CT-P17 Adalimumab Biosimilar in Patients with Moderate-to-Severe Chronic Plaque Psoriasis: An Open-Label Extension of a Phase 3 Interchangeability Study

Introduction A 27-week analysis of this phase 3 study demonstrated the interchangeability of the adalimumab biosimilar CT-P17 and reference adalimumab. The current 52-week analysis reports secondary data from the open-label extension period (OLE) of the study. Methods In this randomized, double-blin...

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Published in	Dermatology and therapy Vol. 15; no. 5; pp. 1079 - 1092
Main Authors	Pariser, David M., Lebwohl, Mark G., Jaworski, Janusz, Trefler, Jakub, Daniluk, Stefan, Dudek, Anna, Baran, Wojciech, Owczarek, Witold, Brzewski, Pawel, Sikora, Mariusz, Krogulec, Marek, Kim, SungHyun, Suh, JeeHye, Choi, EunJin, Cha, JungBin, Lee, HyunJin, Lee, SungJeong, Koo, John Y.
Format	Journal Article
Language	English
Published	Cheshire Springer Healthcare 01.05.2025 Springer Springer Nature B.V Adis, Springer Healthcare
Subjects	Adalimumab Biological products Biosimilar CT-P17 Dermatology Drug therapy Interchangeability Internal Medicine Medicine Medicine & Public Health Oral and Maxillofacial Surgery Original Research Pharmacokinetics Plastic Surgery Psoriasis Quality of Life Research Switching Testing Poland CT-P17 Psoriasis Tumor necrosis factor inhibitor Yuflyma Adalimumab Interchangeability TNF Biosimilar Switching
Online Access	Get full text
ISSN	2193-8210 2190-9172
DOI	10.1007/s13555-025-01383-5

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Abstract	Introduction A 27-week analysis of this phase 3 study demonstrated the interchangeability of the adalimumab biosimilar CT-P17 and reference adalimumab. The current 52-week analysis reports secondary data from the open-label extension period (OLE) of the study. Methods In this randomized, double-blind, active-controlled phase 3 study, adults with moderate-to-severe chronic plaque psoriasis received (via prefilled syringe) 80 mg subcutaneous reference adalimumab on day 1, then 40 mg 1 week later, and every other week (EOW) until week 11. At week 13, patients were randomized (1:1) to continue reference adalimumab (“continuous” group) or undergo repeated switching between CT-P17 and reference adalimumab (“switching” group) until week 25. Thereafter, patients entered an OLE and received 40 mg CT-P17 EOW from week 27 to 49, with an end-of-study visit at week 52. Here we present findings from the OLE. Pharmacokinetics (PK), efficacy (including mean percent improvement from baseline in Psoriasis Area Severity Index [PASI] score), safety, and immunogenicity were evaluated. Post hoc subgroup analyses were also conducted. Results Of 327 patients who initiated the OLE, 152 and 160 patients from the switching group and continuous group, respectively, completed the study. Mean serum concentrations were similar between groups throughout the OLE. Efficacy improvements observed up to week 27 were maintained during the OLE and were comparable between groups. At week 52, overall mean (standard deviation [SD]) improvement from baseline in PASI score was 90.34% (16.59). Safety profiles were similar between groups, and immunogenicity did not increase during the OLE. The mean (SD) percent improvement from baseline in PASI score was slightly lower in patients who were antidrug antibody (ADA)-positive versus those who were ADA-negative (89.57 [17.27] versus 97.29 [4.08]) at week 52. Conclusions PK, efficacy, safety, and immunogenicity findings remained consistent throughout the OLE, regardless of prior treatment, and were generally comparable across timepoints. Trial registration ClinicalTrials.gov: NCT05495568. Plain Language Summary A biosimilar is a medicine made using living cells that is highly similar to an original (“reference”) medicine. As biosimilars are typically cheaper than reference medicines, their use may make it easier for patients to get treatment. CT-P17, approved to treat inflammatory conditions, is a biosimilar of a reference medicine called adalimumab. CT-P17 is highly concentrated (40 mg/0.4 mL) and does not contain citrate, which may