Abstract

The goal of project 3 is to examine the relationship between hepatocyte proliferation and expression of liver specific genes. Alphafetoprotein production is a characteristic of proliferating hepatocytes while albumin expression is a product of the adult, quiescent liver. Conditions that provoke hepatocyte division (regeneration, tumorigenic states, and fetal development) are associated with AFP synthesis. An understanding of the molecular basis for the regulation AFP and albumin expression may provide insight into the complex events that alter the proliferative state of the hepatocyte.
Our specific aims i nclude, 1) defining the cis-acting regulatory regions of alphafetoprotein and albumin that are responsive to factors that induce or inhibit proliferation, such as the membrane associated inhibitors of DNA synthesis isolated from normal senescent fibroblasts and immortalized human cells and stimulatory factors obtained from livers and serum of mice following hepatectomy. These assays will employ gene transfer of regulatory regions of each gene coupled to the bacterial enzyme chloramphenicol actyltransferase into human hepatoma cells. 2) characterizing biochemically, the DNA binding proteins that interact with regions of the DNA that have functional activity defined in specific aim 1. These studies will utilize """"""""band competition"""""""" or gel retardation assays and footprinting to identify the specific sequences in the gene with which the proteins interact. 3) the third aim is to identify and clone the regulatory gene(s) that govern alphafetoprotein expression by a novel genetic scheme. This study will utilize gene transfer and mutant selection to obtain a """"""""trans-acting factor"""""""" mutant. Complementation of the mutant phenotype and selection for the complementing gene will enable direct cloning of the regulatory loci. The trans-factor gene would then be available for an assessment of its role in the complex phenotype of hepatocytic proliferation at the molecular level. 4) a final aim is to immortalize human primary hepatocytes in order to examine the cellular genes that are modified.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Aging (NIA)
Type
Research Program Projects (P01)
Project #
1P01AG007123-01
Application #
3821929
Study Section
Project Start
Project End
Budget Start
Budget End
Support Year
1
Fiscal Year
1987
Total Cost
Indirect Cost

  Institution

Name
Baylor College of Medicine
Department
Type
DUNS #
074615394
City
Houston
State
TX
Country
United States
Zip Code
77030

  Publications

Duttaroy, A; Qian, J F; Smith, J S et al. (1997) Up-regulated P21CIP1 expression is part of the regulation quantitatively controlling serum deprivation-induced apoptosis. J Cell Biochem 64:434-46
Smith, J R; Nakanishi, M; Robetorye, R S et al. (1996) Studies demonstrating the complexity of regulation and action of the growth inhibitory gene SDI1. Exp Gerontol 31:327-35
Yang, L; Didenko, V V; Noda, A et al. (1995) Increased expression of p21Sdi1 in adrenocortical cells when they are placed in culture. Exp Cell Res 221:126-31
Kaul, S C; Wadhwa, R; Matsuda, Y et al. (1995) Mouse and human chromosomal assignments of mortalin, a novel member of the murine hsp70 family of proteins. FEBS Lett 361:269-72
Wadhwa, R; Pereira-Smith, O M; Reddel, R R et al. (1995) Correlation between complementation group for immortality and the cellular distribution of mortalin. Exp Cell Res 216:101-6
Nakanishi, M; Robetorye, R S; Pereira-Smith, O M et al. (1995) The C-terminal region of p21SDI1/WAF1/CIP1 is involved in proliferating cell nuclear antigen binding but does not appear to be required for growth inhibition. J Biol Chem 270:17060-3
Hensler, P J; Pereira-Smith, O M (1995) Human replicative senescence. A molecular study. Am J Pathol 147:1-8
Khaoustov, V I; Ozer, A; Smith, J R et al. (1995) Induction of senescent cell-derived inhibitor of DNA synthesis gene, SDI1, in hepatoblastoma (HepG2) cells arrested in the G2-phase of the cell cycle by 9-nitrocamptothecin. Lab Invest 73:118-27
Nakanishi, M; Robetorye, R S; Adami, G R et al. (1995) Identification of the active region of the DNA synthesis inhibitory gene p21Sdi1/CIP1/WAF1. EMBO J 14:555-63
Aggarwal, B B; Totpal, K; LaPushin, R et al. (1995) Diminished responsiveness of senescent normal human fibroblasts to TNF-dependent proliferation and interleukin production is not due to its effect on the receptors or on the activation of a nuclear factor NF-kappa B. Exp Cell Res 218:381-8

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