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3. Crucial functions of alpha-actinin 2 in the embryonic heart

Author

Gehmlich, K, primary, Jiang, A, additional, Wadmore, K, additional, Hooper, C, additional, Douglas, G, additional, Ehler, E, additional, Broadway-Stringer, S, additional, Kalisch-Smith, J, additional, Sparrow, D, additional, Gautel, M, additional, Davies, B, additional, and Watkins, H, additional

Published
2022
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10. INTEREST IN CD2, a global patient-centred study of long-term cervical dystonia treatment with botulinum toxin

Author

Misra, Vijay P., Colosimo, Carlo, Charles, David, Chung, Tae Mo, Maisonobe, Pascal, Om, Savary, Abdulnayef, A., Adatepe, N. U., Araujo Leite, M. A., Badarny, S., Bajenaru, O., Bares, M., Bejjani, P., Bergmans, B., Bhidayasiri, R., Bozic, H., Cardoso Costa, F. E., Carlstrom, C., Castelnovo, G., Chang, M. H., Chang, Y. Y., Coletti-Moja, M., Delvaux, V., Dioszhegy, P., Dogu, O., Duzynski, W., Ehler, E., Espinosa Sierra, L., Fabbrini, G., Ferreira, J., Ferreira Valadas, A., Foresti, C., Girlanda, P., Goh, K. J., Graca Velon, A., Grill, S., Gurevitch, T., Hadidi, M., Hamimed, M. A., Hamri, A., Harrower, T., Hassin, S., Hedera, P., Hernandez, J. F. J. G., Hernandez Franco, J., Ho, B., Ho, S. L., Hughes, A., Ilic, T., Inshasi, J. S., Ip, C. W., Jamieson, S., Jamora, R. D. G., Jech, R., Jeon, B. S., Kaminska, A., Karpova, M., Khasanova, D., Kim, J. M., Kim, J. W., Kok, C. Y., Korenko, A., Korv, J., Koussa, S., Kovacs, T., Kreisler, A., Krystkowiak, P., Kumthornthip, W., Lin, C. H., Lundin, F., Lus, G., Magalhaes, M., Masmoudi, A. N., Mercelis, R., Misbahuddin, A., Moebius, C., Mohammadi, B., Nazem, B., Ng, K., Nurlu, G., Nyberg, J., Nyholm, D., Ochudlo, S., Otruba, P., Pfister, R., Pirtosek, Z., Pokhabov, D., Quinones Aguilar, S., Quinones Canales, G., Raghev, S., Rickmann, H., Romano, M., Rosales, R. L., Rubanovits, I., Santilli, V., Schoels, L., Simonetta-Moreau, M., Simu, M. A., Sohn, Y. H., Soulayrol, S., Supe, I., Svetel, M., Sycha, T., Tan, E. K., Timerbaeva, S., Tokcaer, A. B., Trosch, R., Tugnoli, V., Tumas, V., van der Linden, C., Vetra, A., Vial, C., Vidry, E., Williams, D., Wimalaratna, S., Yiannikas, C., Misra, Vijay P., Colosimo, Carlo, Charles, David, Chung, Tae Mo, Maisonobe, Pascal, Om, Savary, Abdulnayef, A., Adatepe, N. U., Araujo Leite, M. A., Badarny, S., Bajenaru, O., Bares, M., Bejjani, P., Bergmans, B., Bhidayasiri, R., Bozic, H., Cardoso Costa, F. E., Carlstrom, C., Castelnovo, G., Chang, M. H., Chang, Y. Y., Coletti-Moja, M., Delvaux, V., Dioszhegy, P., Dogu, O., Duzynski, W., Ehler, E., Espinosa Sierra, L., Fabbrini, G., Ferreira, J., Ferreira Valadas, A., Foresti, C., Girlanda, P., Goh, K. J., Graca Velon, A., Grill, S., Gurevitch, T., Hadidi, M., Hamimed, M. A., Hamri, A., Harrower, T., Hassin, S., Hedera, P., Hernandez, J. F. J. G., Hernandez Franco, J., Ho, B., Ho, S. L., Hughes, A., Ilic, T., Inshasi, J. S., Ip, C. W., Jamieson, S., Jamora, R. D. G., Jech, R., Jeon, B. S., Kaminska, A., Karpova, M., Khasanova, D., Kim, J. M., Kim, J. W., Kok, C. Y., Korenko, A., Korv, J., Koussa, S., Kovacs, T., Kreisler, A., Krystkowiak, P., Kumthornthip, W., Lin, C. H., Lundin, F., Lus, G., Magalhaes, M., Masmoudi, A. N., Mercelis, R., Misbahuddin, A., Moebius, C., Mohammadi, B., Nazem, B., Ng, K., Nurlu, G., Nyberg, J., Nyholm, D., Ochudlo, S., Otruba, P., Pfister, R., Pirtosek, Z., Pokhabov, D., Quinones Aguilar, S., Quinones Canales, G., Raghev, S., Rickmann, H., Romano, M., Rosales, R. L., Rubanovits, I., Santilli, V., Schoels, L., Simonetta-Moreau, M., Simu, M. A., Sohn, Y. H., Soulayrol, S., Supe, I., Svetel, M., Sycha, T., Tan, E. K., Timerbaeva, S., Tokcaer, A. B., Trosch, R., Tugnoli, V., Tumas, V., van der Linden, C., Vetra, A., Vial, C., Vidry, E., Williams, D., Wimalaratna, S., and Yiannikas, C.

Subjects
Male, Neurology, SATISFACTION, International Cooperation, Cohort Studies, 0302 clinical medicine, QUALITY-OF-LIFE, Botulinum toxin, Observational study, Tremor, Epidemiology, 030212 general & internal medicine, Cervical dystonia, Botulinum Toxins, Type A, Torticollis, Neuroradiology, BLEPHAROSPASM, education.field_of_study, Original Communication, INTEREST IN CD2 study group, Middle Aged, Treatment Outcome, Neuromuscular Agents, Female, Life Sciences & Biomedicine, medicine.drug, Adult, medicine.medical_specialty, Population, Clinical Neurology, DIAGNOSIS, 03 medical and health sciences, Patient satisfaction, Neurology (clinical), Internal medicine, medicine, Humans, education, Aged, Science & Technology, Neurology & Neurosurgery, Electromyography, GUIDANCE, business.industry, 1103 Clinical Sciences, medicine.disease, NEUROTOXIN, REGISTRY, UPDATE, Neurosciences & Neurology, 1109 Neurosciences, business, 030217 neurology & neurosurgery
Abstract