reduce pain at the injection site. This study is important because it aimed to demonstrate that patients with psoriasis could switch between CT-P17 and reference adalimumab safely and without losing effectiveness and secure status known as “interchangeability”. This would allow pharmacists to dispense CT-P17 directly when reference adalimumab is initially prescribed, providing flexibility, timely treatment access, and potentially reducing patient costs. In this study, patients with psoriasis were switched between CT-P17 and adalimumab multiple times (switching period). Results showed that CT-P17 can be used interchangeably with reference adalimumab by demonstrating similar pharmacokinetics (how the body absorbs, processes, and excretes a drug), effectiveness, safety, and immunogenicity (risk of unwanted immune reactions) between patients who switched medicines and those receiving reference adalimumab throughout. These results have been previously published. This article reports results from the last part of the study, which followed the switching period. In this part, all patients received CT-P17 every other week. Pharmacokinetics, effectiveness, safety, and immunogenicity findings remained similar to those observed during the switching period. These results provide further support for the interchangeability of CT-P17 and reference adalimumab.
AbstractList	A 27-week analysis of this phase 3 study demonstrated the interchangeability of the adalimumab biosimilar CT-P17 and reference adalimumab. The current 52-week analysis reports secondary data from the open-label extension period (OLE) of the study. In this randomized, double-blind, active-controlled phase 3 study, adults with moderate-to-severe chronic plaque psoriasis received (via prefilled syringe) 80 mg subcutaneous reference adalimumab on day 1, then 40 mg 1 week later, and every other week (EOW) until week 11. At week 13, patients were randomized (1:1) to continue reference adalimumab ("continuous" group) or undergo repeated switching between CT-P17 and reference adalimumab ("switching" group) until week 25. Thereafter, patients entered an OLE and received 40 mg CT-P17 EOW from week 27 to 49, with an end-of-study visit at week 52. Here we present findings from the OLE. Pharmacokinetics (PK), efficacy (including mean percent improvement from baseline in Psoriasis Area Severity Index [PASI] score), safety, and immunogenicity were evaluated. Post hoc subgroup analyses were also conducted. Of 327 patients who initiated the OLE, 152 and 160 patients from the switching group and continuous group, respectively, completed the study. Mean serum concentrations were similar between groups throughout the OLE. Efficacy improvements observed up to week 27 were maintained during the OLE and were comparable between groups. At week 52, overall mean (standard deviation [SD]) improvement from baseline in PASI score was 90.34% (16.59). Safety profiles were similar between groups, and immunogenicity did not increase during the OLE. The mean (SD) percent improvement from baseline in PASI score was slightly lower in patients who were antidrug antibody (ADA)-positive versus those who were ADA-negative (89.57 [17.27] versus 97.29 [4.08]) at week 52. PK, efficacy, safety, and immunogenicity findings remained consistent throughout the OLE, regardless of prior treatment, and were generally comparable across timepoints. ClinicalTrials.gov: NCT05495568. Introduction A 27-week analysis of this phase 3 study demonstrated the interchangeability of the adalimumab biosimilar CT-P17 and reference adalimumab. The current 52-week analysis reports secondary data from the open-label extension period (OLE) of the study. Methods In this randomized, double-blind, active-controlled phase 3 study, adults with moderate-to-severe chronic plaque psoriasis received (via prefilled syringe) 80 mg subcutaneous reference adalimumab on day 1, then 40 mg 1 week later, and every other week (EOW) until week 11. At week 13, patients were randomized (1:1) to continue reference adalimumab (“continuous” group) or undergo repeated switching between CT-P17 and reference adalimumab (“switching” group) until week 25. Thereafter, patients entered an OLE and received 40 mg CT-P17 EOW from week 27 to 49, with an end-of-study visit at week 52. Here we present findings from the OLE. Pharmacokinetics (PK), efficacy (including mean percent improvement from baseline in Psoriasis Area Severity Index [PASI] score), safety, and immunogenicity were evaluated. Post hoc subgroup analyses were also conducted. Results Of 327 patients who initiated the OLE, 152 and 160 patients from the switching group and continuous group, respectively, completed the study. Mean serum concentrations were similar between groups throughout the OLE. Efficacy improvements observed up to week 27 were maintained during the OLE and were comparable between groups. At week 52, overall mean (standard deviation [SD]) improvement from baseline in PASI score was 90.34% (16.59). Safety profiles were similar between groups, and immunogenicity did not increase during the OLE. The mean (SD) percent improvement from baseline in PASI score was slightly lower in patients who were antidrug antibody (ADA)-positive versus those who were ADA-negative (89.57 [17.27] versus 97.29 [4.08]) at week 52. Conclusions PK, efficacy, safety, and immunogenicity findings remained consistent throughout the OLE, regardless of prior treatment, and were generally comparable across timepoints. Trial registration ClinicalTrials.gov: NCT05495568. Plain Language Summary A biosimilar is a medicine made using living cells that is highly similar to an original (“reference”) medicine. As biosimilars are typically cheaper than reference medicines, their use may make it easier for patients to get treatment. CT-P17, approved to treat inflammatory conditions, is a biosimilar of a reference medicine called adalimumab. CT-P17 is highly concentrated (40 mg/0.4 mL) and does not contain citrate, which may reduce pain at the injection site. This study is important because it aimed to demonstrate that patients with psoriasis could switch between CT-P17 and reference adalimumab safely and without losing effectiveness and secure status known as “interchangeability”. This would allow pharmacists to dispense CT-P17 directly when reference adalimumab is initially prescribed, providing flexibility, timely treatment access, and potentially reducing patient costs. In this study, patients with psoriasis were switched between CT-P17 and adalimumab multiple times (switching period). Results showed that CT-P17 can be used interchangeably with reference adalimumab by demonstrating similar pharmacokinetics (how the body absorbs, processes, and excretes a drug), effectiveness, safety, and immunogenicity (risk of unwanted immune reactions) between patients who switched medicines and those receiving reference adalimumab throughout. These results have been previously published. This article reports results from the last part of the study, which followed the switching period. In this part, all patients received CT-P17 every other week. Pharmacokinetics, effectiveness, safety, and immunogenicity findings remained similar to those observed during the switching period. These results provide further support for the interchangeability of CT-P17 and reference adalimumab. Abstract Introduction A 27-week analysis of this phase 3 study demonstrated the interchangeability of the adalimumab biosimilar CT-P17 and reference adalimumab. The current 52-week analysis reports secondary data from the open-label extension period (OLE) of the study. Methods In this randomized, double-blind, active-controlled phase 3 study, adults with moderate-to-severe chronic plaque psoriasis received (via prefilled syringe) 80 mg subcutaneous reference adalimumab on day 1, then 40 mg 1 week later, and every other week (EOW) until week 11. At week 13, patients were randomized (1:1) to continue reference adalimumab (“continuous” group) or undergo repeated switching between CT-P17 and reference adalimumab (“switching” group) until week 25. Thereafter, patients entered an OLE and received 40 mg CT-P17 EOW from week 27 to 49, with an end-of-study visit at week 52. Here we present findings from the OLE. Pharmacokinetics (PK), efficacy (including mean percent improvement from baseline in Psoriasis Area Severity Index [PASI] score), safety, and immunogenicity were evaluated. Post hoc subgroup analyses were also conducted. Results Of 327 patients who initiated the OLE, 152 and 160 patients from the switching group and continuous group, respectively, completed the study. Mean serum concentrations were similar between groups throughout the OLE. Efficacy improvements observed up to week 27 were maintained during the OLE and were comparable between groups. At week 52, overall mean (standard deviation [SD]) improvement from baseline in PASI score was 90.34% (16.59). Safety profiles were similar between groups, and immunogenicity did not increase during the OLE. The mean (SD) percent improvement from baseline in PASI score was slightly lower in patients who were antidrug antibody (ADA)-positive versus those who were ADA-negative (89.57 [17.27] versus 97.29 [4.08]) at week 52. Conclusions PK, efficacy, safety, and immunogenicity findings remained consistent throughout the OLE, regardless of prior treatment, and were generally comparable across timepoints. Trial registration ClinicalTrials.gov: NCT05495568. A biosimilar is a medicine made using living cells that is highly similar to an original (“reference”) medicine. As biosimilars are typically cheaper than reference medicines, their use may make it easier for patients to get treatment. CT-P17, approved to treat inflammatory conditions, is a biosimilar of a reference medicine called adalimumab. CT-P17 is highly concentrated (40 mg/0.4 mL) and does not contain citrate, which may reduce pain at the injection site. This study is important because it aimed to demonstrate that patients with psoriasis could switch between CT-P17 and reference adalimumab safely and without losing effectiveness and secure status known as “interchangeability”. This would allow pharmacists to dispense CT-P17 directly when reference adalimumab is initially prescribed, providing flexibility, timely treatment access, and potentially reducing patient costs. In this study, patients with psoriasis were switched between CT-P17 and adalimumab multiple times (switching period). Results showed that CT-P17 can be used interchangeably with reference adalimumab by demonstrating similar pharmacokinetics (how the body absorbs, processes, and excretes a drug), effectiveness, safety, and immunogenicity (risk of unwanted immune reactions) between patients who switched medicines and those receiving reference adalimumab throughout. These results have been previously published. This article reports results from the last part of the study, which followed the switching period. In this part, all patients received CT-P17 every other week. Pharmacokinetics, effectiveness, safety, and immunogenicity findings remained similar to those observed during the switching period. These results provide further support for the interchangeability of CT-P17 and reference adalimumab. Introduction A 27-week analysis of this phase 3 study demonstrated the interchangeability of the adalimumab biosimilar CT-P17 and reference adalimumab. The current 52-week analysis reports secondary data from the open-label extension period (OLE) of the study. Methods In this randomized, double-blind, active-controlled phase 3 study, adults with moderate-to-severe chronic plaque psoriasis received (via prefilled syringe) 80 mg subcutaneous reference adalimumab on day 1, then 40 mg 1 week later, and every other week (EOW) until week 11. At week 13, patients were randomized (1:1) to continue reference adalimumab ("continuous" group) or undergo repeated switching between CT-P17 and reference adalimumab ("switching" group) until week 25. Thereafter, patients entered an OLE and received 40 mg CT-P17 EOW from week 27 to 49, with an end-of-study visit at week 52. Here we present findings from the OLE. Pharmacokinetics (PK), efficacy (including mean percent improvement from baseline in Psoriasis Area Severity Index [PASI] score), safety, and immunogenicity were evaluated. Post hoc subgroup analyses were also conducted. Results Of 327 patients who