1 / 33

Medical Treatment for High Grade Gliomas – An Overview

Medical Treatment for High Grade Gliomas – An Overview. Dr Daphne Tsoi MBBS MSc FRACP Medical Oncologist Royal Perth Hospital SJOG Hospitals Subiaco, Murdoch. Incidence. ~ 1400 cases of primary brain tumour diagnosed in Australia each year Primary CNS cancers – 7/100,000/year

uzuri
Download Presentation

Medical Treatment for High Grade Gliomas – An Overview

An Image/Link below is provided (as is) to download presentation Download Policy: Content on the Website is provided to you AS IS for your information and personal use and may not be sold / licensed / shared on other websites without getting consent from its author. Content is provided to you AS IS for your information and personal use only. Download presentation by click this link. While downloading, if for some reason you are not able to download a presentation, the publisher may have deleted the file from their server. During download, if you can't get a presentation, the file might be deleted by the publisher.

E N D

Presentation Transcript


  1. Medical Treatment for High Grade Gliomas – An Overview Dr Daphne Tsoi MBBS MSc FRACP Medical Oncologist Royal Perth Hospital SJOG Hospitals Subiaco, Murdoch

  2. Incidence • ~ 1400 cases of primary brain tumour diagnosed in Australia each year • Primary CNS cancers – 7/100,000/year • (Colon cancer – 60/100,000/year) • 14th most common cancer in Australia • Highest in terms of average year lost (12 years per patient)

  3. Average years of life lost for patients in Australia and the UK, 2001, by cancer type Sources: Burnet et al , Australian Institute of Health and Welfare (AIHW)

  4. Glial cells http://ovidsp.com/spb/ovidweb.cgi Chamberlain MC et al. West J Med. 1998;168:114-120.

  5. Glioma: Grading Chamberlain MC, et al. West J Med. 1998;168:114-120.

  6. Median Survival: Importance of Histologic Grading • Pathologic diagnosis is crucial in determining treatment and prognosis 1Bruce J. Available at: http://www.emedicine.com. 2Hariharan S. Available at: http://www.emedicine.com. 3DeAngelis LM. N Engl J Med. 2001;344:114-123.

  7. Primary vs Secondary GBM • Primary GBM • Develops de novo from glial cells • Accounts for > 90% of biopsied or resected cases • Clinical history of 6 months • Occurs in older patients (median age: 60 years) • Secondary GBM • Develops from low-grade or anaplastic astrocytoma • ~ 70% of lower grade gliomas develop into advanced disease within 5-10 years of diagnosis • Comprises < 5% of GBM cases • Occurs in younger patients (median age: 45 years)

  8. Presentation • Headache • Seizure • Motor weakness/speech deficit • Altered personality • Loss of memory/cognition • Dizziness

  9. MRI Biopsy Investigations

  10. Features of Glioblastoma Multiforme • Rapid progression • Enhancing tumor • Surrounding edema • Contains tumour • ~ 5% multifocal

  11. Treatment • Surgery • Radiotherapy • Chemotherapy

  12. Temozolomide(Temodal) Methylating agent Principal mechanism is causing damage to DNA of tumour cell, leading to cell death Taken orally, rapidly absorbed Penetrates the blood-brain barrier Dose according to ‘body surface area’ (height/weight)

  13. Temozolomide – Side Effects • Tiredness / fatigue • Nausea • Constipation (from anti-emetics) • Low blood counts – red/white/platelets • Particularly lymphocytes (risk of Pneumocystis carinii pneumonia) • Rash

  14. Standard Treatment for GBM • Radiotherapy concurrently with Temozolomide followed by 6 months of Temozolomide

  15. Phase III Study: New GBM Radiation ± Temozolomide Concomitant TMZ + RT* Adjuvant TMZ R 0 6 10 14 18 22 26 30 Wks RT Alone TMZ 75 mg/m2 PO QD for 6 weeks, then 150-200 mg/m2 PO QD on Days 1-5 every 28 days for 6 cycles Focal RT daily—30 x 200 cGy;total dose: 60 Gy *PCP prophylaxis was required for patients receiving TMZ during the concomitant phase. Stupp R, et al. N Engl J Med. 2005;352:987-996.

