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Do acetaminophen and an NSAID combined relieve osteoarthritis pain better than either alone?
Combining nonsteroidal anti-inflammatory drugs (NSAIDs) and acetaminophen for short courses provides more relief of pain in osteoarthritis with-out an increase in side effects (strength of recommendation [SOR]=B). Combining acetaminophen at 4 g/d with an NSAID can also decrease the daily dose of NSAID required for pain relief, thus reducing the potential risk from higher-dose NSAID therapy (SOR=B).
Over the long term, however, this combination may increase the risk of upper gastrointestinal (GI) bleeding more than that conferred by the NSAID alone (SOR=B). If combination therapy is necessary, limiting the dose of acetaminophen to 2 g/d minimizes gastrointestinal toxicity. Acetaminophen alone at the lowest dose to provide pain relief is the safest pharmacologic choice for patients with osteoarthritis.
Evidence summary
Clinical guidelines for osteoarthritis recommend acetaminophen as first-line therapy followed by an NSAID or cyclooxygenase-2 (COX-2) inhibitor, and many patients are treated with combination therapy.
Several small randomized controlled trials have compared the individual efficacy of NSAIDs and acetaminophen in osteoarthritis and have found that both provide more pain relief than placebo.1-3There is a trend toward improved pain relief with NSAIDs compared with acetaminophen in the initial treatment period; however, few long-term studies of efficacy have been reported. One randomized controlled trial comparing 750 mg/d naproxen (Aleve, Naprosyn) with 2600 mg/d acetaminophen for 2 years found similar pain relief for both medications and a dropout rate of 65% in both groups.2 Similar numbers of persons taking acetaminophen or naproxen dropped out because of adverse effects (20%) or lack of efficacy (19%), and no difference was seen in functional improvement between the 2 groups.
A 6-week randomized double-blind crossover trial of 227 patients comparing 75 mg diclofenac and 200 mg misoprostol (Arthrotec) with acetaminophen 4 g/d found the diclofenac-misoprostol combination provided more pain control than acetaminophen alone. Adverse events were slightly more common in the diclofenac group (54% vs 46%; P=.046).4
The COX-2 inhibitors rofecoxib (Vioxx) and celecoxib (Celebrex) have been shown to provide equal pain relief compared with naproxen for patients with osteoarthritis.5 One industry-sponsored randomized trial found rofecoxib superior to celecoxib, and both superior to acetaminophen in treatment of osteoarthritis pain.6 There was no difference in the incidence of side effects among the 3 medications. Thirty percent of patients taking 4 g/d acetaminophen discontinued the study because of lack of efficacy, compared with 20% of those taking either celecoxib or rofecoxib.6
Few studies have evaluated the safety or efficacy of the combination of NSAIDs and acetaminophen in osteoarthritis. One double-blind, double-dummy crossover trial of 18 patients with osteoarthritis of the hip compared naproxen at doses of 500 mg and 1000 mg, with and without 4 g/d of acetaminophen, and 1500 mg/d of naproxen alone over 5 one-week trial periods.7Adding acetaminophen improved patient-reported pain scores compared with naproxen alone. Higher doses of naproxen alone provided less pain relief than a lower dose of naproxen combined with acetaminophen. GI side effects increased with the increase in naproxen dose, but were unaffected by the addition of acetaminophen. Functional ability was not affected during this short study. A similar study by the same researchers of patients with rheumatoid arthritis found similar results.7
One randomized, double-blind, crossover trial compared single doses of tolmetin (Tolectin, 100, 150, 200 mg) and acetaminophen (400 mg) alone and in combination with placebo in the control of experimentally induced pain (thermal and electrical stimulation). Acetaminophen alone did not differ from placebo in pain control; however, the combinations of acetaminophen with tolmetin provided similar pain relief to higher doses of tolmetin alone.8 No studies have evaluated the efficacy or safety of acetaminophen combined with rofecoxib or celecoxib.
Regarding the risks of combining acetaminophen with NSAIDs, 1 nested case-control study based on the entire enrollment panel of the British National Health Service characterized the risk of upper GI side effects among persons taking NSAIDs or acetaminophen alone or in combination. The study evaluated medications in use at the time of an upper GI bleed, controlling for age, sex, and concomitant medications (corticosteroids, H2 receptor antagonists, omeprazole, anticoagulants, and others) and excluding patients with varices, alcohol-related disorders, liver disease, and cancer; no attempt was made to control other comorbidities. The relative risk of upper GI perforation or bleeding for patients taking 2g/d acetaminophen or high-dose NSAIDs was 2.4 (95% confidence interval [CI], 1.7–3.5) and 3.6 (95% CI, 2.9–4.3), respectively. Concomitant use of an NSAID with 2 g/d of acetaminophen showed a relative risk of upper GI perforation or bleed of 16.6 (95% CI, 11.0–24.9). Acetaminophen doses <2 g/d conferred no additional risk for serious upper GI side effects.9
A systematic review of selective COX-2 inhibitors vs naproxen found fewer endoscopically detected ulcers in patients taking celecoxib but no difference in serious gastrointestinal bleeds.5 A meta-analysis of randomized controlled trials found a higher incidence of serious thrombotic cardiovascular events among patients taking COX-2 inhibitors compared with naprosyn.10 The safety profile of rofecoxib and celecoxib in the long-term treatment of pain is not fully understood at this time.
