overdiagnosis of lung244o831fi1kd234mqc48ph9x-wpengine.netdna-ssl.com/wp-content/uploads/... ·...
TRANSCRIPT
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OVERDIAGNOSIS OF LUNG
CANCERAppropriate Treatment for Lung
Cancer National Lung Cancer Roundtable Annual Meeting
Crystal City, Virginia
December 11, 2018
William D. Travis, M.D.
Attending Thoracic Pathologist
Memorial Sloan Kettering Cancer Center
New York, NY
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NOTHING TO DISCLOSE
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OVERDIAGNOSIS
IN LUNG CANCER SCREENING
▪ Detection of disease, that in the absence of
screening, would have never been diagnosed
▪ Screening seeks to detect occult disease in
asymptomatic individuals
▪ Concern – results in unnecessary treatment,
morbidity, follow-up, cost and anxiety for patients
with disease that otherwise would not have been
detected
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OVERDIAGNOSIS
IN LUNG CANCER SCREENING
▪ Pathologic features may explain favorable
outcome for the minority of lung cancers
▪ ADC - lepidic growth (AIS, MIA, LPA)
▪ Histologic grade
▪ Invasive characteristics: visceral pleural
invasion, STAS, vascular invasion
▪ Molecular characteristics (EGFR/ALK mut)
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2015 WHO CLASSIFICATION OF
LUNG ADENOCARCINOMA▪Comprehensivehistologicsubtyping – 5% increments
▪Solid ADC – mucin + or TTF-1 + (from large cell ca)
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Lepidic
Papillary
Acinar Solid
Micropapillary
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STAGE I ADENOCARCINOMA (N=514)RECURRENCE-FREE SURVIVAL (RFS) BY IASLC HISTOLOGIC TYPE
Yoshizawa, A et al; Modern Pathology 24: 653-664, 2011
Histologic Type
(N)
5 Year
RFS
%
AIS (1) 100
MIA (8) 100
Lepidic NM (29) 90
Papillary (143) 83
Acinar (232) 85
Inv Mucinous Ad (13) 76
Solid (67) 71
Micropapillary (12) 64
Colloid (9) 71
P=0.003
Micropapillary &
Solid Predominant
Colloid, Mucinous Ad
AIS, MIA
Lepidic, Papillary & Acinar
Predominant
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Hung, JJ et al: J Clin Oncol 32:2357-2364, 2014
▪573 resected lung Adenoca
▪Predominant histologic pattern was prognostic for overall, recurrence free and disease specific survival
▪MV analysis: Independent MIP/SOL vs LEP/AC/PAP: HR 1.6 (CI:1.1-2.3) p=0.01
▪For patient group that received adjuvant chemotherapy, solid predominant AD was a significant predictor for OS.
Recurrence Free Survival
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IASLC/ATS/ERS ADENOCARCINOMA
CLASSIFICATION
▪ PREINVASIVE LESIONS
• ATYPICAL ADENOMATOUS HYPERPLASIA
• ADENOCARCINOMA IN SITU (≤3 cm, formerly BAC
pattern) †
– non-mucinous
– mucinous
▪ MINIMALLY INVASIVE ADENOCARCINOMA (≤3 cm, a lepidic
predominant tumor with ≤5mm invasion)
▪ INVASIVE ADENOCARCINOMA† Size should be specified. AIS and MIA should be completely sampled histologically
–J Thoracic Oncol 6:244-285, 2011
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ADENOCARCINOMA IN SITU
NONMUCINOUS
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ADENOCARCINOMA IN SITU
NONMUCINOUS
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MINIMALLY INVASIVE ADENOCA
NONMUCINOUS
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MINIMALLY INVASIVE ADENOCA
NONMUCINOUS
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LEPIDIC PREDOMINANT
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Patients distribution by lepidic pattern and their recurrence-free probability (RFP)
–p=0.001
Subtype n5-yr
RFP
AIS+MIA 2+34 100%
Lepidic 103 91%
Others 907 80%
–AIS: n=2
–(0.2%)
–MIA: n=34
–(3%)
–Lepidic: n=103
–(10%)
–Others: n=907
–(87%)
–Lepidic pattern (patient, %) –RFP by lepidic pattern
–AIS/MIA/Lepidic
–Totally n=138 (13%)
–Clinicopathologic characteristics of AIS, MIA, and lepidic predominant ADC of the lung
–Kadota K et al: Am J Surg Pathol 2014; 38:448-60
1038 Stage I Adca
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Clinicopathologic characteristics of four recurrent cases in lepidic predominant ADC
Casesurgical
proceduretype of rec.
duration
until rec.
staple
marginstage Ly V PL
micro-
papillary
1 lobectomydistant
(bone)1.4 yrs NA IA + + 0 30
2wedge
resection
local rec.
(lung)1.1 yrs 2 mm IA + - 0 20
3wedge
resection
distant
(chest wall)3.3 yrs 5 mm IA - - 0 0
4 lobectomylocal rec.