initiated the OLE, 152 and 160 patients from the switching group and continuous group, respectively, completed the study. Mean serum concentrations were similar between groups throughout the OLE. Efficacy improvements observed up to week 27 were maintained during the OLE and were comparable between groups. At week 52, overall mean (standard deviation [SD]) improvement from baseline in PASI score was 90.34% (16.59). Safety profiles were similar between groups, and immunogenicity did not increase during the OLE. The mean (SD) percent improvement from baseline in PASI score was slightly lower in patients who were antidrug antibody (ADA)-positive versus those who were ADA-negative (89.57 [17.27] versus 97.29 [4.08]) at week 52. Conclusions PK, efficacy, safety, and immunogenicity findings remained consistent throughout the OLE, regardless of prior treatment, and were generally comparable across timepoints. Trial registration ClinicalTrials.gov: NCT05495568. A 27-week analysis of this phase 3 study demonstrated the interchangeability of the adalimumab biosimilar CT-P17 and reference adalimumab. The current 52-week analysis reports secondary data from the open-label extension period (OLE) of the study. In this randomized, double-blind, active-controlled phase 3 study, adults with moderate-to-severe chronic plaque psoriasis received (via prefilled syringe) 80 mg subcutaneous reference adalimumab on day 1, then 40 mg 1 week later, and every other week (EOW) until week 11. At week 13, patients were randomized (1:1) to continue reference adalimumab ("continuous" group) or undergo repeated switching between CT-P17 and reference adalimumab ("switching" group) until week 25. Thereafter, patients entered an OLE and received 40 mg CT-P17 EOW from week 27 to 49, with an end-of-study visit at week 52. Here we present findings from the OLE. Pharmacokinetics (PK), efficacy (including mean percent improvement from baseline in Psoriasis Area Severity Index [PASI] score), safety, and immunogenicity were evaluated. Post hoc subgroup analyses were also conducted. Of 327 patients who initiated the OLE, 152 and 160 patients from the switching group and continuous group, respectively, completed the study. Mean serum concentrations were similar between groups throughout the OLE. Efficacy improvements observed up to week 27 were maintained during the OLE and were comparable between groups. At week 52, overall mean (standard deviation [SD]) improvement from baseline in PASI score was 90.34% (16.59). Safety profiles were similar between groups, and immunogenicity did not increase during the OLE. The mean (SD) percent improvement from baseline in PASI score was slightly lower in patients who were antidrug antibody (ADA)-positive versus those who were ADA-negative (89.57 [17.27] versus 97.29 [4.08]) at week 52. PK, efficacy, safety, and immunogenicity findings remained consistent throughout the OLE, regardless of prior treatment, and were generally comparable across timepoints. IntroductionA 27-week analysis of this phase 3 study demonstrated the interchangeability of the adalimumab biosimilar CT-P17 and reference adalimumab. The current 52-week analysis reports secondary data from the open-label extension period (OLE) of the study.MethodsIn this randomized, double-blind, active-controlled phase 3 study, adults with moderate-to-severe chronic plaque psoriasis received (via prefilled syringe) 80 mg subcutaneous reference adalimumab on day 1, then 40 mg 1 week later, and every other week (EOW) until week 11. At week 13, patients were randomized (1:1) to continue reference adalimumab (“continuous” group) or undergo repeated switching between CT-P17 and reference adalimumab (“switching” group) until week 25. Thereafter, patients entered an OLE and received 40 mg CT-P17 EOW from week 27 to 49, with an end-of-study visit at week 52. Here we present findings from the OLE. Pharmacokinetics (PK), efficacy (including mean percent improvement from baseline in Psoriasis Area Severity Index [PASI] score), safety, and immunogenicity were evaluated. Post hoc subgroup analyses were also conducted.ResultsOf 327 patients who initiated