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MANAGEMENT OF
LOCALLY
ADVANCED NSCLC
DR BOAZ VINCENT
14.07.2017
EPIDEMOLOGY
 Lung cancer is the leading cause of cancer death in
the world
WORLD INDIA
New cancer cases 13 % 6.9 %
Cancer related mortality 19% 9.3%
Lung cancer: Prevalent trends & emerging concepts,
Indian J Med Res 141, January 2015, pp 5-7
Risk Factors
 Active Cigarette Smoking
 Other causal agents:
 Second hand smoking
 Ionizing radiation (including radon)
 Occupational exposures (arsenic, chromium, nickel, asbestos)
 Indoor and outdoor pollution
 Additional risk indicators: age, male sex, family history, acquired lung
disease
Screening
 At least 6 large RCTs evaluated lung cancer screening with CXR, and
none showed a mortality benefit to screening
 Screening with low dose CT – Reduced mortality
 Average dose 2 mSv.
 Eligible patients:
 55-74 years
 30 pack years of smoking; if quit, then within 15 years
 53,454 randomized to 3 annual LDCTs vs. 3 annual CXRs
• 20% relative reduction in lung cancer mortality
• 6.7% relative reduction in all-cause mortality
35%
50%
Routes of spread
 Local extension –
o pleural surfaces, chest wall, ribs, and mediastinal structures
o Apical tumours – Superior sulcus syndrome, SVCO
o Recurrent Laryngeal Nerve - Vocal Cord paralysis
o Phrenic Nerve – Diaphragmatic paralysis
 Regional LNs – Hilar, Interlobar, mediastinal
 Distant metastases
Lung – AJCC 8Th Edition
T1 Tumour 3 cm or less
T1mi Minimally invasive adenocarcinoma
T1a Tumour 1 cm or less
T1b Tumour more than 1 cm but not more than 2 cm
T1c Tumour more than 2 cm but not more than 3 cm
T2 Tumour more than 3 cm but not more than 5 cm; or tumour with any of the
following features:
Involves main bronchus without involvement of the carina, or
invades visceral pleura or associated with atelectasis or obstructive
pneumonitis
T2a Tumour more than 3 cm but not more than 4 cm
T2b Tumour more than 4 cm but not more than 5 cm
Lung – AJCC 8Th Edition
T3 Tumour more than 5 cm but not more than 7 cm or directly invades:
parietal pleura, chest wall, phrenic nerve, or parietal pericardium; or
separate tumour nodule(s) in the same lobe.
T4 Tumour more than 7 cm or of any size that invades any of the following:
diaphragm, mediastinum, heart, great vessels, trachea, recurrent laryngeal
nerve, oesophagus, vertebral body, carina; or separate tumour nodule(s) in
a different ipsilateral lobe to the primary
N Category- No Change
M Category
M1a Separate tumour nodule(s) in a contralateral lobe; tumour with pleural or
pericardial nodules or malignant pleural or pericardial effusion
M1b Single extrathoracic metastasis in a single organ
M1c Multiple extrathoracic metastasis in a single or multiple organs
Right Lung
Upper-1,2,3,4,7
Middle-1,2,3,4,7
Lower-1,2,3,4,7,8,9
Left Lung
Upper-4,5,6,7
Lower-4,5,6,7,8,9
Work up
RADIOLOGICAL
INVESTIGATIONS
 Chest X ray
 CT scan - Base of the neck to below adrenal glands
 Tumour size, mediastinal & vascular invasion
 Lymph node involvement
 Estimate the proximal extent of the tumour within the
airways.
 Distant mets
 Sensitivity is 64% and specificity is 74%
 Bone Scan
 MRI
PET CT SCAN
 Confirm staging
 Detecting metabolically active intrathoracic LNs
 Any occult distant metastaic disease
 Sensitivity & specificity for staging is 83 and 91%,
respectively.
