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Leading Substances for
Brain Tumour
By: SHIVANI CHAUHAN
• Introduction
• Definition
• Causes of Brain tumor
• Types of Brain tumor
• Chemotherapy in brain tumor
• Leading Substances for Brain tumor
Outlines
Brain tumor
Definition of Brain tumor
A brain tumor is a localized intracranial lesion which
occupies space with the skull and tends to cause a rise
in intracranial pressure.
Causes of Brain Cancer
 DNA Damage
 Radiation
 Genetics
 NF-1 (acoustic neuromas)
 Li Fraumeni syndrome
 Tuberous sclerosis (astrocytomas)
 Multiple endocrine neoplasia type-1(Pituitary
macroadenoma)
 Infection
 HIV
Distribution of Primary CNS
Tumors By Histology
I Primary Brain Tumors:
Benign
• Pituitary – adenoma,
Cranic-pharyngioma
• Meningioma
• Acoustic neuroma
• Dermoid tumor
Malignant:
• Glioma
• Primary cerebral Lymphoma
• Germinoma
• Pineoblastoma
• Medullablastoma
II Secondary Brain Tumors
• Lung
• Breast
• GI
• Any primary potentially
Chemotherapy
in
Brain Tumors
Timing of Chemotherapy
 Adjuvant
 After surgery or radiation
 Defined number of cycles
 Aim
Prolong time of recurrence
 Recurrence
 Number of cycles limited by side effects
 Aim
Improve symptoms, quality of life and slow progression
A BIT of HISTORY….
• Surgery & radiation mainstays of treatment (and still are)
• Chemotherapy options
• PCV standard of care for many years
• Procarbazine
• Carmustine
• Vincristine
• Single agent nitrosurea (Lomustine/carmustine) are equivalent
Rationale For The Use Of
Chemotherapy in Neuro-Oncology
 1 gram of tumor = one billion cells
 GTR = removal of 99% (990,000,000 cells)
 Still have 10,000,000 tumor cells
 Radiation may remove 99% (9,900,000 cells),
leaving 100,000 cells
Barriers to Use of Chemotherapy
 Uncommon (2% of all malignancies)
 Blood-brain barrier
 Interaction of chemotherapeutic agents with EIAC
Solutions to Barriers to Use of
Chemotherapy
 Lipophilic molecules (Nitrosureas)
 Small molecules (Gefitinib)
 Osmotic Blood Brain Barrier Disruption
 Design drugs that do not interfere with EIAC
medications
 Make chemotherapy drugs very expensive
How to overcome BBB ??
Newer delivery method includes:
 Interstitial chemotherapy uses disc-shaped polymer wafers (known as Gliadel
wafers) soaked with carmustine, the standard chemotherapeutic drug for brain
cancer.
 Intrathecal chemotherapy delivers chemotherapeutic drugs directly into the
spinal fluid
 Intra-arterial chemotherapy delivers high-dose chemotherapy into arteries in
the brain using tiny catheters.
 Convection-enhanced delivery (CED) involves placing catheters into the brain
tumor or nearby brain tissue to deliver slowly and continuously a cancer drug
over several days.
Chemotherapeutic Agents
 Carmustine (BCNU)
 Lomustine (CCNU)
 Procarbazine
 Temozolomide
 Vincristine
 Camptothecans (Irinotecan, Edotecarin)
 Gefitinib
Carmustine and Lomustine
 Highly lipophilic nitrosureas
 Hydrolysis in vivo to form reactive metabolites
 Metabolites cause alkylation and cross-linking of DNA
 CSF equilibrates within one hour to > 50% of plasma levels
 Metabolism = hepatic microsomal enzyme
 Excretion = predominantly renal
Nitrosurea Toxicities
 Dose limiting toxicity is myelosuppression
 Nadir 25-60 days, recovery 35-85 days
 Nausea and vomiting
 Dizziness, ataxia, lethargy, disorientation
 Pulmonary fibrosis (dose dependent)
 Infertility and mutagenesis
 Carmustine is a vesicant
Procarbazine
 Multiple sites of action (inhibits DNA, RNA and
protein synthesis)
 Rapid equilibration with CSF
 Metabolism = microsomal enzymes
 Excretion = predominately renal
Procarbazine Toxicities
 DLT = myelosuppression, nadir 14-21 days, recovery 28 days
 Nausea and vomiting
 CNS depression, lethargy, peripheral neuropathy
 Hypersensitivity pneumonitis
 Infertility, mutagenesis
 Radiation enhancer
Standard ones include:
Temozolomide
 Taken oral
 First approved in 1999 for adult patients with anaplastic astrocytoma that did
not respond to other treatments.
 In 2005, it was approved for use during and after radiation therapy for
patients newly diagnosed with glioblastoma multiforme.
 Adverse effects: Relatively minor, but may include constipation, nausea and
vomiting, fatigue, and headache..
Temozolomide
 Classification = alkylating agent
 Rapid conversion at physiologic pH to MTIC, CSF concentration is
30% of serum
 MTIC cytotoxicity due to methylation of DNA at the O6 position of
guanine
 Antitumor activity is schedule dependent
 Cytotoxicity influenced by levels of MGMT
 Levels not infuenced by cytochrome p450
 Renal and hepatic clearance minor
Treatment Schedule
*PCP prophylaxis was required for patients receiving TMZ during the concomitant phase
Significant Improvement in Survival
Gefitinib
 Potent and selective inhibitor of EGFR tyrosine kinase
 EGFR expression and over-expression in GBM other brain
cancers
 Over-expression correlated with poor prognosis in many
cancers
 Once-daily, oral dosing
 Lipophilic compound but CNS levels are low
THANK YOU
For any queries, please contact me at: shivanichauhan232@gmail.com

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Leading substances for brain cancer

  • 1. Leading Substances for Brain Tumour By: SHIVANI CHAUHAN
  • 2. • Introduction • Definition • Causes of Brain tumor • Types of Brain tumor • Chemotherapy in brain tumor • Leading Substances for Brain tumor Outlines
  • 4. Definition of Brain tumor A brain tumor is a localized intracranial lesion which occupies space with the skull and tends to cause a rise in intracranial pressure.
