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Abstract

Grant Number: 5R21CA095475-02

Project Title: Prognosis in childhood ALL

PI Information: Name Email Title

KEES, URSULA R. ursula@ichr.uwa.edu.au

Abstract: DESCRIPTION (provided by applicant) Despite the high rate of cure, resistant forms of childhood acute lymphoblastic leukemia (ALL) constitute a leading cause of cancer-related deaths in children. We propose to study childhood ALL patients in order to arrive at a better risk stratification, based on gene expression profiles measured in microarray studies which allow simultaneous testing of the expression levels of thousands of genes. The primary aim of the study is to characterise the profiles of relapsing and non-relapsing patients in order to identity features with prognostic value. This will be achieved by studying complementary sets of patient specimens banked at our own institution. The quality of this set of more than 130 patient specimens makes them particularly suited for microarray studies. They allow us to ask very specific questions. (1) Which genes are expressed in leukemia specimens from patients who will relapse because their disease is resistant to chemotherapy, while not expressed (or expressed at lower levels) in patients who will respond to therapy? (2) Which genes are expressed at low levels in specimens from relapsing patients? (3) Are the same genes differentially expressed in the leukemia cells at relapse, compared to the time of diagnosis? The answers to these three questions will provide the basis for the selection of a panel of suitable prognostic marker genes. The aim of the project is to establish tests to measure expression levels of these candidate prognostic markers by realtime quantitative polymerase chain reaction (PCR). These will subsequently be studied in a separate cohort of patients who have received uniform treatment to verify that they are indeed of prognostic significance. The overall goal is to develop a prognostic test to be used at the time of diagnosing a child with ALL to determine whether the patient is likely to be successfully treated on current therapy protocols or has a high risk of relapse, hence, should be receiving more intensive therapy.
Public Health Relevance:
This Public Health Relevance is not available.
Thesaurus Terms:
acute lymphocytic leukemia, gene expression, neoplasm /cancer relapse /recurrence, pediatric neoplasm /cancer, prognosis, technology /technique development
bone marrow, complementary DNA, genetic marker, longitudinal human study, neoplasm /cancer chemotherapy, neoplasm /cancer diagnosis, neoplasm /cancer genetics
clinical research, flow cytometry, human tissue, microarray technology, polymerase chain reaction

Institution: TELETHON INSTITUTE FOR CHILD HEALTH RES

100 ROBERTS RD

SUBIACO,

Fiscal Year: 2003

Department:

Project Start: 19-JUN-2002

Project End: 30-APR-2004

ICD: NATIONAL CANCER INSTITUTE

IRG: ZCA1

Grant Number:	5R21CA095475-02
Project Title:	Prognosis in childhood ALL

PI Information:	Name	Email	Title
	KEES, URSULA R.	ursula@ichr.uwa.edu.au

Institution:	TELETHON INSTITUTE FOR CHILD HEALTH RES
	100 ROBERTS RD
	SUBIACO,
Fiscal Year:	2003
Department:
Project Start:	19-JUN-2002
Project End:	30-APR-2004
ICD:	NATIONAL CANCER INSTITUTE
IRG:	ZCA1