Modeling rectal cancer to advance neoadjuvant precision therapy

克拉斯 结直肠癌 医学 西妥昔单抗 癌症 新辅助治疗 肿瘤科 生物标志物 放射治疗 类有机物 内科学 人口 靶向治疗 癌症研究 病理 生物 生物化学 遗传学 环境卫生 乳腺癌
作者
Harinarayanan Janakiraman,Yun Zhu,Scott A. Becker,Cindy Wang,Ashley W. Cross,Emily Curl,David Lewin,Brenda J. Hoffman,Graham Warren,Elizabeth G. Hill,Cynthia Timmers,Victoria J. Findlay,E. Ramsay Camp
出处
期刊:International Journal of Cancer [Wiley]
卷期号:147 (5): 1405-1418 被引量:30
标识
DOI:10.1002/ijc.32876
摘要

Progress in rectal cancer therapy has been hindered by the lack of effective disease-specific preclinical models that account for the unique molecular profile and biology of rectal cancer. Thus, we developed complementary patient-derived xenograft (PDX) and subsequent in vitro tumor organoid (PDTO) platforms established from preneoadjuvant therapy rectal cancer specimens to advance personalized care for rectal cancer patients. Multiple endoscopic samples were obtained from 26 Stages 2 and 3 rectal cancer patients prior to receiving 5FU/RT and implanted subcutaneously into NSG mice to generate 15 subcutaneous PDXs. Second passaged xenografts demonstrated 100% correlation with the corresponding human cancer histology with maintained mutational profiles. Individual rectal cancer PDXs reproduced the 5FU/RT response observed in the corresponding human cancers. Similarly, rectal cancer PDTOs reproduced significant heterogeneity in cellular morphology and architecture. PDTO in vitro 5FU/RT treatment response replicated the clinical 5FU/RT neoadjuvant therapy pathologic response observed in the corresponding patient tumors (p < 0.05). The addition of cetuximab to the 5FU/RT regiment was significantly more sensitive in the rectal cancer PDX and PDTOs with wild-type KRAS compared to mutated KRAS (p < 0.05). Considering the close relationship between the patient's cancer and the corresponding PDX/PDTO, rectal cancer patient-derived research platforms represent powerful translational research resources as population-based tools for biomarker discovery and experimental therapy testing. In addition, our findings suggest that cetuximab may enhance RT effectiveness by improved patient selection based on mutational profile in addition to KRAS or by developing a protocol using PDTOs to identify sensitive patients.
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