Cachexia causes time-dependent activation of the inflammasome in the liver

IF 8.9 1区医学

Journal of Cachexia, Sarcopenia and Muscle Pub Date : 2023-05-12 DOI:10.1002/jcsm.13236

Rodrigo Xavier das Neves, Alex S. Yamashita, Daniela M.R. Riccardi, Julia K?hn-Gaone, Rodolfo G. Camargo, Nelson I. Neto, Daniela Caetano, Silvio P. Gomes, Felipe H. Santos, Joanna D.C.C. Lima, Miguel L. Batista Jr, José Cesar Rosa-Neto, Paulo Sérgio Martins De Alcantara, Linda F. Maximiano, José P. Otoch, Giorgio Trinchieri, Janina E.E. Tirnitz-Parker, Marília Seelaender

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Abstract

Background

Cachexia is a wasting syndrome associated with systemic inflammation and metabolic disruption. Detection of the early signs of the disease may contribute to the effective attenuation of associated symptoms. Despite playing a central role in the control of metabolism and inflammation, the liver has received little attention in cachexia. We previously described relevant disruption of metabolic pathways in the organ in an animal model of cachexia, and herein, we adopt the same model to investigate temporal onset of inflammation in the liver. The aim was thus to study inflammation in rodent liver in the well-characterized cachexia model of Walker 256 carcinosarcoma and, in addition, to describe inflammatory alterations in the liver of one cachectic colon cancer patient, as compared to one control and one weight-stable cancer patient.

Methods

Colon cancer patients (one weight stable [WSC] and one cachectic [CC]) and one patient undergoing surgery for cholelithiasis (control, n = 1) were enrolled in the study, after obtainment of fully informed consent. Eight-week-old male rats were subcutaneously inoculated with a Walker 256 carcinosarcoma cell suspension (2 × 10⁷ cells in 1.0 mL; tumour-bearing [T]; or phosphate-buffered saline—controls [C]). The liver was excised on Days 0 (n = 5), 7 (n = 5) and 14 (n = 5) after tumour cell injection.

Results

In rodent cachexia, we found progressively higher numbers of CD68⁺ myeloid cells in the liver along cancer-cachexia development. Similar findings are described for CC, whose liver showed infiltration of the same cell type, compared with both WSC and control patient organs. In advanced rodent cachexia, hepatic phosphorylated c-Jun N-terminal kinase protein content and the inflammasome pathway protein expression were increased in relation to baseline (P < 0.05). These changes were accompanied by augmented expression of the active interleukin-1β (IL-1β) form (P < 0.05 for both circulating and hepatic content).

Conclusions

The results show that cancer cachexia is associated with an increase in the number of myeloid cells in rodent and human liver and with modulation of hepatic inflammasome pathway. The latter contributes to the aggravation of systemic inflammation, through increased release of IL-1β.

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恶病质引起肝脏中炎性体的时间依赖性激活

背景恶病质是一种与全身炎症和代谢紊乱相关的消耗综合征。发现疾病的早期症状可能有助于有效地减轻相关症状。尽管肝脏在代谢和炎症的控制中起着核心作用，但在恶病质中却很少受到关注。我们之前在一个恶病质动物模型中描述了器官代谢途径的相关破坏，在这里，我们采用相同的模型来研究肝脏炎症的时间性发作。因此，目的是在具有良好特征的Walker 256癌肉瘤恶病质模型中研究啮齿动物肝脏中的炎症，此外，描述一名恶病质结肠癌患者肝脏中的炎症改变，与一名对照和一名体重稳定的癌症患者进行比较。方法在获得完全知情同意后，将1例体重稳定型(WSC)和1例重质型(CC)的结肠癌患者和1例接受胆石症手术的患者(对照组，n = 1)纳入研究。8周龄雄性大鼠皮下接种Walker 256癌肉瘤细胞悬液(2 × 107个细胞，1.0 mL;tumour-bearing [T];磷酸盐缓冲盐碱控制[C]。在注射肿瘤细胞后第0天(n = 5)、第7天(n = 5)和第14天(n = 5)切除肝脏。结果在啮齿类动物的恶病质中，我们发现随着癌症-恶病质的发展，肝脏中CD68+髓样细胞的数量逐渐增加。与WSC和对照患者器官相比，CC的肝脏浸润相同的细胞类型，也有类似的发现。在晚期啮齿动物恶病质中，肝脏磷酸化c-Jun n -末端激酶蛋白含量和炎性体途径蛋白表达与基线相比增加(P <0.05)。这些变化伴随着活性白介素-1β (IL-1β)形式的表达增强(P <循环和肝脏含量均为0.05)。结论肿瘤恶病质与鼠、人肝脏髓系细胞数量增加及肝炎性体通路调节有关。后者通过增加IL-1β的释放，有助于全身炎症的加重。

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来源期刊

Journal of Cachexia, Sarcopenia and Muscle Medicine-Orthopedics and Sports Medicine

自引率

12.40%

发文量

期刊介绍： The Journal of Cachexia, Sarcopenia, and Muscle is a prestigious, peer-reviewed international publication committed to disseminating research and clinical insights pertaining to cachexia, sarcopenia, body composition, and the physiological and pathophysiological alterations occurring throughout the lifespan and in various illnesses across the spectrum of life sciences. This journal serves as a valuable resource for physicians, biochemists, biologists, dieticians, pharmacologists, and students alike.