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Abstract

Grant Number: 5R01CA046274-14

Project Title: Genetics of Pediatric Rhabdoid Tumors

PI Information: Name Email Title

BIEGEL, JACLYN A. biegel@mail.med.upenn.edu ASSOCIATE PROFESSOR

Abstract: DESCRIPTION: (Adapted from the investigator's abstract) Rhabdoid tumor is a rapidly fatal malignancy that generally presents in the first two years of life. The most common sites of presentation are the brain and kidney. We and others used a combination of cytogenetic and molecular studies to define a critical region in 22q11.2 that contained a rhabdoid tumor suppressor gene. Recently, Versteege et al (1998) reported hSNF5/INI1 as a candidate gene for renal and extrarenal rhabdoid tumors. We identified germline and somatic mutations of INI1 in pediatric rhabdoid tumors of the central nervous system (Biegel et al, 1999), and have now documented germline mutations in patients with primary tumors of the brain and kidney. INI1 is a member of the SWIJSNF complex, one of several cell- cycle and ATP-dependent nucleosome remodeling complexes in mammalian cells. The SWTJSNF complex functions in both activation and repression of downstream target genes. In this proposal, we will define the spectrum of INI1 deletions and mutations in pediatric rhabdoid tumors of the brain, kidney and soft tissues. The frequency of inherited and de novo germline mutations in patients and their parents will be determined. Homozygous deletion of INI1 in chromosome band 22q 11.2 has been observed in 11 percent of tumors, whereas nonsense and frameshift mutations have been demonstrated in almost 50 percent of cases. In contrast, approximately 25 percent of primary tumors demonstrate alterations of the exon-intron 1 region of INI1 that result in absent INI1 gene expression. We propose that genomic rearrangements in this region or hypermethylation of CpG dinucleotides could decrease INI1 expression. Monosomy or deletion of the other chromosome 22 would thus result in homozygous inactivation of INI1, leading to tumor formation. The specificity of INTl mutations for rhabdoid tumors will also be addressed in this program, with particular emphasis on evaluating a larger series of medulloblastoma-primitive neuroectodermal tumors and choroid plexus carcinomas of the brain, as well as a series of pediatric rhabdomyosarcomas. These studies will lead to a better understanding of the role of INTl in the development of malignancy, improvements in determining diagnosis and prognosis for patients and their families, and ultimately, biologically based treatment strategies.
Public Health Relevance:
This Public Health Relevance is not available.
Thesaurus Terms:
kidney neoplasm, medulloblastoma, neoplasm /cancer genetics, pediatric neoplasm /cancer, rhabdomyosarcoma
CpG island, DNA methylation, frameshift mutation, gene deletion mutation, gene expression, gene rearrangement, loss of heterozygosity, nucleic acid sequence
child (0-11), clinical research, human subject, polymerase chain reaction, southern blotting

Institution: CHILDREN'S HOSPITAL OF PHILADELPHIA

Research Institute

PHILADELPHIA, PA 191044318

Fiscal Year: 2003

Department:

Project Start: 13-JAN-1989

Project End: 30-MAR-2006

ICD: NATIONAL CANCER INSTITUTE

IRG: PTHB

Grant Number:	5R01CA046274-14
Project Title:	Genetics of Pediatric Rhabdoid Tumors

PI Information:	Name	Email	Title
	BIEGEL, JACLYN A.	biegel@mail.med.upenn.edu	ASSOCIATE PROFESSOR

Institution:	CHILDREN'S HOSPITAL OF PHILADELPHIA
	Research Institute
	PHILADELPHIA, PA 191044318
Fiscal Year:	2003
Department:
Project Start:	13-JAN-1989
Project End:	30-MAR-2006
ICD:	NATIONAL CANCER INSTITUTE
IRG:	PTHB