IRSG STUDIES OF ALVEOLAR RHABDOMYOSARCOMA GENE FUSIONS
Project Number5R01CA089461-04
Contact PI/Project LeaderBARR, FREDERIC G
Awardee OrganizationUNIVERSITY OF PENNSYLVANIA
Description
Abstract Text
DESCRIPTION: Alveolar rhabdomyosarcoma (ARMS) is an aggressive soft tissue
tumor of the striated muscle lineage that occurs in children and young adults.
This cancer is associated with 2;13 and 1;13 chromosomal translocations that
juxtapose the PAX3 and PAX7 loci with the FKHR locus to create chimeric genes
encoding PAX3-FKHR or PAX7-FKHR fusion products. To detect these fusions in
tumor specimens, polymerase chain reaction, in situ hybridization, and Southern
blot strategies have been developed. Using these assays, Intergroup
Rhabdomyosarcoma Study Group (IRSG) pilot studies provided evidence to indicate
that these gene fusions are specific markers for ARMS diagnosis, that the
PAX3-FKHR and PAX&-FKHR subtypes are associated with differing outcomes in ARMS
patients, and that high sensitivity assays are capable of detecting clinically
significant submicroscopic metastatic disease. In addition, recent studies
suggest the existence of additional fusion subtypes in ARMS cases that do not
detectably express the typical PAX3-FKHR or PAX7-FKHR fusion transcripts. The
preliminary studies support the hypotheses that fusion gene detection will play
a significant role in the diagnosis, monitoring, and management of ARMS
patients. To further explore this hypothesis in the setting of a large
multi-institutional clinical trial with uniformly treated and diagnosed
patients and centrally collected clinical specimens and clinical data, the IRSG
Biology Committee will study the relationship of fusion subtype to clinical
outcome, other patient characteristics, histopathologic features, and other
biological parameters in the patients prospectively entered on the IRS-V study.
Gene fusion subtype of the primary tumor will be compared with clinical data to
determine the predictive value of these genetic markers in ARMS management.
Fusion negative ARMS tumors will be investigated for variant and cryptic gene
fusions to establish additional fusion categories for consideration in these
clinical correlative studies. Bone marrow and peripheral blood specimens from
these patients will also be assayed to determine the predictive value of
submicroscopic disease detection in metastatic sites. Finally, biological
markers of proliferation and apoptosis status will be examined to determine
their relationship with fusion subtype and other parameters in these patients.
These studies will provide a definitive analysis of the occurrence and clinical
significance of these genetic alterations in ARMS, and will ultimately impact
on the future design of clinical protocols for the treatment of ARMS patients.
Public Health Relevance Statement
Data not available.
NIH Spending Category
No NIH Spending Category available.
Project Terms
DNA damageDNA topoisomerasesapoptosiscell proliferationchromosome translocationclinical researchenzyme activityfluorescent in situ hybridizationgene rearrangementhuman subjectimmunocytochemistrymetastasisneoplasm /cancer geneticspolymerase chain reactionrhabdomyosarcomasouthern blottingtranscription factor
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