Onco 2: cancer in the poo tube

Question 1

risk factors for colorectla cancer

Answer 1

• Hx of polyps
• IBD
  
  • UC
  • Chron’s
  • Chronic inflammation
• Family hx and genetics
  
  • FAP : much much adenomatous polyps
  • HNPCC/Lynch syndrome): mutations in DNA msmatch repair genes
• Smoking
• Heavy EtOH use
• Physical inactiivty
• Low socioeconomic status
• Diabetes
• Increasing age
• Race

Question 1

presentation of colorectal cacner

Answer 1

usually no symptoms early on in disease progression

• Bright red or dark blood in stool, anemia
• Change in frequency of bowel movements
• Constipation or feeling that bowel doesn’t empty completely
• Stool narrow than usualy
• General abdominal discomfort (frequent gas pains, bloating, and/or cramps)
• Wt loss with no known reason
• Constant fatigue
• N/V

Question 2

gold sstandard for screening

Answer 2

colonoscopy
- start at age 45 for most people
- earlie in high risk
- Decision to screen in older pts should be individualized

Question 3

colorectal chemo consdierations

Answer 3

we want good performing pts for chemo otherwise we might be doing more harm than good

• stage of disease
• performance status
• co-morbidities
• genomics
• if metastatic: previous agents used

Question 4

favorable pronostic factors for colorectal cancer

Answer 4

• early disease: stage I-II
• grade 1-2 lesions
• no angiolymphatic invasion
• nevative margins

Question 5

unfavorable prognositc factors for colorectal cncer

Answer 5

• advanced disease : stage III-IV
• grade 3-4 lesioins
• signet-ring cell or mucnous
• lyphovascular invasion
• positive margins
• bowel obstruction/perforation
• T4 disease
• performance status
• lymph node involvement > 4

Question 6

stage I colocrectal treament

Answer 6

surgery alone, no adjuvant chemo

Question 7

stage II colocrectal treament

Answer 7

Surgery +/- adjuvent cehmo (high risk stage II may benefit but no real data atm)
- if giving chemo, capecitabine preferred (can also do FOLFOX or CapeOx)

high risk
- < 12 lymph nodes examined
- Poorly differentiated histology (grade 3-4)
- Lymphovascular invasion
- Bowel obstruction
- Localized perforation
- Positive margins

Question 8

5-FU metabolism

Answer 8

metabolized by DPD (rate limiting)
- some pts can be deficient in DPD (2 nonfunctional copies) -> life threatening tox -> avoid

Question 8

5-FU MOA

Answer 8

breaks down into fDUMP -> inhibit thymidylate synthase -> inhibit DNA synthess

give with leucovrin (folinic acid) -> stabilies fDUMP

Question 9

5-FU ADR

Answer 9

slow infusion -> ADR more tolerable and reduced myelosuppression
- still some hand-foot syndrome, diarrhea, and mucositis though

Question 10

FOLFOX

Answer 10

• folinic acid
• 5-FU
• oxaliplatin

Question 11

FOLFIRI

Answer 11

• folinic acid
• 5-FU
• irinotecan

neoadjuvant only, not adjuvant

Question 12

FOLFOXIRI

FOLFIRINOX

Answer 12

• folinic acid
• 5-FU
• oxaliplatin
• irinotecan

the differene (per NiH i guess?) is that FOLFIRINOX has a higher dose of irinotecan and a bolus 5-FU

Question 13

CapeOx

Answer 13

• capecitabine
• oxaliplatin

Question 14

capecitabine MOA

Answer 14

it’s a 5-FU prodrug

can also be used as a radio-sensitizer (makes people more sensitive to raidation)

Question 15

capecitabine admn

Answer 15

• renally dose adjusted
• BID wihtin 30 min of end of meal

Question 16

dose limiting tox of capecitabine

Answer 16

• hyper ibli
• diarrhea
• hand-foot sydrome
• mucositis

CI in DPD deficiency

DDI with warfarin and phenytoin (CYP2C9)

Question 17

oxaliplatin MOA

Answer 17

• platinum analog, alkyalting agent (creates cross links in DNA)
• not cell-cycle specific

Question 18

oxaliplatin ADR

Answer 18

• peripheral neuroapthy (dose dependent)
  
  • dt accumulation of platinum in dorsal root gannglia
  • duloxetine may help
• cold intolerancesensitivity (type of neuro tox)
  
  • happens right away
  • dt drug being metabolized to oxalate (chelates Ca) → Na voltage gates remain open - hyperexcitability
• myelosupppresion

Question 19

Irinotecan MOA

Answer 19

• topoisomerase-1 inhibitor
• SN-38 is the active drug

Question 20

irinnotecan ADR

Answer 20

• diarrhea
  
  • acute: dt cholinergic symptoms (diarrhea, watery eyes, flusshing, sweating) → give atropine in infusion center
  • chronic: general gut tox dt cytotixc action of drug → loperamide
• fatigue
• alopecia
• myelosuppresion, neutropena

Question 21

Bevacizumab use in colorectal cancer

Answer 21

• Given with chemo for synergistic effect (cuts off blood flow to tumor)
• Used for metastatic colorectal cancer with infusional 5-FU based regimens as 1st or 2nd line

can alternatively use Ziv-aflibercept, but bevacizumab is preferred

Question 22

ramucirumab use in colorectal cancer

Answer 22

FDA approved for use in combo with FOLFIRI in pts who have progressed while being treated with 1st line bevacizumab, oxaplatin, and 5-FU/capecitabine regimen

