Integrating Systems Biology and an Ex Vivo Human Tumor Model Elucidates PD-1 Blockade Response Dynamics

Smalley, Munisha; Przedborski, Michelle; Thiyagarajan, Saravanan; Pellowe, Moriah; Verma, Amit; Brijwani, Nilesh; Datta, Debika; Jain, Mayank; Shanthappa, Basavaraja; Kapoor, Vidushi; Gopinath, K. S.; Doval, DC; Sabitha, K.S.; Taroncher-Oldenburg, Gaspar; Majumder, Biswanath; Majumder, Pradip K.; Kohandel, Mohammad; Goldman, Aaron

doi:10.1016/j.isci.2020.101229

Cited by 7 publications

(3 citation statements)

References 53 publications

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“…We have previously deployed this platform for the quantification of spatial and phenotypic heterogeneity in a variety of heterogeneous cancers, including non-small cell lung cancer ( Craig et al., 2019 ). Glioblastoma tissue (n = 4 patient samples) was cut manually into slices or fragments of various sizes up to 1 mm thick, and treated with rQNestin (0.1–5 PFU per cell, for 24 h) by adding the virus in a 100

L drop of saline to the piece of tissue submerged in 400

L of complete medium and incubated at 37

with 5% CO2 ( Smalley et al., 2020 ). Using a “sequential imaging strategy”, which we described recently ( Smalley et al., 2019 ), serial sections were then fixed and either stained with hematoxylin and eosin (H&E), or immunostained for HSV-1 (DAKO, B0114), GFP (GFP antibody CAT# AM1009a from Abgent, clone 168AT1211), or cleaved caspase-3 (Cell signaling Tech, for clone information see Goldman et al., 2015 ).…”

Section: Methodsmentioning

confidence: 99%

Agent-based computational modeling of glioblastoma predicts that stromal density is central to oncolytic virus efficacy

Jenner

Smalley

Goldman³

et al. 2022

iScience

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L drop of saline to the piece of tissue submerged in 400

L of complete medium and incubated at 37

Section: Methodsmentioning

confidence: 99%

Agent-based computational modeling of glioblastoma predicts that stromal density is central to oncolytic virus efficacy

Jenner

Smalley

Goldman³

et al. 2022

iScience

Self Cite

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“…Mathematical modeling of tumor treatments has become a critical area in mathematical oncology and computational systems biology, with numerous studies highlighting its significance [13][14][15][16][17][18][19][20][21][22][23][24][25][26][27][28]. Various mathematical methods, including response-diffusion equations, have been applied to predict the dynamic evolution of tumors during combination therapy by quantifying inter-regulatory relationships between tumor cells, immune cells, and cytokines in the tumor microenvironment [29][30][31][32][33][34][35][36][37].…”

Section: Discussionmentioning

confidence: 99%

“…Robertson-Tessi et al [17,18] proposed a comprehensive mathematical model of tumor-immunity interactions, incorporating a negative feedback loop to account for immunosuppressive mechanisms. Additionally, numerous studies have developed mathematical models to investigate various aspects of tumor-immunity interactions, thus expanding the breadth of research in this field [19][20][21][22][23][24][25][26][27][28]. While attempting to encompass all the cell types and signaling molecules involved in tumor-immunity interactions may be ambitious, it is crucial to strike a balance, as overly simplistic models may fail to capture the complex dynamics observed both experimentally and clinically.…”

Section: Introductionmentioning

confidence: 99%

Quantitative cancer-immunity cycle modeling for predicting disease progression in advanced metastatic colorectal cancer

Li,

Wei,

Lei

2024

Preprint

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Patients diagnosed with advanced metastatic colorectal cancer (mCRC) often exhibit heterogeneous disease progression and face poor survival prospects. In order to comprehensively analyze the varied treatment responses among individuals and the challenge of tumor recurrence resistant to drugs in advanced mRCR, we developed a novel quantitative cancer-immunity cycle (QCIC) model. The proposed model was meticulously crafted utilizing a blend of differential equations and randomized modeling techniques to quantitatively elucidate the intricate mechanisms governing the cancer-immunity cycle and forecast tumor dynamics under different treatment modalities. Furthermore, by integrating diverse clinical datasets and rigorous model analyses, we introduced two pivotal concepts: the treatment response index (TRI) and the death probability function (DPF). These concepts are crucial tools for translating model predictions into clinically relevant evaluation indexes. Using virtual patient technology, we extrapolated tumor predictive biomarkers from the model to predict survival outcomes for mCRC patients. Our findings underscore the significance of tumor-infiltrating CD8+CTL cell density as a key predictive biomarker for short-term treatment responses in advanced mCRC while emphasizing the potential predict value of the tumor-infiltrating CD4+Th1/Treg ratio in determining patient survival. This study presents a pioneering methodology bridging the divide between diverse clinical data sources and the generation of virtual patients, offering invaluable insights into understanding inter-individual treatment variations and forecasting survival outcomes in mCRC patients.

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Systems biology informed neural networks (SBINN) predict response and novel combinations for PD-1 checkpoint blockade

et al. 2021

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Anti-PD-1 immunotherapy has recently shown tremendous success for the treatment of several aggressive cancers. However, variability and unpredictability in treatment outcome have been observed, and are thought to be driven by patient-specific biology and interactions of the patient’s immune system with the tumor. Here we develop an integrative systems biology and machine learning approach, built around clinical data, to predict patient response to anti-PD-1 immunotherapy and to improve the response rate. Using this approach, we determine biomarkers of patient response and identify potential mechanisms of drug resistance. We develop systems biology informed neural networks (SBINN) to calculate patient-specific kinetic parameter values and to predict clinical outcome. We show how transfer learning can be leveraged with simulated clinical data to significantly improve the response prediction accuracy of the SBINN. Further, we identify novel drug combinations and optimize the treatment protocol for triple combination therapy consisting of IL-6 inhibition, recombinant IL-12, and anti-PD-1 immunotherapy in order to maximize patient response. We also find unexpected differences in protein expression levels between response phenotypes which complement recent clinical findings. Our approach has the potential to aid in the development of targeted experiments for patient drug screening as well as identify novel therapeutic targets.

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Integrating Systems Biology and an Ex Vivo Human Tumor Model Elucidates PD-1 Blockade Response Dynamics

Cited by 7 publications

References 53 publications

Agent-based computational modeling of glioblastoma predicts that stromal density is central to oncolytic virus efficacy

Agent-based computational modeling of glioblastoma predicts that stromal density is central to oncolytic virus efficacy

Quantitative cancer-immunity cycle modeling for predicting disease progression in advanced metastatic colorectal cancer

Systems biology informed neural networks (SBINN) predict response and novel combinations for PD-1 checkpoint blockade

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