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Abstract

Grant Number: 5R01CA051105-17

Project Title: HUMAN V(D)J RECOMBINASE IN NEOPLASTIC AND PRIMARY CELLS

PI Information: Name Email Title

LIEBER, MICHAEL R. lieber@usc.edu PROFESSOR

Abstract: Description: (Adapted from the investigator's abstract) V(D)J recombination is responsible for mistaken chromosomal translocations in almost 50% of human lymphoid malignancies. The goal of this proposal is to determine the molecular basis for how these chromosomal translocations occur. Three specific hypotheses for such chromosomal translocations are proposed, and experimental strategies are described to test these proposed mechanisms. The first hypothesis (Aim 1) proposes misrecognition of cryptic heptamer/nonamer signal sequences. This hypothesis can be tested by utilizing the human V(D)J recombination assay developed by the investigator. The major breakpoint regions for bcl-2, SCL, SIL, Hox11, Ttg-1, and LMO2 will be quantitatively tested for their recombination activity. The effect of transcription through these regions and the effect of the surrounding DNA sequences will be tested. The second hypothesis (Aim 2) proposes that signal end intermediates of V(D)J recombination function as transposons and catalyze chromosomal translocations. This mechanism will be tested in lymphoid cells from normal individuals and from cells derived from lymphoid malignancies. This mechanism could account for reciprocal translocations or in isolated chromosome breaks that are then paired with V, D, or J segments. The third hypothesis (Aim 3) proposes that some major breakpoint regions are prone to breakage not because they are misrecognized for cutting by the V(D)J recombination enzymes, but rather because they are fragile and subject to nuclease action (breakage) because they assume a non-B DNA conformation. The investigator proposes to examine the structure of DNA sequences at translocation breakpoints. Corresponding studies of such regions on minichromosomes will permit the testing of the effects of the direction of DNA replication and transcription.
Public Health Relevance:
This Public Health Relevance is not available.
Thesaurus Terms:
blood /lymphatic neoplasm, chromosome translocation, genetic recombination, neoplastic cell, recombinase
enzyme activity, genetic transcription, immunogenetics, neoplasm /cancer genetics, nucleic acid sequence, transposon /insertion element
human tissue

Institution: UNIVERSITY OF SOUTHERN CALIFORNIA

DEPARTMENT OF CONTRACTS AND GRANTS

LOS ANGELES, CA 90033

Fiscal Year: 2004

Department: PATHOLOGY

Project Start: 01-JAN-1990

Project End: 31-AUG-2005

ICD: NATIONAL CANCER INSTITUTE

IRG: PTHB

Grant Number:	5R01CA051105-17
Project Title:	HUMAN V(D)J RECOMBINASE IN NEOPLASTIC AND PRIMARY CELLS

PI Information:	Name	Email	Title
	LIEBER, MICHAEL R.	lieber@usc.edu	PROFESSOR

Institution:	UNIVERSITY OF SOUTHERN CALIFORNIA
	DEPARTMENT OF CONTRACTS AND GRANTS
	LOS ANGELES, CA 90033
Fiscal Year:	2004
Department:	PATHOLOGY
Project Start:	01-JAN-1990
Project End:	31-AUG-2005
ICD:	NATIONAL CANCER INSTITUTE
IRG:	PTHB