Hepatic signal transducer and activator of transcription-3 signalling drives early-stage pancreatic cancer cachexia via suppressed ketogenesis

IF 9.4 1区 医学 Q1 GERIATRICS & GERONTOLOGY Journal of Cachexia Sarcopenia and Muscle Pub Date : 2024-04-17 DOI:10.1002/jcsm.13466
Paige C. Arneson-Wissink, Heike Mendez, Katherine Pelz, Jessica Dickie, Alexandra Q. Bartlett, Beth L. Worley, Stephanie M. Krasnow, Robert Eil, Aaron J. Grossberg
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Abstract

Background

Patients with pancreatic ductal adenocarcinoma (PDAC) often suffer from cachexia, a wasting syndrome that significantly reduces both quality of life and survival. Although advanced cachexia is associated with inflammatory signalling and elevated muscle catabolism, the early events driving wasting are poorly defined. During periods of nutritional scarcity, the body relies on hepatic ketogenesis to generate ketone bodies, and lipid metabolism via ketogenesis is thought to protect muscle from catabolizing during nutritional scarcity.

Methods

We developed an orthotopic mouse model of early PDAC cachexia in 12-week-old C57BL/6J mice. Murine pancreatic cancer cells (KPC) were orthotopically implanted into the pancreas of wild-type, IL-6−/−, and hepatocyte STAT3−/− male and female mice. Mice were subject to fasting, 50% food restriction, ad libitum feeding or ketogenic diet interventions. We measured longitudinal body composition by EchoMRI, body mass and food intake. At the endpoint, we measured tissue mass, tissue gene expression by quantitative real-time polymerase chain reaction, whole-body calorimetry, circulating hormone levels, faecal protein and lipid content, hepatic lipid content and ketogenic response to medium-chain fatty acid bolus. We assessed muscle atrophy in vivo and C2C12 myotube atrophy in vitro.

Results

Pre-cachectic PDAC mice did not preserve gastrocnemius muscle mass during 3-day food restriction (−13.1 ± 7.7% relative to food-restricted sham, P = 0.0117) and displayed impaired fatty acid oxidation during fasting, resulting in a hypoketotic state (ketogenic response to octanoate bolus, −83.0 ± 17.3%, P = 0.0328; Hmgcs2 expression, −28.3 ± 7.6%, P = 0.0004). PDAC human patients display impaired fasting ketones (−46.9 ± 7.1%, P < 0.0001) and elevated circulating interleukin-6 (IL-6) (12.4 ± 16.5-fold increase, P = 0.0001). IL-6−/− PDAC mice had improved muscle mass (+35.0 ± 3.9%, P = 0.0031) and ketogenic response (+129.4 ± 44.4%, P = 0.0033) relative to wild-type PDAC mice. Hepatocyte-specific signal transducer and activator of transcription 3 (STAT3) deletion prevented muscle loss (+9.3 ± 4.0%, P = 0.009) and improved fasting ketone levels (+52.0 ± 43.3%, P = 0.018) in PDAC mice. Without affecting tumour growth, a carbohydrate-free diet improved tibialis anterior myofibre diameter (+16.5 ± 3.5%, P = 0.0089), circulating ketone bodies (+333.0 ± 117.6%, P < 0.0001) and Hmgcs2 expression (+106.5 ± 36.1%, P < 0.0001) in PDAC mice. Ketone supplementation protected muscle against PDAC-induced atrophy in vitro (+111.0 ± 17.6%, P < 0.0001 myofibre diameter).

Conclusions

In early PDAC cachexia, muscle vulnerability to wasting is dependent on inflammation-driven metabolic reprogramming in the liver. PDAC suppresses lipid β-oxidation and impairs ketogenesis in the liver, which is reversed in genetically modified mouse models deficient in IL-6/STAT3 signalling or through ketogenic diet supplementation. This work establishes a direct link between skeletal muscle homeostasis and hepatic metabolism. Dietary and anti-inflammatory interventions that restore ketogenesis may be a viable preventative approach for pre-cachectic patients with pancreatic cancer.

