Abstract 640P
Background
Single-arm phase 1/2 trials test new cancer drugs’ safety and establish first evidence of tumor response. The tumor response rate (RR) is measured as radiologic tumor shrinkage by -30% in size (solid cancers) or hematologic regression (hematologic cancers). For promising drugs with substantial RRs in early single-arm trials, the US Food and Drug Administration (FDA) may grant patients fast access using expedited approval. With one-third of drugs approved based on phase 1/2 trials, we meta-analyzed tumor response in single-arm trials for cancer drugs.
Methods
We identified 79 cancer drugs with 163 indications (86 hematologic, 77 solid) approved by the FDA based on single-arm trials (2000-2022). Data were collected from Drugs@FDA, clinicaltrials.gov, and associated peer-reviewed publications. The primary outcomes of interest collected for each trial were the tumor-specific RR and duration of response. RRs were measured by RECIST for solid cancers and by multiple established measures for hematologic cancers. RRs were meta-analyzed with random-effect models.
Results
The mean RR was 46.8% (95%CI 43.1-50.6, p<0.001) with a median response duration of 10.7 months). RRs were higher for hematologic than solid cancers (53.4% vs. 40.3%, p<0.001). Particularly high RRs were observed for thyroid cancer (71.5%), CML (70.2%), and Hodgkin lymphoma (69.9%), whilst lowest RRs were for cervical cancer (18.9%), HNSCC (16.1%), and esophageal/gastric cancer (13.6%). Among solid tumors, greater RRs were measured for targeted agents (48.40%), biomarkers (47.3%), first-line treatments (53.4%), orphan diseases (46.5%), and breakthrough therapy designations (47.3%). Results were consistent for hematologic cancers.
Conclusions
Tumor response rates in pivotal single-arm trials appear substantial – nearly half of the patients (46.8%) receiving a new cancer drug show a positive response for ca. 11 months. These data inform patients and physicians on new drugs’ expected benefits and represent a benchmark for future development efforts. However, drugs showing promising RRs must undergo validation in large, confirmatory randomized-controlled trials to demonstrate an improvement in patient survival.
Clinical trial identification
Editorial acknowledgement
Legal entity responsible for the study
The authors.
Funding
Has not received any funding.
Disclosure
All authors have declared no conflicts of interest.
Resources from the same session
723P - A phase II study of cadonilimab plus chemotherapy in persistent recurrent/ metastatic cervical cancer patients who failed previous immuno/chemotherapy
Presenter: Li Xiaoling Li
Session: Poster session 01
724P - Preliminary outcomes from a phase Ib/II study of the highly potent PI3K-mTOR dual inhibitor WX390 combined with toripalimab in patients with advanced cervical cancer
Presenter: Guiling Li
Session: Poster session 01
725P - Treatment of patients with metastatic or relapsed cervical cancer: Results from a quality assurance program of the AGO Study Group
Presenter: Dominik Denschlag
Session: Poster session 01
726P - Efficacy and safety of pembrolizumab plus olaparib combination therapy in recurrent cervical cancer progressed on platinum-based chemotherapy: Results from the phase II trial of GOTIC-025
Presenter: Kosei Hasegawa
Session: Poster session 01
727P - Real-world efficacy and safety of cadonilimab in recurrent or metastatic cervical cancer: A multicenter retrospective analysis in China
Presenter: Yang Sun
Session: Poster session 01
Resources:
Abstract
728P - Chemotherapy plus tislelizumab in young patients with cervical cancer preserve fertility: A phase II study
Presenter: Danbo Wang
Session: Poster session 01
729P - Patterns of survivorship care of cervical cancer patients with or without HIV infection in Botswana 2015-2022
Presenter: Sheldon Amoo-Mitchual
Session: Poster session 01
730P - Validation of circulating tumor DNA for prognostication and monitoring in metastatic endometrial carcinoma: Ancillary results from the phase II randomized GINECO trial UTOLA
Presenter: Guillaume Beinse
Session: Poster session 01
731P - Post-progression survival outcomes in patients (pts) with primary advanced or recurrent endometrial cancer (pA/rEC) in the ENGOT-EN6-NSGO/GOG-3031/RUBY trial who received follow-up immunotherapy
Presenter: Mansoor Raza Mirza
Session: Poster session 01
732P - Durvalumab + carboplatin/paclitaxel (CP) followed by durvalumab ± olaparib as a first-line treatment for endometrial cancer (EC): Progression-free survival (PFS) by clinical factors in DUO-E
Presenter: Stephanie Blank
Session: Poster session 01