Clinical Trial Details
— Status: Completed
Administrative data
| NCT number |
NCT05626283 |
| Other study ID # |
FMBSUREC/050722022/Mohiee |
| Secondary ID |
|
| Status |
Completed |
| Phase |
Phase 4
|
| First received |
|
| Last updated |
|
| Start date |
December 1, 2022 |
| Est. completion date |
September 1, 2023 |
Study information
| Verified date |
May 2024 |
| Source |
Beni-Suef University |
| Contact |
n/a |
| Is FDA regulated |
No |
| Health authority |
|
| Study type |
Interventional
|
Clinical Trial Summary
Chronic pain could be considered a brain disease as it can affect multiple aspects of brain
function, chemistry, neural networks and structure. Pain is associated with impaired
cognitive function (1). Around 45-50% of these patients report cognitive deficits such as
forgetfulness (23.4%), minor accidents (23.1%), difficulty finishing tasks (20.5%), and
difficulty maintaining attention (18.7%) (2,3). Many studies emphasised an impairment in the
cognitive tests assessing executive functioning, attention abilities, processing speed, and
memory in patients with chronic pain (4,5). Studies of community-dwelling older adults found
that pain, particularly widespread or severe pain, was associated with mobility Limitations
in physical performance (e.g., walking speed, stair climbing, and activities of daily living)
(6-9) in individuals with chronic pain and correspond to the pain level (10,11). Finally,
both pain and impaired cognition affect mobility status in older adults, and mobility is
affected to a greater extent when both are present (12).
Recent data indicate that miR-155 has a typical multifunctional miRNA and plays a crucial
role in various physiological and pathological processes such as immunity, inflammation,
cognitive dysfunction and neuropathies (13). The available experimental evidence indicating
that miR-155 is up-regulated in neuropathies allows us to include this miRNA in the list of
genes of paramount importance in chronic low back pain diagnosis and prognosis. Exogenous
molecular control in vivo of miR-155 expression could open up new ways to restore cognitive
outcome or attenuate the pain intensity (14).
No study searched the role of intervention (epidural steroid injection) on cognitive function
reserve, whether it is a better substitution or not for the conservative medical treatment.
Since exogenous steroid is a part of epidural injection, the systemic effect of a single dose
of steroids does not affect cognitive function, giving superiority to the intervention
modality on the conservative medical therapy approach (15).
Aim ot the work This work aims to study the impact of transforaminal epidural steroid
injection in lumbar disc prolapse on pain intensity and cognitive function in relation to
Micro RNA-155 serum level.
Description:
Study design and Participants:
The study will be conducted in two stages:
Stage (1): It will be a case control study that will include 44 patients diagnosed as having
symptomatic lumbar disc prolapse and 44 age and sex matched healthy controls. Both patients
and control groups will be subjected to measurement of baseline miR-155 expression level.
Stage (2): It will be an interventional non-experimental study that will include only the 44
patients who had symptomatic lumbar disc prolapse. Those patients will be subjected to
transforaminal epidural steroid injection. Assessment of pain intensity, functional
disability, cognitive function, depression, and miR-155 expression level will be done for the
included patients before and 1 month after transforaminal epidural steroid injection to
clarify the effect steroid injection on these variables.
The included patients will be recruited from the neurology and pain clinics of Beni-Suef
University Hospital, in the period from December 2022 to September 2023.
The study will include patients with clinical evidence of disc bulge in the form of disc
related radicular pain of >3 months duration, not responding to conservative treatment and
interfering with daily activities. The selected patients should have radiological evidence of
posterolateral lumbar disc bulge by MRI lumbosacral.
Data collection History will be taken from the selected patients regarding the demographics
and the duration of lumbar disc related radicular pain. The imaging findings regarding the
number of prolapsed discs and the degree of the most prolapsed disc will be also obtained.
Assessment of pain intensity and functional disability Assessment of the pain intensity and
functional disability will be done before and 1 month after the interventional pain
management procedure. Assessment will be done using Numeric Rating Scale (NRS) and Oswestry
Disability Index (ODI).
Cognitive assessment Cognitive assessment will be done before and 1 month after the
interventional pain management procedure. Assessment will be done using Paired Associate
Learning test (PALT), Paced Auditory Serial Addition Test (PASAT), and Controlled Oral Word
Association Test (COWAT).
Interventional pain Procedure:
The selected patients will be brought to the preparation room where reassurance will be done.
Intravenous midazolam 0.2 mg/kg will be given to them, then they will be placed in the prone
position on fluoroscopy table and draped in a sterile manner. They will be connected to a
monitor (SPO2, NIBLP, and ECG) and given supplemental oxygen through a nasal cannula (3
L/min) to maintain the oxygen saturation. A 22-gauge, 3.5-inch spinal needle will be used in
the injection procedure. With each insertion of the spinal needle, 1 ml with 20 mg of local
anesthetic lidocaine 2% will be injected intradermally.
The patients will be given transforaminal epidural injection of steroids with local
anesthetic (7 mg Betamethasone preceded by a test dose of 1 milliliter 2% lidocaine).
Laboratory assessment Estimation of miR-155 expression level: Blood samples (5 mL) will be
collected from the patients (before and 1 month after the interventional procedure) and
controls. The samples will be centrifuged at 3000 rpm for 10 min and plasma and/ or serum
will be stored at -80 C till analysis. Total RNA will be extracted. Quantitative real-time
polymerase chain reaction (PCR) will be performed. miR-155 expression level will be
calculated by the difference in threshold cycle method.
