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Molecular targeted approaches for treatment of pancreatic cancer.

机译:分子靶向治疗胰腺癌的方法。

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Human pancreatic cancer remains a highly malignant disease with almost similar incidence and mortality despite extensive research. Many targeted therapies are under development. However, clinical investigation showed that single targeted therapies and most combined therapies were not able to improve the prognosis of this disease, even though some of these therapies had excellent anti-tumor effects in pre-clinical models. Cross-talk between cell proliferation signaling pathways may be an important phenomenon in pancreatic cancer, which may result in cancer cell survival even though some pathways are blocked by targeted therapy. Pancreatic cancer may possess different characteristics and targets in different stages of pathogenesis, maintenance and metastasis. Sensitivity to therapy may also vary for cancer cells at different stages. The unique pancreatic cancer structure with abundant stroma creates a tumor microenvironment with hypoxia and low blood perfusion rate, which prevents drug delivery to cancer cells. In this review, the most commonly investigated targeted therapies in pancreatic cancer treatment are discussed. However, how to combine these targeted therapies and/or combine them with chemotherapy to improve the survival rate of pancreatic cancer is still a challenge. Genomic and proteomic studies using pancreatic cancer samples obtained from either biopsy or surgery are recommended to individualize tumor characters and to perform drug sensitivity study in order to design a tailored therapy with minimal side effects. These studies may help to further investigate tumor pathogenesis, maintenance and metastasis to create cellular expression profiles at different stages. Integration of the information obtained needs to be performed from multiple levels and dimensions in order to develop a successful targeted therapy.
机译:尽管进行了广泛的研究,人类胰腺癌仍然是高度恶性的疾病,其发病率和死亡率几乎相似。许多靶向疗法正在开发中。然而,临床研究表明,即使其中一些疗法在临床前模型中具有出色的抗肿瘤作用,单一靶向疗法和大多数联合疗法也无法改善该疾病的预后。细胞增殖信号通路之间的串扰可能是胰腺癌中的重要现象,即使某些通路被靶向治疗所阻断,也可能导致癌细胞存活。胰腺癌在发病,维持和转移的不同阶段可能具有不同的特征和靶标。癌细胞在不同阶段对治疗的敏感性也可能不同。具有丰富基质的独特胰腺癌结构可形成具有低氧和低血液灌注率的肿瘤微环境,从而阻止了药物向癌细胞的传递。在这篇综述中,讨论了胰腺癌治疗中最常研究的靶向疗法。然而,如何结合这些靶向疗法和/或将它们与化学疗法结合以提高胰腺癌的存活率仍然是一个挑战。建议使用从活检或手术中获得的胰腺癌样本进行基因组和蛋白质组学研究,以个性化肿瘤特征并进行药物敏感性研究,以设计出量身定制的副作用最小的疗法。这些研究可能有助于进一步研究肿瘤的发病机理,维持和转移,以在不同阶段建立细胞表达谱。为了开发成功的靶向治疗,需要从多个层次和维度进行信息集成。

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