To evaluate the effect of intrathecally (IT) delivered rituximab as a therapeutic intervention for progressive multiple sclerosis (PMS) during a 3-year follow-up period.
Methods
Participants of a 1-year open-label phase 1b study of IT delivered rituximab to patients with PMS were offered extended treatment with follow-up for an additional 2 years. During the extension phase, treatment with 25 mg rituximab was administered every 6 months via a subcutaneous Ommaya reservoir connected to the right frontal horn with a ventricular catheter.
Results
Mild to moderate vertigo and nausea occurred in 4 out of 14 participants as temporary adverse events associated with IT rituximab infusion. During the entire 3-year period, two cases of low-virulent bacterial meningitis occurred, which were successfully treated. Walking speed deteriorated significantly during the study.
Conclusions
IT administration of rituximab via a ventricular catheter was well tolerated. Considering the meningitis cases, the risk of infection was not negligible. The continued loss of walking speed indicates that IT rituximab was not able to stop disease progression.
Classification of evidence
This study provides class IV evidence that intraventricularly administered rituximab in progressive MS is associated with a risk for bacterial meningitis and does not halt disease progression.
EU Clinical Trial Register
EudraCT; 2008-002626-11 and 2012-000721-53
Introduction
B-cells located within the CNS constitute a potential target for treatment in progressive MS (PMS) [7]. Administration of B cell depleting antibodies are highly efficacious in the relapsing phase but results in progressive MS (PMS) have been less convincing [5, 6, 8]. Low penetrance to the CNS compartment may explain the limited treatment effect in PMS [6, 8]. Therapeutic antibodies used in the treatment of RRMS does not readily cross the intact blood–brain barrier (BBB), achieving cerebrospinal fluid (CSF) concentrations of only 0.1–0.5% of the corresponding levels in plasma [9]. Intrathecal (IT) administration of rituximab might, therefore, be beneficial for PMS. We conducted a 1-year phase 1b Intrathecal Treatment Trial in Progressive Multiple Sclerosis (ITT-PMS) study on a group of PMS patients either failing, or not benefitting from, existing immunomodulatory treatments confirming the feasibility and tolerability of that treatment approach [1]. The short-term follow-up of that trial precluded the detection of any disease-modifying effect on disease progression. After an additional 2-year extension study, we have here evaluated the potential clinical benefit of rituximab over the total 3-year period.
Materials and methods
Ethical approval of standard protocols, registrations, and patient consent
The original ITT-PMS study and the extension study were both approved by the Regional Ethical Review Board in Umeå and registered with the EU Clinical Trial Register (EudraCT; 2008-002626-11 and 2012-000721-53, respectively). The trials were performed in accordance with standards of GCP and the principles of the Declaration of Helsinki. Oral and written information about the trials were provided to all participants before written consent was obtained. The studies were monitored by an independent medical monitor.
Anzeige
Study cohort
The recruitment to ITT-PMS and ITT-PMS extension trials is depicted in Fig. 1. Eligible patients had a purely progressive MS, where no available treatment options were considered to be beneficial for the patient. Participants were recruited at the neurology departments of Norrland’s University Hospital, Umeå and Uppsala Hospital, Sweden between 27th June 2009 and 11th May 2015. Inclusion- and exclusion criteria are described in detail elsewhere [1]. Baseline characteristics for both studies are shown in Table 1.
Fig. 1
Flow chart of inclusion and exclusion of patients for the combined trials ITT-PMS and ITT-PMS extension
Table 1
Demographics and disease characteristics
ITT-PMS (n = 23)
ITT-PMS extension (n = 15)
Age at inclusion, years
Mean (SD)
46 (9)
47 (9)
Min–Max
29–66
29–66
Sex, n (%)
Male
7 (30)
4 (27)
Female
16 (70)
11 (73)
Age at disease onset, years
Mean (SD)
32 (11)
32 (12)
Min–Max
12–51
12–51
Disease duration at inclusion, years
Mean (SD)
14 (8)
15 (9)
Min–Max
3–39
3–39
Age at PMS onset, years
Mean (SD)
38 (9)
40 (9)
Min–Max
25–56
25–56
Duration with PMS at inclusion, years
Mean (SD)
8 (4)
8 (4)
Min–Max
3–19
3–19
Type of PMS, n (%)
SPMS
15 (65)
11 (73)
PPMS
8 (35)
4 (27)
EDSS at inclusion
Median (IQR)
6.5 (1.0)
6.5 (1.0)
Min–Max
4.0–7.5
4.0–7.0
Demographic features and disease characteristics at baseline in the ITT-PMS trial for the 23 participants in the ITT-PMS trial and the 15 participants that completed the 2-year extension study
×
Study design and outcome measures
After completion of the ITT-PMS study, participants were offered to continue treatment in the open-label unblinded extension study. The primary endpoints were to evaluate stabilization of neurological deterioration, degree of MS symptoms, quality of life, and fatigue.
Study procedures
Intrathecal (IT) access
In the original ITT-PMS study, participants received an Ommaya reservoir as an access point for intraventricular injections [1].
