Drug repositioning for immunotherapy in breast cancer using single-cell analysis

Elyas Mohammadi; Samira Dashti; Neda Shafizade; Han Jin; Cheng Zhang; Simon Lam; Mojtaba Tahmoorespur; Adil Mardinoglu; Mohammad Hadi Sekhavati

doi:10.1038/s41540-024-00359-z

Drug repositioning for immunotherapy in breast cancer using single-cell analysis

Elyas Mohammadi, Samira Dashti, Neda Shafizade, Han Jin, Cheng Zhang, Simon Lam, Mojtaba Tahmoorespur, Adil Mardinoglu, Mohammad Hadi Sekhavati

Research output: Contribution to journal › Article › peer-review

3 Citations (Scopus)

1 Downloads (Pure)

Abstract

Immunomodulatory peptides, while exhibiting potential antimicrobial, antifungal, and/or antiviral properties, can play a role in stimulating or suppressing the immune system, especially in pathological conditions like breast cancer (BC). Thus, deregulation of these peptides may serve as an immunotherapeutic strategy to enhance the immune response. In this meta-analysis, we utilized single-cell RNA sequencing data and known therapeutic peptides to investigate the deregulation of these peptides in malignant versus normal human breast epithelial cells. We corroborated our findings at the chromatin level using ATAC-seq. Additionally, we assessed the protein levels in various BC cell lines. Moreover, our in-house drug repositioning approach was employed to identify potential drugs that could positively impact the relapse-free survival of BC patients. Considering significantly deregulated therapeutic peptides and their role in BC pathology, our approach aims to downregulate B2M and SLPI, while upregulating PIGR, DEFB1, LTF, CLU, S100A7, and SCGB2A1 in BC epithelial cells through our drug repositioning pipeline. Leveraging the LINCS L1000 database, we propose BRD-A06641369 for B2M downregulation and ST-4070043 and BRD-K97926541 for SLPI downregulation without negatively affecting the MHC complex as a significantly correlated pathway with these two genes. Furthermore, we have compiled a comprehensive list of drugs for the upregulation of other selected immunomodulatory peptides. Employing an immunotherapeutic approach by integrating our drug repositioning pipeline with single-cell analysis, we proposed potential drugs and drug targets to fortify the immune system against BC.

Original language	English
Article number	37
Journal	npj Systems Biology and Applications
Volume	10
Issue number	1
Early online date	8 Apr 2024
DOIs	https://doi.org/10.1038/s41540-024-00359-z
Publication status	Published - 8 Apr 2024

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

Access to Document

10.1038/s41540-024-00359-zLicence: CC BY

Drug repositioning for immunotherapy_MOHAMMADI_Publihsednline8April2024_GOLD_VoR (CC BY)Final published version, 2.17 MBLicence: CC BY

Cite this

@article{60779ca4da644e6a8c738ffd70bf926f,

title = "Drug repositioning for immunotherapy in breast cancer using single-cell analysis",

abstract = "Immunomodulatory peptides, while exhibiting potential antimicrobial, antifungal, and/or antiviral properties, can play a role in stimulating or suppressing the immune system, especially in pathological conditions like breast cancer (BC). Thus, deregulation of these peptides may serve as an immunotherapeutic strategy to enhance the immune response. In this meta-analysis, we utilized single-cell RNA sequencing data and known therapeutic peptides to investigate the deregulation of these peptides in malignant versus normal human breast epithelial cells. We corroborated our findings at the chromatin level using ATAC-seq. Additionally, we assessed the protein levels in various BC cell lines. Moreover, our in-house drug repositioning approach was employed to identify potential drugs that could positively impact the relapse-free survival of BC patients. Considering significantly deregulated therapeutic peptides and their role in BC pathology, our approach aims to downregulate B2M and SLPI, while upregulating PIGR, DEFB1, LTF, CLU, S100A7, and SCGB2A1 in BC epithelial cells through our drug repositioning pipeline. Leveraging the LINCS L1000 database, we propose BRD-A06641369 for B2M downregulation and ST-4070043 and BRD-K97926541 for SLPI downregulation without negatively affecting the MHC complex as a significantly correlated pathway with these two genes. Furthermore, we have compiled a comprehensive list of drugs for the upregulation of other selected immunomodulatory peptides. Employing an immunotherapeutic approach by integrating our drug repositioning pipeline with single-cell analysis, we proposed potential drugs and drug targets to fortify the immune system against BC.",

author = "Elyas Mohammadi and Samira Dashti and Neda Shafizade and Han Jin and Cheng Zhang and Simon Lam and Mojtaba Tahmoorespur and Adil Mardinoglu and Sekhavati, {Mohammad Hadi}",

note = "Publisher Copyright: {\textcopyright} 2024. The Author(s).",

year = "2024",

month = apr,

day = "8",

doi = "10.1038/s41540-024-00359-z",

language = "English",

volume = "10",

journal = "npj Systems Biology and Applications",

issn = "2056-7189",

publisher = "Nature Publishing Group",

number = "1",

}

TY - JOUR

T1 - Drug repositioning for immunotherapy in breast cancer using single-cell analysis

