胰腺癌
Pancreatic cancer.
作者信息
Maitra Anirban, Hruban Ralph H
机构信息
Department of Pathology, The Sol Goldman Pancreatic Cancer Research Center, Johns Hopkins University School of Medicine, Baltimore, MD 21231, USA.
出版信息
Annu Rev Pathol. 2008;3:157-88. doi: 10.1146/annurev.pathmechdis.3.121806.154305.
Abstract
The past two decades have witnessed an explosion in our understanding of pancreatic cancer, and it is now clear that pancreatic cancer is a disease of inherited (germ-line) and somatic gene mutations. The genes mutated in pancreatic cancer include KRAS2, p16/CDKN2A, TP53, and SMAD4/DPC4, and these are accompanied by a substantial compendium of genomic and transcriptomic alterations that facilitate cell cycle deregulation, cell survival, invasion, and metastases. Pancreatic cancers do not arise de novo, and three distinct precursor lesions have been identified. Experimental models of pancreatic cancer have been developed in genetically engineered mice, which recapitulate the multistep progression of the cognate human disease. Although the putative cell of origin for pancreatic cancer remains elusive, minor populations of cells with stem-like properties have been identified that appear responsible for tumor initiation, metastases, and resistance of pancreatic cancer to conventional therapies.
摘要
在过去二十年里,我们对胰腺癌的认识有了极大的飞跃,现在很清楚胰腺癌是一种由遗传性(种系)和体细胞基因突变引起的疾病。胰腺癌中发生突变的基因包括KRAS2、p16/CDKN2A、TP53和SMAD4/DPC4,同时还伴随着大量的基因组和转录组改变,这些改变促进了细胞周期失调、细胞存活、侵袭和转移。胰腺癌并非凭空出现,已鉴定出三种不同的前驱病变。在基因工程小鼠中建立了胰腺癌实验模型,该模型概括了相关人类疾病的多步骤进展。尽管胰腺癌假定的起源细胞仍不清楚,但已鉴定出具有干细胞样特性的少量细胞群体,这些细胞似乎是胰腺癌起始、转移以及对传统疗法产生抗性的原因。
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