Recommendations from others
The American College of Rheumatology (ACR) recommends acetaminophen up to 4 g/d as a first-line pharmacologic treatment for osteoarthritis of the hip and knee, and advises NSAIDs be used at the lowest effective dose if they are necessary for pain control.11 The ACR does not specifically comment on combining NSAID and acetaminophen use. The American Academy of Orthopaedic Surgeons recommends initial use of an NSAID or acetaminophen, but does not comment on the combination of NSAIDs and acetaminophen.12
Adding acetaminophen may be more desirable than switching NSAIDs
Joseph Saseen, PharmD, FCCP, BCPS
University of Colorado Health Sciences Center, Denver
Compared with NSAIDs, acetaminophen has a complementary analgesic mechanism of action and can be safely used in many patients. Additive effects of acetaminophen have not been well described with all NSAIDs (eg, COX-2 inhibitors); however, this combination is inexpensive and overall appears to effectively augment analgesia when combined with NSAIDs. Although observational data demonstrate an increased risk of upper GI bleeding with this combination, selection bias (higher-risk patients being on combination therapy) could reasonably explain this association. Adding acetaminophen may be more desirable than switching NSAIDs for patients with osteoarthritis that have a partial response to their current NSAID therapy.
- Amoxicillin • Amoxil, Biomox, Polymox, Trimox, Wymox
- Cephalexin • Biocef, Keflex
- Celecoxib • Celebrex
- Diclofenac/Misoprostol • Arthrotec
- Ipratropium • Atrovent
- Labetalol • Trandate
- Methyldopa • Aldomet
- Naproxen • Aleve, Anaprox, Naprosyn
- Nitrofurantoin • Furadantin, Macrobid, Macrodantin
- Rofecoxib • Vioxx
- Tiotropium • Spiriva
- Tolmetin • Tolectin
- Triamcinalone • Aristocort, Atolone, Kenacort
- Sulfamethoxazole/Trimethoprim • Bactrim,Cotrim,
- Septra, Sulfatrim
- Sulfisoxazole • Gantrisin
1. Amadio P Jr, Cummings DM. Evaluation of acetaminophen in the management of osteoarthritis of the knee. Curr Ther Res 1983;34:59-66.
2. Williams HJ, Ward JR, Egger MJ, et al. Comparison of naproxen and acetaminophen in a two-year study of treatment of osteoarthritis of the knee. Arthritis Rheum 1993;36:1196-1206.
3. Bradley JD, Brandt KD, Katz BP, Kalasinski LA, Ryan SI. Treatment of knee osteoarthritis: relationship of clinical features of joint inflammation to the response to a nonsteroidal antiinflammatory drug or pure analgesic. J Rheumatol 1992;19:1950-1954.
4. Pincus T, Koch GG, Sokka T, et al. A randomized, double-blind, crossover clinical trial of diclofenac plus misoprostol versus acetaminophen for patients with osteoarthritis of the hip or knee. Arthritis Rheum 2001;44:1587-1598.
5. Deeks JJ, Smith LA, Bradley MD. Efficacy, tolerability, and upper gastrointestinal safety of celecoxib for treatment of osteoarthritis and rheumatoid arthritis: systematic review of randomised controlled trials. BMJ 2002;325:619.-
6. Geba GP, Weaver AL, Polis AB, Dixon ME, Schnitzer TJ. Vioxx. Acetaminophen Celecoxib Trial (VACT) Group. Efficacy of rofecoxib, celecoxib, and acetaminophen in osteoarthritis of the knee: a randomized trial. JAMA 2002;287:64-71.
7. Seideman P, Samuelson P, Neander G. Naproxen and paracetamol compared with naproxen only in coxarthrosis. Increased effect of the combination in 18 patients. Acta Orthop Scand 1993;64:285-288.
8. Stacher G, Bauer P, Ehn I, Schreiber E. Effects of tolmetin, paracetamol, and of two combinations of tolmetin and paracetamol as compared to placebo on experimentally induced pain. A double blind study. Int J Clin Pharmacol Biopharm 1979;17:250-255.
9. Garcia Rodriguez LA, Hernandez-Diaz S. The risk of upper gastrointestinal complications associated with nonsteroidal anti-inflammatory drugs, glucocorticoids, acetaminophen, and combinations of these agents. Arthritis Res 2001;3:98-101.
10. Mukherjee D, Nissen SE, Topol EJ. Risk of cardiovascular events associated with selective COX-2 inhibitors. JAMA 2001;286:954-959.
11. Recommendations for the medical management of osteoarthritis of the hip and knee: 2000 update. American College of Rheumatology Subcommittee on Osteoarthritis Guidelines. Arthritis Rheum 2000;43:1905-1915.
12. AAOS Clinical Guideline on Osteoarthritis of the Knee. Rosemont, IL: American Academy of Orthopaedic Surgeons, 2003. Available at: www.aaos.org/wordhtml/pdfs_r/guidelin/suprt_oakn.pdf. Accessed on May 11, 2004.
Combining nonsteroidal anti-inflammatory drugs (NSAIDs) and acetaminophen for short courses provides more relief of pain in osteoarthritis with-out an increase in side effects (strength of recommendation [SOR]=B). Combining acetaminophen at 4 g/d with an NSAID can also decrease the daily dose of NSAID required for pain relief, thus reducing the potential risk from higher-dose NSAID therapy (SOR=B).
Over the long term, however, this combination may increase the risk of upper gastrointestinal (GI) bleeding more than that conferred by the NSAID alone (SOR=B). If combination therapy is necessary, limiting the dose of acetaminophen to 2 g/d minimizes gastrointestinal toxicity. Acetaminophen alone at the lowest dose to provide pain relief is the safest pharmacologic choice for patients with osteoarthritis.
