PAR1 Is a Candidate Target for the Treatment of Peritoneal Dissemination in Gastric Cancer.

IF 1.6 4区医学 Q4 ONCOLOGY

Anticancer research Pub Date : 2024-11-01 DOI:10.21873/anticanres.17311

Daisuke Fujimoto, Hirotoshi Kobayashi

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引用次数: 0

Abstract

Background/aim: Peritoneal dissemination (PD) is a frequent cause of death in gastric cancer (GC), and there is evidence of an association between protease-activated receptor-1 (PAR1) and the development of PD. This study hypothesized that PD in GC might be influenced by PAR1.

Materials and methods: The cytotoxic effect of paclitaxel (PTX) on PAR1-transfected MKN45 (MKN45/PAR1) cells was analyzed using the MTT assay, and IC₅₀ values were determined. In female athymic nude mice, MKN45/PAR1 cells were suspended in 0.05 ml phosphate-buffered saline (PBS) medium and inoculated into the stomach mid-wall. In each group, intraperitoneal injections of PBS, PTX, SCH79797 (PAR1-antagonist), or PTX plus SCH79797 were administered on days 8, 15, and 22 following tumor inoculation. At 56 days after tumor inoculation, mice were examined for both abdominal tumor nodule status and size and weight of the tumors.

Results: The IC₅₀ of PTX for MKN45/PAR1 cells was 0.0697 μM and that of SCH79797 was 0.0145 μM. Mean survival of the MKN45/PAR1 mice in the PBS group was 28.75 days, whereas survival times for the mice treated with SCH79797, PTX, or a combination of PTX and SCH79797 were 31.2, 49.2, and 48.5 days, respectively. Tumor weight was smaller in the group receiving PTX and SCH79797 intraperitoneally compared with that in the PBS group (1,086±127.2 mg vs. 33.2±19.9 mg; p<0.001).

Conclusion: The PAR1 antagonist was found to inhibit PD in a PAR1-expressing GC cell line. PAR1 may serve as a promising therapeutic target for managing PD in gastric cancer, as it plays a crucial role in its progression.

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PAR1 是治疗胃癌腹膜扩散的候选靶点

背景/目的：腹膜播散（PD）是胃癌（GC）的常见死因，有证据表明蛋白酶激活受体-1（PAR1）与腹膜播散的发生有关。本研究假设胃癌中的PD可能受PAR1的影响：采用 MTT 法分析紫杉醇（PTX）对 PAR1 转染的 MKN45（MKN45/PAR1）细胞的细胞毒性作用，并测定 IC50 值。将 MKN45/PAR1 细胞悬浮于 0.05 ml 磷酸盐缓冲液（PBS）培养基中，接种于雌性无胸腺裸鼠的胃中壁。每组在肿瘤接种后第 8、15 和 22 天腹腔注射 PBS、PTX、SCH79797（PAR1-拮抗剂）或 PTX 加 SCH79797。肿瘤接种后 56 天，检查小鼠腹部肿瘤结节状态以及肿瘤的大小和重量：结果：PTX对MKN45/PAR1细胞的IC50为0.0697 μM，SCH79797的IC50为0.0145 μM。PBS组MKN45/PAR1小鼠的平均存活时间为28.75天，而接受SCH79797、PTX或PTX和SCH79797组合治疗的小鼠的存活时间分别为31.2天、49.2天和48.5天。与 PBS 组相比，腹腔注射 PTX 和 SCH79797 组的肿瘤重量较小（1,086±127.2 mg vs. 33.2±19.9 mg; p结论：研究发现，PAR1 拮抗剂可抑制表达 PAR1 的 GC 细胞系的 PD。PAR1在胃癌的进展过程中起着至关重要的作用，因此可作为治疗胃癌PD的靶点。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Anticancer research 医学-肿瘤学

CiteScore

3.70

自引率

10.00%

发文量

566

审稿时长

2 months

期刊介绍： ANTICANCER RESEARCH is an independent international peer-reviewed journal devoted to the rapid publication of high quality original articles and reviews on all aspects of experimental and clinical oncology. Prompt evaluation of all submitted articles in confidence and rapid publication within 1-2 months of acceptance are guaranteed. ANTICANCER RESEARCH was established in 1981 and is published monthly (bimonthly until the end of 2008). Each annual volume contains twelve issues and index. Each issue may be divided into three parts (A: Reviews, B: Experimental studies, and C: Clinical and Epidemiological studies). Special issues, presenting the proceedings of meetings or groups of papers on topics of significant progress, will also be included in each volume. There is no limitation to the number of pages per issue.