8/27- Cancer Treatment Strategies 1

Question 1

How does cancer cause morbidity and mortality?

Answer 1

• Damages organs via local invasion and compression of vital structures
• Damages organs via metastasis (hallmark of cancer)
• Causes symptoms not related to mass effect (paraneoplastic syndromes)

—-SIADH, hypercalcemia, neurological syndromes

—-But more commonly, causes systemic symptoms via cytokines (cachexia, fatigue) -> wears patients down

Question 2

What makes some cancers more lethal than others?

Answer 2

Absence of effective screening

Delayed diagnosis

• Do not cause symptoms until advanced
• Cause non-specific symptoms
• Hard to diagnose Inherently aggressive “biology”
• Early metastasis
• Relative resistance to available therapies

Question 3

Example of tumor biology affecting behavior

Answer 3

Inherent qualities of tumor

• How much it grows before metastasis (e.g. GIST gets huge while GE jct cancer is small primary with large liver mets)

Question 4

What does “tumor biology” mean?

Answer 4

• Process by which cancer develops from normal tissue (molecular biology, genetics, immunology)
• Pattern of spread

—-Local vs distant

—-“Preferred” distant sites (anatomy, “seed and soil”)

• Speed of growth (kinetics)
• Response to therapy

—-Cytotoxic chemotherapy

—-Biological (targeted) therapy/immunotherapy

—-Radiation

Question 5

Case)

• 65 year old man presents with fatigue and shortness of breath. Laboratory evaluation reveals anemia (hemoglobin 9, ferritin 5). Colonoscopy shows a mass in the ascending colon, biopsy + for adenocarcinoma. CT imaging shows no evidence of metastases.
• The patient undergoes a right hemicolectomy. Pathological evaluation reveals adenocarcinoma invading the pericolonic fat and 4/15 resected lymph nodes, with negative surgical margins. The surgeon informs the patient that he “has gotten it all out” and that the patient does not recommend any further therapy.
• 15 months after his colon surgery, the patient presents to his primary doctor complaining of weight loss, abdominal pain, and fatigue. What happened? Did the surgeon perform an inadequate surgery?

Answer 5

• Not an inadquate surgery
• Stage IIIb colon cancer carries a 50% chance of relapse (micrometastases at time of resection)

Goals now:

• Chemotherapy (palliative)

Question 6

What do localized treatments involve?

Answer 6

• Surgery
• Radiation (standard external beam, intensity-modulated, stereotactic, radioactive beads)
• Ablation (radiofrequency, microwave)
• Chemoembolization

Question 7

What does systemic treatment include?

Answer 7

• Cytotoxic chemotherapy
• Biological (targeted) therapy
• Hormonal therapy
• Immunotherapy (Vaccines, immune modulators, T cell therapy, infectious agents)
• Radiopharmaceuticals

Question 8

How do we choose localized vs. systemic treatment?

Answer 8

Anatomical extent of tumor

• Localized or spread
• Can it be safely resected or irradiated
• Potential morbidity of treatment

Biological behavior of tumor

• Chance of recurrence if resected
• Inherent responsiveness to systemic therapy and/or radiation

Increasingly combining modalities to maximize efficacy and optimize outcome

Question 9

Resecting cancer is frequently feasible and can sometimes cure cancer by itself, but what are the problems?

Answer 9

• Bigger surgery = more morbid
• Cancer can recur locally
• Cancer frequently recurs systemically

Question 10

What is TNM staging?

Answer 10

- T: extent of primary tumor (e.g. in GI wall; through wall; in nearby nodes)

- N: regional lymph nodes

- M: metastases

Question 11

Can anything be done after surgery to lower chance recurrence (think back to adenocarcinoma case)?

