S9719 Gene Damage Following Chemotherapy in Women With Stage II or Stage III Breast Cancer
Status: | Completed |
---|---|
Conditions: | Breast Cancer, Cancer |
Therapuetic Areas: | Oncology |
Healthy: | No |
Age Range: | 18 - 120 |
Updated: | 4/21/2016 |
Start Date: | November 1997 |
End Date: | February 2001 |
S9719: Clonal Hematopoiesis as a Marker of Genetic Damage Following Adjuvant Chemotherapy for Breast Cancer: Pilot Study to Evaluate Incidence. Ancillary to S9623
RATIONALE: Drugs used in chemotherapy for breast cancer may damage the genes of cells. This
may lead to the development of secondary cancers.
PURPOSE: Pilot study to evaluate the degree of gene damage following chemotherapy in women
with stage II or stage III breast cancer involving four to nine axillary lymph nodes.
may lead to the development of secondary cancers.
PURPOSE: Pilot study to evaluate the degree of gene damage following chemotherapy in women
with stage II or stage III breast cancer involving four to nine axillary lymph nodes.
OBJECTIVES: I. Estimate the incidence of early genetic damage, defined by the presence of
clonal hematopoiesis using the human androgen receptor assay (HUMARA), in pretreatment blood
and bone marrow, apheresis, and two sequential post-treatment specimens from women with
stage II/III breast cancer enrolled in SWOG-S9623. II. Detect genetic damage following
dose-intensive adjuvant regimens for breast cancer by screening for the presence of
defective DNA mismatch repair mechanisms and loss of heterozygosity using microsatellite
instability assays. III. Estimate the incidence of myeloid lymphoid leukemia gene fusion
transcripts in cases where either the HUMARA or microsatellite repeat assays are positive
for clonal hematopoiesis. IV. Determine the frequency of RAS gene mutations (H-, K-, and
N-RAS) following dose-intensive adjuvant regimens for breast cancer.
OUTLINE: Prior to beginning treatment on SWOG-9623, blood samples and bone marrow aspirates
(when available) are collected from each patient. Patients randomized to autologous
peripheral stem cell transplant have specimens collected again at 3 months (apheresis
aliquot and blood). At 3 and 12 months after completing chemotherapy, blood samples are
collected from all patients. Samples are collected again from any patient presenting with a
second malignancy in the future. DNA is collected from blood or bone marrow samples.
Clonality at the HUMARA locus is examined. Microsatellite instability is assessed at
multiple chromosomal loci: 7q31, 5q31, 17p12, 8p22, 11q23, and the BAT loci. If the HUMARA
or microsatellite repeat assays are positive for clonal hematopoiesis, then specimens are
examined for myeloid lymphoid leukemia fusion transcripts commonly reported in acute myeloid
leukemia with 11q23 abnormalities. Specimens are also examined for RAS mutations (H-, K-,
N-RAS). Patients do not receive the results of the genetic testing and the results do not
influence the type or duration of treatment.
PROJECTED ACCRUAL: This study will accrue 100 patients for each arm of SWOG-9623, for a
total of 200 patients.
clonal hematopoiesis using the human androgen receptor assay (HUMARA), in pretreatment blood
and bone marrow, apheresis, and two sequential post-treatment specimens from women with
stage II/III breast cancer enrolled in SWOG-S9623. II. Detect genetic damage following
dose-intensive adjuvant regimens for breast cancer by screening for the presence of
defective DNA mismatch repair mechanisms and loss of heterozygosity using microsatellite
instability assays. III. Estimate the incidence of myeloid lymphoid leukemia gene fusion
transcripts in cases where either the HUMARA or microsatellite repeat assays are positive
for clonal hematopoiesis. IV. Determine the frequency of RAS gene mutations (H-, K-, and
N-RAS) following dose-intensive adjuvant regimens for breast cancer.
