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6. Expression of STAT‐ and T‐cell‐related genes in women with first‐line treatment of relapsing‐remitting multiple sclerosis.

Author

Szewczak, Ludmiła, Machcińska, Maja, Kierasińska, Magdalena, Zawadzka‐Więch, Urszula, Maruszewska‐Cheruiyot, Marta, Majewski, Paweł, Karlińska, Anna, Rola, Rafał, and Donskow‐Łysoniewska, Katarzyna

Subjects
*STAT proteins, *DIMETHYL fumarate, *GENE expression, *GLATIRAMER acetate, *T cells
Abstract

Relapsing‐remitting multiple sclerosis is associated with changes in Jak/STAT pathways in immune cells, but the influence of disease‐modifying drugs on these pathways is poorly understood. The aim of this study was to evaluate the impact of first‐line disease‐modifying drugs used in treatment of RRMS on expression of the STAT pathway and T‐cell‐related genes in the blood and on serum concentrations of sgp130 and TGF‐β1 in women, as well as on the level of phosphorylated STAT3 and STAT5 proteins in T cells of untreated patients and heathy controls. Expression of STAT1, STAT3, STAT5A, STAT5B, SOCS1, SOCS3, FOXP3, IKZF2, RORC and ICOS genes in the blood of untreated RRMS patients, in the blood of patients treated with interferon‐β, glatiramer acetate, dimethyl fumarate or teriflunomide and in the blood of healthy controls was evaluated using droplet digital PCR. Serum concentrations of sgp130 and TGF‐β1 were evaluated by ELISA. Phosphorylated STAT3 and STAT5 protein levels in T cells were evaluated by flow cytometry. STAT3 gene expression was significantly higher in untreated patients than in healthy control, but the level of phosphorylated STAT3 in T cells was significantly lower. Patients treated with interferon‐β or dimethyl fumarate had significantly lower STAT3 gene expression. Patients treated with teriflunomide had higher STAT1 gene expression, than untreated patients. Patients treated with dimethyl fumarate also had significantly lower RORC gene expression than untreated patients. The study shows the impact of drugs used in first‐line treatment of relapsing‐remitting multiple sclerosis on expression of STAT and T‐cell‐related genes. [ABSTRACT FROM AUTHOR]

Published
2024
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7. The impact of COVID-19 infection on multiple sclerosis disease course across 12 countries: a propensity-score-matched cohort study.

Author

Levitz, David, Chao Foong, Yi, Sanfilippo, Paul, Spelman, Tim, Rath, Louise, Roldan, Angie, Lal, Anoushka, Monif, Mastura, Jokubaitis, Vilija, Ozakbas, Serkan, Alroughani, Raed, Boz, Cavit, Terzi, Murat, Kalincik, Tomas, Blanco, Yolanda, Foschi, Matteo, Surcinelli, Andrea, Buzzard, Katherine, Skibina, Olga, and Laureys, Guy

Subjects
COVID-19, GLATIRAMER acetate, PROPENSITY score matching, DISEASE relapse, DISEASE duration
Abstract

Background: The relationship between coronavirus disease 2019 (COVID-19) infection and multiple sclerosis (MS) relapse and disease progression remains unclear. Previous studies are limited by small sample sizes and most lack a propensity-matched control cohort. Objective: To evaluate the effect of COVID-19 infection on MS disease course with a large propensity-matched cohort. Design: This multi-centre cohort study analysed relapse and disability outcomes post-COVID-19 infection after balancing covariates using a propensity score matching method. The study period was from the 11th of September 2019 to the 16th of February 2023. The mean follow-up period was 1.7 years. Methods: Data were retrieved from the MSBase Registry. Propensity scores were obtained based on age, sex, disease duration, baseline Expanded Disability Status Scale (EDSS), MS course, relapses pre-baseline, disease-modifying therapy (DMT) class and country. Primary outcomes were time to first relapse, annualised relapse rate (ARR) and time to confirm EDSS progression. Secondary outcomes were time to EDSS of 3, 4 or 6. Sensitivity analyses with baseline DMT classes were performed. Results: The study included 2253 cases and 6441 controls. After matching, there were 2161 cases and an equal number of matched controls. Cases had a significantly higher ARR (ARR = 0.10 [95% CI 0.09–0.11]) compared to controls (ARR = 0.07 [95% CI 0.06–0.08]). Cases had a significantly greater hazard of time to first relapse compared to controls (hazard ratio (HR) = 1.54 [95% CI 1.29–1.84]). There was no association between COVID-19 infection and 24-week EDSS progression (HR = 1.18 [95% CI 0.92–1.52]), or time to EDSS of 3, 4 or 6. For patients on interferons and glatiramer acetate (BRACE), COVID-19 infection was associated with a greater hazard of time to first relapse (HR = 1.83 [95% CI 1.25–2.68]) and greater hazard of time to EDSS of 3 (HR = 2.04 [95% CI 1.06–3.90]) compared to patients on BRACE therapy without COVID-19 infection. Conclusion: COVID-19 infection was associated with a significantly increased MS relapse rate and a shorter time to first relapse. There was no effect on confirmed EDSS progression over the short term. These results support ongoing COVID-19 risk minimisation strategies to protect patients with MS. [ABSTRACT FROM AUTHOR]

Published
2024
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8. MS Australia: Progress in MS Research Conference 2023.

Subjects
*MULTIPLE sclerosis, *GLATIRAMER acetate, *PATIENT compliance, *COLOR vision, *MULTIPLE regression analysis
Abstract

The abstract of the "MS Australia: Progress in MS Research Conference 2023" discusses the feasibility testing of an online nutrition education program for individuals with multiple sclerosis (MS), showing improved food literacy and diet quality scores. Another study explores the association between adherence to the Mediterranean diet and the time between MS relapses in Australian individuals, finding that a higher Mediterranean diet score is linked to longer time between relapses. Additionally, research on amide proton transfer weighted imaging (APTWI) suggests its potential as a sensitive tool for evaluating MS lesions and normal-appearing white matter, providing insights into tissue changes associated with MS pathology. Lastly, a study comparing ofatumumab to oral disease modifying therapies in relapsing MS demonstrates superior efficacy in reducing relapses and delaying disease progression. [Extracted from the article]

Published
2024
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9. Glycyrrhetinic acid blocks SARS‐CoV‐2 infection by activating the cGAS‐STING signalling pathway.

Author

Qi, Hui, Ma, Qin‐hai, Feng, Wei, Chen, Si‐mian, Wu, Cai‐sheng, Wang, Yanan, Wang, Tong‐xing, Hou, Yun‐long, and Jia, Zhen‐hua

Subjects
*INTERFERON regulatory factors, *CHINESE medicine, *TRANSGENIC mice, *CELLULAR signal transduction, *SARS-CoV-2 Omicron variant, *GLATIRAMER acetate
Abstract

Background and Purpose: Traditional Chinese medicine (TCM) played an important role in controlling the COVID‐19 pandemic, but the scientific basis and its active ingredients are still weakly studied. This study aims to decipher the underlying anti‐SARS‐CoV‐2 mechanisms of glycyrrhetinic acid (GA). Experimental Approach: GA's anti‐SARS‐CoV‐2 effect was verified both in vitro and in vivo. Homogeneous time‐resolved fluorescence assays, biolayer interferometry technology, and molecular docking were employed to examine interactions of GA with human stimulator of interferon genes (hSTING). Immunofluorescence staining, western blot, and RT‐qPCR were used to investigate nuclear translocation of interferon regulatory factor 3 (IRF3) and levels of STING target genes. Pharmacokinetics of GA was studied in mice. Key Results: GA could directly bind to Ser162 and Tyr240 residues of hSTING, thus up‐regulating downstream targets and activation of the STING signalling pathway. Such activation is crucial for limiting the replication of SARS‐CoV‐2 Omicron in Calu‐3 cells and protecting against lung injury induced by SARS‐CoV‐2 Omicron infection in K18‐ACE2 transgenic mice. Immunofluorescence staining and western blot indicated that GA increased levels of phosphorylated STING, phosphorylated TANK‐binding kinase‐1, and cyclic GMP‐AMP synthase (cGAS). Importantly, GA increased nuclear translocation of IRF3. Pharmacokinetic analysis of GA in mice indicated it can be absorbed into circulation and detected in the lung at a stable level. Conclusion and Implications: Activation of the cGAS‐STING pathway through the GA‐STING‐IRF3 axis is essential for the antiviral activity of GA in mice, providing new insights into the potential translation of GA for treating SARS‐CoV‐2 in patients. [ABSTRACT FROM AUTHOR]

Published
2024
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10. N-acetylglucosamine inhibits inflammation and neurodegeneration markers in multiple sclerosis: a mechanistic trial.

