Abstract

Cancer arises as a result of the inability of damaged cells to initiate a signaling cascade that results in the destruction of the cell and clearance from the body. This process, known as apoptosis, is necessary to prevent reproduction of damaged cells that leads to cancer. A family of proteins known as the Bcl-2 protein family regulates apoptosis. The Bcl-2 protein family works to promote cell death through the interaction of death promoting proteins. Bax, a pro-apoptotic member of this family, initiates the cell death cascade by releasing cytochrome C. Bax has the ability to mediate cytochrome c release by working in conjunction with cardiolipin. Previous studies have shown that the presence of cardiolipin enhances the ability of Bax to form pores in reconstituted membranes through an, as yet, unknown mechanism. Preliminary data from our lab has begun to elucidate the mechanism of interaction between Bax and cardiolipin. In the presence of cardiolipin Bax undergoes a unique conformational change that facilitates the release of molecules from model membranes. The goals of the current project are to determine the impact that this conformational change has on the active and functional conformation of Bax. Our goals are to detail the structural changes and to correlate these changes with the function of Bax at the membrane. This will be achieved by studying pore formation and oligomerization of membrane-associated Bax using fluorescent spectroscopic techniques. We will also study how regions of Bax contribute to membrane recognition pore formation and oligomerization through the use of mutants. The two regions of Bax that are of interest are the BH3 domain, also called the putative cardiolipin binding region, and the c-terminal hydrophobic domain. Understanding the mechanisms of pore formation and oligomerization as well as how domains of Bax contribute to the membrane-active conformation will enhance our understanding of apoptosis and aid in our ability to overcome the barriers that cancer cells erect to evade apoptosis.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Minority Biomedical Research Support - MBRS (S06)
Project #
5S06GM008043-40
Application #
8126432
Study Section
Minority Programs Review Committee (MPRC)
Project Start
Project End
Budget Start
2010-08-01
Budget End
2011-07-31
Support Year
40
Fiscal Year
2010
Total Cost
$106,626
Indirect Cost

  Institution

Name
Chicago State University
Department
Type
DUNS #
108109182
City
Chicago
State
IL
Country
United States
Zip Code
60628

  Publications

Al-Ghoul, Walid M; Kim, Margarita S; Fazal, Nadeem et al. (2014) Evidence for simvastatin anti-inflammatory actions based on quantitative analyses of NETosis and other inflammation/oxidation markers. Results Immunol 4:14-22
Al-Ghoul, Walid M; Abu-Shaqra, Steven; Park, Byeong Gyu et al. (2010) Melatonin plays a protective role in postburn rodent gut pathophysiology. Int J Biol Sci 6:282-93
Lange, Yvonne; Ye, Jin; Duban, Mark-Eugene et al. (2009) Activation of membrane cholesterol by 63 amphipaths. Biochemistry 48:8505-15
Reyes, Juan F; Stone, Karen; Ramos, Jeanie et al. (2009) Formation of Hirano bodies after inducible expression of a modified form of an actin-cross-linking protein. Eukaryot Cell 8:852-7
Mody, Purvi D; Cannon, Judy L; Bandukwala, Hozefa S et al. (2007) Signaling through CD43 regulates CD4 T-cell trafficking. Blood 110:2974-82
Fazal, Nadeem; Al-Ghoul, Walid M (2007) Thermal injury-plus-sepsis contributes to a substantial deletion of intestinal mesenteric lymph node CD4 T cell via apoptosis. Int J Biol Sci 3:393-401
Fazal, Nadeem; Raziuddin, Syed; Khan, Mehdi et al. (2006) Antigen presenting cells (APCs) from thermally injured and/or septic rats modulate CD4+ T cell responses of naive rat. Biochim Biophys Acta 1762:46-53
Ford, S H; Gallery, J; Nichols, A et al. (1991) High-performance liquid chromatographic analysis of the (cyanoaquo) stereoisomers of several putative vitamin B12 precursors. J Chromatogr 537:235-47
Ford, S H; Nichols, A; Gallery, J M (1991) Separation and study of corrinoid cobalt-ligand isomers by high-performance liquid chromatography. J Chromatogr 536:185-91
Ford, S H; Nichols, A; Shambee, M (1991) The preparation and characterization of the diaquo- forms of several incomplete corrinoids: cobyric acid, cobinamide, and three isomeric cobinic acid pentaamides. J Inorg Biochem 41:235-44