Early-stage (I-II) Non-small cell lung cancer

Question 1

Estimated annual # of new lung cancer cases diagnosed in the US and the # of deaths from lung cancers

Answer 1

2017 ACS estimates - 222,500 new cases and 155,870 deaths

Question 2

What is the lifetime risk of developing lung cancer - in men and women? Any differences by race?

Answer 2

Men: 1 in 14; Women: 1 in 17
Black men have a 20% higher incidence of lung cancer than white men. Black women have a 10% lower incidence than white women

Question 3

What is the 5 yr survival rate for lung cancer patients by stage?

Answer 3

Stage IA: 49%
Stage IB: 45%
Stage IIA: 30%
Stage IIB: 31%
Stage IIIA: 14%
Stage IIIB: 5%

Question 4

How many lobes are in the lung? How many segments are there per lobe?

Answer 4

There are 5 lobes in the lung (RUL, RML, RLLL, LUL, LLL)
The lingula is part of the LUL
There are 5 segments per lobe, except the RUL and RML have 3 and 2 segments respectively

Question 5

What are the 9 N2 nodal stations?

Answer 5

Station 1: highest mediastinal
Station 2: upper paratracheal
Station 3: prevascular (3A) and retrotracheal/prevertebral (3P)
Station 4: lower paratracheal
Station 5: subaortic (AP window)
Station 6: P-A
Station 7: subcarinal
Station 8: paraesophageal
Station 9: pulmonary ligament

Question 6

Where are the intrapulmonary and hilar nodes located?

Answer 6

Intrapulmonary nodes are along the secondary bronchi
The hilar nodes are along the mainstem bronchi
These are all considered N1 nodes

Question 7

What are the 5 N1 nodal stations?

Answer 7

Station 10: hilar
Station 11: interlobar
Station 12: lobar
Station 13: segmental
Station 14: subsegmental

Question 8

What are the 3 histologic subtypes of NSCLC in decreasing order of frequency?

Answer 8

Adenocarcinoma (>50%) > SCC (35%) > Large cell (15%)

Question 9

In addition to tobacco smoke, what are 3 other environmental exposure risk factors for developing lung cancers?

Answer 9

Radon
Asbestos
Occupational exposure

Question 10

What is the estimated RR for lung cancer in heavy smokers vs. nonsmokers?

Answer 10

Heavy smokers have a 20-fold excess of lung cancer

Also have a 2-3% per yr risk of tobacco induced 2nd primary cancer

Question 11

What is the risk of lung cancer in former smokers compared to current smokers?

Answer 11

The risk of developing lung cancer in former smokers is around half that of current smokers

Question 12

What is the risk of lung cancer from passive smoke exposure?

Answer 12

RR 1.24 for developing lung cancer from passive smoke exposure

Question 13

What % of smokers develop lung cancer?

Answer 13

<20% of smokers actually develop lung cancer

Question 14

What histology subtype of NSCLC is least associated with smoking?

Answer 14

Adenocarcinoma is least associated with smoking

Question 15

Name 3 histologic variants of adenocarcinoma of the lung

Answer 15

Adenocarcinoma in situ (previously bronchoalveolar)
Acinar
Papillary

Question 16

Discuss the natural history and treatment response of adenocarcinoma in situ (formerly bronchoalveolar) carcinoma

Answer 16

Not associated with smoking. Presents as solitary nodule or multifocally. Pneumonitic form can spread along alveoli without basement membrane invasion. These tumors have good response rates to TKIs

Question 17

Name 2 variants of large cell cancer of the lung

Answer 17

Giant cell and clear cell

Question 18

What is the most common stage at initial presentation?

Answer 18

Stage IV (30%)

Question 19

What are the most common sites of distant metastases for lung cancer?

Answer 19

Bone, adrenals and brain

Question 20

What are the paraneoplastic syndromes associated with lung cancers?

