Differences

This shows you the differences between two versions of the page.

Link to this comparison view

Both sides previous revision Previous revision
Next revision
Previous revision
group_5_presentation_2_-_chronic_myeloid_leukemia [2016/03/11 16:26]
hanaf2
group_5_presentation_2_-_chronic_myeloid_leukemia [2018/01/25 15:18] (current)
Line 1: Line 1:
 +{{:​cml.jpg|}}
  
-{{:screen_shot_2016-03-09_at_2.51.36_pm.png?​750}} +Powerpoint:  
 +{{:group_5_chronic_myeloid_leukemia.pptx|}}
  
 ====== CHRONIC MYELOID LEUKEMIA ====== ====== CHRONIC MYELOID LEUKEMIA ======
Line 37: Line 38:
 ===== Pathogenesis ===== ===== Pathogenesis =====
  
-Chronic Myeloid Leukemia (CML) is a result of the reciprocal translocation between chromosome 9 and chromosome 22 (Apperley, 2015). Abnormal chromosome 22 is also referred to as the Philadelphia chromosome (Ph), since it was in Philadelphia,​ USA where scientists first discovered it (Apperley, 2015). The Abl  gene is a non-receptor tyrosine kinase and is located on chromosome 9 (Corey & Cortes, 2010). Abl stands for Abelson murine Leukemia and it is the v-abl oncogene (viral gene) human homologue (Deniniger et al., 2000). SH1, SH2 and SH3 are the 3 SRC homology domains found on Abl (Deniniger et al., 2000). SH1 domain is important in carrying out tyrosine kinase function, whereas SH2 & SH3 allow Abl to interact with other proteins (Deniniger et al., 2000). ​The Bcr gene is located on chromosome 22, and it is a serine/​threonine kinase that is involved in the activation of RAc and CDc42 GTPases (Corey & Cortes, 2010). Bcr stands for breakpoint cluster region, due to the different breakpoints that are found  at the site for transcription (Corey & Cortes, 2010). Chromosome 9 has a constant breakpoint, whereas, chromosome 22 can have breakpoints in up to 3 different areas: m-bcr, M-bcr, and µ-bcr (Hurtado et al., 2007). These three breakpoints produce proteins that contain different molecular weights: p190, p210, or p230 (Hurtado et al., 2007). The protein with molecular weight p210 is the one that is seen in 95% of CML patients (Hurtado et al., 2007).+Chronic Myeloid Leukemia (CML) is a result of the reciprocal translocation between chromosome 9 and chromosome 22 (Apperley, 2015). Abnormal chromosome 22 is also referred to as the Philadelphia chromosome (Ph), since it was in Philadelphia,​ USA where scientists first discovered it (Apperley, 2015). The Abl  gene is a non-receptor tyrosine kinase and is located on chromosome 9 (Corey & Cortes, 2010). Abl stands for Abelson murine Leukemia and it is the v-abl oncogene (viral gene) human homologue (Deniniger et al., 2000). SH1, SH2 and SH3 are the 3 SRC homology domains found on Abl (Deniniger et al., 2000). SH1 domain is important in carrying out tyrosine kinase function, whereas SH2 & SH3 allow Abl to interact with other proteins (Deniniger et al., 2000). 
 + 
  
-{{:group5pic8.png?550}}+{{:group5pic9.png|}}
  
-**Figure 4**: Abl gene with its respective exons+**Figure 4**: Abl gene with its respective exons 
  
-{{:group5pic9.png?550}}+The Bcr gene is located on chromosome 22, and it is a serine/​threonine kinase that is involved in the activation of RAc and CDc42 GTPases (Corey & Cortes, 2010). Bcr stands for breakpoint cluster region, due to the different breakpoints that are found  at the site for transcription (Corey & Cortes, 2010). Chromosome 9 has a constant breakpoint, whereas, chromosome 22 can have breakpoints in up to 3 different areas: m-bcr, M-bcr, and µ-bcr (Hurtado et al., 2007). These three breakpoints produce proteins that contain different molecular weights: p190, p210, or p230 (Hurtado et al., 2007). The protein with molecular weight p210 is the one that is seen in 95% of CML patients (Hurtado et al., 2007). 
 + 
 +{{:group5pic8.png?550}}
  
 **Figure 5**: Bcr gene with its respective exons **Figure 5**: Bcr gene with its respective exons
Line 75: Line 79:
 ===== Therapeutics ===== ===== Therapeutics =====
  
-==== Options: ​==== +=== Options: ===
  
 The only truly curative treatment is bone marrow transplant or allogeneic stem cell transplant. However, these treatments can be invasive and hence other treatment options include tyrosine kinase inhibitors. The only truly curative treatment is bone marrow transplant or allogeneic stem cell transplant. However, these treatments can be invasive and hence other treatment options include tyrosine kinase inhibitors.
Line 83: Line 87:
 **Figure 9**: Curative treatment options for CML  **Figure 9**: Curative treatment options for CML 
  
-==== Inhibiting Bcr-Abl as a potential drug target: ​====+=== Inhibiting Bcr-Abl as a potential drug target: ===
  
