有 98 名患者返回了吞咽状态问卷,96 名患者返回了语音障碍指数问卷,回复率分别为 55%和 54%。吞咽:48%的患者报告说吞咽困难比对照组更严重。单一 mtDNA 缺失的患者最有可能报告有问题(65.2%),而 m.8344A>G 点突变的患者最不可能(33.3%)。所有基因型的平均严重程度评分均超过正常范围,单一大规模 mtDNA 缺失组的平均评分最高(10.12),m.3243A>G 组最低(5.56)。声音:48%的患者报告存在一些声音问题。单一大规模缺失的患者患病率最高(65.2%),m.3243A>G 突变的患者患病率最低(33%)。m.8344A>G 点突变的患者报告了最严重的声音困难。m.3243A>G 点突变的患者声音问题最轻微,发生率最低。所有基因型在 VHI 总体上的正常范围之外评分(对照组试验中≥11.5)。m.8344A>G 点突变的患者报告的身体声音障碍程度明显高于 m.3243A>G 患者(13.13 比 4.40,p=0.02)。在单一或多种 mtDNA 缺失的患者中,可能的病理生理机制是近端肌肉无力,而在 m.8344A>G 突变的患者中,可能的病理生理机制是小脑共济失调。
先前的研究已经确定了吞咽困难和构音障碍是这些疾病的症状,但这些症状的患病率和病理生理学尚未得到探讨。本文表明,声音和吞咽问题是线粒体疾病的常见症状,尽管主要是轻度的,但存在与声音和吞咽问题相关的核心组病理生理症状。本文建议尽早向言语治疗师转介,以发现新出现的发声困难和吞咽困难,并提供适当的干预。
