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首页> 外文期刊>Clinical cancer research: an official journal of the American Association for Cancer Research >Pancreatic Cancer: 'A Riddle Wrapped in a Mystery inside an Enigma'
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Pancreatic Cancer: 'A Riddle Wrapped in a Mystery inside an Enigma'

机译:胰腺癌:“一个谜团裹在谜内的谜团”

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Pancreatic ductal adenocarcinoma (PDAC) is one of the most difficult-to-treat cancers. With an increasing incidence and inability to make major progress, it represents the very definition of unmet medical need. Progress has been made in understanding the basic biology-systematic genomic sequencing has led to the recognition that PDAC is not typically a heavily mutated tumor, although there are exceptions. The most consistently mutated genes are KRAS, CDKN2A, TP53, and SMAD4/DPC4. Study of familial PDAChas led to the recognition that a variety of defects in DNA repair genes can be associated with the emergence of pancreatic cancer. Recent studies suggest that epigenetics may play a larger role than previously recognized. A major new understanding is the recognition that PDAC should be considered a composite of tumor cells, as well as pancreatic stellate cells, immune cells, and extracellular matrix. The individual components contribute to metabolic aberration, immune dysfunction, and chemotherapy resistance, and therapeutic innovationsmaybe needed to address them individually. It has also been recognized that metastatic seeding from PDAC occurs very early in the disease course-in an estimated 73% of cases, once the tumor reaches 2 cm. The implication of this is that therapies directed toward micrometastatic disease and increasing fractional cell kill are most needed. Neoadjuvant approaches have been taken to increase resectability and improve outcome. So much work remains, and most critical is the need to understand how this tumor originates and develops.
机译:胰腺导管腺癌(PDAC)是最难以治疗的癌症之一。随着发病率的增加和无法进行重大进展,它代表了未满足医疗需求的定义。在理解基础生物学系统基因组测序已经导致识别PDAC通常不突变肿瘤,尽管存在异常,但已经取得了进展。最常见的突变基因是KRA,CDKN2A,TP53和SMAD4 / DPC4。对家族性PDACHAS的研究导致了识别DNA修复基因的各种缺陷可以与胰腺癌的出现相关。最近的研究表明表观遗传学可能比以前认可的方式发挥更大的作用。主要的新理解是识别PDAC应该被认为是肿瘤细胞的复合物,以及胰腺星状细胞,免疫细胞和细胞外基质。各组分有助于代谢畸变,免疫功能障碍和化疗抵抗,以及治疗性创新需要单独解决它们。还认识到,一旦肿瘤达到2厘米,估计患者的疾病课程早期就会发生来自PDAC的转移性播种。对此的含义是,最需要针对微转移疾病和增加分数细胞杀灭的疗法。已经采取了新辅助的方法来增加重新分配和改善结果。这么多工作仍然存在,最重要的是需要了解这种肿瘤是如何源性和发展的。

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