0521779407-C02 CUNY1086/Karliner 0 521 77940 7 June 4, 2007 20:53
Chronic Myelogenous Leukemia 3391–2 mg P0 qd as maintenance until count l0,000, then stop. Can com-
promise the ability of a patient to be transplanted and therefore not
used for primary therapy.Side Effects & Contraindications
■Interferon-alpha: flu-like symptoms (fatigue, myalgia, fever, bone
pain), rash, depression
■Contraindication – known hypersensitivity to interferon or vehicle
■Cytarabine: myelosuppression, mucositis, diarrhea, alopecia; Con-
traindication – known hypersensitivity to cytarabine or vehicle
■Hydroxyurea: myelosuppression, mucositis, diarrhea, rash, nausea
■Contraindication – known hypersensitivity to cytarabine or vehicle
■Busulfan: myelosuppression, marrow aplasia, mucositis, diarrhea,
hyperpigmentationfollow-up
■For responding patients on imatinib, especially potential trans-
plant candidates, frequent surveillance (∼q 3 months) of symptoms,
blood counts, and Q-PCR for changes in bcr/abl level are recom-
mended. Evidence for imatinib resistance or disease acceleration
should prompt rapid intervention with increased dose of imatinib,
second-generation abl kinase inhibitor, or transplantation for those
who are candidates.complications and prognosis
■Patients who respond to imatinib with complete cytogenetic
response and 3- to 5-fold reduction of bcr/abl transcripts have excel-
lent prognosis. It is unknown if such patients are “clinically cured,”
as follow-up times are still relatively short.
➣∼4% of patients on imatinib will develop resistance per year. Such
patients may be salvaged with higher doses of imatinib, second-
generation abl kinase inhibitors, use of the above-mentioned
cytostatic or cytotoxic agents alone or in combination, or prefer-
ably stem cell transplant if the patient is still in chronic phase of
disease.
➣Prognosis is poor for patients who cannot be transplanted and
who develop abl kinase inhibitor resistance. GVHD remains the
major complication of allogeneic stem cell transplantation.
➣Patients who relapse after allogeneic stem cell transplantation
can be salvaged by donor lymphocyte infusions. Vaccines and
other forms of immunotherapy are under investigation and may
prove useful.