(lung)3.8 yrs NA IA - - 0 0
–Lepidic predominant ADC with no recurrence (n=99)
– lymphatic invasion: 6% (n=6)
– vascular invasion: 4% (n=4)
– micropapillary pattern: 2% (average)
–Clinicopathologic characteristics of AIS, MIA, and lepidic predominant ADC of the lung
–Kadota K et al: Am J Surg Pathol 2014; 38:448-60
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LUNG CANCER – PART SOLID NODULES
IN NLST▪ 19 part solid nodules screen baseline dxd lung ca
▪ No LN enlargement or mets at resection
▪ Path: 18 AD (6 BAC, 1 mixed BAC, 1 acinar, 1
mucinous); 1 Squamous cell ca
▪ Stage: 1A (n=15), 1B (n=3); Multilobar stage IV
(T4N0M1) BAC dxd in one pt 25 months after study
randomization died 68 months later
▪ All 18 pts with solitary or dominant part solid
nodule underwent surgery and none died of lung ca
Yip, R et al: AJR 2017;208:1011-1021
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LUNG CANCER – PART SOLID NODULES
IN NLST▪ From randomization average time to dx was 18.6
months and average time of followup was 79.2
months
▪ Median volume doubling time was 476 days
(total) and 240 days (solid component)
▪ No pts with solitary or dominant part solid
nodule had LN enlargement or metastases at
pathology and none died of lung cancer within
followup time of NLST
Yip, R et al: AJR 2017;208:1011-1021
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GRADING OF LUNG CANCER
▪ No established grading system for lung ca
▪ Grading system for adenocarcinoma will need
to be different from squamous cell carcinoma
▪ Adenoca
• Predominant subtypes
• Two most predominant patterns
• Highest grade
• Nuclear features
• Mitotic count
–Travis W et al ERJ 47:720-23 , 2016
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PROPOSED GRADING SYSTEM FOR
SQUAMOUS CELL CARCINOMA
Travis W et al ERJ 47:720-23 , 2016 adapted from
Weichert W et al : Eur Resp J 47: 938-46, 2015
–
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SPREAD THROUGH AIR SPACES (STAS) IN INKED
MARGIN OF RESECTION
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SPREAD THROUGH AIR SPACES (STAS) IN INKED
MARGIN OF RESECTION
Kadota K et al; JTO 2015; 10:806-14
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STAS – Cumulative Incidence of
Recurrence in Limited Resections
–multivariate analysis, presence of tumor STAS remained independently associated with the risk
–of developing recurrence (hazard ratio, 3.08; P=0.014).
Multivariate analysis, presence of tumor STAS remained independently associated with the risk of recurrence (hazard ratio, 3.08; P=0.014).
Kadota K et al; JTO 2015; 10:806-14
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CLINICAL SIGNIFICANCE OF STAS
GROWING EVIDENCE▪ Adenocarcinoma (n=13)
• Kadota K et al: JTO 10: 806-814, 2015; Warth A et al: AJSP 39:793-801, 2015
• Warth A et al: AJSP 40:818-26, 2016; Onozato ML et al: AJSP 37:287-294, 2013
• Shiono S et al: Int CV Thor Surg 23:567-72, 2016
• Morimoto J et al: J Thor Cardiov Surg 152:64-72, 2016
• Dai, C. JTO 2017, 12:1052-60; Uraga H, JTO 2017; 12:1046-1051
• Sun PL et al Zhonghua Bing Li Xue Za Zhi 2017;46:303-8; Yi E et al; ANZ J Surg 2018;88:327-31
• Masai K et al: JTO 12 12:1788-1797 2017; Toyokawa G et al: ATS 2018 epub
• Terada Y et al: JTO 12 S1: S54, 2017; Nakao K et al: JTO 12 S1: S148, 2017
▪ Squamous cell carcinoma (n=3)
• Lu S et al: JTO 12:223-234, 2017
• Kadota K et al: AJSP, 2017, 41:1077-86
• Yanagawa N et al: Lung Cancer 120; 14-21, 2018
▪ Small cell carcinoma: Toyokawa G et al: Anticancer Res 38:1821-25, 2018
▪ Carcinoid
• Beasley M et al: Hum Path 31: 1255-65, 2000
▪ Non-angiogenic pattern – co-option of blood vessels
• Szabo, V J Pathol 2015; 235: 384–396
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CLASSIFICATION OF LUNG CANCER NOW
REQUIRES GENETIC TESTING
MSK-IMPACT NGD data, 2017 – now includes 468 genesCourtesy of Marc Ladanyi
–Jordan EJ Ca Discovery 7:596-609, 2017
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OVERDIAGNOSIS
IN LUNG CANCER SCREENING
▪ Pathologic features may explain favorable
outcome for the minority of lung cancers
▪ ADC - lepidic growth (AIS, MIA, LPA)
▪ Histologic grade
▪ Invasive characteristics: STAS, vascular
invasion, visceral pleural invasion
▪ Molecular characteristics (EGFR/ALK mut)
▪ Goal – less intervention for GGN/PSN
detected by screening