 PPV is ~80% (false-positive rate ~10–20%)
 NPV is ~95% (false-negative rate ~5–16%)
Getting tissue from thorax
 Sputum cytology
 Bronchoscopy
 Endobronchial ultrasound
 Esophageal ultrasound
 Transthoracic biopsy
 Mediastinoscopy
 Electromagnetic navigation
 VATS
Pathology
 ADENO CA – Neoplastic gland formation or intra-
cytoplasmic mucin
 SQUAMOUS CELL CA – Presence of Keratin
production or intra cellular desmosomes
 ADENO SQUAMOUS- Greater than 10% malignant
glandular and squamous components
Immunohistochemistry
DRIVER MUTATIONS
 Somatic gene alterations
 Occurs in genes encoding for proteins which are
critical in cell growth and survival
 1. EGFR – 15% - US ; up to 62% - Asians
Non smokers
Erlotinib, Gefitinib, osemertinib
2. ALK Mutation(Anaplastic Lymphoma Kinase)
 4% in US
 Non smokers and younger patients
 Crizotanib, Ceritinib, alectinib
3. ROS1 translocation 1-2 %
 Adenocarcinoma, young, never smokers
 Crizotinib
MANAGEMENT OF STAGE III NSCLC
1. UNRESECTABLE
2. RESECTABLE
UNRESECTABLE NSCLC
 T4 or N2 disease
 Concurrent chemo radiotherapy is now the standard of
care in unresectable Stage III
Unresectabe - RT alone
Perez at al , IJROBP 1986
• Compared 60 Gy , 50 Gy, 40 Gy and 40 Gy Split course
• Found wit 60 Gy
• Higher complete response – 24%
• Intra-thoracic tumor control – 57%
• 3 year overall survival – 15%
With 60 Gy
• Higher complete
response – 24%
• Intra-thoracic tu
control – 57%
• 3 year OS – 15%
Chemo + RT Vs RT alone
 Although dose escalation was achievable and
appeared to be associated with improvements in local
control in locally advanced NSCLC, the dominant
pattern of failure was distant dissemination in about
75% to 80% of patients.
 To address the issue of systemic therapy was
considered
• Six trials were received (1,205 patients).
• Median follow-up was 6 years.
• Significant benefit of concomitant Rx on overall survival),
• with an absolute benefit of 5.7% at 3 years
• and 4.5% at 5 years.
• For progression-free survival – better with concuurent chemo RT
• No effect on distant progression
• Increased acute esophageal toxicity (grade 3-4) from 4% to 18%
• No significant difference regarding acute pulmonary toxicity
Optimal chemotherapy
regime?
• Identified patients treated with EP and CP with
concurrent radiotherapy - 2001 to 2010.
• Survival rates were compared
Conclusion :
• Patients treated with
EP versus CP had
similar overall
survival, but EP was
associated with
increased morbidity.
Optimal dose
Interpretation
• 74 Gy in 2 Gy fraction
with conc chemo was
not better than 60 Gy,
and might be
potentially harmful.
• Addition of cetuximab
to concurrent chemRT
provided no benefit in
OS
Un-resectable Stage III - Summary
 Concurrent chemo-radiotherapy is preferred
 Optimal chemotherapy is an open question
 Randomized evidence supports a total dose of 60Gy in 2Gy
daily fractions with concurrent chemotherapy
 Sequential chemo-radiation, and radiation alone are options in
less-fit patients
RESECTABLE STAGE III
 In carefully selected patients with limited stage IIIA disease
that can be completely resected, initial surgery is often the
treatment of choice
 Examples include T3N1 disease, or T4 disease due to
multiple tumor nodules in one lung
POST OP CHEMOTHERAPY
• Individual patient data pooled from the five largest trials
(4,584 patients) of cisplatin-based chemotherapy in
completely resected patients conducted after 1995
5-year absolute
benefit of 5.4%
from chemotherapy
POST OPERATIVE
RADIOTHERAPY
 Why consider PORT?
