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Biologics : Targets & Therapy logoLink to Biologics : Targets & Therapy
. 2009 Jul 13;3:257–271.

Early stage and long term treatment of multiple sclerosis with interferon-β

Angela Applebee 1, Hillel Panitch 1,
PMCID: PMC2726076  PMID: 19707414

Abstract

Multiple sclerosis (MS) affects young adults during the most productive years of their lives, and until recently many neurologists were limited to treating symptoms and attacks without any ability to alter the disease course. The 1990s ushered in an era of possibility with the approval of three interferon-beta (IFNβ) therapies for the treatment of MS. Though the mechanism of action of these agents is not completely understood, it is clear they reduce magnetic resonance imaging (MRI) activity as well as improve clinical outcomes. The principal randomized, blinded, multicenter trials of IFNβ all point to the need for early treatment soon after the diagnosis of MS is made. Efficacy has also been shown in patients treated after a first demyelinating event. Data on IFNβ in the treatment of secondary progressive MS (SPMS) is not impressive, although it shows some benefit in SPMS patients who continue to experience MRI activity and clinical relapses, signifying a continued inflammatory component to their disease. There has been no proven efficacy of IFNβ in the treatment of primary progressive MS (PPMS). The IFNβ therapies are generally well tolerated with a favorable side effect profile. Despite benefits in MRI and clinical measures such as relapse rates and Expanded Disability Status Scale progression, patients continue to exhibit clinical progression and radiological atrophy, pointing to confounding factors and perhaps multiple etiologies of a disease that is not yet fully understood. In addition, the subject of neutralizing antibodies has recently assumed importance. The significance of these on treatment efficacy is uncertain, and until a universally accepted reliable assay is adopted, the decision to change treatment continues to rely on the clinical interpretation of the patient’s history and physical examination. Additional recommendations for management of patients, informed by the best available evidence, are also presented.

Keywords: interferon-β, multiple sclerosis, clinical trials, neutralizing antibodies

Introduction

Multiple sclerosis (MS) is characterized by unpredictable signs and symptoms involving the sensory, motor, visual, and brainstem systems. Recently, cognitive and mood disturbances have also become more widely recognized in these patients. The disease is also highly variable in terms of the frequency and severity of attacks, as well as the extent and rate of progression of disability. Despite this unpredictability, neurologists categorize patients into one of four forms based on disease course. The currently accepted classification of MS into four forms was established by an international survey.1 The most common form is relapsing remitting MS (RRMS), which accounts for 85% of MS cases at onset. This is characterized by relapses, also known as attacks or exacerbations, followed either by full recovery, or a residual neurological deficit. Relapses are defined as neurologic symptoms lasting more than 24 hours, preceded by at least one month of stability, and accompanied by a change in the neurologic examination that cannot be explained by an infection or other illness. The time between attacks is characterized as a remission or lack of disease progression whether or not the patient’s neurologic status returns to baseline. Approximately 50% of RRMS patients will go on to develop secondary progressive MS (SPMS) within 10 years. SPMS is defined by an initial relapsing remitting course, followed by gradual progression with or without occasional relapses or plateaus. These patients are usually more disabled than RRMS patients, and the disability results from incomplete recovery from exacerbations as well as steady progression.

Patients with primary progressive MS (PPMS) make up approximately 10% of the population. PPMS patients have disease progression from onset, sometimes with infrequent plateaus or minor improvements. The hallmark of PPMS is continued worsening of the baseline without clear relapses. Progressive relapsing MS (PRMS) is the rarest form, compromising approximately 5% of MS patients. These individuals have a progressive course from disease onset with one or more superimposed acute relapses, following which the progression continues. A related condition is the clinically isolated syndrome (CIS), defined as a single demyelinating event suggestive of an initial MS attack. These patients are at risk of developing RRMS, but do not meet currently accepted criteria for MS because of a lack of clinical or radiologic episodes separated in time and space. Patients with T2 magnetic resonance imaging (MRI) lesions at onset have a substantially greater risk of developing MS and progression of disability, than those with normal MRI scans.2

Treatment of MS patients can be divided into three types: acute, disease-modifying, and symptomatic. Prior to the early 1990s, management of MS patients was limited to acute and symptomatic treatment, leaving neurologists at a loss as to what to do between attacks. In 1993, the first disease-modifying agent for the treatment of MS was approved by the US Food and Drug Administration (FDA), and over the course of the next few years, two other IFNβ agents gained FDA approval for treatment of relapsing forms of MS. There is still much to be learned regarding the pathogenesis of this disease, one clear aspect being that a component of immune dysregulation occurs which responds moderately well to immunomodulating treatment. A complete review of all the disease-modifying therapies, or even all aspects of IFNβ, is beyond the scope of this review. Our aim, rather, is to address briefly the proposed mechanisms of action of the IFNβ preparations, describe their proven efficacy and safety in clinical trials, discuss the importance of neutralizing antibodies and other safety issues, and conclude with therapeutic recommendations based on these factors, and on our own experience, for the treatment of patients with MS.

Mechanism of action

Experimental evidence supports the hypothesis that the MS disease process is due, at least in part, to autoimmunity.35 The currently prevalent theory involves the activation of autoreactive type 1 T helper (Th1) cells in the peripheral immune system. Th1 cells are exposed either to self antigens or to molecules that closely mimic them, and become activated in the presence of co-stimulatory molecules, leading to the release of proinflammatory cytokines such as interleukin 12 (IL-12), IL-17, interferon gamma (IFNγ), and tumor necrosis factors. Associated with this, there is an up-regulation of adhesion molecules allowing for binding of T cells and transmigration across the endothelial surface of CNS venules. The activated T cells then attack the basement membrane component of the blood–brain barrier (BBB) by secreting matrix metalloproteinases (MMP), proteolytic enzymes that increase BBB permeability and allow for passage of the T cell into the CNS. This process is then amplified upon entry into the CNS by presentation of myelin autoantigens and further production of inflammatory cytokines, leading to the destruction of myelin and axons. This is, of course, a greatly simplified view of the process, many aspects of which are still under investigation.

