CEBPA Full Gene Sequence with Interpretation, Bone Marrow
| Label Mnemonic: | CEBBM |
| Epic code: | LAB7765 |
| Order form: | Comprehensive Hematopathology Requisition |
| Supply order: | Supply Order Form |
| Billing: | Billing Policies |
| CPT code: | 81218 |
Specimen(s):
Bone Marrow Aspirate
Formalin fixed, paraffin-embedded tissue
Formalin fixed, paraffin-embedded tissue
Collection Medium:
|
| Pink top tube 6 mL (K2-EDTA) |
Minimum:
2 mL bone marrow aspirate. Specimens for which the AML blast count
is at least 20% will be tested. Testing on specimens with a lower
blast count may be attempted with approval of lab director. However,
such testing is not recommended due to the increased possibility of
a false- negative result.
Rejection Criteria:
Blast count less than 20%, hemolyzed, green top, decalcified bone
marrow.
Testing Schedule:
Weekly
Turn Around Time:
7-10 working days
Reference Range:
Unaffected samples will lack disease-associated
CEBPA mutations, but may harbor previously identified
single nucleotide polymorphisms (SNPs) that are reported as
incidental findings.
Comments:
In the bone marrow, the CCAAT/enhancer-binding protein, alpha
(CEBPA) is a myelomonocytic lineage-specific transcription factor
that promotes myeloid differentiation (1). Mutations in the
CEBPA
gene have been reported in acute myelogenous leukemia (AML; 5-14% of
cases) and myelodysplastic syndromes (2-7). In the absence of other
genetic lesions known to confer a poor prognosis (e.g.,
FLT3-ITD mutation), mutations in CEBPA are
associated with a favorable prognosis for AML. However, the benefit
appears to be restricted to cases in which there are biallelic
CEBPA mutations, often consisting of two discrete (compound
heterozygous) mutations affecting different functional domains of
the CEBPA protein (3-5). A variety of inactivating point mutations,
deletions and insertions have been described, requiring evaluation
of the entire CEBPA coding sequence.
References
1. Zhang P, et al. Immunity 2004;21(6):853-63.
2. Nerlov C. Nature Reviews Cancer 2004;4(5):394-400.
3. Dufour A, et al. J Clin Oncol 2010;28(4):570-7.
4. Wouters BJ, et al. Blood 2009;113(13):3088-91.
5. Taskesan E, et al. Blood 2011;117:2469-75.
6. Gombart AF, et al. Blood 2002;99(4):1332-1340.
7. Shih LY, et al. Clin Cancer Res 2005;11(5):1821-26.
References
1. Zhang P, et al. Immunity 2004;21(6):853-63.
2. Nerlov C. Nature Reviews Cancer 2004;4(5):394-400.
3. Dufour A, et al. J Clin Oncol 2010;28(4):570-7.
4. Wouters BJ, et al. Blood 2009;113(13):3088-91.
5. Taskesan E, et al. Blood 2011;117:2469-75.
6. Gombart AF, et al. Blood 2002;99(4):1332-1340.
7. Shih LY, et al. Clin Cancer Res 2005;11(5):1821-26.
Test Limitations:
20% mutant allele
Methodology:
PCR amplification of CEBPA-specific fragments followed by
DNA cycle sequencing (Sanger method).
Instructions:
Testing is generally not available on a STAT basis. However,
expedited testing can be arranged by contacting the Molecular
Pathology Laboratory at 384-9568 or the Molecular Genetic Pathology
Fellow (pager #8682).
Sample Processing:
Label transport tube with two patient identifiers, date and time of
collection.
Patient's age and sex is required on requisition for processing.
Relevant clinical information must be submitted with specimen in order to provide correct interpretation of test results.
Patient's age and sex is required on requisition for processing.
Relevant clinical information must be submitted with specimen in order to provide correct interpretation of test results.
Sample Storage:
Refrigerate.
Transport Instructions:
Place requisition into outside pocket of bag.
Recommend early AM overnight shipping or equivalent if not on courier service.
Ship refrigerated.
Recommend early AM overnight shipping or equivalent if not on courier service.
Ship refrigerated.