胰腺癌诱导的恶病质及相关小鼠模型。
Pancreatic Cancer-Induced Cachexia and Relevant Mouse Models.
作者信息
Henderson Sally E, Makhijani Neil, Mace Thomas A
机构信息
Department of Internal Medicine, Division of Gastroenterology, Hepatology and Nutrition.
出版信息
Pancreas. 2018 Sep;47(8):937-945. doi: 10.1097/MPA.0000000000001124.
Abstract
Pancreatic cancer is the third leading cause of cancer death in the United States, with projections that it will become the second leading cause by the year 2030. It carries a dismal prognosis with a 5-year overall survival rate of less than 9% and is associated with numerous comorbidities, the most notable being cachexia. Defined as the loss of muscle mass not reversible by conventional nutritional support, cachexia is seen in over 85% of pancreatic cancer patients and contributes significantly to mortality, where nearly 30% of pancreatic cancer deaths are due to cachexia rather than tumor burden. Therefore, there is an urgent need to identify the mechanisms behind the development of muscle wasting in pancreatic cancer patients and design novel therapeutics targeting cachexia. This review highlights the current understanding surrounding the mechanisms underpinning the development of cachexia in pancreatic cancer, as well as the current mouse models of pancreatic cancer-induced muscle wasting described in the literature.
摘要
胰腺癌是美国癌症死亡的第三大主要原因,预计到2030年它将成为第二大主要原因。其预后不佳,5年总生存率低于9%,并且与多种合并症相关,最显著的是恶病质。恶病质被定义为常规营养支持无法逆转的肌肉量减少,超过85%的胰腺癌患者会出现恶病质,它对死亡率有显著影响,近30%的胰腺癌死亡是由恶病质而非肿瘤负荷导致的。因此,迫切需要确定胰腺癌患者肌肉萎缩发展背后的机制,并设计针对恶病质的新型疗法。本综述重点介绍了目前对胰腺癌恶病质发展机制的理解,以及文献中描述的当前胰腺癌诱导肌肉萎缩的小鼠模型。
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