opiates for acute low back pain??

JAMA just published a randomized clinical trial on the use of opioids or cyclobenzaprine in addition to naproxen for patients going to the emergency room with acute low back pain (see LBP opioids JAMA2015 in dropbox, or JAMA. 2015;314(15):1572-1580​). details:

--setting: inner city ER in the Bronx, New York City, looked at patients with nontraumatic, nonradicular low back pain (LBP) of <2 weeks' duration and had score >5 on Roland-Morris Disability Questionnaire (RMDQ), a 24-item instrument used to assess functional impairment in patients with LBP, with scores ranging from 0 to 24. a 5-point improvement is considered clinically significant
--323 patients (mean age 39, 50% men, 45% never had LBP before and 12% had it >1x/year, 28% had on-the-job injury, 5% positive depression screen, and mean RMDQ was 20) were randomized to naproxen 500 bid, along with either placebo, cyclobenzaprine 5mg , or oxycodone/acetaminophen 5/325 mg (all to take 1-2 q8hrs as needed, 60 pills given). all received a standard 10-minute LBP educational session prior to discharge from the ER
--patients were contacted 7 days and 3 months after the ER visit
--results, assessed 1 week later:
    --mean RMDQ in placebo group = 9.8
    ​--mean RMDQ in cyclobenzaprine group = 10.1
    ​--mean RMDQ in oxycodone/acetaminophen group = 11.1
    --none of these were a statistically significant difference in terms of functional pain
    ​--at 7 days, 40% rated their pain as moderate-to-severe, >50% of those in each group continued to need pain meds after 7 days, and 70% would want the same treatment with subsequent LBP episodes (no significant difference between groups)
    --also no difference in use of health care resources (ER/primary care/specialty/PT visits), frequency of naproxen use or frequency of use of study med
    -- more than 75% took naproxen daily and 2/3 took it bid; only 1/3 used the study medicine >1x/day and 40% used it intermittently, though there was no significant difference in outcome if limit the analysis to those taking the study medicine >1x. secondary analysis did find that of those who took their study meds >1x, more on opiates rated their pain as mild to none.
    --more adverse events in those not on placebo (mostly drowsiness, dizziness, nausea/vomiting with oxycodone/acetaminophen; less impressive increase in drowsiness with cyclobenzaprine)
    ​--3 months later: 1 in 4 patients in each group still had moderate or severe LBP, and 2.3% were taking opioids. 80% of each group had resumed their usual activities and 80% were back to fulltime work. again, no difference between the groups.

the JAMA authors cite other studies finding that 70% of patients still have functional impairment and continued analgesic use 1 week after an ER visit for acute LBP. also, despite the prevalent usage, studies suggest that combining meds (eg cyclobenzaprine and opioids) is no more efficacious than prescribing monotherapy.

so, this article does raise a few issues: 
    --most of these patients with pretty severe acute LBP did not take their full complement of pain medications (only 2/3 took the naproxen bid and most did not take their additional study med very much)
    --in my (limited) experience, very few patients who go to the ER with acute low back pain do not leave without an array of scripts including opiates (and i have seen several patients who were given opiate meds even though they explicitly asked not to get them, with "well, take the prescription anyway, just in case you need it...."). this and other studies suggest that polypharmacy does not add anything
    --it is impressive but not surprising that 1 week later, there was pretty dramatic improvement in the disability scores. But it seemed that adding the cyclobenzaprine or oxycodone did not seem to add anything to the naproxen.
    --one difficult issue for some patients might be to convince them that simple over-the-counter remedies (eg naproxen, or even acetaminophen from other studies) is sufficient to treat their pretty disabling pain. but, perhaps a persuasive "this is really the best medication for you, works as well as any other medication, and has many fewer side-effects than the others" may work (we have had pretty good success with a similar line of argument in decreasing the use of antibiotics for viral illnesses, esp when given in a positive, reasonably exuberant and reassuring fashion).

Comments

Post a Comment

if you would like to receive the near-daily emails regularly, please email me at gmodest@uphams.org

Popular posts from this blog

HDL a negative risk factor? or cholesterol efflux??

Although the data on HDL being protective of atherosclerotic disease is pretty consistent, there are negative studies, and the data on medications which dramatically improve HDL levels (eg, the cholesteryl ester transfer protein --CETP --inhibitors, such as torcetrapib) are clinically disappointing. there have been several explanations for this. for example, some HDL particles are "pro-inflammatory" and elicit an atherosclerotic response (which may be related to apolipoprotein C-III). a new article in NEJM highlights another angle -- that the issue is not the HDL number, but HDL's functionality in the reverse transport of cholesterol, as measured by the cholesterol efflux capacity (see  lipids HDL efflux capacity vs amt NEJM 2014 in dropbox, or  DOI: 10.1056/NEJMoa1409065). This article looks at the Dallas Heart Study, where they measured HDL levels, HDL particle concentrations, and cholesterol efflux capacity in 2924 adults free of cardiovascular disease and followed p
Read more

Drug company shenanigans: narcolepsy drug

I have not done a blog for a long time on drug company shenanigans. So it is my great pleasure to bring up a brand-new drug company approach to garner huge amounts of money (see  https://www.nytimes.com/2023/02/28/business/jazz-narcolepsy-avadel-patents.html?smid=nytcore-ios-share&referringSource=articleShare  ).  Based on an article by  Rebecca Robbins of the New York Times, who has written several articles on drug company excesses   As background, this will be my 42 nd  such blog: for the array, see  https://bucommunitymed.wpengine.com/page/4/?s=drug+company+shenanigans   Th e drug company  approach  this time  to extending  their  patents has a few “interesting” angles: -- this is a medication manufactured by Jazz Pharmaceuticals to treat narcolepsy: there are 2 versions: Xyrem and Xywav (Xywav has less sodium, so is marketed to those who should be on a low sodium diet). These meds are basically derivatives of gammahydroxybutyric acid (GHB)      -- the drug actually has a pretty
Read more

UPDATE: ASCVD risk factor critique

  I decided to do an extensive update of my prior ASCVD (atherosclerotic cardiovascular disease) risk analysis and critique of risk calculators, with much more information about the “non-traditional” risk factors. I felt that there should be more data/clarification, since I think we are really undertreating/not preventing the most common cause of death by relying on the ASCVD risk calculators   -- Cardiovascular risk models:      -- many of us rely on the various cardiovascular risk models to determine the appropriate approach to patients, and these are often integrated into the electronic medical records      -- these risk models have several very important limitations:          -- they are typically based on community data, eg from the Framingham study etc. But, in clinical practice, we are dealing with the individual and not the community:              -- there is very clear evidence that there are many individual risk factors that are associated with increased risk of a cardiovascu
Read more