A 2-year observational study of patients with relapsing-remitting multiple sclerosis converting to glatiramer acetate from other disease-modifying therapies: the COPTIMIZE trial

Ziemssen, Tjalf; Băjenaru, Ovidiu; Carrá, Adriana; Klippel, Nina De; Sà, João de; Edland, Astrid; Frederiksen, Jette Lautrup; Heinzlef, Olivier; Karageorgiou, K; Delgado, Rafael H. Lander; Landtblom, Anne‐Marie; Islas, Miguel Ángel Macías; Tubridy, Niall; Gilgun-Sherki, Yossi

doi:10.1007/s00415-014-7446-0

Cited by 35 publications

(28 citation statements)

References 38 publications

(50 reference statements)

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“…Switching to glatiramer acetate Several trials have evaluated switching to GA from other MS therapies for safety and efficacy reasons [81][82][83]. For patients not responding to first line therapies GA can be offered as an alternative to so-called second line medications if there are concerns of tolerability/adverse events with the latter therapies.…”

Section: Once-daily Formulation In Relapsing-remitting Multiple Sclermentioning

confidence: 99%

“…For patients not responding to first line therapies GA can be offered as an alternative to so-called second line medications if there are concerns of tolerability/adverse events with the latter therapies. Most studies describe switches from IFNβ-1a or -1b to GA, reporting reductions in mean ARR after switching [81][82][83]. However, in those situations when the shift is due to failure of the previous treatment, results should be interpreted with caution because the regression to the mean phenomenon is a major concern.…”

Section: Once-daily Formulation In Relapsing-remitting Multiple Sclermentioning

confidence: 99%

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The heritage of glatiramer acetate and its use in multiple sclerosis

Comı

Amato

Bertolotto

et al. 2016

Mult Scler Demyelinating Disord

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Multiple sclerosis (MS) is a chronic and progressively debilitating disease of the central nervous system. Treatment of MS involves disease-modifying therapies (DMTs) to reduce the incidence of relapses and prevent disease progression. Glatiramer acetate (Copaxone®) was the first of the currently approved DMTs to be tested in human subjects, and it is still considered a standard choice for first-line treatment. The mechanism of action of glatiramer acetate appears to be relatively complex and has not been completely elucidated, but it is likely that it involves both immunomodulating and neuroprotective properties. The efficacy of glatiramer acetate 20 mg/mL once daily as first-line treatment in relapsingremitting MS is well established, with ample evidence of efficacy from both placebo-controlled and active-comparator controlled clinical trials as well as real-world studies. There is also a considerable body of evidence indicating that the efficacy of glatiramer acetate is maintained in the long term. Clinical trial and real-world data have also consistently shown glatiramer acetate to be safe and well tolerated. Notably, glatiramer acetate has a good safety profile in women planning a pregnancy, and is not associated with foetal toxicity. Until recently, glatiramer acetate was only approved as 20 mg/mL once daily, but a new formulation with less frequent administration, 40 mg/mL three times weekly, has been developed and is now approved in many countries, including Italy. This review examines the mechanism of action, clinical efficacy, safety and tolerability of glatiramer acetate to provide suggestions for optimizing the use of this drug in the current MS therapeutic scenario.

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Section: Once-daily Formulation In Relapsing-remitting Multiple Sclermentioning

confidence: 99%

Section: Once-daily Formulation In Relapsing-remitting Multiple Sclermentioning

confidence: 99%

The heritage of glatiramer acetate and its use in multiple sclerosis

Comı

Amato

Bertolotto

et al. 2016

Mult Scler Demyelinating Disord

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“…Our study provides further insight into the effect of glatiramer acetate after treatment switch, supporting the improvement in MSrelated fatigue from the 6th month on glatiramer acetate. In addition, a recently published study has shown greater fatigue reduction in patients switching their immunomodulatory therapy as a result of lack of efficacy compared to those who switched due to adverse events [18] . These findings warrant further research to maximize fatigue benefits and prolong them in the long term.…”

