Computational Discovery of Cancer Immunotherapy Targets by Intercellular CRISPR Screens

Soorin Yim; Woochang Hwang; Namshik Han; Doheon Lee

doi:10.3389/fimmu.2022.884561

Computational Discovery of Cancer Immunotherapy Targets by Intercellular CRISPR Screens

Front Immunol. 2022 May 16:13:884561. doi: 10.3389/fimmu.2022.884561. eCollection 2022.

Authors

Soorin Yim^{1

2}, Woochang Hwang³, Namshik Han^{3

4}, Doheon Lee^{1

2}

Affiliations

¹ Department of Bio and Brain Engineering, Korea Advanced Institute of Science and Technology (KAIST), Daejeon, South Korea.
² Bio-Synergy Research Center, Daejeon, South Korea.
³ Milner Therapeutics Institute, University of Cambridge, Cambridge, United Kingdom.
⁴ Cambridge Centre for AI in Medicine, Department of Applied Mathematics and Theoretical Physics, University of Cambridge, Cambridge, United Kingdom.

Abstract

Cancer immunotherapy targets the interplay between immune and cancer cells. In particular, interactions between cytotoxic T lymphocytes (CTLs) and cancer cells, such as PD-1 (PDCD1) binding PD-L1 (CD274), are crucial for cancer cell clearance. However, immune checkpoint inhibitors targeting these interactions are effective only in a subset of patients, requiring the identification of novel immunotherapy targets. Genome-wide clustered regularly interspaced short palindromic repeats (CRISPR) screening in either cancer or immune cells has been employed to discover regulators of immune cell function. However, CRISPR screens in a single cell type complicate the identification of essential intercellular interactions. Further, pooled screening is associated with high noise levels. Herein, we propose intercellular CRISPR screens, a computational approach for the analysis of genome-wide CRISPR screens in every interacting cell type for the discovery of intercellular interactions as immunotherapeutic targets. We used two publicly available genome-wide CRISPR screening datasets obtained while triple-negative breast cancer (TNBC) cells and CTLs were interacting. We analyzed 4825 interactions between 1391 ligands and receptors on TNBC cells and CTLs to evaluate their effects on CTL function. Intercellular CRISPR screens discovered targets of approved drugs, a few of which were not identifiable in single datasets. To evaluate the method's performance, we used data for cytokines and costimulatory molecules as they constitute the majority of immunotherapeutic targets. Combining both CRISPR datasets improved the recall of discovering these genes relative to using single CRISPR datasets over two-fold. Our results indicate that intercellular CRISPR screens can suggest novel immunotherapy targets that are not obtained through individual CRISPR screens. The pipeline can be extended to other cancer and immune cell types to discover important intercellular interactions as potential immunotherapeutic targets.

Keywords: cell-cell communication; cytotoxic T cells; genome-wide CRISPR screen; immune checkpoint inhibitors; intercellular interactions; ligand-receptor interactions; target discovery; triple-negative breast cancer.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

CRISPR-Cas Systems
Clustered Regularly Interspaced Short Palindromic Repeats* / genetics
Humans
Immunotherapy
T-Lymphocytes, Cytotoxic
Triple Negative Breast Neoplasms* / genetics