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eISSN: 2581-9615 || CODEN (USA): WJARAI || Impact Factor: 8.2 || ISSN Approved Journal

CRISPR-engineered probiotics for targeted production of inosine as an immunomodulatory metabolite to enhance cancer immunotherapy response: A review

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  • CRISPR-engineered probiotics for targeted production of inosine as an immunomodulatory metabolite to enhance cancer immunotherapy response: A review

Reisya Irfanny Farizaldi * and Vianca Sashira Asmoro

Undergraduate Student, Faculty of Dental Medicine, Universitas Airlangga, Surabaya, Indonesia.

Review Article

World Journal of Advanced Research and Reviews, 2026, 29(01), 1917-1924

Article DOI: 10.30574/wjarr.2026.29.1.0257

DOI url: https://doi.org/10.30574/wjarr.2026.29.1.0257

Received on 22 December 2025; revised on 28 January 2026; accepted on 31 January 2026

Background: Cancer immunotherapy, especially immune checkpoint inhibitors (ICIs), has improved cancer survival but remains limited by variable response and adverse effects. Emerging evidence demonstrated that gut microbiome, particularly inosine, is a critical determinant of immunotherapy efficacy through its capacity to produce immunomodulatory metabolites that enhance T-cell activation, promote dendritic cell function, and restore anti-tumor immunity. Advances in CRISPR-Cas technology has enabled precise engineering of probiotic strains for targeted inosine production, offering a potentially safer and more effective immunomodulatory approach.

Purpose: This study aims to evaluate CRISPR-engineered probiotics for targeted production of inosine as an immunomodulatory metabolite to enhance cancer immunotherapy response.

Method: A narrative literature review was conducted using secondary data collected from online databases such as PubMed, ScienceDirect, and ResearchGate.

Results: A total of 11 studies were analyzed, showing that CRISPR-engineered probiotics can precisely enhance inosine production via targeted purine metabolic pathways. Microbiota-derived inosine promotes T-cell and dendritic cell activation through A2A receptor signaling, driving Th1 polarization, IFN-γ secretion, CD8+ cytotoxic T-cell activity, and supporting T-cell metabolism under stress. Engineered probiotics demonstrated more consistent inosine production and predictable immunomodulatory effects compared to conventional strains, potentially synergizing with ICIs to reduce tumor growth and improve antitumor immunity.

Conclusion: CRISPR-engineered probiotics for targeted production of inosine suggest potential to enhance cancer immunotherapy response.

CRISPR-Engineered Probiotics; Cancer Immunotherapy; Gut Microbiome; Inosine; Immune Checkpoint Inhibitors

https://journalwjarr.com/sites/default/files/fulltext_pdf/WJARR-2026-0257.pdf

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Reisya Irfanny Farizaldi and Vianca Sashira Asmoro. CRISPR-engineered probiotics for targeted production of inosine as an immunomodulatory metabolite to enhance cancer immunotherapy response: A review. World Journal of Advanced Research and Reviews, 2026, 29(01), 1917-1924. Article DOI: https://doi.org/10.30574/wjarr.2026.29.1.0257.

Copyright © 2026 Author(s) retain the copyright of this article. This article is published under the terms of the Creative Commons Attribution Liscense 4.0

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