Background Human neural stem cell implantation may offer improved recovery from stroke. We investigated the feasibility of intracerebral implantation of the allogeneic human neural stem cell line CTX0E03 in the subacute—chronic recovery phase of stroke and potential measures of therapeutic response in a multicentre study.
Methods We undertook a prospective, multicentre, single-arm, open-label study in adults aged >40 years with significant upper limb motor deficits 2–13 months after ischaemic stroke. 20 million cells were implanted by stereotaxic injection to the putamen ipsilateral to the cerebral infarct. The primary outcome was improvement by 2 or more points on the Action Research Arm Test (ARAT) subtest 2 at 3 months after implantation.
Findings Twenty-three patients underwent cell implantation at eight UK hospitals a median of 7 months after stroke. One of 23 participants improved by the prespecified ARAT subtest level at 3 months, and three participants at 6 and 12 months. Improvement in ARAT was seen only in those with residual upper limb movement at baseline. Transient procedural adverse effects were seen, but no cell-related adverse events occurred up to 12 months of follow-up. Two deaths were unrelated to trial procedures.
Interpretation Administration of human neural stem cells by intracerebral implantation is feasible in a multicentre study. Improvements in upper limb function occurred at 3, 6 and 12 months, but not in those with absent upper limb movement at baseline, suggesting a possible target population for future controlled trials.
Funding ReNeuron, Innovate UK (application no 32074-222145).
Trial registration number EudraCT Number: 2012-003482-18
- stem cells
- human neural stem cells
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Stroke is the second most common cause of death and the primary cause of long-term adult disability.1 Cell therapies may modify early brain injury, or may enhance subsequent recovery from stroke through mechanisms that include modulation of inflammation, neural plasticity and neovascularisation via secretion of cytokines, growth and other factors in response to injury.2 Prior clinical studies have explored safety and feasibility of stem cell administration in either early subacute or chronic stages. Intravenous or intra-arterial administration of bone marrow or peripheral blood-derived cells of various kinds have been delivered predominantly in the subacute phase days to weeks after stroke, intended to modulate early secondary brain injury through systemic action. This has been explored in several small feasibility studies3–8 and in two completed randomised trials of insufficient size to reliably determine efficacy.9 10 In chronic stroke, intracerebral delivery of allogeneic cells of various types has been explored.11–13
The human neural stem cell line CTX0E03 modifies the local inflammatory response, and in animal models promotes both host cell neurogenesis after stroke, and host cell angiogenesis after limb ischaemia.14 15 CTX0E03 cells injected 4 weeks after middle cerebral artery occlusion in rats showed a dose-dependent11 and implantation site-16dependent improvement in behavioural outcome along with histological evidence of increased host striatal angiogenesis13 and neurogenesis.14 Preclinical observations suggest that implanted CTX0E03 cells enhance tissue repair in vivo.14 15 17
In a phase I safety trial, 11 patients with stable, moderate to severe functional neurological impairments after ischaemic stroke underwent intracerebral implantation of CTX0E03 cells an average of 30 months after stroke in doses of up to 20 million cells.11 No cell-related safety issues were observed up to 24 months postimplantation, and modest neurological and functional improvements were observed in some patients. Continuing follow-up has identified no cell-related safety issues up to 8 years postimplantation.
We undertook the current study of CTX0E03 cell implantation to explore effects on arm motor function during earlier stages of stroke recovery, gain further safety data and assess practicality of multicentre recruitment.
We undertook an open-label, single-arm, multicentre study to investigate the motor response of the weak arm following stereotaxic intrastriatal injection of 20 million CTX0E03 cells ipsilateral to a supratentorial ischaemic stroke that had occurred between 2 and 13 months earlier. The study was overseen by an independent data and safety monitoring board.
Full inclusion and exclusion criteria are detailed in the online supplementary material. We included male or non-pregnant female patients aged ≥40 years, with imaging-confirmed supratentorial ischaemic stroke, and with stable arm weakness satisfying both of the following criteria at time of consent: National Institutes of Health Stroke Scale (NIHSS) Motor Arm score of 2, 3 or 4; and a score of 0 or 1 for test 2 of the Action Research Arm Test (ARAT: grasp a 2.5 cm3 block and move it from the starting position to the target end position).
