Utilizing gastric cancer organoids to assess tumor biology and personalize medicine

被引:0
作者
Miranda Lin [1 ]
Mei Gao [1 ]
Michael J Cavnar [1 ]
Joseph Kim [1 ]
机构
[1] Department of Surgery, University of Kentucky
关键词
Organoids; Gastric cancer; Cancer models; Drug sensitivity; Drug screening; Personalized medicine;
D O I
暂无
中图分类号
R735.2 [胃肿瘤];
学科分类号
100214 ;
摘要
While the incidence and mortality of gastric cancer(GC) have declined due to public health programs, it remains the third deadliest cancer worldwide. For patients with early disease, innovative endoscopic and complex surgical techniques have improved survival. However, for patients with advanced disease, there are limited treatment options and survival remains poor. Therefore,there is an urgent need for more effective therapies. Since novel therapies require extensive preclinical testing prior to human trials, it is important to identify methods to expedite this process. Traditional cancer models are restricted by the inability to accurately recapitulate the primary human tumor, exorbitant costs,and the requirement for extended periods of development time. An emerging in vitro model to study human disease is the patient-derived organoid, which is a three-dimensional system created from fresh surgical or biopsy tissues of a patient’s gastric tumor. Organoids are cultured in plastic wells and suspended in a gelatinous matrix, providing a substrate for extension and growth in all dimensions. They are rapid-growing and highly representative of the molecular landscape, histology, and morphology of the various subtypes of GC. Organoids uniquely model tumor initiation and growth, including steps taken by normal stomach cells to transform into invasive, intestinal-type tumor cells. Additionally,they provide ample material for biobanking and screening novel therapies.Lastly, organoids are a promising model for personalized therapy and warrant further investigation in drug sensitivity studies for GC patients.
引用
收藏
页码:509 / 517
页数:9
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