Colorectal Carcinoma Clinical Trial
Official title:
Microparticles in Peritoneal Carcinomatosis of Colorectal Origin
Peritoneal carcinomatosis (PC), a tumoral tumor of the peritoneum, is a frequent metastatic
localization of colorectal cancer (CRC, 13%). Long regarded as a palliative situation, its
management has progressed significantly with a curative treatment based on a complete
cytoreduction surgery coupled with intraperitoneal hyperthermic chemotherapy. However current
screening tools, tumor markers (ACE, CA19-9, CA125) and abdominopelvic CT scan are
insufficient, to diagnose CP early. A non-invasive biomarker, more sensitive and more
specific than currently available tumor markers, would be a major advance in oncology.
Microparticles (MPs), vesicles from extracellular membrane budding in response to cell
activation or apoptosis of different cell types, have been described as implicated in tumor
progression, procoagulant activity associated with cancer, and initiation of metastatic
niches. A specific microparticulate (microparticulosome) signature has been reported in
patients with CRC, particularly in the presence of a thromboembolic event. However, there is
currently no data on PMs and their involvement in CP. In addition, CP and surgery coupled
with hyperthermic intraperitoneal chemotherapy are major risk factors for thromboembolic
complications. The characterization of prothrombotic PMs is therefore essential to predict
such event.
The main objective of this project is to characterize the microparticulate signature of CP of
colorectal origin and to compare it with that of CP without CP. The secondary objectives are
to compare the microparticulate signature obtained on peripheral venous samples and
intraoperative tumor samples, evaluate the evolution of the microparticulate signature
between the beginning and the end of the intervention, then correlate the peripheral
signature to the oncological follow-up of the patients with CP and the occurrence of a
thromboembolic event.
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