Treatment within the study
Initial treatment in the ITT-PMS trial was three injections of 25 mg rituximab (Mabthera®) 1 week apart [1]. In the extension study, patients were treated with 25 mg rituximab followed by 2 mL NaCl solution IT every sixth month for a total of five injections (Fig. 2). The dose was originally chosen from dose-ranging studies performed for treating CNS lymphoma, in which 25 mg as single injections intraventricularly was the highest dose without any tolerability issues [9].
Fig. 2
Overview of the study design of the ITT-PMS and the ITT-PMS extension trials. Treatment within the trials are marked with ‘RTX’. Month 12 was the last visit in the ITT-PMS trial and at the same time the first visit in the ITT-PMS extension trial with treatment according to the protocols of the extension trial. The reflex hammers indicate the timing of clinical evaluation. The scalpel indicates the insertion of the Ommaya reservoir. ITT-PMS Intrathecal Treatment Trial in Progressive Multiple Sclerosis, ITT-PMS ext Intrathecal Treatment Trial in Progressive Multiple Sclerosis extension, RTX rituximab
×
Clinical assessments
Clinical assessments were performed to evaluate cognitive function (symbol digit modality test; SDMT), fatigue (fatigue scale for motor and cognitive function; FSMC), walking speed (6-min walk test and 25-foot walk test), and arm function (9-hole peg test). Adverse events (AEs) were recorded at each follow-up and as required.
Statistical analysis
Statistical analyses were performed using IBM SPSS Statistics for Windows, version 23.0 (IBM Corp., Armonk, NY). Results are summarized with median, min. and max. values, together with interquartile range (IQR), and p values were calculated using Wilcoxon signed-rank test. Only patients completing the full 3-year period of both trials were included in the final data analysis. For patients that lost the ability to perform a walking test during the study due to disease progression, the value for walking speed obtained at the last measured point was used in the calculations.
Data availability
The study protocol is available on request to the Principal Investigator (PI; AS). Raw data can be made available in a de-identified form upon written request to the PI under condition that an additional ethical approval is obtained from the Ethical Review Board.
Anzeige
Results
Adverse events
Table 2 summarizes all adverse events from both ITT-PMS trials. Mild to moderate vertigo and mild nausea was common in direct association with the injection procedure, commonly lasting 5–20 min and rarely needed symptomatic medication. Two cases of low-virulent bacterial meningitis caused by Propionibacterium were recorded, one in the ITT-PMS and one in the extension trial. Both were treated successfully with antibiotics. No other SAE were recorded.
Table 2
Adverse events recorded from the beginning of the 1-year ITT-PMS trial to the end of the 2-year extension trial for all participants
The results of clinical assessments for the 15 participants that completed the full 3-year ITT-PMS trial are summarized in Table 3 and Fig. 3. Compared with baseline, walking speed deteriorated by 33% (p = 0.006) and SDMT improved by 1 point (p = 0.016). Other assessments did not change significantly over the trial period. As a sensitivity analysis, we also performed the same calculations on all patients entering the original ITT-PMS trial using the last measured value on each parameter even if the patient had discontinued during the course of the studies. We then obtained virtually identical median change of each parameter as reported in this study based on only completers of the two trials, not altering any significance level (data not shown).
Table 3
Clinical assessments
N
Median
IQR
Max
Min
Z value
p value
Walking speed (m/s)
Baseline ITT-PMS study
12
1.00
0.37
1.59
0.44
Endpoint in extension trial
13
0.65
0.67
1.56
0.10
Change
11
− 0.33
0.38
0.06
− 0.91
− 2.756
0.006
9HPT—Dominant hand
Baseline ITT-PMS study
15
25.00
20.40
56.10
17.00
Endpoint in extension trial
14
26.38
34.55
114.65
16.60
Change
14
0.25
6.95
71.44
− 6.00
0.471
0.638
9HPT—non-dominant hand
Baseline ITT-PMS study
15
27.40
12.45
58.50
21.35
Endpoint in extension trial
15
30.30
18.55
56.90
19.45
Change
15
2.30
8.04
30.50
17.65
0.568
0.570
FSMC
Cognitive Score
Baseline ITT-PMS study
15
32
12
42
12
Endpoint in extension trial
15
32
14
48
20
Change
15
1
11
13
− 12
0.220
0.826
Motor Score
Baseline ITT-PMS study
15
41
7
50
19
Endpoint in extension trial
15
36
10
48
29
Change
15
− 4
8
12
− 15
− 1.592
0.111
Total Score
Baseline ITT-PMS study
15
74
15
87
31
Endpoint in extension trial
15
67
23
95
54
Change
15
− 2
18
25
− 27
− 1.194
0.232
SDMT
Baseline ITT-PMS study
15
48
15
65
22
Endpoint in extension trial
15
49
19
68
23
Change
15
1
6
13
− 6
2.404
0.016
Results from clinical assessments of the 15 participants that completed the full 3-year ITT-PMS + ITT-PMS extension studies
Fig. 3
Development of walking speed in the patients, where this could be assessed at the onset of the ITT-PMS trial
×
Discussion
The original ITT-PMS study was designed to evaluate safety and feasibility of IT rituximab treatment with the idea to target compartmentalized inflammation in patients with purely progressive MS [1]. As exploratory endpoints, several clinical variables were assessed to detect trends of improvement or continued deterioration. Considering the insidious course of PMS, the addition of an extension trial with continued treatment was thought to increase the possibility to detect a clinically meaningful effect.