Answer 20

Hypercalcemia of malignancy - PTHrP
SIADH - leads to hyponatremia
Cushing - increased ACTH
Lambert-Eaton syndrome 
Hypercoagulability (adenocarcinoma)
Gynecomastia (large cell)
Carcinoid (vasoactive intestinal peptide), diarrhea
Hypertrophic osteoarthropathy (adenocarcinoma)

Question 21

What is the cause of Lambert-Eaton syndrome? Clinically how do you distinguish L-E syndrome from myasthenia gravis?

Answer 21

Circulating antibodies against against presynaptic P/Q calcium channel. With repeat motion, patients with L-E have improved strength whereas MG patients fatigue with repitition

Question 22

What histologic subtypes of lung cancer are associated with peripheral and central lesions?

Answer 22

Peripheral: adenocarcinoma, large cell
Central: squamous cell

Question 23

With which histologic subtypes of lung cancer is Thyroid Transcription Factor-1 (TTF-1) staining associated?

Answer 23

Adenocarcinoma, nonmucinous bronchioalveolar carcinoma (adenocarcinoma in situ) and neuroendocrine tumors
TTF-1 is rare in squamous cell

Question 24

In NSCLC what is the role of CXR or CT screening for high risk patients?

Answer 24

CXR is not recommended. The USPSTF recommends annual screening with LDCT in people between ages 55 and 80 with a greater than 30 pack-year smoking history in current smokers and those who quit <15 yrs ago

Question 25

What RCT reported low dose CT screening for lung cancer?

Answer 25

The national lung cancer screening trial - prospective RCT comparing LDCT vs. annual CXR for 3 years
LDCT reduced RR of lung cancer death by 20%
To prevent 1 death: 320 high risk pts need to be screened

Question 26

What factors define high risk group for lung cancer according to NCCN?

Answer 26

Age 55-74 and >30 pack-year smoking history and <15 years cessation OR age >50 and >20 pack-year history of smoking and additional risk factors that increase risk (COPD, cancer hx, FHx, ethnicity)

Question 27

What is lead-time bias and how could it affect the results of a screening trial?

Answer 27

Lead time in diagnosis is the time between detecting the cancer from screening and when the diagnosis would have otherwise occurred due to symptoms or imaging studies. This can lead to an apparent increase in survival.

Question 28

What is length-time bias and how could it affect the results of a screening trial?

Answer 28

Length-time bias occurs when a screening test detects cancers that take longer to become symptomatic due to the detection of slower growing or indolent cancers. This leads to an apparent increase in survival.

Question 29

What is the single most clinically significant acquired genetic abnormality in NSCLC?

Answer 29

EGFR mutation in exon 19 and exon 21

Question 30

Among patients with NSCLC, in what particular groups are the EGFR mutations common and for what do these mutations predict?

Answer 30

EGFR mutations only occur in ~10% but at high rates in nonsmokers, adenocarcinomas and Asians
These predict a high response rate >80% to TKIs (gefitinib, erlotinib, afatinib, osimertinib)

Question 31

Is EGFR overexpression more common in SCC or adenocarcinoma?

Answer 31

EGFR may be overexpressed in 80-90% of SCCs vs. 30% of adenocarcinomas

Question 32

What are common mechanisms associated with TKI resistance?

Answer 32

T790M is a point mutation that accounts for 60% of TKI resistence, usually devlop after 9-13 months of therapy
Other mechanisms: KRAS, ALK, ROS1, exon 20 insertion, small cell transformation, epithelial-mesenchymal transition phenotype

Question 33

What is the initial workup for a patient suspected of having lung cancer?

Answer 33

H&P, focus on weight loss >5% over prior 3 months, KPS, tobacco history, neck exam for N3 disease, CBC, CMP, CT chest (include adrenals), PET/CT scan, MRI brain for presumed stage II-III, MRI for paraspinal/superior sulcus tumors, biopsy via bronch or FNA, mediastinoscopy, PFTs

Question 34

What is the most cost effective first step in a patient presenting with a new lung lesion on CXR or CT?

Answer 34

Obtain prior imaging for comparison

Question 35

What are the 3 most common presenting symptoms of NSCLC?

Answer 35

Dyspnea, cough, weight loss, chest pain, hemoptysis

Question 36

What is the sensitivity and specificity of sputum cytology for diagnosis of lung cancer?