the OLE, 152 and 160 patients from the switching group and continuous group, respectively, completed the study. Mean serum concentrations were similar between groups throughout the OLE. Efficacy improvements observed up to week 27 were maintained during the OLE and were comparable between groups. At week 52, overall mean (standard deviation [SD]) improvement from baseline in PASI score was 90.34% (16.59). Safety profiles were similar between groups, and immunogenicity did not increase during the OLE. The mean (SD) percent improvement from baseline in PASI score was slightly lower in patients who were antidrug antibody (ADA)-positive versus those who were ADA-negative (89.57 [17.27] versus 97.29 [4.08]) at week 52.ConclusionsPK, efficacy, safety, and immunogenicity findings remained consistent throughout the OLE, regardless of prior treatment, and were generally comparable across timepoints.Trial registrationClinicalTrials.gov: NCT05495568.Plain Language SummaryA biosimilar is a medicine made using living cells that is highly similar to an original (“reference”) medicine. As biosimilars are typically cheaper than reference medicines, their use may make it easier for patients to get treatment. CT-P17, approved to treat inflammatory conditions, is a biosimilar of a reference medicine called adalimumab. CT-P17 is highly concentrated (40 mg/0.4 mL) and does not contain citrate, which may reduce pain at the injection site. This study is important because it aimed to demonstrate that patients with psoriasis could switch between CT-P17 and reference adalimumab safely and without losing effectiveness and secure status known as “interchangeability”. This would allow pharmacists to dispense CT-P17 directly when reference adalimumab is initially prescribed, providing flexibility, timely treatment access, and potentially reducing patient costs. In this study, patients with psoriasis were switched between CT-P17 and adalimumab multiple times (switching period). Results showed that CT-P17 can be used interchangeably with reference adalimumab by demonstrating similar pharmacokinetics (how the body absorbs, processes, and excretes a drug), effectiveness, safety, and immunogenicity (risk of unwanted immune reactions) between patients who switched medicines and those receiving reference adalimumab throughout. These results have been previously published. This article reports results from the last part of the study, which followed the switching period. In this part, all patients received CT-P17 every other week. Pharmacokinetics, effectiveness, safety, and immunogenicity findings remained similar to those observed during the switching period. These results provide further support for the interchangeability of CT-P17 and reference adalimumab. A 27-week analysis of this phase 3 study demonstrated the interchangeability of the adalimumab biosimilar CT-P17 and reference adalimumab. The current 52-week analysis reports secondary data from the open-label extension period (OLE) of the study.INTRODUCTIONA 27-week analysis of this phase 3 study demonstrated the interchangeability of the adalimumab biosimilar CT-P17 and reference adalimumab. The current 52-week analysis reports secondary data from the open-label extension period (OLE) of the study.In this randomized, double-blind, active-controlled phase 3 study, adults with moderate-to-severe chronic plaque psoriasis received (via prefilled syringe) 80 mg subcutaneous reference adalimumab on day 1, then 40 mg 1 week later, and every other week (EOW) until week 11. At week 13, patients were randomized (1:1) to continue reference adalimumab ("continuous" group) or undergo repeated switching between CT-P17 and reference adalimumab ("switching" group) until week 25. Thereafter, patients entered an OLE and received 40 mg CT-P17 EOW from week 27 to 49, with an end-of-study visit at week 52. Here we present findings from the OLE. Pharmacokinetics (PK), efficacy (including mean percent improvement from baseline in Psoriasis Area Severity Index [PASI] score), safety, and immunogenicity were evaluated. Post hoc subgroup analyses were also conducted.METHODSIn this