There are multiple mechanisms by which IFNβ is proposed to work, beginning with down regulation of major histocompatibility complex type 2 (MHC II) expression. The antigen-MHC II complex is recognized on the surface of an antigen presenting cell by a Th1 cell, leading to activation. Downregulation of MHC II leads to decreased presentation of self antigens and decreased Th1 activation. IFNγ, a pro-inflammatory cytokine, usually up-regulates MHC II complexes and IFNβ is thought to interfere with this process.6 IFNβ also affects IFNγ another way, by decreasing its release from activated T cells.7 IFNβ has been shown to decrease the co-stimulatory molecules necessary to activate T cells,8 and may also bring about a shift from a pro-inflammatory (Th1) state to an anti-inflammatory state characterized by proliferation of type 2 (Th2) T helper cells. A recent study showed a shift of cytokines from those that promote inflammation, eg, IL-12, to anti-inflammatory cytokines, such as IL-10, thus supporting a shift from a Th1 to a Th2 type milieu.9

IFNβ can affect BBB permeability to cells and proteins via multiple mechanisms, the most important of which is probably inhibition of MMP production by T cells, thereby preventing breakdown of the subendothelial extracellular matrix and passage of activated T cells into the CNS.10,11 This effect is most vividly demonstrated by the dramatic reduction in gadolinium-enhancing lesions seen on MRI almost immediately after treatment with IFNβ is begun.12 Interferons were also recently found to demonstrate a direct stabilizing effect on endothelial cells in vitro limiting the migration of small particles into the CNS.13 Another potential mechanism involves the adhesion of activated T cells to the endothelial surface. Patients receiving IFNβ have been shown to produce soluble vascular cell adhesion molecule (VCAM), corresponding to a reduction in contrast enhancing lesions on MRI.14,15 Thus soluble VCAM may act as a decoy, binding to activated T cells and keeping them from crossing into the CNS.

IFNβ also inhibits the expansion of T cell clones16 and was found to increase T cell death through inhibition of FLIP, an antiapoptotic protein.17 Other investigators have focused on regulation of cytokine and growth factor production in MS. For example, IFNβ may promote production of the suppressive cytokine IL-10 by activated T cells in early MS, but not in later stage progressive forms of the disease.18 Effects on IFNγ and brain-derived neurotrophic factor (BDNF) have also been studied, with interesting but sometimes paradoxical results that require further analysis.19

Researchers have also turned their attention to molecular mechanisms by which interferon therapy may exert its action. Because interferons act by promoting gene activation via intracellular transcription factors, changes in mRNA expression can be identified in patients exposed to interferon therapy. Many studies, eg,20 have focused on expression of genes thought to be involved in MS. Recently, however, investigators have attempted to cast a broader net, using cDNA microarrays to detect changes in gene expression related to IFNβ therapy,21 or to identify responders and non-responders to IFNβ therapy.22 Although this area of research is preliminary, it may represent an important step toward linking MS etiology and therapy.23

Currently, there are two forms of IFNβ approved for the treatment of MS, both of which are produced by recombinant DNA technology. IFNβ-1a (Avonex®, Biogen Idec and Rebif®, Merck Serono) is produced in Chinese hamster ovary cell lines. These molecules are glycoproteins with a 166 amino acid sequence, identical to that of human IFNβ; however, the glycosylation patterns are different, and not necessarily identical to those found in human IFN-β. IFNβ-1b (Betaseron®, Bayer HealthCare or Betaferon®, Schering AG) is produced in an Escherichia Coli cell line and is not glycosylated, as bacteria cannot glycosylate proteins. IFNβ-1b has an amino acid substitution, serine for cysteine at position 17, to prevent aggregation and preserve proper folding and biologic function. This molecule also differs slightly from IFNβ-1a in length, as it contains only 165 amino acids due to deletion of the N-terminal methionine. The differences between IFNβ-1b and IFNβ-1a have certain consequences that are thought to be important, such as lower specific activity of IFNβ-1b, as well as an increased tendency to neutralizing antibody (NAb) formation in patients treated with IFNβ-1b. The 1990s saw several randomized controlled trials addressing the efficacy of IFNβ in the treatment of multiple sclerosis. Tables 1 and 2 list the large multicenter studies for the treatment of MS and CIS with the different forms of IFNβ.24

Table 1.

Principal randomized clinical trials in relapsing-remitting MS

Trial (number enrolled; follow-up time) Treatment Primary outcome measures Key results
IFNβ-1b (RRMS; 372; 2,3,5 years) Placebo vs 8 MIU vs 1.6 MIU IFNβ-1b SC QOD Reduction in annual exacerbation rates and proportion of exacerbation free patients. Showed a significant reduction in relapses and MRI disease burden. Outcome on relapse free patients was significant at 2 years. Not powered to assess disability outcomes.
MSCRG (RRMS; 301; 2 years, though stopped early) Placebo vs 30 μg IFN-β-1a IM weekly Time to sustained disability of at least one point on the EDSS. Time to sustained progression significant at 104 weeks. Significant reduction in new MRI lesions and relapse rate also noted.
PRISMS (RRMS; 560; 2, 4, 8 years) Placebo vs 22 or 44 mg IFNβ-1a SC TIW Relapse count over the course of the study. Both treatment arms showed significance in time to sustained disability. Affect on relapse rate, severity of relapses, and MRI burden of disease was also significant.
INCOMIN (RRMS; 188; 2 years) IFN-β1a 30 μg IM weekly vs IFNβ-1b 8 MIU SC QOD Proportion of patients free from relapses during the 2 years of study. IFN β-1b showed significant difference in remaining relapse free over IFNβ-1a (56% vs 36% p = 0.036). Significant reduction in T2 lesions also seen in the IFNβ-1b group.
EVIDENCE (RRMS; 412; 6, 12, 16 months) IFNβ-1a 30 μg IM weekly vs IFNβ-1a 44 μg SC TIW Proportion of patients relapse- free and number of active MRI lesions per patient at 6 months, extended to 12 and 16 months. IFNβ-1a SC superior to IFNβ-1a IM in proportion relapse free at 24 weeks (75% vs 63%, p = 0.005), 48 weeks (62% vs 52%) and 64 weeks (56% vs 48%). IFNβ-1a SC also had significant effect on MRI measures throughout the study.
Danish MS Group (RRMS; 292 randomized and 120 NR; 2 years) Randomized IFNβ-1a SC 22 μg weekly vs IFNβ-1b 250 μg QOD; NR 250 μg IFNβ-1b QOD Annualized relapse rates, time to first relapse, and NAb formation. Annualized relapse rates were equal in randomized treatment arms. Time to first relapse and sustained progression were also equal. NR patients showed a trend toward shorter progression time but no other significant differences.