Background Longitudinal cohort studies provide important information about the clinical effectiveness of an intervention in the routine clinical setting, and are an opportunity to understand how a population presents for treatment and is managed. Methods INTEREST IN CD2 (NCT01753349) is a prospective, international, 3-year, longitudinal, observational study following the course of adult idiopathic cervical dystonia (CD) treated with botulinum neurotoxin type A (BoNT-A). The primary objective is to document long-term patient satisfaction with BoNT-A treatment. Here we report baseline data. Results This analysis includes 1036 subjects (67.4% of subjects were female; mean age was 54.7 years old; mean TWSTRS Total score was 31.7). BoNT-A injections were usually given in line with BoNT-A prescribing information. The most commonly injected muscles were splenius capitis (87.3%), sternocleidomastoid (82.6%), trapezius (64.3%), levator scapulae (40.9%) and semispinalis capitis (26.9%); 35.5% of subjects were injected using a guidance technique. Most subjects (87.8%) had been previously treated with BoNT-A (median interval between last pre-study injection and study baseline was 4 months); of these 84.8% reported satisfaction with BoNT-A treatment at peak effect during their previous treatment cycle and 51.5% remained satisfied at the end of the treatment. Analyses by geographical region revealed heterogeneity in the clinical characteristics and BoNT-A injection practice of CD subjects presenting for routine treatment. Conclusions These baseline analyses provide sizeable data regarding the epidemiology and clinical presentation of CD, and demonstrate an international heterogeneity of clinical practice. Future longitudinal analyses of the full 3-year study will explore how these factors impact treatment satisfaction. Electronic supplementary material The online version of this article (10.1007/s00415-017-8698-2) contains supplementary material, which is available to authorized users.

Published
2017
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14. Onemocnění bederní páteře - nová neurologická nemoc z povolání.

Author

Ehler, E., Nakládalová, M., Heřman, M., and Urban, P.

Subjects
*OCCUPATIONAL diseases, *LUMBAR pain, *LUMBAR vertebrae, *NEUROLOGISTS, *GOVERNMENT regulation, *LUMBAR vertebrae diseases
Abstract

Minimonography describes the algorithm of the assessment and acknowledgment of the new occupational disease: "chronic lumbar spine disorder caused by heavy physical work," focusing on the role of a neurologist in this process. The new item has been added to the List of Occupational Diseases by Government Regulation No. 506/2021 Coll. From January 1st, 2023, the illness can be acknowledged and compensated as an occupational disease. However, the necessary prerequisite is the fulfillment of strict assessment standards, which include both clinical and hygienic criteria. The neurologist plays a partial, but significant role in the assessment whether the criteria have been met. Neurologist does not decide whether it is or it is not an occupational disease. Neurologist´s role is to judge if the patient's disease corresponds to the diagnosis in question, i.e., the chronic lumbar spine disorder having the form of Low Back Pain with and/or without a radicular syndrome. Making the differential diagnosis, neurologist has to rule out other significant causes of the patient's difficulties. Using seven defined parameters of the neurological examination, neurologist rates the severity of the disease and decides whether it reaches the required degree with respect to the patient's age. Only if the neurological criteria are met, the acknowledgment of the occupational disease comes into consideration. This is a necessary condition – but it is still inadequate. [ABSTRACT FROM AUTHOR]

Published
2022

17. Mild traumatic brain injury

Author

Vos, P. E., Alekseenko, Y., Battistin, L., Ehler, E., Gerstenbrand, F., Muresanu, D. F., Potapov, A., Stepan, C. A., Traubner, P., Vecsei, L., and von Wild, K.

Published
2012
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18. Totální locked-in syndrom u nemocného s těžkou formou akutní polyradikuloneuritidy.

Author

Prax, T., Drlík, J., Ungermann, L., and Ehler, E.

Subjects
AUDITORY evoked response, NEUROMYELITIS optica, ELECTROENCEPHALOGRAPHY, DIABETES, ATORVASTATIN
Abstract

Pri prijetí mel dysartrickou, tichou a srozumitelnou rec, izokorii, bez poruchy okulomotoriky, snízené korneální reflexy, plossí mimiku vlevo, krátce nadzvedl hlavu nad podlozku, jen velmi omezene zvedl patrové oblouky bilaterálne, nesvedl elevaci horních koncetin (HK) nad podlozku, stisk jen naznacen, u DK pouze náznak pohybu v kycelních kloubech, RR C5-8, L2-S2 vyhaslé, s difuzní poruchou cití HK i DK. První zemrel po 6 tydnech a druhy po 3 tydnech po období umelé ventilace s vysazením sedace, kdy kontakt byl mozny pomocí funkcní MR. Byla provedena MR hlavy s následujícími sekvencemi: v axiální rovine T2 vázené obrazy, fluid attenuated inversion recovery (FLAIR), suscetibilne vázené obrazy (susceptibility weighted images; SWI) a difuzí vázené obrazy (diffusion weighted images; DWI); v sagitální rovine T1 vázené obrazy; v koronární rovine FLAIR obrazy. [Extracted from the article]

Published
2023

19. How satisfied are cervical dystonia patients after 3 years of botulinum toxin type A treatment? Results from a prospective, long-term observational study

Author

Colosimo, C, Charles, D, Misra, VP, Maisonobe, P, Om, S, Abdulnayef, A, Adatepe, NU, Leite, AMA, Badarny, S, Bajenaru, O, Bares, M, Bejjani, P, Bergmans, B, Bhidayasiri, R, Bozic, H, Costa, CFE, Carlstrom, C, Castelnovo, G, Chang, MH, Chang, YY, Chung, TM, Coletti-Moja, M, Delvaux, V, Dioszhegy, P, Dogu, O, Duzynski, W, Ehler, E, Sierra, EL, Fabbrini, G, Ferreira, J, Valadas, FA, Foresti, C, Girlanda, P, Goh, KJ, Velon, GA, Grill, S, Gurevitch, T, Hadidi, M, Hamimed, MA, Hamri, A, Harrower, T, Hassin, S, Hedera, P, Hernandez, JFJG, Franco, HJ, Ho, B, Ho, SL, Hughes, A, Ilic, T, Inshasi, JS, Ip, CW, Jamieson, S, Jamora, RDG, Jech, R, Jeon, BS, Kaminska, A, Karpova, M, Khasanova, D, Kim, JM, Kim, JW, Kok, CY, Korenko, A, Korv, J, Koussa, S, Kovacs, T, Kreisler, A, Krystkowiak, P, Kumthornthip, W, Lin, CH, Lundin, F, Lus, G, Magalhaes, M, Masmoudi, AN, Mercelis, R, Misbahuddin, A, Moebius, C, Mohammadi, B, Nazem, B, Ng, K, Nurlu, G, Nyberg, J, Nyholm, D, Ochudlo, S, Otruba, P, Pfister, R, Pirtosek, Z, Pokhabov, D, Aguilar, QS, Canales, QG, Raghev, S, Rickmann, H, Romano, M, Rosales, RL, Rubanovits, I, Santilli, V, Schoels, L, Simonetta-Moreau, M, Ma, S, Sohn, YH, Soulayrol, S, Supe, I, Svetel, M, Sycha, T, Tan, EK, Timerbaeva, S, Tokcaer, AB, Trosch, R, Tugnoli, V, Tumas, V, Van der Linden, C, Vetra, A, Vial, C, Vidry, E, Williams, D, Wimalaratna, S, and Yiannikas, C