randomized, double-blind, active-controlled phase 3 study, adults with moderate-to-severe chronic plaque psoriasis received (via prefilled syringe) 80 mg subcutaneous reference adalimumab on day 1, then 40 mg 1 week later, and every other week (EOW) until week 11. At week 13, patients were randomized (1:1) to continue reference adalimumab ("continuous" group) or undergo repeated switching between CT-P17 and reference adalimumab ("switching" group) until week 25. Thereafter, patients entered an OLE and received 40 mg CT-P17 EOW from week 27 to 49, with an end-of-study visit at week 52. Here we present findings from the OLE. Pharmacokinetics (PK), efficacy (including mean percent improvement from baseline in Psoriasis Area Severity Index [PASI] score), safety, and immunogenicity were evaluated. Post hoc subgroup analyses were also conducted.Of 327 patients who initiated the OLE, 152 and 160 patients from the switching group and continuous group, respectively, completed the study. Mean serum concentrations were similar between groups throughout the OLE. Efficacy improvements observed up to week 27 were maintained during the OLE and were comparable between groups. At week 52, overall mean (standard deviation [SD]) improvement from baseline in PASI score was 90.34% (16.59). Safety profiles were similar between groups, and immunogenicity did not increase during the OLE. The mean (SD) percent improvement from baseline in PASI score was slightly lower in patients who were antidrug antibody (ADA)-positive versus those who were ADA-negative (89.57 [17.27] versus 97.29 [4.08]) at week 52.RESULTSOf 327 patients who initiated the OLE, 152 and 160 patients from the switching group and continuous group, respectively, completed the study. Mean serum concentrations were similar between groups throughout the OLE. Efficacy improvements observed up to week 27 were maintained during the OLE and were comparable between groups. At week 52, overall mean (standard deviation [SD]) improvement from baseline in PASI score was 90.34% (16.59). Safety profiles were similar between groups, and immunogenicity did not increase during the OLE. The mean (SD) percent improvement from baseline in PASI score was slightly lower in patients who were antidrug antibody (ADA)-positive versus those who were ADA-negative (89.57 [17.27] versus 97.29 [4.08]) at week 52.PK, efficacy, safety, and immunogenicity findings remained consistent throughout the OLE, regardless of prior treatment, and were generally comparable across timepoints.CONCLUSIONSPK, efficacy, safety, and immunogenicity findings remained consistent throughout the OLE, regardless of prior treatment, and were generally comparable across timepoints.ClinicalTrials.gov: NCT05495568.TRIAL REGISTRATIONClinicalTrials.gov: NCT05495568.
Audience	Academic
Author	Kim, SungHyun Sikora, Mariusz Pariser, David M. Brzewski, Pawel Cha, JungBin Suh, JeeHye Choi, EunJin Owczarek, Witold Trefler, Jakub Baran, Wojciech Koo, John Y. Jaworski, Janusz Dudek, Anna Lee, SungJeong Daniluk, Stefan Lee, HyunJin Lebwohl, Mark G. Krogulec, Marek
Author_xml	– sequence: 1 givenname: David M. surname: Pariser fullname: Pariser, David M. organization: Eastern Virginia Medical School and Virginia Clinical Research, Inc – sequence: 2 givenname: Mark G. surname: Lebwohl fullname: Lebwohl, Mark G. organization: Icahn School of Medicine at Mount Sinai – sequence: 3 givenname: Janusz surname: Jaworski fullname: Jaworski, Janusz organization: Centrum Medyczne Reuma Park – sequence: 4 givenname: Jakub orcidid: 0009-0003-3912-3518 surname: Trefler fullname: Trefler, Jakub organization: Reuma Centrum – sequence: 5 givenname: Stefan surname: Daniluk fullname: Daniluk, Stefan organization: ClinicMed Daniluk, Nowak Sp.k – sequence: 6 givenname: Anna surname: Dudek fullname: Dudek, Anna organization: Centrum Medyczne AMED – sequence: 7 givenname: Wojciech surname: Baran fullname: Baran, Wojciech organization: Department of Dermatology, Venereology and Allergology, Wrocław Medical University – sequence: 8 givenname: Witold surname: Owczarek fullname: Owczarek, Witold organization: Royalderm, Department of Dermatology, Military