Acute polyneuropathy: a serious complication of levodopa/ /carbidopa intestinal gel treatment for Parkinson's Disease

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Authors	HAVRANKOVA Petra ROTH Jan CAPEK Vaclav KLEMPIR Jiri BALÁŽ Marek REKTOROVÁ Irena HAN Vladimir SKORVANEK Matej GMITTEROVA Karin MINAR Michal VALKOVIC Peter KAISEROVA Michaela KANOVSKY Petr GROFIK Milan KURCA Egon NECPAL Jan JECH Robert
Year of publication	2024
Type	Article in Periodical
Magazine / Source	Neurologia i neurochirurgia polska
MU Faculty or unit	Faculty of Medicine
Citation
web	https://journals.viamedica.pl/neurologia_neurochirurgia_polska/article/view/100132/80387
Doi	http://dx.doi.org/10.5603/pjnns.100132
Keywords	acute polyneuropathy; Parkinson's Disease; levodopa/carbidopa intestinal gel; levodopa equivalent daily dose
Description	Aim of study. To determine whether a high dose of levodopa-carbidopa intestinal gel (LCIG), expressed as levodopa equivalent daily dose (LE daily dose), is a risk factor for acute polyneuropathy in patients treated with LCIG. Clinical rationale for study. Treatment with LCIG is an effective device-assisted therapy in the advanced stages of Parkinson's Disease (PD). Polyneuropathy is a well-known complication of PD treatment. Patients treated with oral levodopa usually suffer from sub-clinical or mild chronic sensory polyneuropathy. However, severe acute polyneuropathy occurs in patients treated with LCIG, which is causally related to the treatment and leads to its immediate discontinuation.The etiology is not yet clear, but some patients with acute polyneuropathy have been given high doses of LCIG. Material and methods. A retrospective multicentre study of patients treated with LCIG was performed. Patients with acute polyneuropathy were subjected to a detailed analysis including statistical processing. Results. Of 183 patients treated with LCIG in seven centres, six patients (five females, median age 63 years) developed acute polyneuropathy with LCIG discontinuation.The median (interquartile range) initial and final LE daily dose in patients with and without acute polyneuropathy was 3,015 (2,695-3,184) and 1,898 (1,484-2,167) mg, respectively.The final LE daily dose of 2,605 mg cut-off had 83% sensitivity and 93% specificity for the prediction of acute polyneuropathy. Conclusions and clinical implications. The risk of acute polyneuropathy in LCIG-treated patients was associated with a daily LE dose of greater than 2,605 mg or with more than a 62% increase in the daily LE dose during LCIG treatment.
Related projects:	Národní ústav pro neurologický výzkum