Answer 11

Yes: adjuvant therapy

Question 12

Terminology: definitive

Answer 12

Potientially curable by itself; potentially curable

Question 13

Terminology: adjuvant

Answer 13

Administered after definitive treatment to improve the chance for cure; potentially curable

Question 14

Terminology: neoadjuvant

Answer 14

Given before definitive treatment to improve the chance for cure; potentially curable

Question 15

Terminology: palliative

Answer 15

Given to shrink tumor bulk, alleviate cancer-related symptoms, prolong life, and maintain QOL; incurable

Question 16

Scenarios in which we use systemic therapy to treat cancer

Answer 16

• Advanced/metastatic and curable (definitive)

OR

• Advanced/metastatic and incurable (palliative)

OR

• Resected, likely to recur remotely (adjuvant)

OR

• Potentially resectable but local therapy would be morbid and/or cancer likely to recur (neoadjuvant)

AND

• Proven benefit (based on clinical trial data)

Question 17

Processes for systemic therapies: inception -> approval

Answer 17

Step 1: Prove benefit in advanced, incurable cancer:

• Shrinking tumor
• Improving length of survival (by months or sometimes years)

Step 2: Apply this antitumor activity to improve cure rate for earlier stage disease (adjuvant, neoadjuvant, or definitive therapy)

More meaningful advances in cancer survival

Question 18

Systemic therapy: lab -> clinic

Answer 18

- Preclinical: study cell lines, animal models to show in vitro benefit

- Phase I (human trial): establish maximum tolerated dose and safety

- Phase II trial: detect signal of efficacy (response), gather more safety data

- Phase III: randomized controlled trial to prove benefit (survival)

• FDA approval

Question 19

Endpoints of clinical trials: objective tumor response in the presence of measurable disease. What is partial response (PR)?

Answer 19

Shrinking of tumor(s) clinically and/or radiographically by >30%

Question 20

Endpoints of clinical trials: objective tumor response in the presence of measurable disease. What is complete response (CR)?

Answer 20

No tumor seen radiographically or clinically)

Question 21

Endpoints of clinical trials: objective tumor response in the presence of measurable disease. What is progression (PD)?

Answer 21

Growth of tumor(s) by >20% and/or new tumors

Question 22

Endpoints of clinical trials: objective tumor response in the presence of measurable disease. What is stable disease (SD)?

Answer 22

Does not meet criteria for PR or PD

Question 23

Endpoints of clinical trials: objective tumor response in the presence of measurable disease. What is response rate (RR)?

Answer 23

PR + CR

Question 24

Endpoints of clinical trials: objective tumor response in the presence of measurable disease. What is disease control rate (DCR)?

Answer 24

PR + CR + SD

Question 25

Endpoints of clinical trials: survival. What is progression-free survival (PFS)?

Answer 25

Time from starting therapy until cancer progression or death (in the presence of active, measurable disease)

Question 26

Endpoints of clinical trials: survival. What is overall survival (OS)?

Answer 26

Time from starting therapy until death from any cause

Question 27

Endpoints of clinical trials: survival. What is disease-free survival?

Answer 27

Time between definitive treatment until recurrence of cancer or death

Question 28

Picture for survival endpoints (DFS, PFS, OS) over the course of cancer therapy

Answer 28

Question 29

What does a phase III randomized controlled trial for palliative therapy in advanced cancer look like?

Primary endpoints? Secondary?

Answer 29

• Primary endpoint: PFS or OS
• Secondary endpoint: response rate, toxicity

Question 30

What does a phase III randomized controlled trial for adjuvant therapy in advanced cancer look like?

Primary endpoints? Secondary?

Answer 30

• Primary endpoint: DFS or OS
• Secondary endpoints: toxicity

Question 31

Problems with current approach?

Answer 31

• Resources – process requires large numbers of subjects, lots of time, and lots of money
• Not individualized – therapy may show benefit over large populations, but we can’t tell if it will benefit the patient sitting in our clinic

—-Be mindful of statistical significance vs clinical significance (NNT = number needed to treat)

—-Develop biological markers (biomarkers) to predict who will benefit and who will not

• Pitfall of “median overall survival”

Question 32

How does cytotoxic chemotherapy work?

Answer 32

“Cyto-toxic”- kills actively dividing cells by various mechanisms

Question 33

How come chemo works well on cancer cells (more than our own)? Pitfall?

