With the advent of targeted agents and immunological therapies, the medical research community has become increasingly aware that conventional methods for determining the best dose or schedule of a new agent are inadequate. It has been well established that conventional phase I designs cannot reliably identify safe and effective doses. This problem applies, generally, for cytotoxic agents, radiation therapy, targeted agents, and immunotherapies. To address this, the US Food and Drug Administration’s Oncology Center of Excellence initiated Project Optimus, with the goal “to reform the dose optimization and dose selection paradigm in oncology drug development.” As a response to Project Optimus, the articles in this special issue of Clinical Trials review recent advances in methods for choosing the dose or schedule of a new agent with an overall objective of informing clinical trialists of these innovative designs. This introductory article briefly reviews problems with conventional methods, the regulatory changes that encourage better dose optimization designs, and provides brief summaries of the articles that follow in this special issue.
BuchdungerEMatterADrukerBJ. Bcr-Abl inhibition as a modality of CML therapeutics. Biochim Biophys Acta2001; 1551(1): M11–M18.
2.
DrukerBJO’BrienSGCortesJ, et al. Chronic myelogenous leukemia. Hematology Am Soc Hematol Educ Program2002; 2002: 111–135.
3.
LiuEMarinDBanerjeeP, et al. Use of CAR-transduced natural killer cells in CD19-positive lymphoid tumors. N Engl J Med2020; 382(6): 545–553.
4.
GladstoneDED’AlessioFHowardC, et al. Randomized, double-blinded, placebo-controlled trial of allogeneic cord blood T-regulatory cells for treatment of COVID-19 ARDS. Blood Adv2023; 7(13): 3075–3079.
5.
DicklerMNBarryWTCirrincioneCT, et al. Phase III trial evaluating letrozole as first-line endocrine therapy with or without bevacizumab for the treatment of postmenopausal women with hormone receptor-positive advanced-stage breast cancer: CALGB 40503 (Alliance). J Clin Oncol2016; 34(22): 2602–2609.
6.
MsaouelPGoswamiSThallPF, et al. A phase 1-2 trial of sitravatinib and nivolumab in clear cell renal cell carcinoma following progression on antiangiogenic therapy. Sci Transl Med2022; 14(641): eabm6420.
7.
ClarkeNWArmstrongAThiery-VuilleminA, et al. Abiraterone and olaparib for metastatic castration-resistant prostate cancer. NEJM Evid2022; 1(9): EVIDoa2200043.
8.
SartorOde BonoJChiKN, et al. Lutetium-177-PSMA-617 for metastatic castration-resistant prostate cancer. N Engl J Med2021; 385(12): 1091–1103.
9.
Le TourneauCLeeJJSiuLL. Dose escalation methods in phase I cancer clinical trials. J Natl Cancer Inst2009; 101(10): 708–720.
10.
O’QuigleyJPepeMFisherL. Continual reassessment method: a practical design for phase 1 clinical trials in cancer. Biometrics1990; 46(1): 33–48.
11.
CheungYK. Dose finding by the continual reassessment method. Boca Raton, Fl: Taylor & Francis, 2011.
12.
RogatkoASchoeneckDJonasW, et al. Translation of innovative designs into phase I trials. J Clin Oncol2007; 25(31): 4982–4986.
13.
Fourie ZirkelbachJShahMVallejoJ, et al. Improving dose-optimization processes used in oncology drug development to minimize toxicity and maximize benefit to patients. J Clin Oncol2022; 40(30): 3489–3500.
14.
YanFThallPFLuKH, et al. Phase I-II clinical trial design: a state-of-the-art paradigm for dose finding. Ann Oncol2018; 29(3): 694–699.
15.
ShahMRahmanATheoretMR, et al. The drug—dosing conundrum in oncology—when less is more. N Engl J Med2021; 385(16): 1445–1447.
16.
AlatrashGSaberianCBassettR, et al. Vorinostat combined with busulfan, fludarabine, and clofarabine conditioning regimen for allogeneic hematopoietic stem cell transplantation in patients with acute leukemia: long-term study outcomes. Transplant Cell Ther2022; 28(8): 501e1–501.
17.
ThallPFZangYChappleAG, et al. Novel clinical trial designs with dose optimization to improve long-term outcomes. Clin Cancer Res2023; 29(22): 4549–4554.
18.
RiveraDRHenkHJGarrett-MayerE, et al. The friends of cancer research real-world data collaboration pilot 2.0: methodological recommendations from oncology case studies. Clin Pharmacol Ther2022; 111(1): 283–292.
19.
YuanYHessKRHilsenbeckSG, et al. Bayesian optimal interval design: a simple and well-performing design for phase I oncology trials. Clin Cancer Res2016; 22(17): 4291–4301.
20.
AnanthakrishnanRLinRHeC, et al. An overview of the BOIN design and its current extensions for novel early-phase oncology trials. Contemp Clin Trials Commun2022; 28: 100943.
21.
CheungYKChappellR. Sequential designs for phase I clinical trials with late-onset toxicities. Biometrics2000; 56(4): 1177–1182.
22.
HuangBKuanPF. Time-to-event continual reassessment method incorporating treatment cycle information with application to an oncology phase I trial. Biom J2014; 56(6): 933–946.
JimenezRBSchenkelCLevitLA, et al. Oncologists’ perspectives on individualizing dose selection for patients with metastatic cancer. JCO Oncol Pract2022; 18(11): e1807–e1817.
