tumor treatment

Question 1

What is bevacizumab?

Answer 1

An angiogenes inhibiting agent.

Question 2

What finding might be seen on MRI after use of Bevacizumab and other angiogenes inhibitors?

Answer 2

Psudoregression of the tumor. - but its the effect of a BBB stabilisation that is seen, not tumor regression.

Question 3

What is “RANO”?

Answer 3

Response Assessment in Neuro-Oncology. the size of the contrast enhancing tumorcomponent is measured in a special way. That is combined w info of cortison treatment and clinical status.
Non-contrast enhancing tumors with high T2 or T2 FLAIR intensity are also measured.
Smallest “countable” lesion acording to RANO is 1 cm2.

Question 4

What are the outcomes in RANO?

Answer 4

• response
• partiell response
• stable disease
• progression

Question 5

What is the difference in diagnostication of glioma between WHO CNS 2016 and 2021?

Answer 5

In 2016, molecular alterations together with histopathology were defining diagnosis.

In 2021 molecular data are implemented to a large extent and will form the basis for a continous revision of CNS tumor classification.

Question 6

What is the drug used for flourescence based visualization of tumor tissue called?

Answer 6

5-aminolevulinic acid.

Question 7

What is the goal of radiotherapy for glioma?

Answer 7

To improve local control without inducing neurotoxicity

Question 8

What determibes the timing, dosing and scheduling of radiotherapy?

Answer 8

• disease subtype
• age
• KPS
• recidual tumor volume.

Question 9

When should radiotherapy start after surgery?

Answer 9

3-5 weeks

Question 10

What is the most common dose of radiotherapy for grade 2-3 gliomas?

Answer 10

50-60 Gy, in 1.8-2 Gy daily fractions.

Question 11

What does hypofractioned radiotherapy mean?

Answer 11

Higher dose per fraction, and a lower total dose. ex 15x2.67Gy.

Question 12

When is hypofractionate radiotherapy after glioma considered?

Answer 12

Typically in older patients (more than 65-70yo) and in those with PKS under 70.

Question 13

What does KPS under 70 mean for an oncologist?

Answer 13

poor prognosis

Question 14

How much is added to “the gross tumour volume” to account for microscopic invasion?

Answer 14

1-2 cm.

Question 15

What structures are at higher risk of toxicity from radiotherapy?

Answer 15

Optic nerves
Optic chiasm
Retinae
Lenses
Brainstem
Pituitary
Cochlea
Hippocampi.

Question 16

What are the good things with proton therapy instead of conventional radiotherapy?

Answer 16

It avoids delayed toxicities and might be options for tumors close to brain regions at risk.

Question 17

What are requirements for pharmacological treatment of glioma pt?

Answer 17

• hepatic and renal laboratory values within the normal ranges
• exclusion of major lung or heart disease
• exclusion of ongoing infection

Question 18

What is the most commonly used drug in glioma treatment?

Answer 18

Temozolomide.

Question 19

What is Temozolomide?

Answer 19

An oral DNA alkylating agent that penetrates the BBB.

Question 20

What are the risks with Temozolomide treatment?

Answer 20

After 2-3 weeks:
* myelosuppression - noteably thrombocytopenia as its main dose-limiting toxicity
* hepatic function

Question 21

name alkylating agents from the nitrosurea class

Answer 21

Lomustine
Carmustine
w more

Question 22

Nitrosurea alkylating agents have their worst sideeffects after 4-6 weeks. What are they?

Answer 22

cumulative leukopenia and thrombocytopenia that might necessitate treatment interruptions.

Question 23

What is usually the composition of PCV?

Answer 23

• Lomustine (nitrosurea alkylating)
• Procarbazine
• Vincristine

Question 24

What are feared long term risks of alkylating agent chemotherapy?

Answer 24

• potential long-term toxicities
• risk of inducing hypermutator phenotype of the tumor.