Author

Sy, Michael, Newton, Barbara, Pawling, Judy, Hayama, Ken, Cordon, Andres, Kuhle, Jens, Dennis, James, Brandt, Alexander, Yu, Zhaoxia, and Demetriou, Michael

Subjects
Chronic-active brain inflammation, Multiple sclerosis, N-acetylglucosamine, N-glycan branching, Humans, Animals, Mice, Acetylglucosamine, Interleukin-17, Glatiramer Acetate, Interleukin-6, Multiple Sclerosis, Inflammation, Encephalitis, Cytokines
Abstract

BACKGROUND: In the demyelinating disease multiple sclerosis (MS), chronic-active brain inflammation, remyelination failure and neurodegeneration remain major issues despite immunotherapy. While B cell depletion and blockade/sequestration of T and B cells potently reduces episodic relapses, they act peripherally to allow persistence of chronic-active brain inflammation and progressive neurological dysfunction. N-acetyglucosamine (GlcNAc) is a triple modulator of inflammation, myelination and neurodegeneration. GlcNAc promotes biosynthesis of Asn (N)-linked-glycans, which interact with galectins to co-regulate the clustering/signaling/endocytosis of multiple glycoproteins simultaneously. In mice, GlcNAc crosses the blood brain barrier to raise N-glycan branching, suppress inflammatory demyelination by T and B cells and trigger stem/progenitor cell mediated myelin repair. MS clinical severity, demyelination lesion size and neurodegeneration inversely associate with a marker of endogenous GlcNAc, while in healthy humans, age-associated increases in endogenous GlcNAc promote T cell senescence. OBJECTIVES AND METHODS: An open label dose-escalation mechanistic trial of oral GlcNAc at 6 g (n = 18) and 12 g (n = 16) for 4 weeks was performed in MS patients on glatiramer acetate and not in relapse from March 2016 to December 2019 to assess changes in serum GlcNAc, lymphocyte N-glycosylation and inflammatory markers. Post-hoc analysis examined changes in serum neurofilament light chain (sNfL) as well as neurological disability via the Expanded Disability Status Scale (EDSS). RESULTS: Prior to GlcNAc therapy, high serum levels of the inflammatory cytokines IFNγ, IL-17 and IL-6 associated with reduced baseline levels of a marker of endogenous serum GlcNAc. Oral GlcNAc therapy was safe, raised serum levels and modulated N-glycan branching in lymphocytes. Glatiramer acetate reduces TH1, TH17 and B cell activity as well as sNfL, yet the addition of oral GlcNAc dose-dependently lowered serum IFNγ, IL-17, IL-6 and NfL. Oral GlcANc also dose-dependently reduced serum levels of the anti-inflammatory cytokine IL-10, which is increased in the brain of MS patients. 30% of treated patients displayed confirmed improvement in neurological disability, with an average EDSS score decrease of 0.52 points. CONCLUSIONS: Oral GlcNAc inhibits inflammation and neurodegeneration markers in MS patients despite concurrent immunomodulation by glatiramer acetate. Blinded studies are required to investigate GlcNAcs potential to control residual brain inflammation, myelin repair and neurodegeneration in MS.

Published
2023

12. Stable excess mortality in a multiple sclerosis cohort diagnosed 1970–2010.

Author

Sumelahti, M.‐L., Verkko, A., Kytö, V., and Sipilä, J. O. T.

Subjects
*DEMYELINATION, *GLATIRAMER acetate, *MULTIPLE sclerosis, *LIFE expectancy, *AUTOIMMUNE diseases
Abstract

Background and purpose: Multiple sclerosis (MS) is associated with excess mortality. The use of disease‐modifying treatments (DMTs) has recently been associated with survival benefits. Methods: A regional MS database was linked with national registries. People with MS (pwMS) diagnosed in 1971–2010 were included and followed up until the end of the year 2019. Five matched controls were acquired for every person with MS. DMTs included in the analyses were interferon and glatiramer acetate. Results: Median follow‐up time of the 1795 pwMS was 20.0 years (range 0.1–48.7 years). Survival did not differ between decades of diagnosis (p = 0.20). Amongst pwMS, male sex (adjusted hazard ratio [aHR] 1.70; 95% confidence interval [CI] 1.41–2.06), higher age at diagnosis (aHR 1.83; 95% CI 1.65–2.03 per 10‐year increment) and primary progressive disease course (aHR 1.29; 95% CI 1.04–1.60) were independently associated with poorer survival. DMT use was associated with better survival (p < 0.0001) and better survival during follow‐up (aHR 0.56; 95% CI 0.38–0.81). Compared to matched controls, median life expectancy was 8–9 years shorter in pwMS with survival diverging from controls during the first decade after diagnosis, more clearly in men than women. Conclusion: Despite DMT use being associated with better survival, relative life expectancy of pwMS did not change over five decades in Western Finland. Male sex was an independent risk factor for death amongst pwMS, but excess mortality was higher in women. More work and methods are needed to improve survival in pwMS. [ABSTRACT FROM AUTHOR]

Published
2024
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13. Old and New Strategies in the Treatment of Pediatric Multiple Sclerosis: A Personal View for a New Treatment Approach

Author

Angelo Ghezzi

Subjects
Pediatric multiple sclerosis, Interferon-beta, Glatiramer acetate, Dimethyl fumarate, Teriflunomide, Fingolimod, Neurology. Diseases of the nervous system, RC346-429
Abstract

Abstract Up to 10 years ago the most common approach to the treatment of pediatric MS (ped-MS) was to start with IFNB or GA (so-called first-line therapies or moderate-efficacy disease-modifying therapies [ME-DMTs]) and to switch to more aggressive treatments (or high-efficacy disease-modifying therapies [HE-DMTs]) in non-responder patients. The use of HE-DMTs as first choice was recommended in selected cases with an active, aggressive form of MS. Indications for the treatment of ped-MS were essentially derived from data of observational studies. Recently, results of three randomized clinical trials have been published as well as data from many observational studies evaluating the effect of new and more active DMTs, with clear evidence that HE-DMTs are more effective than ME-DMTs. Therefore, the paradigm of treatment for patients with MS onset before 18 years of age should be changed, offering treatment with HE-DMTs as first option, because of their superior effectiveness to prevent relapses and disease progression. HE-DMTs present an overall reassuring safety profile and obtain better adherence to treatment.

Published
2024
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14. Evaluation of ovarian reserve and the assisted reproductive technology (ART) cycles' outcome as well as the relapse rate within one year after ART in women with multiple sclerosis: a case-control study.

Author

Arabipoor, Arezoo, Moini, Ashraf, Nabavi, Seyed Massood, Mohiti, Shima, Mashayekhi, Mehri, and Zolfaghari, Zahra

Subjects
*OVARIAN reserve, *ANTI-Mullerian hormone, *GLATIRAMER acetate, *REPRODUCTIVE technology, *ARTIFICIAL insemination, *INDUCED ovulation, *NATALIZUMAB
Abstract

Objective: To compare the ovarian reserve and the results of infertility treatment, as well as to investigate the relapse rate in the first year after the assisted reproductive technology (ART) cycle in patients with multiple sclerosis (MS) referred to Royan Institute. Materials and methods: This retrospective study was carried out to evaluate all women diagnosed with MS and referred to Royan Institute for assessment and treatment of possible infertility between 2011 and 2022. The control group consisted of randomly selected healthy women with tubal factor infertility who were referred for treatment during the same time period and matched in terms of age. A comparison was made between groups in terms of ovarian reserve and infertility treatment outcomes. Additionally, patients with MS who met the criteria were monitored via telephone to evaluate the symptoms, disability and relapse rate both pre- and post-ART. Results: Over the course of a decade, the database documented a total of 60 cases diagnosed with MS. Upon examination of the records, it was found that in 27 patients only admission was done without any hormonal assessment or infertility treatment cycle and 5 patients proceeded with the intrauterine insemination cycle. Eventually, 28 women with MS underwent the ART cycle and all of them were treated with interferon beta, glatiramer acetate, or some oral disease modifying therapies. No statistically significant difference in terms of the basal levels of luteinizing hormone, follicle-stimulating hormone and anti-Müllerian hormone was found between the MS and control groups (P > 0.05). Two groups were comparable in terms of menstrual status. The study revealed that both groups exhibited similarities in terms of the controlled ovarian stimulation protocol and duration, the dosage of gonadotropin administered, as well as the ovarian response type, clinical pregnancy rate, and live birth rate (P > 0.05). After follow up, only 2 patients (9.5%) reported relapse of symptoms within one year after ART. Conclusion: The ovarian reserve and ovarian stimulation cycle and pregnancy outcomes following the ART cycle in MS patients were similar to the age-matched control group. The relapse rate of multiple sclerosis did not show a significant increase within a year following the ART cycle. [ABSTRACT FROM AUTHOR]

Published
2024
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15. Old and New Strategies in the Treatment of Pediatric Multiple Sclerosis: A Personal View for a New Treatment Approach.

Author

Ghezzi, Angelo

Subjects
*PEDIATRIC therapy, *MULTIPLE sclerosis, *PATIENT compliance, *DISEASE relapse, *GLATIRAMER acetate
Abstract

Up to 10 years ago the most common approach to the treatment of pediatric MS (ped-MS) was to start with IFNB or GA (so-called first-line therapies or moderate-efficacy disease-modifying therapies [ME-DMTs]) and to switch to more aggressive treatments (or high-efficacy disease-modifying therapies [HE-DMTs]) in non-responder patients. The use of HE-DMTs as first choice was recommended in selected cases with an active, aggressive form of MS. Indications for the treatment of ped-MS were essentially derived from data of observational studies. Recently, results of three randomized clinical trials have been published as well as data from many observational studies evaluating the effect of new and more active DMTs, with clear evidence that HE-DMTs are more effective than ME-DMTs. Therefore, the paradigm of treatment for patients with MS onset before 18 years of age should be changed, offering treatment with HE-DMTs as first option, because of their superior effectiveness to prevent relapses and disease progression. HE-DMTs present an overall reassuring safety profile and obtain better adherence to treatment. [ABSTRACT FROM AUTHOR]

Published
2024
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16. Comparing ocrelizumab to interferon/glatiramer acetate in people with multiple sclerosis over age 60.

