TY - JOUR
T1 - Network-based matching of patients and targeted therapies for precision oncology
AU - Liu, Qingzhi
AU - Ha, Min Jin
AU - Bhattacharyya, Rupam
AU - Garmire, Lana
AU - Baladandayuthapani, Veerabhadran
N1 - Funding Information:
* This work is supported by NIH grants: R01-CA160736, R01-CA160736, R21-CA220299, P30-CA-46592, R01-LM012373, R01-HD084633, K01-ES025434 (BD2K), NSF grant DMS-1463233 and start-up funds from the UM Rogel Cancer Center and School of Public Health. † Corresponding author. Email: veerab@umich.edu © 2019 The Authors. Open Access chapter published by World Scientific Publishing Company and distributed under the terms of the Creative Commons Attribution Non-Commercial (CC BY-NC) 4.0 License.
Publisher Copyright:
© 2019 The Authors.
PY - 2020
Y1 - 2020
N2 - The extensive acquisition of high-Throughput molecular profiling data across model systems (human tumors and cancer cell lines) and drug sensitivity data, makes precision oncology possible allowing clinicians to match the right drug to the right patient. Current supervised models for drug sensitivity prediction, often use cell lines as exemplars of patient tumors and for model training. However, these models are limited in their ability to accurately predict drug sensitivity of individual cancer patients to a large set of drugs, given the paucity of patient drug sensitivity data used for testing and high variability across different drugs. To address these challenges, we developed a multilayer networkbased approach to impute individual patients' responses to a large set of drugs. This approach considers the triplet of patients, cell lines and drugs as one inter-connected holistic system. We first use the omics profiles to construct a patient-cell line network and determine best matching cell lines for patient tumors based on robust measures of network similarity. Subsequently, these results are used to impute the "missing link" between each individual patient and each drug, called Personalized Imputed Drug Sensitivity Score (PIDS-Score), which can be construed as a measure of the therapeutic potential of a drug or therapy. We applied our method to two subtypes of lung cancer patients, matched these patients with cancer cell lines derived from 19 tissue types based on their functional proteomics profiles, and computed their PIDS-Scores to 251 drugs and experimental compounds. We identified the best representative cell lines that conserve lung cancer biology and molecular targets. The PIDS-Score based top sensitive drugs for the entire patient cohort as well as individual patients are highly related to lung cancer in terms of their targets, and their PIDS-Scores are significantly associated with patient clinical outcomes. These findings provide evidence that our method is useful to narrow the scope of possible effective patient-drug matchings for implementing evidence-based personalized medicine strategies.
AB - The extensive acquisition of high-Throughput molecular profiling data across model systems (human tumors and cancer cell lines) and drug sensitivity data, makes precision oncology possible allowing clinicians to match the right drug to the right patient. Current supervised models for drug sensitivity prediction, often use cell lines as exemplars of patient tumors and for model training. However, these models are limited in their ability to accurately predict drug sensitivity of individual cancer patients to a large set of drugs, given the paucity of patient drug sensitivity data used for testing and high variability across different drugs. To address these challenges, we developed a multilayer networkbased approach to impute individual patients' responses to a large set of drugs. This approach considers the triplet of patients, cell lines and drugs as one inter-connected holistic system. We first use the omics profiles to construct a patient-cell line network and determine best matching cell lines for patient tumors based on robust measures of network similarity. Subsequently, these results are used to impute the "missing link" between each individual patient and each drug, called Personalized Imputed Drug Sensitivity Score (PIDS-Score), which can be construed as a measure of the therapeutic potential of a drug or therapy. We applied our method to two subtypes of lung cancer patients, matched these patients with cancer cell lines derived from 19 tissue types based on their functional proteomics profiles, and computed their PIDS-Scores to 251 drugs and experimental compounds. We identified the best representative cell lines that conserve lung cancer biology and molecular targets. The PIDS-Score based top sensitive drugs for the entire patient cohort as well as individual patients are highly related to lung cancer in terms of their targets, and their PIDS-Scores are significantly associated with patient clinical outcomes. These findings provide evidence that our method is useful to narrow the scope of possible effective patient-drug matchings for implementing evidence-based personalized medicine strategies.
KW - Drug response prediction
KW - Functional proteomics
KW - Network analysis
KW - Precision oncology
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M3 - Conference article
C2 - 31797633
AN - SCOPUS:85076052151
SN - 2335-6928
VL - 25
SP - 623
EP - 634
JO - Pacific Symposium on Biocomputing
JF - Pacific Symposium on Biocomputing
IS - 2020
T2 - 25th Pacific Symposium on Biocomputing, PSB 2020
Y2 - 3 January 2020 through 7 January 2020
ER -