Ocrelizumab or Alemtuzumab Compared With Autologous Hematopoietic Stem Cell Transplantation in Multiple Sclerosis - a Phase-2 Randomised Controlled Trial (COAST)

Inclusion Criteria (Based on CARE-MS-II3, guidelines and Rio-criteria for treatment failure):

• Written informed consent and agreement to comply to study protocol
• Age: 18-55 years
• EDSS: 0.0 - 6.0
• RRMS according to McDonald 2010
• < 10 years of disease course after symptom onset
• Active disease with one of the following treatment failures occur-ring not earlier than 6 months after initiation of an approved DMT
• 2 or more relapses within the last 12 months

or

• 1 relapse within the last 12 months and a Gd-enhancing lesion on MRI > 3 mm > 3 months before or after relapse onset or 2 new T2-lesions

or

• On-going signs of MRI activity in the last 6 months (either Gd-en-hancing of ≥ 3 mm lesion at any exam in the last year; or more than 5 new T2 lesions (≥ 3 mm)

or

• Patients stable under natalizumab but who have to stop treatment due to an increasing PML risk are defined as active, if a MRI within 6 months after termination of natalizumab shows new T2 or Gd-enhancing lesions and at least one other treatment fail-ure prior to natalizumab is documented.

Exclusion Criteria:

• Secondary or primary progressive MS

• Pregnancy, or other medical condition incompatible with aHSCT

• Any treatment or medical condition that, according to the haematologist / transplant specialist precludes the use of aHSCT

• John Cunningham virus (JCV) antibody index of > 1.5 in previ-ously natalizumab-treated patients, if a negative CSF JCV-PCR prior to screening is not available

• Relapse during 30 days before initiation of treatment. If a relapse occurs during this period and eligibility criteria are otherwise ful-filled, start of treatment will be delayed until at least 30 days after receiving steroids.

• Concurrent clinically significant (as determined by the investiga-tors and haematologist / transplant specialist) cardiac, immuno-logical, pulmonary, neurological, renal or other major disease such as:

  • Prominent cardial disease (Left ventricular ejection frac-tion (LVEF) < 40%, myocardial infarction or ischemia, un-controlled arrhythmias, pericardial effusion > 1 cm)
  • Cerebrovascular disease
  • Renal disease (creatinine clearance < 30 ml/min/m2)
  • Respiratory disease (DLCO < 40% predicted)
  • Active bleeding or clotting disease
  • History of human immunodeficiency virus (HIV) or posi-tive HIV antibody testing
  • Any uncontrolled acute or chronic infection, including HIV, hepatitis B surface antigen positivity and hepatitis C PCR positivity
  • Cancer except in situ cervix or cutaneous

• Unwillingness or inability to comply with the requirements of this protocol including the presence of any condition (physical, men-tal, or social) that is likely to affect the patient returning for follow-up visits on schedule. Unwillingness to use contraception.

• Previous participation in this study, previous treatment with aHSCT or already both comparators

• Ongoing immunotherapy. Treatment with interferon or glati-rameracetate will need no wash-out. Treatment pause before oc-relizumab/alemtuzumab or aHSCT will be:

  • for dimethylfumarate and fingolimod: 8 weeks
  • for natalizumab: 8 weeks
  • for ocrelizumab: 12 weeks
  • for alemtuzumab: 12 months
  • for teriflunomide: 4 weeks after elimination with cholesty-ramine
  • for cladribine: 24 weeks

• Patients with cognitive impairments who are unable to provide written, informed consent prior to any testing under this protocol, including screening and baseline investigations that are not con-sidered part of routine patient care.