Abstract

Tumor cell growth can be controlled by surrounding normal cells. This process is called """"""""heterologous growth control"""""""". The goal of this project is to elucidate mechanisms underlying this process. We will determine how nontransformed cells affect the Src signaling cascade in neighboring transformed cells. The need for heterologous gap junctional communication in heterologous growth control will be evaluated in Specific Aim 1. We hypothesize that nontransformed cells do not need to form active gap junction channels with Src transformed cells to normalize their growth. We will utilize connexin knockout cells, chemical blockers or antisense nucleic acids to suppress gap junctional communication. Intercellular communication will be examined by the transfer of fluorescent dyes, endogenous metabolites, and electrical conductance. If heterologous growth control occurs in the absence of gap junctional communication, then, as we hypothesize, gap junctional communication is not required for heterologous growth control. Effects of nontransformed cells on the Src kinase activity, and the activity of kinases acting downstream of Src, in Src transformed cells will be evaluated in Specific Aims 2 and 3, respectively. We hypothesize that nontransformed cells quell Src kinase activity, and affect the activity of downstream kinases, in neighboring transformed cells. We will use novel techniques that we have developed to examine kinase activity in transformed cells that are morphologically reversed to a normal phenotype by neighboring nontransformed cells. Our hypothesis will be proven if the Src signaling in transformed cells cascade is blocked by communication with nontransformed cells. Effects of nontransformed cells on the global expression pattern of genes in neighboring transformed cells will be examined in Specific Aim 4. We hypothesize that nontransformed cells alter the expression of specific genes in neighboring transformed cells. We will utilize DNA chips to compare the gene profiles of transformed cells cocultured with nontransformed cells to transformed cells and nontransformed cells grown alone. The hypothesis will be proven if the expression levels of some genes, but not others, in transformed cells are affected by contact with nontransformed cells during heterologous growth control.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA088805-05
Application #
7109343
Study Section
Experimental Therapeutics Subcommittee 1 (ET)
Program Officer
Ault, Grace S
Project Start
2005-08-08
Project End
2008-06-30
Budget Start
2006-07-01
Budget End
2008-06-30
Support Year
5
Fiscal Year
2006
Total Cost
$216,380
Indirect Cost

  Institution

Name
University of Medicine & Dentistry of NJ
Department
Biochemistry
Type
Schools of Osteopathy
DUNS #
140757589
City
Stratford
State
NJ
Country
United States
Zip Code
08084

  Publications

Khusial, P Raaj; Vadla, Bhaskar; Krishnan, Harini et al. (2010) Src activates Abl to augment Robo1 expression in order to promote tumor cell migration. Oncotarget 1:198-209
Li, X; Shen, Y; Ichikawa, H et al. (2009) Regulation of miRNA expression by Src and contact normalization: effects on nonanchored cell growth and migration. Oncogene 28:4272-83
Li, Xun; Jia, Zhenyu; Shen, Yongquan et al. (2008) Coordinate suppression of Sdpr and Fhl1 expression in tumors of the breast, kidney, and prostate. Cancer Sci 99:1326-33
Pahujaa, Madhuri; Anikin, Michael; Goldberg, Gary S (2007) Phosphorylation of connexin43 induced by Src: regulation of gap junctional communication between transformed cells. Exp Cell Res 313:4083-90
Shen, Yongquan; Khusial, P Raaj; Li, Xun et al. (2007) SRC utilizes Cas to block gap junctional communication mediated by connexin43. J Biol Chem 282:18914-21
Shen, Yongquan; Jia, Zhenyu; Nagele, Robert G et al. (2006) SRC uses Cas to suppress Fhl1 in order to promote nonanchored growth and migration of tumor cells. Cancer Res 66:1543-52
Goldberg, Gary S; Kunimoto, Takehiko; Alexander, David B et al. (2005) Full length and delta lactoferrin display differential cell localization dynamics, but do not act as tumor markers or significantly affect the expression of other genes. Med Chem 1:57-64
Valiunas, Virginijus; Bechberger, John F; Naus, Christian C G et al. (2005) Nontransformed cells can normalize gap junctional communication with transformed cells. Biochem Biophys Res Commun 333:174-9
Goldberg, Gary S; Valiunas, Virginijus; Brink, Peter R (2004) Selective permeability of gap junction channels. Biochim Biophys Acta 1662:96-101
Alexander, David B; Ichikawa, Hitoshi; Bechberger, John F et al. (2004) Normal cells control the growth of neighboring transformed cells independent of gap junctional communication and SRC activity. Cancer Res 64:1347-58

Showing the most recent 10 out of 11 publications