本地克氏锥虫钙网蛋白在感染期间是否介导乳腺肿瘤的生长抑制?
Does native Trypanosoma cruzi calreticulin mediate growth inhibition of a mammary tumor during infection?
作者信息
Abello-Cáceres Paula, Pizarro-Bauerle Javier, Rosas Carlos, Maldonado Ismael, Aguilar-Guzmán Lorena, González Carlos, Ramírez Galia, Ferreira Jorge, Ferreira Arturo
机构信息
Institute of Biomedical Sciences (ICBM), Faculty of Medicine, University of Chile, Avenida Independencia 1027, Independencia, Santiago, Chile.
Faculty of Veterinary Medicine and Livestock Sciences, University of Chile, Avenida Santa Rosa 11735, La Pintana, Santiago, Chile.
出版信息
BMC Cancer. 2016 Sep 13;16(1):731. doi: 10.1186/s12885-016-2764-5.
BACKGROUND
For several decades now an antagonism between Trypanosoma cruzi infection and tumor development has been detected. The molecular basis of this phenomenon remained basically unknown until our proposal that T. cruzi Calreticulin (TcCRT), an endoplasmic reticulum-resident chaperone, translocated-externalized by the parasite, may mediate at least an important part of this effect. Thus, recombinant TcCRT (rTcCRT) has important in vivo antiangiogenic and antitumor activities. However, the relevant question whether the in vivo antitumor effect of T. cruzi infection is indeed mediated by the native chaperone (nTcCRT), remains open. Herein, by using specific modified anti-rTcCRT antibodies (Abs), we have neutralized the antitumor activity of T. cruzi infection and extracts thereof, thus identifying nTcCRT as a valid mediator of this effect.
METHODS
Polyclonal anti-rTcCRT F(ab')2 Ab fragments were used to reverse the capacity of rTcCRT to inhibit EAhy926 endothelial cell (EC) proliferation, as detected by BrdU uptake. Using these F(ab')2 fragments, we also challenged the capacity of nTcCRT, during T. cruzi infection, to inhibit the growth of an aggressive mammary adenocarcinoma cell line (TA3-MTXR) in mice. Moreover, we determined the capacity of anti-rTcCRT Abs to reverse the antitumor effect of an epimastigote extract (EE). Finally, the effects of these treatments on tumor histology were evaluated.
RESULTS
The rTcCRT capacity to inhibit ECs proliferation was reversed by anti-rTcCRT F(ab')2 Ab fragments, thus defining them as valid probes to interfere in vivo with this important TcCRT function. Consequently, during infection, these Ab fragments also reversed the in vivo experimental mammary tumor growth. Moreover, anti-rTcCRT Abs also neutralized the antitumor effect of an EE, again identifying the chaperone protein as an important mediator of this anti mammary tumor effect. Finally, as determined by conventional histological parameters, in infected animals and in those treated with EE, less invasive tumors were observed while, as expected, treatment with F(ab')2 Ab fragments increased malignancy.
CONCLUSION
We have identified translocated/externalized nTcCRT as responsible for at least an important part of the anti mammary tumor effect of the chaperone observed during experimental infections with T. cruzi.
背景
几十年来,人们已检测到克氏锥虫感染与肿瘤发展之间存在拮抗作用。在我们提出寄生虫内质网驻留伴侣蛋白克氏锥虫钙网蛋白(TcCRT)易位并外化,可能至少介导了这种效应的重要部分之前,这一现象的分子基础基本未知。因此,重组TcCRT(rTcCRT)具有重要的体内抗血管生成和抗肿瘤活性。然而,克氏锥虫感染的体内抗肿瘤作用是否确实由天然伴侣蛋白(nTcCRT)介导这一相关问题仍未解决。在此,通过使用特异性修饰的抗rTcCRT抗体(Abs),我们中和了克氏锥虫感染及其提取物的抗肿瘤活性,从而确定nTcCRT是这种效应的有效介导因子。
方法
使用多克隆抗rTcCRT F(ab')2抗体片段来逆转rTcCRT抑制EAhy926内皮细胞(EC)增殖的能力,这通过BrdU摄取来检测。使用这些F(ab')2片段,我们还挑战了克氏锥虫感染期间nTcCRT抑制侵袭性乳腺癌细胞系(TA3-MTXR)在小鼠体内生长的能力。此外,我们确定了抗rTcCRT抗体逆转前鞭毛体提取物(EE)抗肿瘤作用的能力。最后,评估了这些处理对肿瘤组织学的影响。
结果
抗rTcCRT F(ab')2抗体片段逆转了rTcCRT抑制内皮细胞增殖的能力,从而将它们定义为在体内干扰这种重要的TcCRT功能的有效探针。因此,在感染期间,这些抗体片段也逆转了体内实验性乳腺肿瘤的生长。此外,抗rTcCRT抗体也中和了EE的抗肿瘤作用,再次确定伴侣蛋白是这种抗乳腺肿瘤作用的重要介导因子。最后,根据传统组织学参数确定,在感染动物和用EE处理的动物中,观察到侵袭性较小的肿瘤,而正如预期的那样,用F(ab')2抗体片段处理会增加恶性程度。
结论
我们已确定易位/外化的nTcCRT至少是在克氏锥虫实验感染期间观察到的伴侣蛋白抗乳腺肿瘤作用的重要部分的原因。
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