ALL, Childhood Clinical Trial
Official title:
Detection of IKZF1 Deletion Mutation in Patients With Acute Lymphoblastic Leukemia and Its Impact in Therapy
1. To detect IKZF-1 deletion mutations in patients with ALL.
2. To study the impact of IKZF-1 deletion mutation on therapy of ALL.
3. To study the correlation between IKZF-1 deletion mutations and BCR-ABL.
Acute lymphoblastic leukemia (ALL) a malignant transformation and proliferation of lymphoid
progenitor cells in the bone marrow, blood and extramedullary sites. While 80% of ALL occurs
in children, it represents a devastating disease when it occurs in adults . predisposing
factors include exposure to ionizing radiation, pesticides, certain solvents or viruses such
as Epstein-Barr Virus and Human Immunodeficiency Virus. However, in the majority of cases, it
appears as a de novo malignancy in previously healthy individuals. Chromosomal aberrations
are the hallmark of ALL, but are not sufficient to generate leukemia. Characteristic
translocations include t(12;21) [ETV6-RUNX1], t(1;19) [TCF3-PBX1], t(9;22) [BCR-ABL1] . More
recently, a variant with a similar gene expression profile to (Philadelphia) Ph-positive ALL
but without the BCR-ABL1 rearrangement has been identified. In more than 80% of cases of this
so-called Ph-like ALL, the variant possesses deletions in key transcription factors involved
in B-cell development including IKAROS family zinc finger 1 (IKZF1) . IKZF1 codes Ikaros,
which is a member of a family of zinc- finger nuclear proteins that is required for the
earliest stages of lymphoid lineage commitment and acts as tumor suppressor. Most IKZF1
mutations (94%) are deletion mutations, and there are rare point mutations resulting in loss
of function of Ikaros .
There are two major deletions occur in the IKZF1 gene:
- The first one was characterized by loss of exons 4 to 7 ( 4-7) with breakpoints
occurring in introns 3 and 7 on chromosome 7p12.
- The second deletion involved exons 2 to 7 ( 2-7) with a variable pattern of breakpoints
in intron 1 and intron 7 in the same region as those of the 4-7 deletion.
IKZF1 mutations in cases of B-ALL are associated with poor prognosis and high risk of
relapse. IKZF1 mutations are found in approximately 15% to 20% of pediatric B-ALL cases and
in >75% of pediatric BCR-ABL positive ALL cases. The incidences of IKZF1 mutations in adults
are approximately 50% in B-ALL cases and approximately 65% in BCR-ABL positive ALL cases .
The presence of either IKZF1 mutation or BCR- ABL has been reported to be an independent risk
factor of poor prognosis for patients with B-ALL .
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