Answer 36

Sensitivity <70%, specificity >90%

Accuracy increases with more # of specimens, at least 3 are recommended

Question 37

What is the sensitivity and specificity of FDG-PET compared to CT for staging of lung cancers?

Answer 37

PET: sensitivity 83%, specificity 91%
CT: sensitivity 64%, specificity 74%

Question 38

What is the estimated % of patients who will have false + N2 nodes on PET/CT?

Answer 38

10-20%. N2 nodes by PET/CT need pathologic confirmation before deferring to potentially curative surgery

Question 39

What is the estimated % of patients who will have false - N2 nodes based on PET/CT?

Answer 39

5-16%.

Question 40

What is the rate of occult mets from lung cancer detected by FDG-PET?

Answer 40

6-18%

Question 41

If a PET is being ordered, should a bone scan be ordered to evaluate for bone mets as well?

Answer 41

No. In NSCLC, PET is just as sensitive as a bone scan but more specific. However, consider pathologic confirmation of solitary PET+ lesions given the risk of false + results

Question 42

What clinical characteristics are important to focus on to determine the nature of a solitary pulmonary nodule?

Answer 42

Nodule size (and whether there are changes in size in the past 2 years), history of smoking, age, and nodule margin on CT (spiculation?)

Question 43

Stage for stage, does adenocarcinoma or SCC have a worse prognosis? Why?

Answer 43

Adenocarcinoma has worse prognosis as it has a greater propensity to metastasize, particularly to the brain

Question 44

Does large cell carcinoma have a natural history and prognosis more similar to SCC or adenocarcinoma?

Answer 44

Large cell carcinoma has a natural history and prognosis more similar to adenocarcinoma

Question 45

Describe the T-staging of NSCLC

Answer 45

T1: ≤3 cm, surrounded by lung parenchyma (T1a ≤1 cm; T1b 1.1–1.9 cm; T1c 2.0–2.9 cm)
T2: >3 but ≤5 cm, + visceral pleura, main bronchus (not carina), +atelectasis of lobe (T2a 3.1–3.9 cm; T2b 4.0–4.9 cm)
T3: >5 but ≤7 cm, tumor invading invasion to CW, pericardium, phrenic nerve or separate tumor nodule in same lobe
T4: >7 cm any size, invading mediastinum, diaphragm, heart, great vessels, trachea, recurrent laryngeal nerve, esophagus, vertebral body, carina, or with separate tumor nodules in a different ipsi lung lobe

Question 46

Describe the N staging of NSCLC

Answer 46

N1: ipsi hilar or pulmonary nodes
N2: ipsi mediastinal or subcarinal nodes
N3: any SCV/scalene nodes or contralat mediastinal/hilar nodes

Question 47

How are malignant pleural/pericardial nodules/effusion or opposite lung tumor nodules noted in the newest TNM staging?

Answer 47

M1a includes malignant pleural/pericardial nodules/effusion and opposite lung tumor nodules

Question 48

According to AJCC 8th ed, is a single brain met staged the same as brain mets and bone mets. What about 2 brain mets?

Answer 48

A single extrathoracic met is M1b

Multiple extrathoracic mets (1 organ or >1 organ) is M1c

Question 49

What is the nodal subclassification in AJCC 8th edition?

Answer 49

N1: N1a-Single station N1 involvement, N1b-Multiple station N1 involvement; N2a1-single station N2 without N1 involvement (skip), N2a2-single station N2 with N1 involvement, N2b-multiple station N2 involvement; N3-N3 LN involvement

Question 50

What is considered early stage NSCLC?

Answer 50

Stages I and II

Question 51

What procedures prior to thoracotomy can be used to evaluate the level 1 L and R stations, 2, 4 and 7. What aboust stations 5 and 6?

Answer 51

Mediastinoscopy or EBUS can evaluate L/R 2, 3 and 7

VATS or anterior mediastinotomy can evaluate stations 5-6

Question 52

When should pre-treatment mediastinal nodal assessment be done?

Answer 52

To confirm PET or CT + nodes
All suspicous sulcus tumors
If T3 or central T1-2 lesions

Question 53

What PFT results indicate that patient needs further testing prior to undergoing resection?

