Longitudinal Progression of Dysphagia in Huntington's Disease and Dentatorubral-Pallidoluysian Atrophy: ≥10 Years Retrospection in Twelve Patients
Journal Title: Biomedical Journal of Scientific & Technical Research (BJSTR) - Year 2018, Vol 9, Issue 4
Abstract
Huntington's disease (HD) and Dentatorubral-pallidoluysian atrophy (DRPLA) are progressive and currently incurable neurodegenerative diseases which shares common features such as choreic involuntary movements, dementia, psychosis, and pathologic expansion of triplet nucleotide repeats in the causative genes [1,2]. In HD, the prevalence of dysphagia is approximately 30 % and several reports have been examined the features [3-5]. In DRPLA, dysphagia can be clinically challenging considering a report that approximately 50 % of the DRPLA patients decease by aspiration pneumonia [6]. However, the data is scarce about the natural course of dysphagia in both HD and DRPLA in long term. Thereby, we examined the progression to clarify the features and to seek clues for potential treatments. Introduction We performed a retrospective chart-review of patients with HD (N=7) and DRPLA (N=5) whose swallowing function was examined at least once in our institution. The diagnosis of HD was made by simultaneous presence of following three features; a) Triad of movement abnormality (i.e. involuntary movement, especially chorea, and/or bradykinesia), cognitive dysfunction, and psychiatric symptoms, b) Atrophy of caudate in brain imaging, and c) Pathologic expansion of CAG repeats in HTT in their own or their families; if gene testing not done, presence of both (a) and (b) in their family members. DRPLA was diagnosed by; a) characteristic neurological symptoms/signs (e.g. chorea, epilepsy, ataxia, and psyhosis), b) atrophy of brainstem and/or cerebellum, with or without leukoencephalopathy in brain imaging, and c) mutation of ATN1 or family history, in the same way as HD above. The chart-review was concluded if the patients deceased, transferred to other institutions, or received percutaneous endoscopic gastrostomy (PEG). The onset of disease was defined as the initiation of movement abnormality, excluding the start of congnitive-psychiatric symptoms or epilepsy. The level of nutritional modification was reviewed to express the severity of dysphagia in the following five stages (the mildest: I, the severest: V); (I) unmodified, (II) partially modified (e.g. particular foods were minced), (III) pasted, (IV) high-caloric jelly, and (V) enteral feeding via PEG. The activity in daily lives (ADL), when they became wheelchair-bound and/or bedridden, was reviewed to express the systemic motor function. The result of video fluorography (VF), using liquid barium, was also reviewed. Owing to the small sample size, the continuous variables were expressed in median (range). In the background of HD (case 1-7) and DRPLA (case 8-12), the age at disease onset was 49 (26-57) and 27(10-38) year-old (yo), the disease duration was 19 (10-29) and 17 (12-25) year in the last examination, respectively (Table 1). All had involuntary movements, prevalently chorea. For the preceding non-motor symptoms, case 5 had cognitive decline and case 8, 10, and 12 had epilepsy. As the endpoints, case 2 and 12 deceased, case 3 transferred to another institution, case 4, 7, 8, 10, and 11 received PEG, and the rest survived by oral intake. If the data was missing or the test was not done, it was described as no data (ND), and pathological expansion of the triplet repeats without precise repeat number was described as Exp in Table 1. All of the gene mutation was heterozygous. 6 patients took haloperidol with the dose (mg/ day) of 4.5 in case 1, 3.0 in case 2, 4.5 in case 3, 0.375 in case 5, 1.5 in case 6, 1.0 in case 10. As to dysphagia, two (28.6 %) of HD and two (40 %) of DRPLA received PEG due to the disease progression in ≥10 year or longer disease duration, while case 11 received PEG due to brain infarction (annotated by * in Table 1). Plotting of longitudinal decline in swallowing function (Figure 1) suggested that younger disease onset and having DRPLA are potential risk factors of poorer functional prognosis, although the small sample size and absence of young-onset HD and elderly-onset DRPLA were undesirable for statistical analysis. The decline in ADL due to disease progression, with exception of case 6 who became wheelchair-bound by spinal compressive fracture (annotated by # in Table 1), seemed accompanying to the dysphagic progression with the lag within ±4 years. VF was evaluatable in 3 HD patients and 4 DRPLA patients, showing that insufficient mastication, impaired oropharyngeal transfer, delay in swallowing reflex, and aspiration in a certain number of patients. Swallowing whole foods (positivity: 66 % in HD and 75 % in DRPLA), and pharyngeal residue (positivity: 100 % in HD and 50 % in DRPLA) had relatively high prevalence in both groups. Notably, only case 10 experienced positional change from sitting position to reclining position in VF (Figure 2). The result was disappearance of aspiration (penetration of balium into the trachea: arrowhead) and pharyngeal residue (residue of balium in the pyriform sinus: arrow), as the fixation of his head and neck against choreic movement was ameliorated.
Authors and Affiliations
Hiroyuki Todo, Kengo Hasegawa, Keisuke Nishimoto, Katsuya Nishida, Naonobu Futamura
Keywords
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- EP ID EP598222
- DOI 10.26717/BJSTR.2018.09.001833
- Views 171
- Downloads 0
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