Literature DB >> 19783900

The biology of hormone refractory breast and prostate cancer: An NCI workshop report.

Suresh Mohla1, Vered Stearns, Neeraja Sathyamoorthy, Michael G Rosenfeld, Peter Nelson.   

Abstract

The molecular regulation of growth and progression of hormone refractory breast and prostate cancers remains challenging. The Division of Cancer Biology, NCI organized a small "think tank" style workshop and invited scientists in relevant areas to assess the state of science on the biology of hormone refractory tumors and to identify potential research opportunities to enhance a better understanding of the molecular regulation of these tumors. The meeting, held on May 27-29, 2008 in Bethesda, MD, was co-chaired by Drs. Michael Geoffrey Rosenfeld and Michael Press. While expression of estrogen or progesterone receptors (ER/PR) is required for benefit from endocrine manipulations, many women with breast cancer will not respond to primary endocrine manipulations despite ER/PR expression, and others acquire resistance while on treatment. Understanding the mechanisms that lead to Hormone Refractory Breast Cancer (HRBC) and defining interventions that may modulate the resistance to endocrine therapy are currently lacking. In contrast to breast cancers, the vast majority of both early and advanced prostate carcinomas exhibit androgen-pathway activity at diagnosis and the vast majority respond to treatments designed to inhibit AR-signaling. However, after initial benefit, advanced prostate cancers regularly progress to a clinical state termed Castration Resistant Prostate Cancer (CRPC) that reflects a diverse array of molecular events maintaining AR signaling. The workshop focused on both common and unique features of hormone refractory breast and prostate cancer with an orientation toward defining major research questions, delineating opportunities and recommending strategies for overcoming barriers to progress in understanding these important clinical disease states.

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Year:  2009        PMID: 19783900     DOI: 10.4161/cbt.8.21.9918

Source DB:  PubMed          Journal:  Cancer Biol Ther        ISSN: 1538-4047            Impact factor:   4.742


  9 in total

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Authors:  Sean C Harrington; S John Weroha; Carol Reynolds; Vera J Suman; Wilma L Lingle; Paul Haluska
Journal:  Growth Horm IGF Res       Date:  2012-04-30       Impact factor: 2.372

5.  CAMK2N1 inhibits prostate cancer progression through androgen receptor-dependent signaling.

Authors:  Tao Wang; Shuiming Guo; Zhuo Liu; Licheng Wu; Mingchao Li; Jun Yang; Ruibao Chen; Xiaming Liu; Hua Xu; Shaoxin Cai; Hui Chen; Weiyong Li; Shaohua Xu; Liang Wang; Zhiquan Hu; Qianyuan Zhuang; Liping Wang; Kongming Wu; Jihong Liu; Zhangqun Ye; Jun-Yuan Ji; Chenguang Wang; Ke Chen
Journal:  Oncotarget       Date:  2014-11-15

6.  Exosomes Promote the Transition of Androgen-Dependent Prostate Cancer Cells into Androgen-Independent Manner Through Up-Regulating the Heme Oxygenase-1.

Authors:  Yiming Zhang; Binshen Chen; Naijin Xu; Peng Xu; Wenfeng Lin; Chunxiao Liu; Peng Huang
Journal:  Int J Nanomedicine       Date:  2021-01-12

7.  LXXLL peptide converts transportan 10 to a potent inducer of apoptosis in breast cancer cells.

Authors:  Kairit Tints; Madis Prink; Toomas Neuman; Kaia Palm
Journal:  Int J Mol Sci       Date:  2014-04-03       Impact factor: 5.923

8.  The tumor suppressive role of CAMK2N1 in castration-resistant prostate cancer.

Authors:  Tao Wang; Zhuo Liu; Shuiming Guo; Licheng Wu; Mingchao Li; Jun Yang; Ruibao Chen; Hua Xu; Shaoxin Cai; Hui Chen; Weiyong Li; Liang Wang; Zhiquan Hu; Qianyuan Zhuang; Shaohua Xu; Liping Wang; Jihong Liu; Zhangqun Ye; Jun-Yuan Ji; Chenguang Wang; Ke Chen
Journal:  Oncotarget       Date:  2014-06-15

9.  Tetrahydro-iso-alpha Acids Antagonize Estrogen Receptor Alpha Activity in MCF-7 Breast Cancer Cells.

Authors:  Maëlle Lempereur; Claire Majewska; Amandine Brunquers; Sumalee Wongpramud; Bénédicte Valet; Philippe Janssens; Monique Dillemans; Laurence Van Nedervelde; Dominique Gallo
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  9 in total

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