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Rosiglitazone and imidapril alone or in combination alleviate muscle and adipose depletion in a murine cancer cachexia model

机译:罗格列酮和吡虫啉单独使用或联合使用可减轻鼠癌恶病质模型中的肌肉和脂肪消耗

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Rosiglitazone (RGZ) and imidapril improve cancer cachexia via different mechanisms. Therefore, we hypothesized that combination therapy of RGZ+imidapril would further attenuate cancer cachexia in vivo. After injection with colon-26 adenocarcinoma for 9 days, BALB/c mice were randomly divided into the following four treatment groups for 7 days (n = 8 per group): (1) placebo, (2) RGZ, (3) imidapril, and (4) RGZ+imidapril. Eight healthy control animals were also assessed. Body weight, tumor volume, gastrocnemius muscle and epididymal adipose mass, serum metabolic markers and cytokines, and the expression of nuclear factor-κB and two E3 ubiquitin ligases, atrogin-1 and MuRF-1, were measured. From days 14 to 16, all treatments significantly reduced tumor volume (P < 0.05). From days 10 to 16, improvements in the tumor-free body weight were observed in the RGZ and RGZ+imidapril groups. In addition, significant improvements in both gastrocnemius muscle and epididymal adipose mass were observed in all treatment groups (all, P < 0.05). Furthermore, all treatments significantly increased tumor necrosis factor alpha levels as compared to those observed in the healthy control animals (P < 0.001). Insulin levels significantly increased in the placebo group as compared to those in the healthy control group (P < 0.05), which were reduced in all the treatment groups (P < 0.05). Finally, whereas all treatments significantly reduced atrogin-1 levels as compared to the placebo group (all, P < 0.05), significant reductions in MuRF-1 levels were only observed in the RGZ and RGZ+imidapril groups (both, P < 0.05). Thus, all three treatments reduce tumor growth and alleviate cancer cachexia; however, synergistic effects of RGZ+imidapril combination therapy were not observed.
机译:罗格列酮(RGZ)和吡虫啉通过不同的机制改善癌症恶病质。因此,我们假设RGZ +咪达普利的联合治疗将进一步减轻体内癌症恶病质。在将结肠26腺癌注射9天后,将BALB / c小鼠随机分为以下四个治疗组,持续7天(每组n = 8):( 1)安慰剂,(2)RGZ,(3)吡虫啉, (4)RGZ +咪达普利。还评估了八只健康对照动物。测量体重,肿瘤体积,腓肠肌和附睾脂肪量,血清代谢标志物和细胞因子,以及核因子-κB和两种E3泛素连接酶atrogin-1和MuRF-1的表达。从第14天到第16天,所有治疗均显着降低肿瘤体积(P <0.05)。从第10天到第16天,在RGZ和RGZ +咪达普利组中观察到无瘤体重的改善。此外,在所有治疗组中均观察到腓肠肌和附睾脂肪质量均显着改善(所有,P <0.05)。此外,与在健康对照动物中观察到的那些治疗相比,所有治疗均显着增加了肿瘤坏死因子α水平(P <0.001)。与健康对照组相比,安慰剂组的胰岛素水平显着升高(P <0.05),而在所有治疗组中胰岛素水平均降低(P <0.05)。最后,尽管与安慰剂组相比,所有治疗均显着降低atrogin-1水平(所有,P <0.05),但仅在RGZ和RGZ +咪达普利组中观察到了MuRF-1水平的显着降低(两者,P <0.05) 。因此,这三种治疗均会降低肿瘤的生长并减轻癌症恶病质。然而,未观察到RGZ +咪达普利联合治疗的协同作用。

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