Evidence summary
Clinical guidelines for osteoarthritis recommend acetaminophen as first-line therapy followed by an NSAID or cyclooxygenase-2 (COX-2) inhibitor, and many patients are treated with combination therapy.
Several small randomized controlled trials have compared the individual efficacy of NSAIDs and acetaminophen in osteoarthritis and have found that both provide more pain relief than placebo.1-3There is a trend toward improved pain relief with NSAIDs compared with acetaminophen in the initial treatment period; however, few long-term studies of efficacy have been reported. One randomized controlled trial comparing 750 mg/d naproxen (Aleve, Naprosyn) with 2600 mg/d acetaminophen for 2 years found similar pain relief for both medications and a dropout rate of 65% in both groups.2 Similar numbers of persons taking acetaminophen or naproxen dropped out because of adverse effects (20%) or lack of efficacy (19%), and no difference was seen in functional improvement between the 2 groups.
A 6-week randomized double-blind crossover trial of 227 patients comparing 75 mg diclofenac and 200 mg misoprostol (Arthrotec) with acetaminophen 4 g/d found the diclofenac-misoprostol combination provided more pain control than acetaminophen alone. Adverse events were slightly more common in the diclofenac group (54% vs 46%; P=.046).4
The COX-2 inhibitors rofecoxib (Vioxx) and celecoxib (Celebrex) have been shown to provide equal pain relief compared with naproxen for patients with osteoarthritis.5 One industry-sponsored randomized trial found rofecoxib superior to celecoxib, and both superior to acetaminophen in treatment of osteoarthritis pain.6 There was no difference in the incidence of side effects among the 3 medications. Thirty percent of patients taking 4 g/d acetaminophen discontinued the study because of lack of efficacy, compared with 20% of those taking either celecoxib or rofecoxib.6
Few studies have evaluated the safety or efficacy of the combination of NSAIDs and acetaminophen in osteoarthritis. One double-blind, double-dummy crossover trial of 18 patients with osteoarthritis of the hip compared naproxen at doses of 500 mg and 1000 mg, with and without 4 g/d of acetaminophen, and 1500 mg/d of naproxen alone over 5 one-week trial periods.7Adding acetaminophen improved patient-reported pain scores compared with naproxen alone. Higher doses of naproxen alone provided less pain relief than a lower dose of naproxen combined with acetaminophen. GI side effects increased with the increase in naproxen dose, but were unaffected by the addition of acetaminophen. Functional ability was not affected during this short study. A similar study by the same researchers of patients with rheumatoid arthritis found similar results.7
One randomized, double-blind, crossover trial compared single doses of tolmetin (Tolectin, 100, 150, 200 mg) and acetaminophen (400 mg) alone and in combination with placebo in the control of experimentally induced pain (thermal and electrical stimulation). Acetaminophen alone did not differ from placebo in pain control; however, the combinations of acetaminophen with tolmetin provided similar pain relief to higher doses of tolmetin alone.8 No studies have evaluated the efficacy or safety of acetaminophen combined with rofecoxib or celecoxib.
Regarding the risks of combining acetaminophen with NSAIDs, 1 nested case-control study based on the entire enrollment panel of the British National Health Service characterized the risk of upper GI side effects among persons taking NSAIDs or acetaminophen alone or in combination. The study evaluated medications in use at the time of an upper GI bleed, controlling for age, sex, and concomitant medications (corticosteroids, H2 receptor antagonists, omeprazole, anticoagulants, and others) and excluding patients with varices, alcohol-related disorders, liver disease, and cancer; no attempt was made to control other comorbidities. The relative risk of upper GI perforation or bleeding for patients taking 2g/d acetaminophen or high-dose NSAIDs was 2.4 (95% confidence interval [CI], 1.7–3.5) and 3.6 (95% CI, 2.9–4.3), respectively. Concomitant use of an NSAID with 2 g/d of acetaminophen showed a relative risk of upper GI perforation or bleed of 16.6 (95% CI, 11.0–24.9). Acetaminophen doses <2 g/d conferred no additional risk for serious upper GI side effects.9
A systematic review of selective COX-2 inhibitors vs naproxen found fewer endoscopically detected ulcers in patients taking celecoxib but no difference in serious gastrointestinal bleeds.5 A meta-analysis of randomized controlled trials found a higher incidence of serious thrombotic cardiovascular events among patients taking COX-2 inhibitors compared with naprosyn.10 The safety profile of rofecoxib and celecoxib in the long-term treatment of pain is not fully understood at this time.
Recommendations from others
The American College of Rheumatology (ACR) recommends acetaminophen up to 4 g/d as a first-line pharmacologic treatment for osteoarthritis of the hip and knee, and advises NSAIDs be used at the lowest effective dose if they are necessary for pain control.11 The ACR does not specifically comment on combining NSAID and acetaminophen use. The American Academy of Orthopaedic Surgeons recommends initial use of an NSAID or acetaminophen, but does not comment on the combination of NSAIDs and acetaminophen.12
Adding acetaminophen may be more desirable than switching NSAIDs
Joseph Saseen, PharmD, FCCP, BCPS
University of Colorado Health Sciences Center, Denver
Compared with NSAIDs, acetaminophen has a complementary analgesic mechanism of action and can be safely used in many patients. Additive effects of acetaminophen have not been well described with all NSAIDs (eg, COX-2 inhibitors); however, this combination is inexpensive and overall appears to effectively augment analgesia when combined with NSAIDs. Although observational data demonstrate an increased risk of upper GI bleeding with this combination, selection bias (higher-risk patients being on combination therapy) could reasonably explain this association. Adding acetaminophen may be more desirable than switching NSAIDs for patients with osteoarthritis that have a partial response to their current NSAID therapy.