Question 25

Therapy recommendations for IDH-mutant 1p/19q codeleted oligodendroglioma WHO grade 2

Answer 25

1. surgery
2. watch and wait in gross total resection and also possibly for younger (40) w incomplete resection if the tumor has not caused neurological deficits beyond EP.
3. If more is deemed necessary:
4. Radiotherapy
5. PCV.

Question 26

2nd line treatment for all gliomas

Answer 26

Options determined by KPS, neurologic function and prior treatment.
* repeat surgery
* alkylating chemotherapy
* Re-irradiation
* Experimental therapy

Question 27

How many times is re-irradiation possible?

Answer 27

For those with disease relapse after radiotherapy, re-irradiation after a minimum interval of ~12 months following the first course of radiotherapy is an option, although tumour size and patterns of recurrence limit the option of re-irradiation and the overall efficacy of this strategy remains uncertain in the absence of data from RCTs.

Question 28

How many times can Themozolomide treatment be given?

Question 29

Do we know if Temozolomide would work as well as PCV for the lower grade tumors?

Answer 29

No. There are ongoing studies.

Question 30

Is there any “rescue” third line treatment for low grade glioma if neither radiotherapy or alkylating worked or patient was intolerant?

Answer 30

Only for IDH mut, 1p/19q codeletion tumors=oligodendrogliomas.
Bevacizumab, but its unknown what effect it would have.

Question 31

First line treatment for Astrocytoma, IDH mut, WHO 2?

Answer 31

Same as for oligodendroglioma, IDH mutant, 1p19q codeleted.

• GTR, age under 40, no neurologic deficit (except EP)
  Wait and see OR radiotherapy (50Gy 1.8fractions) followed by PCV. (or when needed)

Obs progression free survival, but not OS has been shown to be prolonged by early radiotherapy but not by RT at disease progression.

Question 32

EANO:
The standard of care for IDH-mutant astrocytomas, WHO grade 2 requiring further treatment ?

Answer 32

Resection as feasible or biopsy followed by involved field radiotherapy and maintenance PCV polychemotherapy.

Question 33

Whats the recomendations for 1st line treatment of grade 3 IDH mut astrocytomas?

Answer 33

The standard of care for IDH-mutant astrocytomas, WHO grade 3 includes resection as feasible or biopsy followed by involved field radiotherapy and maintenance temozolomide (CATNON)88. C: II; L: B.

Question 34

What 2nd line treatment is recomended for IDH mut, 1p/19q codel tumors grade 2 ?

Answer 34

Always consider surgery.
Patients with IDH-mutant and 1p/19q-codeleted oligodendrogliomas, WHO grade 2 requiring further treatment should be treated with radiotherapy followed by PCV polychemotherapy. C: III; L: B.

Question 35

What 2nd line treatment is recomended for IDH mut, 1p/19q codel tumors grade 3 ?

Answer 35

Always consider surgery.
Patients with IDH-mutant and 1p/19q-codeleted oligodendrogliomas, WHO grade 3 should be treated with radiotherapy followed by PCV polychemotherapy (EORTC 26951, RTOG 9402)79,80. C: II; L: B.

Question 36

2nd line recomendation for IDH mut astrocytomas, grade 2 or 3.

Answer 36

Always consider surgery.
Temozolomide chemotherapy is standard treatment at progression after surgery and radiotherapy for most patients with IDH-mutant gliomas, WHO grade 2 or 3. C: II; L: B.

Question 37

What is the standard of care after surgery for adults with newly diagnosed glioblastoma who are in good general and neurological condition and are aged <70 years?

Answer 37

CONCOMITANT radiotherapy and chemotherapy with temozolomide (75 mg/m2 DAILY throughout radiotherapy, including at weekends) plus SIX cycles of maintenance temozolomide (150–200 mg/m2, 5 out of 28 days).

Question 38

Does radiotherapy have a role in the treatment of Glioblastomas?

Answer 38

For decades, radiotherapy (60 Gy in 1.8–2 Gy fractions) has been the standard of care for glioblastoma, approximately doubling median OS duration.