Answer 33

Tumors have high “growth fraction” (high percentage rapidly dividing cells)

• Benefit derived from “debulking”
• Response plateaus b/c chemo kills constant fraction of cells each course (rather than fixed number): log-kill hypothesis

Question 34

How do we use cytotoxic agents?

Answer 34

• Combine drugs w/ different mechanisms and compatible toxicity profiles
• Administer in cycles
• Anti-emetics beforehand
• Generally outpatient
• Intermittent radiographic evaluation

Question 35

Common chemo toxicities?

Answer 35

- Bone marrow suppression: pancytopenia

- GI toxicity – nausea, diarrhea (or constipation), oral mucositis

• General: fatigue, loss of appetite, dysgeusia

- Alopecia

Question 36

Specific chemo toxicities?

Answer 36

- Neuropathy: taxanes, platinum (oxaliplatin), vinca alkaloids

- Cardiac: anthracyclines (doxorubicin)

- Hand-foot syndrome: 5FU/capecitabine

- Nephrotoxicity: cisplatin

- Diarrhea: 5FU, irinotecan

Question 37

What do pts fear most about chemo? What can be done?

Answer 37

Nausea, but now we have some great anti-emetics:

• 5HT antagonists (ondansetron)
• Steroids (dexamethasone)
• NK1 antagonists (aprepitant)

Question 38

Fun Fact: With few exceptions, solid tumors with residual gross disease cannot be cured with chemotherapy alone (cancer stem cells)

Answer 38

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Question 39

Who is more likely to benefit from chemo?

Answer 39

• Patients with more chemoresponsive tumors
• Patients with fewer comorbidities
• Patients with good social support and understanding of their condition
• Patients with a good performance status

While these patients’ cancer cells don’t have a higher chance of being killed by chemotherapy, they have a higher chance of tolerating treatment and clinically deriving benefit

Question 40

What is ECOG performance status?

Answer 40

Grades given to people…

• Associated highly with prognosis
• Validated score for determining who has an acceptable chance of benefiting from chemotherapy (ECOG PS 0-2)
• Good PS usually a criterion for clinical trials

Question 41

Case 2) - An 18 year old male presents with a large testicular mass. Orchiectomy is performed, and pathology reveals choriocarcinoma (nonseminomatous germ cell tumor). He is in otherwise excellent health, and his only additional complaints are vague abdominal pain and shortness of breath with vigorous exertion (ECOG PS 1).

• What is the treatment recommendation? - What is the goal of treatment?
• What is the pt prognosis?
• Why is this pt’s disease potentially curable?

Answer 41

• Recommend: combo chemo -> resection of residual
• Goal = cure
• Prognosis: Excellent (75-80% complete response rate to chemotherapy, 85-90% 5 year progression-free survival)
• Dz is curable due to biology (exquisite chemoresponsiveness)

Question 42

What can be done with stage III colorectal cancer to improve prognosis after surgery?

Answer 42

Adjuvant therapy with 5FU-based chemo

• Adjuvant chemotherapy for Stage III colon cancer improve DFS and OS

Question 43

When is adjuvant chemo for Stage III colon rectal cancer recommended; what are the outcomes?

Answer 43

Question 44

How can neoadjuvant chemo improve outcomes in locally advanced cancer?

Answer 44

• May improve resectability by shrinking tumor
• Increases the chance that patients actually receive adjuvant therapy (chemo better tolerated pre-op)
• Maximizes the benefit of surgery by weeding out those with occult aggressive disease and those who cannot tolerate surgery
• Tests chemosensitivity in vivo
• Facilitates research – tissue studies
• Makes sense for cancers that metastasize early

Question 45

Conclusions:

• Cancer is a heterogeneous group of diseases (highly variable tumor biology)
• Treatment (local vs systemic) is based on tumor stage and biology
• Cytotoxic chemotherapy can be used with palliative, definitive, adjuvant, and neoadjuvant intent (depends on disease)
• We still have far to go, especially with personalizing therapy (tomorrow’s lecture)

Answer 45

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