Subjects
0301 basic medicine, Male, Pediatrics, Neurology, SATISFACTION, Botulinum toxin, Cervical dystonia, Observational study, Satisfaction, Treatment, 0302 clinical medicine, QUALITY-OF-LIFE, Outcome Assessment, Health Care, Prospective Studies, Botulinum Toxins, Type A, Torticollis, Neuroradiology, BLEPHAROSPASM, INTEREST IN CD2 study group, Middle Aged, Neuromuscular Agents, Patient Satisfaction, SAFETY, Female, Life Sciences & Biomedicine, medicine.drug, Adult, medicine.medical_specialty, Adolescent, MEDLINE, Clinical Neurology, Treatment results, DIAGNOSIS, 03 medical and health sciences, Young Adult, medicine, Humans, Aged, Science & Technology, Neurology & Neurosurgery, business.industry, Correction, 1103 Clinical Sciences, medicine.disease, EFFICACY, 030104 developmental biology, Neurology (clinical), Neurosciences & Neurology, business, FOLLOW-UP, 1109 Neurosciences, 030217 neurology & neurosurgery, Botulinum toxin type
Abstract

Background Patients with cervical dystonia (CD) typically require regular injections of botulinum toxin to maintain symptomatic control. We aimed to document long-term patient satisfaction with CD symptom control in a large cohort of patients treated in routine practice. Methods This was a prospective, international, observational study (NCT01753349) following the course of adult CD treated with botulinum neurotoxin type A (BoNT-A) over 3 years. A comprehensive clinical assessment status was performed at each injection visit and subjects reported satisfaction in two ways: satisfaction with symptom control at peak effect and at the end of treatment cycle. Results Subject satisfaction remained relatively stable from the first to the last injection visit. At 3 years, 89.9% of subjects reported satisfaction with symptom control at peak effect and 55.6% reported satisfaction with symptom control at end of treatment cycle. By contrast, objective ratings of CD severity showed an overall reduction over 3 years. Mean ± SD Toronto Western Spasmodic Rating Scale (TWSTRS) Total scores (clinician assessed at end of treatment cycle) decreased from 31.59 ± 13.04 at baseline to 24.49 ± 12.43 at 3 years (mean ± SD reduction from baseline of − 6.97 ± 11.56 points). Tsui scale scores also showed gradual improvement; the percent of subjects with a tremor component score of 4 reduced from 12.4% at baseline to 8.1% at 3 years. Conclusions Despite objective clinical improvements over 3 years, subject satisfaction with symptom control remained relatively constant, indicating that factors other than symptom control also play a role in patient satisfaction.

Published
2019

24. The M-band:The underestimated part of the sarcomere

Author

Lange, S., Pinotsis, Nikos, Agarkova, I., and Ehler, E.

Subjects
Sarcomeres, Serum Response Factor, Transcription, Genetic, Cardiomyopathy, Sarcomere, Myosins, bcs, Article, Actins, Myomesin, Myofibrils, Humans, Connectin, Obscurin, Cytoskeleton, Muscle Contraction
Abstract

The sarcomere is the basic unit of the myofibrils, which mediate skeletal and cardiac Muscle contraction. Two transverse structures, the Z-disc and the M-band, anchor the thin (actin and associated proteins) and thick (myosin and associated proteins) filaments to the elastic filament system composed of titin. A plethora of proteins are known to be integral or associated proteins of the Z-disc and its structural and signalling role in muscle is better understood, while the molecular constituents of the M-band and its function are less well defined. Evidence discussed here suggests that the M-band is important for managing force imbalances during active muscle contraction. Its molecular composition is fine-tuned, especially as far as the structural linkers encoded by members of the myomesin family are concerned and depends on the specific mechanical characteristics of each particular muscle fibre type. Muscle activity signals from the M-band to the nucleus and affects transcription of sarcomeric genes, especially via serum response factor (SRF). Due to its important role as shock absorber in contracting muscle, the M-band is also more and more recognised as a contributor to muscle disease., Highlights • This article reviews the structure, composition and function of the M-band, the central structure of the sarcomere, the basic unit of a myofibril. • In addition, signalling pathways emanating from the M-band, which may affect protein turnover from triggering transcription (via SRF) to promoting degradation are discussed. • A particular strength of the review is the links that it provides throughout the text to disease.

Published
2019
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27. COVID-19 u nemocných s myasthenia gravis.

Author

Ehler, E., Medová, N., Wurst, Z., Peisker, T., Vaško, P., and Štětkářová, I.

Abstract

Various infections can frequently lead to the exacerbation of myasthenia gravis (MG). COVID- 19 infection characterized by lung impairment with respiration failure, massive inflammatory reaction and high mortality may lead to worsening of many neuromuscular disorders including MG. Published series of patients with MG and COVID-19 are considerably variable and diff er in disease severity and selected therapeutic approach. In our group of 11 MG patients, substantial worsening was present in 3 patients, and in 4 there was a mild worsening of clinical myasthenic symptoms. In 3 patients, we used high doses of methylprednisolone intravenously, in 2 patients, the oral doses of prednisone were increased to 40 mg/ 60 mg a day, 1 patient was treated with intravenous immunoglobulin (2 g/ kg), and 1 was treated with remdesivir. An 88-year-old woman was diagnosed with MG after COVID-19 infection. A 77-year-old man died after 6 days of mechanical ventilation. COVID-19 infection leads to an exacerbation of clinical symptoms in a large proportion of MG patients with ventilation disorder due to increased muscle fatigue and inflammatory changes in the lung parenchyma. [ABSTRACT FROM AUTHOR]

Published
2021
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33. Combination of Whole Genome Sequencing, Linkage, and Functional Studies Implicates a Missense Mutation in Titin as a Cause of Autosomal Dominant Cardiomyopathy with Features of Left Ventricular Noncompaction

Author

Hastings R, Cp, Villiers, Hooper C, Elizabeth Ormondroyd, Pagnamenta A, Lise S, Salatino S, Sj, Knight, Jc, Taylor, Kl, Thomson, Arnold L, Sd, Chatziefthimiou, Pv, Konarev, Wilmanns M, Ehler E, Ghisleni A, Gautel M, Blair E, Watkins H, and Gehmlich K

Subjects
whole genome sequencing, missense mutation, left ventricular noncompaction, titin, cardiomyopathy, telethonin
Abstract

