Establishment and characterisation of patient-derived xenografts as paraclinical models for gastric cancer

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作者
Yoon Young Choi
Jae Eun Lee
Hyunki Kim
Moon Hee Sim
Ka-Kyung Kim
Gunho Lee
Hyoung-Il Kim
Ji Yeong An
Woo Jin Hyung
Choong-Bai Kim
Sung Hoon Noh
Sangwoo Kim
Jae-Ho Cheong
机构
[1] Yonsei University College of Medicine,Department of Surgery
[2] Yonsei Biomedical Research Institute,Department of Pathology
[3] Yonsei University College of Medicine,Department of Biochemistry & Molecular Biology
[4] Yonsei University College of Medicine,Department of Surgery
[5] Severance Biomedical Science Institute,Open NBI Convergence Technology Research Laboratory of Department of Surgery
[6] Yonsei University College of Medicine,undefined
[7] Brain Korea 21 PLUS Project for Medical Science,undefined
[8] Yonsei University College of Medicine,undefined
[9] Yonsei University College of Medicine,undefined
[10] Samsung Medical Center,undefined
[11] Sungkyunkwan University School of Medicine,undefined
[12] Yonsei University College of Medicine,undefined
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摘要
The patient-derived xenograft (PDX) model is emerging as a promising translational platform to duplicate the characteristics of tumours. However, few studies have reported detailed histological and genomic analyses for model fidelity and for factors affecting successful model establishment of gastric cancer. Here, we generated PDX tumours surgically-derived from 62 gastric cancer patients. Fifteen PDX models were successfully established (24.2%, 15/62) and passaged to maintain tumours in immune-compromised mice. Diffuse type and low tumour cell percentage were negatively correlated with success rates (p = 0.005 and p = 0.025, respectively), while reducing ex vivo and overall procedure times were positively correlated with success rates (p = 0.003 and p = 0.01, respectively). The histology and genetic characteristics of PDX tumour models were stable over subsequent passages. Lymphoma transformation occurred in five cases (33.3%, 5/15), and all were in the NOG mouse, with none in the nude mouse. Together, the present study identified Lauren classification, tumour cell percentages, and ex vivo times along with overall procedure times, as key determinants for successful PDX engraftment. Furthermore, genetic and histological characteristics were highly consistent between primary and PDX tumours, which provide realistic paraclinical models, enabling personalised development of treatment options for gastric cancer.
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