Main exclusion criteria were prior disabling stroke; history of intracranial haemorrhage; other significant functional impairment of the affected arm; contraindications to MRI; life expectancy <12 months; malignancy (except for non-melanoma skin cancer) within the previous 5 years; malignant brain tumours or metastases; current tamoxifen treatment; intermittent oral antispasticity medication.
A minimum sample size of 21 treated patients was estimated to ensure that a response rate of ≥20% could not be excluded at the lower one-sided 50% CI for the population mean using the Clopper-Pearson method. The desired minimum response rate was 20% (5/21 subjects) achieving improvement of ≥2 points on ARAT test item 2, for which the probability of spontaneous improvement was predicted to be <5%.
The primary outcome was the response (improvement by ≥2 points 3 months after cell implantation) on ARAT item 2. Secondary efficacy outcomes were numbers of participants showing a predefined minimum response on total ARAT score (≥6 points); NIHSS score (≥10 points); Barthel Index (≥9 points); Fugl-Meyer motor score (≥10 points) on either Motor Function Upper Extremity score or Motor Function Lower Extremity score (added in protocol amendment 8) and modified Rankin Scale (mRS, ≥1 grade).
Data were analysed for the overall dataset. Post hoc subgroup analysis was undertaken for primary and secondary efficacy measures in patients grouped by baseline upper limb function defined by NIHSS arm motor score (4 vs 3 or 2).
The study schedule is detailed in online supplementary table 1. Pretreatment assessments occurred from day 28 (±7 days) following the stroke up to 1–14 days prior to implantation of CTX0E03 DP (day 0). Functional outcomes were evaluated 30, 90, 180 and 360 days after treatment.
Antiplatelet or anticoagulant treatment was withheld for a maximum of 7 days prior to surgery but stroke treatments as determined by the treating clinician otherwise continued throughout. All patients received a minimum 1.5 hours/week physiotherapy directed at the weak arm for 6 weeks. Additional physical and other therapy inputs were delivered according to individual patient needs, determined by the local clinical team.
CTX0E0318 is clonally derived from human fetal cortical neuroepithelial cells and incorporates a retrovirally inserted c-mycERTAM transgene that confers phenotypic and genotypic stability. CTX0E03 drug product (CTX0E03 DP) is a sterile suspension composed of CTX0E03 cells at a passage of ≤37 and formulated in HypoThermosol at a concentration of 5×104 cells/μL. Growth factors and 4-hydroxytamoxifen (4-OHT) used in the manufacturing process are not part of the final formulation. Myc-dependent cell replication is curtailed by removing 4-OHT in cultures, restoring the cells’ capability to differentiate.19 Cryopreserved CTX0E03 DP has a shelf life of 6 months at −135°C and was thawed rapidly at the time of use.
Under general anaesthesia, a neurosurgeon experienced in stereotaxic surgery injected a single intracerebral dose of 20 million CTX cells (400 μL CTX0E03 DP) into the putamen ipsilateral to the ischaemic stroke using coordinates and trajectories based on individual preoperative imaging, as previously described.11 20 CTX cells were delivered in 20 μL deposits at a rate of 5 μL /min, pausing for at least 20 s between each bolus. The deepest implant was delivered first and the cannula withdrawn for subsequent boluses along any single trajectory. Five deposits of 20 μL each were placed along each of four needle tracts. Administration of the entire dose was completed within 3 hours of CTX0E03 DP being brought to room temperature.
The protocol and amendment history are included as online supplementary material. The initial eligibility criteria required an NIHSS arm score of 2 or 3: this was later amended to include NIHSS arm score of 4 (no movement). The primary endpoint was modified to day 90 from day 180 (amendment 8). Eligibility criteria were modified during the course of the study to remove an upper age limit. The Fugl-Meyer Assessment was added to the protocol and was therefore not conducted in all trial participants. A statistical analysis plan was finalised and approved prior to database lock.
Role of the funding source
ReNeuron funded the study and designed the protocol with input from investigators. An independent contract research organisation managed data collection. Analysis was undertaken by an independent statistician contracted to provide the study report. The funder was not aware of outcomes until database lock. The corresponding author had full access to all study data and had final responsibility for submission for publication.