OUTLINE: Prior to beginning treatment on SWOG-9623, blood samples and bone marrow aspirates
(when available) are collected from each patient. Patients randomized to autologous
peripheral stem cell transplant have specimens collected again at 3 months (apheresis
aliquot and blood). At 3 and 12 months after completing chemotherapy, blood samples are
collected from all patients. Samples are collected again from any patient presenting with a
second malignancy in the future. DNA is collected from blood or bone marrow samples.
Clonality at the HUMARA locus is examined. Microsatellite instability is assessed at
multiple chromosomal loci: 7q31, 5q31, 17p12, 8p22, 11q23, and the BAT loci. If the HUMARA
or microsatellite repeat assays are positive for clonal hematopoiesis, then specimens are
examined for myeloid lymphoid leukemia fusion transcripts commonly reported in acute myeloid
leukemia with 11q23 abnormalities. Specimens are also examined for RAS mutations (H-, K-,
N-RAS). Patients do not receive the results of the genetic testing and the results do not
influence the type or duration of treatment.
PROJECTED ACCRUAL: This study will accrue 100 patients for each arm of SWOG-9623, for a
total of 200 patients.
DISEASE CHARACTERISTICS: Must be enrolled in SWOG-9623 at time of registration to this
study, but must not have started treatment Hormone receptor status: Not specified
PATIENT CHARACTERISTICS: Age: Adult Sex: Female Menopausal status: Not specified
Performance status: See Disease Characteristics Life expectancy: SWOG 0 or 1
Hematopoietic: See Disease Characteristics Hepatic: See Disease Characteristics Renal: See
Disease Characteristics
PRIOR CONCURRENT THERAPY: See Disease Characteristics
We found this trial at
83
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Cleveland Clinic Taussig Cancer Center At Taussig Cancer Institute, more than 250 highly skilled doctors,...
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Barbara Ann Karmanos Cancer Institute Karmanos is based in southeast Michigan, in midtown Detroit, and...
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Brooke Army Medical Center Brooke Army Medical Center (BAMC) is the Flagship of Army Medicine!...
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CCOP - Greenville Cancer care in the last decade has made many advances. Most of...
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Cancer Research Center of Hawaii The University of Hawaii Cancer Center is the only National...
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University of Mississippi Medical Center The University of Mississippi Medical Center, located in Jackson, is...
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529 West Markham Street
Little Rock, Arkansas 72205
Little Rock, Arkansas 72205
(501) 686-7000
University of Arkansas for Medical Sciences The University of Arkansas for Medical Sciences (UAMS) in...
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10833 Le Conte Avenue # 8-950
Los Angeles, California 90095
Los Angeles, California 90095
(310) 825-5268
Jonsson Comprehensive Cancer Center at UCLA In the late 1960s, a group of scientists and...
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4502 Medical Drive
San Antonio, Texas 78284
San Antonio, Texas 78284
(210) 567-7000
University of Texas Health Science Center at San Antonio The University of Texas Health Science...
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1500 East Medical Center Drive
Ann Arbor, Michigan 48109
Ann Arbor, Michigan 48109
800-865-1125
University of Michigan Comprehensive Cancer Center The U-M Comprehensive Cancer Center's mission is the conquest...
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CCOP - Columbus As one of the original 20 CCOPs, the Columbus Community Clinical Oncology...
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Henry Ford Hospital Founded in 1915 by auto pioneer Henry Ford and now one of...
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1441 Eastlake Ave
Los Angeles, California 90033
Los Angeles, California 90033
(323) 865-3000
U.S.C./Norris Comprehensive Cancer Center The USC Norris Comprehensive Cancer Center, located in Los Angeles, is...
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CCOP - Bay Area Tumor Institute he Bay Area Tumor Institute Community Clinical Oncology Program...
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2315 Stockton Blvd.
Sacramento, California 95817
Sacramento, California 95817
(916) 734-2011
University of California, Davis Medical Center UC Davis Medical Center serves a 65,000-square-mile area that...
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CCOP - Cancer Research for the Ozarks Cancer Research for the Ozarks (CRO), also known...
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