Abbreviations: MS, multiple sclerosis; IFN, interferon; RRMS, relapsing remitting MS; MIU, million international units; SC, subcutaneous; MSCRG, multiple sclerosis collaborative research group; μg, micrograms; IM, intramuscularly; EDSS, expanded disability scale; TIW, three times weekly; QOD, every other day; NAb, neutralizing antibodies; NR, nonrandomized.

Table 2.

Principal randomized clinical trials in SPMS and CIS

Trial (MS form; number enrolled; follow-up time) Treatments Primary outcome tested Key results
European IFNβ-1b (SPMS; 718; 3 years, early termination for efficacy) Placebo vs IFNβ-1b 8 MIU SC QOD Time to confirmed disability as measured by EDSS. Treatment showed significant difference in time to confirmed progression. Significant reductions in relapse rate and MRI activity also noted.
North American IFN-β1b (SPMS; 939; 3 years with early termination for lack of efficacy) Placebo vs IFNβ-1b 8 MIU SC or 5 MIU/M2 SC QOD Time to confirmed disability as measured by EDSS. No effect on disease progression or EDSS. Significant effects on relapse rate and MRI activity were noted.
IMPACT (SPMS; 436; 2 years) Placebo vs IFNβ-1a 60 μg IM weekly MSFC change from baseline to months 24. Treatment improved median MSFC by 40%. No benefit on EDSS. Significant benefits seen in relapse rate and MRI outcomes.
SPECTRIMS (SPMS; 618; 3 years) Placebo vs IFNβ-1a 22 μg or 44 μg SC TIW Time to confirmed disability as measured by EDSS. No affect on disability progression. Significant beneficial effects on relapse rates and MRI outcomes.
BENEFIT (CIS; 468; 2, 3 years) Placebo vs IFN-β1b 250 μg QOD. Delay of conversion to CDMS and McDonald MS. Delayed conversion to CDMS and McDonald MS (31% vs 15%, p < 0.0001). Significant effect on MRI measures also. At 3 yrs delayed EDSS progression
CHAMPS (CIS; 383; 3 years with early termination due to efficacy) IV and oral steroids first, followed by placebo vs IFNβ-1a 30 μg IM weekly Delay of conversion to CDMS. Delayed conversion to CDMS (50% vs 35%, p = 0.002).
Significant effect on MRI measures.
ETOMS (CIS; 309; 2 years) Placebo vs IFNβ-1a 22 μg SC weekly Delay of conversion to CDMS. Delayed conversion to CDMS (45% vs 34%, p = 0.047).
Significant effect on MRI measures.

Abbreviations: MS, multiple sclerosis; SPMS, secondary progressive MS; IFN, interferon; SC, subcutaneous; IM, intramuscular; μg, micrograms; MSFC, MS functional composite; CIS, clinically isolated syndrome; CDMS, clinically definite MS; QOD, every other day; TIW, three times weekly.

Efficacy of IFNβ in MS

The first pilot study of IFNβ-1b for the treatment of MS was performed in the late 1980s.25 Thirty RRMS patients were randomized to receive 0.8, 4, 8, or 16 million international units (MIU) of IFNβ-1b or placebo via subcutaneous (SC) injection administered three times per week (TIW). The 8 MIU dose was reasonably well tolerated; however, the 16 MIU caused excessive side effects. This study showed a dose dependent reduction in attacks, but an effect of treatment on disease progression could not be assessed.

A phase III trial of IFNβ-1b in MS was initiated in 1988.26 The primary outcome measures were reduction in annual exacerbation rate and proportion of exacerbation free patients. Three hundred seventy-two clinically definite RRMS patients were enrolled at 11 centers in the United States and Canada. Patients were between the ages of 18 and 50, had a history of two exacerbations within the previous two years, and an Expanded Disability Status Scale (EDSS) score27 of 5.5 or less. Subjects were randomized to receive placebo, high dose (8 MIU), or low dose (1.6 MIU) of IFNβ-1b by SC injection every other day. MRI scans were performed yearly with the exception of a subset of patients at a single site who were scanned every six weeks for the first two years to assess the effect of treatment more closely. This study was initially planned for two years, was subsequently extended to three years, and then to five years. The three-year data revealed statistically significant results in the treatment arms compared to placebo.26,28 The annual exacerbation rate for the high dose group (0.84) was less than for the placebo group (1.27), with a p value of 0.0001, approximately a one-third reduction in the frequency of exacerbations. Moderate and severe attacks were decreased by 50% compared to placebo. The number of exacerbation-free patients at two years was statistically significant in the high dose group; however this was not maintained at three years. The effect of IFNβ-1b on disease progression, as measured by change in EDSS scores, did not reach statistical significance. Inclusion of the low dose group revealed a dose-response effect, with values for most outcome measures falling between the placebo and high-dose groups.

Cumulative disease burden (an approximation of lesion volume) on MRI showed a highly significant effect of high dose IFNβ-1b compared to placebo (p = 0.002). MRI activity assessed by measuring new or enlarging lesions in the subset of patients undergoing frequent MRI scanning every six weeks for two years showed an 80% reduction of activity with high dose treatment. In a subsequent report29 the median time on study for patients was 4 years, with a few reaching 5 years. When all data were pooled for all time points in the study, a 30% reduction in relapse rate persisted in the high dose treatment arm (0.78 per year compared with 1.12 for placebo; p = 0.0006). Although the exacerbation rates each year were approximately one-third lower in the high dose treatment arm, after year 2 this was not statistically significant, probably due to dropouts and loss of statistical power. The MRI efficacy of IFNβ-1b persisted through year 5, with no significant increase in lesion burden. The study was not powered to show a significant effect on disease progression. Both doses of IFNβ-1b were tolerated well enough for the FDA to grant approval without undue concern for serious adverse events.

