1°C ± 0.46°C) in a mean time of 15.5 minutes (range 4-21 minutes) with variations of less than 0.5°C along the procedure. Temperature was dependent on the flow rate and was unstable at a flow of less than 15 ml/min. Tolerance to HIPEC was poor. Only 3 out of 5 rats survived until the end of the experiment. The others presented an abnormal respiratory rhythm at about 45 minutes and died before the end. This precluded the performance of a 2-hour LY2606368 HIPEC. In contrast, all of the animals that were treated at 37°C, for either 1 or 2 hours, with or without adrenaline, were alive and well at the end of the experiment. Platinum
concentrations in rat organs and peritoneal Niraparib clinical trial nodules were measured according to the different treatments (Figure 3). Regarding the platinum content in peritoneal nodules, the difference between group 1 (control, 1 hour IPC), and groups 4 (2 hours IPC) or 2 (HIPEC) did not reach significance (p = 0.06 and 0.19, respectively). In contrast, a 3-fold increase in tumor platinum content was found in group 3 (adrenaline) as compared to groups 1 (control, p = 0.005) and 2 (HIPEC, p = 0.005). Platinum
concentration in the abdominal muscle lining the peritoneal cavity was also significantly greater in group INCB028050 chemical structure 3 (adrenaline) as compared to group 4 (HIPEC) (p = 0.006), but did not reach significance in the diaphragm (p = 0.08). Figure 3 In vivo accumulation of platinum in peritoneal tumor and organs. Intraperitoneal chemotherapy was performed using 30 mg/l of cisplatin. Tumor and organs were sampled: after 1 hour cisplatin at 37°C (a), after 1 hour cisplatin at 42°C (b), after 2 hours cisplatin with (c) or without (d) 2 mg/l adrenaline. Mean and SD of 5 animals. Asterisk Reverse transcriptase indicates a statistical difference (p < 0.01) between the 2 hours treatment at 37°C with 2 mg/L adrenaline, and the 1 hour treatment at 42°C. ABD/MU = abdominal muscle and THOR/MU = thoracic muscle. Out of the peritoneal cavity (kidney and thoracic muscle), the accumulation
of platinum was lower in group 3 (adrenaline) than in groups 1 (control) and 4 (HIPEC) (p = 0.05 and p = 0.001, for the kidney and the thoracic muscle, respectively). Discussion The present study reports the greater uptake of platinum in peritoneal nodules and in peritoneum lining muscle when adrenaline was used in combination with cisplatin, as compared to HIPEC. This underlines the interest of adrenaline to increase the tissue concentration of chemotherapy and the fact that the best method to deliver of IPC remains to be defined [10, 17, 21]. The rats treated with adrenaline (group 3) received this treatment for 2 hours, as compared to those undergoing HIPEC (group 2) during only 1 hour. A 1-hour adrenaline group was not performed because a previous unpublished experiment found no significant difference after this treatment as compared to the control group.