Off-target toxicity is a common mechanism of action of cancer drugs undergoing clinical trials
Cold Spring Harbor Laboratory · Stony Brook University · +3 more institutions
Abstract
Ninety-seven percent of drug-indication pairs that are tested in clinical trials in oncology never advance to receive U.S. Food and Drug Administration approval. While lack of efficacy and dose-limiting toxicities are the most common causes of trial failure, the reason(s) why so many new drugs encounter these problems is not well understood. Using CRISPR-Cas9 mutagenesis, we investigated a set of cancer drugs and drug targets in various stages of clinical testing. We show that-contrary to previous reports obtained predominantly with RNA interference and small-molecule inhibitors-the proteins ostensibly targeted by these drugs are nonessential for cancer cell proliferation. Moreover, the efficacy of each drug…
Citation impact
- FWCI
- 28.79
- Percentile
- 100%
- References
- 258
Authors
13- ALAnn LinCorresponding
Cold Spring Harbor Laboratory, Stony Brook University
- CJChristopher J. GiulianoCorresponding
Cold Spring Harbor Laboratory, Stony Brook University
- APAnn Palladino
Cold Spring Harbor Laboratory
- KMKristen M. John
Hofstra University, Cold Spring Harbor Laboratory
- CAConnor Abramowicz
Cold Spring Harbor Laboratory, New York Institute of Technology
Topics & keywords
- Clinical trial
- Toxicity
- Drug
- Biology
- Cancer drugs
- Drug toxicity
- Mechanism of action
- Pharmacology
- Good health and well-being