TY - JOUR
T1 - Clinical trials for new drug development
T2 - Optimal investment and application
AU - Kouvelis, Panos
AU - Milner, Joseph
AU - Tian, Zhili
N1 - Publisher Copyright:
© 2017 INFORMS.
PY - 2017/6/1
Y1 - 2017/6/1
N2 - Phase III clinical trials are expensive and require enrolling and treating hundreds or thousands of patients at many sites. The time and cost required to do so are uncertain, as is the economic value of the drug upon completion. We consider the problem of determining when and how many test sites should be opened and the rate at which patients should be recruited. We model the problem as a discrete time, discounted dynamic program with the objective of maximizing the expected net present value of a drug based on the costs of conducting the trial and on the drug's quality-moderated likelihood of approval and its subsequent expected revenue stream if approved.We show the optimal policy is characterized by a series of thresholds on the number of patients enrolled over time that indicate when additional test centers should be opened and how many patients should be targeted. We demonstrate using data from completed clinical trials that for low- to moderate-valued drugs, these thresholds are relevant to the firm's decisions. We extend the problem to the case with multiple interim analyses and demonstrate that optimizing the clinical trial capacity and its utilization provides significant value in addition to the option value of stopping the trial early.
AB - Phase III clinical trials are expensive and require enrolling and treating hundreds or thousands of patients at many sites. The time and cost required to do so are uncertain, as is the economic value of the drug upon completion. We consider the problem of determining when and how many test sites should be opened and the rate at which patients should be recruited. We model the problem as a discrete time, discounted dynamic program with the objective of maximizing the expected net present value of a drug based on the costs of conducting the trial and on the drug's quality-moderated likelihood of approval and its subsequent expected revenue stream if approved.We show the optimal policy is characterized by a series of thresholds on the number of patients enrolled over time that indicate when additional test centers should be opened and how many patients should be targeted. We demonstrate using data from completed clinical trials that for low- to moderate-valued drugs, these thresholds are relevant to the firm's decisions. We extend the problem to the case with multiple interim analyses and demonstrate that optimizing the clinical trial capacity and its utilization provides significant value in addition to the option value of stopping the trial early.
KW - Clinical trial
KW - Optimal investment
KW - Pharmaceutical drug development
KW - R&D project management
UR - https://www.scopus.com/pages/publications/85026303016
U2 - 10.1287/msom.2017.0616
DO - 10.1287/msom.2017.0616
M3 - Article
AN - SCOPUS:85026303016
SN - 1523-4614
VL - 19
SP - 437
EP - 452
JO - Manufacturing and Service Operations Management
JF - Manufacturing and Service Operations Management
IS - 3
ER -