AU - Mohammadi, Elyas

AU - Dashti, Samira

AU - Shafizade, Neda

AU - Jin, Han

AU - Zhang, Cheng

AU - Lam, Simon

AU - Tahmoorespur, Mojtaba

AU - Mardinoglu, Adil

AU - Sekhavati, Mohammad Hadi

PY - 2024/4/8

Y1 - 2024/4/8

N2 - Immunomodulatory peptides, while exhibiting potential antimicrobial, antifungal, and/or antiviral properties, can play a role in stimulating or suppressing the immune system, especially in pathological conditions like breast cancer (BC). Thus, deregulation of these peptides may serve as an immunotherapeutic strategy to enhance the immune response. In this meta-analysis, we utilized single-cell RNA sequencing data and known therapeutic peptides to investigate the deregulation of these peptides in malignant versus normal human breast epithelial cells. We corroborated our findings at the chromatin level using ATAC-seq. Additionally, we assessed the protein levels in various BC cell lines. Moreover, our in-house drug repositioning approach was employed to identify potential drugs that could positively impact the relapse-free survival of BC patients. Considering significantly deregulated therapeutic peptides and their role in BC pathology, our approach aims to downregulate B2M and SLPI, while upregulating PIGR, DEFB1, LTF, CLU, S100A7, and SCGB2A1 in BC epithelial cells through our drug repositioning pipeline. Leveraging the LINCS L1000 database, we propose BRD-A06641369 for B2M downregulation and ST-4070043 and BRD-K97926541 for SLPI downregulation without negatively affecting the MHC complex as a significantly correlated pathway with these two genes. Furthermore, we have compiled a comprehensive list of drugs for the upregulation of other selected immunomodulatory peptides. Employing an immunotherapeutic approach by integrating our drug repositioning pipeline with single-cell analysis, we proposed potential drugs and drug targets to fortify the immune system against BC.

AB - Immunomodulatory peptides, while exhibiting potential antimicrobial, antifungal, and/or antiviral properties, can play a role in stimulating or suppressing the immune system, especially in pathological conditions like breast cancer (BC). Thus, deregulation of these peptides may serve as an immunotherapeutic strategy to enhance the immune response. In this meta-analysis, we utilized single-cell RNA sequencing data and known therapeutic peptides to investigate the deregulation of these peptides in malignant versus normal human breast epithelial cells. We corroborated our findings at the chromatin level using ATAC-seq. Additionally, we assessed the protein levels in various BC cell lines. Moreover, our in-house drug repositioning approach was employed to identify potential drugs that could positively impact the relapse-free survival of BC patients. Considering significantly deregulated therapeutic peptides and their role in BC pathology, our approach aims to downregulate B2M and SLPI, while upregulating PIGR, DEFB1, LTF, CLU, S100A7, and SCGB2A1 in BC epithelial cells through our drug repositioning pipeline. Leveraging the LINCS L1000 database, we propose BRD-A06641369 for B2M downregulation and ST-4070043 and BRD-K97926541 for SLPI downregulation without negatively affecting the MHC complex as a significantly correlated pathway with these two genes. Furthermore, we have compiled a comprehensive list of drugs for the upregulation of other selected immunomodulatory peptides. Employing an immunotherapeutic approach by integrating our drug repositioning pipeline with single-cell analysis, we proposed potential drugs and drug targets to fortify the immune system against BC.

UR - http://www.scopus.com/inward/record.url?scp=85190320576&partnerID=8YFLogxK

U2 - 10.1038/s41540-024-00359-z

DO - 10.1038/s41540-024-00359-z

M3 - Article

C2 - 38589404

AN - SCOPUS:85190320576

SN - 2056-7189

VL - 10

JO - npj Systems Biology and Applications

JF - npj Systems Biology and Applications

IS - 1

M1 - 37

ER -

Drug repositioning for immunotherapy in breast cancer using single-cell analysis

Abstract

UN SDGs

Access to Document

Other files and links

Fingerprint

Cite this