Susu Liu, Jianjun Lyu, Qian-qian Li, Xi Wu, Yanwei Yang, Guitao Huo, Qingfen Zhu, Ming Guo, Yuelei Shen, Sanlong Wang, Changfa Fan
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引用次数: 2
摘要
淋巴瘤是儿童第三大常见癌症,根据临床观察,t细胞淋巴瘤预后最差。迄今为止,尚未建立具有均匀外显率的淋巴瘤模型。在这项研究中,我们通过靶向来自C57BL/6J小鼠品系的胚胎干细胞,建立了p53缺陷小鼠模型。纯合子p53缺陷小鼠自发肿瘤发生率较高,恶性淋巴瘤自发发生率高(93.3%)。由于目前需要具有高表型一致性的肿瘤模型,我们通过向p53缺陷小鼠单次腹腔注射37.5或75 mg/kg n -甲基-n -亚硝基脲来建立淋巴瘤模型。在给予高浓度n -甲基-n -亚硝基脲的p53+/−小鼠中,100%发生淋巴瘤和视网膜变性,比先前报道的模型反应大得多。淋巴瘤的主要解剖部位为胸腺、脾脏、骨髓和淋巴结。胸腺和脾脏的诱导和自发淋巴瘤CD3抗原均呈阳性,流式细胞术检测到CD4和/或CD8细胞阳性。根据我们的观察和先前的数据,我们假设具有B6背景的小鼠容易发生淋巴瘤。
Generation of a uniform thymic malignant lymphoma model with C57BL/6J p53 gene deficient mice
Lymphoma is the third most common cancer diagnosed in children, and T-cell lymphoma has the worst prognosis based on clinical observations. To date, a lymphoma model with uniform penetrance has not yet been developed. In this study, we generated a p53 deficient mouse model by targeting embryonic stem cells derived from a C57BL/6J mouse strain. Homozygous p53 deficient mice exhibited a higher rate of spontaneous tumorigenesis, with a high spontaneous occurrence rate (93.3%) of malignant lymphoma. Because tumor models with high phenotypic consistency are currently needed, we generated a lymphoma model by a single intraperitoneal injection of 37.5 or 75 mg/kg N-methyl-N-nitrosourea to p53 deficient mice. Lymphoma and retinal degeneration occurred in 100% of p53+/− mice administered with higher concentrations of N-methyl-N-nitrosourea, a much greater response than those of previously reported models. The main anatomic sites of lymphoma were the thymus, spleen, bone marrow, and lymph nodes. Both induced and spontaneous lymphomas in the thymus and spleen stained positive for CD3 antigen, and flow cytometry detected positive CD4 and/or CD8 cells. Based on our observations and previous data, we hypothesize that mice with a B6 background are prone to lymphomagenesis.
期刊介绍:
JTP is a scientific journal that publishes original studies in the field of toxicological pathology and in a wide variety of other related fields. The main scope of the journal is listed below.
Administrative Opinions of Policymakers and Regulatory Agencies
Adverse Events
Carcinogenesis
Data of A Predominantly Negative Nature
Drug-Induced Hematologic Toxicity
Embryological Pathology
High Throughput Pathology
Historical Data of Experimental Animals
Immunohistochemical Analysis
Molecular Pathology
Nomenclature of Lesions
Non-mammal Toxicity Study
Result or Lesion Induced by Chemicals of Which Names Hidden on Account of the Authors
Technology and Methodology Related to Toxicological Pathology
Tumor Pathology; Neoplasia and Hyperplasia
Ultrastructural Analysis
Use of Animal Models.