Author

Yi Chao Foong, Merlo, Daniel, Gresle, Melissa, Buzzard, Katherine, Zhong, Michael, Wei Zhen Yeh, Jokubaitis, Vilija, Monif, Mastura, Skibina, Olga, Ozakbas, Serkan, Patti, Francesco, Grammond, Pierre, Amato, Maria Pia, Kalincik, Tomas, Horakova, Dana, Havrdova, Eva Kubala, Weinstock-Guttman, Bianca, Scott, Jeanette Lechner, Boz, Cavit, and Sa, Maria Jose

Subjects
SEX factors in disease, CLINICAL trials, MEDICAL sciences, HEALTH facilities, GLATIRAMER acetate
Published
2024
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17. Correction: Ziemssen et al. Immune Response to Initial and Booster SARS-CoV-2 mRNA Vaccination in Patients Treated with Siponimod—Final Analysis of a Nonrandomized Controlled Clinical Trial (AMA-VACC). Vaccines 2023, 11 , 1374.

Author

Ziemssen, Tjalf, Groth, Marie, Winkelmann, Veronika Eva, and Bopp, Tobias

Subjects
MONONUCLEAR leukocytes, GLATIRAMER acetate, DIMETHYL fumarate, MEDIAN (Mathematics), BOOSTER vaccines
Abstract

This correction notice addresses mistakes in a published paper titled "Immune Response to Initial and Booster SARS-CoV-2 mRNA Vaccination in Patients Treated with Siponimod." The errors include incorrect figures, legends, and labels, as well as missing data. The authors have made the necessary corrections, and the scientific conclusions remain unaffected. The notice was approved by the Academic Editor, and the original publication has been updated. [Extracted from the article]

Published
2024
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18. Switching from injectable to other Disease Modifying Therapies may improve sexual dysfunction in people with Multiple Sclerosis.

Author

Ala, Sara, Amirkafi, Ali, Kohandel, Kosar, Shahmohammadi, Sareh, and Sahraian, Mohammad Ali

Subjects
*SEXUAL dysfunction, *MULTIPLE sclerosis, *INTERFERON beta-1a, *IMPOTENCE, *WILCOXON signed-rank test, *GLATIRAMER acetate, *AUTOIMMUNE diseases
Abstract

Background: Multiple Sclerosis (MS) a central nervous system autoimmune disorder, mainly affecting young adults and more prevalent among women, can lead to sexual dysfunction (SD) among both males and females with MS. Female sexual dysfunction can be defined as dyspareunia, a lack of sexual desire, disorders in the arousal and orgasm phases, and sexual pain disorders. The purpose of this study is to investigate the changes in sexual function among females with MS whose treatment was switched from first-line injectable medications to other agents after a six-month duration. And assess the changes in all three domains of SD. Methods: In this longitudinal study females diagnosed with MS, aged between 18 and 50 years old, and were candidates for switching their treatment from interferon beta-1a (intra-muscular and subcutaneous), and Glatiramer Acetate (GA), to Fingolimod, Dimethyl Fumarate (DMF), or Natalizumab (NTZ) due to patients' convenience and tolerability and adverse events were included. "Multiple Sclerosis Intimacy and Sexuality Questionnaire-19" was used to evaluate the SD changes before and six months after the new treatment initiation. Statistical analysis was conducted using SPSS V.24 software. Histograms and the Shapiro-Wilk test were used to assess the normality of the variables; due to the non-normal distribution of quantitative variables (except for age), the Wilcoxon signed-rank test was used to compare the scores, before and six months after the medication change. The level of significance was considered less than 0.05. Results: Out of 107 female participants (average age: 35.09 ± 5.61), The mean of overall MSISQ-19 scores, before and six months after the medication change were not significant (p-value = 0.091). However, considering the subdomains, the medication changes only affected the tertiary subdomain of MSISQ-19 (p-value = 0.017). Still, the scores of other subdomains did not change significantly (p-value = 0.761 for primary SD and 0.479 for secondary SD). Also, there wasn't any significant difference between EDSS before and after the medication change (p-value = 0.461). Conclusions: To our knowledge, this was the first study, assessing the effect of MS medication change on the improvement of SD among patients. According to the results of the presented cross-sectional study, we found that during a six-month period, the tertiary subdomain of MSISQ-19 symptoms improved significantly, while the changes in other SD domains were not significant. [ABSTRACT FROM AUTHOR]

Published
2024
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19. Clinical Experience with Dimethyl Fumarate and Natalizumab in Pregnant Women with Multiple Sclerosis: A Four‐Patient Case Series.

Author

Saito, Satoshi, Ikeguchi, Ryotaro, Kitagawa, Kazuo, Shimizu, Yuko, and Fee, Dominic B.

Subjects
*DIMETHYL fumarate, *FETAL growth retardation, *PERINATAL period, *MORNING sickness, *GLATIRAMER acetate
Abstract

Interferon β and glatiramer acetate are the disease‐modifying drugs (DMDs) considered relatively safe for use in pregnant women with multiple sclerosis (MS); however, the safety profile of dimethyl fumarate (DMF) and natalizumab (NTZ) in this population remains inconclusive. Here, we present four cases of pregnant women with MS who were treated with DMF and NTZ (n = 2 patients, each) during their pregnancy and discuss our observations with the use of these drugs and the clinical courses of the patients. We retrospectively examined relapse of MS during pregnancy and after delivery; duration of exposure to DMDs; maternal, fetal, and neonatal adverse events; breastfeeding; and timing of resumption of DMDs. The two patients treated with DMF discontinued treatment 5 or 6 weeks after the discovery of pregnancy. DMF was resumed 1 week postpartum, and mixed breastfeeding was initiated. Brain magnetic resonance imaging in one patient 9 months after delivery revealed a new lesion; however, it was not classified as a clinical relapse. In two patients treated with NTZ, the dosing interval was extended to 6 weeks after the discovery of pregnancy. One patient discontinued NTZ at 30 weeks and the other at 25 weeks of gestation, as a slight restriction in fetal growth was observed owing to hyperemesis gravidarum. Both patients opted for formula feeding, and no relapse was observed within 1 year postpartum. Additionally, no abnormalities were observed in any of the patients during the perinatal period, and their development was normal. Investigation of drug safety in pregnant and parturient women primarily relies on registries, postmarketing surveillance, and case reports due to ethical limitations on conducting randomized controlled trials. Our findings demonstrated that DMF and NTZ were not contraindicated during pregnancy or the perinatal period in women with MS; nevertheless, vigilant monitoring is essential to ensure the safety of these drugs. [ABSTRACT FROM AUTHOR]

Published
2024
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20. Multiple sclerosis disease activity, a multi-biomarker score of disease activity and response to treatment in multiple sclerosis.

Author

Tatomir, Alexandru, Anselmo, Freidrich, Boodhoo, Dallas, Chen, Hegang, Mekala, Armugam P., Nguyen, Vinh, Cuevas, Jacob, Rus, Violeta, and Rus, Horea

Subjects
MULTIPLE sclerosis, GLATIRAMER acetate, SIRTUINS, REFERENCE values
Abstract

Regular assessment of disease activity in relapsing-remitting multiple sclerosis (RRMS) is required to optimize clinical outcomes. Biomarkers can be a valuable tool for measuring disease activity in multiple sclerosis (MS) if they reflect the pathological processes underlying MS pathogenicity. In this pilot study, we combined multiple biomarkers previously analyzed in RRMS patients into an MS disease activity (MSDA) score to evaluate their ability to predict relapses and treatment response to glatiramer acetate (GA). Response Gene to Complement 32 (RGC-32), FasL, IL-21, SIRT1, phosphorylated SIRT1 (p-SIRT1), and JNK1 p54 levels were used to generate cut-off values for each biomarker. Any value below the cutoff for RGC-32, FasL SIRT1, or p-SIRT1 or above the cutoff for IL-21 or JNK1 p54 was given a +1 value, indicating relapse or lack of response to GA. Any value above the cutoff value for RGC-32, FasL, SIRT1, p-SIRT1 or below that for IL-21 or JNK1 p54 was given a -1 value, indicating clinical stability or response to GA. An MSDA score above +1 indicated a relapse or lack of response to treatment. An MSDA score below -1 indicated clinical stability or response to treatment. Our results showed that the MSDA scores generated using either four or six biomarkers had a higher sensitivity and specificity and significantly correlated with the expanded disability status scale. Although these results suggest that the MSDA test can be useful for monitoring therapeutic response to biologic agents and assessing clinically challenging situations, the present findings need to be confirmed in larger studies. [ABSTRACT FROM AUTHOR]

Published
2024
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21. Real‐world persistence of multiple sclerosis disease‐modifying therapies.