 R1 resection (positive margins)
 R0 resection with positive nodes
PORT : Positive margins
• Patients with path stage N0-2 / stage II or III NSCLC
• Undergone a lobectomy or pneumonectomy with positive
surgical margins
• PORT – 50 to 74 Gy Vs observation
• Conclusion : PORT is associated with improved overall
survival
PORT in N2 nodes ??
 Still controversial
 Ongoing Trial EORTC 22055 – Phase III European
LUNG-ART randomized trial
 Dose is 54 Gy in 30 fractions
EORTC 22055
 Chemo RT followed by Surgery Vs Chemo RT alone-
 Intergroup 0139 (Lancet. 2009)
 Surgery arm – Better local control and PFS , No OS benefit
 Benefit those who underwent Lobectomy, high post operative
complications in pneumonectomy patients
 Chemo – Surgery Vs chemo followed by RT
 EORTC 08941
 Median survival and five-year overall survival rates were similar.
 RT is the preferred local treatment
Stage III resectable - summary
RADIOTHERAPY PLANNING
RTOG 0839
Immobilisation
 Patient is made to lie in a supine position with arms above or in an
akimbo position
 Immobilised using a VacLoc
 CT simulation is done in the same position
 CT images are aquired in 3mm/5mm cuts from level of cricoid
superiorly to include whole of liver inferiorly
 </=3mm slices are recommended throug the regions of gross
tumour, Enlarged LNs
Tumor volumes
GTV
Primary tumour + Gross nodes as visualised on CT/PET
(Nodes >1cm short axis diameter and/or with PET
uptake of suvMax of 3)
CTV
GTV + 0.5-1 cm margin - microscopic tumor extension.
All known levels of mediastinal nodal involvement
(defined both clinically and pathologically )
ITV / PTV
Simulation Techniques
OARs
PORT – LUNG ART Trial
 To start PORT as soon as possible after randomization.
 No concomitant chemotherapy is allowed.
 At least 10 days’ interval between the last day of chemotherapy
and PORT is requested – more in case of radio-sensitizing
chemotherapy.
 Dose - 54 Gy in 27 fractions of 2.0 Gy / fraction
 Treat once a day, 5 days per week.
Volume definitions
 rCTV in the mediastinum :
 Pathologic positive LN stations
 The bronchial stump, the homolateral hilar node region
will always be included in the rCTV.
 CTV in the mediastinum
 rCTV plus a margin corresponding to the upper and lower LN
station
 All LNs between two invoved noncontiguous node stations
will be included
 Because of the frequent involvement of subcarinal (LN7) and
paratracheal nodes (LN4) on surgical series, these stations
will also be systematically
 Left sided tumor - subaortic and PA nodes (LN 5 and 6)
should be included because they are very often involved
 Homolateral supraclavicular region will not be included
systematically in the CTV
PTV-
 Owing to organ movements and to setup uncertainties, an
additional margin of
 at least 0.5 cm (lateral, anterior, and posterior) and
 1 cm (superior and inferior) is recommended.
Right Lung
Upper-1,2,3,4,7
Middle-1,2,3,4,7
Lower-1,2,3,4,7,8,9
Left Lung
Upper-4,5,6,7
Lower-4,5,6,7,8,9
SEQUELAE OF THERAPY
Acute Sequelae
 Acute toxicities: Esophagitis, cough, skin reaction
 Acute radiation esophagitis: begins in the 3rd week of
R/T, approximately 30 Gy
 Nutritional status is compromised: N-G tube,
temporary gastrostomy
 Radiation pneumonitis:
Bed rest, bronchodilators, and steroids
SEQUELAE OF THERAPY
Late Sequelae
 Pneumonitis (10% grade 2 and 4.6% grade 3)
 Pulmonary fibrosis (20% grade 2 and 8% grade 3 or greater)
 Esophageal stricture
 Cardiac sequelae (pericardial effusion, constrictive
pericarditis, cardiomyopathy)
 Spinal cord myelopathy
 Brachial plexopathy.