IFNβ-1b was subsequently tested in patients with SPMS with conflicting results in two placebo-controlled multi-center randomized studies. In the European study,30 718 patients with SPMS and EDSS scores of 3.0 to 6.5, with confirmed progression or at least two exacerbations in the prior two years, were randomized to either 8 MIU of IFNβ-1b or placebo every other day. The primary outcome was time to confirmed progression of disability, as measured by a one-point increase on the EDSS, sustained for three months (or a 0.5-point increase if the baseline EDSS was 6.0 or 6.5). The study was terminated shortly before its planned end point of three years because of statistically convincing evidence of efficacy. A significant difference in time to confirmed progression was found in favor of IFNβ-1b (p = 0.0008). The IFN group had a 21.7% reduction in rate of progression, or a 12-month delay in reaching similar disability levels compared with placebo. This effect was also seen in time to becoming wheelchair bound (EDSS 7.0 or greater) being delayed by nine months. There were significant reductions in relapse rates and in MRI activity as measured by contrast enhancing lesions; however, there was no reduction in brain atrophy. The results of this study led to the approval of IFNβ-1b in Europe and Canada for the treatment of patients with SPMS.

The second trial of IFNβ-1b in SPMS was performed in the United States and Canada.31 Patients eligible for randomization had EDSS scores of 3.0–6.5, and an increase in their EDSS scores of at least one point in the two years prior to screening. There was no relapse requirement other than a history of one relapse at some time in the past, to confirm the diagnosis of SPMS. Nine hundred thirty-nine patients were randomized to IFNβ-1b 8 MIU, or a variable dose of 5 MIU/m2, or to one of two matching placebo arms administered SC every other day. The planned outcome measures were the same as in the European study. This trial was planned for a three year end-point, but was stopped early because an interim data analysis indicated the inability to achieve a significant difference in the primary outcome measure. In contrast to the European study, treatment with IFNβ-1b did not improve disability measures compared with placebo. Consistent with previous studies, there was a significant reduction in the already low relapse rates and in MRI measures of activity.

The disparity between these two studies has been the subject of much debate. When differences in baseline demographics were analyzed,32 patients in the European trial were found to be younger, to have higher relapse rates prior to entry, shorter disease duration, and a higher proportion of contrast enhancing lesions. The entry criteria for these two studies may have added to the differences seen, as the European trial required either two relapses or a one-point increase in the EDSS over two years to document disease progression, whereas the North American trial excluded patients with relapses and required a one-point deterioration in two years. In the European study, this may have selected for patients earlier in the disease course, characterized by more intense inflammation, and therefore a greater tendency to respond to IFNβ-1b. Kappos and colleagues (2004) also remarked on the lack of approved therapies in Europe for the treatment of MS at the time of enrollment in the trial. In North America, during enrollment of the SPMS trial there was already one approved immunomodulatory therapy, and two others became available during the course of the study. Thus, patients in the North American group may have been preselected for a lower likelihood of responding to IFNβ-1b. The authors of the retrospective analysis concluded that SPMS patients with continuing superimposed relapses may be more likely to benefit from IFNβ-1b treatment.

The efficacy and tolerability of IFNβ-1b in the treatment of clinically isolated syndromes (CIS) was recently reported.33 The Betaferon in Newly Emerging Multiple Sclerosis for Initial Treatment (BENEFIT) trial was a multicenter, randomized, double-blind, placebo controlled trial assessing the effect of treatment on the rate of conversion to clinically definite MS (CDMS) as defined by the Poser criteria34 and furthermore, as defined by the newer McDonald criteria.35 Four hundred sixty-eight patients with a first clinical demyelinating event (either monosymptomatic or polysymptomatic) and at least two clinically silent MRI lesions were randomized in a five to three ratio to receive either 8 MIU of IFNβ-1b or placebo subcutaneously every other day. Exacerbations were documented by an examining physician and when the diagnosis of CDMS was confirmed, the patient was offered open-label treatment. IFNβ-1b significantly delayed the onset of CDMS and “McDonald MS” (p < 0.0001). At the end of the two year study, the probability of not developing “McDonald MS” was twice as high with IFNβ-1b (31%) as with placebo (15%). IFNβ-1b significantly reduced MRI activity and was well tolerated, as indicated by the low dropout rate (7.2%) in the IFNβ-1b group.

Following the two year placebo-controlled phase, patients were eligible to enter an open-label follow-up phase and were offered IFNβ-1b 250 μg subcutaneously every other day for up to five years from randomization.36 Follow-up visits occurred every six months with a blinded examiner performing a standardized neurological assessment and EDSS score. The primary outcomes of this analysis were time to diagnosis of CDMS, time to confirmed EDSS progression, and score on a patient-reported functional assessment scale. Eighty-nine percent of patients entered the follow-up phase with 84% completing three years. At that time, early treatment was shown to reduce the risk of developing CDMS by 41% (absolute risk reduction of 14%) compared to delayed treatment. More importantly, early treatment reduced the risk for progression of disability, as measured by a sustained one point change in the EDSS, by 40% compared to the delayed treatment group.

The pivotal trial of IFNβ-1a (Avonex®) was the first to use delay of disability, as measured by time to progression of the EDSS score by one point sustained for six months, as the primary outcome measure.37 The investigators enrolled 301 relapsing MS patients with at least two exacerbations during the previous three years, and EDSS scores of 1.0 to 3.5. Patients were randomized to receive either IFNβ-1a 6 MIU (30 μg) or placebo by weekly intramuscular (IM) injection. This study was designed with a two-year end-point in mind; however, the number of dropouts was lower than anticipated, and the study was terminated early. Only 57% of patients completed two years, and 77% completed 18 months. Time to sustained progression was significantly greater in IFNβ-1a treated patients (21.9%) compared with placebo (34.9%) at 104 weeks (p = 0.02). There was a significant reduction in relapse rates, most evident at the end of year 2. This reduction was 31% for those completing two years, but only 18% for all patients in the study.

A significant reduction in gadolinium enhancing lesions was present at year 1, and was maintained at year 2 (p = 0.02), but the effect on total T2 lesion volume was not significant. Tolerance of the drug was acceptable, considering the inherent discomfort of the IM injection route. Subsequent re-analysis of the data by the investigators38 included a change of EDSS greater than two points, or sustained progression by one point for one year, with the conclusion that the previous results underestimated the effect of IFNβ-1a. Further post-hoc analysis revealed benefit in some areas of neuropsychological testing and degree of brain atrophy in patients treated with IFNβ-1a.39,40

Although IM IFNβ-1a was modestly effective in the treatment of relapsing MS patients, the optimal dose was not established. A randomized, double-blind, dose-comparison study of weekly IFNβ-1a comparing 30 μg versus 60 μg by weekly IM injection was therefore conducted.41 The primary endpoint was six-month EDSS progression, and there were multiple other clinical and MRI secondary outcome measures. Eight hundred two relapsing MS patients with EDSS scores of 2.0 to 5.5 were enrolled and randomized to either treatment arm. At 36 months, there was no statistical difference between the two treatment arms in either primary or secondary endpoints. 608 patients completed 36 months, and 448 patients remained in an extension of the trial to 48 months. At that time, there continued to be no statistical difference between the 30 μg and 60 μg weekly doses in terms of efficacy or safety.42 In the absence of a placebo group, the meaning of these findings is dubious.

