TY - JOUR
T1 - Expert consensus recommendations on the use of randomized clinical trials for drug approval in psychiatry- comparing trial designs
AU - Similon, Miriam von Mücke
AU - Paasche, Cecilia
AU - Krol, Fas
AU - Lerer, Bernard
AU - Goodwin, Guy M.
AU - Berk, Michael
AU - Meyer-Lindenberg, Andreas
AU - Ketter, Terence A.
AU - Yatham, Lakshmi N.
AU - Goldberg, Joseph F.
AU - Malhi, Gin S.
AU - El-Mallakh, Rif
AU - Licht, Rasmus W.
AU - Young, Allan H.
AU - Kapczinski, Flavio
AU - Swartz, Marnina
AU - Hagin, Michal
AU - Torrent, Carla
AU - Serretti, Alessandro
AU - Yildiz, Ayşegül
AU - Martínez-Arán, Anabel
AU - Strejilevich, Sergio
AU - Rybakowski, Janusz
AU - Sani, Gabriele
AU - Grunze, Heinz
AU - Vázquez, Gustavo
AU - Pinto, Ana Gonzales
AU - Azorin, Jean Michel
AU - Nolen, Willem
AU - Sentissi, Othman
AU - López-Jaramillo, Carlos
AU - Frey, Benicio N.
AU - Nierenberg, Andrew
AU - Parker, Gordon
AU - Bond, David J.
AU - Cohen, Adam
AU - Tortorella, Alfonso
AU - Perugi, Giulio
AU - Vieta, Eduard
AU - Popovic, Dina
N1 - Publisher Copyright:
© 2022 Elsevier B.V. and ECNP
PY - 2022/7
Y1 - 2022/7
N2 - The use of randomized clinical trials, in particular placebo-controlled trials, for drug approval, is the subject of long-standing debate in the scientific community and beyond. This study offers consensus recommendations from clinical and academic experts to guide the selection of clinical trial design in psychiatry. Forty-one highly cited clinical psychiatrists and/or researchers participated in a Delphi survey. Consensus statements were developed based on the findings of a published, peer-reviewed systematic review. Participants evaluated statements in two survey rounds, following the Delphi method. The expert panel achieved consensus on 7 of 21 recommendations regarding the use of randomized clinical trials. The endorsed recommendations were: (i) Results from placebo-controlled trials are the most reliable and (ii) are necessary despite the growing placebo-effect; (iii) it is ethical to enroll patients in placebo-arms when established treatment is available, if there is no evidence of increased health risk; (iv) There is a need to approve new drugs with the same efficacy as existing treatments, but with different side-effect profiles; (v) Non-inferiority trials incur an increased risk of approving ineffective medications; (vi) The risk of approving an ineffective drug justifies trial designs that incur higher costs, and (vii) superiority trials incur the risk of rejecting potentially efficacious treatments. The endorsed recommendations inform the choice of trial-design appropriate for approval of psychopharmacological drugs. The recommendations strongly support the use of randomized clinical trials in general, and the use of placebo-controlled trials in particular.
AB - The use of randomized clinical trials, in particular placebo-controlled trials, for drug approval, is the subject of long-standing debate in the scientific community and beyond. This study offers consensus recommendations from clinical and academic experts to guide the selection of clinical trial design in psychiatry. Forty-one highly cited clinical psychiatrists and/or researchers participated in a Delphi survey. Consensus statements were developed based on the findings of a published, peer-reviewed systematic review. Participants evaluated statements in two survey rounds, following the Delphi method. The expert panel achieved consensus on 7 of 21 recommendations regarding the use of randomized clinical trials. The endorsed recommendations were: (i) Results from placebo-controlled trials are the most reliable and (ii) are necessary despite the growing placebo-effect; (iii) it is ethical to enroll patients in placebo-arms when established treatment is available, if there is no evidence of increased health risk; (iv) There is a need to approve new drugs with the same efficacy as existing treatments, but with different side-effect profiles; (v) Non-inferiority trials incur an increased risk of approving ineffective medications; (vi) The risk of approving an ineffective drug justifies trial designs that incur higher costs, and (vii) superiority trials incur the risk of rejecting potentially efficacious treatments. The endorsed recommendations inform the choice of trial-design appropriate for approval of psychopharmacological drugs. The recommendations strongly support the use of randomized clinical trials in general, and the use of placebo-controlled trials in particular.
KW - Clinical trial
KW - Delphi
KW - Placebo
KW - Trial-design
UR - http://www.scopus.com/inward/record.url?scp=85132424534&partnerID=8YFLogxK
UR - http://www.scopus.com/inward/citedby.url?scp=85132424534&partnerID=8YFLogxK
U2 - 10.1016/j.euroneuro.2022.05.002
DO - 10.1016/j.euroneuro.2022.05.002
M3 - Article
C2 - 35665655
AN - SCOPUS:85132424534
SN - 0924-977X
VL - 60
SP - 91
EP - 99
JO - European Neuropsychopharmacology
JF - European Neuropsychopharmacology
ER -