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人前列腺癌LNCaP模型中的雄激素非依赖性癌症进展和骨转移。

Androgen-independent cancer progression and bone metastasis in the LNCaP model of human prostate cancer.

作者信息

Thalmann G N, Anezinis P E, Chang S M, Zhau H E, Kim E E, Hopwood V L, Pathak S, von Eschenbach A C, Chung L W

机构信息

Department of Urology, University of Texas M.D. Anderson Cancer Center, Houston 77030.

出版信息

Cancer Res. 1994 May 15;54(10):2577-81.

PMID:8168083
Abstract

Our laboratory has previously reported on the derivation of LNCaP cell sublines from LNCaP tumors maintained in castrated and intact athymic male mice. These LNCaP sublines differ from the parental line in tumorigenicity and androgen dependence. This paper demonstrates that one of these sublines acquired metastatic potential. When inoculated either s.c. or orthotopically, the C4-2 subline metastasized to the lymph node and bone with an incidence of 11-50%. Interestingly, the incidence of osseous metastasis was higher in castrated than in intact male hosts. We evaluated the chromosomal, immunohistochemical, and biochemical characteristics of the LNCaP sublines derived from C4-2 tumors that metastasized to the lymph node and bone. Cytogenetic analysis showed that all sublines were human and shared common marker chromosomes with the parental LNCaP cells. This experimental human prostate cancer model may permit, for the first time, the study of the molecular mechanisms underlying human prostate cancer metastasis.

摘要

我们实验室之前曾报道过,从在去势和未去势无胸腺雄性小鼠体内维持的LNCaP肿瘤中获得LNCaP细胞亚系。这些LNCaP亚系在致瘤性和雄激素依赖性方面与亲代细胞系不同。本文证明这些亚系之一获得了转移潜能。当皮下或原位接种时,C4-2亚系转移至淋巴结和骨骼,转移发生率为11%-50%。有趣的是,去势雄性宿主的骨转移发生率高于未去势雄性宿主。我们评估了从转移至淋巴结和骨骼的C4-2肿瘤衍生的LNCaP亚系的染色体、免疫组化和生化特征。细胞遗传学分析表明,所有亚系均为人类细胞,且与亲代LNCaP细胞共享共同的标记染色体。这种实验性人类前列腺癌模型可能首次允许对人类前列腺癌转移的分子机制进行研究。

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