The effect of IM IFNβ-1a in SPMS was evaluated in the International Multiple Sclerosis Secondary Progressive Avonex Clinical Trial (IMPACT), which enrolled 436 SPMS patients with progression over the previous year, and EDSS scores of 3.5 to 6.5.43 This trial was designed to determine whether 60 μg IFNβ-1a given once weekly by the IM route was more effective than placebo as measured by changes at two years in the MS Functional Composite (MSFC), a novel measure of disability.44 IFNβ-1a treatment reduced median MSFC worsening by 40% (p = 0.033). This effect was primarily driven by the nine-hole peg test and the paced auditory serial addition test. No benefit was seen on the EDSS, a secondary endpoint. Significant benefits in relapse rate and MRI outcomes were noted in IFN-treated subjects. This was the first study to use the MSFC to assess disability, but because it had not yet been validated as an outcome measure, the FDA refused to approve IM IFNβ-1a for the treatment of SPMS.

The Controlled High-Risk Avonex Multiple Sclerosis Prevention Study (CHAMPS) trial45 sought to determine whether patients with CIS treated with 30 μg of IFNβ-1a intramuscularly once weekly are less likely to develop CDMS. This randomized double-blind study enrolled 383 patients with a first isolated demyelinating event of optic neuritis, incomplete transverse myelitis, or brainstem – cerebellar dysfunction. Patients were also required to have two or more T2 signal abnormalities consistent with demyelination on their MRI scans. Patients were screened within two weeks of symptom onset and all received a three-day course of one gram of intravenous methylprednisolone followed by 14 days of oral prednisone. Treatment with IFNβ-1a began within four weeks of the initial event. The primary outcome measure was conversion to CDMS, which required documentation of new symptoms suggesting a relapse, and confirmation by a central end-point committee. MRI scans were performed every six months for the first 18 months, but were not required to confirm the diagnosis of CDMS. When CDMS was confirmed, subjects were removed from the study and offered treatment with IFNβ-1a. This trial was terminated early because of significant evidence of efficacy in the treatment group compared to controls. There was a cumulative probability of 50% of placebo patients having a second attack, compared to 35% of those treated with IFNβ-1a (p = 0.002). Changes in the volume of brain lesions on T2 weighted MRI were statistically significant in the treatment arm as well. Following publication of this study, the FDA approved the use of IM IFNβ-1a for the treatment of CIS.

In a small randomized controlled trial of PPMS patients treated with IFNβ-1a,46 fifty patients were randomized to weekly IM injections of IFNβ-1a at doses of 30 μg, 60 μg, or placebo for two years. The primary endpoint of sustained progression in disability was not met in either active treatment arm. Larger studies in PPMS have not been performed.

The pivotal study of IFNβ-1a (Rebif®) given by SC injection was PRISMS (Prevention of Relapses and Disability by Interferon β-1a Subcutaneously in Multiple Sclerosis), a multicenter, randomized, placebo controlled trial of 560 patients with RRMS.47 Patients were eligible if they had had at least two relapses in the preceding two years and EDSS scores between 0 and 5.0. They were randomized to either 22 μg, 44 μg, or placebo treatment arms, and were treated TIW for two years. The primary outcome measure was relapse count over the course of the study. Both treatment groups had significant reductions in relapse rate compared with controls, achieving 27% and 33% reductions for the 22 μg and 44 μg doses respectively over the study period (p < 0.0002). Both doses also showed significance in percentage of relapse free patients, time to first relapse, and severity of relapses. Time to sustained progression was significantly longer (p < 0.05) in both interferon IFNβ-1a treatment groups than in the placebo group. A composite score of integrated disability (area under the EDSS curve over time) showed a 77% reduction in accumulated burden of disability during the study. The number of enhancing lesions as well as T2 lesion volume on MRI were significantly lower in both treatment groups (p < 0.0001).48 Although the higher dose group did better, there was no statistical difference between the two doses on major clinical outcomes.

After completion of the initial two-year PRISMS trial, the study was extended (PRISMS-4) and patients initially receiving placebo were re-randomized to either high or low dose IFNβ-1a.49 Those already on interferon therapy remained on their current dose. The primary outcome was relapse count per patient over four years. Ninety percent of patients randomized in the initial trial were enrolled in PRISMS-4. At the end of four years, there was continued evidence of efficacy, and a dose effect became more apparent, particularly on MRI outcomes. Most notably, confirmed progression of disability was lowest in the patients who took high dose IFNβ-1a for four years, and highest in those who received placebo for two years followed by low dose IFNβ-1a for the next two years. The effect was intermediate for the other two groups, supporting the idea of starting therapy as soon as possible after diagnosis.

A long-term follow up (LTFU) at 7–8 years of the PRISMS study was recently published.50 Sixty-eight percent (382/560) of patients from the original PRISMS trial returned for assessment. At LTFU, 80% of the cohort had not progressed to SPMS, and the mean T2 lesion load and relapse rate remained lowest in those treated with high dose IFNβ-1a for eight years. Interestingly, brain parenchymal volume, as a measure of atrophy, declined in all groups. This measurement was limited by the lack of a placebo cohort for the full duration of the study. The authors commented that brain parenchymal volume was a promising new measure of chronicity of disease, but that it could be confounded by physiologic fluctuations. Importantly, there were no new safety concerns identified and long-term safety and tolerability were maintained. The inherent weaknesses in LTFU studies should be considered when interpreting these results.

The Once Weekly Interferon for MS Study (OWIMS) ran nearly concurrently with the PRISMS study.51 This was a randomized, double-blind study of IFNβ-1a 22 μg, 44 μg, or placebo administered by SC injection weekly for one year. A total of 293 RRMS patients were enrolled. The primary outcome measure was the number of combined unique (CU) active lesions (PD/T2 or T1-enhancing) at 24 weeks. No clinical variables, other than steroid use in the 44 μg group, reached statistical significance. The MRI features of CU lesions and burden of disease significantly favored the treatment arms. The authors concluded that when taken together with other studies, a dose-effect relationship exists for both clinical and MRI variables.

