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Dacarbazine and Temozolomide

These are structurally related cytotoxic agents. They have undergone trials in a range of solid tumours and sarcomas as well as in metastatic melanoma, Hodgkin's disease and brain tumours. Further trials are ongoing but some guidelines have emerged with, for example, the approval by the United States Food and Drug Administration (FDA) of temozolomide (TMZ) in March 2005 for newly diagnosed glioblastoma multiforme. NICE made similar recommendations in 2007.1

Mode of action

Dacarbazine

Dacarbazine (Dimethyl triazenoimidazole carboxamide or DTIC) was used intravenously in the early 1980s for sarcomas of the female pelvis and found, in combination, to be effective.2 It is thought to act as an alkylating agent. Alkylating agents cause cross linking of guanine bases in DNA, thus preventing cell division.

Temozolomide

TMZ undergoes hydrolysis in the body to produce monomethyl triazenoimidazole carboxamide (MTIC). It is thus structurally related to DTIC and is thought also to act as an alkylating agent. It is a newer agent than DTIC and is given orally. It is undergoing trials for conditions treated with DTIC.

Indications

Dacarbazine

  • Hodgkin's lymphoma. Dacarbazine is well established as a cytotoxic chemotherapeutic agent in Hodgkin's lymphoma. Although new combinations are being developed ABVD (Adriamycin-now doxorubicin, bleomycin, vinblastine and dacarbazine) offers a high cure rate and is still considered the best choice when combined with optimal limited irradiation.3,4,5 There are dangers with over treatment as well as under treatment in advanced Hodgkin's lymphoma and most patients can be cured with an extended course of ABVD.6
  • Metastatic melanoma. Chemotherapy with single agent dacarbazine is the only FDA approved chemotherapeutic agent for metastatic melanoma.7 Other novel agents are being developed. Stage IV melanoma has a very poor prognosis with a median survival of 6-9 months. Although a variety of agents have been tried there is as yet no known agent which can prolong this.
  • Solid tumours and sarcomas. In a study done between 1981 and 1984 dacarbazine was used for sarcomas of the female pelvis and found, in combination with other drugs to have some benefit.2 It has been tried in other sarcomas since then with varying success.

Temozolomide

  • Malignant gliomas (including glioblastoma multiforme or GBM):
    • GBM is a devastating tumour characterised by aggressive infiltration of the central nervous system and associated with marked disability. Radiotherapy with TMZ (chemo radiotherapy) followed by adjuvant systemic TMZ has shown modest improvements in survival.8,9
    • It is of note that:
      • The FDA approved TMZ for newly diagnosed adult GBM with radiotherapy and then maintenance TMZ in March 2005.10 NICE in 200111 reported on the use of TMZ for recurrent GBM and recommended its' use for recurrent glioma not responding to first line chemotherapy. More recently NICE has called for more trials to investigate use of TMZ in newly diagnosed GBM with radiotherapy as approved by the FDA.1 The latest NICE guidance is more in line with the FDA, recommending use in newly diagnosed glioblastoma multiforme in patients essentially able to carry out normal activities.1
      • The improvements in survival are modest. The mean overall survival with TMZ and radiotherapy is 14.6 months, compared with 12.1 months for radiotherapy alone.10
      • Good responses to treatment can be predicted with certain genetic lesions.12
      • Improved survival without any measured negative effect on quality of life has been reported.9
      • Some have questioned whether the modest benefits are worth the relatively high cost.13 It is certainly suggested that treatments should be given selectively, perhaps with the benefit of more research to identify subgroups of patients with more responsive tumours.14
      • NICE have called for more trials to identify the impact of treatment on quality of life, the effects in children and identification of helpful biological markers.1 Poor responses in paediatric brain tumours have been reported.15
  • Metastatic melanoma.
    • TMZ is not licensed for use in metastatic melanoma.
    • TMZ therapy has been tried16 and may have benefits over dacarbazine. It has been shown to be as effective as dacarbazine and has the advantage of being orally administered.17 It may offer better protection from the development of brain metastases.18,19 It has even been used in isolated limb infusions with hyperthermia.20
    • Low grade gliomas. Use in these rare unpredictable tumours is being investigated.21
    • Reports can be found on use in other tumours:
      • Neuroendocrine tumours22
      • Sarcomas23,24,25
      • Brain metastases26
Initiation of treatment
  • Treatment will usually be in specialist centres.
  • Patients should, when possible, be invited to enrol in clinical trials.
  • Patient selection for treatments and trials demands good information and communication with patient, carers and medical staff.
Side effects