Answer 53

FEV1 < 80% predicted or DLCO < 80% predicted

Question 54

What is the minimum absolute FEV1 necessary for pneumonectomy and lobectomy

Answer 54

Pneumonectomy >2L

Lobectomy: Postop >1.0L

Question 55

Which subset of lung cancer patients are at high risk for surgical morbidity?

Answer 55

pCO2 > 45, pO2 <50, Preop FEV1 <40%, poor exercise tolerance, DLCO <40% (desired > 60%), postop FEV1 < 0.71 or <30% predicted value, cardiac problems, obesity

Question 56

What are some factors that predict postop complications?

Answer 56

Active smoking, poor nutrition, advanced age, poor lung function

Question 57

What % of patients clinically at stage I are upstaged at surgery?

Answer 57

5-25% of stage I lung cancer patients are upstaged at surgery

Question 58

In addition to stage, name 3 poor prognostic factors in lung cancer patients?

Answer 58

KPS < 80%, weight loss >5% in 3 months (10% in 6 months), age > 60y

Question 59

What is the treatment paradigm for stage I-II medically operable NSCLC?

Answer 59

Surgical resection (lobectomy) + mediastinal LND followed by adjuvant chemo (unless stage IA w/ negative margins)

Question 60

What should be the first step for a stage I-II medically operable NSCLC patient with a positive margin resection

Answer 60

Re-resection if possible, +/- chemothearpy depending on other factors

Question 61

If re-resection is not possible, what RT dose is used for a +margin after surgery?

Answer 61

Microscopic +margin: 54-60Gy

Gross +margin: 60-70 Gy

Question 62

What is the treatment paradigm for stage I-II medically inoperable NSCLC?

Answer 62

Stages I-II medically inoperable NSCLC Tx paradigm: if T1-2N0, consider definitive hypofractionated SBRT or SABR. If T1-T2N1 or T3N0 use definitive CRT

Question 63

Name 3 surgical options to resect a T1-T2 tumor

Answer 63

Surgical options to resect a T1-T2 tumor:
wedge or segmental resection
lobectomy
pneumonectomy

Question 64

For a T1N0 NSCLC, what is the estimated LC for wedge/segmental resection vs. lobectomy?

Answer 64

Wedge/segmental LC is 82% vs. lobectomy LC is 94% based on RCT LCSG 821. Lobectomy is preferred when feasible.
*CALGB 140503 is ongoing phase III trial of lobectomy vs. sublobar resection for <2cm peripheral NSCLC

Question 65

What % of stage I NSCLC patients will develop a 2nd primary after definitive surgical resection?

Answer 65

Up to 30% will develop a 2nd primary

Question 66

What is the estimated 5 yr OS of completely resected T1-2N0 NSCLC with no adjuvant chemo?

Answer 66

T1N0 ~80%

T2N0 ~68%

Question 67

What is the 5yr OS, CSS and MS for patients who refuse any treatment for T1-2N0 NSCLC?

Answer 67

5yr OS 6%, CSS 22%, MS is 13 months

Tumor size is a prognostic factor independent of T stage

Question 68

What are the indications for adjuvant chemo after definitive resection for stages I-II NSCLC?

Answer 68

High risk stages IB-IIB
N1 disease
T2N0, if tumor > 4cm

Also consider: poorly differentiated, LVSI, wedge resection, visceral pleural involvement, incomplete nodal sampling

Question 69

Whats the estimated 5 yr OS benefit with adjuvant chemo for patients with completely resected stage I or II NSCLC?

Answer 69

~5% at 5 yrs for adjuvant cisplatin based regimens based on LACE meta-analysis

Question 70

What are possible chemo regimens for adjuvant/neoadjuvant treatment of NSCLC per NCCN?

Answer 70

Cisplatin/vinorelbine
Cisplatin/etoposide
Cisplatin/gemcitabine
Cisplatin/docetaxel
Cisplatin/pemetrexed

Question 71

Is there a role for preop chemotherapy in early stage lung cancer patients?