 CML is caused by the reciprocal translocation between chromosome 9 (location of Abl1 gene) and 22 (location of BCR gene) which creates the Philadelphia chromosome. This molecular pathogenesis generates the Bcr-Abl fusion protein which has elevated tyrosine kinase activity. The Bcr-Abl fusion protein is found predominately in CML cells and thus provides the desired specificity (minimized systemic toxicity) for an inhibitor or therapeutic to interfere with this fusion protein’s function (Deininger, Goldman, Melo 2000). It is easy to target the ATP pocket of this fusion protein (something common to kinase proteins) than other protein-protein interactions as ATP pockets are well defined and mimicking ATP is an easy starting point for drug development (Deininger, Goldman, Melo 2000). ​ CML is caused by the reciprocal translocation between chromosome 9 (location of Abl1 gene) and 22 (location of BCR gene) which creates the Philadelphia chromosome. This molecular pathogenesis generates the Bcr-Abl fusion protein which has elevated tyrosine kinase activity. The Bcr-Abl fusion protein is found predominately in CML cells and thus provides the desired specificity (minimized systemic toxicity) for an inhibitor or therapeutic to interfere with this fusion protein’s function (Deininger, Goldman, Melo 2000). It is easy to target the ATP pocket of this fusion protein (something common to kinase proteins) than other protein-protein interactions as ATP pockets are well defined and mimicking ATP is an easy starting point for drug development (Deininger, Goldman, Melo 2000). ​
Line 93: Line 97:
 **Figure 10**: Bcr-Abl kinase being inhibited by a compound, imatinib, in red **Figure 10**: Bcr-Abl kinase being inhibited by a compound, imatinib, in red
  
-==== Gleevec: a tyrosine kinase inhibitor ​=====+=== Gleevec: a tyrosine kinase inhibitor ===
  
 Gleevec (imatinib mesylate) is a therapeutic that was FDA approved for CML treatment in 2001. It is now used to treat gastrointestinal stroll tumours (Pray, 2008). Though at first the rationale was that Gleevec would compete with ATP in the active Bcr-Abl conformer, however that wasn't the case. Gleevec doesn’t compete with ATP, instead it just keeps the kinase in a closed state preventing ATP from binding to the conformer. There has been vast improvement seen for CML patient survival over other therapeutics. However, there is acquired drug resistance seen too. Drug resistance is common for chemotherapies due to prolonged exposure to drugs. In particular, some CML cell populations survive due to a genetic mutation in Bcr-Abl, giving rise to a new population of Bcr-Abl CML cells that are resistant to Gleevec. This mutation is at Thr315Ile location and it pushed Gleevec out of its pocket (Pray, 2008). ​ Gleevec (imatinib mesylate) is a therapeutic that was FDA approved for CML treatment in 2001. It is now used to treat gastrointestinal stroll tumours (Pray, 2008). Though at first the rationale was that Gleevec would compete with ATP in the active Bcr-Abl conformer, however that wasn't the case. Gleevec doesn’t compete with ATP, instead it just keeps the kinase in a closed state preventing ATP from binding to the conformer. There has been vast improvement seen for CML patient survival over other therapeutics. However, there is acquired drug resistance seen too. Drug resistance is common for chemotherapies due to prolonged exposure to drugs. In particular, some CML cell populations survive due to a genetic mutation in Bcr-Abl, giving rise to a new population of Bcr-Abl CML cells that are resistant to Gleevec. This mutation is at Thr315Ile location and it pushed Gleevec out of its pocket (Pray, 2008). ​
Line 101: Line 105:
 **Figure 11**: Pharmacodynamics of imatinib, Gleevec **Figure 11**: Pharmacodynamics of imatinib, Gleevec
  
-==== Results from tyrosine kinase inhibitors: ​====+=== Results from tyrosine kinase inhibitors: ===
 In the study by Deininger, Goldman, Lydon and Melo (1997), Bcr-Abl positive CML cells were exposed to tyrosine kinase inhibitor CGP57148B. Of all the cell lines examined, most showed a drastic reduction showing that tyrosine kinase inhibitors were effective in treating CML cells. Two cells that were resistant to the initial 1.0uM were treated with 10uM of the inhibitor. ​ In the study by Deininger, Goldman, Lydon and Melo (1997), Bcr-Abl positive CML cells were exposed to tyrosine kinase inhibitor CGP57148B. Of all the cell lines examined, most showed a drastic reduction showing that tyrosine kinase inhibitors were effective in treating CML cells. Two cells that were resistant to the initial 1.0uM were treated with 10uM of the inhibitor. ​
  
Line 108: Line 112:
 **Figure 12**: Results from study showing effectiveness of tyrosine kinase inhibitors on Bcr-Abl positive CML cells **Figure 12**: Results from study showing effectiveness of tyrosine kinase inhibitors on Bcr-Abl positive CML cells
  
-==== Implications of treatment: ​====+=== Implications of treatment: ===
 One strategy to overcome resistance is to develop new inhibitors of Bcr-Abl. For example, Dasatinib inhibits most Bcr-Abl mutants, except for the Thr351Ile mutant. Also Ponatinib is able to inhibit the T35I mutant (Shah, Tran, Lee, Chen, Norris, Sawyers 2004). ​ One strategy to overcome resistance is to develop new inhibitors of Bcr-Abl. For example, Dasatinib inhibits most Bcr-Abl mutants, except for the Thr351Ile mutant. Also Ponatinib is able to inhibit the T35I mutant (Shah, Tran, Lee, Chen, Norris, Sawyers 2004). ​
  
Print/export
QR Code
QR Code group_5_presentation_2_-_chronic_myeloid_leukemia (generated for current page)