Question 39

How many times can PCV be given?

Answer 39

Alkylating agent-based chemotherapy should be considered for patients who have not received previous chemotherapy and with disease progression after radiotherapy. Temozolomide and nitrosoureas are probably equally effective in this setting.
My note: It seems like PCV is given (the three substances in a special pattern that takes 3 weeks in total) once every 6th week for up to 4-6 times or until progress is seen. I have not found info that the whole schedule can be given more than once.

Question 40

What is first line treatment for Oligodendroglioma grade 3?

Answer 40

For grade 3, usually straight to Radiotherapy followed by PCV.

Question 41

1st line treatment for Astrocytoma IDH mutant WHO grade 3

Answer 41

(or if grade 2 and older pt, neurological deficit or residual tumor)

Radiotherapy followed by
TEMOZOLOMIDE

Question 42

1st line treatment for Astrocytoma, IDH mutant, WHO grade 4?

Answer 42

Radiotherapy followed by TEMOZOLOMIDE wo/w CONCOMITANT temozolomide

Question 43

Treatment of Glioblastoma after surgery/biopsy for pt over 70 yo

Answer 43

Patients with tumours lacking MGMT promoter methylation or of unknown MGMT promoter methylation status should be treated with hypofractionated radiotherapy alone. Those with tumours with MGMT promoter methylation status should receive temozolomide alone (5 out of 28 days until disease progression or for 12 month).

Question 44

Glioblastoma - what cyto to use in the newly diagnosed setting?

Answer 44

Combining temozolomide with lomustine might extend OS in patients with MGMT promoter-methylated glioblastoma

Question 45

Glioblastoma - second surgery?

Answer 45

Second surgery is an option for ~20–30% of patients, commonly with symptomatic but circumscribed relapses diagnosed not earlier than 6 months after initial surgery. Second surgery earlier than 6 months after initial surgery increases the risk of unnecessary intervention on the basis of pseudoprogression and is unlikely to provide durable benefit if the initial surgery followed by radiotherapy did not provide tumour control for more than a few months. ( If the reason was not inadequate surgery)

Question 46

EANO _ rec:
The standard of care for patients with IDH-wild-type glioblastoma aged <70 years and with a KPS >70 ?

Answer 46

Resection as feasible or biopsy followed by involved-field radiotherapy AND concomitant radiotherapy AND six cycles of maintenance temozolomide chemotherapy

Question 47

EANO _ rec:
Does it matter if a glioblastoma patient has a methylated MGMT promotor?

Answer 47

Temozolomide might only be active in patients with MGMT promoter-methylated tumours whereas its activity in patients with MGMT promoter-unmethylated tumours is probably marginal

Question 48

What is involved field radiotherapy?

Question 49

EANO _ rec:
The findings of MGMT methylation dependency for reslut of treatment has changed rec. for elderly (over 70 yo). How?

Answer 49

Elderly patients not considered candidates for temozolomide chemoradiotherapy should be treated on the basis of MGMT promoter methylation status (NOA-08, Nordic Trial) with radiotherapy (such as 15 × 2.66 Gy) or temozolomide (5 out of 28 days) alone

Question 50

EANO _ rec:
What to do when the glioblastoma reoccur?

Answer 50

At recurrence, standards of care are less well defined. Surgery and radiotherapy might be considered. Nitrosourea regimens, temozolomide rechallenge and, with consideration of the country-specific label, bevacizumab are options of pharmacotherapy but an impact on OS remains unproven. ( inte i EU) When available, recruitment into appropriate clinical trials should be considered.

Question 51

EANO rec:
Steroids in glioblastoma?

Answer 51

Steroids should not be given to treat asymptomatic or minimally symptomatic oedema and should be tapered as soon as possible, considering their unfavourable safety profile upon long-term administration. Furthermore, steroid use has been shown to be a negative prognostic factor for OS in patients with glioblastoma from three separate large cohorts123 and might interfere with the efficacy of radiotherapy, chemotherapy and immunotherapy.