Patients were enrolled and treated between July 2014 and August 2016, and follow-up completed in August 2017. Of 41 patients who underwent screening for eligibility, 23 proceeded to cell injection (figure 1). One patient died before 12-month follow-up (sepsis of unknown cause on day 241), and two others did not attend for 12-month review. Demographics, medical history and baseline stroke characteristics are described in table 1. Baseline ARAT item 2 scores were 0 in 22/23 and 1 in one participant. Successful implantation of CTX0E03 DP was completed in all 23 patients.
Numbers of participants exhibiting predefined response criteria are detailed in table 2. Individual patient data are detailed in online supplementary material.
At 3 months, one patient showed ≥2 points improvement on ARAT item 2. Three patients exhibited a response at 6 and at 12 months: one patient exhibiting a response at 6 months did not achieve the response at 12 months, but had increased scores for other ARAT test items (5 cm3 and 7.5 cm3 blocks).
Total ARAT score improved at the last observation in 7/23 patients, with individual improvements ranging between 1 and 54 points. Five (22%) patients met the response criterion of improvement by ≥6 points. No participant exhibited a change in total NIHSS score of 10 or more points as defined in the statistical analysis plan therefore this is omitted from table 2; however, only four participants had baseline NIHSS >10. Change in Barthel Index of ≥9 points was seen in 8/20 participants at 12 months, but could not be evaluated in six subjects in whom baseline score was 95 or 100 (ceiling). Fugl-Meyer motor scores were undertaken in only 10 participants and improved by ≥10 points in 3. Improvement in mRS by ≥1 grade was seen in 7/20 participants at 12 months (details in table 2).
Responses rates in prespecified assessments were explored with respect to age, time elapsed since stroke and baseline NIHSS arm motor scores. No participant exhibited a response to all four scales at any time point; the number of participants exhibiting a response to 3, 2 or 1 scales was 1, 4 and 8 at 3 months, 2, 3 and 8 at 6 months, and 3, 3 and 8 at 12 months (online supplementary figure 1). Changes in mRS grade were from grade 5 to 3 in one patient; from grade 4 to grade 3 in two patients, both of whom returned to grade 4 at subsequent visits, and one of whom died before the 12 months assessment; grade 3 to grade 2 in five patients and grade 2 to grade 1 in one patient.
At 6 months, 4/22 participants exhibited improvement in either ARAT subitem 2 or total ARAT: the responders were significantly younger (mean 53±6 years vs 64±11 years, p=0.025) but had no differences in time elapsed from stroke to intervention or total baseline NIHSS compared with non-responders. At 12 months, 5/20 participants exhibited ARAT response as above, but no differences were seen in age, baseline NIHSS or time to intervention compared with non-responders.
In nine participants, baseline NIHSS arm motor score was 4 (no movement); 14 participants had scores of 2 or 3, signifying at least some movement. Compared with patients with NIHSS arm scores of 2 or 3, patients with no upper limb movement (NIHSS 4) at baseline were significantly older (70±8 vs 57±9 years, p=0.002), had higher total NIHSS scores (median 7.5 (IQR 7) vs 6 (IQR 4), p=0.019) and lower Barthel scores (median 55 (IQR 38) vs 90 (IQR 31), p=0.003), but interval from stroke onset to treatment did not differ (median 8.5 (IQR 5) months vs 7 (IQR 6)). Responses on ARAT item 2 or total score were seen in none of those with baseline NIHSS arm score of 4 (figure 2 and online supplementary table 2). Improvement by one or more grades of the mRS at month 12 was seen in 6/12 (50%) patients with baseline NIHSS 2 or 3, and in 1/8 (12.5%) of those with baseline NIHSS arm score of 4. Individual patient data for all endpoints are detailed in online supplementary table 3. Responses were seen in both those with cortical and isolated subcortical infarcts (online supplementary table 4).