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肝脏信号转导和转录激活因子-3 信号通过抑制酮体生成驱动早期胰腺癌恶病质的发生
背景胰腺导管腺癌(PDAC)患者经常会出现恶病质,这是一种消瘦综合征,会大大降低患者的生活质量和存活率。虽然晚期恶病质与炎症信号传导和肌肉分解代谢增加有关,但导致消瘦的早期事件还不十分明确。在营养匮乏期间,机体依靠肝脏生酮来生成酮体,而通过生酮进行的脂质代谢被认为能保护肌肉在营养匮乏期间不被分解。将小鼠胰腺癌细胞(KPC)正位植入野生型、IL-6-/-和肝细胞STAT3-/-雄性和雌性小鼠的胰腺中。对小鼠进行禁食、50%食物限制、自由采食或生酮饮食干预。我们通过 EchoMRI 测量纵向身体成分、体重和食物摄入量。在终点,我们测量了组织质量、通过实时聚合酶链式反应定量的组织基因表达、全身热量计、循环激素水平、粪便蛋白质和脂质含量、肝脏脂质含量以及对中链脂肪酸栓剂的生酮反应。我们对体内肌肉萎缩和体外 C2C12 肌管萎缩进行了评估。0117),并在禁食期间表现出脂肪酸氧化受损,导致低酮症状态(对辛酸栓的生酮反应,-83.0 ± 17.3%,P = 0.0328;Hmgcs2 表达,-28.3 ± 7.6%,P = 0.0004)。PDAC 人类患者显示出空腹酮体受损(-46.9 ± 7.1%,P = 0.0001)和循环白细胞介素-6(IL-6)升高(12.4 ± 16.5 倍,P = 0.0001)。与野生型 PDAC 小鼠相比,IL-6-/- PDAC 小鼠的肌肉质量(+35.0 ± 3.9%,P = 0.0031)和生酮反应(+129.4 ± 44.4%,P = 0.0033)均有所改善。肝细胞特异性信号转导和激活转录 3 (STAT3) 基因缺失可防止 PDAC 小鼠的肌肉损失(+9.3 ± 4.0%,P = 0.009),并改善空腹酮体水平(+52.0 ± 43.3%,P = 0.018)。在不影响肿瘤生长的情况下,无碳水化合物饮食可改善 PDAC 小鼠的胫骨前肌纤维直径(+16.5 ± 3.5%,P = 0.0089)、循环酮体(+333.0 ± 117.6%,P < 0.0001)和 Hmgcs2 表达(+106.5 ± 36.1%,P < 0.0001)。结论在早期 PDAC 恶病质中,肌肉易消瘦取决于肝脏中炎症驱动的代谢重编程。PDAC 会抑制肝脏中的脂质 β 氧化并损害酮体生成,而在缺乏 IL-6/STAT3 信号的转基因小鼠模型中或通过补充生酮饮食可逆转这种情况。这项研究建立了骨骼肌稳态与肝脏代谢之间的直接联系。对胰腺癌前期患者来说,恢复生酮的饮食和抗炎干预可能是一种可行的预防方法。
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来源期刊
Journal of Cachexia Sarcopenia and Muscle
Journal of Cachexia Sarcopenia and Muscle MEDICINE, GENERAL & INTERNAL-
CiteScore
13.30
自引率
12.40%
发文量
234
审稿时长
16 weeks
期刊介绍: The Journal of Cachexia, Sarcopenia and Muscle is a peer-reviewed international journal dedicated to publishing materials related to cachexia and sarcopenia, as well as body composition and its physiological and pathophysiological changes across the lifespan and in response to various illnesses from all fields of life sciences. The journal aims to provide a reliable resource for professionals interested in related research or involved in the clinical care of affected patients, such as those suffering from AIDS, cancer, chronic heart failure, chronic lung disease, liver cirrhosis, chronic kidney failure, rheumatoid arthritis, or sepsis.
期刊最新文献
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