Cell-type specific MyD88 signaling is required for intestinal tumor initiation and progression to malignancy

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Abstract

The signal adapter MyD88, an essential component of Toll-like receptor (TLR) signaling, is important for gut-microbiome interactions. However, its contribution to cancer and its cell-type specific functions are controversially discussed. Therefore, we generated new tissue-specific mouse models and analyzed the clinical importance in human colorectal cancer. A gene-trap was inserted into the murine Myd88 gene (Myd88LSL), yielding MyD88-deficient background with Cre-mediated re-expression in myeloid (MYEL) or intestinal epithelial cells (IECs). These lines were bred with the Apc1638N model that develops invasive adenocarcinoma and analyzed at 12 months. Further, two patient collectives of colorectal cancer (n = 61, and n = 633) were analyzed for expression of Myd88 and TLRs. MyD88 expression was significantly increased in carcinomas, and increased intratumoral levels of MyD88 and TLR pathway components were associated with significantly shorter disease-free (P =.011), and overall survival (P

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Holtorf, A., Conrad, A., Holzmann, B., & Janssen, K. P. (2018). Cell-type specific MyD88 signaling is required for intestinal tumor initiation and progression to malignancy. OncoImmunology, 7(8). https://doi.org/10.1080/2162402X.2018.1466770

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