Follow up
Thank You!!
CHART
HART

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Management of Locally advanced NSCLC

  • 1. MANAGEMENT OF LOCALLY ADVANCED NSCLC DR BOAZ VINCENT 14.07.2017
  • 2. EPIDEMOLOGY  Lung cancer is the leading cause of cancer death in the world WORLD INDIA New cancer cases 13 % 6.9 % Cancer related mortality 19% 9.3% Lung cancer: Prevalent trends & emerging concepts, Indian J Med Res 141, January 2015, pp 5-7
  • 3. Risk Factors  Active Cigarette Smoking  Other causal agents:  Second hand smoking  Ionizing radiation (including radon)  Occupational exposures (arsenic, chromium, nickel, asbestos)  Indoor and outdoor pollution  Additional risk indicators: age, male sex, family history, acquired lung disease
  • 4. Screening  At least 6 large RCTs evaluated lung cancer screening with CXR, and none showed a mortality benefit to screening  Screening with low dose CT – Reduced mortality  Average dose 2 mSv.  Eligible patients:  55-74 years  30 pack years of smoking; if quit, then within 15 years  53,454 randomized to 3 annual LDCTs vs. 3 annual CXRs
  • 5.
  • 6. • 20% relative reduction in lung cancer mortality • 6.7% relative reduction in all-cause mortality
  • 8. Routes of spread  Local extension – o pleural surfaces, chest wall, ribs, and mediastinal structures o Apical tumours – Superior sulcus syndrome, SVCO o Recurrent Laryngeal Nerve - Vocal Cord paralysis o Phrenic Nerve – Diaphragmatic paralysis  Regional LNs – Hilar, Interlobar, mediastinal  Distant metastases
  • 9.
  • 10.
  • 11. Lung – AJCC 8Th Edition T1 Tumour 3 cm or less T1mi Minimally invasive adenocarcinoma T1a Tumour 1 cm or less T1b Tumour more than 1 cm but not more than 2 cm T1c Tumour more than 2 cm but not more than 3 cm T2 Tumour more than 3 cm but not more than 5 cm; or tumour with any of the following features: Involves main bronchus without involvement of the carina, or invades visceral pleura or associated with atelectasis or obstructive pneumonitis T2a Tumour more than 3 cm but not more than 4 cm T2b Tumour more than 4 cm but not more than 5 cm
  • 12. Lung – AJCC 8Th Edition T3 Tumour more than 5 cm but not more than 7 cm or directly invades: parietal pleura, chest wall, phrenic nerve, or parietal pericardium; or separate tumour nodule(s) in the same lobe. T4 Tumour more than 7 cm or of any size that invades any of the following: diaphragm, mediastinum, heart, great vessels, trachea, recurrent laryngeal nerve, oesophagus, vertebral body, carina; or separate tumour nodule(s) in a different ipsilateral lobe to the primary N Category- No Change M Category M1a Separate tumour nodule(s) in a contralateral lobe; tumour with pleural or pericardial nodules or malignant pleural or pericardial effusion M1b Single extrathoracic metastasis in a single organ M1c Multiple extrathoracic metastasis in a single or multiple organs
  • 13.
