Clinical Trial Details
— Status: Completed
Administrative data
| NCT number |
NCT04626063 |
| Other study ID # |
2018/1330 |
| Secondary ID |
|
| Status |
Completed |
| Phase |
N/A
|
| First received |
|
| Last updated |
|
| Start date |
June 10, 2018 |
| Est. completion date |
March 8, 2020 |
Study information
| Verified date |
November 2020 |
| Source |
Istanbul University |
| Contact |
n/a |
| Is FDA regulated |
No |
| Health authority |
|
| Study type |
Interventional
|
Clinical Trial Summary
Acute non-specific low back pain (LBP) is one of the most common complaints at the emergency
department. It is more prevalent in countries with high-income economies, where 60-80% of the
population report back pain at some point in their life. Numerous medication options are
available for acute LBP relief such as non-steroid anti-inflammatory drugs (NSAIDs),
myorelaxant drugs, opioids, and benzodiazepines. Magnesium is a physiological
voltage-dependent blocker of N-methyl-D-aspartate NMDA)-coupled channels that can influence
inflammatory pain and neuropathic pain through several different mechanisms. In this study
the investigators aimed to investigate the effect of magnesium oral supplementation for acute
low back pain.
Description:
This study was conducted at our emergency department between June 2018 and March 2020 after
receiving approval from our institutions' ethics committee (2018/1330). This study was
registered as a randomized controlled trial with the US National Institute of Health
(clinical trials.gov). We conducted a three-arm, prospective randomized open label clinical
trial to compare isolated NSAID group, NSAID with paracetamol group and NSAID with oral
magnesium supplementation group (described below) for treatment of acute LBP. Patients were
included after providing informed consent predicated on their understanding of expected
complications and treatment outcomes. Consolidate Standards of Reporting Trials (CONSORT)
guidelines were followed reporting the results of the study Patients from a single university
hospital were recruited for this study between June 2018 and March 2020. Inclusion criteria
were defined as (1) age>18 years old, (2) duration of symptoms <2 weeks and (3) functionally
impairing LBP which we defined as a score of > 5 on Roland-Morris Disability Questionnaire
(RMDQ).
Exclusion criteria included (1) age>65 years old, (2) history of trauma, (3) presence of
radicular pain physical examination which was defined as pain radiating below the gluteal
folds, (4) history of primary vertebral tumor or metastasis, (4) patients who were pregnant
or lactating, (5) presence of any contraindication or allergy to investigational medications,
(6) history of chronic analgesic use, (7) history of autoimmune diseases or inflammatory
rheumatic disorders, (8) history of cardiopulmonary restrictions, severe kidney or liver
function disorders and (9) history of prior surgery of lumbar spine.
We based our sample size calculation assumptions on a recently published clinical trial [11]
and widely accepted minimum clinically important improvement of 5 points on the RMDQ.(14)
With alpha and beta values were set at 0.05 and 0.20 respectively, sample size calculation
revealed that 50 patients were needed in each study group. To account for protocol
violations, lost-to-follow-up and to ensure sufficient power for the intention to treat
analysis (in previous work, up to 1/3 of enrolled patients did not use the investigational
medication), we enrolled 80 patients for each group.
A computer generated random list was established with an online sequencer
(www.random.org/sequences) according to which participants were randomly assigned to one of
three study groups with 1:1:1 allocation ratio. Group A included isolated NSAID treatment and
received 400 mg etodolac twice a day. Group B included NSAID and magnesium treatment and
received a combination of 400 mg etodolac twice a day with 365 mg oral magnesium
supplementation once a day. Group C included NSAID and paracetamol treatment and combination
of 400 mg etodolac twice a day with 500 mg paracetamol twice a day was administered to the
participants of this group (Figure-1). We effort to prevent the placebo effect by comparing
the NSAID + magnesium therapy with both a NSAID plus paracetamol therapy and an isolated
NSAID therapy. Treatment was performed by two authors (S.B and K.Ş) and patients were
followed-up by same authors throughout the study. External medication was not allowed with
the exception of topical analgesics. Patients who received any intravenous or intramuscular
analgesia during the treatment period were excluded from study. Co-medications for any
accompanying chronic condition (diabetes, hypertension etc.) were unchanged.
Clinical evaluation of participants was performed at first admission to emergency department,
at 4th and 10th days after the initiation of designated treatment. Outcome measures included
pain, mobility of lumbar spine and functional outcome. Pain intensity was assessed using a
visual analogue scale (VAS). Lumbar spine mobility was assessed using the "finger to floor"
test. Participants were asked to stand on erect posture with knees extended and then to bend
forward in an attempt to reach for the floor with their fingertips without losing knee
extension. Distance between patient's fingertips and the floor was then measured with a
measuring tape. Functional outcome was evaluated with Roland-Morris Disability Questionnaire
(RMDQ) score. RMDQ is a 24-item LBP functional scale and is recommended for research
purposes. Higher scores signify greater low back-related functional impairment. An
improvement of 5 points was considered clinically significant.
