Session Information
Session Type: Abstract Submissions (ACR)
Background/Purpose:
Results from randomized controlled trials indicate that about one-third of rheumatoid arthritis (RA) patients initially treated with anti-TNF agents do not respond, show a sub-optimal response, lose response, or develop adverse events (Kwoh et al 2002). Patients who discontinue their first biologic DMARD therapy might need to switch to a second or subsequent biologic DMARD treatment. The objective of this analysis is to describe reasons for discontinuation of their first anti-TNF for the treatment of RA and subsequently discontinuing either a second anti-TNF or biologic DMARDs with other mechanisms of action (oMOA).
Methods:
An observational, non-interventional, retrospective chart review study was conducted in 8 centers in the United States from February to September 2012. Patient charts were eligible if the patient’s first biologic DMARD was a anti-TNF; they were 18 years or older at time of the second DMARD; and they were prescribed the second and/or third biologic DMARD during the period July 1, 2006 and October 1, 2011. The proportion of patients stating each reason for treatment discontinuation are described for patients discontinuing anti-TNF vs. oMOA as their second and/or third biologic DMARD.
Results:
A total of 176 charts were abstracted for patients who discontinued a anti-TNF as their first biologic DMARD and received a second biologic DMARD. Second biologic DMARD treatments were another anti-TNF for 122 patients and treatments with oMOA for 54 patients. At time of chart abstraction 108 patients had discontinued the second DMARD. Of these, 98 then received a third biologic DMARD (36 anti-TNF and 62 with oMOA) with 43 of these patients discontinuing the third biologic DMARD. Reasons for discontinuation are shown in the table:
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Reasons for discontinuation of Biologic DMARDs |
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Second biologic |
Third biologic |
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First anti-TNF (n=176) |
anti-TNF (n=122) |
oMOA (n=54) |
anti-TNF (n=36) |
oMOA (n=62) |
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Discontinued, n (%) |
176 (100) |
87 (71.3) |
21 (38.9) |
21 (58.3) |
22 (35.5) |
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Reason, n (%)* |
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Lack of initial efficacy |
40 (22.7) |
35 (40.2) |
4 (19.0) |
10 (47.6) |
12 (54.5) |
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Failure to maintain response (disease flare) |
82 (46.6) |
27 (31.0) |
7 (33.3) |
2 (9.5) |
6 (27.3) |
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Safety/tolerance |
30 (17.0) |
18 (20.7) |
3 (14.3) |
4 (19.0) |
1 (4.5) |
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Patient doing well |
0 (0.0) |
0 (0.0) |
0 (0.0) |
0 (0.0) |
0 (0.0) |
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Patient or physician preference |
1 (0.6) |
0 (0.0) |
1 (4.8) |
0 (0.0) |
0 (0.0) |
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Cost, insurance, or formulary |
13 (7.4) |
1 (1.1) |
3 (14.3) |
1 (4.8) |
2 (9.1) |
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Other or not reported |
13 (7.4) |
7 (8.0) |
3 (14.3) |
4 (19.1) |
1 (4.5) |
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*Among those who discontinued |
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Conclusion:
The most common reasons for discontinuation of the first anti-TNF agent were efficacy related (69.3%). A numerically greater proportion of patients receiving anti-TNF as their second biologic discontinued due to lack of initial efficacy compared with those that received second biologic with other mechanism of action. In addition, safety/tolerance was a more common reason for discontinuation among those receiving anti-TNF than those receiving treatment with other mechanisms of action.
Disclosure:
E. Elkin,
Genentech Inc.,
9;
M. J. Bergman,
Genentech Inc.,
5;
T. Kamath,
Genentech Inc.,
3;
S. Ogale,
Genentech Inc.,
3;
A. Turpcu,
Genentech Inc.,
3;
K. King,
Genentech Inc.,
9;
J. Oh,
Genentech Inc.,
9;
M. Shah,
Genentech Inc.,
9;
M. I. Hamburger,
Genentech, Inc.,
5.
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