There were 17 serious adverse events (SAEs) in 11 patients (table 3). These included two deaths (sepsis on day 241, and completed suicide 7 days after the final study visit) considered unrelated to study procedures. Six SAEs in four patients were considered related to the surgical procedure, all of which resolved. These were: cerebral infarction identified on day 1 postprocedure, in a patient with carotid artery stenosis who had required prolonged general anaesthesia; subdural haemorrhage identified on day 2 postprocedure; headache and vomiting (days 2–4 postprocedure); and partial seizures and sepsis in one participant (day 22 postprocedure) considered by local investigators to be possibly related to CTX0E03 cells. The seizure episode was a single, 1-hour long episode of shaking, commencing focally in one upper limb then spreading to the opposite arm and whole body. The patient was conscious throughout. Onset was concurrent with sepsis. Cerebrospinal fluid screen and culture were both negative, and no source of infection could be confirmed.
One patient experienced the serious event of transient, weakly detectable human leucocyte antigen antibody, to antigens which are not expressed by the CTX0E03 cell line, coincident with an intercurrent chest infection 33 days postprocedure. Infection was considered to be the likely stimulus for a non-specific immunological reaction.
Three patients experienced hypotension during the surgery, and two of these also experienced bradycardia, one during the surgery and one during the postoperative inpatient period.
This second study of intracerebral CTX0E03 human neural stem cell injection extends the initial clinical data in several important respects. First, the feasibility of a multicentre clinical study was confirmed. The development of frozen cell product was an important technical development since the first Pilot Investigation of Stem Cells in Stroke (PISCES-1) trial to enable this. Second, additional safety data at the 20 million cell dose confirm few potentially cell-related adverse events up to 1 year of follow-up in both male and female participants, and in a wider age range than previously studied. Third, the feasibility of recruitment at earlier time points following stroke has been established. In the previous PISCES-1 study, median time from stroke to cell implantation was 30 months, compared with 7.5 months in the present study. Finally, exploratory data on functional outcome measures indicate both that the responder rate in a population expected to have a low incidence of functionally useful clinical improvement was sufficient to justify further clinical investigation, and that response rates on measures of upper limb function are likely to be poor among patients with completely absent upper limb movement at baseline assessment a median of 7.5 months after stroke. Preliminary data exploring activities of daily living, general disability and motor function suggest a range of suitable clinical outcome measures for future research.
The original study design sought to determine whether a sufficient proportion of patients experienced response of their weak arm 3 months after implantation of CTX0E03 DP to justify further investigation. The intent was to exclude response rates below 20% with 90% CI at this 3 month time point. At the 3-month evaluation, only one patient met criteria for ARAT test 2 response, and so the primary efficacy endpoint was not met. However, additional patients responded at 6 and 12 months suggesting that improvement continues beyond the 3-month time point. Overall, three participants (15% of those who completed 12-month follow-up) achieved an increase of at least 2 points at 12 months, and one further patient responded at 6 months but not at 12 months, although increased scores for the larger sized blocks assessed in the ARAT. Given the arbitrary selection of 3 months as a time point for endpoint evaluation, and absence of safety issues, further evaluation of CTX0E03 DP in randomised clinical trials is justified.
Most stroke patients experience some functional recovery in the first 6 months poststroke,21–23 varying with severity of the initial deficit.24 Patients who improve early have more favourable functional outcome regardless of clinical syndrome, while patients who fail to show significant recovery by day 10 retain significant disability at day 90.25 Prediction models adjusted for the effects of time after stroke onset suggest that outcome is largely defined within the first weeks poststroke.26 Clinical predictors of dexterity at 6 months are severity of initial arm weakness, and arm motor recovery in the first month after stroke, with no further improvement in prediction accuracy beyond this time.26–29 PISCES-2 participants were selected on the basis of poor predicted recovery, yet showed functionally relevant improvement in motor functions. Observations from the current study as well as the previous PISCES-1 study indicate potential worthwhile functional improvements even with intervention occurring in the late subacute or chronic stages after stroke.
The functional improvements observed in the study population are unlikely to have arisen as a consequence of additional physical therapy at the dose delivered, since very much larger doses appear to be necessary for an effect in chronic stroke.30 31 However, the possibility that lower doses of physical therapy interact with stem cell administration could not be excluded. We did not specifically assess other potential confounders that may lead to falsely low motor performance such as pain or perceptual deficits, therefore, cannot completely exclude the possibility that other factors may have been relevant in the observed improvement.
