Hydroxychloroquine in Primary Progressive Multiple Sclerosis

University of Calgary

Status and phase

Completed

Phase 2

Conditions

Multiple Sclerosis, Primary Progressive

Treatments

Drug: Hydroxychloroquine

Study type

Interventional

Funder types

Other

Identifiers

NCT02913157

HCQ_MS01

Details and patient eligibility

About

The purpose of this clinical trial is to determine if HCQ in a dose of 400mg daily can prevent worsening of walking ability in people PPMS. The number of participants in this study will be 35. A maximum of 42 people with PPMS will be included. The trial is funded through a private donation to the Hotchkiss Brain Institute MS Translational Clinical Trials Research Program and the University of Calgary. There is no sponsorship from the pharmaceutical industry.

Full description

In patients with primary progressive multiple sclerosis (PPMS) there is ongoing slow and continuous loss of nerve cells, which causes damage to the brain and spinal cord. This ultimately becomes noticeable as slowly and continuously worsening disability. While the cause of this ongoing damage is unknown, it appears that at least part of the damage may be caused by cells in the brain called "microglia" (a type of immune cell that reside in the brain and spinal cord). These microglial cells can have beneficial roles, for instance when they clear away debris, but they can also cause damage to brain cells. In PPMS, microglial cells are often found to be in a state of activation, and it is currently believed that this constant activation of microglial cells is likely an important cause of the ongoing damage to brain cells.

Current treatments for MS only work in relapsing-remitting MS, and can prevent relapses, but so far there are no treatments that effectively target PPMS. Therapies for PPMS are needed. The investigators believe that treatments that target and reduce the activation of microglial cells may be a useful treatment strategy.

Hydroxychloroquine (HCQ) is a medication that has been shown to decrease the activity of human microglia in laboratory experiments. Animal experiments have also shown that treatment with HCQ can reduce the disease activity of an animal model of MS. HCQ, therefore, may also reduce the activity of microglia in people with PPMS, and hopefully prevent or slow down the progression of disability in PPMS.

HCQ is currently approved in Canada to treat malaria and the rheumatic diseases Systemic Lupus Erythematodes (SLE) and Rheumatoid Arthritis (RA). HCQ is available as a tablet that is usually taken two times per day. Doses up to 600mg per are used in clinical practice, but the investigators estimate that a dose of only 400mg daily, given as two doses of 200mg, will be sufficient to decrease the activity of microglia in patients with PPMS. HCQ is usually well tolerated.

Following a MinMax Simon-2-stage design, the study will require 35 patients with complete 18 month follow-up. Presuming 20% drop-out, the investigators anticipate recruiting up to 42 patients. The trial will be conducted as follows: patients will continuously enter into the study until 35 patients have completed 18 months of follow-up with at least 75% adherence which will be measured by study drug count.

Enrollment

35 patients

Sex

All

Ages

18 to 65 years old

Volunteers

No Healthy Volunteers

Inclusion criteria

Written informed consent obtained
Men and women aged of 18 and 65 years inclusive
Who are followed at the Calgary MS Clinic
With Primary Progressive Multiple Sclerosis, according to current diagnostic criteria
Screening Expanded Disability Status Scale score between 4.0 and 6.5 inclusive.
Screening timed 25 foot walk (average of two trials) of 5.5 seconds or more.

Exclusion criteria

Patients undergoing treatment with antimalarial drugs, amiodarone, dapsone or digoxin
Patients with known retinopathy
Patients whose screening ophthalmological exam shows retinopathy
Patients whose screening MRI scan shows gadolinium enhancing lesions
Patients with known renal insufficiency
Patients with known significant hepatic impairment
Patients with known porphyria
Patients with known allergy or other intolerability to HCQ, or to gadolinium MRI contrast agent
Patients currently using Fampridine or 4-aminopyridine
Patients planning to start Fampridine or 4-aminopyridine during the study period
Patients planning to start Baclofen or Tizanidine during the duration of the study
Patients who increase the dose of Baclofen or Tizanidine during the study period
Patients who receive treatment with Botulinum toxin in the leg muscles during the study period
Patients using amiodarone, dapsone, digoxin or antimalarial drugs other than HCQ
Patients who are unable or unwilling to undergo gadolinium enhanced MRI scans
Pregnant or breast-feeding women