Background—High throughput next generation sequencing techniques have made whole genome sequencing accessible in clinical practice, however, the abundance of variation in the human genomes makes the identification of a disease-causing mutation on a background of benign rare variants challenging. Methods and Results—Here we combine whole genome sequencing with linkage analysis in a three-generation family affected by cardiomyopathy with features of autosomal dominant left-ventricular non-compaction cardiomyopathy. A missense mutation in the giant protein titin is the only plausible disease-causing variant that segregates with disease amongst the eight surviving affected individuals, with interrogation of the entire genome excluding other potential causes. This A178D missense mutation, affecting a conserved residue in the second immunoglobulin-like domain of titin, was introduced in a bacterially expressed recombinant protein fragment and biophysically characterised in comparison to its wild-type counterpart. Multiple experiments, including size exclusion chromatography, small angle X-ray scattering and circular dichroism spectroscopy suggest partial unfolding and domain destabilisation in the presence of the mutation. Moreover, binding experiments in mammalian cells show that the mutation markedly impairs binding to the titin ligand telethonin. Conclusions—Here we present genetic and functional evidence implicating the novel A178D missense mutation in titin as the cause of a highly penetrant familial cardiomyopathy with features of left-ventricular non-compaction. This expands the spectrum of titin's roles in cardiomyopathies. It furthermore highlights that rare titin missense variants, currently often ignored or left un-interpreted, should be considered to be relevant for cardiomyopathies and can be identified by the approach presented here.

Published
2016
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34. MLP and CARP are linked to chronic PKCα signalling in dilated cardiomyopathy

Author

Gehmlich, K, Lange, S, Lun, A, Blondelle, J, Hooper, C, Dalton, N, Alvarez, E, Zhang, X, Bang, M, Abassi, Y, dos Remedios, C, Peterson, K, Chen, J, and Ehler, E

Subjects
Male, Heart Failure, Protein Kinase C-alpha, Cardiomyopathy, Science, Muscle Proteins, Nuclear Proteins, LIM Domain Proteins, Cardiovascular, Cell Line, Repressor Proteins, Mice, Heart Disease, Gene Expression Regulation, COS Cells, Dilated, Chlorocebus aethiops, Escherichia coli, 2.1 Biological and endogenous factors, Animals, Humans, Aetiology, Signal Transduction
Abstract

MLP (muscle LIM protein)-deficient mice count among the first mouse models for dilated cardiomyopathy (DCM), yet the exact role of MLP in cardiac signalling processes is still enigmatic. Elevated PKCα signalling activity is known to be an important contributor to heart failure. Here we show that MLP directly inhibits the activity of PKCα. In end-stage DCM, PKCα is concentrated at the intercalated disc of cardiomyocytes, where it is sequestered by the adaptor protein CARP in a multiprotein complex together with PLCβ1. In mice deficient for both MLP and CARP the chronic PKCα signalling chain at the intercalated disc is broken and they remain healthy. Our results suggest that the main role of MLP in heart lies in the direct inhibition of PKCα and that chronic uninhibited PKCα activity at the intercalated disc in the absence of functional MLP leads to heart failure.

Published
2016

35. Rotigotine transdermal system for long-term treatment of patients with advanced Parkinson’s disease: results of two open-label extension studies, CLEOPATRA-PD and PREFER

Author

Lewitt, P, Boroojerdi, B, Surmann, E, Poewe, W, Calabrese, V, Cleeremans, B, Curran, T, Chang, F, Dewey, R, Elmer, L, Higgins, D, Gazda, S, Glyman, S, Golbe, L, Grimes, D, Kostyk, S, Jankovic, J, Jennings, D, Taber, L, Kishner, R, Singer, C, Leopold, N, Margolin, D, Martin, W, Camicioli, R, Murphy, J, Panisset, M, Truong, D, Patton, J, Petzinger, G, Lew, M, Racette, B, Rajput, A, Rao, J, Scott, B, Singer, R, Samanta, J, Suchowersky, O, Tarsy, D, Waters, C, Evatt, M, Wendt, J, Pahwa, R, Siegel, K, Banas, T, Nausieda, P, Hull, K, Hull, R, Chumley, W, Cohen, S, Brew, B, Crimmins, D, Fung, V, Hayes, M, Thyagarajan, D, Brinar, V, Demarin, V, Bar, M, Ehler, E, Polivka, J, Rektor, I, Ruzicka, E, Svatova, J, Broussolle, E, Destee, A, Viallet, F, Jolma, T, Myllyla, V, Kronenbuerger, M, Mueller, T, Rózsa, C, Pal, E, Takacs, A, Valikovics, A, Djaldetti, R, Giladi, N, Anderson, T, Mossman, S, Snow, B, Aasly, J, Hestnes, A, Larsen, J, Tysnes, O, Chmielewska, B, Kotowicz, J, Nyka, W, Pruchnik Wolinska, D, Szczudlik, A, Tutaj, A, Badenhorst, F, Carr, J, Fine, J, Guldenphennig, W, Kies, B, Smuts, J, Hallström, Y, Barone, P, Battistin, U, Bonucceli, L, Pezzoli, G, Ruggieri, S, Stanzione, P, Aguilar, M, Balaguer, M, Francesc, E, Grandas, F, Kulisevsky, J, Linazasoro, G, Tolosa, E, Boothman, B, Grosset, D, and Sagar, H

Subjects
Male, Time Factors, Parkinson's disease, Severity of Illness Index, law.invention, Randomized controlled trial, law, Outcome Assessment, Health Care, Activities of Daily Living, 80 and over, Medicine, Open-label, Longitudinal Studies, Rotigotine transdermal system, Aged, 80 and over, Administration, Cutaneous, Double-Blind Method, Humans, Aged, Outcome Assessment (Health Care), Thiophenes, Dopamine Agonists, Parkinson Disease, Adult, Tetrahydronaphthalenes, Middle Aged, Female, Clinical trial, Psychiatry and Mental health, Neurology, Tolerability, Administration, Settore MED/26 - Neurologia, medicine.symptom, Somnolence, medicine.drug, medicine.medical_specialty, Clinical Neurology, Neurology and Preclinical Neurological Studies - Original Article, rotigotine, Parkinson´s disease, cleopatra-pd study, prefer study, Internal medicine, Severity of illness, Adverse effect, Biological Psychiatry, business.industry, Rotigotine, medicine.disease, Cutaneous, Parkinson’s disease, Physical therapy, Neurology (clinical), business
Abstract

Open-label extensions [studies SP516 (NCT00501969) and SP715 (NCT00594386)] of the CLEOPATRA-PD and PREFER studies were conducted to evaluate the safety, tolerability and efficacy of the dopaminergic agonist, rotigotine, over several years of follow-up in patients with advanced Parkinson’s disease (PD). Eligible subjects completing the double-blind trials received open-label adjunctive rotigotine (≤16 mg/24 h) for up to 4 and 6 years in Studies SP516 and SP715, respectively. Safety and tolerability were assessed using adverse events, vital signs and laboratory parameters, and efficacy assessed using the unified Parkinson’s disease rating scale (UPDRS). Of the 395 and 258 patients enrolled in the SP516 and SP715 studies, 48 and 45 % completed, respectively. Adverse events were typically dopaminergic effects [e.g., somnolence (18–25 %/patient-year), insomnia (5–7 %/patient-year), dyskinesias (4–8 %/patient-year) and hallucinations (4–8 %/patient-year)], or related to the transdermal application of a patch (application site reactions: 14–15 %/patient-year). There were no clinically relevant changes in vital signs or laboratory parameters in either study. Mean UPDRS part II (activities of daily living) and part III (motor function) total scores improved from double-blind baseline during dose titration, then gradually declined over the maintenance period. In study SP516, mean UPDRS part II and III total scores were 0.8 points above and 2.8 points below double-blind baseline, respectively, at end of treatment. In study SP715, mean UPDRS part II and III total scores were 4.1 points above and 0.2 points below baseline, respectively, at end of treatment. In these open-label studies, adjunctive rotigotine was efficacious with an acceptable safety and tolerability profile in patients with advanced PD for up to 6 years.