Author

Tallantyre, Emma C., Dobson, Ruth, Froud, Joseph L. J., St John, Frederika A., Anderson, Valerie M., Arun, Tarunya, Buckley, Lauren, Evangelou, Nikos, Ford, Helen L., Galea, Ian, George, Sumi, Gray, Orla M., Hibbert, Aimee M., Hu, Mo, Hughes, Stella E., Ingram, Gillian, Kalra, Seema, Lim, Chia‐Hui E., Mathews, Joela T. M., and McDonnell, Gavin V.

Subjects
*MULTIPLE sclerosis, *GLATIRAMER acetate, *TREATMENT effectiveness, *AGE of onset, *CONFIDENCE intervals
Abstract

Background and purpose: Treatment persistence is the continuation of therapy over time. It reflects a combination of treatment efficacy and tolerability. We aimed to describe real‐world rates of persistence on disease‐modifying therapies (DMTs) for people with multiple sclerosis (pwMS) and reasons for DMT discontinuation. Methods: Treatment data on 4366 consecutive people with relapse‐onset multiple sclerosis (MS) were pooled from 13 UK specialist centres during 2021. Inclusion criteria were exposure to at least one MS DMT and a complete history of DMT prescribing. PwMS in blinded clinical trials were excluded. Data collected included sex, age at MS onset, age at DMT initiation, DMT treatment dates, and reasons for stopping or switching DMT. For pwMS who had received immune reconstituting therapies (cladribine/alemtuzumab), discontinuation date was defined as starting an alternative DMT. Kaplan–Meier survival analyses were used to express DMT persistence. Results: In 6997 treatment events (1.6 per person with MS), median time spent on any single maintenance DMT was 4.3 years (95% confidence interval = 4.1–4.5 years). The commonest overall reasons for DMT discontinuation were adverse events (35.0%) and lack of efficacy (30.3%). After 10 years, 20% of people treated with alemtuzumab had received another subsequent DMT, compared to 82% of people treated with interferon or glatiramer acetate. Conclusions: Immune reconstituting DMTs may have the highest potential to offer a single treatment for relapsing MS. Comparative data on DMT persistence and reasons for discontinuation are valuable to inform treatment decisions and in personalizing treatment in MS. [ABSTRACT FROM AUTHOR]

Published
2024
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22. Constructing Stable Polyvinyl Alcohol/Gelatin/Cellulose Nanocrystals Composite Electrospun Membrane with Excellent Filtration Efficiency for PM2.5.

Author

He, Yang, Liu, Haijun, and Ying, Weijun

Subjects
*COMPOSITE membranes (Chemistry), *CELLULOSE nanocrystals, *POLYVINYL alcohol, *PARTICULATE matter, *MEMBRANE separation, *MEMBRANE filters, *FILTERS & filtration, *GLATIRAMER acetate, *TERIPARATIDE
Abstract

Considering the high demand for air quality, the development of biomass-based air filtration membranes with high air filtration efficiency and good stability is an urgent task. In this work, polyvinyl alcohol (PVA), gelatin (GA), and cellulose nanocrystals (CNC) were mixed and prepared into a membrane through an electrospinning method for air filtration. After a hydrophobic modification, the modified PVA/GA/CNC composite membrane showed excellent filtration efficiency for PM2.5 (97.65%) through the internal three-dimensional structure barrier and the electrostatic capture effect of the CNC with a negative charge, as well as a low-pressure drop (only 50 Pa). In addition, the modified PVA/GA/CNC composite membrane had good mechanical properties (maximum tensile fracture rate of 78.3%) and high stability (air filtration efficiency of above 90% after five wash-filter cycles and a high-temperature treatment at 200 °C). It is worth noting that the whole preparation process is completed without organic solvents, putting forward a new strategy for the construction of green air filtration membranes. [ABSTRACT FROM AUTHOR]

Published
2024
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23. The sphingosine 1‐phosphate analogue, FTY720, modulates the lipidomic signature of the mouse hippocampus.

Author

Magalhães, Daniela M., Stewart, Nicolas A., Mampay, Myrthe, Rolle, Sara O., Hall, Chloe M., Moeendarbary, Emad, Flint, Melanie S., Sebastião, Ana M., Valente, Cláudia A., Dymond, Marcus K., and Sheridan, Graham K.

Subjects
*GLATIRAMER acetate, *FINGOLIMOD, *MONOUNSATURATED fatty acids, *HIPPOCAMPUS (Brain), *UNSATURATED fatty acids, *ION channels, *CENTRAL nervous system, *MEMBRANE lipids
Abstract

The small‐molecule drug, FTY720 (fingolimod), is a synthetic sphingosine 1‐phosphate (S1P) analogue currently used to treat relapsing–remitting multiple sclerosis in both adults and children. FTY720 can cross the blood–brain barrier (BBB) and, over time, accumulate in lipid‐rich areas of the central nervous system (CNS) by incorporating into phospholipid membranes. FTY720 has been shown to enhance cell membrane fluidity, which can modulate the functions of glial cells and neuronal populations involved in regulating behaviour. Moreover, direct modulation of S1P receptor‐mediated lipid signalling by FTY720 can impact homeostatic CNS physiology, including neurotransmitter release probability, the biophysical properties of synaptic membranes, ion channel and transmembrane receptor kinetics, and synaptic plasticity mechanisms. The aim of this study was to investigate how chronic FTY720 treatment alters the lipid composition of CNS tissue in adolescent mice at a key stage of brain maturation. We focused on the hippocampus, a brain region known to be important for learning, memory, and the processing of sensory and emotional stimuli. Using mass spectrometry‐based lipidomics, we discovered that FTY720 increases the fatty acid chain length of hydroxy‐phosphatidylcholine (PCOH) lipids in the mouse hippocampus. It also decreases PCOH monounsaturated fatty acids (MUFAs) and increases PCOH polyunsaturated fatty acids (PUFAs). A total of 99 lipid species were up‐regulated in the mouse hippocampus following 3 weeks of oral FTY720 exposure, whereas only 3 lipid species were down‐regulated. FTY720 also modulated anxiety‐like behaviours in young mice but did not affect spatial learning or memory formation. Our study presents a comprehensive overview of the lipid classes and lipid species that are altered in the hippocampus following chronic FTY720 exposure and provides novel insight into cellular and molecular mechanisms that may underlie the therapeutic or adverse effects of FTY720 in the central nervous system. [ABSTRACT FROM AUTHOR]

Published
2024
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24. Clinical trial evidence of quality-of-life effects of disease-modifying therapies for multiple sclerosis: a systematic analysis.

Author

Hirt, Julian, Dembowska, Kinga, Woelfle, Tim, Axfors, Cathrine, Granziera, Cristina, Kuhle, Jens, Kappos, Ludwig, Hemkens, Lars G., and Janiaud, Perrine

Subjects
*MULTIPLE sclerosis, *CLINICAL trial registries, *GLATIRAMER acetate, *CLINICAL trials, *QUALITY of life
Abstract

Background: Increasingly, patients, clinicians, and regulators call for more evidence on the impact of innovative medicines on quality of life (QoL). We assessed the effects of disease-modifying therapies (DMTs) on QoL in people with multiple sclerosis (PwMS). Methods: Randomized trials assessing approved DMTs in PwMS with results for at least one outcome referred to as "quality of life" were searched in PubMed and ClinicalTrials.gov. Results: We identified 38 trials published between 1999 and 2023 with a median of 531 participants (interquartile range (IQR) 202 to 941; total 23,225). The evaluated DMTs were mostly interferon-beta (n = 10; 26%), fingolimod (n = 7; 18%), natalizumab (n = 5; 13%), and glatiramer acetate (n = 4; 11%). The 38 trials used 18 different QoL instruments, with up to 11 QoL subscale measures per trial (median 2; IQR 1–3). QoL was never the single primary outcome. We identified quantitative QoL results in 24 trials (63%), and narrative statements in 15 trials (39%). In 16 trials (42%), at least one of the multiple QoL results was statistically significant. The effect sizes of the significant quantitative QoL results were large (median Cohen's d 1.02; IQR 0.3–1.7; median Hedges' g 1.01; IQR 0.3–1.69) and ranged between d 0.14 and 2.91. Conclusions: Certain DMTs have the potential to positively impact QoL of PwMS, and the assessment and reporting of QoL is suboptimal with a multitude of diverse instruments being used. There is an urgent need that design and reporting of clinical trials reflect the critical importance of QoL for PwMS. [ABSTRACT FROM AUTHOR]

Published
2024
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25. SARS-CoV-2-Specific Immune Cytokine Profiles to mRNA, Viral Vector and Protein-Based Vaccines in Patients with Multiple Sclerosis: Beyond Interferon Gamma.