In 2001, a trial of SC IFNβ-1a in SPMS was reported.52 This study enrolled 618 patients in Europe, Canada, and Australia with EDSS scores of 3.0 to 6.5, a history of clinical progression for at least six months, and an increase in EDSS of one or more points in the two previous years (0.5 if the EDSS was 6.0–6.5). Subjects were randomized to receive 22 μg, 44 μg, or placebo by SC injection TIW for three years. The study’s primary endpoint was time to confirmed disability progression, defined as an increase from baseline by at least 1 EDSS point (0.5 if baseline greater than 5.5) confirmed three months later. The primary outcome measure was not statistically affected by treatment, as was also seen in the North American IFNβ-1b trial. There was a significant effect of treatment on relapse rates, and MRI measures including lesion load, and new or enlarging T2 lesions.53 A subgroup analysis suggested that maximal benefit with IFNβ-1a treatment in SPMS was seen in patients who continued to experience relapses, tending to confirm the outcomes of the European and North American IFNβ-1b studies.

A trial of IFNβ-1a in patients with CIS was reported by the Early Treatment of Multiple Sclerosis (ETOMS) Study Group.54 Eligible patients experienced their first event suggestive of monosymptomatic or polysymptomatic demyelinating disease within 3 months, had one or more abnormalities present on neurologic examination, and an MRI consistent with demyelinating disease. Steroid treatment of the initial attack was allowed only for moderate or severe exacerbations. Three hundred eight patients were randomized to either placebo or 22 μg IFNβ-1a by SC injection once weekly. The primary outcome measure was conversion to CDMS as defined by a second clinical relapse, confirmed when the evaluating physician could detect an objective change on neurologic examination. At the end of two years, 45% of placebo treated patients converted to CDMS, compared with 34% of those receiving active treatment (p = 0.047). The treatment arm showed a significant effect on the number of T2 lesions and total lesion volume. Subsequently, in a reanalysis of the data, Eilippi and colleagues55 reported a significant treatment effect on brain atrophy at two years compared to baseline (p = 0.0031). This study may be interpreted as showing that when MS is treated in its earliest stages, even a dose of IFNβ-1a that is considered subtherapeutic (22 μg once weekly) may be effective in preventing or delaying relapses.

Head-to-head studies

There have been three head-to-head trials of IFNβ therapy published to date. The longest of these was the INCOMIN (Independent Comparison of Interferons) trial, comparing every other day SC IFNβ-1b to once weekly IM IFNβ-1a.56 Patients included in this study had clinically definite RRMS, EDSS scores between 1.0 and 3.5, and two documented relapses within the previous two years. One-hundred eighty-eight patients enrolled at 15 Italian centers were randomized to either IFNβ-1a 30 μg IM weekly or IFNβ-1b 8 MIU SC every other day. The MRI evaluators were blinded, but clinical evaluators were not. The primary outcome measure was the proportion of relapse-free patients during the two years of study. The IFNβ-1b cohort showed a significant difference in freedom from relapses compared with IFNβ-1a (56% vs 36% p = 0.036), and a significant reduction in new T2 lesions on blinded MRI (p < 0.0003).

In the EVIDENCE (Evidence of Interferon Dose-response: European North American Comparative Efficacy) trial,57 investigators compared the efficacy and safety of once weekly IFNβ-1a 30 μg IM with high-dose IFNβ-1a 44 μg SC TIW. The 677 patients enrolled in this study had definite RRMS, EDSS scores of 0 to 5.5, were IFN naïve, and had experienced two or more exacerbations within the previous two years. The patients were aware of their treatment assignment, but evaluators of the clinical and MRI outcomes were blinded. The primary clinical endpoint was the proportion of relapse-free patients, and the primary MRI endpoint was the number of active lesions per patient per scan at six months, later extended to 12 and 16 months.58 Patients were evaluated every four weeks during the initial 24-week period, and again at 36, 48, and 64 weeks. The 44 μg treatment group showed significant effects on freedom from relapses compared to the 30 μg group at all time points. There was a 32% relative reduction in the proportion of relapse-free patients treated with 44 μg TIW at 24 weeks, and a 21% relative reduction at 48 weeks (p = 0.003). There was a 27% relative reduction in relapse rates at 24 weeks in the 44 μg TIW treatment cohort (p = 0.022); these relapse rates were 0.29 for the 44 μg TIW group and 0.40 for the 30 μg weekly group, however the reduction in relapses with 44 μg TIW did not maintain significance at 48 weeks. At 24 weeks, the 44 μg TIW group showed a significant effect on MRI lesions (p < 0.0001). This effect was also maintained at 48 weeks (p < 0.001). Injection site reactions, asymptomatic liver enzyme elevations, and altered leukocyte counts were more frequent in the 44 μg TIW arm compared to the once weekly 30 μg arm.

In 2005, an extension of the EVIDENCE trial was reported59 in which patients in the 30 μg IM weekly IFNβ-1a group were permitted to cross over to 44 μg SC TIW. The primary outcome measure was the annualized relapse rate compared to the rate prior to transition. Several secondary MRI endpoints were also included. The MRI evaluators remained blinded. Patients previously on 44 μg TIW were allowed to remain on that dose. The post-transitional relapse rate decreased from 0.64 to 0.32 for patients switching to 44 μg TIW (p < 0.001) and from 0.46 to 0.34 for patients remaining on 44 μg TIW (p = 0.02). Patients converting to the higher dose regimen had fewer active T2 MRI lesions in comparison to pre-transition values (p = 0.02). There were no significant MRI changes in patients maintained on high dose therapy. Patients switching to high dose therapy were noted to have an increase in mild to moderately severe adverse events.

A multicenter, randomized open label Danish trial60 recently compared IFNβ-1a (Rebif®) 22 μg once weekly to the standard dose of IFNβ-1b (Betaferon®) 250 μg every other day. Patients enrolled in this study had definite RRMS, EDSS scores of 0 to 5.5, and two relapses within the last two years. Blinding was not attempted in this trial except for MRI evaluations. Three hundred one patients were randomized to either dose regimen. A third cohort was included in this study, containing patients with newly diagnosed RRMS who refused randomization but were treated with 250 μg IFNβ-1b every other day. Annual relapse rates, time to first relapse, and time to sustained progression were virtually identical in the two arms of the randomized study. In the nonrandomized treatment group, the annual relapse rate was not significantly different, but there was a trend toward shorter time to progression. The conclusion of this study was that IFNβ-1b 250 μg every other day was not clinically superior to IFNβ-1a 22 μg once weekly, a surprising and uninterpretable finding in light of the INCOMIN and EVIDENCE trial results.