Published
2012
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36. Phase III Dose-Comparison Study of Glatiramer Acetate for Multiple Sclerosis

Author

Comi, G, Cohen, Ja, Arnold, Dl, Wynn, D, Filippi, M, FORTE Study Group, Rocc, Ma, Perego, E, Absinta, M, Mesaros, S, Vuotto, R, Misci, P, Petrolini, M, Coyle, P, Wolinsky, J, Antel, J, Zamvil, S, Feigin, P, Carra, Aj, Bettinelli, Rj, Luetic, Gg, Vrech, Ca, Dubois, Bd, Metz, L, Bar Or, A, Bhan, V, Myles, M, Havrdova, E, Ehler, E, Kanovsky, P, Talab, R, Zapletalova, O, Gross Paju, K, Taba, P, Elovaara, I, Erälinna, Jp, Kinnunen, E, Koivisto, K, Reunanen, M, Brochet, B, Camu, W, Damier, P, Defer, G, Tumani, H, Becker, E, Buettner, T, Diener, Hc, Franz, P, Haas, J, Heesen, C, Heidenreich, F, Koelmel, Hw, Reifschneider, G, Retzlaff, K, Thoemke, F, Ziemssen, T, Rozsa, C, Bartos, L, Csanyi, A, Deme, I, Komoly, S, Panczel, G, Simo, M, Achiron, A, Milo, R, Bergamaschi, R, Bertolotto, A, Capra, R, Caputo, D, Cavalla, P, Centonze, D, Cottone, S, DE STEFANO, Nicola, Gasperini, C, Mancardi, G, Provinciali, L, Ruggieri, S, Scarpini, E, Zaffaroni, M, Metra, M, Kizlaitiene, R, Vaitkus, A, Zwanikken, Cp, Hupperts, Rm, Jongen, Pj, Szczudlik, A, Fryze, W, Kazibutowska, Z, Pierzchaa, K, Pniewski, J, Podemski, R, Stepień, A, Bajenaru, O, Campeanu, A, Marginean, I, Popescu, Cd, Toldisan, I, Boiko, A, Gustov, A, Malkova, N, Perfilyev, S, Poverennova, I, Saykhunov, M, Shutov, A, Skoromets, A, Spirin, N, Stolyarov, I, Volkova, L, Rodriguez Antigüedad, A, Arbizu, T, Arroyo, R, Barcena, J, Casanova, B, Fernández, O, Montalban, X, Ramió, L, Saiz Hinarejos, A, Sharrack, B, Silber, E, Young, C, Agius, M, Birnbaum, G, Campagnolo, D, Chaudhary, K, Cohen, J, Ford, C, Fox, E, Goodman, A, Green, B, Gupta, A, Hughes, B, Javed, A, Jeffery, D, Kasper, L, Kaufman, M, Khan, O, Kresa Reahl, K, Leist, T, Lynch, S, Markowitz, C, Mattson, D, Moses, H, Parks, B, Parry, G, Phillips, T, Picone, M, Rammohan, K, Rizvi, S, Royal, W, Scarberry, S, Sheppard, C, Simnad, V, Thrower, B, Whitham, R, Wynn, D., Comi, G, Cohen, Ja, Arnold, Dl, Wynn, D, Filippi, M, FORTE Study, Group, Diener, Hans Christoph (Beitragende*r), Klinische Neurowetenschappen, and RS: MHeNs School for Mental Health and Neuroscience

Subjects
Male, Medizin, MULTICENTER, Relapsing-Remitting, Gastroenterology, law.invention, DOUBLE-BLIND, Randomized controlled trial, law, Recurrence, Drug Toxicity, Clinical endpoint, Secondary Prevention, administration /&/ dosage/adverse effects/therapeutic use, Middle Aged, drug therapy, Intention to Treat Analysis, Treatment Outcome, Neurology, Tolerability, Disease Progression, RELAPSE RATE, TRIAL, Female, Settore MED/26 - Neurologia, Drug, Immunosuppressive Agents, medicine.drug, Adult, medicine.medical_specialty, Multiple Sclerosis, Drug-Related Side Effects and Adverse Reactions, Adolescent, Endpoint Determination, DOUBLE-BLIND, RELAPSE RATE, FOLLOW-UP, DISABILITY, TRIAL, MULTICENTER, MS, Dose-Response Relationship, Multiple Sclerosis, Relapsing-Remitting, Adolescent, Adult, Disease Progression, Dose-Response Relationship, Drug, Drug Toxicity, Endpoint Determination, Female, Humans, Immunosuppressive Agents, administration /&/ dosage/adverse effects/therapeutic use, Intention to Treat Analysis, Male, Middle Aged, Multiple Sclerosis, drug therapy, Multiple Sclerosis, drug therapy, Peptides, administration /&/ dosage/adverse effects/therapeutic use, Recurrence, prevention /&/ control, Treatment Outcome, Internal medicine, medicine, Humans, Glatiramer acetate, Expanded Disability Status Scale, Intention-to-treat analysis, Peptides, Dose-Response Relationship, Drug, business.industry, DISABILITY, MS, Glatiramer Acetate, Confidence interval, Surgery, Relative risk, prevention /&/ control, Neurology (clinical), FOLLOW-UP, business
Abstract

Objective: To evaluate the safety, tolerability, and efficacy of glatiramer acetate (GA) 40mg compared to a 20mg dose. Methods: Patients with multiple sclerosis (MS) with ≥1 documented relapse in 12 months prior to screening, or ≥2 documented relapses in 24 months prior to screening, and Expanded Disability Status Scale (EDSS) score 0 to 5.5 were enrolled. Patients were evaluated at screening, baseline, and at months 1, 2, 3, 6, 9, and 12. Primary endpoint was rate of confirmed relapses observed during 12-month study. Analysis was by intent-to-treat. Results: A total of 1,155 patients randomized to GA 20mg (n = 586) or 40mg (n = 569). The groups were well-matched at baseline on demographic, clinical, and magnetic resonance imaging (MRI) characteristics. The primary endpoint was similar in both groups (relative risk [RR] = 1.07; 95% confidence interval [CI], 0.88–1.31; p = 0.486) with mean annualized relapse rates (ARRs) of 0.33 for the 20mg group, 0.35 for the 40mg group, and 0.27 for patients from both groups who completed the entire 1-year treatment. A total of 77% of patients remained relapse-free in both groups. Both groups showed a reduction in mean number of gadolinium-enhancing and new T2 lesions over time with trend for faster reduction in the first trimester with the 40mg dose compared with 20mg dose. Both doses were well-tolerated with a safety profile similar to that observed in previous studies of 20mg GA. Interpretation: In relapsing-remitting MS patients, both the currently-approved GA 20mg and 40mg doses were safe and well-tolerated, with no gain in efficacy for the higher dose. Ann Neurol 2011;69:75–82.

