Abstract

Paclitaxel/Taxol prevents microtubule disassembly, resulting in cell cycle arrest and apoptosis. It is used clinically as a frontline therapy for ovarian tumors and has shown increasing efficacy in the treatment of breast cancer. The most encouraging data were obtained with a combination therapy using paclitaxel and anti-Her2/neu antibody. However, improvements in combination therapy with paclitaxel/Taxol for the treatment of breast cancer are still needed. Our past effort has focused on the effects of paclitaxel on gene expression signaling and apoptosis in epithelial cancer cells. We first found that paclitaxel induces the JNK/SAPK kinase system in breast carcinomas, and this activation is involved in paclitaxel-induced apoptosis. In contrast paclitaxel also activates MEK1 kinase leading to an elevation of ERK1 and ERK2 activity. MEK1 members are known to be critical for cell growth and proliferation in a number of systems. By using a combination of MEK inhibitors and paclitaxel, we were able to obtain greatly enhanced tumor killing by using suboptimal levels of the two drugs. Apoptosis in the presence of both drugs is five to tenfold more than with each drug alone. Additionally, we have also initiated an analysis of a derivative of epothilone B, dEpoB, which has similar effects as paclitaxel. We found that dEpoB also exhibits enhanced tumor killing activity in the presence of MEK inhibitor. DEpoB has the advantage over paclitaxel in that it is not transported by the multi-drug resistant transporter system, which allows many tumors to acquire chemotherapy-resistance. Thus, dEpoB may be effective where paclitaxel is not. Used in a clinical setting, these combinations may lower toxicity and enhance tumor killing. Accordingly, the four aims of this project are: (1) To determine if paclitaxel and an MEK inhibitor can cause enhanced tumor elimination in a preclinical model. (2) To similarly study the combined effects of dEpoB and an MEK inhibitor. (3) To use Affymetrix analysis and microchip arrays to identify genes that are altered by the use of these drug combinations. (4) In the event that Specific Aim (1) and/or Specific Aim (2) show efficacy in the preclinical models, we propose to initiate a clinical trial to test the effects of combination therapy studied in Specific Aims 1 and/or 2.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Specialized Center (P50)
Project #
5P50CA058223-10
Application #
6659196
Study Section
Special Emphasis Panel (ZCA1)
Project Start
2002-09-13
Project End
2003-07-31
Budget Start
Budget End
Support Year
10
Fiscal Year
2002
Total Cost
Indirect Cost

  Institution

Name
University of North Carolina Chapel Hill
Department
Type
DUNS #
078861598
City
Chapel Hill
State
NC
Country
United States
Zip Code
27599

  Publications

McRee, Autumn J; Marcom, Paul K; Moore, Dominic T et al. (2018) A Phase I Trial of the PI3K Inhibitor Buparlisib Combined With Capecitabine in Patients With Metastatic Breast Cancer. Clin Breast Cancer 18:289-297
DeBono, Nathan L; Robinson, Whitney R; Lund, Jennifer L et al. (2018) Race, Menopausal Hormone Therapy, and Invasive Breast Cancer in the Carolina Breast Cancer Study. J Womens Health (Larchmt) 27:377-386
Nasarre, Patrick; Bonilla, Ingrid V; Metcalf, John S et al. (2018) TRAF3-interacting protein 3, a new oncotarget, promotes tumor growth in melanoma. Melanoma Res 28:185-194
Pearce, Oliver M T; Delaine-Smith, Robin M; Maniati, Eleni et al. (2018) Deconstruction of a Metastatic Tumor Microenvironment Reveals a Common Matrix Response in Human Cancers. Cancer Discov 8:304-319
Williams, Lindsay A; Nichols, Hazel B; Hoadley, Katherine A et al. (2018) Reproductive risk factor associations with lobular and ductal carcinoma in the Carolina Breast Cancer Study. Cancer Causes Control 29:25-32
Couture, Heather D; Williams, Lindsay A; Geradts, Joseph et al. (2018) Image analysis with deep learning to predict breast cancer grade, ER status, histologic subtype, and intrinsic subtype. NPJ Breast Cancer 4:30
Lei, Jonathan T; Shao, Jieya; Zhang, Jin et al. (2018) Functional Annotation of ESR1 Gene Fusions in Estrogen Receptor-Positive Breast Cancer. Cell Rep 24:1434-1444.e7
Troester, Melissa A; Sun, Xuezheng; Allott, Emma H et al. (2018) Racial Differences in PAM50 Subtypes in the Carolina Breast Cancer Study. J Natl Cancer Inst 110:
Williams, Michelle M; Lee, Linus; Werfel, Thomas et al. (2018) Intrinsic apoptotic pathway activation increases response to anti-estrogens in luminal breast cancers. Cell Death Dis 9:21
Allott, Emma H; Geradts, Joseph; Cohen, Stephanie M et al. (2018) Frequency of breast cancer subtypes among African American women in the AMBER consortium. Breast Cancer Res 20:12

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