Cancer. 9p21.3 deletion. t(12;21) t(15;17)



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CANCER FISH PROBES INDIVIDUAL AND PANEL S Acute Lymphoblastic Leukemia (ALL) ALL FISH Panel (includes all probes below) 8010 LSI MYB/CEP6 LSI p16 (CDKN2A) LSI BCR/ABL with ASS LSI ETV6 (TEL)/AML1 (RUNX1) 6q23 deletion 9p21.3 deletion t(9;22) t(12;21) LSI MLL t(11;?), del (11) Associated with variable prognosis, overall, similar to normal chromosome group. Found in ~5% adult ALL cases and 10-20% childhood ALL. Variable prognosis. Childhood ALL: Frequencies vary in different ALLs, average ~10%. Adult ALL: Found in ~10% adult ALL cases. Associated with poor prognosis. Found in ~20% adult ALL and 2-5% childhood ALL cases. Associated with favorable prognosis. Childhood ALL: Found in 25% B-cell childhood ALL cases. Associated with favorable prognosis. Adult ALL: Found in 1-4% adult ALL. Associated with poor prognosis. MLL rearrangements are found in ~22% of all ALL cases and in 70-90% of infants ALL. Prognosis is dependent on translocation partner. Found in 2-3% of ALL cases. Acute Myeloid Leukemia (AML) AML FISH Panel (includes all probes below) 8000 CEP 8 (D8Z2) Trisomy 8 LSI AML1 (RUNX1)/ETO LSI MLL LSI PML/ RARα LSI CBFB t(8;21) t(11;?), del(11) t(15;17) t(16;16), inv(16) Associated with intermediate to poor prognosis. Found in 10-15% AML cases. 7-12% AML cases. Reported at higher frequency in children than adults. Associated with poor prognosis. MLL-associated rearrangements are found in 10% of all AML cases and in 50% of infants with AML. Associated with favorable prognosis. Found in 5-8% AML cases. Found in ~100% of acute promyelocytic cases. 5-8% AML cases. 1

Chronic Lymphocytic Leukemia (CLL) CLL FISH Panel (includes all probes below) 8040 LSI MYB/ CEP 6 LSI ATM 6q23 deletion Del (11q22) CEP 12 Trisomy 12 LSI p53/cep 17 Del (17p13) Associated with intermediate prognosis. Found in 3-10% CLL cases. Associated with poor prognosis. Found in 12-21% CLL cases. Trisomy 12: Associated with intermediate prognosis. Found in 15-18% CLL cases. Associated with poor prognosis. Found in 5-10% CLL cases. Associated with chemotherapy resistance. Prognosis associated with translocation partner. Determines presence of translocation. Found in 2-7% CLL cases. LSI D13S319/ LSI LAMP1 Mono 13, del (13) Chromosome 13 deletion alone: Associated with favorable prognosis found in 40-55% CLL cases. Myelodysplastic Syndrome (MDS) MDS FISH Panel (includes all probes below) 8005 LSI EGR1/5p15.2 LSI D75486/ CEP 7 Mono 5, del (5) Mono 7, del (7) CEP 8 Trisomy 8 Associated with favorable prognosis as only cytogenetic abnormality in MDS. Associated with poor prognosis in therapy-related MDS/AML or de novo AML (10-25% of cases). Most common cytogenetic abnormality in MDS and AML (found in 20-30% MDS cases). Associated with poor prognosis. Found in ~30% and ~20% cases of RAEB and CMML, respectively. Associated with treatment resistance. Intermediate prognosis as sole abnormality. Found in 10-20% of all MDS and AML cases. About 90% of cases with trisomy 8 as the only chromosome aberration have AML or MDS. LSI MLL t(11;?), del (11) Associated with poor prognosis. LSI D20S108 Del (20q12) 4-5% MDS cases as sole abnormality. 2

Multiple Myeloma (MM) MM FISH Panel (includes all probes below) 8015 CEP 9 Trisomy 9 LSI RB1 Del (13q14.3) CEP 15 Trisomy 15 LSI p53 Del (17p13) Hyperdiploidy associated with favorable prognosis. Found in 12-58% of all MM cases. Associated with poor prognosis. Found in 30-50% of all MM cases. Prognosis associated with translocation partner. Incidence increases with stage of disease. Associated with favorable prognosis if as part of hyperdiploidy. Found in 25-40% of all MM cases. Trisomy 15 is uncommon as the sole chromosomal abnormality. Associated with poor prognosis. Found in 5-10% of cases at time of diagnosis. Non-Hodgkin s Lymphoma (NHL) NHL FISH Panel (includes all probes below) 8020 LSI ALK LSI BCL-6 LSI ATM/p53 t(2;5) t(3;?) Del (11q22), Del (17p11) Found in over 50% of anaplasic large cell lymphoma (ALCL) cases. Associated with favorable prognosis. Increased expression of BCL-6 is found to be associated with favorable prognosis. It is unclear as to what effect a BCL-6 translocation has on prognosis. Found in 5% to 15% of follicular lymphomas, and 20% to 40% of DLBCL cases. Del (11) : The overall incidence in NHL is 4-5%. Found in up to 70% of all mantle cell lymphoma cases. Associated with variable to poor prognosis. Del (17) : Found in 10-15% of follicle center cell lymphoma (FCCL) and mantle cell lymphomas (MCL). Associated with poor prognosis. Limited prognostic significance. IGH translocations found in ~50% of all NHLs, 12-35% of diffuse large B-cell lymphomas (DLBCL), ~ 90% of follicular lymphoma cases, 50-70% cases of MCL, and 20-60% of marginal zone lymphoma (MZL) cases. Used as diagnostic depending on translocation partner. 3