Published
2011
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37. Timing and Course of Clinical Response to Intravenous Immunoglobulin in Chronic Inflammatory Demyelinating Polyradiculoneuropathy

Author

Latov, N, Deng, C, Dalakas, Mc, Bril, V, Donofrio, P, Hanna, K, Hartung, Hp, Hughes, Ra, Merkies, Is, van Doorn, Pa, Ice, Sg, Apostolski, S, Banach, M, Barroso, F, Bartosik Psujek, H, Basta, I, Bednarik, J, Belniak, E, Benedetti, L, Buchman, A, Caress, J, Chapman, K, Chyrchel, U, del Carro, U, Drory, V, Dubrovsky, A, Ehler, E, Fryze, W, Fulgenzi, E, Gibson, G, Gonzalez Cornejo, S, Gonzalez Jaime, Jd, Grandis, Marina, Haas, J, Kaminski, M, Marchesoni, C, Munch, C, Narciso, E, Nations, S, Nogues, M, Patwa, H, Pavlovic, S, Pizzorno, M, Reisin, R, Romero Vargas, S, Ruiz Sandoval, Jl, Ruiz Sandoval, Md, Schenone, Angelo, Selmaj, K, Stelmasiak, Z, Szczudlik, A, Thomas, Fp, Tsao, B, Trivedi, J, Uncini, A, Villa, A, Vohanka, S, Wolfe, G, Zapletalova, O., Klinische Neurowetenschappen, RS: MHeNs School for Mental Health and Neuroscience, and Neurology

Subjects
Adult, Male, medicine.medical_specialty, Time Factors, CONTROLLED TRIAL, POLYNEUROPATHY, Neural Conduction, Action Potentials, Placebo, Loading dose, Drug Administration Schedule, law.invention, Grip strength, Disability Evaluation, Arts and Humanities (miscellaneous), Maintenance therapy, Randomized controlled trial, Double-Blind Method, law, Internal medicine, medicine, Humans, Immunologic Factors, Muscle Strength, Aged, Aged, 80 and over, Cross-Over Studies, Hand Strength, Maintenance dose, business.industry, Immunoglobulins, Intravenous, Middle Aged, Crossover study, Clinical trial, Treatment Outcome, Polyradiculoneuropathy, Chronic Inflammatory Demyelinating, Physical therapy, Female, Neurology (clinical), business
Abstract

Objective To investigate the timing, course, and clinical characteristics of the response to intravenous immunoglobulin in chronic inflammatory demyelinating polyradiculoneuropathy (CIDP). Design Data were extracted from the ICE trial, a randomized, double-blind, placebo-controlled trial of immune globulin intravenous, 10% caprylate/chromatography purified (IGIV-C). Setting Multiple international centers. Participants One hundred seventeen individuals with CIDP. Intervention Treatment with IGIV-C (Gamunex, n = 59) or placebo (n = 58), with IGIV-C administered as a 2-g/kg loading dose followed by a 1-g/kg maintenance dose every 3 weeks, for up to 24 weeks. Main Outcome Measures The primary efficacy parameter was an improvement of 1 or more points in adjusted Inflammatory Neuropathy Cause and Treatment (INCAT) disability score. Participants treated with IGIV-C were divided into subgroups based on meeting responder vs nonresponder definitions and by time to first improvement. Results Among 30 responders to IGIV-C, 14 (47%) patients had improved adjusted INCAT scores by week 3, and 16 (53%) patients improved at week 6 after a second infusion. Participants who improved by week 3 were more severely disabled at baseline than those who improved at 6 weeks. In patients who improved, the number of individuals reaching maximal improvement continued to increase during maintenance therapy for up to 24 weeks. For patients with first improvement by week 3, the change in dominant-hand grip strength over time tended to parallel the INCAT score. In patients with first improvement by week 6, however, the improvement in dominant-hand grip strength preceded initial improvement in INCAT score. Conclusions Data suggest that treatment with 2 courses of IGIV-C administered 3 weeks apart may be required for initial improvement, and continued maintenance therapy may be necessary to achieve a maximal therapeutic response. Trial Registration clinicaltrials.gov Identifier:NCT00220740

Published
2010
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39. Kompresivní neuropatie jako nemoc z povolání.

Author

Ehler, E., Ridzoň, P., Fenclová, Z., and Urban, P.

Abstract

Some lesions of the peripheral nerves caused by physical factors can, under certain conditions, be acknowledged as an occupational dis-ease. The decision whether it is an occupational dis-ease or not is authorized by the "Centre of occupational dis-eases". Neurological consultants have a very important role in the process of acknowledgement of an occupational dis-ease. Dur--ing the last 20 years, disorders of neurological character represented 29.6% of all occupational dis-eases. At the same time, the lesions of the peripheral nerves due to overload or vibration constituted 98.5%. Carpal tun-nel syndrome is most frequent, fol-lowed less often by an ulnar nerve lesion in the elbow, and rarely by an ulnar nerve lesion in the wrist and hand –  the Guyon's chan-nel. In the development of occupational compres-sive neuropathies, various mechanisms take place: mechanical pres-sure, hand overload, transmis-sion of vibration on the upper extremity, cold, inappropriate position dur--ing work, and other factors. For acknowledgement of occupational origin of such a lesion, it is es-sential to determine clinical signs and symp-toms, and EMG examination cor-respond--ing to at least the moderately severe lesion. Anamnestic, clinical, and EMG characteristics includ--ing electrophysiological parameters of a moderately severe lesion for the median and ulnar nerves were defined. The authors declare they have no potential conflicts of interest concerning drugs, products, or services used in the study. The Editorial Board declares that the manu-script met the ICMJE "uniform requirements" for biomedical papers. [ABSTRACT FROM AUTHOR]

Published
2019

40. Rekonstrukce paréz dolní končetiny po zlomeninách pánve svalovými transfery.

Author

ČIŽMÁŘ, I., VLČEK, M., EHLER, E., and DRÁČ, P.

