Abstract

We have demonstrated statistical evidence for a major gene in kindreds of childhood and adolescent soft tissue and bone sarcoma patients. To date, some of these kindreds that provide strong evidence for a major gene have been, found to have germline mutations in the tumor suppressor gene, p53. Statistical findings, however, suggest that a major gene may not account for all of the variation in cancer risk observed within or among kindreds. For example, siblings of probands are at greater risk of childhood cancer than siblings of parents; additional risk to relatives was observed in families of patients with embryonal rhabdomyosarcoma as compared to other histologic soft tissue sarcoma types; a significant multifactorial contribution in addition to a major gene was observed in the bone sarcoma kindreds. We therefore propose to determine the contribution of p53 germline mutations to the overall cancer risk using a strategy of combined linkage and segregation analysis. Initially we will be testing for linkage to p53 specifically. However, if the findings support involvement of other genetic loci, the strategy we have proposed could be generalized to identify other major genes or modifying genes. The immediate goals remain to identify the extent to which germline p53 mutations can account for the observed familial cancer aggregation in the sarcoma cohort. With this approach we can characterize the age-, sex- and site- specific penetrance for p53 germline mutations, the extent of phenocopies in the kindreds, and can identify any variation in risk not attributable to p53 as a major gene. In addition, we will determine the frequency of de novo mutations in p53, and the contribution of p53 germline mutations to the phenotype of a second malignant neoplasm. Findings from this project should provide sufficient information to develop guidelines for genetic testing of childhood sarcoma patients, guidelines for genetic counseling regarding the implications of a p53 germline mutation, and a framework from which to investigate the role of other genetic loci in familial cancer aggregates.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Program Projects (P01)
Project #
5P01CA034936-13
Application #
6236707
Study Section
Project Start
1997-08-01
Project End
1999-07-31
Budget Start
1996-10-01
Budget End
1997-09-30
Support Year
13
Fiscal Year
1997
Total Cost
Indirect Cost

  Institution

Name
University of Texas MD Anderson Cancer Center
Department
Type
DUNS #
001910777
City
Houston
State
TX
Country
United States
Zip Code
77030

  Publications

Peng, Gang; Bojadzieva, Jasmina; Ballinger, Mandy L et al. (2017) Estimating TP53 Mutation Carrier Probability in Families with Li-Fraumeni Syndrome Using LFSPRO. Cancer Epidemiol Biomarkers Prev 26:837-844
Maturu, Paramahamsa; Jones, Devin; Ruteshouser, E Cristy et al. (2017) Role of Cyclooxygenase-2 Pathway in Creating an Immunosuppressive Microenvironment and in Initiation and Progression of Wilms' Tumor. Neoplasia 19:237-249
Huang, Le; Mokkapati, Sharada; Hu, Qianghua et al. (2016) Nephron Progenitor But Not Stromal Progenitor Cells Give Rise to Wilms Tumors in Mouse Models with ?-Catenin Activation or Wt1 Ablation and Igf2 Upregulation. Neoplasia 18:71-81
Palculict, Timothy Blake; Ruteshouser, E Cristy; Fan, Yu et al. (2016) Identification of germline DICER1 mutations and loss of heterozygosity in familial Wilms tumour. J Med Genet 53:385-8
Liu, Changlu; Ma, Jianzhong; Amos, Christopher I (2015) Bayesian variable selection for hierarchical gene-environment and gene-gene interactions. Hum Genet 134:23-36
Mokkapati, Sharada; Niopek, Katharina; Huang, Le et al. (2014) ?-catenin activation in a novel liver progenitor cell type is sufficient to cause hepatocellular carcinoma and hepatoblastoma. Cancer Res 74:4515-25
Quintás-Cardama, Alfonso; Post, Sean M; Solis, Luisa M et al. (2014) Loss of the novel tumour suppressor and polarity gene Trim62 (Dear1) synergizes with oncogenic Ras in invasive lung cancer. J Pathol 234:108-19
Maturu, Paramahamsa; Overwijk, Willem W; Hicks, John et al. (2014) Characterization of the inflammatory microenvironment and identification of potential therapeutic targets in wilms tumors. Transl Oncol 7:484-92
Shahidul Makki, Mohammad; Cristy Ruteshouser, E; Huff, Vicki (2013) Ubiquitin specific protease 18 (Usp18) is a WT1 transcriptional target. Exp Cell Res 319:612-22
Kaftanovskaya, Elena M; Neukirchner, Giselle; Huff, Vicki et al. (2013) Left-sided cryptorchidism in mice with Wilms' tumour 1 gene deletion in gubernaculum testis. J Pathol 230:39-47

Showing the most recent 10 out of 214 publications