ALL LSI ETV6 (TEL)/AML1 (RUNX1) t(12;21) ALL TCF3/PBX1 t(1;19)(q23;p13) ALL/AML LSI MLL t(11;?), del(11) AML LSI CBFB t(16;16), inv(16) AML AML Bone Marrow Transplantation Brain Cancer Breast Cancer LSI AML1 (RUNX1)/ETO LSI PML/ RARα X/Y 1p/19q CEP ERBB2 (HER2/neu) t(8;21) t(15;17) DXZ1/DYZ3 1p36-19q13 codeletion 17q12 amplification Associated with favorable prognosis. Childhood ALL: Found in 25% B-cell childhood ALL cases. Associated with favorable prognosis. Adult ALL: Found in ~5% adult ALL. This test detects t(1;19)(q23;p13) translocation in ALL. The chromosome anomaly is associated with adverse prognostic features. ALL: Associated with poor prognosis. MLL rearrangements are found in ~22% of all ALL cases and in 70-90% of infants ALL. AML: Associated with poor prognosis. MLL rearrangements are found in 10% of all AML cases and in 50% of infants with AML. 5-8% AML cases. 7-12% AML cases. Reported at higher frequency in children than adults. 5-8% AML cases. Found in ~100% of all acute promyelocytic cases. This test determines the level of donor bone marrow engraftment for sex mismatched bone marrow transplantation. Combined 1p36-19q13 deletions are highly associated with classic oligodendroglioma histology and a longer survival rate Associated with poor prognosis. Found in ~30% of all breast cancer cases. HER2/neu overexpression predicts sensitivity to trastuzumab treatment Burkitt's lymphoma LSI MYC t(8;?) Found in 75-90% cases of Burkitt's lymphoma. 8760 CML/ALL/AML LSI BCR/ABL t(9;22) Follicular Lymphoma /BCL2 t(14;18) CML: Limited prognostic significance. Found in ~95% of CML cases. Favorable prognosis compared to BCR/ABL negative CML. ALL: Associated with poor prognosis. Found in ~25% to 44% adult ALL cases. AML: Found in less than 1% of AML cases. Associated with poor prognosis. Limited prognostic significance. Found ~90% and ~30% of all follicular lymphomas and DLBCL cases. Hypereosinophilic Syndrome CHIC2 Del (4q12) Uncertain at this time. 8730 Lung Cancer, Colorectal Cancer, triple-negative Breast Cancer EGFR 7p12 amplification The presence of EGFR amplification is associated with a poor prognosis but may predict response to various EGFR-targeted therapies. 8755 8080 8745 8740 8725 8735 8065 8055 8025 8750 8765 8035 4

Lung Cancer (NSCLC) LSI ALK t(2;?) Lung Cancer (NSCLC) LSI MET 7q31 implication Lung Cancer (NSCLC) LSI ROS1 t(6;?) Mantle Cell Lymphoma (MCL) / CCND1 t(11;14) Associated with favorable prognosis compared to NSCLC without a rearrangement. ALK rearrangements are found in 3-5% NSCLC. FDA-approved companion diagnostic for ALK inhibitor, Xalkori. Found in 2-4% of previously untreated NSCLC cases. Found in 5-20% of cases with EGFRmutated tumors and is correlated with aquired reisitance to EGFR TKIs. Found in 1-2% of NSCLC cases. May respond to crizotinib treatment. Limited prognostic significance. Diagnostic for MCL. Found in 50-70% of cases. 8030 8095 8781 8770 MDS CEP 8 Trisomy 8 MDS LSI EGR1/5p15.2 Mono 5, del (5) MDS LSI D20S108 Del (20q12) MDS LSI D75486/ CEP 7 Mono 7, del (7) Synovial Sarcoma SS18 t(x;18)(p11.2;q11.2) Intermediate prognosis as sole abnormality. Found in 10-20% of all MDS and AML cases. About 90% of cases with trisomy 8 as the only chromosome aberration have AML or MDS. Associated with favorable prognosis as only cytogenetic abnormality in MDS. Poor prognosis with associated with therapy and de novo-related MDS/AML (10-25% of cases). Most common cytogenetic abnormality in MDS and AML (found in 20-30% MDS cases). 4-5% MDS cases as sole abnormality. Associated with poor prognosis. Found in ~30% and ~20% cases of RAEB and CMML, respectively. Associated with treatment resistance. Identification of t(x;18)(p11.2;q11.2) or its variant in synovial sarcoma. A t(x;18)(p11.2;q11.2) translocation or its variant is found in almost all synovial sarcomas at all the histologic types. 8385 8710 8720 8715 8075 5