Marked inactivation of O6-alkylguanine-DNA alkyltransferase activity with protracted temozolomide schedules

Tolcher, Anthony W.; Gerson, Stanton L.; Lairon, Denis; Geyer, Christiane; Hammond, Lisa A.; Patnaik, Amita; Goetz, Andrew; Schwartz, Garry; Edwards, Tammy L.; Reyderman, Larisa; Statkevich, Paul; Cutler, David L.; Rowinsky, Eric K.

doi:10.1038/sj.bjc.6600827

Cited by 342 publications

(223 citation statements)

References 22 publications

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“…This regimen may yield similar results with respect to efficacy, but a higher rate of toxicity, specifically lymphopenia and infection, have been reported [8,9]. The latter two regimens aim at a dose intensification, which could enhance the direct cytotoxic effect of TMZ and which might deplete the DNA repair enzyme O 6 -methylguanine DNA Hau, 5 methyltransferase (MGMT) [10]. This enzyme modulates resistance to alkylating chemotherapeutic agents [11].…”

Section: Introductionmentioning

confidence: 95%

Rechallenge with temozolomide in patients with recurrent gliomas

et al. 2009

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Temozolomide (TMZ) is the standard of care for patients with newly diagnosed glioblastoma (GBM) as well as those with recurrent anaplastic glioma (AG) and GBM. It has become common practice to re-expose patients to TMZ who had been previously treated with TMZ, or to switch patients to alternative dosing regimens of TMZ when there are signs of relapse or progress on standard TMZ therapeutic regimens. To date, however, there is a scarcity of data on the efficacy of this therapeutic strategy, currently referred to as TMZ rechallenge. We have conducted a retrospective review of patients with recurrent glioma rechallenged with TMZ. Patients experiencing progressive disease (PD) during TMZ therapy who were rechallenged with alternative TMZ regimens and patients rechallenged after stable disease in a TMZ-free interval were evaluated separately. A total of 90 rechallenges were identified in 80 patients. The progression-free survival at 6 months (PFS-6) was 48% in patients with AG (12/25) and 27.7% in those with GBM (14/47). The PFS-6 was 16.7% in AG and 26.3% in GBM for patients switched during TMZ and 57.9 and 28.6% in patients rechallenged after a TMZ-free interval of at least 8 weeks. Relevant hematological toxicity (NCI-CTC grade 3-5) was observed in 22 of 90 rechallenges, and relevant non-hematological in ten of 90 rechallenges. Temozolomide was well tolerated and generated promising PFS-6 in patients who had previously failed TMZ, regardless if they progressed during TMZ treatment, or if they were rechallenged after a TMZ-free interval. These results suggest that the TMZ rechallenge strategy warrants further investigation in a prospective randomized trial.

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Section: Introductionmentioning

confidence: 95%

Rechallenge with temozolomide in patients with recurrent gliomas

et al. 2009

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“…This was somewhat higher than previous values (Middleton et al, 2000b: range 2.2 -25.6, mean 12.6) but similar to other ongoing studies (range 2.3 -51.6, mean 15.5: GPM unpublished results). Another study of adult patients has reported a range of B0.6 to B19 Fm mg À1 DNA and a much lower mean of 6.974.7 Fm mg À1 DNA (Tolcher et al, 2003). Some of these differences may be a consequence of the age or disease status of the study groups.…”

Section: Discussionmentioning

confidence: 95%

“…Previous studies reporting MGMT in adult PBMCs have also shown a range of extents of depletion by temozolomide. A variety of dose regimen and schedules have been examined but complete depletion of MGMT has been observed in very few patients and very wide variations in depletion are always observed (Lee et al, 1994;Gander et al, 1999;Middleton et al, 2000b;Tolcher et al, 2003). The reasons for this have yet to be established.…”

Section: Discussionmentioning

confidence: 99%

“…Although our evaluations are in a limited number of samples and need to be confirmed and extended by further studies, they are supported by previous studies. Thus, lower MGMT activities in PBMCs have been associated with increased haematological toxicity in a phase II study of temozolomide in adult melanoma patients (Middleton et al, 2000b) and inactivation of MGMT was correlated with haematological toxicity in a phase I study of temozolomide (Tolcher et al, 2003). Nevertheless, to address the questions of MGMT inactivation by cisplatin in relation to tumour responses and toxicities, it would be necessary to undertake larger studies, ideally in direct comparison with equivalent numbers of patients receiving temozolomide alone.…”