Author

Al Rahbani, Georges Katoul, Woopen, Christina, Dunsche, Marie, Proschmann, Undine, Ziemssen, Tjalf, and Akgün, Katja

Subjects
SARS-CoV-2, GENETIC vectors, INTERFERON gamma, TUMOR necrosis factors, MULTIPLE sclerosis
Abstract

Disease-modifying therapies (DMTs) impact the cellular immune response to severe acute respiratory syndrome coronavirus type 2 (SARS-CoV-2) vaccines in patients with multiple sclerosis (pwMS). In this study, we aim to elucidate the characteristics of the involved antigen-specific T cells via the measurement of broad cytokine profiles in pwMS on various DMTs. We examined SARS-CoV-2-specific T cell responses in whole blood cultures characterized by the release of interleukin (IL)-2, IL-4, IL-5, IL-10, IL-13, IL-17A, interferon-gamma (IFN-γ), and tumor necrosis factor-alpha (TNF-α), as well as antibodies (AB) targeting the SARS-CoV-2 spike protein in pwMS following either two or three doses of mRNA or viral vector vaccines (VVV). For mRNA vaccination non-responders, the NVX-CoV2373 protein-based vaccine was administered, and immune responses were evaluated. Our findings indicate that immune responses to SARS-CoV-2 vaccines in pwMS are skewed towards a Th1 phenotype, characterized by IL-2 and IFN-γ. Additionally, a Th2 response characterized by IL-5, and to a lesser extent IL-4, IL-10, and IL-13, is observed. Therefore, the measurement of IL-2 and IL-5 levels could complement traditional IFN-γ assays to more comprehensively characterize the cellular responses to SARS-CoV-2 vaccines. Our results provide a comprehensive cytokine profile for pwMS receiving different DMTs and offer valuable insights for designing vaccination strategies in this patient population. [ABSTRACT FROM AUTHOR]

Published
2024
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26. Neuroprotective Effects of Curcumin in Neurodegenerative Diseases.

Author

Genchi, Giuseppe, Lauria, Graziantonio, Catalano, Alessia, Carocci, Alessia, and Sinicropi, Maria Stefania

Subjects
CURCUMIN, NANOCARRIERS, NEURODEGENERATION, HUNTINGTIN protein, ALZHEIMER'S disease, HUNTINGTON disease, PRION diseases, AMYOTROPHIC lateral sclerosis, GLATIRAMER acetate
Abstract

Curcumin, a hydrophobic polyphenol extracted from the rhizome of Curcuma longa, is now considered a candidate drug for the treatment of neurological diseases, including Parkinson's Disease (PD), Alzheimer's Disease (AD), Huntington's Disease (HD), Multiple Sclerosis (MS), Amyotrophic Lateral Sclerosis (ALS), and prion disease, due to its potent anti-inflammatory, antioxidant potential, anticancerous, immunomodulatory, neuroprotective, antiproliferative, and antibacterial activities. Traditionally, curcumin has been used for medicinal and dietary purposes in Asia, India, and China. However, low water solubility, poor stability in the blood, high rate of metabolism, limited bioavailability, and little capability to cross the blood–brain barrier (BBB) have limited the clinical application of curcumin, despite the important pharmacological activities of this drug. A variety of nanocarriers, including liposomes, micelles, dendrimers, cubosome nanoparticles, polymer nanoparticles, and solid lipid nanoparticles have been developed with great success to effectively deliver the active drug to brain cells. Functionalization on the surface of nanoparticles with brain-specific ligands makes them target-specific, which should significantly improve bioavailability and reduce harmful effects. The aim of this review is to summarize the studies on curcumin and/or nanoparticles containing curcumin in the most common neurodegenerative diseases, highlighting the high neuroprotective potential of this nutraceutical. [ABSTRACT FROM AUTHOR]

Published
2024
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27. Current perspectives on Multiple Sclerosis.

Author

ÇİMEN, Sema and KÜÇÜKOĞLU, Kaan

Subjects
EPSTEIN-Barr virus diseases, GLATIRAMER acetate, DIMETHYL fumarate, NEUROLOGICAL disorders, SYMPTOMS
Abstract

Multiple Sclerosis (MS) is a chronic, autoimmune disease that affects the central nervous system. It is characterized by inflammation, demyelination and axonal loss, and is typically manifested by relapses and remissions. It is the most prevalent neurological disorder worldwide, with a significant prevalence in many countries. It is the leading cause of non-traumatic neurological impairment in young adults. Although the etiology is not fully understood, genetic predisposition, environmental factors (exposure to inadequate sunlight and/or inadequate dietary intake of vitamin D, Epstein-Barr virus infection, etc.) Furthermore, an individual's lifestyle, including obesity, smoking, and other factors, plays a significant role in the development of the disease. The clinical subtypes of MS, as defined in 2013, are classified into four categories: The four main clinical subtypes of MS are: Isolated Syndrome, Relapsing-Remitting MS, Primary Progressive MS and Secondary Progressive MS. The clinical subtypes of MS are further subdivided according to the activity and progression of the disease. MS is a heterogenous disease, with lesions affecting multiple systems. The most common clinical manifestations include fatigue, blurred vision, and ocular pain (optic neuritis), as well as weakness and sensory changes in specific body regions, such as the face, arms, and legs. Furthermore, the patient presented with symptoms including balance impairment, vertigo, memory and cognitive difficulties, and bladder control issues. Although there is currently no cure for MS, existing treatments focus on alleviating acute attacks, improving symptoms, and reducing the impact of the disease through biological therapies. Modifying therapies for the disease (e.g., interferons, glatiramer acetate, dimethyl fumarate, teriflunomide, fingolimod, ocrelizumab, natalizumab, etc.) These drugs, which reduce the frequency of clinical attacks and slow the progression of the disease, also reduce the activity of MRI lesions, making them an important component of MS treatment. They are effective due to their diverse mechanisms of action, administration routes, and dosages. [ABSTRACT FROM AUTHOR]

Published
2024
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28. GC-MS Analysis and Evaluation of Essential Oils as Volatile Biopesticides: Assessing Their Acaricidal Potential against Varroa destructor.

Author

Raza, Muhammad Fahad, Hyder, Moazam, Zhao, Chonghui, and Li, Wenfeng

Subjects
VARROA destructor, ESSENTIAL oils, HONEY, ACARICIDES, BIOPESTICIDES, GAS chromatography/Mass spectrometry (GC-MS), HONEYBEES, BEE venom, GLATIRAMER acetate
Abstract

Honey bees are crucial for ecosystem pollination and honey production, yet the Varroa destructor mite hinders their productivity and health. Efforts to manage Varroa mites with synthetic pesticides have had limited success, highlighting the need for naturally derived acaricides as a primary option. However, the acaricidal efficacy of essential oils from Salvia officinalis L. (sage), Cannabis sativa (hemp), and Laurus nobilis (laurel) remains to be fully understood. This study aims to investigate the acaricidal efficacy of these three essential oils at varying concentrations and their impact on honey production, focusing on the efficient reduction in Varroa mites. The sugar roll method was employed to assess Varroa mite infestation levels, while GC-MS analysis was utilized to verify the composition of the essential oils. Honey production measurements were also performed. The efficacy rates (%) at concentrations of 15%, 10%, and 5% for hemp oil were 95.4% ± 0.30%, 85.71% ± 0.85%, and 64.48% ± 0.26%, respectively; for sage oil, they were 81.08% ± 0.57%, 69.42% ± 1.72%, and 50.35% ± 0.70%; and for laurel oil, they were 68.96% ± 0.34%, 54.66% ± 0.37%, and 33.58% ± 0.30%, respectively. Key compounds identified include trans-caryophyllene, α-pinene, and viridiflorol in hemp oil; myrcene, limonene, and β-caryophyllene in sage oil; and phytol, β-myrcene, and n-heneicosane in laurel oil. The overall findings indicate that hemp oil is highly effective in controlling Varroa mites. However, further research is needed to evaluate its potential side effects on bees to ensure its sustainability and safety. [ABSTRACT FROM AUTHOR]

Published
2024
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33. Diagnostic efficacy of long non-coding RNAs in multiple sclerosis: a systematic review and meta-analysis.

Author

Yongdong Wang, Jing Wang, Xinyin Zhang, Chengyan Xia, and Zhiping Wang

Subjects
LINCRNA, GLATIRAMER acetate, MULTIPLE sclerosis, RECEIVER operating characteristic curves, ODDS ratio
Abstract

Background: Currently, an increasing body of research suggests that bloodbased long non-coding RNAs (lncRNAs) could serve as biomarkers for diagnosing multiple sclerosis (MS). This meta-analysis evaluates the diagnostic capabilities of selected lncRNAs in distinguishing individuals with MS from healthy controls and in differentiating between the relapsing and remitting phases of the disease. Methods: We conducted comprehensive searches across seven databases in both Chinese and English to identify relevant studies, applying stringent inclusion and exclusion criteria. The quality of the selected references was rigorously assessed using the QUADAS-2 tool. The analysis involved calculating summarized sensitivity (SSEN), specificity (SSPE), positive likelihood ratio (SPLR), negative likelihood ratio (SNLR), and diagnostic odds ratio (DOR) with 95% confidence intervals (CIs). Accuracy was assessed using summary receiver operating characteristic (SROC) curves. Results: Thirteen high-quality studies were selected for inclusion in the metaanalysis. Our meta-analysis assessed the combined diagnostic performance of lncRNAs in distinguishing MS patients from healthy controls. We found a SSEN of 0.81 (95% CI: 0.74-0.87), SSPE of 0.84 (95% CI: 0.78-0.89), SPLR of 5.14 (95% CI: 3.63-7.28), SNLR of 0.22 (95% CI: 0.16-0.31), and DOR of 23.17 (95% CI: 14.07-38.17), with an AUC of 0.90 (95% CI: 0.87-0.92). For differentiating between relapsing and remitting MS, the results showed a SSEN of 0.79 (95% CI: 0.71-0.85), SSPE of 0.76 (95% CI: 0.64-0.85), SPLR of 3.34 (95% CI: 2.09-5.33), SNLR of 0.28 (95% CI: 0.19-0.40), and DOR of 12.09 (95% CI: 5.70-25.68), with an AUC of 0.84 (95% CI: 0.81-0.87). Conclusion: This analysis underscores the significant role of lncRNAs as biomarkers in MS diagnosis and differentiation between its relapsing and remitting forms. [ABSTRACT FROM AUTHOR]

Published
2024
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34. Tolerability and Acceptance of Switching from Brand to Generic Glatiramer Acetate in Multiple Sclerosis.

