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丙谷胺,一种胃泌素受体拮抗剂,可抑制结肠癌的生长并提高小鼠的生存率。

Proglumide, a gastrin receptor antagonist, inhibits growth of colon cancer and enhances survival in mice.

作者信息

Beauchamp R D, Townsend C M, Singh P, Glass E J, Thompson J C

出版信息

Ann Surg. 1985 Sep;202(3):303-9. doi: 10.1097/00000658-198509000-00005.

Abstract

Some tumors are responsive to hormone manipulation. Some gastric and colonic adenocarcinomas from both humans and animals have specific gastrin receptors. A transplantable mouse colon adenocarcinoma cell line (MC-26) contains gastrin receptors; growth of MC-26 colon cancer in vivo is stimulated by pentagastrin (PG). The purpose of this study was to determine whether a gastrin-receptor antagonist, proglumide (PGL), would inhibit growth of MC-26 colon cancer and prolong survival in tumor-bearing mice. Subcutaneous tumors were induced by injecting single-cell suspensions of MC-26 cells into 50 mice divided into 10/group. In Experiment 1, all mice received 1 X 10(5) tumor cells and treatment groups were divided as follows: Group A received intraperitoneal (IP) saline (0.2 ml tid beginning on day 1); B, IP, PGL (250 mg/kg tid) from day of tumor cell inoculation; and C, IP PGL (250 mg/kg tid) from day 7 after tumor implantation. In Experiment 2, mice were inoculated with half the number of tumor cells. Group I mice received saline and Group II received PGL in the same manner starting on day 1. Tumors were measured and all mice were sacrificed on day 23. In Experiment 1, mean tumor area in Group B (PGL-treated) was significantly smaller than Group A on days 11, 14, 17, and 21. Tumors of Group C were significantly smaller than controls on day 21. Survival of PGL-treated mice was significantly prolonged. In Experiment 2, mean tumor area, mean tumor weight, and tumor DNA and RNA content were significantly less in the PGL-treated group than control. It was concluded that growth of a gastrin-responsive colon cancer was inhibited and host survival was enhanced by treatment with a gastrin-receptor antagonist. Hormone manipulation may be a useful treatment for gastrointestinal cancers.

摘要

某些肿瘤对激素调控有反应。人和动物的一些胃及结肠腺癌具有特定的胃泌素受体。一种可移植的小鼠结肠腺癌细胞系(MC - 26)含有胃泌素受体;五肽胃泌素(PG)可刺激MC - 26结肠癌在体内生长。本研究的目的是确定胃泌素受体拮抗剂丙谷胺(PGL)是否会抑制MC - 26结肠癌的生长并延长荷瘤小鼠的生存期。将MC - 26细胞单细胞悬液注射到50只小鼠体内诱导皮下肿瘤形成,将小鼠分为10组。在实验1中,所有小鼠均接种1×10⁵个肿瘤细胞,治疗组划分如下:A组腹腔注射生理盐水(从第1天开始,0.2 ml,每日3次);B组从接种肿瘤细胞之日起腹腔注射丙谷胺(250 mg/kg,每日3次);C组在肿瘤植入后第7天开始腹腔注射丙谷胺(250 mg/kg,每日3次)。在实验2中,小鼠接种一半数量的肿瘤细胞。I组小鼠从第1天开始以相同方式接受生理盐水,II组接受丙谷胺。测量肿瘤大小,所有小鼠在第23天处死。在实验1中,B组(丙谷胺治疗组)在第11、14、17和21天的平均肿瘤面积显著小于A组。C组肿瘤在第21天显著小于对照组。丙谷胺治疗组小鼠的生存期显著延长。在实验2中,丙谷胺治疗组的平均肿瘤面积、平均肿瘤重量以及肿瘤DNA和RNA含量均显著低于对照组。得出的结论是,胃泌素受体拮抗剂治疗可抑制胃泌素反应性结肠癌的生长并提高宿主的生存率。激素调控可能是胃肠道癌症的一种有效治疗方法。

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