Answer 71

No. Meta-analysis did not show survival difference between pre and postop chemo.
Trials: MRC LU22/EORTC 08012, The CHEST Trial, NATCH Spanish Trial

Question 72

Is there a benefit of full mediastinal dissection vs. nodal sampling in early stage patients undergoing surgical resection?

Answer 72

Possibly. Pooled analysis of 3 trials demonstrated a 4yr OS benefit of mediastinal dissection in stages I-IIIA NSCLC (HR 0.78)

Question 73

What are the indications for PORT after definitive resection for stages I-II NSCLC?

Answer 73

+Margins, +ECE, unexpected N2 disease

NCCN: Concurrent CRT for R2+ margin, sequential chemo followed by RT for R1+ margin

Question 74

Which randomized study demonstrated improved LC and survival with PORT after surgical resection for early stage (IA and IB) NSCLC?

Answer 74

Italian study: 104 stage I patients resected with N0, randomized to PORT vs. observation
PORT: bronchial stump + ipsilateral hilum, 50.4 Gy 
LF rates (2% vs. 23%), trend to improved 5yr OS (67% vs. 58%)

Question 75

What is the maximum RT dose that has been used for definitive RT alone in stage I-II NSCLC?

Answer 75

Up to 84 Gy in standard fractionation if lung dose-volume constraints are respected.

RTOG dose escalation study found 90.3 Gy was too toxic

Question 76

What is the 2 year LR rate for RT alone using standard fractionation?

Answer 76

50-78% 2 yr LR based on RTOG 9311 (although this includes stage III pts)

Question 77

In stages I-II patients treated with definitive RT alone, should elective nodal regions be treated? What is the estimated elective nodal failure rate if untreated?

Answer 77

No. Elective nodal failure rate < 10% in RTOG 9311.

In hypofrac/SBRT trials, nodal failure rate 5-10%

Question 78

What are the estimated 3-5yr LC and OS for medically inoperable stage I patients treated with definitive SBRT?

Answer 78

3 yr LC 85-95%

3 yr OS 55-91%

Question 79

How does SBRT compare to lobectomy for operable stage I NSCLC?

Answer 79

Pooled analysis of STARS and ROSEL trials, 3yr OS was 95% with SBRT and 79% for surgery
Still controversial, ongoing RCTs
SEER and NCDB analysis have conflicting results

Question 80

What BED should be achieved to attain maximum LC and survival in patients with stage I lung cancer treated with SBRT?

Answer 80

Japanese data suggset BED > 100 Gy results in 5 yr LC rate 92% and 5 yr OS 71%
BED < 100 Gy results in 5 yr LC 57% and OS 30%

Question 81

What is the estimated 5 yr rate of nodal failure, LF, and DM in early stage NSCLC after definitive SBRT?

Answer 81

LRR (nodal) tends to be higher in SBRT patients and increased with time - 5yr LR 7% (RTOG 0236), involved lobar recurrence 20% and regional recurrence 38%
Distant recurrence was 31%

Question 82

What is the SBRT technique evaluated in RTOG 0236? What is the 2 yr LC and OS rate for this group of inoperable patients?

Answer 82

SBRT 20Gy x 3 fractions (18Gy x 3 fractions with heterogeneity correction)
3yr primary tumor control 97.6%, but 3yr primary tumor and involved lobe control 90.6%, DFS 48.3% and OS 55.8%

Question 83

How should the SBRT dose be modified for centrally located tumors?

Answer 83

Lesions located centrally (w/in 2 cm of bronchial tree) are not good candidates for 20Gy/3 fraction due to risk for grade 3-5 toxicities. Studies have shown 12.5Gy x 4 fx (MDACC) and 10-11Gy x 5 fx (RTOG 0813) to be safe for centrally located lesions

MDACC also looked at 70Gy in 10 fx

Question 84

What CTV and PTV margins are used for SBRT?

Answer 84

PTV = ITV + 5mm (MDACC) w/ 4D CT scan (MDACC)

PTV = GTV + 5mm (axial) + 1cm (long) w/o 4D CT scan (RTOG 0915)

Question 85

What studies have attempted to address the role of SBRT in both operable early stage lung cancer patients?

