Role of pathogenetic therapy for diabetic polyneuropathy

D. A. Iskra; V. V. Kovalchuk; E. R. Barantsevich

doi:10.14412/2074-2711-2021-1-44-50

Неврология, нейропсихиатрия, психосоматика (Feb 2021)

Role of pathogenetic therapy for diabetic polyneuropathy

D. A. Iskra,
V. V. Kovalchuk,
E. R. Barantsevich

Affiliations

D. A. Iskra: Saint Petersburg State Pediatric Medical University, Ministry of Health of Russia
V. V. Kovalchuk: Saint Petersburg Center of Medical Rehabilitation, N.A. Semashko City Hospital Thirty-Eight
E. R. Barantsevich: Acad. I.P. Pavlov First Saint Petersburg State Medical University, Ministry of Health of Russia

DOI: https://doi.org/10.14412/2074-2711-2021-1-44-50
Journal volume & issue: Vol. 13, no. 1
pp. 44 – 50

Abstract

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In our country, alpha-lipoic acid is widely used as a pathogenetic therapy for diabetic polyneuropathy (DPN).Objective: to compare the efficiency and safety of using oral and injectable α-lipoic acid for DPN.Patients and methods. The investigation enrolled 47 patients with a verified diagnosis of DPN, who were divided into two groups. Group 1 included 23 patients (10 men and 13 women; mean age, 62.9±7.5 years), Group 2 consisted of 24 patients (9 men and 15 women, mean age, 65.5±7.9 years). All the patients used Berlithione: Group 1 received its intravenous doses of 600 mg for 14 days, then oral ones of 600 mg for other 16 days; Group 2 took oral doses of 600 mg for 30 days. The therapy results were assessed using the digital rating scale (DRS), the Douleur Neuropathique 4 (DN4) neuropathic pain rating scale, and the neurological soft signs (NSS), and electroneuromyography (ENMG) data.Results and discussion. Berlithione was found to have a good tolerability. No adverse reactions were detected in any case; and there was no need to discontinue this drug. On day 21 of therapy, there were statistically significant differences in the indicators of pain intensity on DRS in Group 1 patients (p<0.05), some of them (n=8) had positive clinical changes as a reduction in the severity of hypesthesia. Both groups showed a tendency to improve ENMG parameters as a certain increase in excitation propagation velocity and M-response amplitude; however, these changes did not reach a statistical significance level. At the same time, in 6 out of the 8 patients in Group 1 with positive clinical changes, the described ENMG changes correlated with a reduction in the severity of hypesthesia. There were no significant changes on the NSS scale after 3 weeks of therapy. On day 30 of treatment, both groups were recorded to have statistically significant changes in pain intensity measures versus the baseline values, but no significant inter-group differences.Conclusion. Thus, Berlithione demonstrated its efficacy in both patient groups, but its positive effect occurred 1 week earlier in the step therapy group. It is noted that it is expedient to use this drug long (>1 month) for DPN.

Published in Неврология, нейропсихиатрия, психосоматика

ISSN: 2074-2711 (Print); 2310-1342 (Online)
Publisher: IMA-PRESS LLC
Country of publisher: Russian Federation
LCC subjects: Medicine: Internal medicine: Neurosciences. Biological psychiatry. Neuropsychiatry: Neurology. Diseases of the nervous system
Website: http://nnp.ima-press.net/index.php/nnp

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