Decoy-resistant IL18: how engineered E. coli enhances immune responses against tumors

Romee, Rizwan

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Topics Covered

Tumor microenvironment
Non-pathogenic Escherichia coli
Immune-activating cytokines
Live bacteria-based immunotherapeutic system
Anti-tumor responses

Biography

Dr. Rizwan Romee, MD is a medical oncologist and translational physician-scientist based at the Dana-Farber Cancer Institute, USA. He serves as Director of the Haploidentical Donor Transplantation Program and is an Associate Professor of Medicine at Harvard Medical School. His clinical expertise includes advanced myeloid malignancies, haploidentical stem cell transplantation, and NK-cell based cellular therapies.

Dr. Romee’s research focuses on genetically manipulating human natural killer (NK) cells to enhance their anti-tumor activity and modulate the tumor microenvironment, including pioneering work on memory-like NK cells and their application in clinical trials for hematologic malignancies and other cancers. He leads the Romee Lab for NK cell gene manipulation and therapy and collaborates on developing innovative immunotherapy approaches.

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Oncology

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Non-pathogenic E. coli displaying decoy-resistant IL18 mutein boosts anti-tumor and CAR NK cell responses

Talk Citation

Romee, R. (2026, February 26). Decoy-resistant IL18: how engineered E. coli enhances immune responses against tumors [Audio file]. In The Biomedical & Life Sciences Collection, Henry Stewart Talks. Retrieved April 19, 2026, from https://doi.org/10.69645/LWMF1161.
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Publication History

Published on February 26, 2026

Financial Disclosures

Dr. Rizwan Romee has not informed HSTalks of any commercial/financial relationship that it is appropriate to disclose.

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Decoy-resistant IL18: how engineered E. coli enhances immune responses against tumors

Dr. Rizwan Romee – Harvard Medical School, USA

Published on February 26, 2026 13 min

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Interviewer: Dr. Rizwan Romee, you and your colleagues at the Dana-Farber Cancer Institute recently published a paper in Nature Biotechnology, introducing a novel immunotherapeutic system that is effective in treatment-resistant solid tumors. What is particularly interesting here is that this is a system that is based on live non-pathogenic E. coli. So, to set the scene, can you start by providing some background information on the way in which the tumor microenvironment hinders the effectiveness of traditional cancer therapies, and how this study aims to overcome those challenges? Dr. Romee: Thank you, Eyal, for asking this question. The tumor microenvironment is one of the biggest challenges in cancer immunotherapy in general. It's almost across the board that multiple types of cancer have this highly immunosuppressive tumor microenvironment, which leads to dysfunction of immune effector cells. There are multiple factors involved in this dysfunction, including, first of all, the trafficking of immune cells into the tumor microenvironment. So the tumor microenvironment vasculature is structured in such a way that it does not favor trafficking or migration of immune cells from the blood to the tumor microenvironment. That's number 1. Number 2, once the cells are in, if they make it, then they get dysfunctional, and that dysfunction is mediated by several factors, including things like TGFβ, prostaglandins, low pH mediated by higher levels of lactate, and also low oxygen, which we also call hypoxemia.

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Decoy-resistant IL18: how engineered E. coli enhances immune responses against tumors