MND-SMART is investigating whether selected drugs can slow down the progression of motor neuron disease (MND) and improve survival. The study is 'multi-arm' meaning more than one treatment will be tested at the same time. The trial started with 3 arms; drug 1 (memantine), drug 2 (trazodone) and placebo (dummy drug). A third drug, amantadine, was added in April 2023. A fourth drug, tacrolimus, was added in March 2025 in Edinburgh and across all sites in April 2025. The first two drugs, memantine and trazodone, were removed from the trial in September 2023 due to lack of benefit. The trial currently has 4 recruiting arms; amantadine, liquid placebo (matched to amantadine), tacrolimus, and tablet placebo (matched to tacrolimus). This allows the evaluation of each drug versus placebo. Participants will be randomly allocated between the treatment arms they are eligible for. Medicines being tested are already approved for use in other conditions. MND-SMART has an 'adaptive' design. This means medicines being studied can change according to emerging results. Treatments shown to be ineffective can be dropped and new drugs can be added over the duration of the study. This will allow many treatments, over time, to be efficiently and definitively evaluated. The medicines being tested have been selected following a rigorous process involving a systematic, unbiased, and comprehensive review of past clinical trials data, as well as information from pre-clinical research (studies in laboratories), for MND and other related neurodegenerative disorders. Drugs have been ranked for inclusion in MND-SMART by a group of independent MND experts according to set criteria. These include consideration of how the drugs work, their safety profiles, and the quality of previous studies. New drugs will be selected for investigation in MND-SMART based on continuous review of constantly updated scientific evidence as well as findings from state-of-the-art human stem cell based drug discovery platforms. These can be added by substantial amendment to the protocol.
For further information, please visit: https://mnd-smart.org/
Participants will be considered eligible for randomisation if they fulfil all the core
inclusion criteria and none of the exclusion criteria as defined below. In addition,
investigators must simultaneously check and ensure participants do not meet any of the
drug specific exclusion criteria. If exclusion criteria are met for an arm, participants
can still be considered for other arms and randomised accordingly to eligible arms.
Core inclusion criteria:
- Confirmed diagnosis of MND. This includes the following subtypes: ALS by El Escorial
Criteria (possible, probable, and definite) or Gold Coast Criteria, Primary Lateral
Sclerosis, and Progressive Muscular Atrophy
- Over 18
- Women of childbearing potential according to CTFG guidelines must have a negative
pregnancy test within 7 days prior to, or at, the baseline visit
- Women of childbearing potential and fertile men must be using an appropriate method
of contraception to avoid any unlikely teratogenic effects of the selected drugs
from time of consent, to 4 weeks after treatment inclusive
- Willing and able to comply with the trial protocol and ability to understand and
complete questionnaires
- Written informed consent (in the case of limb dysfunction verbal consent can be
given in the presence of a witness who can sign)
Core Exclusion Criteria:
- Patients diagnosed with Frontotemporal Dementia (FTD-MND) or any other significant
psychiatric disorder that prevents informed consent being given.
- Alcoholism (current self-reported - at the investigator's discretion)
- Active suicide ideation assessed using the Columbia-Suicide Severity Rating Scale
- On concurrent investigational devices and medication (including biological therapy)
- Pregnancy or breast-feeding females
- If ALT, ALP, bilirubin or GGT >3 times the upper limit of normal.
- If creatinine clearance (creatinine clearance or eGFR) <35 ml/min.
- If TSH 25pmol/l)
- If corrected QT interval on 12 lead ECG >500 ms
- Patient's diagnosed with ventricular arrhythmias, significant heart block (at the
investigator's discretion)) or in the immediate recovery period after myocardial
infarction (< 6 weeks).
- Patients who the PI considers will not be able to comply with the study protocol.
Amantadine Exclusion Criteria:
- Patients in the manic phase of bipolar disorder.
- Patients with history of proven peptic ulcer confirmed on endoscopy
- Patients with active epilepsy
- Already taking the IMP in this comparison
- Known hypersensitivity, including hereditary fructose intolerance, or adverse
reaction to the active substances and their excipients (as per SPCs for this
comparison) or any past medical history contraindicating use of the IMP in this
comparison
Tacrolimus Exclusion Criteria:
- Poorly controlled hypertension (Systolic BP>180 mmHg or Diastolic BP>100mmHg)
- Poorly controlled diabetes (HbA1c>6.4% or 48mmol/mol)
- Hypertrophic cardiomyopathy or history of QT prolongation (including family
history), congestive heart failure, bradyarrhythmias, and electrolyte abnormalities
- History of bleeding disorders or significant haematological or immune diseases
including, congenital or acquired immune deficiency, anaemia (Hb<130g/L for males
and Hb<120 g/L in females) and thrombocytopenia (platelet count <150 × 109/L), use
of other biological agents and immunosuppressant medications including oral/IV
steroids
- Active or chronic infection (at PI discretion)
- History of Hepatitis B or C
- History of lymphoma and active malignancy
- Risk of dehydration due to reduced oral intake and lack of parenteral route
- Patient's contraindicated to tacrolimus according to SPC section 4.3
- Use of concomitant medications that interacts with tacrolimus according to the SPC,
including but not limited to strong CYP3A4 inhibitors (i.e. azoles, protease
inhibitors) or CYP3A4 inducers (rifampicin, phenytoin, carbamazepine), barbiturates,
macrolides, digoxin, statins, PPI inhibitors, ergotamine, tricyclic antidepressants,
herbal supplements (St. John's wort, extracts of Schisandra sphenanthera)
- Inability to swallow capsules
- Already taking the IMP in this comparison
- Known hypersensitivity, including lactose and gelatin intolerance, or adverse
reaction to the active substances and their excipients (as per SPCs for this
comparison) or any past medical history contraindicating use of the IMP in this
comparison
- Receipt of a live attenuated vaccine within four weeks prior to receipt of
tacrolimus. These include, but are not limited to live influenza vaccine (Fluenz
Tetra), Shingles (varicella zoster virus) Zostavax, Varicella (Varilrix, Varilvax),
Oral typhoid (Ty21a), and yellow fever vaccines.