Disparity between Inter-Patient Molecular Heterogeneity and Repertoires of Target Drugs Used for Different Types of Cancer in Clinical Oncology

6533b82efe1ef96bd1292a6d

RESEARCH PRODUCT

Disparity between Inter-Patient Molecular Heterogeneity and Repertoires of Target Drugs Used for Different Types of Cancer in Clinical Oncology

Elena Poddubskaya Alf Giese Marianna Zolotovskaia Marianna Zolotovskaia Sergey A. Roumiantsev Alexey Moiseev Ella Kim Andrey Kaprin Anton Buzdin Nicolas Borisov Nicolas Borisov Victor Tkachev Andrew Garazha Maxim Sorokin Peter V. Shegay Ivan Petrov Marina Sekacheva

subject

Gene mutation Medical Oncology chemotherapy Genome Transcriptome lcsh:Chemistry Drug Delivery Systems Prostate Neoplasms tumor heterogeneity Medicine Cluster Analysis Molecular Targeted Therapy Pathology Molecular Precision Medicine lcsh:QH301-705.5 targeted therapeutics cancer drugs Spectroscopy Exome sequencing General Medicine Genomics personalized medicine Computer Science Applications Drug repositioning medicine.anatomical_structure Antineoplastic Agents Computational biology Catalysis Article Inorganic Chemistry molecular diagnostics Genetic Heterogeneity Drug Therapy Exome Sequencing Humans Physical and Theoretical Chemistry Molecular Biology genome clinical oncology business.industry Organic Chemistry Molecular diagnostics mutations lcsh:Biology (General)lcsh:QD1-999 Mutation Personalized medicine business transcriptome

description

Inter-patient molecular heterogeneity is the major declared driver of an expanding variety of anticancer drugs and personalizing their prescriptions. Here, we compared interpatient molecular heterogeneities of tumors and repertoires of drugs or their molecular targets currently in use in clinical oncology. We estimated molecular heterogeneity using genomic (whole exome sequencing) and transcriptomic (RNA sequencing) data for 4890 tumors taken from The Cancer Genome Atlas database. For thirteen major cancer types, we compared heterogeneities at the levels of mutations and gene expression with the repertoires of targeted therapeutics and their molecular targets accepted by the current guidelines in oncology. Totally, 85 drugs were investigated, collectively covering 82 individual molecular targets. For the first time, we showed that the repertoires of molecular targets of accepted drugs did not correlate with molecular heterogeneities of different cancer types. On the other hand, we found that the clinical recommendations for the available cancer drugs were strongly congruent with the gene expression but not gene mutation patterns. We detected the best match among the drugs usage recommendations and molecular patterns for the kidney, stomach, bladder, ovarian and endometrial cancers. In contrast, brain tumors, prostate and colorectal cancers showed the lowest match. These findings provide a theoretical basis for reconsidering usage of targeted therapeutics and intensifying drug repurposing efforts.

year	journal	country	edition	language
2020-02-01	International Journal of Molecular Sciences

10.3390/ijms21051580 http://dx.doi.org/10.3390/ijms21051580