  • 16. RADIOLOGICAL INVESTIGATIONS  Chest X ray  CT scan - Base of the neck to below adrenal glands  Tumour size, mediastinal & vascular invasion  Lymph node involvement  Estimate the proximal extent of the tumour within the airways.  Distant mets  Sensitivity is 64% and specificity is 74%  Bone Scan  MRI
  • 17. PET CT SCAN  Confirm staging  Detecting metabolically active intrathoracic LNs  Any occult distant metastaic disease  Sensitivity & specificity for staging is 83 and 91%, respectively.  PPV is ~80% (false-positive rate ~10–20%)  NPV is ~95% (false-negative rate ~5–16%)
  • 18. Getting tissue from thorax  Sputum cytology  Bronchoscopy  Endobronchial ultrasound  Esophageal ultrasound  Transthoracic biopsy  Mediastinoscopy  Electromagnetic navigation  VATS
  • 19. Pathology  ADENO CA – Neoplastic gland formation or intra- cytoplasmic mucin  SQUAMOUS CELL CA – Presence of Keratin production or intra cellular desmosomes  ADENO SQUAMOUS- Greater than 10% malignant glandular and squamous components
  • 21. DRIVER MUTATIONS  Somatic gene alterations  Occurs in genes encoding for proteins which are critical in cell growth and survival  1. EGFR – 15% - US ; up to 62% - Asians Non smokers Erlotinib, Gefitinib, osemertinib
  • 22. 2. ALK Mutation(Anaplastic Lymphoma Kinase)  4% in US  Non smokers and younger patients  Crizotanib, Ceritinib, alectinib 3. ROS1 translocation 1-2 %  Adenocarcinoma, young, never smokers  Crizotinib
  • 23. MANAGEMENT OF STAGE III NSCLC 1. UNRESECTABLE 2. RESECTABLE
  • 24. UNRESECTABLE NSCLC  T4 or N2 disease  Concurrent chemo radiotherapy is now the standard of care in unresectable Stage III
  • 25. Unresectabe - RT alone Perez at al , IJROBP 1986 • Compared 60 Gy , 50 Gy, 40 Gy and 40 Gy Split course • Found wit 60 Gy • Higher complete response – 24% • Intra-thoracic tumor control – 57% • 3 year overall survival – 15%
  • 26. With 60 Gy • Higher complete response – 24% • Intra-thoracic tu control – 57% • 3 year OS – 15%
  • 27. Chemo + RT Vs RT alone  Although dose escalation was achievable and appeared to be associated with improvements in local control in locally advanced NSCLC, the dominant pattern of failure was distant dissemination in about 75% to 80% of patients.  To address the issue of systemic therapy was considered
  • 28.
  • 29.
  • 30. • Six trials were received (1,205 patients). • Median follow-up was 6 years. • Significant benefit of concomitant Rx on overall survival), • with an absolute benefit of 5.7% at 3 years • and 4.5% at 5 years. • For progression-free survival – better with concuurent chemo RT • No effect on distant progression • Increased acute esophageal toxicity (grade 3-4) from 4% to 18% • No significant difference regarding acute pulmonary toxicity
  • 31.
  • 33. • Identified patients treated with EP and CP with concurrent radiotherapy - 2001 to 2010. • Survival rates were compared Conclusion : • Patients treated with EP versus CP had similar overall survival, but EP was associated with increased morbidity.
  • 35. Interpretation • 74 Gy in 2 Gy fraction with conc chemo was not better than 60 Gy, and might be potentially harmful. • Addition of cetuximab to concurrent chemRT provided no benefit in OS
  • 36.
  • 37. Un-resectable Stage III - Summary  Concurrent chemo-radiotherapy is preferred  Optimal chemotherapy is an open question  Randomized evidence supports a total dose of 60Gy in 2Gy daily fractions with concurrent chemotherapy  Sequential chemo-radiation, and radiation alone are options in less-fit patients
  • 38. RESECTABLE STAGE III  In carefully selected patients with limited stage IIIA disease that can be completely resected, initial surgery is often the treatment of choice  Examples include T3N1 disease, or T4 disease due to multiple tumor nodules in one lung
  • 39. POST OP CHEMOTHERAPY • Individual patient data pooled from the five largest trials (4,584 patients) of cisplatin-based chemotherapy in completely resected patients conducted after 1995
  • 40.