Author

Maraffi, Isabella, Mallucci, Giulia, Disanto, Giulio, Sacco, Rosaria, Tiberti, Massimiliano, Gobbi, Claudio, and Zecca, Chiara

Subjects
*GLATIRAMER acetate, *BRAND mobility, *MULTIPLE sclerosis, *VISUAL analog scale
Abstract

Background: The costs of disease-modifying therapies (DMTs) for multiple sclerosis (MS) have increased interest in generic alternatives. Methods: This prospective and observational study aims to investigate the safety, tolerability, and acceptance of switching from brand glatiramer acetate (GA) 40 mg/mL three times per week (Copaxone®) to generic GA 40 mg/mL three times per week (Glatiramyl®). Conducted at the Neurocenter of Southern Switzerland from September 2020 to September 2021, the study enrolled 27 patients; 21 completed the study. Participants reported on local and systemic side effects three months before and after the switch, and on switch acceptance by means of visual analogue scales (from 0 to 10). Results: Results indicated that those on generic GA experienced fewer local (81.0% vs. 96.3%) and systemic (33.3% vs. 59.3%) adverse events than with the brand drug. The median intensity of local adverse events was 8 (4–20) on generic GA vs. 16 (9–22) on brand GA, while the median intensity of systemic adverse events was similar between generic and brand GA [0 (0–27) vs. 0 (0–21.5), respectively]. Seventy-one percent of participants rated their acceptance of generic GA as 7/10 or higher. Conclusions: The results suggest that switching from brand to generic GA 40 mg/mL is safe, well-tolerated, and accepted by patients with MS. [ABSTRACT FROM AUTHOR]

Published
2024
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35. AMP‐activated protein kinase as a mediator of mitochondrial dysfunction of multiple sclerosis in animal models: A systematic review.

Author

Askari, Hamid, Rabiei, Fatemeh, Lohrasbi, Fatemeh, Ghadir, Sara, Mehdipour Arbastan, Ahmad, and Ghasemi‐Kasman, Maryam

Subjects
*MULTIPLE sclerosis, *AMP-activated protein kinases, *ANIMAL models in research, *MITOCHONDRIA, *MITOCHONDRIAL pathology, *GLATIRAMER acetate, *PROTEIN kinases, *MYELIN oligodendrocyte glycoprotein
Abstract

Multiple sclerosis (MS) is a chronic central nervous system (CNS) disorder characterized by demyelination, neuronal damage, and oligodendrocyte depletion. Reliable biomarkers are essential for early diagnosis and disease management. Emerging research highlights the role of mitochondrial dysfunction and oxidative stress in CNS disorders, including MS, in which mitochondria are central to the degenerative process. Adenosine monophosphate‐activated protein kinase (AMPK) regulates the mitochondrial energy balance and initiates responses in neurodegenerative conditions. This systematic review, following Preferred Reporting Items for Systematic Reviews and Meta‐Analyses guidelines, aimed to comprehensively assess the literature on AMPK pathways, mitochondrial dysfunction, and in vivo studies using MS animal models. The search strategy involved the use of AMPK syntaxes, MS syntaxes, and animal model syntaxes. The PubMed, Scopus, Web of Science, and Google Scholar databases were systematically searched on August 26, 2023 without publication year restrictions. The review identified and analyzed relevant papers to provide a comprehensive overview of the current state of related research. Eight studies utilizing various interventions and methodological approaches were included. Risk of bias assessment revealed some areas of low risk but lacked explicit reporting in others. These studies collectively revealed a complex relationship between AMPK, mitochondrial dysfunction, and MS pathogenesis, with both cuprizone and experimental autoimmune encephalomyelitis models demonstrating associations between AMPK and mitochondrial disorders, including oxidative stress and impaired expression of mitochondrial genes. These studies illuminate the multifaceted role of AMPK in MS animal models, involving energy metabolism, inflammatory processes, oxidative stress, and gene regulation leading to mitochondrial dysfunction. However, unanswered questions about its mechanisms and clinical applications underscore the need for further research to fully harness its potential in addressing MS‐related mitochondrial dysfunction. [ABSTRACT FROM AUTHOR]

Published
2024
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36. Pregnancy and fetal outcomes following paternal exposure to glatiramer acetate.

Author

Kaplan, Sigal, Dragut, Claudia Florentina, and Ghimpeteanu, Andra

Subjects
*PREGNANCY outcomes, *GLATIRAMER acetate, *ABORTION, *MISCARRIAGE, *LOW birth weight, *PRECONCEPTION care, *ABORTION statistics
Abstract

This study aimed to examine pregnancy and fetal outcomes following paternal exposure to glatiramer acetate (GA). Pregnancy reports of paternal GA-exposure at time of conception from 2001 to 2022 were extracted from Teva Global Pharmacovigilance database. Pregnancy reports obtained prior to (prospective) or after (retrospective) knowledge of the pregnancy outcome were included. The primary endpoint was major congenital malformation (MCM) in the offspring according to the US Metropolitan Atlanta Congenital Defects Program (MACDP) and European Surveillance of Congenital Anomalies and Twins (EUROCAT) classification. Other pregnancy and fetal outcomes, including spontaneous abortion, pregnancy termination, fetal death, preterm birth, and low birth weight, were assessed. A total of 466 paternal GA-exposed pregnancies were retrieved, 232 prospective cases and 234 retrospective cases. Of 349 (74.9%) pregnancies with known outcomes, 316 (90.5%) were live births, 28 (8.0%) were spontaneous abortions, 3 (0.9%) were elective pregnancy terminations, and 2 (0.6%) were stillbirths. In prospective live birth cases, there were 7/111 (6.3%) preterm births and 5/115 (4.3%) neonates with a low birth weight. The prevalence of total MCM among prospective cases was 1.7% (2 cases of 116 live births and fetal death/stillbirth), which is slightly lower than the background rates from MACDP (3%) and EUROCAT (2.1%). This study did not indicate an increase in the rate of adverse pregnancy and fetal outcomes after paternal exposure to GA. These results provide additional information regarding pregnancy outcomes following paternal exposure to GA for healthcare professionals, male patients and their female partners who are considering pregnancy while their male partner is using GA. This research aimed to look at how pregnancies and babies were affected when fathers with multiple sclerosis have been prescribed and taken the medication, glatiramer acetate (GA). Researchers looked at reports of pregnancies where the father had taken GA around the time of conception, from 2001 to 2022. They got this information from the Teva Global Pharmacovigilance database. They included reports where the pregnancy was known about either before (prospective) or after (retrospective) the outcome was known. They looked at outcomes like major birth defects, miscarriages, pregnancy terminations, fetal deaths, premature births, and low birth weight. The study found a total of 466 pregnancies where the father had taken GA. Of these pregnancies, the final outcome of pregnancy was found for 349 pregnancies. Most of these pregnancies (90.5%) resulted in live births, 8.0% ended in miscarriage, 0.9% in termination, and 0.6% in stillbirth. Among prospective live births, 6.3% were premature, and 4.3% had low birth weight. The amount of major birth defects was 1.7%, which was slightly lower than usual. The study did not suggest that exposure of the father to GA negatively affects the pregnancy or the baby. These findings can help healthcare providers, male patients taking GA, and their partners who are thinking about pregnancy while the male partner is taking GA. [ABSTRACT FROM AUTHOR]

Published
2024
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37. The effect of complement C3 or C5 inhibition on geographic atrophy secondary to age-related macular degeneration: A living systematic review and meta-analysis.