These include fatigue, nausea and vomiting, rashes, infection and myelosuppression.1 See individual drugs.

Cautions, contraindications

See individual drugs.

Shared care

Good communication between specialist centre, patient, carers and the primary health care team is essential. Shared care protocols may be helpful to all concerned.

Document references
  1. Glioma (newly diagnosed and high grade) - carmustine implants and temozolomide, NICE Technology Appraisal Guidance (2007)
  2. Piver MS, Lele SB, Patsner B; cis-Diamminedichloroplatinum plus dimethyl-triazenoimidazole carboxamide as second- and third-line chemotherapy for sarcomas of the female pelvis.; Gynecol Oncol. 1986 Mar;23(3):371-5. [abstract]
  3. Gobbi PG, Levis A, Chisesi T, et al; ABVD versus modified stanford V versus MOPPEBVCAD with optional and limited radiotherapy in intermediate- and advanced-stage Hodgkin's lymphoma: final results of a multicenter randomized trial by the Intergruppo Italiano Linfomi.; J Clin Oncol. 2005 Dec 20;23(36):9198-207. Epub 2005 Sep 19. [abstract]
  4. Advani R, Ai WZ, Horning SJ; Management of advanced stage Hodgkin lymphoma.; J Natl Compr Canc Netw. 2006 Mar;4(3):241-7. [abstract]
  5. Johnson PW, Radford JA, Cullen MH, et al; Comparison of ABVD and alternating or hybrid multidrug regimens for the treatment of advanced Hodgkin's lymphoma: results of the United Kingdom Lymphoma Group LY09 Trial (ISRCTN97144519).; J Clin Oncol. 2005 Dec 20;23(36):9208-18. Epub 2005 Nov 28. [abstract]
  6. Connors JM; Evolving approaches to primary treatment of hodgkin lymphoma.; Hematology (Am Soc Hematol Educ Program). 2005;:239-44. [abstract]
  7. Tarhini AA, Agarwala SS; Cutaneous melanoma: available therapy for metastatic disease.; Dermatol Ther. 2006 Jan-Feb;19(1):19-25. [abstract]
  8. Reardon DA, Rich JN, Friedman HS, et al; Recent advances in the treatment of malignant astrocytoma.; J Clin Oncol. 2006 Mar 10;24(8):1253-65. [abstract]
  9. Taphoorn MJ, Stupp R, Coens C, et al; Health-related quality of life in patients with glioblastoma: a randomised controlled trial.; Lancet Oncol. 2005 Dec;6(12):937-44. [abstract]
  10. Cohen MH, Johnson JR, Pazdur R; Food and Drug Administration Drug approval summary: temozolomide plus radiation therapy for the treatment of newly diagnosed glioblastoma multiforme.; Clin Cancer Res. 2005 Oct 1;11(19 Pt 1):6767-71. [abstract]
  11. Brain cancer - temozolomide, NICE (2001); ref TA23
  12. Wemmert S, Ketter R, Rahnenfuhrer J, et al; Patients with high-grade gliomas harboring deletions of chromosomes 9p and 10q benefit from temozolomide treatment.; Neoplasia. 2005 Oct;7(10):883-93. [abstract]
  13. Hamilton D; Evidence, economics, and emotions: the case for temozolomide.; N Z Med J. 2005 Dec 16;118(1227):U1774. [abstract]
  14. Nieder C, Grosu AL, Astner S, et al; Treatment of unresectable glioblastoma multiforme.; Anticancer Res. 2005 Nov-Dec;25(6C):4605-10. [abstract]
  15. Barone G, Maurizi P, Tamburrini G, et al; Role of temozolomide in pediatric brain tumors.; Childs Nerv Syst. 2006 Mar 25;. [abstract]
