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源自单一骨转移灶的两个人前列腺癌细胞系的建立。

Establishment of two human prostate cancer cell lines derived from a single bone metastasis.

作者信息

Navone N M, Olive M, Ozen M, Davis R, Troncoso P, Tu S M, Johnston D, Pollack A, Pathak S, von Eschenbach A C, Logothetis C J

机构信息

The University of Texas M.D. Anderson Cancer Center, Houston, Texas 77030, USA.

出版信息

Clin Cancer Res. 1997 Dec;3(12 Pt 1):2493-500.

PMID:9815652
Abstract

Human prostate cancer cell lines are particularly difficult to establish, and most existing cell lines do not exhibit features commonly seen in human prostate cancer. Most available models either grow only in vivo as xenografts or are androgen insensitive and fail to express prostate-specific antigen (PSA). The lack of functionally relevant model systems of advanced prostate cancer has limited prostate cancer research and therapy development. Of 30 processed samples derived from patients with prostate cancer, we established two cell lines (MDA PCa 2a and MDA PCa 2b) that express PSA and androgen receptor, grow in vitro, and are androgen sensitive. Cells from these lines produced tumors in nude mice when injected either s. c. or orthotopically (intraprostatic). Both cell lines were established from a bone metastasis of a patient whose cancer was exhibiting androgen-independent growth. Although both were derived from two samples of the same specimen, they have different genetic features (as assessed by karyotype analysis) and different phenotypes (e.g., morphology and growth rate). It is likely that they are distinct clones isolated by the use of different culture procedures and reflect the genetic heterogeneity of the tumor. These new cell lines are the first available derived from a bone metastasis of an androgen-independent prostatic adenocarcinoma that grow both in vivo and in vitro and have retained PSA expression and androgen sensitivity. They therefore constitute important model systems to address critical questions related to the androgen-independent growth of human prostate cancer and to the complex process of bone metastasis.

摘要

人类前列腺癌细胞系特别难以建立,并且大多数现有的细胞系并不具备人类前列腺癌常见的特征。大多数可用模型要么仅在体内作为异种移植生长,要么对雄激素不敏感且无法表达前列腺特异性抗原(PSA)。缺乏与晚期前列腺癌功能相关的模型系统限制了前列腺癌的研究和治疗发展。在从前列腺癌患者获取的30个处理样本中,我们建立了两个细胞系(MDA PCa 2a和MDA PCa 2b),它们表达PSA和雄激素受体,可在体外生长,并且对雄激素敏感。当将这些细胞系的细胞皮下或原位(前列腺内)注射到裸鼠体内时,会产生肿瘤。这两个细胞系均从一名癌症呈现雄激素非依赖性生长的患者的骨转移灶中建立。尽管它们都源自同一份标本的两个样本,但它们具有不同的遗传特征(通过核型分析评估)和不同的表型(例如形态和生长速率)。它们很可能是通过使用不同培养程序分离出的不同克隆,反映了肿瘤的遗传异质性。这些新的细胞系是首个源自雄激素非依赖性前列腺腺癌骨转移灶的细胞系,它们既能在体内生长也能在体外生长,并且保留了PSA表达和雄激素敏感性。因此,它们构成了重要的模型系统,可用于解决与人类前列腺癌雄激素非依赖性生长以及骨转移复杂过程相关的关键问题。

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