  16. Phase III Study: New GBM Radiation ± Temozolomide 100 Median Survival 90 RT + temozolomide: 14.6 months 80 RT alone: 12.1 months 70 60 50 Probability of OS (%) 40 30 20 10 0 0 6 12 18 24 30 36 42 Months • Phase III study (N = 573): 2-year OS rate improved from 10.4% with RT alone to 26.5% with temozolomide Stupp R, et al. N Engl J Med. 2005;352:987-996.

  17. Temozolomide - indications • Recurrence of anaplastic astrocytoma and glioblastoma multiforme

  18. Surgical Implantation of Chemotherapy Wafers: Gliadel® • BCNU-infused wafers • implanted to tumour bed at time of surgery • chemotherapy released to surrounding brain tissue over a period of 2 to 3 weeks • Clinical trials showed survival benefit • PBS difficulties Gliadelis a trademark of Guilford Pharmaceuticals.

  19. Progressive Disease • Challenges of diagnosing progressive disease • Pseudo-progression • increase in enhancement without tumor progression • Especially after chemo-radiation • First post-RT MR scan should not be used for treatment decisions • ‘Treat the patient not the scan’ • Techniques to help distinguish - MRS (spectroscopy), PET scans, SPECT scans

  20. Pseudoprogression: The Index Case Male, gross total resection for anaplastic ependymoma in August ’97, no neurological deficits, pre-RT MRI: Deterioration during/after radiation therapy (10/97-12/97, 65 Gy) Thereafter slight clinical improvement for more than 1 year

  21. Further Treatment for Progression • Surgery • Radiation (stereotactic radio-surgery) • 2nd line chemotherapy

  22. 2nd line Chemotherapy • No consensus • Low dose temozolomide (+/- procarbazine) • Carboplatin • BCNU/CCNU • Bevacizumab (+/- Irinotecan) • Clinical trials if possible

  23. Glioblastoma: A Highly Vascular Tumour • The vascular network formed in GBM is abnormal • vessels are dilated, tortuous, disorganised, highly leaky

  24. Angiogenesis

  25. Avastin (Bevacizumab) – mechanism of action

  26. Bevacizumab: Anti-VEGF Antibody • After 4 cycles bev/irinotecan • Recurrent GBM at baseline • Vredenburgh JJ, et al. J Clin Oncol. 2007;25:4722-4729. • National Comprehensive Cancer Network guideline: CNS cancers (V.1.2008)

  27. Bevacizumab for recurrent glioblastoma • Unanswered questions • Phase II results only • ?changes on MRI reflect tumour shrinkage, or reduced swelling from stopping leaking blood vessels • Concerns about rapid progression upon stopping treatment • Phase III trials underway

  28. New drugs that failed to impress • Erlotinib • Enzastaurin • Edotecarin • Cediranib

  29. Approach to Patients • Complex challenges specific to brain tumour patients • Disease • Physical impairment – weakness, poor mobility, speech, vision • Cognitive impairment – memory, insight, judgment, personality, disinhibition • Depression • Seizures

  30. Approach to Patients • Polypharmacy • Steroids • weight gain, elevated BSL, proximal myopathy, emotional lability, reversal of sleep/wake cycle • Anticonvulsants • Antiemetics / aperients / antibiotics • Anticoagulants • Medications for other medical conditions • ?compliance

  31. Approach to Patients • Financial / income source • Family / dependents • Transfers to frequent clinic visits • Home modifications / hire equipments • Carers • burn-out, financial source

  32. Approach to Patients • Multidisciplinary approach • Neurosurgeon • Radiation Oncologist • Medical Oncologist • Rehabilitation team • Clinical specialist nurse • Neurologist • Endocrinologist • OT/physio/dietitian/speech pathologist • Community/palliative care/hospice • Social worker • Inpatient team • GP

  33. Conclusions • Management of GBM remains challenging with median survival at 9-15 months • Survival improved by • Resection • Adjuvant radiotherapy plus concurrent chemotherapy • Temozolomide is component of standard of care • Promising investigational directions – the use of targeted therapy • Individually tailored therapy based on genetic profile • Clinical trials participation should be considered • Multidisciplinary team approach is paramount

More Related