Author

Garg, Anubhav, Nanji, Keean, Tai, Felicia, Phillips, Mark, Zeraatkar, Dena, Garg, Sunir J., Sadda, SriniVas R., Kaiser, Peter K., Guymer, Robyn H., Sivaprasad, Sobha, Wykoff, Charles C., and Chaudhary, Varun

Subjects
*MACULAR degeneration, *ECULIZUMAB, *COMPLEMENT inhibition, *ATROPHY, *GLATIRAMER acetate, *VISUAL acuity, *SQUARE root
Abstract

With the introduction of therapies to treat geographic atrophy (GA), GA management in clinical practice is now possible. A living systematic review can provide access to timely and robust evidence synthesis. This review found that complement factor 3 and 5 (C3 and C5) inhibition compared to sham likely reduces change in square root GA area at 12 months and untransformed GA area at 24 months. There is likely little to no difference in the rate of systemic treatment-emergent adverse events compared to sham. C3 and C5 inhibition, however, likely does not improve best-corrected visual acuity (BCVA) at 12 months, and the evidence is uncertain regarding change in BCVA at 24 months. Higher rates of ocular treatment emergent adverse effects with complement inhibition occur at 12 months and likely at 24 months. Complement inhibition likely results in new onset neovascular age-related macular degeneration at 12 months. This living meta-analysis will continuously incorporate new evidence. [ABSTRACT FROM AUTHOR]

Published
2024
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38. Capillary zone electrophoresis method for quantification of therapeutic peptide glatiramer acetate.

Author

Niaei, Navid, Vališ, Martin, and Petr, Jan

Abstract

This study presents the development and validation of a novel capillary zone electrophoresis method for the precise determination of glatiramer acetate and its amino acid constituents. A 120 mmol dm−3 phosphoric acid solution adjusted to pH 1.9 with Tris, supplemented with 20 mmol dm−3 triethylamine to achieve a final of pH 2.1, resulted in a repeatable analysis of glatiramer acetate. The method demonstrated a limit of detection and quantification of 39.2 µg cm−3 and 130.7 µg cm−3, respectively. This method allows for the rapid control of glatiramer acetate-based pharmaceuticals and distinguishes glatiramer acetate from the amino acids used in its synthesis. [ABSTRACT FROM AUTHOR]

Published
2024
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39. Protective Effects of Glatiramer Acetate Against Paclitaxel-Induced Peripheral Neuropathy in Rats: A Role for Inflammatory Cytokines and Oxidative Stress.

Author

Dekamin, Sajad, Ghasemi, Mehdi, Dehpour, Ahmad Reza, Ghazi-Khansari, Mahmoud, and Shafaroodi, Hamed

Subjects
*GLATIRAMER acetate, *PACLITAXEL, *PERIPHERAL neuropathy, *OXIDATIVE stress, *SCIATIC nerve, *RATS
Abstract

Chemotherapy-induced peripheral neuropathy (CIPN) is a major challenge for cancer patients who undergo chemotherapy with paclitaxel. Therefore, finding effective therapies for CIPN is crucial. Glatiramer acetate is used to treat multiple sclerosis that exerts neuroprotective properties in various studies. We hypothesized that glatiramer acetate could also improve the paclitaxel-induced peripheral neuropathy. We used a rat model of paclitaxel (2 mg/kg/every other day for 7 doses)-induced peripheral neuropathy. Rats were treated with either different doses of glatiramer acetate (1, 2, 4 mg/kg/day) or its vehicle for 14 days in separate groups. The mechanical and thermal sensitivity of the rats by using the Von Frey test and the Hot Plate test, respectively, were assessed during the study. The levels of oxidative stress (malondialdehyde and superoxide dismutase), inflammatory markers (TNF-α, IL-10, NF-kB), and nerve damage (H&E and S100B staining) in the sciatic nerves of the rats were also measured at the end of study. Glatiramer acetate (2 and 4 mg/kg) exerted beneficial effects on thermal and mechanical allodynia tests. It also modulated the inflammatory response by reducing TNF-α and NF-κB levels, enhancing IL-10 production, and improving the oxidative stress status by lowering malondialdehyde and increasing superoxide dismutase activity in the sciatic nerve of the rats. Furthermore, glatiramer acetate enhanced nerve conduction velocity in all treatment groups. Histological analysis revealed that glatiramer acetate (2 and 4 mg/kg) prevented paclitaxel-induced damage to the nerve structure. These results suggest that glatiramer acetate can alleviate the peripheral neuropathy induced by paclitaxel. [ABSTRACT FROM AUTHOR]

Published
2024
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40. Can Glatiramer Acetate Prevent Cognitive Impairment by Modulating Oxidative Stress in Patients with Multiple Sclerosis?

Author

Gil-Sánchez, Anna, Gonzalo, Hugo, Canudes, Marc, Nogueras, Lara, González-Mingot, Cristina, Valcheva, Petya, Torres, Pascual, Serrano, Jose Carlos, Peralta, Silvia, Solana, Maria José, and Brieva, Luis

Subjects
*GLATIRAMER acetate, *OXIDATIVE stress, *MULTIPLE sclerosis, *COGNITION disorders, *INTERFERON beta 1b, *COGNITIVE ability, *COGNITIVE therapy
Abstract

Multiple sclerosis (MS) is an autoimmune disease characterized by demyelination and neuroinflammation, often accompanied by cognitive impairment. This study aims (1) to investigate the potential of glatiramer acetate (GA) as a therapy for preventing cognitive decline in patients with MS (pwMS) by modulating oxidative stress (OS) and (2) to seek out the differences in cognition between pwMS in a cohort exhibiting good clinical evolution and control subjects (CS). An exploratory, prospective, multicentre, cross-sectional case–control study was conducted, involving three groups at a 1:1:1 ratio—41 GA-treated pwMS, 42 untreated pwMS, and 42 CS. The participants performed a neuropsychological battery and underwent venepuncture for blood sampling. The inclusion criteria required an Expanded Disability Status Scale score of ≤3.0 and a minimum of 5 years of MS disease. Concerning cognition, the CS had a better performance than the pwMS (p = <0.0001), and between those treated and untreated with GA, no statistically significant differences were found. Regarding oxidation, no statistically significant differences were detected. Upon categorizing the pwMS into cognitively impaired and cognitively preserved groups, the lactate was elevated in the pwMS with cognitive preservation (p = 0.038). The pwMS exhibited a worse cognitive performance than the CS. The pwMS treated with GA did not show an improvement in oxidation. Lactate emerged as a potential biomarker for cognitive preservation. [ABSTRACT FROM AUTHOR]

Published
2024
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41. Nicolau syndrome following glatiramer acetate for multiple sclerosis: Case and review of reports.

Author

Udawatta, Methma and Mateen, Farrah J.

Subjects
*GLATIRAMER acetate, *MULTIPLE sclerosis, *CONSCIOUSNESS raising, *RISK perception, *SYNDROMES
Abstract

Nicolau syndrome is a rare, iatrogenic skin reaction after parental drug administration, characterized by severe pain at an injection site, followed by hemorrhage, ulceration, and often necrosis. We present a case of a patient on glatiramer acetate for many years (initially Copaxone then Glatopa) who developed Nicolau syndrome, the second reported case after generic glatiramer acetate. All reported cases of Nicolau syndrome after glatiramer acetate are reviewed. The case highlights the importance of prompt recognition of this skin reaction by neurologists and raises awareness of the risks of skin reactions even in low‐risk injectable DMTs. [ABSTRACT FROM AUTHOR]

Published
2024
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42. Treatment switches of disease-modifying therapies in people with multiple sclerosis: long-term experience from the German MS Registry.

Author

Frahm, Niklas, Ellenberger, David, Stahmann, Alexander, Fneish, Firas, Lüftenegger, Daniel, Salmen, Hans C., Schirduan, Ksenija, Schaak, Tom P. A., Flachenecker, Peter, Kleinschnitz, Christoph, Paul, Friedemann, Krefting, Dagmar, Zettl, Uwe K., Peters, Melanie, and Warnke, Clemens

Subjects
MULTIPLE sclerosis treatment, SOCIODEMOGRAPHIC factors, BETA interferon, MONOCLONAL antibodies, GLATIRAMER acetate
Abstract

Background: The spectrum of disease-modifying therapies (DMTs) for people with multiple sclerosis (PwMS) has expanded over years, but data on treatment strategies is largely lacking. DMT switches are common clinical practice. Objective: To compare switchers and non-switchers, characterize the first DMT switch and identify reasons and predictors for switching the first DMT. Methods: Data on 2722 PwMS from the German MS Registry were retrospectively analyzed regarding sociodemographic/clinical differences between 1361 switchers (PwMS discontinuing the first DMT) and non-switchers matched according to age, sex, and observation period. Frequencies of first and second DMTs were calculated and switch reasons identified. Predictors for DMT switches were revealed using univariable and multivariable regression models. Results: Switchers and non-switchers differed significantly regarding time to first DMT, education, calendar period of the first DMT start (2014–2017 versus 2018–2021), first DMT class used [mild-to-moderate efficacy (MME) versus high-efficacy (HE) DMT], time on first DMT, and disease activity at first DMT start or cessation/last follow-up. The majority of PwMS started with MME DMTs (77.1%), with the most common being glatiramer acetate, dimethyl/diroximel fumarate, and beta-interferon variants. Switchers changed treatment more often to HE DMTs (39.6%), most commonly sphingosine-1-phosphate receptor modulators, anti-CD20 monoclonal antibodies, and natalizumab. Fewer PwMS switched to MME DMTs (35.9%), with the most common being dimethyl/diroximel fumarate, teriflunomide, or beta-interferon. Among 1045 PwMS with sufficient data (76.8% of 1361 switchers), the most frequent reasons for discontinuing the first DMT were disease activity despite DMT (63.1%), adverse events (17.1%), and patient request (8.3%). Predictors for the first DMT switch were MME DMT as initial treatment [odds ratio (OR) = 2.83 (1.76–4.61), p < 0.001; reference: HE DMT], first DMT initiation between 2014 and 2017 [OR = 11.55 (6.93–19.94), p < 0.001; reference: 2018–2021], and shorter time on first DMT [OR = 0.22 (0.18–0.27), p < 0.001]. Conclusion: The initial use of MME DMTs was among the strongest predictors of DMT discontinuation in a large German retrospective MS cohort, arguing for the need for prospective treatment strategy trials, not only but also on the initial broad use of HE DMTs in PwMS. [ABSTRACT FROM AUTHOR]

Published
2024
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43. Preparation and characterization of zein/gelatin electrospun film loaded with ε‐polylysine and gallic acid as tuna packaging system.

