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一种用于局部晚期乳腺癌的新型动物模型。

A novel animal model for locally advanced breast cancer.

作者信息

Bogachek Maria V, Park Jung Min, De Andrade James P, Kulak Mikhail V, White Jeffrey R, Wu Tong, Spanheimer Philip M, Bair Thomas B, Olivier Alicia K, Weigel Ronald J

机构信息

Department of Surgery, University of Iowa, Iowa City, IA, USA.

出版信息

Ann Surg Oncol. 2015 Mar;22(3):866-73. doi: 10.1245/s10434-014-4174-8. Epub 2014 Oct 18.

Abstract

BACKGROUND

Locally advanced breast cancer (LABC) poses complex management issues due to failure of response to chemotherapy and progression to local complications such as skin erosion, superinfection, and lymphedema. Most cell line and animal models are not adequate to study LABC.

METHODS

A patient-derived xenograft (IOWA-1T) from a patient with LABC was characterized for expression profile, short tandem repeat profile, oncogenic mutations, xenograft growth, and response to therapy.

RESULTS

Short tandem repeat profile authenticated the cell line as derived from a human woman. The primary tumor and derived xenografts were weakly estrogen receptor alpha positive (<5%), progesterone receptor negative, and HER2 nonamplified. Expression array profile compared to MCF-7 and BT-549 cell lines indicate that IOWA-1T was more closely related to basal breast cancer. IOWA-1T harbors a homozygous R248Q mutation of the TP53 gene; in vitro invasion assay was comparable to BT-549 and greater than MCF-7. IOWA-1T xenografts developed palpable tumors in 9.6 ± 1.6 days, compared to 49 ± 13 days for parallel experiments with BT-20 cells (p < 0.002). Tumor xenografts became locally advanced, growing to >2 cm in 21.6 ± 2 days, characterized by skin erosion necessitating euthanasia. The SUMO inhibitor anacardic acid inhibited the outgrowth of IOWA-1T xenografts, while doxorubicin had no effect on tumorigenesis.

CONCLUSIONS

IOWA-1T is a novel cell line with an expression pattern consistent with basal breast cancer. Xenografts recapitulated LABC and provide a novel model for testing therapeutic drugs that may be effective in cases resistant to conventional chemotherapy.

摘要

背景

局部晚期乳腺癌(LABC)因对化疗无反应以及进展为局部并发症(如皮肤糜烂、继发感染和淋巴水肿)而带来复杂的管理问题。大多数细胞系和动物模型不足以用于研究局部晚期乳腺癌。

方法

对一名局部晚期乳腺癌患者的患者来源异种移植瘤(IOWA-1T)进行了表达谱、短串联重复序列谱、致癌突变、异种移植瘤生长及对治疗反应的特征分析。

结果

短串联重复序列谱证实该细胞系源自一名人类女性。原发肿瘤及衍生的异种移植瘤雌激素受体α弱阳性(<5%)、孕激素受体阴性且HER2未扩增。与MCF-7和BT-549细胞系相比,表达阵列谱表明IOWA-1T与基底样乳腺癌关系更为密切。IOWA-1T携带TP53基因的纯合R248Q突变;体外侵袭试验结果与BT-549相当且高于MCF-7。IOWA-1T异种移植瘤在9.6±1.6天出现可触及肿瘤,而BT-20细胞平行实验为49±13天(p<0.002)。肿瘤异种移植瘤发展为局部晚期,在21.6±2天内生长至>2 cm,其特征为皮肤糜烂,最终需要实施安乐死。SUMO抑制剂没食子酸抑制了IOWA-1T异种移植瘤的生长,而阿霉素对肿瘤发生无影响。

结论

IOWA-1T是一种新型细胞系,其表达模式与基底样乳腺癌一致。异种移植瘤重现了局部晚期乳腺癌的特征,并为测试可能对传统化疗耐药病例有效的治疗药物提供了一种新模型。

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