• Admin 60 min prior to FOLFIRI inf
• Continue until disease progression or unacceptable tox

Question 23

EGFR inhibitors MOA

Answer 23

• Inhibit epidermal growth factor receptor → skin ADR
• pt must be KRAS wild type (no mutation)

If KRAS wt → qualify EGFR inhibitor
Cetuximab
Panitumumab

Question 24

EGFR use in colorectal cancer

Answer 24

used in metastatic colorectal cancer

colorectal gents
- cetuximab
- panitumumab

Question 25

regorafenib MOA

Answer 25

• multikinase inhibitor: nhibit VEGFR 2 and 3, RET, KIT, PDGFR, and Raf kinase

Question 26

regorafenib use in colorectal cancer

Answer 26

FDA approved for later line treatment in metastatic colorectal cancer as monotherapy (salvage therapy)

Question 27

regorafenib DDI

Answer 27

CYP3A4

Question 28

regorafenib admi

Answer 28

• PO QD with low fat meal 3W on, 1W off
• Sotre in original container, 28D expiration date after opening

Question 29

regorafib ADR

Answer 29

• hepatoox (BBW): check LFTs prior to starting
• hemorrhage, delayed wound healing
• cardiac issues
• GI perforation
• hand foot syndrome
• diarrhea
• mucositits
• ifection
• much much much more (try ot match adr to what the drug targets)

very hard for pts to tolerate, many adr

Question 30

HER2 therapy in colorectal cancers

Answer 30

Only indicated in HER2 amplifed tumors that are also RAS and BRAF wild type
- HER2 amplication rare in colorectal cancer
- recommenedd as subequent therapy options in pts who meet the above criteria

Agents
- trastuzumab + (pertuzumab or lapatinib): initial or subsequent
- fam-trastuzumab deruxtecan: subsequent

Question 31

Trifluridine + tipiracil (Lonsurf) use in colorectal cancer

Answer 31

metastatic colorectal cancer if pt has previously received 5-FU/capecitabie-, oxaplatin-, and irinotecan- based chemo, an anti-VEGF biotherapy
- Additionally, if pt KRAS wild type, they need to have tried anti-EGFR therapy
- this bitch very last line

Question 32

Trifluridine + tipiracil MOA

Answer 32

• PO chemo
• interefere iwth DNA syntehsis and inhibit cell proliferation by incorporation in DNA

• trifluridine: thymidine based nucleoside analog (main cytotoxic agent)
• tipiracil: thymidine phophorylase inhibitor → increases trifluridine exposure and has modest cytotoxic activity

Question 33

Trifluridine + tipiracil admin

Answer 33

• PO BID on days 1-5 and 8-12 of a 28 day cycle
  
  • take within 1 hr of the end of breakfast and dinner
  • no need to dose adjust for hepatic or renal impairment
  • could potentially do a regimen of this + bevacizumab

Question 34

Trifluridine + tipiracil ADR

Answer 34

• severe myelosuppression: monitor blood coutns prior to and on day 1 and 15 of each cycle
  
  • dose reduce and/or hold admin as clincally indicated
• anemia
• neutropenia
• thrombocytopenia
• fatigue
• N/V/D
• decreased appetite
• abdominal pain

Question 35

immunotherapy use in colorectal cancer

Answer 35

only for MSI-H tumors (typically in stage 4)

agets:
- pembrolizumab
- nivolizumab

Question 36

BRAF inhibitor use in colorectal cacner

Answer 36

• Only for BRAF genotyped tumor tissue (BRAF V600E mutation postiive) - aggressive tumor with poor prognosis
  **- Doublet therapy (Cetuximab + Encorafenib)
• not first line (typically second or third)**
• Resistance to BRAF inhibitors by feedback re-activaation of EGFR and downstream MEK and ERK pathways

Question 37

stage III colorectal cancer tratment

Answer 37

• surgery + adjuvat chemo in most pts (5-Fu is our standard of care here - FOLFOX or CapeOx)
• start chemo 4-8 weeks after surgery (can go up to 12 but not great), and do it for 6 months
  - If pt was low risk, could consider only 3 months (best evidence for 3 months is pts with low risk and on CapeOx)

Question 38

stage IV colorectal cancer treatment: resectable liver only or lung only metases

Answer 38

can consider sugery
- Give neoadjuvant first
- FOLFIRI, CapeOx, or FOLFOX +/- bevacizumab (remeber to dc bevacizumab 4 weeks prior
- FOLFIRI or FOLFOX +/- panitumumab or cetuximab if KRAS wildype
- Surgery, and then 2-3 months of chemo followed by staged resection of metastataic disease

Question 39

stage IV colorectal cancer treatment: unresectable liver only or lung only metases

or resecctable not doing surgery

Answer 39

• chemo, targeted therapy, immunotherapy and evaluate disease Q2mo to determine resectability of live and/or lung mestases
• Consider coloc resection if risk of obstruction or significant bleeding

Question 40

EGFR MAb ADR

Answer 40

• infusion related reactions (pre-medicate before cetuximab admin)
• hypoMg
• paronchyia: infection of folds of tissue surrounding nails
• acneiform rash