- Amoxicillin • Amoxil, Biomox, Polymox, Trimox, Wymox
- Cephalexin • Biocef, Keflex
- Celecoxib • Celebrex
- Diclofenac/Misoprostol • Arthrotec
- Ipratropium • Atrovent
- Labetalol • Trandate
- Methyldopa • Aldomet
- Naproxen • Aleve, Anaprox, Naprosyn
- Nitrofurantoin • Furadantin, Macrobid, Macrodantin
- Rofecoxib • Vioxx
- Tiotropium • Spiriva
- Tolmetin • Tolectin
- Triamcinalone • Aristocort, Atolone, Kenacort
- Sulfamethoxazole/Trimethoprim • Bactrim,Cotrim,
- Septra, Sulfatrim
- Sulfisoxazole • Gantrisin
Combining nonsteroidal anti-inflammatory drugs (NSAIDs) and acetaminophen for short courses provides more relief of pain in osteoarthritis with-out an increase in side effects (strength of recommendation [SOR]=B). Combining acetaminophen at 4 g/d with an NSAID can also decrease the daily dose of NSAID required for pain relief, thus reducing the potential risk from higher-dose NSAID therapy (SOR=B).
Over the long term, however, this combination may increase the risk of upper gastrointestinal (GI) bleeding more than that conferred by the NSAID alone (SOR=B). If combination therapy is necessary, limiting the dose of acetaminophen to 2 g/d minimizes gastrointestinal toxicity. Acetaminophen alone at the lowest dose to provide pain relief is the safest pharmacologic choice for patients with osteoarthritis.
Evidence summary
Clinical guidelines for osteoarthritis recommend acetaminophen as first-line therapy followed by an NSAID or cyclooxygenase-2 (COX-2) inhibitor, and many patients are treated with combination therapy.
Several small randomized controlled trials have compared the individual efficacy of NSAIDs and acetaminophen in osteoarthritis and have found that both provide more pain relief than placebo.1-3There is a trend toward improved pain relief with NSAIDs compared with acetaminophen in the initial treatment period; however, few long-term studies of efficacy have been reported. One randomized controlled trial comparing 750 mg/d naproxen (Aleve, Naprosyn) with 2600 mg/d acetaminophen for 2 years found similar pain relief for both medications and a dropout rate of 65% in both groups.2 Similar numbers of persons taking acetaminophen or naproxen dropped out because of adverse effects (20%) or lack of efficacy (19%), and no difference was seen in functional improvement between the 2 groups.
A 6-week randomized double-blind crossover trial of 227 patients comparing 75 mg diclofenac and 200 mg misoprostol (Arthrotec) with acetaminophen 4 g/d found the diclofenac-misoprostol combination provided more pain control than acetaminophen alone. Adverse events were slightly more common in the diclofenac group (54% vs 46%; P=.046).4
The COX-2 inhibitors rofecoxib (Vioxx) and celecoxib (Celebrex) have been shown to provide equal pain relief compared with naproxen for patients with osteoarthritis.5 One industry-sponsored randomized trial found rofecoxib superior to celecoxib, and both superior to acetaminophen in treatment of osteoarthritis pain.6 There was no difference in the incidence of side effects among the 3 medications. Thirty percent of patients taking 4 g/d acetaminophen discontinued the study because of lack of efficacy, compared with 20% of those taking either celecoxib or rofecoxib.6
Few studies have evaluated the safety or efficacy of the combination of NSAIDs and acetaminophen in osteoarthritis. One double-blind, double-dummy crossover trial of 18 patients with osteoarthritis of the hip compared naproxen at doses of 500 mg and 1000 mg, with and without 4 g/d of acetaminophen, and 1500 mg/d of naproxen alone over 5 one-week trial periods.7Adding acetaminophen improved patient-reported pain scores compared with naproxen alone. Higher doses of naproxen alone provided less pain relief than a lower dose of naproxen combined with acetaminophen. GI side effects increased with the increase in naproxen dose, but were unaffected by the addition of acetaminophen. Functional ability was not affected during this short study. A similar study by the same researchers of patients with rheumatoid arthritis found similar results.7
One randomized, double-blind, crossover trial compared single doses of tolmetin (Tolectin, 100, 150, 200 mg) and acetaminophen (400 mg) alone and in combination with placebo in the control of experimentally induced pain (thermal and electrical stimulation). Acetaminophen alone did not differ from placebo in pain control; however, the combinations of acetaminophen with tolmetin provided similar pain relief to higher doses of tolmetin alone.8 No studies have evaluated the efficacy or safety of acetaminophen combined with rofecoxib or celecoxib.
