Abstract

The human TCL-1 gene maps at chromosome 14q32.1 and is activated in T cell leukemias and lymphomas by either chromosome translocations or inversions that juxtapose the TCL-1 gene to the alpha/delta or beta locus of the T cell receptor. The hTCL-1 protein is 41% identical and 61% similar to the hMTCP-1 protein on chromosome Xq28 which is also involved in T cell lymphoproliferative diseases. The hTCL-1 and hMTCP-1 proteins may be new members of an oncogene family involved in lymphoid proliferation and/or survival and in T cell malignancies. The major role of the Protein Chemistry Core Laboratory in this project is to produce and purify the TCL-1 and MTCP-1 proteins in milligram amounts which are necessary to conduct functional analysis and three- dimensional structural analysis of these proteins. The hTCL-1 and hMTCP-1 proteins have been expressed in C. coli both with and without 6xHis tag sequence, and the recombinant proteins have been purified to homogeneity in milligram amounts. The hTCL-1 and hMTCP-1 proteins will be produced using a eukaryotic expression system, purified to homogeneity in milligram amounts, and their properties compared to the E. coli produced proteins. The E. coli system will also be used for the preparation of mutant forms of hTCL-1. Core B will conduct studies to characterize the properties of all recombinant TCL-1 and MTCP-1 proteins produced in this laboratory using the techniques of N-terminal sequence analysis, electrospray mass spectrometry (ES-MS), isoelectric focusing (IEF), gel filtration chromatography and polyacrylamide gel electrophoresis (PAGE). The Protein Chemistry Core will map putative nucleotide binding sites and the exposed hydrophobic sites of both TCL-1 and MTCP-1 proteins using photoincorporation of [32P]-labeled and fluorescent probes, fragmentation by chemical or enzymatic methods, separation by HPLC, and peptide sequencing. Core B will conduct studies to determine the binding of wild-type and mutant forms of TCL-1 and MTCP-1 to interacting proteins such as EWS and TAF/II68 and also further studies to identify new molecular partners of TCL-1 and MTCP-1 using the biosensor technology. The Core will also prepare monoclonal and polyclonal antibodies to TCL-1 and MTCP-1, mutant forms, peptides, and interacting proteins. Core B will prepare by solid phase synthesis all peptide analogs of TCL-1 and MTCP-1 designed by molecular modeling to act a potential inhibitors of their protein function.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Program Projects (P01)
Project #
5P01CA076259-03
Application #
6483406
Study Section
Special Emphasis Panel (ZCA1)
Project Start
2001-05-01
Project End
2002-04-30
Budget Start
Budget End
Support Year
3
Fiscal Year
2001
Total Cost
Indirect Cost

  Institution

Name
Thomas Jefferson University
Department
Type
DUNS #
061197161
City
Philadelphia
State
PA
Country
United States
Zip Code
19107

  Publications

Thompson, Lorraine H; Whiston, Roy A; Rakhimov, Yerzhan et al. (2010) A LIF/Nanog axis is revealed in T lymphocytes that lack MARCH-7, a RINGv E3 ligase that regulates the LIF-receptor. Cell Cycle 9:4213-21
Almanza, Gonzalo; Fernandez, Antonio; Volinia, Stefano et al. (2010) Selected microRNAs define cell fate determination of murine central memory CD8 T cells. PLoS One 5:e11243
Garzon, Ramiro; Liu, Shujun; Fabbri, Muller et al. (2009) MicroRNA-29b induces global DNA hypomethylation and tumor suppressor gene reexpression in acute myeloid leukemia by targeting directly DNMT3A and 3B and indirectly DNMT1. Blood 113:6411-8
Ghosh, Asish K; Shanafelt, Tait D; Cimmino, Amelia et al. (2009) Aberrant regulation of pVHL levels by microRNA promotes the HIF/VEGF axis in CLL B cells. Blood 113:5568-74
Pufnock, Jeff S; Rothstein, Jay L (2009) Oncoprotein signaling mediates tumor-specific inflammation and enhances tumor progression. J Immunol 182:5498-506
Croce, Carlo M (2009) Causes and consequences of microRNA dysregulation in cancer. Nat Rev Genet 10:704-14
Garzon, Ramiro; Volinia, Stefano; Liu, Chang-Gong et al. (2008) MicroRNA signatures associated with cytogenetics and prognosis in acute myeloid leukemia. Blood 111:3183-9
Volinia, Stefano; Mascellani, Nicoletta; Marchesini, Jlenia et al. (2008) Genome wide identification of recessive cancer genes by combinatorial mutation analysis. PLoS One 3:e3380
Garzon, Ramiro; Garofalo, Michela; Martelli, Maria Paola et al. (2008) Distinctive microRNA signature of acute myeloid leukemia bearing cytoplasmic mutated nucleophosmin. Proc Natl Acad Sci U S A 105:3945-50
Tili, Esmerina; Michaille, Jean-Jacques; Cimino, Amelia et al. (2007) Modulation of miR-155 and miR-125b levels following lipopolysaccharide/TNF-alpha stimulation and their possible roles in regulating the response to endotoxin shock. J Immunol 179:5082-9

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