One side of (o, m and p) benzene diamine reacted with aromatic aldehyde to give Schiff bases (Ia-d) or (IIa-d) and (IIIa-d) respectively. The second amine group of the synthesized Schiff bases (Ia-d or IIa-d and IIIa-d) was reacted with substituted-9-chloroacridine to give the final compounds namely N-(Substituted benzylidene)-N'-(Substituted acridine-9-yl) (1,2 or 1,3 and 1,4) benzene diamine (V,VI,VII).The reaction progress was followed by thin layer chromatography (TLC), and R f values were recorded. I.R. Spectral data for all the synthesized derivatives were reported. The U.V-Vis., and the 1 HNMR(300and 400MHz) were recorded for some derivatives to support the structure of the synthesized compounds.
Objective: To evaluate the cytogenetic, molecular response, effect particularly on bone and heart for imatinib and nilotinib respectively in patients with chronic myeloid leukemia (CML). Methods: The study was conducted on eighty seven patients on imatinib and twenty nine patients on nilotinib as second line treatment who were treated at Ibn-Sena Teaching Hospital /Outpatient Hematology Department were reviewed from April 2002 to April 2014. The Fluorescent in situ hybridization (FISH) analysis was carried on at central authorized laboratory in Baghdad. The reverse transcriptase-polymerase chain reaction (RT-PCR) carried on authorized laboratory initially in Baghdad then in Mosul, (both laboratory using the same standard and sponsored by Novartis). To study the effect of imatinib mesylate on bone mineral density fifty out of 87 patients were enrolled for this purpose. For all the patients ionized calcium, total calcium, serum albumin, serum alkaline phosphatase, serum phosphate, urea, creatinine and serum levels of intact parathyroid hormone measured at baseline, 6 months and 12 months. Dual energy X-ray absorptiometry (DEXA) measurements of the lumbar spine (L2-L4 vertebrae), and femoral neck were performed using a DEXA scanner. For the nilotinib group, all patients had a base-line standard 12-lead electrocardiography (ECG), with a follow-up ECG's performed every 6 months during the study period to assess any occurrence of QT prolongation, ischemic changes, or arrhythmias Noninvasive cardiac imaging was performed using the resting transthoracic Echocardiography (Echo) with its 2-dimentional and M-mode views. Results: The median duration of CML is 8 years (range 4-12) and the median duration of treatment by the first generation of the brand tyrosine kinase inhibitor is 8 years (range 4-12). Of the 87 patients who were eligible for follow up 86 (98.8%) achieved complete and major cytogenetic response and 86.21% have complete and major molecular response. For those on nilotinb 68.94% have complete and major cytogenetic and molecular response. The overall survival rate is 86.20% at 12 year of imatinib therapy. The 5 years survival rate after nilotinib treatment is 68.94% (20 out of 29). DEXA analysis revealed no significant changes in L2-L4 lumbar vertebral bone mineral density (BMD) but there is significant change at femoral neck. Prolongation of QTcF was observed in 80% of patients on nilotinib with a mean of 13.56 millisecond. There were no significant difference in left ventricular ejection fraction % from the baseline and none of the patient develop major cardiac event. Conclusion: Complete and major molecular response is 86.20% on imatinib therapy whereas it is 68.94% on nilotinib as second line therapy. The overall survival rate is 86.20% at 12 year of imatinib therapy. The 5 years survival rate after nilotinib treatment is 68.94%. Significant decrease in femoral neck bone mineral density (BMD) observed after 12 month time point. Nilotinib prolonged the QTcF interval by an average of 13.56 millisecond with no...
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