  16. Gonzalez Cao M, Malvehy J, Marti R, et al; Biochemotherapy with temozolomide, cisplatin, vinblastine, subcutaneous interleukin-2 and interferon-alpha in patients with metastatic melanoma.; Melanoma Res. 2006 Feb;16(1):59-64. [abstract]
  17. Kaufmann R, Spieth K, Leiter U, et al; Temozolomide in combination with interferon-alfa versus temozolomide alone in patients with advanced metastatic melanoma: a randomized, phase III, multicenter study from the Dermatologic Cooperative Oncology Group.; J Clin Oncol. 2005 Dec 10;23(35):9001-7. Epub 2005 Oct 31. [abstract]
  18. Weber RW, O'Day S, Rose M, et al; Low-dose outpatient chemobiotherapy with temozolomide, granulocyte-macrophage colony stimulating factor, interferon-alpha2b, and recombinant interleukin-2 for the treatment of metastatic melanoma.; J Clin Oncol. 2005 Dec 10;23(35):8992-9000. Epub 2005 Oct 31. [abstract]
  19. Ron IG, Sarid D, Ryvo L, et al; A biochemotherapy regimen with concurrent administration of cisplatin, vinblastine, temozolomide (Temodal), interferon-alfa and interleukin-2 for metastatic melanoma: a phase II study.; Melanoma Res. 2006 Feb;16(1):65-9. [abstract]
  20. Ko SH, Ueno T, Yoshimoto Y, et al; Optimizing a novel regional chemotherapeutic agent against melanoma: hyperthermia-induced enhancement of temozolomide cytotoxicity.; Clin Cancer Res. 2006 Jan 1;12(1):289-97. [abstract]
  21. Neyns B, Sadones J, Chaskis C, et al; The role of chemotherapy in the treatment of low-grade glioma. A review of the literature.; Acta Neurol Belg. 2005 Sep;105(3):137-43. [abstract]
  22. Kulke MH, Stuart K, Enzinger PC, et al; Phase II study of temozolomide and thalidomide in patients with metastatic neuroendocrine tumors.; J Clin Oncol. 2006 Jan 20;24(3):401-6. [abstract]
  23. Geoerger B, Vassal G, Doz F, et al; Dose finding and O6-alkylguanine-DNA alkyltransferase study of cisplatin combined with temozolomide in paediatric solid malignancies.; Br J Cancer. 2005 Sep 5;93(5):529-37. [abstract]
  24. Garcia del Muro X, Lopez-Pousa A, Martin J, et al; A phase II trial of temozolomide as a 6-week, continuous, oral schedule in patients with advanced soft tissue sarcoma: a study by the Spanish Group for Research on Sarcomas.; Cancer. 2005 Oct 15;104(8):1706-12. [abstract]
  25. Warren KE, Aikin AA, Libucha M, et al; Phase I study of O6-benzylguanine and temozolomide administered daily for 5 days to pediatric patients with solid tumors.; J Clin Oncol. 2005 Oct 20;23(30):7646-53. [abstract]
  26. Abrey LE, Mehta MP; Treatment of brain metastases: a short review of current therapies and the emerging role of temozolomide.; Clin Adv Hematol Oncol. 2003 Apr;1(4):231-6. [abstract]
AcknowledgementsEMIS is grateful to Dr Richard Draper for writing this article. The final copy has passed scrutiny by the independent Mentor GP reviewing team. ©EMIS 2007.
DocID: 311
Document Version: 2
DocRef: bgp25242
Last Updated: 24 Aug 2007
Review Date: 23 Aug 2008








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