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ALL in which the Philadelphia chromosome is present

Last reviewed dd mmm yyyy. Last edited dd mmm yyyy

Authoring team

The presence of the Philadelphia chromosome in patients with ALL is a poor prognostic factor:

  • occurs in 20-30% of adult ALL and in 3% of childhood ALL (1)

  • prior to the advent of tyrosine kinase inhibitors (TKI), Ph+ ALL was associated with a very poor prognosis despite the use of intensive chemotherapy and frequently hematopoietic stem-cell transplantation (HSCT) in first remission
    • development of TKIs revolutionized the therapy of Ph+ ALL. Addition of the first generation ABL1 class TKI imatinib to intensive chemotherapy dramatically increased the survival for children with Ph+ ALL and established that many patients can be cured without HSCT (2)

  • in patients with ALL and a Philadelphia chromosome:
    • 1/3 - have M-bcr (major breakpoint-cluster region) rearrangements (resulting in a 210-kd protein) similar to those in patients with CML
    • 2/3 - have m-bcr (minor breakpoint-cluster region) rearrangements with a consequent 190-kd protein
    • outcome for patients with either variant is equally poor

Reference:


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