One important feature of PMS is the deterioration in walking ability. In the ITT-PMS trial walking speed was essentially unchanged but with the additional data from this 2-year extension trial, a statistically significant worsening could be demonstrated (Fig. 3). The magnitude in the degree of worsening (33%) is considered to be of clinical significance when evaluating walking tests [3]. To place our results in perspective, we compared the rate of deterioration with the data obtained in the phase 3 trial of interferon (IFN) beta-1a in progressive MS [2]. The rate of deterioration of walking speed in the IFN group (no raw data was available for the placebo group) over 2 years was 0.15 m/s corresponding to approximately 0.22 m/s over a 3-year period [3]. This is slightly lower rate than the 0.33 m/s deterioration observed in our study. Although a strict comparison is not possible, these data are in line with the conclusion that our data do not support a meaningful treatment effect of the IT rituximab treatment on walking speed.
Hand function has recently been emphasized as a better outcome measure for clinical trials in PMS, due to higher sensitivity in detection of positive treatment effects [4]. In the present study, the results of the 9-HPT were essentially unchanged, which could be interpreted as a successful outcome in a trial of PMS. However, the lack of a control group prohibits any strong conclusions about the effects on hand function. Fatigue, and to some extent cognitive functions, may on the other hand be more directly affected by meningeal inflammation. Unfortunately, there was no indication of a clinically relevant improvement in these parameters. A statistically significant improvement was seen in the SDMT, but the magnitude was not clinically meaningful, and a learning effect is expected.
The recently performed trials of ocrelizumab in primary progressive MS (the ORATORIO trial) imply that anti-CD20 therapy indeed may have a beneficial effect also in the progressive phase of MS [8]. In that respect, one has to consider that the study population at baseline in the ORATORIO trial was younger (mean age approximately 45 years), had a considerably lower EDSS (mean 4.7) and approximately 25% of the patients displayed Gadolinium-enhancing lesions at baseline. All these factors favor a possible treatment effect based on inflammatory activity, which all our patients lacked by definition. The small treatment effect seen on EDSS progression in the ORTORIO trial is, therefore, still not in complete disagreement with our data.
Intrathecally delivered rituximab treatment was generally well tolerated and no specific safety concern was observed related to rituximab per se. Two cases of low-virulent bacterial meningitis were recorded, likely the result of skin puncture and contamination from an area rich in sebaceous glands. Other side effects occurred immediately following the injection and were most likely due to an effect of altered dynamic of CSF pressure and flow in the ventricular system. Intraventricular administration was chosen for this study to secure adequate distribution in the full CSF compartment, but cannot be recommended for a possible clinical use because of its risk for infections. In case of any signs of positive effect from our study, we would have pursued further studies using the more conventional lumbar route for the delivery of the monoclonal antibodies.
The major shortcoming of this trial is the lack of control group. The invasive nature of the treatment precluded a larger trial directly and without clear indications of beneficial effects we chose to follow the initial study population for a longer period rather than initiating a controlled trial. Although we could document worsening in walking speed of most patients our data does not exclude a possible treatment effect in some individuals. With that in mind, the approach of IT administration of treatment in MS may still be an option to consider based on the idea of sequestered inflammation.
Anzeige
Compliance with ethical standards
Conflicts of interest
Joakim Bergman reports no disclosures. Joachim Burman reports no disclosures. Tommy Bergenheim reports no disclosures. Anders Svenningsson reports no disclosures.
Ethical approval
The original ITT-PMS study and the extension study were both approved by the Regional Ethical Review Board in Umeå and registered with the EU Clinical Trial Register (EudraCT; 2008-002626-11 and 2012-000721-53, respectively). The trials were performed in accordance with standards of GCP and the principles of the Declaration of Helsinki.
Open AccessThis article is licensed under a Creative Commons Attribution 4.0 International License, which permits use, sharing, adaptation, distribution and reproduction in any medium or format, as long as you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons licence, and indicate if changes were made. The images or other third party material in this article are included in the article's Creative Commons licence, unless indicated otherwise in a credit line to the material. If material is not included in the article's Creative Commons licence and your intended use is not permitted by statutory regulation or exceeds the permitted use, you will need to obtain permission directly from the copyright holder. To view a copy of this licence, visit http://creativecommons.org/licenses/by/4.0/.
Mit e.Med Neurologie & Psychiatrie erhalten Sie Zugang zu CME-Fortbildungen der Fachgebiete, den Premium-Inhalten der dazugehörigen Fachzeitschriften, inklusive einer gedruckten Zeitschrift Ihrer Wahl.
Mit e.Med Neurologie erhalten Sie Zugang zu CME-Fortbildungen des Fachgebietes, den Premium-Inhalten der neurologischen Fachzeitschriften, inklusive einer gedruckten Neurologie-Zeitschrift Ihrer Wahl.