  • 41. 5-year absolute benefit of 5.4% from chemotherapy
  • 42. POST OPERATIVE RADIOTHERAPY  Why consider PORT?  R1 resection (positive margins)  R0 resection with positive nodes
  • 43. PORT : Positive margins • Patients with path stage N0-2 / stage II or III NSCLC • Undergone a lobectomy or pneumonectomy with positive surgical margins • PORT – 50 to 74 Gy Vs observation • Conclusion : PORT is associated with improved overall survival
  • 44.
  • 45. PORT in N2 nodes ??  Still controversial  Ongoing Trial EORTC 22055 – Phase III European LUNG-ART randomized trial  Dose is 54 Gy in 30 fractions
  • 47.  Chemo RT followed by Surgery Vs Chemo RT alone-  Intergroup 0139 (Lancet. 2009)  Surgery arm – Better local control and PFS , No OS benefit  Benefit those who underwent Lobectomy, high post operative complications in pneumonectomy patients  Chemo – Surgery Vs chemo followed by RT  EORTC 08941  Median survival and five-year overall survival rates were similar.  RT is the preferred local treatment
  • 48. Stage III resectable - summary
  • 50. RTOG 0839 Immobilisation  Patient is made to lie in a supine position with arms above or in an akimbo position  Immobilised using a VacLoc  CT simulation is done in the same position  CT images are aquired in 3mm/5mm cuts from level of cricoid superiorly to include whole of liver inferiorly  </=3mm slices are recommended throug the regions of gross tumour, Enlarged LNs
  • 51. Tumor volumes GTV Primary tumour + Gross nodes as visualised on CT/PET (Nodes >1cm short axis diameter and/or with PET uptake of suvMax of 3) CTV GTV + 0.5-1 cm margin - microscopic tumor extension. All known levels of mediastinal nodal involvement (defined both clinically and pathologically ) ITV / PTV
  • 52.
  • 54. OARs
  • 55. PORT – LUNG ART Trial
  • 56.  To start PORT as soon as possible after randomization.  No concomitant chemotherapy is allowed.  At least 10 days’ interval between the last day of chemotherapy and PORT is requested – more in case of radio-sensitizing chemotherapy.  Dose - 54 Gy in 27 fractions of 2.0 Gy / fraction  Treat once a day, 5 days per week.
  • 57. Volume definitions  rCTV in the mediastinum :  Pathologic positive LN stations  The bronchial stump, the homolateral hilar node region will always be included in the rCTV.
  • 58.  CTV in the mediastinum  rCTV plus a margin corresponding to the upper and lower LN station  All LNs between two invoved noncontiguous node stations will be included  Because of the frequent involvement of subcarinal (LN7) and paratracheal nodes (LN4) on surgical series, these stations will also be systematically  Left sided tumor - subaortic and PA nodes (LN 5 and 6) should be included because they are very often involved  Homolateral supraclavicular region will not be included systematically in the CTV
  • 59. PTV-  Owing to organ movements and to setup uncertainties, an additional margin of  at least 0.5 cm (lateral, anterior, and posterior) and  1 cm (superior and inferior) is recommended.
  • 60.
  • 62. SEQUELAE OF THERAPY Acute Sequelae  Acute toxicities: Esophagitis, cough, skin reaction  Acute radiation esophagitis: begins in the 3rd week of R/T, approximately 30 Gy  Nutritional status is compromised: N-G tube, temporary gastrostomy  Radiation pneumonitis: Bed rest, bronchodilators, and steroids
  • 63. SEQUELAE OF THERAPY Late Sequelae  Pneumonitis (10% grade 2 and 4.6% grade 3)  Pulmonary fibrosis (20% grade 2 and 8% grade 3 or greater)  Esophageal stricture  Cardiac sequelae (pericardial effusion, constrictive pericarditis, cardiomyopathy)  Spinal cord myelopathy  Brachial plexopathy.
  • 66. CHART
  • 67. HART