Section: Discussionmentioning

confidence: 99%

“…Fatigue decrease over this first year was even sustained after 2 years of glatiramer acetate and was predicted by fatigue improvements achieved 6 months after starting the treatment [17] . Although similar reductions seem to occur in patients previously treated with other immunomodulatory/immunosuppressive therapies [17,18] , the evidence available is still limited, less consistent [16,17] , and potentially affected by secondary causes of fatigue such as depressive symptoms [16][17][18] .…”

Section: Introductionmentioning

confidence: 91%

Fatigue Improvement after Switching Multiple Sclerosis Treatment from Interferon-β to Glatiramer Acetate in Clinical Practice

Meca-Lallana

Hernández²,

Caminero

et al. 2016

Eur Neurol

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Background/Aims: The immunomodulatory effect of glatiramer acetate may help in reducing multiple sclerosis (MS)-related fatigue; however, evidence to prove this notion especially after switching from another immunomodulatory therapy is limited. We assessed the 6-month effect of glatiramer acetate on MS-related fatigue in patients switching from interferon-β (IFN-β) in clinical practice. Methods: This was an observational study including 54 patients with relapsing-remitting MS that showed moderate/severe fatigue primarily caused by MS before switching from IFN-β to glatiramer acetate and received glatiramer acetate for ≥6 months in daily practice. Study data were retrospectively collected through chart review at treatment switch and over the following 6 months on glatiramer acetate. Results: Over the 6-month administration of glatiramer acetate, scores on the Modified Fatigue Impact Scale decreased: overall (p < 0.001), physical scale (p < 0.001), cognitive scale (p < 0.001), and psychosocial scale (p < 0.001). The Work Productivity and Activity Impairment Questionnaire showed improvements in work (p = 0.009) and other daily activity impairment (p < 0.001). Health-related quality of life as per the Multiple Sclerosis Impact Scale also improved: physical score (p < 0.001) and psychological score (p < 0.001). Conclusion: Patients with moderate/severe fatigue switching from IFN-β to glatiramer acetate may benefit from fatigue improvements that contribute to reduce their work/activity impairment and improve their quality of life.

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“…These Also Natalizumab, the first monoclonal antibody to treat highly active multiple sclerosis, with studies demonstrating better efficacy on disease activity and disability progression compared to interferons (e.g., Ref. 37,38 ), demonstrated in a reanalysis of the SENTINEL 39 and AFFIRM 40 phase III studies that treatment with Natalizumab reduced the risk of confirmed progression of cognitive deficits by 43% in comparison with a placebo. 41 The same applies to the STRATA extension study, where cognitive impairments were assessed monthly using the SDMT and MSNQ until the end of the study after 48 weeks.…”

Section: Immunomodulatory Treatments and Cognitionmentioning

confidence: 99%

Immunomodulatory treatments and cognition in MS

2016

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Cognitive impairments occur frequently and early in multiple sclerosis (MS) and contribute significantly to a reduced quality of life of patients with MS. Executive functions (EFs) play a pivotal role for the behavioral adaption to the environment and are also crucial for compensatory processes of cognitive impairments. Disease-modifying drugs (DMDs) are effective in reducing the frequency of relapses and slow the disease progression in MS. The effects of DMDs on cognitive impairments were reviewed with a special focus on EFs. Most studies show some beneficial effects of DMDs on cognition in MS, but the evidence for effects on EFs is sparse. Additionally, most studies suffer from methodological issues, small sample sizes and learning effects. We discuss that EFs may constitute a viable cognitive endpoint for cognitive impairments in MS, which could foster the early detection of subtle cognitive changes in MS. K E Y W O R D Scognition, disease-modifying drugs, executive functions, multiple sclerosis 1

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A 2-year observational study of patients with relapsing-remitting multiple sclerosis converting to glatiramer acetate from other disease-modifying therapies: the COPTIMIZE trial

Cited by 35 publications

References 38 publications

The heritage of glatiramer acetate and its use in multiple sclerosis

The heritage of glatiramer acetate and its use in multiple sclerosis

Fatigue Improvement after Switching Multiple Sclerosis Treatment from Interferon-β to Glatiramer Acetate in Clinical Practice

Immunomodulatory treatments and cognition in MS

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