Regarding the risks of combining acetaminophen with NSAIDs, 1 nested case-control study based on the entire enrollment panel of the British National Health Service characterized the risk of upper GI side effects among persons taking NSAIDs or acetaminophen alone or in combination. The study evaluated medications in use at the time of an upper GI bleed, controlling for age, sex, and concomitant medications (corticosteroids, H2 receptor antagonists, omeprazole, anticoagulants, and others) and excluding patients with varices, alcohol-related disorders, liver disease, and cancer; no attempt was made to control other comorbidities. The relative risk of upper GI perforation or bleeding for patients taking 2g/d acetaminophen or high-dose NSAIDs was 2.4 (95% confidence interval [CI], 1.7–3.5) and 3.6 (95% CI, 2.9–4.3), respectively. Concomitant use of an NSAID with 2 g/d of acetaminophen showed a relative risk of upper GI perforation or bleed of 16.6 (95% CI, 11.0–24.9). Acetaminophen doses <2 g/d conferred no additional risk for serious upper GI side effects.9
A systematic review of selective COX-2 inhibitors vs naproxen found fewer endoscopically detected ulcers in patients taking celecoxib but no difference in serious gastrointestinal bleeds.5 A meta-analysis of randomized controlled trials found a higher incidence of serious thrombotic cardiovascular events among patients taking COX-2 inhibitors compared with naprosyn.10 The safety profile of rofecoxib and celecoxib in the long-term treatment of pain is not fully understood at this time.
Recommendations from others
The American College of Rheumatology (ACR) recommends acetaminophen up to 4 g/d as a first-line pharmacologic treatment for osteoarthritis of the hip and knee, and advises NSAIDs be used at the lowest effective dose if they are necessary for pain control.11 The ACR does not specifically comment on combining NSAID and acetaminophen use. The American Academy of Orthopaedic Surgeons recommends initial use of an NSAID or acetaminophen, but does not comment on the combination of NSAIDs and acetaminophen.12
Adding acetaminophen may be more desirable than switching NSAIDs
Joseph Saseen, PharmD, FCCP, BCPS
University of Colorado Health Sciences Center, Denver
Compared with NSAIDs, acetaminophen has a complementary analgesic mechanism of action and can be safely used in many patients. Additive effects of acetaminophen have not been well described with all NSAIDs (eg, COX-2 inhibitors); however, this combination is inexpensive and overall appears to effectively augment analgesia when combined with NSAIDs. Although observational data demonstrate an increased risk of upper GI bleeding with this combination, selection bias (higher-risk patients being on combination therapy) could reasonably explain this association. Adding acetaminophen may be more desirable than switching NSAIDs for patients with osteoarthritis that have a partial response to their current NSAID therapy.
- Amoxicillin • Amoxil, Biomox, Polymox, Trimox, Wymox
- Cephalexin • Biocef, Keflex
- Celecoxib • Celebrex
- Diclofenac/Misoprostol • Arthrotec
- Ipratropium • Atrovent
- Labetalol • Trandate
- Methyldopa • Aldomet
- Naproxen • Aleve, Anaprox, Naprosyn
- Nitrofurantoin • Furadantin, Macrobid, Macrodantin
- Rofecoxib • Vioxx
- Tiotropium • Spiriva
- Tolmetin • Tolectin
- Triamcinalone • Aristocort, Atolone, Kenacort
- Sulfamethoxazole/Trimethoprim • Bactrim,Cotrim,
- Septra, Sulfatrim
- Sulfisoxazole • Gantrisin
1. Amadio P Jr, Cummings DM. Evaluation of acetaminophen in the management of osteoarthritis of the knee. Curr Ther Res 1983;34:59-66.
2. Williams HJ, Ward JR, Egger MJ, et al. Comparison of naproxen and acetaminophen in a two-year study of treatment of osteoarthritis of the knee. Arthritis Rheum 1993;36:1196-1206.
3. Bradley JD, Brandt KD, Katz BP, Kalasinski LA, Ryan SI. Treatment of knee osteoarthritis: relationship of clinical features of joint inflammation to the response to a nonsteroidal antiinflammatory drug or pure analgesic. J Rheumatol 1992;19:1950-1954.
4. Pincus T, Koch GG, Sokka T, et al. A randomized, double-blind, crossover clinical trial of diclofenac plus misoprostol versus acetaminophen for patients with osteoarthritis of the hip or knee. Arthritis Rheum 2001;44:1587-1598.
5. Deeks JJ, Smith LA, Bradley MD. Efficacy, tolerability, and upper gastrointestinal safety of celecoxib for treatment of osteoarthritis and rheumatoid arthritis: systematic review of randomised controlled trials. BMJ 2002;325:619.-
6. Geba GP, Weaver AL, Polis AB, Dixon ME, Schnitzer TJ. Vioxx. Acetaminophen Celecoxib Trial (VACT) Group. Efficacy of rofecoxib, celecoxib, and acetaminophen in osteoarthritis of the knee: a randomized trial. JAMA 2002;287:64-71.
7. Seideman P, Samuelson P, Neander G. Naproxen and paracetamol compared with naproxen only in coxarthrosis. Increased effect of the combination in 18 patients. Acta Orthop Scand 1993;64:285-288.
8. Stacher G, Bauer P, Ehn I, Schreiber E. Effects of tolmetin, paracetamol, and of two combinations of tolmetin and paracetamol as compared to placebo on experimentally induced pain. A double blind study. Int J Clin Pharmacol Biopharm 1979;17:250-255.
9. Garcia Rodriguez LA, Hernandez-Diaz S. The risk of upper gastrointestinal complications associated with nonsteroidal anti-inflammatory drugs, glucocorticoids, acetaminophen, and combinations of these agents. Arthritis Res 2001;3:98-101.
10. Mukherjee D, Nissen SE, Topol EJ. Risk of cardiovascular events associated with selective COX-2 inhibitors. JAMA 2001;286:954-959.
11. Recommendations for the medical management of osteoarthritis of the hip and knee: 2000 update. American College of Rheumatology Subcommittee on Osteoarthritis Guidelines. Arthritis Rheum 2000;43:1905-1915.
