{"id":2598053,"date":"2023-12-18T19:00:00","date_gmt":"2023-12-19T00:00:00","guid":{"rendered":"https:\/\/platoai.gbaglobal.org\/platowire\/a-study-on-the-off-tumour-toxicities-of-t-cell-engaging-bispecific-antibodies-using-donor-matched-intestinal-organoids-and-tumouroids\/"},"modified":"2023-12-18T19:00:00","modified_gmt":"2023-12-19T00:00:00","slug":"a-study-on-the-off-tumour-toxicities-of-t-cell-engaging-bispecific-antibodies-using-donor-matched-intestinal-organoids-and-tumouroids","status":"publish","type":"platowire","link":"https:\/\/platoai.gbaglobal.org\/platowire\/a-study-on-the-off-tumour-toxicities-of-t-cell-engaging-bispecific-antibodies-using-donor-matched-intestinal-organoids-and-tumouroids\/","title":{"rendered":"A Study on the Off-Tumour Toxicities of T-Cell-Engaging Bispecific Antibodies using Donor-Matched Intestinal Organoids and Tumouroids"},"content":{"rendered":"

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A Study on the Off-Tumour Toxicities of T-Cell-Engaging Bispecific Antibodies using Donor-Matched Intestinal Organoids and Tumouroids<\/p>\n

Introduction:
\nT-cell-engaging bispecific antibodies (BsAbs) have emerged as a promising immunotherapy approach for the treatment of various cancers. These antibodies are designed to redirect and activate T-cells to specifically target and kill tumor cells. However, the use of BsAbs can also lead to off-tumour toxicities, which can limit their therapeutic potential. To better understand and mitigate these toxicities, a recent study utilized donor-matched intestinal organoids and tumouroids to investigate the off-tumour effects of T-cell-engaging BsAbs.<\/p>\n

Understanding Off-Tumour Toxicities:
\nOff-tumour toxicities occur when T-cells activated by BsAbs target healthy tissues instead of cancer cells. This can result in severe adverse effects, including organ damage and systemic inflammation. The mechanisms underlying these toxicities are not fully understood, highlighting the need for comprehensive studies to elucidate the factors contributing to off-tumour effects.<\/p>\n

The Role of Intestinal Organoids and Tumouroids:
\nIntestinal organoids are three-dimensional structures derived from human pluripotent stem cells or adult tissue that mimic the architecture and functionality of the human intestine. These organoids provide a valuable model to study the effects of drugs or therapies on the intestinal epithelium. Tumouroids, on the other hand, are organoids derived from patient tumor samples and can be used to study tumor-specific responses.<\/p>\n

Study Design and Findings:
\nIn this study, researchers generated donor-matched intestinal organoids and tumouroids from patient-derived samples. They then treated these organoids with T-cell-engaging BsAbs to investigate their off-tumour toxicities. The researchers observed that BsAbs induced significant damage to the intestinal epithelium, leading to impaired barrier function and increased permeability.<\/p>\n

Furthermore, the study revealed that the off-tumour toxicities were mediated by the activation of T-cells within the intestinal organoids. The activated T-cells released pro-inflammatory cytokines, such as interferon-gamma (IFN-\u03b3), which contributed to the disruption of the intestinal epithelium. The researchers also found that the severity of off-tumour toxicities varied among different BsAbs, suggesting that the design and properties of these antibodies play a crucial role in determining their safety profile.<\/p>\n

Implications and Future Directions:
\nThe findings from this study provide valuable insights into the off-tumour toxicities associated with T-cell-engaging BsAbs. By utilizing donor-matched intestinal organoids and tumouroids, researchers were able to recapitulate the complex interactions between T-cells, tumor cells, and healthy tissues. This model can be further utilized to evaluate the safety and efficacy of BsAbs before clinical trials, potentially reducing the risk of off-tumour toxicities in patients.<\/p>\n

Moving forward, future studies could focus on identifying specific biomarkers or genetic signatures associated with off-tumour toxicities. This could aid in predicting patient susceptibility to these toxicities and developing personalized treatment strategies. Additionally, investigating strategies to mitigate off-tumour effects, such as co-administration of immunomodulatory agents or engineering BsAbs with improved selectivity, could enhance the therapeutic potential of this promising immunotherapy approach.<\/p>\n

Conclusion:
\nThe study on off-tumour toxicities of T-cell-engaging BsAbs using donor-matched intestinal organoids and tumouroids provides valuable insights into the mechanisms underlying these toxicities. By utilizing advanced in vitro models, researchers can better understand the factors contributing to off-tumour effects and develop strategies to enhance the safety and efficacy of T-cell-engaging immunotherapies. This research paves the way for more targeted and personalized cancer treatments, ultimately improving patient outcomes.<\/p>\n