Project description:To identify the proteome of human peritoneal tissue, 43 FFPE and 5 fresh frozen peritoneal tissue samples at healthy or non-cancerous state were collected and subjected to mass spectrometry analysis. The resulting findings represnt a baseline catalog of the proteomic composition of the peritoneum, as a comparison dataset for future studies focused on alterations in pathologic states such as peritoneal carcinomatosis.

Project description:Peritoneal carcinomatosis (PC) originating from colorectal cancer (CRC) is associated with a poor prognosis and rapid disease progression. Metastasis is the major cause of death in patients with CRC whereas primary locoregionally circumscribed tumors are mostly curable. Due to the lack of appropriate and realistic mouse models for metastasis of CRC until recently, the research about metastasis of these tumors and possible therapeutic options is still in its infancy. With the establishment of murine CRC tumor organoids, mouse models were established which realistically mimic the process of tumor cell metastasis to the liver and the lung. However, to date no appropriate model for PC is described. Here, we establish a realistic model for peritoneal metastasis of colorectal cancer upon surgical transplantation of tumor organoids into the cecum wall. This mouse model for PC recapitulates human PC which makes it an ideal model for research of the biology of metastasis of colorectal cancer to the peritoneal cavity and for its usage for preclinical drug screening as well as for the evaluation of new therapeutic approaches which are highly needed in clinical reality.

Project description:The omentum, a specialized adipose tissue within the peritoneum, is a key metastatic niche for ovarian cancer (OC) dissemination during peritoneal carcinomatosis. The prevailing view is that omental adipocytes promote tumor growth by providinglipids, since global FABP4 deficiency curbs tumor growth. Here, we generated mice lacking mature adipocytes in the peritoneum and omentum. ID8p53–/–Brca2–/– , BPPNM, and KPCA OC cells retained a propensity to seed at regions typically associated with adipocytes, even without mature adipocytes. However, lack of mature adipocytes did not suppress peritoneal OC expansion, whereas removing the adipocyte-free omentum did. Murine and human single-cell RNA sequencing analysis revealed that endothelial FABP4 was high in the omentum. Indeed, endothelial cell-selective deficiency of FABP4 reduced OC growth in the peritoneum. These findings prompt a re-evaluation of adipocyte contributions to OC progression and point to a key role of the omental vasculature in supporting OC growth metabolically.

Project description:Peritoneal carcinomatosis is a frequent finding in patients with primary gastric cancer, and it is associated with a poor prognosis. A major mechanism in peritoneal carcinomatosis is the dissemination of cancer cells into the abdominal cavity, mainly in diffuse gastric adenocarcinoma. The features that enable diffuse primary gastric tumours to develop peritoneal dissemination have been little investigated and are only incompletely understood. We therefore compared the gene expression profile in patients with diffuse primary gastric cancer with and without peritoneal carcinomatosis. Specimens from consecutive gastric cancer patients with and without peritoneal carcinomatosis were investigated using oligonucleotide microarrays. Keywords: Disease state analysis

Project description:Characterizations of ascites proteome from ovarian peritoneal carcinomatosis (PC) and gastric PC have demonstrated that ascites contains elevated pro-tumorigenic factors. Reasoning that the composition of ascitic fluid might offer insight into the memory of key biological events occurring intra-abdominally, we hypothesized that paracrine factors essential for survival and growth of peritoneal deposits are secreted into and circulate within ascitic fluid. Our data from cytokine array profile suggest that ascites contains biologically active ligands capable of supporting cellular functions of cancer cells. To decipher downstream signalling pathways activated in cancer cells when exposed to ascites, we performed gene expression analysis of Colo-205 cells upon exposure to PC ascites and ligand inhibitor.

Project description:In this study, we generated patient-derived organoids (PDOs) from patients with colorectal cancer peritoneal mestasis and performed RNA- and ATAC-sequencing to study mechanisms for doxorubicin response.

Project description:In this study, we generated patient-derived organoids (PDOs) from patients with colorectal cancer peritoneal and liver mestases and performed RNA- and ATAC-sequencing to study mechanisms for doxorubicin response.

Project description:Peritoneal carcinomatosis (PC) occurs frequently in gastric adenocarcinoma (GAC) patients and confers poor prognosis. Multiplex profiling of primary GACs has been insightful but the underpinnings of PC’s development/progression remain largely unknown. Here we characterized exome/transcriptome/immune landscapes of PC cells from 43 patients.

Project description:Interventions: Group 1: During primary curative surgery for gastric or colon carcinoma with synchronous or metachronous peritoneal carcinomatosis, the peritoneal carcinomatosis index (PCI) is determined and biopsies of the PC foci are taken before resection. Surgery is performed according to standard and includes both resection of the primarius and any metastases present and (as far as possible) complete cytoreductive surgery (CCS 0-1) by peritonectomy of the affected sites, followed by HIPEC according to the respective hospital standard. After 6 months, a planned re-operation (laparoscopy/laparotomy) may be performed, depending on the local standard at the respective study center. If a macroscopic PC recurrence is detected, the PCI will be recalculated and a new (as far as possible) complete cytoreductive surgery (CCS 0-1) will be performed by peritonectomy of the affected sites followed by HIPEC according to the respective hospital standard. The aim of this pilot study is to generate patient-derived tumor organoid models as well as orthotopic mouse models from peritoneal carcinomatosis lesions and to investigate their response to different therapies. Based on the findings of the pilot study, a main clinical trial will then be designed. Aims of the study are: 1. to describe individualized HIPEC regimens in vitro based on organoid response to therapy and next generation sequencing (NGS) data. 2. the evaluation of individualized HIPEC regimens in vivo in an orthotopic mouse model. 3. the collection of the oncological courses of the patients in the context of the standard tumor follow-up and comparison with the models. Primary outcome(s): The primary endpoint is to analyze the predictive accuracy of patient-generated tumor organoids (PDOs) for predicting response to HIPEC treatment in patients with peritoneal carcinomatosis (PC). Study Design: Allocation: ; Masking: ; Control: ; Assignment: ; Study design purpose: treatment

Project description:Peritoneal carcinomatosis (PC) remains a significant clinical challenge, with limited therapeutic options. Adoptive cell therapy (ACT) using tumor-specific T cells has emerged as a promising strategy; however, its efficacy is often hindered by the immunosuppressive tumor microenvironment (TME). Interleukin-33 (IL-33), a member of the IL-1 family, plays a dual role in immunity and inflammation, with the potential to enhance antitumor responses. Here, we investigated the impact of IL-33 mRNA-engineered T cells on ACT efficacy in murine models of PC and explored the potential synergy with IL-12 mRNA.