12. AAOS Clinical Guideline on Osteoarthritis of the Knee. Rosemont, IL: American Academy of Orthopaedic Surgeons, 2003. Available at: www.aaos.org/wordhtml/pdfs_r/guidelin/suprt_oakn.pdf. Accessed on May 11, 2004.
1. Amadio P Jr, Cummings DM. Evaluation of acetaminophen in the management of osteoarthritis of the knee. Curr Ther Res 1983;34:59-66.
2. Williams HJ, Ward JR, Egger MJ, et al. Comparison of naproxen and acetaminophen in a two-year study of treatment of osteoarthritis of the knee. Arthritis Rheum 1993;36:1196-1206.
3. Bradley JD, Brandt KD, Katz BP, Kalasinski LA, Ryan SI. Treatment of knee osteoarthritis: relationship of clinical features of joint inflammation to the response to a nonsteroidal antiinflammatory drug or pure analgesic. J Rheumatol 1992;19:1950-1954.
4. Pincus T, Koch GG, Sokka T, et al. A randomized, double-blind, crossover clinical trial of diclofenac plus misoprostol versus acetaminophen for patients with osteoarthritis of the hip or knee. Arthritis Rheum 2001;44:1587-1598.
5. Deeks JJ, Smith LA, Bradley MD. Efficacy, tolerability, and upper gastrointestinal safety of celecoxib for treatment of osteoarthritis and rheumatoid arthritis: systematic review of randomised controlled trials. BMJ 2002;325:619.-
6. Geba GP, Weaver AL, Polis AB, Dixon ME, Schnitzer TJ. Vioxx. Acetaminophen Celecoxib Trial (VACT) Group. Efficacy of rofecoxib, celecoxib, and acetaminophen in osteoarthritis of the knee: a randomized trial. JAMA 2002;287:64-71.
7. Seideman P, Samuelson P, Neander G. Naproxen and paracetamol compared with naproxen only in coxarthrosis. Increased effect of the combination in 18 patients. Acta Orthop Scand 1993;64:285-288.
8. Stacher G, Bauer P, Ehn I, Schreiber E. Effects of tolmetin, paracetamol, and of two combinations of tolmetin and paracetamol as compared to placebo on experimentally induced pain. A double blind study. Int J Clin Pharmacol Biopharm 1979;17:250-255.
9. Garcia Rodriguez LA, Hernandez-Diaz S. The risk of upper gastrointestinal complications associated with nonsteroidal anti-inflammatory drugs, glucocorticoids, acetaminophen, and combinations of these agents. Arthritis Res 2001;3:98-101.
10. Mukherjee D, Nissen SE, Topol EJ. Risk of cardiovascular events associated with selective COX-2 inhibitors. JAMA 2001;286:954-959.
11. Recommendations for the medical management of osteoarthritis of the hip and knee: 2000 update. American College of Rheumatology Subcommittee on Osteoarthritis Guidelines. Arthritis Rheum 2000;43:1905-1915.
12. AAOS Clinical Guideline on Osteoarthritis of the Knee. Rosemont, IL: American Academy of Orthopaedic Surgeons, 2003. Available at: www.aaos.org/wordhtml/pdfs_r/guidelin/suprt_oakn.pdf. Accessed on May 11, 2004.
Evidence-based answers from the Family Physicians Inquiries Network
Vaccinations containing thimerosal do not increase rates of autism
This retrospective cohort study found that autism rates in children receiving vaccines containing thimerosal were not statistically different than for children receiving thimerosal-free vaccines.
This study refutes any connection between the thimerosal preservative and autistic disorders, but does not evaluate the risk of autistic disorders in vaccinated children compared with those who are not vaccinated. No routine pediatric vaccinations currently used in the United States contain thimerosal.
This retrospective cohort study found that autism rates in children receiving vaccines containing thimerosal were not statistically different than for children receiving thimerosal-free vaccines.
This study refutes any connection between the thimerosal preservative and autistic disorders, but does not evaluate the risk of autistic disorders in vaccinated children compared with those who are not vaccinated. No routine pediatric vaccinations currently used in the United States contain thimerosal.
This retrospective cohort study found that autism rates in children receiving vaccines containing thimerosal were not statistically different than for children receiving thimerosal-free vaccines.
This study refutes any connection between the thimerosal preservative and autistic disorders, but does not evaluate the risk of autistic disorders in vaccinated children compared with those who are not vaccinated. No routine pediatric vaccinations currently used in the United States contain thimerosal.
False-positive mammograms increase follow-up rates
This population-based study found that women who had a false-positive mammogram had higher rates of rescreening at 18- and 30-month follow-up. In 10 years of annual screening, 50% of women will have a false-positive mammogram. However, the consequences of false-positives do not deter women from continued breast cancer screening.
When evaluating screening tests it is important to consider the effect of a false-positive test on the people being screened. The subsequent work-up for each false-positive may increase patient anxiety, total costs, and the risk of morbidity from unnecessary interventions.
This population-based study found that women who had a false-positive mammogram had higher rates of rescreening at 18- and 30-month follow-up. In 10 years of annual screening, 50% of women will have a false-positive mammogram. However, the consequences of false-positives do not deter women from continued breast cancer screening.
When evaluating screening tests it is important to consider the effect of a false-positive test on the people being screened. The subsequent work-up for each false-positive may increase patient anxiety, total costs, and the risk of morbidity from unnecessary interventions.
This population-based study found that women who had a false-positive mammogram had higher rates of rescreening at 18- and 30-month follow-up. In 10 years of annual screening, 50% of women will have a false-positive mammogram. However, the consequences of false-positives do not deter women from continued breast cancer screening.