Safety and tolerability

The most common side effects of IFNβ therapy are flu-like symptoms, increased spasticity, hematologic and hepatic laboratory abnormalities, inflamed injection sites, cutaneous necrosis, and depression.61 Experience has shown that patient education about side effects prior to treatment, and proper management of adverse events, improves adherence to treatment.62,63 Injection site reactions are more common when beta interferon is administered SC compared to the IM route. These reactions are characterized by local pain, erythema, and induration. In the EVIDENCE trial,57 83% of patients on SC IFNβ-1a versus 28% on IM IFNβ-1a experienced injection site reactions. Koch-Henriksen and colleagues60 reported the equal occurrence of injection site reactions in patients treated SC with either IFNβ-1a or IFNβ-1b. However, an observational prospective study of 306 Betaferon® and 148 Rebif® patients found significantly more pain-free days and fewer injection site reactions in the IFNβ-1b group.64

The cause of injection site reactions probably varies from one patient to another. Management strategies for treatment of these reactions include careful attention to aseptic technique, avoidance of intradermal injections, making sure the solution is completely dissolved and at room temperature, avoiding excessive sun exposure, local application of heat or cold, and use of nonsteroidal anti-inflammatory drugs (NSAIDS) to alleviate pain and prevent fever. Patients should be encouraged to keep a log of injection sites, making sure to alternate regularly to avoid skin breakdown. Injection site reactions usually diminish over a 3–6 month time period. Skin necrosis is a rare but serious complication of SC therapy, and to date no cases have been reported with the IM delivery route. Improper injection technique, including failure to alternate sites, has been shown to increase the risk of skin necrosis. If necrosis occurs, subcutaneous interferon should be discontinued and alternative therapy, including IM therapy, should be considered. Patients should be cautioned not to use topical steroids on these sites as they can delay recovery.61

Flu-like symptoms of chills, fatigue, headache, and myalgias can occur a few hours after administering IFNβ, and may persist for 24 hours or more. Kümpfel and colleagues65 found IFN-β injections at night led to increased IL-6 levels and temperature, correlating with decreased cortisol levels and more intense systemic side effects when compared to morning injections, with acute effects moderating after six months. This variation in time of injection administration may assist some patients with tolerability. Clinical experience has shown flu-like symptoms to become less frequent in most patients within three months of beginning therapy. Gradual dose escalation, as well as taking NSAIDS, reduces the occurrence of flu-like symptoms.66 Occasionally patients treated with IFNβ may notice an increase in spasticity during initiation of treatment. This typically occurs in patients who already have increased muscle tone and known temperature sensitivity, usually within hours of treatment, and lasting for days. Management with NSAIDS or antispasticity medications is often effective. Cases of hypothyroidism and hyperthyroidism are occasionally reported in patients on interferon therapy, and may require stopping therapy or switching to a non-IFN agent such as glatiramer acetate.

There is conflicting evidence to date regarding the relationship of IFNβ treatment to depression. Patients with known depression prior to treatment should be monitored carefully, and initiation of an antidepressant at the time of treatment should be considered. One should caution patients and family members to watch for depressive symptoms, and alert the prescribing provider should they occur. If patients on IFNβ therapy develop signs or symptoms of a mood disorder, the IFNβ should be discontinued, and if symptoms persist, treatment with psychotherapy, antidepressants, or both may be required. Occasionally, treatment may be re-instituted without recurrence of the depression.

Patients on IFNβ therapy commonly develop transient elevations of liver enzymes (AST and ALT), neutropenia, and less commonly, anemia. Tremlett and colleagues67 performed a retrospective chart review of 844 MS patients treated with IFNβ-1a or IFNβ-1b therapy, and found that 37% of patients developed new elevations of ALT. The effect of IM IFN was less than that of the SC IFNs on ALT levels. To date, two patients have been described with liver failure requiring transplantation,68 one of whom was concurrently taking nefazodone, another potentially hepatotoxic medication.69 No potential confounders could be identified in the second patient.

Francis and colleagues68 reviewed a pooled database of patients treated with IFNβ-1a, and found ALT elevations in 59% of patients on IFNβ-1a 44 μg TIW and 40% of patients taking IFNβ-1a 30 μg per week. More than 50% of the elevations occurred within three months, 75% occurred within six months, and most elevations remitted spontaneously. Men were found to be more susceptible than women to liver enzyme elevations. Dosage reductions were necessary in 5% of treated patients, and universally led to normalization of values. Propionic acid derivatives taken concomitantly were the only medications shown to statistically be associated with increased risk of liver dysfunction. The authors recommended liver function analysis prior to treatment and at 1, 3, and 6 months, with dose reductions for patients with ALT values of 5–20 times normal and discontinuation of treatment for those whose ALT levels are over 20 times normal. Despite these caveats, high dose IFNβ therapy is reasonably well tolerated, with an acceptable safety profile, as its continued long-term use in the MS population attests.

Neutralizing antibodies

The effect of neutralizing antibodies (NAbs) on IFNβ therapy remains a topic of controversy. In the IFNβ-1a (Avonex®) trial,37 22% of patients developed NAbs; however an effect on endpoint measures could not be ascertained because of the short duration of the study. After reformulation, this product led to development of NAbs in only 5%–7% of patients.56,57 In the PRISMS-4 study,49 low dose interferon 22 μg TIW was associated with the development of NAbs in 23.7% of patients while in the 44 μg TIW group 14.3% developed NAbs. Though no clinical effect was noted at two years, a reduction in clinical outcome measures was found at four years. In the multicenter trial of IFNβ-1b in RRMS, 38% of patients developed NAbs by the third year with a noticeable attenuation of treatment effect. Perini and colleagues70 found 40% of β-1b patients, 6.7% of IM IFNβ-1a, and 27% of SC IFNβ-1a patients developed antibodies. This study found the presence of high titers of both binding and neutralizing antibodies to be indicative of loss of treatment effect. There are also data suggesting that Nab titers can revert to negative over time.71 This was shown in the IFNβ-1b follow-up study,72 in which 80% of NAb positive patients converted to antibody-negative status after 8 years despite continued therapy. NAbs to one IFNβ product cross-react with the others,73 so switching therapy to another IFNβ is not likely to be an effective strategy. In a recent phase III trial of a new and less immunogenic formulation of SC IFNβ-1a (Rebif®), an interim analysis74 showed reduced antibody formation and improved tolerability. Publication of the results of this trial is awaited with interest.