Subjects
PARALYSIS, PELVIC fractures, MOTOR ability, TENODESIS, FASCIAE (Anatomy)
Abstract

PURPOSE OF THE STUDY The prevalence of nerve structure injuries accompanying pelvic and acetabular fractures is stated to be 5-25 %, with most frequent injuries to motor nerve structures associated with fractures of the posterior wall of the acetabulum. Prognostically worse outcomes of regeneration are documented mainly in iatrogenic, intraoperative injuries to nerve structures. This study aims to document the functional effect of muscle transfers restoring the movement of lower extremities with irreversible nerve lesion caused by the pelvic and acetabular fracture. MATERIAL AND METHODS A total of 18 patients with irreversible palsy of lower extremities in L4-S1 segments underwent a reconstruction surgery in the period 2006-2016, of whom 13 patients with the mean age of 42 (21-79) years arrived for a follow-up. The group included 10 patients with the loss of function of peroneal portion of the sciatic nerve, one patient sustained femoral nerve lesion and two patients suffered complete sciatic nerve lesion (both the peroneal and tibial portion). The patients were evaluated at the average follow-up of 77 (24-129) months after the reconstruction surgery. The average time interval from pelvic fracture to reconstruction by muscle transfer was 47 (18-151) months. Due to a wide spectrum of functional damage, the patients were evaluated in terms of the overall effect of the reconstruction surgery on the activities of daily living using the LEFS (The Lower Extremity Functional Scale). The surgical techniques used transposition of tensor fascie latae for femoral nerve lesion, transposition of tibialis posterior muscle for palsy of the peroneal division of the sciatic nerve and tenodesis of tibialis anterior tendon and peroneus longus tendon for the palsy of the peroneal and tibial portion of sciatic nerve. RESULTS The effect of movement restoration on daily living evaluated using the LEFS achieved 65 points (53-79) which is 85% of the average value of LEFS in healthy population. The transposition of active muscles tibialis posterior and tensor fasciae latae resulted in all the patients in active movement restoration. A loss of correction of foot position following the performed tenodesis of the paralysed tibialis anterior muscle was observed in one patient, with no significant impact on function. No infection complication was reported in the group. In 78% of patients the intervention was performed as day surgery. DISCUSSION There is a better prognosis for restoration in incomplete nerve lesion than in complete lesions and also in the loss of sensation than in the loss of motor function. The mini-invasive stabilisation of pelvic ring according to literature does not increase the risk of nerve lesions, while on the other hand a higher incidence of femoral nerve damage by INFIX fixator is documented. The type of muscle transfer is selected based on the availability of active muscles suitable for transposition and also with respect to functional requirements of the patient. CONCLUSIONS Irreversible palsy of lower extremity after the pelvic fracture is easily manageable as to the restoration of function. Surgical interventions using the preserved active muscles to restore the lost movement should be a component part of comprehensive surgical care for patients who sustained a pelvic fracture and should be performed centrally at a centre availing of comprehensive expertise. [ABSTRACT FROM AUTHOR]

Published
2019

41. Zkušenosti s elektrofyziologickou dia-gnostikou profesionální léze loketního nervu v oblasti lokte.

Author

Ehler, E., Nakládalová, M., Urban, P., and Štěpánek, L.

Abstract

Aim: For uniform assessment of occupational ulnar nerve entrapment at elbow (UNE) assessment methods using electrophysiological criteria were introduced in 2011. The study aimed at determining changes in selected EMG parameters in UNE recognized as occupational disease using the methods in 2012–2016. Patients and methods: In 55 participants (49 males), follow-up EMG at 1 to 5 years from recognition as occupational disease was assessed. Eighty-one arms were affected by UNE. Changes in the amplitude of motor nerve conduction velocity of the ulnar nerve across the elbow (MNCV-U) and in compound muscle action potential over the abductor digiti minimi (CMAP ADM) were compared with initial EMG. Results: The MNCV-U parameter remained unchanged in 54% of cases, deteriorated in 16% and improved in 30%. The mean MNCV-U increased significantly between the measurements. The CMAP ADM amplitude was unchanged in 89% of cases, worse in 4% and better only in 7%. Its mean value at follow-up was not statistically significantly different. There was no case of completely normalized EMG. Conclusion: Occupational UNE is a chronic condition with an unsatisfactory prognosis even after the occupational risk is removed. The authors declare they have no potential conflicts of interest concerning drugs, products, or services used in the study. The Editorial Board declares that the manuscript met the ICMJE "uniform requirements" for biomedical papers. [ABSTRACT FROM AUTHOR]

Published
2019

45. Lehká mozková poranění -  konsenzuální odborné stanovisko České neurologické společnosti ČLS JEP.

Author

Chudomel, O., Růžička, F., Brázdil, M., Marusič, P., Růžička, E., Ehler, E., and Bednařík, J.

Abstract

Copyright of Česká a Slovenská Neurologie a Neurochirurgie is the property of Czech Medical Association of JE Purkyne and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published
2019

46. Nové poznatky v dia gnostice a léčbě amyotrofické laterální sklerózy.

Author

Štětkářová, I., Matěj, R., and Ehler, E.

Abstract

Copyright of Česká a Slovenská Neurologie a Neurochirurgie is the property of Czech Medical Association of JE Purkyne and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published
2018
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47. Chronická zánětlivá demyelinizační polyradikuloneuropatie.

Author

Ehler, E.

Abstract

Chronic infl am matory demyelinating polyradiculoneuropathy (CIDP) is a chronic demyelinat ing polyneuropathy with a relaps ing or progres sive course. This is a dysim mune polyneuropathy with activation of humoral and cel lular mechanisms with a primary lesion of myelin sheath in the peripheral nerves. Most frequent is a typical sym metrical polyneuropathy, multifocal neuropathy with a conduction block is less frequent, then distal sym metrical motor and sensory neuropathy, pure sensory or pure motor neuropathies occur rarely. Development of signs and symp toms beyond 2 months is a com mon feature for all variants. Dia gnosis of CIDP is based on clinical fi ndings, precisely developed electrophysiological criteria, and some laboratory fi ndings - hyperproteinor rhachia with normal cell count, and MRI with thicken ing and enhancement of nerves in brachalis and lumbar plexuses or roots. Corticosteroids or intravenous im munoglobulins are used as induction ther apy as the fi rst-line treatment of CIDP. Therapeutic plasma exchange is a second-line ther apy in patients with ineffi cacy or intolerability of the fi rst-line treatment. As adjuvant ther apy, they use azathioprin, mycofenolate mofetil, ciclosporin A, cyclophosphamide, and methotrexate. CIDP is a treatable neuropathy though in some patients it leads to invalidity. [ABSTRACT FROM AUTHOR]

Published
2018
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48. Results of Membrane-Activated Chelator Stroke Intervention randomized trial of DP-b99 in acute ischemic stroke