When evaluating screening tests it is important to consider the effect of a false-positive test on the people being screened. The subsequent work-up for each false-positive may increase patient anxiety, total costs, and the risk of morbidity from unnecessary interventions.
Can a bedside blood test predict death or myocardial infarction (MI) in patients with chest pain?
BACKGROUND: Emergency departments triage more than 5 million patients with chest pain each year. Cardiac blood tests are used to identify patients at higher risk for MI or death. The bedside instrument in this study is a new approach to the immediate risk stratification of patients with symptoms suggestive of myocardial ischemia.
POPULATION STUDIED: The investigators enrolled 1005 patients older than 18 years with possible myocardial ischemia who presented to the emergency room of 6 US hospitals. Patients were excluded if electrocardiography showed ST-segment elevation or left bundle branch block. The average patient age was 51years; 51% were women; 14% had a previous MI; 21% had diabetes; 53% had hypertension; and 38% were current cigarette smokers. The researchers were able to provide complete results for 95% of the patients.
STUDY DESIGN AND VALIDITY: This was a prospective study looking at the prognostic value of a bedside instrument measuring cardiac enzymes at the point of care. Blood samples were obtained from patients at baseline and at 3 and 6 hours. If the patient was hospitalized, samples were obtained at 9, 12, and 16 to 24 hours. These were analyzed by the Dade-Behring Stratus CS STAT near-patient instrument, which assays myoglobin; creatine kinase, myocardial bound (CK-MB); and troponin I (cTnI) from a blood sample in 15 to 20 minutes. Two multimarker strategies (MMS) were defined: MMS-1 included all 3 markers, and MMS-2 included only CK-MB and cTnI. A strategy was considered positive if any of the markers was positive. The CS STAT assay was compared with the CK-MB result of the local hospital laboratory. All patients underwent both local laboratory testing and bedside testing, but treating physicians used only local CK-MB results in making management decisions. This study was well designed for comparing the prognostic value of the CS STAT values with conventional CK-MB values. However, a more useful outcome would be the utility of this bedside instrument in the diagnosis of MI. Also, whether such an instrument would lead to clinically significant changes in prognosis outside of special chest pain units is unclear.
OUTCOMES MEASURED: The rate of MI or death at 30 days was determined for patients with either a positive or negative MMS or CK-MB test result. Additional assessments included time from arrival to a positive test result and the relation of MMS status to the rates of MI, death, and revascularization at 30 days.
RESULTS: Testing at baseline (on initial evaluation in the emergency department) predicted death or MI within 30 days in 19% of patients with a positive MMS-1, 22% with a positive MMS-2, and 13% with a positive CK-MB result. Conversely, only 3% with a negative MMS-1 or MMS-2 and 6% with a negative CK-MB result died or had a MI at 30 days. With serial testing 55% of persons with an abnormal CK-MB result had a MI at 30 days, while serial MMS testing did not discriminate any better than the single test. The bedside 3-marker strategy was superior in predicting 30-day mortality; all 3 patients who died had a positive MMS-1 at baseline, while only 1 of 3 had an abnormal CK-MB on serial testing. An abnormal CK-MB result predicted revascularization within 30-days better than bedside testing using both single and serial measurements. After emergency department arrival, positive test results were obtained more quickly using the bedside instrument (MMS-1=2.5 hours, MMS-2=2.8 hours, LL=3.4 hours; P=.0001).
A single bedside multimarker test (myoglobin, troponpin I, and CK-MB) is more likely than a single CK-MB result to determine risk for MI or death within 30 days after an episode of chest pain. Serial CK-MB testing outperformed both single and serial MMS testing in predicting 30-day MI, need for revascularization, and combined outcome of MI or death. This single bedside test may be a useful adjunct to standard tests in identifying patients at higher risk for MI or death. However, it should not replace serial CK-MB testing in the diagnosis of MI.
BACKGROUND: Emergency departments triage more than 5 million patients with chest pain each year. Cardiac blood tests are used to identify patients at higher risk for MI or death. The bedside instrument in this study is a new approach to the immediate risk stratification of patients with symptoms suggestive of myocardial ischemia.
POPULATION STUDIED: The investigators enrolled 1005 patients older than 18 years with possible myocardial ischemia who presented to the emergency room of 6 US hospitals. Patients were excluded if electrocardiography showed ST-segment elevation or left bundle branch block. The average patient age was 51years; 51% were women; 14% had a previous MI; 21% had diabetes; 53% had hypertension; and 38% were current cigarette smokers. The researchers were able to provide complete results for 95% of the patients.
STUDY DESIGN AND VALIDITY: This was a prospective study looking at the prognostic value of a bedside instrument measuring cardiac enzymes at the point of care. Blood samples were obtained from patients at baseline and at 3 and 6 hours. If the patient was hospitalized, samples were obtained at 9, 12, and 16 to 24 hours. These were analyzed by the Dade-Behring Stratus CS STAT near-patient instrument, which assays myoglobin; creatine kinase, myocardial bound (CK-MB); and troponin I (cTnI) from a blood sample in 15 to 20 minutes. Two multimarker strategies (MMS) were defined: MMS-1 included all 3 markers, and MMS-2 included only CK-MB and cTnI. A strategy was considered positive if any of the markers was positive. The CS STAT assay was compared with the CK-MB result of the local hospital laboratory. All patients underwent both local laboratory testing and bedside testing, but treating physicians used only local CK-MB results in making management decisions. This study was well designed for comparing the prognostic value of the CS STAT values with conventional CK-MB values. However, a more useful outcome would be the utility of this bedside instrument in the diagnosis of MI. Also, whether such an instrument would lead to clinically significant changes in prognosis outside of special chest pain units is unclear.
