The search for a melanoma-tailored chemotherapy in the new era of personalized therapy: a phase II study of chemo-modulating temozolomide followed by fotemustine and a cooperative study of GOIM (Gruppo Oncologico Italia Meridionale)

被引:12
|
作者
Guida, Michele [1 ]
Tommasi, Stefania [2 ]
Strippoli, Sabino [1 ]
Natalicchio, Maria Iole [3 ]
De Summa, Simona [2 ]
Pinto, Rosamaria [2 ]
Cramarossa, Antonio [4 ]
Albano, Anna [1 ]
Pisconti, Salvatore [5 ]
Aieta, Michele [6 ]
Ridolfi, Ruggiero [7 ]
Azzariti, Amalia [8 ]
Guida, Gabriella [9 ]
Lorusso, Vito [1 ]
Colucci, Giusepe [1 ]
机构
[1] Natl Canc Res Ctr Giovanni Paolo II, Med Oncol Dept, Via O Flacco 65, I-70124 Bari, Italy
[2] Natl Canc Res Ctr Giovanni Paolo II, Mol Genet Lab & Radiol, Via O Flacco 65, I-70124 Bari, Italy
[3] Osped Riuniti Foggia, Lab Mol Oncol Solid Tumors & Pharmacogen, Viale Pinto 1, I-71122 Foggia, Italy
[4] Natl Canc Res Ctr Giovanni Paolo II, Radiol Dept, Bari, Italy
[5] San Giuseppe Moscati Hosp, Med Oncol Dept, Via Martina Franca, I-74010 Statte, Taranto, Italy
[6] Natl Inst Canc, Med Oncol Dept, Via Padre Pio 1, I-85028 Potenza, Italy
[7] Natl Canc Inst Romagna IRST, Med Oncol Dept, Via Piero Maroncelli 40, I-47014 Meldola, Forli, Italy
[8] Natl Canc Res Ctr Giovanni Paolo II, Clin & Preclin Pharmacol Lab, Via O Flacco 65, I-70124 Bari, Italy
[9] Univ Bari, Dept Basic Med Sci Neurosci & Sense Organs, Piazza Giulio Cesare 1, I-70124 Bari, Italy
来源
BMC CANCER | 2018年 / 18卷
关键词
Melanoma; Chemotherapy; Base excision repair; MGMT; Fotemustine; Temozolomide; Biomarkers; MGMT PROMOTER METHYLATION; METASTATIC MELANOMA; MALIGNANT-MELANOMA; IPILIMUMAB; CHEMORESISTANCE; COMBINATION; DACARBAZINE; RESISTANCE; EXPRESSION; SURVIVAL;
D O I
10.1186/s12885-018-4479-2
中图分类号
R73 [肿瘤学];
学科分类号
100214 ;
摘要
Background: It is frequently asked whether chemotherapy can still play a role in metastatic melanoma considering the effectiveness of the available drugs today, including antiCTLA4/antiPD1 immunotherapy and antiBRAF/antiMEK inhibitors. However, only approximately half of patients respond to these drugs, and the majority progress after 6-11 months. Therefore, a need for other therapeutic options is still very much apparent. We report the first large trial of a sequential full dose of fotemustine (FM) preceded by a low dose of temozolomide (TMZ) as a chemo-modulator in order to inactivate the DNA repair action of O(6)-methylguanine DNA-methyltransferase (MGMT). Primary endpoints were overall response and safety. We also evaluated specific biological parameters aiming to tailor these chemotherapies to selected patients. Methods: A total of 69 consecutive patients were enrolled. The main features included a median age of 60 years (21-81) and M1c stage, observed in 74% of the patients, with brain metastases in 15% and high LDH levels in 42% of the patients. The following schedule was used: oral TMZ 100 mg/m(2) on days 1 and 2 and FMiv 100 mg/m(2) on day 2, 4 h after TMZ; A translational study aiming to analyse MGMT methylation status and base-excision repair (BER) gene expression was performed in a subset of 14 patients. Results: We reported an overall response rate of 30.3% with 3 complete responses and a disease control rate of 50.5%. The related toxicity rate was low and mainly of haematological types. Although our population had a very poor prognosis, we observed a PFS of 6 months and an OS of 10 months. A non-significant correlation with response was found with the mean expression level of the three genes involved in the BER pathway (APE1, XRCC1 and PARP1), whereas no association was found with MGMT methylation status. Conclusion: This schedule could represent a good alternative for patients who are not eligible for immune or targeted therapy or whose previous therapies have failed.
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