Author

Lees, K, Bornstein, N, Diener, H, Gorelick, P, Rosenberg, G, Shuaib, A, Fazekas, F, Ford, I, Mohr, J, Marshall, L, Geffen, P, Bibliowicz, A, Michel, D, Rotmensch, H, Schuckelt, R, Ding, D, Soeder, T, Gatterer, A, Gruber, F, Willeit, J, Weber, J, Moro, C, Silva, G, Rocha, M, Fabio, S, Buck, B, Tomek, A, Krajickova, D, Bauer, J, Ehler, E, Vaclavik, D, Dolezil, D, Sramek, M, Skoda, O, Sablot, D, Rouanet, F, Hosseini, H, Amarenco, P, Moulin, T, Ludolph, A, Hetzel, A, Kastrup, A, Griewing, B, Hobohm, C, Weimar, C, Reinhard, C, Nabavi, D, Schneider, D, Busch, E, Scherzinger, G, Glahn, J, Faiss, J, Klingelhofer, J, Wasser, K, Groeschel, K, Kohrmann, M, Maschke, M, Von Mering, M, Seidel, G, Goertler, M, Kaminski, R, Els, T, Walter, U, Limmroth, V, Csanyi, A, Valikovics, A, Panczel, G, Csiba, L, Szegedi, N, Horvath, S, Weller, B, Tanne, D, Dorodnicov, E, Leker, R, Lampl, Y, Micieli, G, Eleopra, R, Guidetti, D, Bottacchi, E, Agnelli, G, Comi, G, Bono, G, Melis, M, Stanzione, P, Di Lazzaro, V, Schreuder, T, Stepien, A, Czlonkowska, A, Kuczynska Zardzewialy, A, Stoinski, J, Jackowski, M, Brola, W, Fryze, W, Stelmasiak, Z, Cunha, L, Melo, T, Salgado, V, Cruz, V, Savic, M, Krastev, G, Vyletelka, J, Dvorak, M, Brozman, M, Nosal, V, Kok, A, Van Dyk, C, Bester, F, Roos, J, Gardiner, J, De Vries Basson, M, Davalos, A, de la Ossa, N, Rodríguez, C, Tejedor, A, E, Masjuan, J, Fábregas, J, Serena, J, Alvarez, J, Castillo, J, Pons, J, Vivancos, J, Arenillas, J, Segura, T, Lyrer, P, Vaishnav, A, Pineda, C, Veznedaroglu, E, Mallenbaum, S, Lees, Kr, Bornstein, N, Diener, Hc, Gorelick, Pb, Rosenberg, G, Shuaib, A, Comi, Giancarlo, and Macsi, Investigators

Subjects
Male, Time Factors, Medizin, Severity of Illness Index, law.invention, Randomized controlled trial, law, 80 and over, Acute treatment, Neuroprotection, Egtazic Acid, Acute ischemic stroke, Stroke, Chelating Agents, Aged, 80 and over, education.field_of_study, Middle Aged, Treatment Outcome, Administration, Administration, Intravenous, Female, Settore MED/26 - Neurologia, Drug, Intravenous, Cardiology and Cardiovascular Medicine, medicine.medical_specialty, Endpoint Determination, Population, Dose-Response Relationship, Double-Blind Method, Intervention (counseling), Internal medicine, Severity of illness, medicine, Humans, education, Aged, Advanced and Specialized Nursing, Dose-Response Relationship, Drug, business.industry, Therapeutic effect, medicine.disease, Surgery, Neurology (clinical), business
Abstract

Background and Purpose— DP-b99, a lipophilic moderate-affinity chelator of zinc, was postulated to improve recovery after acute ischemic stroke. We evaluated the safety and therapeutic effects of DP-b99 in patients with acute hemispheric ischemic stroke. Methods— The Membrane-Activated Chelator Stroke Intervention trial was a randomized, double-blind, placebo-controlled, multicenter, parallel-group trial of intravenous DP-b99 administered for 4 consecutive days (NCT00893867). Acute ischemic stroke patients within 9 hours of onset, but untreated by alteplase, with a baseline National Institutes of Health Stroke Scale score of 10 to 16, and evidence of language dysfunction, visual field defect, and neglect were eligible. The primary efficacy analysis compared distributions of functional status measured by modified Rankin score in the intent-to-treat population of patients with any post-treatment outcome, adjusted for initial severity. Functional and neurological recovery were secondary measures. Home time was an exploratory end point. Results— Enrollment terminated at n=446 after the planned interim analysis determined futility; follow-up continued. Final modified Rankin score distributions were equal between DP-b99 and placebo-treated groups ( P =0.10; P adj adjusted for baseline age and National Institutes of Health Stroke Scale=0.21). Fewer patients recovered to modified Rankin score ≤1 in the DP-b99–treated group (45/218; 20.6%) than after placebo (63/219; 28.8%) ( P =0.05; P adj =0.10). Similarly, fewer patients attained National Institutes of Health Stroke Scale ≤1 after DP-b99 (42/218; 19.3%) than placebo (56/219; 25.6%; P =0.10; P adj =0.26). Mortality was similar between DP-b99 and placebo intent-to-treat groups (36/218; 16.5% vs 33/219; 15.1%; P =0.68). Home time was unchanged by treatment (median 36 vs 36.5 days; P =0.25). Conclusions— Despite encouraging preclinical and phase II trial data, DP-b99 shows no evidence of efficacy in treating human ischemic stroke.

Published
2013

50. Mechanistic insights into arrhythmogenic right ventricular cardiomyopathy caused by desmocollin-2 mutations

Author

Gehmlich, K. Syrris, P. Peskett, E. Evans, A. Ehler, E. Asimaki, A. Anastasakis, A. Tsatsopoulou, A. Vouliotis, A.-I. Stefanadis, C. Saffitz, J.E. Protonotarios, N. McKenna, W.J.

Abstract

Aims Recent immunohistochemical studies observed the loss of plakoglobin (PG) from the intercalated disc (ID) as a hallmark of arrhythmogenic right ventricular cardiomyopathy (ARVC), suggesting a final common pathway for this disease. However, the underlying molecular processes are poorly understood. Methods and resultsWe have identified novel mutations in the desmosomal cadherin desmocollin 2 (DSC2 R203C, L229X, T275M, and G371fsX378). The two missense mutations (DSC2 R203C and T275M) have been functionally characterized, together with a previously reported frameshift variant (DSC2 A897fsX900), to examine their pathogenic potential towards PGs functions at the ID. The three mutant proteins were transiently expressed in various cellular systems and assayed for expression, processing, localization, and binding to other desmosomal components in comparison to wild-type DSC2a protein. The two missense mutations showed defects in proteolytic cleavage, a process which is required for the functional activation of mature cadherins. In both cases, this is thought to cause a reduction of functional DSC2 at the desmosomes in cardiac cells. In contrast, the frameshift variant was incorporated into cardiac desmosomes; however, it showed reduced binding to PG. Conclusion Despite different modes of action, for all three variants, the reduced ability to provide a ligand for PG at the desmosomes was observed. This is in agreement with the reduced intensity of PG at these structures observed in ARVC patients. © 2010 The Author.

Published
2011

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