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在小鼠中,围手术期用Flt3配体进行免疫调节后,剖腹手术相关的肺转移和皮下肿瘤显著减少。

Significant reduction of laparotomy-associated lung metastases and subcutaneous tumors after perioperative immunomodulation with flt3 ligand in mice.

作者信息

Carter Joseph J, Feingold Daniel L, Wildbrett Peer, Oh Anthony, Kirman Irena, Asi Zishan, Stapleton George, Huang Emina, Fine Robert L, Whelan Richard L

机构信息

Laparoscopic Physiology and Oncology Laboratory, Department of Surgery, College of Physician and Surgeons, Columbia University, New York, NY 10032, USA.

出版信息

Surg Innov. 2005 Dec;12(4):319-25. doi: 10.1177/155335060501200406.

Abstract

Laparotomy has been associated with increased rates of tumor establishment and metastasis formation postoperatively in animal models. The purpose of this study was to determine the impact on postoperative tumor growth of perioperative upregulation of immune function via fetal liver tyrosine kinase 3 (Flt3 ligand). Two murine studies were carried out: the first utilized a lung metastases model, and the second involved a subcutaneous tumor model. Each study included four groups: anesthesia control (AC), AC plus Flt3 ligand (ACFlt3), sham laparotomy (OP), and OP plus Flt3 ligand (OPFlt3). Flt3 ligand was administered by daily intraperitoneal injection (10 mug/dose) beginning 5 days preoperatively and continuing for 1 week postoperatively. In study 1, A/J mice were given tail vein injections of 1.5 x 10(5) TA3Ha cancer cells on the day of surgery. The mice were sacrificed 14 days after surgery, the lungs processed, and the surface metastases counted by a blinded observer. In study 2 C3H/He mice were given a dorsal subcutaneous injection of 10(4) MC-2 cancer cells on the day of surgery. The mice were sacrificed 31 days after surgery, and the injection sites were evaluated for subcutaneous tumors grossly and histologically. In study 1, the median number of surface lung metastases per mouse was 166 in the OP group and 38 in the OPFlt3 (P = .021). Mice in the AC group developed a median 50 lung metastases per animal compared with mice in the ACFlt3 group who had a median of 10 metastases per mouse (P = .001). The OP group had significantly more metastases than the AC group (P = .048). In study 2, the percentage of animals that developed tumors in the AC, OP, ACFlt3, and OPFlt3 groups was 43, 80, 0, and 20, respectively. The incidence of tumors in the OPFLt3 group and the ACFlt3 group was significantly less than their respective control groups (P < .01). The difference between the OP and AC groups was not significant (P > .05). Perioperatively administered Flt3 ligand was associated with significantly fewer lung metastases and a lower incidence of subcutaneous tumor formation after laparotomy and anesthesia alone. Perioperative immunomodulation may limit untoward surgery-related oncologic effects.

摘要

在动物模型中,剖腹手术与术后肿瘤形成率和转移形成率增加有关。本研究的目的是确定通过胎儿肝酪氨酸激酶3(Flt3配体)围手术期上调免疫功能对术后肿瘤生长的影响。进行了两项小鼠研究:第一项采用肺转移模型,第二项涉及皮下肿瘤模型。每项研究包括四组:麻醉对照组(AC)、AC加Flt3配体组(ACFlt3)、假剖腹手术组(OP)和OP加Flt3配体组(OPFlt3)。Flt3配体通过每日腹腔注射给药(10微克/剂量),从术前5天开始,持续至术后1周。在研究1中,手术当天给A/J小鼠尾静脉注射1.5×10⁵个TA3Ha癌细胞。术后14天处死小鼠,处理肺组织,由一位不知情的观察者计数表面转移灶。在研究2中,手术当天给C3H/He小鼠背部皮下注射10⁴个MC - 2癌细胞。术后31天处死小鼠,对注射部位进行大体和组织学皮下肿瘤评估。在研究1中,OP组每只小鼠表面肺转移灶的中位数为166个,OPFlt3组为38个(P = 0.021)。AC组每只动物肺转移灶的中位数为50个,而ACFlt3组每只小鼠的中位数为10个转移灶(P = 0.001)。OP组的转移灶明显多于AC组(P = 0.048)。在研究2中,AC、OP、ACFlt3和OPFlt3组发生肿瘤的动物百分比分别为43%、80%、0%和20%。OPFLt3组和ACFlt3组的肿瘤发生率明显低于各自的对照组(P < 0.01)。OP组和AC组之间的差异不显著(P > 0.05)。围手术期给予Flt3配体与单独剖腹手术和麻醉后肺转移明显减少以及皮下肿瘤形成发生率降低有关。围手术期免疫调节可能会限制与手术相关的不良肿瘤学效应。

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