The American Academy of Neurology recently reported the recommendations of a subcommittee focusing on the effect of NAbs on clinical and radiologic outcomes.75 The committee concurred that there is probably a reduction in efficacy of treatment because of NAbs. They also concurred that there is likely to be greater antibody production in response to IFNβ-1b than to IFNβ-1a, and that IM IFNβ-1a is clearly less immunogenic than other interferon therapies. Despite the consistent finding of NAb levels greater than 1:200 being associated with a reduction of efficacy, the committee was unable to make definite recommendations for changing therapy. This report highlights the fact that many questions remain unanswered in regard to the NAb issue.

The differences in assays used to measure NAbs, criteria for NAb positivity, and varying clinical assessment measures, make comparison between the studies difficult, if not impossible. Until clear data are available regarding the importance of neutralizing antibodies, decisions to change treatment should be based on the clinical picture. If a patient continues to have relapses despite IFNβ treatment, the physician should consider testing for NAbs and switching to another therapy. If NAbs are detected at a titer of 1:20 or greater on repeated testing, a non-interferon therapy such as glatiramer acetate should be considered. However, in a patient doing well clinically, there currently appears to be no benefit in testing for NAbs. The value of periodic MRI evaluation in the absence of clinical worsening has not been established.

Quality of life

Studies of IFNβ in the treatment of MS have shown benefit in relapse frequency and severity, as well as a reduction in hospitalizations. MS typically affects patients in the most productive years of their lives, and IFNβ therapy allows for fewer interruptions in activities of daily living. These studies have also shown excellent tolerability and relatively benign side effect profiles. The key to successful adherence to treatment is proper education about side effects and their management.62,63 Patients should be aware that beta interferon therapy is designated as pregnancy category C, meaning that spontaneous abortions have been observed in IFNβ-treated animals. A longitudinal, controlled cohort study found a decrease in mean birth weight and an increased risk of fetal loss in interferon exposed patients, even after correcting for potential cofounders.76 Patients are encouraged not to take any of the IFNβ products while breast feeding because the risks of transmission through breast milk are unknown.

A recent study showed that depression is the principal factor affecting quality of life in patients with MS.77 The effect of interferon therapy on depression remains controversial. Symptoms such as suicidal ideation, decreased interest, feelings of guilt, loss of energy and concentration, and change in appetite may be signs of undiagnosed depression. Patients with these symptoms may require treatment with antidepressants, psychotherapy, or both and should be treated accordingly.

Conclusions and recommendations

The past decade has brought broader treatment options to physicians caring for patients with MS. Numerous randomized controlled trials of IFNβ have been published (Tables 1 and 2), confirming their efficacy on relapse rates, disease severity, and MRI outcomes. Unfortunately, long-term follow up assessments are few, and fraught with limitations. Those long-term studies that are available demonstrate that atrophy and disease progression continue despite early improvement in clinical and MRI outcomes. This suggests that other processes, in addition to inflammation, underlie the pathogenesis of MS, and indicate a need for additional treatment options. Until then, the current studies support treatment with IFNβ at the time of diagnosis of MS, as shown by the inability of placebo cohorts treated later to catch up to patients originally receiving interferon.

The relative importance of dose, frequency, and route of administration remains unclear. This is underlined by the recent study of double dose IFNβ-1b and lack of statistical superiority found in patients treated with 500 μg every other day compared to 250 μg every other day, and to glatiramer acetate, on the risk of relapses.78 The relapse rate was very low in all study arms. Currently it appears that both dose and frequency of administration are important, and the effects of each cannot clearly be distinguished. Decisions about the choice of an IFNβ in each individual case should be made in the context of an informed discussion between physician and patient. Treatment should be customized to the patient with regard to frequency and route of administration, as well as side effects, in order to maximize compliance.

The decision to treat after a first demyelinating event (CIS), and before the diagnosis of MS is established, is also not obvious. The CHAMPS (35% compared to 50%), ETOMS (34% compared to 45%), and BENEFIT (15% compared to 31%) studies all showed modest benefit at 2 years in preventing patients with CIS from having a second relapse. Those patients who have polysymptomatic disease and a larger T2 lesion load on MRI at the time of their first demyelinating event are more likely to convert to definite MS. Clinical suspicion and careful follow-up seems to be the best option in these cases, given that the alternative is prescribing a potentially unpleasant injectable medication that the patient may not need. There is no evidence to indicate that waiting a few months for the patient to meet the McDonald criteria for definite MS increases future risk compared to treating at the first sign of CIS. Furthermore, treatment at the CIS stage removes patients from the pool of potential RRMS subjects eligible for clinical trials. For these reasons, it is our practice to follow these patients with frequent MRIs and clinical examinations every 3–6 months.

The issue of NAbs also needs to be clarified. Any decision to change treatment remains a clinical one based on examination, history, and imaging. If a patient is doing well on treatment, knowing the NAb status is of little value. If a patient is doing poorly on treatment, it is time to change, regardless of NAbs.

Our understanding of MS with regard to pathophysiology and treatment is just beginning, and the prospects for further studies are exciting. The three available IFNβ preparations represent a major breakthrough in the history of MS therapy. In addition, by a process analagous to reverse engineering, they have given rise to a plethora of laboratory studies that have increased our understanding of MS pathogenesis and the mechanism of IFN action. However, numerous other compounds that may be more effective are currently in phase II and phase III clinical trials. Moreover, several of these are administered orally, an obvious advantage in terms of patient acceptance and compliance. Combination therapy also holds promise for MS, although well-designed and adequately controlled studies are difficult to conduct. Fortunately, placebo-controlled clinical trials are still considered ethical, at least under certain circumstances such as time-limited phase II studies and trials in SPMS and PPMS.79 Clinical trials of MS therapy continue to become increasingly complex, and a combination of placebo-controlled studies, trials comparing new agents to the best available current therapy, and combination or add-on studies will be necessary to provide the information needed to manage the broad spectrum of patients with this devastating disease

Footnotes

Disclosure

The authors report no conflicts of interest in this work.

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