Answer 85

• RTOG 0618: phase II, 33 pts w/ stage I-II NSCLC 18Gy x 3 fx
• ROSEL (dutch): phase III, stage I NSCLC 20Gy x 3 (T1), 12Gy x 5 (T2), 7.5Gy x 8 (central) vs. surgery
• STARS (Accuracy/MDACC): phase III cyberknife vs. surgery. 12.5Gy x 4 (central), 16.7 Gy x 3 (peripheral)
• JCOG 0403: phase II, 48Gy in 4 fx

Question 86

What studies have attempted to address the role of SBRT in both inoperable early stage lung cancer patients?

Answer 86

• TROG 09.02: phase III, T1/T2aN0, 54 Gy in 3 fx vs. conventional 60-66Gy/30-33fx
• RTOG 0915: phase II, T1/T2 NSCLC, peripheral tumors, 34Gy single fraction vs. 12Gy in 4 fractions
• SPACE (scandinavian): phase II 3D CRT 70 Gy in 35 fx vs. SBRT 45 Gy in 3 fx
• RTOG 0813: phase I/II dose escalated SBRT for centrally located tumors

Question 87

What are the toxicities seen with SBRT for early stage lung cancer?

Answer 87

Pneumonitis, lung fibrosis/consolidation, cough, dermatitis, chest wall pain, esophagitis and hemoptysis

Question 88

What is the total lung V20 dose-volume constraint for RT alone?

Answer 88

The total lung V20 is <35% (NCCN 2018)

Question 89

What is the MLD constraint for definitive RT to lung cancer?

Answer 89

MLD < 20Gy (NCCN 2018)

Question 90

What is the distinction between grade 2 and grade 3 RTOG pneumonitis?

Answer 90

Grade 2: symptomatic, need for steroids

Grade 3: dyspnea at rest and O2 supplementation needed

Question 91

What are the heart dose-volume constraints for conventionally fractionated RT?

Answer 91

Heart V40<80%, V45 < 60%, V60 < 30%

Mean < 35 Gy

Question 92

What is the dose constraint for the brachial plexus with conventional fractionation?

Answer 92

Max dose <= 66Gy

Question 93

What is the rate of brachial plexopathy seen for patients treated with SBRT for early stage lung cancer?

Answer 93

Max dose < 26 Gy in 3-4 fractions

Dose > 26 Gy –> 46% risk of plexopathy vs. 8% if <26 Gy

Question 94

At a minimum what other (beyond lung,heart, brachial plexus) normal tissue constraints should be considered?

Answer 94

Esophagus, trachea, main bronchus, bronchial tree, major vessels, skin, chest wall

Question 95

What is the esophageal dose constraint for conventionally fractionated RT?

Answer 95

Mean dose < 34 Gy, max < 105% of prescription dose

Question 96

What is the max BED for SBRT resulting in significant complications when centrally located tumors were treated?

Answer 96

180-210 Gy with grade 3 pulmonary complications

BED > 100 may be sufficient for LC and may avert toxicities for central lesions

Question 97

Is a normal SUVmax of FDG-PET required to be considered a good clinical response in f/u scans after SBRT?

Answer 97

No. SUVmax remains elevated for extended period after SBRT d/t an inflammatory response but there is no evidence of correlation with recurrence

Question 98

What % of patients treated with SBRT for early stage lung cancer have grade 3-5 toxicities?

Answer 98

15% of patients have grade 3-5 toxicities based on a review of 15 studies (683 pts)
In RTOG 0236, 16% of patients had grade 3-4 toxicity, no grade 5 toxicities

Question 99

What factors predict grade 3-5 toxicities after SBRT for early lung cancer seen on the IU phase II study?

Answer 99

Location (46% hilar/pericentral, 17% peripheral) and tumor size (GTV > 10cc 8x risk for G3-5 toxicity)

Question 100

What are the PFT changes before and after SBRT for early stage NSCLC?

Answer 100

Minmal based on institutional review of 92 patients
FEV1 -0.05
DLCO -2.59%
No association with location (central vs. peripheral) or dose administered