Imatinib sensitizes CLL lymphocytes to chlorambucil

Aloyz, Raquel; Grzywacz, Kelly; Xu, Zuyan; Loignon, Martin; Ma, Alaoui-Jamali; Panasci, Lawrence C.

doi:10.1038/sj.leu.2403247

Cited by 56 publications

(48 citation statements)

References 25 publications

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“…Preclinical evidence suggests that imatinib may enhance chemosensitivity by several possible mechanisms, including decreasing interstitial fluid pressure (Heuchel et al, 1999;Pietras et al, 2001Pietras et al, , 2002Pietras et al, , 2003Ostman, 2004), decreasing angiogenesis (Bergers et al, 2003;Dudley et al, 2003;Hwang et al, 2003;Uehara et al, 2003;Apte et al, 2004;Pietras and Hanahan, 2005), and by affecting DNA repair mechanisms (Aloyz et al, 2004), stromal chemokines (Ostman, 2004), and multidrug transporter activity (Houghton et al, 2004;Ozvegy-Laczka et al, 2004). However, the uptake and distribution of imatinib in the brain is limited by P-gp/BCRP-mediated efflux (Dai et al, 2003), suggesting that combination regimens with imatinib may be more effective than imatinib monotherapy.…”

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Multicentre phase II studies evaluating imatinib plus hydroxyurea in patients with progressive glioblastoma

Dresemann²,

et al. 2009

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We evaluated the efficacy of imatinib mesylate in addition to hydroxyurea in patients with recurrent glioblastoma (GBM) who were either on or not on enzyme-inducing anti-epileptic drugs (EIAEDs). METHODS: A total of 231 patients with GBM at first recurrence from 21 institutions in 10 countries were enrolled. All patients received 500 mg of hydroxyurea twice a day. Imatinib was administered at 600 mg per day for patients not on EIAEDs and at 500 mg twice a day if on EIAEDs. The primary end point was radiographic response rate and secondary end points were safety, progression-free survival at 6 months (PFS-6), and overall survival (OS). RESULTS: The radiographic response rate after centralised review was 3.4%. Progression-free survival at 6 months and median OS were 10.6% and 26.0 weeks, respectively. Outcome did not appear to differ based on EIAED status. The most common grade 3 or greater adverse events were fatigue (7%), neutropaenia (7%), and thrombocytopaenia (7%). CONCLUSION: Imatinib in addition to hydroxyurea was well tolerated among patients with recurrent GBM but did not show clinically meaningful anti-tumour activity.

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Multicentre phase II studies evaluating imatinib plus hydroxyurea in patients with progressive glioblastoma

Dresemann²,

et al. 2009

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“…6 In conclusion, these results support the notion that Imatinib applied in clinically achievable concentrations may sensitize The interesting results reported by Dr Chow et al are complementary to our findings, bringing insights into the possible mechanism of STI571-induced apoptosis in primary CLL lymphocytes. 1,2 The authors suggest the involvement of a new apoptotic pathway involving the caspase 3 activator, prostate apoptosis response gene 4 (Par-4). Moreover, Par-4 protein levels looks to correlate with the responsiveness to STI571 in a panel of six of CLL primary lymphocytes.…”

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“…Moreover, Par-4 protein levels looks to correlate with the responsiveness to STI571 in a panel of six of CLL primary lymphocytes. 1 Interestingly, it has been proposed that caspase-3 induction is involved in chlorambucil (CLB)-induced CLL lymphocytes apoptosis. 3 In this regard, the fact that we did not find a correlation between the CLB and STI571 IC 50 when used alone suggests that the mechanisms downstream of STI571 and CLBinduced apoptosis are not identical.…”

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“…3 In this regard, the fact that we did not find a correlation between the CLB and STI571 IC 50 when used alone suggests that the mechanisms downstream of STI571 and CLBinduced apoptosis are not identical. 1 Thus, it will be informative to assess the involvement of Par-4 protein levels in CLB-induced apoptosis in primary CLL lymphocytes. If STI571 induces Par-4 while CLB does not, the mechanism of action proposed by Dr …”

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Imatinib induces apoptosis in CLL lymphocytes with high expression of Par-4

Nowak

Hofmann

et al. 2005

Leukemia

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It is known that more than 95% of the serum ALP activity is derived from hepatocytes and osteoblasts. Therefore, in patients with normal liver function, serum ALP seems available as the index of bone formation. Indeed, serum ALP as well as BAP levels were elevated in our case after bortezomib-combined therapy. Bisphosphonate has been reported as the potent inhibitor of osteoclastic activity and to reduce the skeletal complications in MM. 4 But our patient did not show the definite elevation of serum ALP levels after prior incadronate-containing salvage therapy, and the inability of bisphosphonate to repair lytic bone lesions indicates that the functional defect of osteoblasts is also important in the lytic process. 5 In this case, he showed the remarkable elevation of serum ALP as well as BAP levels after receiving bortezomib in combination with incadronate and dexamethasone. Our case suggested that bortezomib might have an effect on the osteoblastic activity in addition to antimyeloma activity. The possible mechanism is the rapid disappearance of myeloma cells induced by bortezomib. Myeloma cells secrete at least two molecules that modulate the bone microenvironment in a manner favorable to tumor growth. Receptor activator of NF-kB ligand (RANKL) acts to stimulate osteoclast formation and activity, leading to bone erosion, whereas dickkopf1 (DKK1) appears to inhibit osteoblasts by the Wnt signal pathway, thus preventing repair of the lesions. 5 Thus, removal of myeloma cells decreased the inhibition of DKK1 on canonical Wnt signal pathway, resulting in osteoblast differentiation. 6 Activation of canonical Wnt pathway induces ALP activity. 7 Another mechanism is that bortezomib directly inhibited the secretion of DKK1 from osteoblasts, which results in the activation of Wnt signal pathway and osteoblast differentiation. Recently, Oyajobi et al demonstrated that bortezomib inhibited DKK1 expression in cell lines of mesenchymal origin, and stimulated the new bone formation in neonatal mouse calvariae. 8 This case suggests the presence of new action of bortezomib on bone formation, and this effect might benefit the bone disease in patients with MM. Further studies are required to clarify this hypothesis.

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“…1,2 The authors suggest the involvement of a new apoptotic pathway involving the caspase 3 activator, prostate apoptosis response gene 4 (Par-4). Moreover, Par-4 protein levels looks to correlate with the responsiveness to STI571 in a panel of six of CLL primary lymphocytes.…”

mentioning

confidence: 99%