  • 5. Causes of Brain Cancer  DNA Damage  Radiation  Genetics  NF-1 (acoustic neuromas)  Li Fraumeni syndrome  Tuberous sclerosis (astrocytomas)  Multiple endocrine neoplasia type-1(Pituitary macroadenoma)  Infection  HIV
  • 6. Distribution of Primary CNS Tumors By Histology
  • 7. I Primary Brain Tumors: Benign • Pituitary – adenoma, Cranic-pharyngioma • Meningioma • Acoustic neuroma • Dermoid tumor Malignant: • Glioma • Primary cerebral Lymphoma • Germinoma • Pineoblastoma • Medullablastoma
  • 8. II Secondary Brain Tumors • Lung • Breast • GI • Any primary potentially
  • 10.
  • 11. Timing of Chemotherapy  Adjuvant  After surgery or radiation  Defined number of cycles  Aim Prolong time of recurrence  Recurrence  Number of cycles limited by side effects  Aim Improve symptoms, quality of life and slow progression
  • 12. A BIT of HISTORY…. • Surgery & radiation mainstays of treatment (and still are) • Chemotherapy options • PCV standard of care for many years • Procarbazine • Carmustine • Vincristine • Single agent nitrosurea (Lomustine/carmustine) are equivalent
  • 13. Rationale For The Use Of Chemotherapy in Neuro-Oncology  1 gram of tumor = one billion cells  GTR = removal of 99% (990,000,000 cells)  Still have 10,000,000 tumor cells  Radiation may remove 99% (9,900,000 cells), leaving 100,000 cells
  • 14. Barriers to Use of Chemotherapy  Uncommon (2% of all malignancies)  Blood-brain barrier  Interaction of chemotherapeutic agents with EIAC
  • 15. Solutions to Barriers to Use of Chemotherapy  Lipophilic molecules (Nitrosureas)  Small molecules (Gefitinib)  Osmotic Blood Brain Barrier Disruption  Design drugs that do not interfere with EIAC medications  Make chemotherapy drugs very expensive
  • 16. How to overcome BBB ?? Newer delivery method includes:  Interstitial chemotherapy uses disc-shaped polymer wafers (known as Gliadel wafers) soaked with carmustine, the standard chemotherapeutic drug for brain cancer.  Intrathecal chemotherapy delivers chemotherapeutic drugs directly into the spinal fluid  Intra-arterial chemotherapy delivers high-dose chemotherapy into arteries in the brain using tiny catheters.  Convection-enhanced delivery (CED) involves placing catheters into the brain tumor or nearby brain tissue to deliver slowly and continuously a cancer drug over several days.
  • 17. Chemotherapeutic Agents  Carmustine (BCNU)  Lomustine (CCNU)  Procarbazine  Temozolomide  Vincristine  Camptothecans (Irinotecan, Edotecarin)  Gefitinib
  • 18. Carmustine and Lomustine  Highly lipophilic nitrosureas  Hydrolysis in vivo to form reactive metabolites  Metabolites cause alkylation and cross-linking of DNA  CSF equilibrates within one hour to > 50% of plasma levels  Metabolism = hepatic microsomal enzyme  Excretion = predominantly renal
  • 19. Nitrosurea Toxicities  Dose limiting toxicity is myelosuppression  Nadir 25-60 days, recovery 35-85 days  Nausea and vomiting  Dizziness, ataxia, lethargy, disorientation  Pulmonary fibrosis (dose dependent)  Infertility and mutagenesis  Carmustine is a vesicant
  • 20. Procarbazine  Multiple sites of action (inhibits DNA, RNA and protein synthesis)  Rapid equilibration with CSF  Metabolism = microsomal enzymes  Excretion = predominately renal
  • 21. Procarbazine Toxicities  DLT = myelosuppression, nadir 14-21 days, recovery 28 days  Nausea and vomiting  CNS depression, lethargy, peripheral neuropathy  Hypersensitivity pneumonitis  Infertility, mutagenesis  Radiation enhancer
  • 22. Standard ones include: Temozolomide  Taken oral  First approved in 1999 for adult patients with anaplastic astrocytoma that did not respond to other treatments.  In 2005, it was approved for use during and after radiation therapy for patients newly diagnosed with glioblastoma multiforme.  Adverse effects: Relatively minor, but may include constipation, nausea and vomiting, fatigue, and headache..
  • 23. Temozolomide  Classification = alkylating agent  Rapid conversion at physiologic pH to MTIC, CSF concentration is 30% of serum  MTIC cytotoxicity due to methylation of DNA at the O6 position of guanine  Antitumor activity is schedule dependent  Cytotoxicity influenced by levels of MGMT  Levels not infuenced by cytochrome p450  Renal and hepatic clearance minor
  • 24. Treatment Schedule *PCP prophylaxis was required for patients receiving TMZ during the concomitant phase
  • 26. Gefitinib  Potent and selective inhibitor of EGFR tyrosine kinase  EGFR expression and over-expression in GBM other brain cancers  Over-expression correlated with poor prognosis in many cancers  Once-daily, oral dosing  Lipophilic compound but CNS levels are low
  • 27. THANK YOU For any queries, please contact me at: shivanichauhan232@gmail.com