Author

Li, Qiuying, Zhou, Wenxuan, Yu, Xinrui, Cui, Fangchao, Tan, Xiqian, Sun, Tong, and Li, Jianrong

Subjects
*GALLIC acid, *TUNA, *CRYSTAL chemical bonds, *SHEWANELLA putrefaciens, *GELATIN, *FOOD packaging, *GLATIRAMER acetate
Abstract

BACKGROUND: Composite nanofiber films loaded with ε‐polylysine (PL) and gallic acid (GA) were prepared using a zein/gelatin (ZG) electrospinning method to develop effective active packaging films for tuna preservation. The morphology, structure, thermal stability, hydrophobicity, antibacterial, and antioxidant properties of the films, and their application for tuna during a period of storage of 4 °C were investigated. RESULTS: PL reduced the average diameter of ZG fibers, whereas GA increased it. The PL/GA/ZG film possessed a well distributed fiber morphology with an average diameter of 810 ± 150 nm. Fourier‐transform infrared spectroscopy and X‐ray diffraction results showed the physical loading of PL and GA in ZG film with the main chemical bonds and crystal structure unchanged. The addition of both PL and GA reduced hydrophobicity of the ZG film while the PL/GA/ZG film was still hydrophobic. GA enhanced its thermal stability and contributed to its antioxidant activity. PL and GA synergetically enhanced the antibacterial activity of ZG film against Shewanella putrefaciens. PL combined with GA is more suitable for modifying ZG film than GA alone. The PL/GA/ZG film effectively inhibited total viable counts, total volatile base nitrogen, fat oxidation, and texture deterioration of tuna fillets at 4 °C storage, and could extend the shelf life by 3 days. CONCLUSIONS: The PL/GA/ZG nanofiber film demonstrated promising potential for application in the preservation of aquatic products as a new antibacterial and antioxidant food packaging. © 2023 Society of Chemical Industry. [ABSTRACT FROM AUTHOR]

Published
2024
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44. Prospective study validating a multidimensional treatment decision score predicting the 24-month outcome in untreated patients with clinically isolated syndrome and early relapsing–remitting multiple sclerosis, the ProVal-MS study.

Author

Bayas, Antonios, Mansmann, Ulrich, Ön, Begum Irmak, Hoffmann, Verena S., Berthele, Achim, Mühlau, Mark, Kowarik, Markus C., Krumbholz, Markus, Senel, Makbule, Steuerwald, Verena, Naumann, Markus, Hartberger, Julia, Kerschensteiner, Martin, Oswald, Eva, Ruschil, Christoph, Ziemann, Ulf, Tumani, Hayrettin, Vardakas, Ioannis, Albashiti, Fady, and Kramer, Frank

Subjects
INTERFERON beta 1b, LONGITUDINAL method, MULTIPLE sclerosis, GLATIRAMER acetate, PROGNOSIS, DISEASE relapse
Abstract

Introduction: In Multiple Sclerosis (MS), patients´ characteristics and (bio)markers that reliably predict the individual disease prognosis at disease onset are lacking. Cohort studies allow a close follow-up of MS histories and a thorough phenotyping of patients. Therefore, a multicenter cohort study was initiated to implement a wide spectrum of data and (bio)markers in newly diagnosed patients. Methods: ProVal-MS (Prospective study to validate a multidimensional decision score that predicts treatment outcome at 24 months in untreated patients with clinically isolated syndrome or early Relapsing–Remitting-MS) is a prospective cohort study in patients with clinically isolated syndrome (CIS) or Relapsing–Remitting (RR)-MS (McDonald 2017 criteria), diagnosed within the last two years, conducted at five academic centers in Southern Germany. The collection of clinical, laboratory, imaging, and paraclinical data as well as biosamples is harmonized across centers. The primary goal is to validate (discrimination and calibration) the previously published DIFUTURE MS-Treatment Decision score (MS-TDS). The score supports clinical decision-making regarding the options of early (within 6 months after study baseline) platform medication (Interferon beta, glatiramer acetate, dimethyl/diroximel fumarate, teriflunomide), or no immediate treatment (> 6 months after baseline) of patients with early RR-MS and CIS by predicting the probability of new or enlarging lesions in cerebral magnetic resonance images (MRIs) between 6 and 24 months. Further objectives are refining the MS-TDS score and providing data to identify new markers reflecting disease course and severity. The project also provides a technical evaluation of the ProVal-MS cohort within the IT-infrastructure of the DIFUTURE consortium (Data Integration for Future Medicine) and assesses the efficacy of the data sharing techniques developed. Perspective: Clinical cohorts provide the infrastructure to discover and to validate relevant disease-specific findings. A successful validation of the MS-TDS will add a new clinical decision tool to the armamentarium of practicing MS neurologists from which newly diagnosed MS patients may take advantage. Trial registration ProVal-MS has been registered in the German Clinical Trials Register, 'Deutsches Register Klinischer Studien' (DRKS)—ID: DRKS00014034, date of registration: 21 December 2018; https://drks.de/search/en/trial/DRKS00014034 [ABSTRACT FROM AUTHOR]

Published
2024
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45. Glatiramer acetate induces mast cell degranulation via MRGPRX2, implications for local and systemic adverse reactions.

Author

Chaki, Shaswati, Amponnawarat, Aetas, Levenstein, Brett, Hui, Yvonne, Oskeritzian, Carole, and Ali, Hydar

Subjects
*GLATIRAMER acetate, *MAST cells, *CELL receptors, *STEM cell factor, *G protein coupled receptors, *MAST cell disease
Abstract

Glatiramer acetate (GA) is a drug used to treat relapsing-remitting multiple sclerosis (RRMS), but it can cause adverse reactions such as injection site reactions (ISRs) and immediate post-injection systemic reactions (IPISR). This study found that GA induces mast cell degranulation, which may contribute to these adverse effects. The researchers discovered that GA activates mast cells through the Mas-related G protein-coupled receptor X2 (MRGPRX2). Inhibitors of MRGPRX2 could potentially be used to prevent adverse reactions in RRMS patients. This finding also suggests that GA's inhibition of T cell responses and its induction of mast cell degranulation may have implications for the treatment of RRMS. [Extracted from the article]

Published
2024
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46. Altered placental immune cell composition and gene expression with isolated fetal spina bifida.

Author

White, Marina, Abdo, Hasan, Grynspan, David, Mieghem, Tim Van, and Connor, Kristin L.

Subjects
*GENE expression, *SPINA bifida, *NUCLEIC acid hybridization, *PREGNANT women, *FOLIC acid, *PLACENTA, *GLATIRAMER acetate, *BODY mass index
Abstract

Problem: Fetal spina bifida (SB) is more common in pregnant people with folate deficiency or anomalies of folate metabolism. It is also known that fetuses with SB have a higher risk of low birthweight, a condition that is typically placental‐mediated. We therefore hypothesized that fetal SB would associate with altered expression of key placental folate transporters and an increase in Hofbauer cells (HBCs), which are folate‐dependent placental macrophages. Method of study: Folate receptor‐α (FRα), proton coupled folate receptor (PCFT), and reduced folate carrier (RFC) protein localization and expression (immunohistochemistry) and HBC phenotypes (HBC abundance and folate receptor‐β [FRβ] expression; RNA in situ hybridization) were assessed in placentae from fetuses with SB (cases; n = 12) and in term (n = 10) and gestational age (GA) – and maternal body mass index – matched (n = 12) controls without congenital anomalies. Results: Cases had a higher proportion of placental villous cells that were HBCs (6.9% vs. 2.4%, p =.0001) and higher average HBC FRβ expression (3.2 mRNA molecules per HBC vs. 2.3, p =.03) than GA‐matched controls. HBCs in cases were largely polarized to a regulatory phenotype (median 92.1% of HBCs). In sex‐stratified analyses, only male cases had higher HBC levels and HBC FRβ expression than GA‐matched controls. There were no differences between groups in the total percent of syncytium and stromal cells that were positive for FRα, PCFT, or RFC protein immunolabeling. Conclusions: HBC abundance and FRβ expression by HBCs are increased in placentae of fetuses with SB, suggesting immune‐mediated dysregulation in placental phenotype, and could contribute to SB‐associated comorbidities. [ABSTRACT FROM AUTHOR]

Published
2024
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