Section: Discussionmentioning

confidence: 99%

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Dose finding and O6-alkylguanine-DNA alkyltransferase study of cisplatin combined with temozolomide in paediatric solid malignancies

et al. 2005

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Cisplatin may have additive activity with temozolomide due to ablation of the DNA repair protein O 6 -alkylguanine-DNA alkyltransferase (MGMT). This phase I/II study determined recommended combination doses using the Continual Reassessment Method, toxicities and antitumour activity in paediatric patients, and evaluated MGMT in peripheral blood mononuclear cells (PBMCs) in order to correlate with haematological toxicity. In total, 39 patients with refractory or recurrent solid tumours (median age B13 years; 14 pretreated with high-dose chemotherapy, craniospinal irradiation, or having bone marrow involvement) were treated with cisplatin, followed the next day by oral temozolomide for 5 days every 4 weeks at dose levels 80 mg m À2 / 150 mg m À2 day À1 , 80/200, and 100/200, respectively. A total of 38 patients receiving 113 cycles (median 2, range 1 -7) were evaluable for toxicity. Dose-limiting toxicity was haematological in all but one case. Treatment-related toxicities were thrombocytopenia, neutropenia, nausea-vomiting, asthenia. Hearing loss was experienced in five patients with prior irradiation to the brain stem or posterior fossa. Partial responses were observed in two malignant glioma, one brain stem glioma, and two neuroblastoma. Median MGMT activity in PBMCs decreased after 5 days of temozolomide treatment: low MGMT activity correlated with increased severity of thrombocytopenia. Cisplatin -temozolomide combinations are well tolerated without additional toxicity to single-agent treatments; the recommended phase II dosage is 80 mg m À2 cisplatin and 150 mg m À2 Â 5 temozolomide in heavily treated, and 200 mg m À2 Â 5 temozolomide in less-heavily pretreated children.

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“…Protracted administration of temozolomide may lead to a marked and sustained inactivation of MGMT leading to an ''autoenhancement" of temozolomide's inherent cytotoxic potential by cumulative reduction of the leukemic blasts' capacity for MGMT-mediated DNA repair and resistance [20]. MGMT activity can be reduced by approximately 80% in patients treated with this dosing schedule [20]. Thus, we designed an exploratory clinical study to test two hypotheses: (1) Can temozolomide therapy be tailored according the MGMT methylation status in patients with AML?…”

Section: Introductionmentioning

confidence: 99%

Tailored temozolomide therapy according to MGMT methylation status for elderly patients with acute myeloid leukemia

et al. 2011

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Temozolomide sensitivity is determined by methylation of the O 6 -methylguanine-DNA methyltransferase (MGMT) promoter. This study assessed whether the temozolomide dose can be tailored by MGMT promoter status and whether protracted, low-dose temozolomide can ''prime'' blasts in patients with unmethylated MGMT (unMGMT). Elderly patients with high-risk AML were stratified by MGMT methylation. Patients with methylated MGMT (mMGMT) received temozolomide 200 mg/m 2 orally for 7 days every 4 weeks, while patients with unMGMT received temozolomide 100 mg/m 2 orally for 14 days followed by 200 mg/m 2 orally for 7 days every 6 weeks. Of 36 patients (median age, 75 years), 31 (86%) had an unMGMT promoter. Overall response rate for the entire cohort was 36%. Patients with mMGMT and unMGMT had similar response rates (40% vs. 29%). Median duration of response and overall survival (OS) among responders were 29 and 35 weeks, respectively. Induction deaths (ID) occurred in 25% of patients, mostly caused by disease progression. Hematological toxicities were the most common adverse event. Toxicities were similar between patients on conventional versus protracted schedules. High HCT-CI scores were predictive of lower CR rate, higher ID, and shorter OS, while bone marrow blast count <50% at screening predicted for improved responses. Temozolomide, dosed according to MGMT methylation status, demonstrated modest clinical activity in elderly patients with AML, especially in those presenting with fewer comorbidities and low disease burden. The trial was registered on www.ClinicalTrials.gov as #NCT00611247. Am. J. Hematol. 87:45-50, 2012. V

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Marked inactivation of O6-alkylguanine-DNA alkyltransferase activity with protracted temozolomide schedules

Cited by 342 publications

References 22 publications

Rechallenge with temozolomide in patients with recurrent gliomas

Rechallenge with temozolomide in patients with recurrent gliomas

Dose finding and O6-alkylguanine-DNA alkyltransferase study of cisplatin combined with temozolomide in paediatric solid malignancies

Tailored temozolomide therapy according to MGMT methylation status for elderly patients with acute myeloid leukemia

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