Institute of Medicine - National Research Institute – sequence: 9 givenname: Pawel surname: Brzewski fullname: Brzewski, Pawel organization: Specjalistyczny Gabinet Dermatologiczny Aplikacyjno-Badawczy, Department of Dermatology, UAFM Kraków – sequence: 10 givenname: Mariusz orcidid: 0000-0002-6162-9916 surname: Sikora fullname: Sikora, Mariusz organization: National Institute of Geriatrics, Rheumatology and Rehabilitation – sequence: 11 givenname: Marek orcidid: 0000-0002-5698-9706 surname: Krogulec fullname: Krogulec, Marek organization: Rheumatology Clinic, NZOZ Lecznica MAK-MED – sequence: 12 givenname: SungHyun orcidid: 0000-0003-3898-0393 surname: Kim fullname: Kim, SungHyun organization: Celltrion, Inc – sequence: 13 givenname: JeeHye orcidid: 0009-0005-9273-0784 surname: Suh fullname: Suh, JeeHye organization: Celltrion, Inc – sequence: 14 givenname: EunJin surname: Choi fullname: Choi, EunJin organization: Celltrion, Inc – sequence: 15 givenname: JungBin surname: Cha fullname: Cha, JungBin organization: Celltrion, Inc – sequence: 16 givenname: HyunJin surname: Lee fullname: Lee, HyunJin organization: Celltrion, Inc – sequence: 17 givenname: SungJeong orcidid: 0000-0003-3974-7999 surname: Lee fullname: Lee, SungJeong organization: Celltrion, Inc – sequence: 18 givenname: John Y. surname: Koo fullname: Koo, John Y. email: john.Koo2@ucsf.edu organization: UCSF Psoriasis and Skin Treatment Center
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Cites_doi	10.1016/j.autrev.2024.103530 10.1007/s12325-024-03100-8 10.1186/s13075-020-02394-7 10.1093/rheumatology/keab460 10.1111/jcpt.12583 10.1002/art.22214 10.2217/imt-2022-0181 10.1111/j.1468-3083.2012.04496.x 10.1111/cts.12967 10.1038/s41584-020-00540-8 10.1001/jamadermatol.2013.8347 10.1016/j.jaad.2010.12.005
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DOI	10.1007/s13555-025-01383-5
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Keywords	CT-P17 Psoriasis Tumor necrosis factor inhibitor Yuflyma Adalimumab Interchangeability TNF Biosimilar Switching
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References	1383_CR2 J Kay (1383_CR5) 2021; 23 MG Lebwohl (1383_CR7) 2025; 42 1383_CR13 1383_CR1 1383_CR17 1383_CR14 SP Menting (1383_CR11) 2014; 150 X Sun (1383_CR12) 2024; 23 DE Furst (1383_CR6) 2022; 61 1383_CR18 K Gordon (1383_CR9) 2012; 66 V Strand (1383_CR15) 2021; 17 KS Yu (1383_CR4) 2021; 14 D Shin (1383_CR8) 2017; 42 K Bendtzen (1383_CR16) 2006; 54 M Haranaka (1383_CR3) 2023; 15 PPM van Lümig (1383_CR10) 2013; 27
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Snippet	Introduction A 27-week analysis of this phase 3 study demonstrated the interchangeability of the adalimumab biosimilar CT-P17 and reference adalimumab. The... A 27-week analysis of this phase 3 study demonstrated the interchangeability of the adalimumab biosimilar CT-P17 and reference adalimumab. The current 52-week... Introduction A 27-week analysis of this phase 3 study demonstrated the interchangeability of the adalimumab biosimilar CT-P17 and reference adalimumab. The... IntroductionA 27-week analysis of this phase 3 study demonstrated the interchangeability of the adalimumab biosimilar CT-P17 and reference adalimumab. The... A biosimilar is a medicine made using living cells that is highly similar to an original (“reference”) medicine. As biosimilars are typically cheaper than... Abstract Introduction A 27-week analysis of this phase 3 study demonstrated the interchangeability of the adalimumab biosimilar CT-P17 and reference...
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SubjectTerms	Adalimumab Biological products Biosimilar CT-P17 Dermatology Drug therapy Interchangeability Internal Medicine Medicine Medicine & Public Health Oral and Maxillofacial Surgery Original Research Pharmacokinetics Plastic Surgery Psoriasis Quality of Life Research Switching Testing
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Title	CT-P17 Adalimumab Biosimilar in Patients with Moderate-to-Severe Chronic Plaque Psoriasis: An Open-Label Extension of a Phase 3 Interchangeability Study
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