Mechanisms of breast cancer cell growth & tumorigenicity

乳腺癌细胞生长的机制

基本信息

批准号：
6897200
负责人：
AMY H. BOUTON
金额：
$ 25.09万
依托单位：
UNIVERSITY OF VIRGINIA
依托单位国家：
美国
项目类别：
财政年份：
2003
资助国家：
美国
起止时间：
2003-07-01 至 2008-06-30
项目状态：
已结题

项目摘要

DESCRIPTION (provided by applicant): There is growing evidence to suggest that changes in expression of the adapter protein p130cas (Cas) in breast tumors may contribute to cancer progression and poor prognosis. In human breast tumors, Cas overexpression is correlated with a high probability of recurrence and a high incidence of intrinsic resistance to the antiestrogen tamoxifen. Antiestrogen resistance is also evident in cultured breast cancer cells that overexpress either Cas or its binding partner AND-34/BCAR3. Cas is comprised of multiple structural domains, each of which has the capacity to interact with a different array of proteins and thus promote potentially distinct functional outcomes. We hypothesize that overexpression of Cas or AND-34 activates signaling pathways through interactions with a defined subset of these proteins, ultimately leading to antiestrogen resistance and changes in cell physiology that are associated with aggressive tumor behavior and poor prognosis. This hypothesis will be tested in Aim 1 by identifying domains and downstream effectors of Cas and AND-34 that function to promote antiestrogen resistance, and investigating how these pathways coordinate with or override estrogen receptor functions during this process. In Aim 2, we will test whether Cas overexpression in cells that serve as models for early-stage breast cancer can induce changes in cell physiology and morphology that coincide with the acquisition of a more aggressive growth and invasion phenotype. Conversely, we will also test whether inhibition of Cas expression or function in cells that serve as models for late-stage breast cancer reverses some of the deleterious phenotypes exhibited by these cells. The potential functional contribution of proteins known to bind to domains that are implicated in the studies described above will be pursued in the context of each of the two Specific Aims. However, in those instances where a domain is implicated that does not have a known binding partner, or when none of the known binding proteins are found to play a role, attempts will be made in Aim 3 to identify additional binding partners and test whether they function in these pathways. Completion of this work will open new avenues of investigation into such areas as the development of molecular screens for predicting responses to tamoxifen treatment, the design of strategies for enhancing the efficacy of tamoxifen in intrinsically resistant patients, and the application of novel molecular approaches to slow tumor progression.

描述（由申请人提供）：越来越多的证据表明，乳腺肿瘤中接头蛋白 p130cas (Cas) 表达的变化可能导致癌症进展和不良预后。在人类乳腺肿瘤中，Cas 过度表达与高复发率和抗雌激素他莫昔芬内在耐药性的高发生率相关。抗雌激素耐药性在过度表达 Cas 或其结合伴侣 AND-34/BCAR3 的培养乳腺癌细胞中也很明显。 Cas 由多个结构域组成，每个结构域都有能力与不同的蛋白质阵列相互作用，从而促进潜在的不同功能结果。我们假设 Cas 或 AND-34 的过度表达通过与这些蛋白质的特定子集相互作用来激活信号通路，最终导致抗雌激素耐药性和细胞生理学的变化，这些变化与侵袭性肿瘤行为和不良预后相关。这一假设将在目标 1 中得到检验，方法是识别 Cas 和 AND-34 的结构域和下游效应器，这些效应器具有促进抗雌激素耐药性的功能，并研究这些途径在此过程中如何协调或超越雌激素受体功能。在目标 2 中，我们将测试作为早期乳腺癌模型的细胞中 Cas 过度表达是否可以诱导细胞生理学和形态学的变化，这些变化与获得更具侵袭性的生长和侵袭表型相一致。相反，我们还将测试抑制晚期乳腺癌模型细胞中的 Cas 表达或功能是否可以逆转这些细胞表现出的一些有害表型。已知与上述研究涉及的结构域结合的蛋白质的潜在功能贡献将在两个具体目标的背景下进行。然而，在涉及的结构域没有已知的结合配偶体的情况下，或者当没有发现已知的结合蛋白发挥作用时，将在目标 3 中尝试鉴定其他结合配偶体并测试它们是否在这些途径中发挥作用。这项工作的完成将为这些领域的研究开辟新的途径，例如开发用于预测对他莫昔芬治疗反应的分子筛选、设计增强他莫昔芬对内在耐药患者的疗效的策略，以及应用新的分子方法来减缓耐药性。肿瘤进展。