OUTCOMES MEASURED: The rate of MI or death at 30 days was determined for patients with either a positive or negative MMS or CK-MB test result. Additional assessments included time from arrival to a positive test result and the relation of MMS status to the rates of MI, death, and revascularization at 30 days.
RESULTS: Testing at baseline (on initial evaluation in the emergency department) predicted death or MI within 30 days in 19% of patients with a positive MMS-1, 22% with a positive MMS-2, and 13% with a positive CK-MB result. Conversely, only 3% with a negative MMS-1 or MMS-2 and 6% with a negative CK-MB result died or had a MI at 30 days. With serial testing 55% of persons with an abnormal CK-MB result had a MI at 30 days, while serial MMS testing did not discriminate any better than the single test. The bedside 3-marker strategy was superior in predicting 30-day mortality; all 3 patients who died had a positive MMS-1 at baseline, while only 1 of 3 had an abnormal CK-MB on serial testing. An abnormal CK-MB result predicted revascularization within 30-days better than bedside testing using both single and serial measurements. After emergency department arrival, positive test results were obtained more quickly using the bedside instrument (MMS-1=2.5 hours, MMS-2=2.8 hours, LL=3.4 hours; P=.0001).
A single bedside multimarker test (myoglobin, troponpin I, and CK-MB) is more likely than a single CK-MB result to determine risk for MI or death within 30 days after an episode of chest pain. Serial CK-MB testing outperformed both single and serial MMS testing in predicting 30-day MI, need for revascularization, and combined outcome of MI or death. This single bedside test may be a useful adjunct to standard tests in identifying patients at higher risk for MI or death. However, it should not replace serial CK-MB testing in the diagnosis of MI.
BACKGROUND: Emergency departments triage more than 5 million patients with chest pain each year. Cardiac blood tests are used to identify patients at higher risk for MI or death. The bedside instrument in this study is a new approach to the immediate risk stratification of patients with symptoms suggestive of myocardial ischemia.
POPULATION STUDIED: The investigators enrolled 1005 patients older than 18 years with possible myocardial ischemia who presented to the emergency room of 6 US hospitals. Patients were excluded if electrocardiography showed ST-segment elevation or left bundle branch block. The average patient age was 51years; 51% were women; 14% had a previous MI; 21% had diabetes; 53% had hypertension; and 38% were current cigarette smokers. The researchers were able to provide complete results for 95% of the patients.
STUDY DESIGN AND VALIDITY: This was a prospective study looking at the prognostic value of a bedside instrument measuring cardiac enzymes at the point of care. Blood samples were obtained from patients at baseline and at 3 and 6 hours. If the patient was hospitalized, samples were obtained at 9, 12, and 16 to 24 hours. These were analyzed by the Dade-Behring Stratus CS STAT near-patient instrument, which assays myoglobin; creatine kinase, myocardial bound (CK-MB); and troponin I (cTnI) from a blood sample in 15 to 20 minutes. Two multimarker strategies (MMS) were defined: MMS-1 included all 3 markers, and MMS-2 included only CK-MB and cTnI. A strategy was considered positive if any of the markers was positive. The CS STAT assay was compared with the CK-MB result of the local hospital laboratory. All patients underwent both local laboratory testing and bedside testing, but treating physicians used only local CK-MB results in making management decisions. This study was well designed for comparing the prognostic value of the CS STAT values with conventional CK-MB values. However, a more useful outcome would be the utility of this bedside instrument in the diagnosis of MI. Also, whether such an instrument would lead to clinically significant changes in prognosis outside of special chest pain units is unclear.
OUTCOMES MEASURED: The rate of MI or death at 30 days was determined for patients with either a positive or negative MMS or CK-MB test result. Additional assessments included time from arrival to a positive test result and the relation of MMS status to the rates of MI, death, and revascularization at 30 days.
RESULTS: Testing at baseline (on initial evaluation in the emergency department) predicted death or MI within 30 days in 19% of patients with a positive MMS-1, 22% with a positive MMS-2, and 13% with a positive CK-MB result. Conversely, only 3% with a negative MMS-1 or MMS-2 and 6% with a negative CK-MB result died or had a MI at 30 days. With serial testing 55% of persons with an abnormal CK-MB result had a MI at 30 days, while serial MMS testing did not discriminate any better than the single test. The bedside 3-marker strategy was superior in predicting 30-day mortality; all 3 patients who died had a positive MMS-1 at baseline, while only 1 of 3 had an abnormal CK-MB on serial testing. An abnormal CK-MB result predicted revascularization within 30-days better than bedside testing using both single and serial measurements. After emergency department arrival, positive test results were obtained more quickly using the bedside instrument (MMS-1=2.5 hours, MMS-2=2.8 hours, LL=3.4 hours; P=.0001).
A single bedside multimarker test (myoglobin, troponpin I, and CK-MB) is more likely than a single CK-MB result to determine risk for MI or death within 30 days after an episode of chest pain. Serial CK-MB testing outperformed both single and serial MMS testing in predicting 30-day MI, need for revascularization, and combined outcome of MI or death. This single bedside test may be a useful adjunct to standard tests in identifying patients at higher risk for MI or death. However, it should not replace serial CK-MB testing in the diagnosis of MI.