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Pharmacological dual inhibition of tumor and tumor-induced functional limitations in transgenic model of breast cancer

机译:乳腺癌转基因模型中肿瘤的药理双重抑制和肿瘤诱导的功能限制

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Breast cancer progression is associated with systemic effects including functional limitations and sarcopenia without the appearance of overt cachexia. Autocrine/paracrine actions of cytokines/chemokines produced by cancer cells mediate cancer progression and functional limitations. The cytokine-inducible transcription factor NF-κB could be central to this process, as it displays oncogenic functions and is integral to the Pax7:MyoD:Pgc-1β:miR-486 myogenesis axis. We tested this possibility using the MMTV-PyMT transgenic mammary tumor model and the NF-κB inhibitor dimethylaminoparthenolide (DMAPT). We observed deteriorating physical and functional conditions in PyMT+ mice with disease progression. Compared to wild type mice, tumor-bearing PyMT+ mice showed decreased fat mass, impaired rotarod performance, and reduced grip strength as well as increased extracellular matrix (ECM) deposition in muscle. Contrary to acute cachexia models described in the literature, mammary tumor progression was associated with reduction in skeletal muscle stem/satellite-specific transcription factor Pax7. Additionally, we observed tumor-induced reduction in Pgc-1β in muscle, which controls mitochondrial biogenesis. DMAPT treatment starting at 6-8 weeks age prior to mammary tumor occurrence delayed mammary tumor onset and tumor growth rates without affecting metastasis. DMAPT overcame cancer-induced functional limitations and improved survival, which was accompanied with restoration of Pax7, Pgc-1β, and mitochondria levels and reduced ECM levels in skeletal muscles. In addition, DMAPT restored circulating levels of six out of 13 cancer-associated cytokines/chemokines changes to levels seen in healthy animals. These results reveal a pharmacological approach for overcoming cancer-induced functional limitations and the above noted cancer/drug-induced changes in muscle gene expression could be utilized as biomarkers of functional limitations.
机译:乳腺癌的进展与全身功能相关,包括功能受限和肌肉减少症,而不会出现明显的恶病质。癌细胞产生的细胞因子/趋化因子的自分泌/旁分泌作用介导了癌症的进展和功能限制。细胞因子诱导的转录因子NF-κB可能是这一过程的中心,因为它显示致癌功能,并且是Pax7:MyoD:Pgc-1β:miR-486肌生成轴所必需的。我们使用MMTV-PyMT转基因乳腺肿瘤模型和NF-κB抑制剂二甲基氨基单酚(DMAPT)测试了这种可能性。我们观察到PyMT + 小鼠随着疾病发展而恶化的身体和功能状况。与野生型小鼠相比,荷瘤的PyMT + 小鼠脂肪减少,旋转杆性能下降,抓地力降低,肌肉中细胞外基质(ECM)沉积增加。与文献中描述的急性恶病质模型相反,乳腺肿瘤进展与骨骼肌干/卫星特异性转录因子Pax7减少有关。此外,我们观察到肿瘤诱导的肌肉Pgc-1β减少,从而控制线粒体的生物发生。在乳腺肿瘤发生之前的6-8周龄开始的DMAPT治疗可延迟乳腺肿瘤的发作和肿瘤的生长速度,而不会影响转移。 DMAPT克服了癌症引起的功能局限性并提高了生存率,伴随着Pax7,Pgc-1β和线粒体水平的恢复以及骨骼肌中ECM水平的降低。此外,DMAPT将13种与癌症相关的细胞因子/趋化因子变化中的6种的循环水平恢复到健康动物体内的水平。这些结果揭示了克服癌症诱导的功能限制的药理学方法,并且上述癌症/药物诱导的肌肉基因表达的改变可以用作功能限制的生物标记。

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