Expert consensus statements on trial reporting standards,32 measurement33 and biomarkers34 were produced after the initiation of PISCES-2, but the trial conformed with many of these recommendations, including the use of NIHSS to characterise stroke severity, ARAT as a measure of upper limb function and the mRS as a measure of global disability. However, the trial framework proposed did not make recommendations regarding stroke recovery studies where the intervention commenced only in the chronic stage of stroke.
Observations in PISCES-2 inform some aspects of future trial design. The ARAT response observed in PISCES-2 was related to the baseline degree of arm motor impairment, with no ARAT responders among those with absence of movement (NIHSS motor arm score of 4) at baseline. Improvements in mRS were also rarely observed in participants with absent arm movement at study entry. The Barthel index has notable ceiling effects that limit its utility, and in keeping with this, six participants could not achieve a response since already scoring near-maximum or maximum scores at baseline.35 Consensus recommendations on appropriate outcome measures from the Stroke Recovery and Rehabilitation Roundtable group33 include the ARAT for upper limb function. Previous exploratory work on sample size requirements for motor recovery trials36 assuming a defined minimum clinically important difference (MCID) on ARAT of 6 points was based on a small sample size and early characterisation of patients: it is unclear whether the assumed MCID or changes over time apply in later subacute or chronic stages after stroke. Additional work to characterise predictors of motor response at later time points poststroke would be beneficial in stratifying patients for future trials, particularly where an invasive therapy is involved. Motor response prediction algorithms developed for early poststroke use, which include clinical evaluation supplemented where necessary by transcranial magnetic stimulation to determine the integrity of corticospinal tracts supplying upper limb muscles,37 may not be applicable to later time points and require validation.34 For confirmation of clinically important functional outcome changes in stroke, the modified Rankin Scale has been favoured by regulatory bodies, and our observations support this approach.
There are a number of limitations to this study. The open-label design was adopted due to the early stage of clinical investigation but may bias functional assessments. Future evaluation in a randomised, controlled trial is essential. Small numbers of participants inevitably mean that the heterogeneity of stroke cannot be adequately represented, and means that any interpretation of factors related to functional or neurological response must be extremely cautious. Factors, such as age, medical comorbidities, infarct volume and location, anatomical and functional involvement of the corticospinal tract, time elapsed since the stroke, the anatomical location and distribution of cell deposits, concomitant physical therapy and its intensity, may all contribute significantly to motor and general recovery, and a much larger study would be required to evaluate these. While we observed a low incidence of potentially cell-related adverse events, the total number of patients implanted is small (23 in the current study and 2 at this dose level in PISCES-1) and follow-up period limited.
In conclusion, PISCES-2 provides additional data to support multicentre clinical trials of intracerebral stem cell injection in subacute stages of stroke recovery. Functionally relevant improvement in arm movement was observed in patients with residual upper limb motor function at baseline. Further clinical investigation in a randomised, controlled clinical trial is warranted.
AM was partially supported by the National Institute for Health Research (NIHR) Sheffield Biomedical Research Centre (BRC) and NIHR Sheffield Clinical Research Facility.
This web only file has been produced by the BMJ Publishing Group from an electronic file supplied by the author(s) and has not been edited for content.
This web only file has been produced by the BMJ Publishing Group from an electronic file supplied by the author(s) and has not been edited for content.
Presented at International Stroke Conference 2018
Contributors The trial protocol was designed by JH, PS, KP and JS with input from AM, LD and other clinical investigators. Data were acquired by KWM, DB, MW, NS, AD, NW, PT and LD. PB chaired the data monitoring committee. KWM undertook analyses and drafted the manuscript. The manuscript was critically reviewed by DB, MW, NS, AD, NW, PT, AM, LD, PB, KP and JS.
Funding This study was funded by ReNeuron Ltd., Innovate UK (application no 32074-222145).
Competing interests JH, PS, KP and JS are employees of ReNeuron. KWM has participated in advisory boards for ReNeuron and is a member of the trial steering committee for the PISCES-3 trial.
Patient consent for publication Not required.
Ethics approval The study was approved by the UK National Research Ethics Service and Gene Therapy Advisory Committee (references 13/LO1174, GTAC161, 12/LO/1963).
Provenance and peer review Not commissioned; externally peer reviewed.
Data availability statement All data relevant to the study are included in the article or uploaded as online supplementary information. All relevant data are included in online suppplementary information.