The efficacy and prognosis analysis after stereotactic body radiotherapy for multiple primary early-stage lung cancer

doi:10.19401/j.cnki.1007-3639.2023.09.005

Abstract

Abstract:

Background and purpose: More and more patients with multiple primary early-stage lung cancer are choosing to receive stereotactic body radiation therapy (SBRT), and this study aimed to retrospectively analyze the efficacy and prognostic factors of SBRT. Methods: In this study, patients who underwent SBRT at Shanghai Chest Hospital, Shanghai Jiao Tong University School of Medicine from August 2014 to December 2020 and who met the inclusion criteria were included. Patients with multiple primary early-stage lung cancer were examined for efficacy and prognostic factors. After using propensity score matching (PSM), the difference in efficacy of SBRT between single and multiple primary early-stage lung cancer was observed. Results: This study included 241 early-stage lung cancer patients with SBRT, including 94 patients with multiple primary early-stage lung cancer. The 3- and 5-year local control rate (LC), progression-free survival (PFS) and overall survival (OS) were 87.1% and 71.3%, 84.0% and 66.9%, 93.3% and 79.3% in multiple primary early-stage lung cancer, respectively. Patients with multiple primary early-stage lung cancer did not experience any grade 3 or higher pulmonary toxicity with an overall toxicity incidence of 54.3%, and grade 2 toxicity occurred in 24 patients (25.5%). There was a total of 18 (19.1%) recurrences, and there were 3 (3.2%), 1 (1.1%), 12 (12.7%) and 2 (2.1%) patients with multiple primary early-stage lung cancers who experienced local recurrence, regional recurrence, distant metastasis and uncertain death, respectively. Patients with multiple primary early-stage lung cancer and those with single primary early-stage lung cancer had significant differences in clinical features prior to PSM. After PSM, there were 56 patients with multiple primary early-stage lung cancer and 56 patients with single primary early-stage lung cancer, and there was no statistically significant difference in LC (P = 0.291), PFS (P = 0.954) and OS (P = 0.880). Age≥70 years was an independent risk factor for OS of multiple primary early-stage lung cancer, according to an analysis of the prognostic variables of SBRT in 94 patients with multiple primary early-stage lung cancer. Regarding synchronous (≤180 d) and metachronous (>180 d) multiple primary early-stage lung cancer, there was no discernible difference between the two groups (P = 0.440). There was no significant difference in the total number of treatments for multiple primary early-stage lung cancer (P = 0.232) and no significant difference in the type of treatment for multiple primary early-stage lung cancer (P = 0.225) among 59 patients with synchronous multiple primary early-stage lung cancer within 5 years of the first-to-last treatment interval. Conclusion: SBRT has a strong and comparable efficacy for multiple primary early-stage lung cancer compared with single primary early-stage lung cancer, making it a viable treatment choice. Based on age and tumor biological behavior of the lesion, future strategies and procedures for local intervention of multiple primary early-stage lung cancer need to be investigated.

Key words: Multiple primary early-stage lung cancer, Stereotactic body radiation therapy, Propensity score matching, Prognosis

CLC Number:

R734.2

WU Han, YANG Zhangru, FENG Wen, ZENG Wanqin, GUO Jindong, LI Hongxuan, WANG Changlu, WANG Jiaming, LÜ Changxing, ZHANG Qin, YU Wen, CAI Xuwei, FU Xiaolong. The efficacy and prognosis analysis after stereotactic body radiotherapy for multiple primary early-stage lung cancer[J]. China Oncology, 2023, 33(9): 844-856.

Figures/Tables 11

Fig. 1

Tab. 1

Analysis of clinical characteristics of patients before and after PSM [n （%）]"

Clinical characteristic	Before PSM			After PSM
Clinical characteristic	Single primary early-stage lung cancer (n=147)	Multiple primary early-stage lung cancer (n=94)	P value	Single primary early-stage lung cancer (n=56)	Multiple primary early-stage lung cancer (n=56)	Pvalue
Median follow-up (range)/month	33 (1-83)	44 (1-95)		32.5 (2-81)	37 (1-93)
Gender			0.001			0.686
Male	109 (74.1)	50 (53.2)		37 (66.1)	39 (69.6)
Female	38 (25.9)	44 (46.8)		19 (33.9)	17 (30.4)
Age/year			<0.001			0.344
<74	53 (36.1)	64 (68.1)		27 (48.2)	32 (57.1)
≥74	94 (63.9)	30 (31.9)		29 (51.8)	24 (42.9)
Tumor Location			0.048			0.303
Upper left	43 (29.3)	20 (21.3)		17 (30.4)	17 (30.4)
Lower left	12 (8.2)	17 (18.1)		3 (5.4)	8 (14.3)
Upper right	51 (34.7)	23 (24.5)		21 (37.5)	13 (23.2)
Middle right	11 (7.5)	11 (11.7)		5 (8.9)	8 (14.3)
Lower right	30 (20.4)	23 (24.5)		10 (17.9)	10 (17.9)
Radiotherapy dose/Gy			0.016			0.451
48	0 (0.0)	1 (1.1)		0 (0.0)	0 (0.0)
50	85 (57.8)	68 (72.3)		41 (73.2)	37 (66.1)
55	0 (0.0)	2 (2.1)		0 (0.0)	1 (1.8)
60	41 (27.9)	11 (11.7)		11 (19.6)	9 (16.1)
64	3 (2.0)	1 (1.1)		1 (1.8)	1 (1.8)
70	18 (12.2)	11 (11.7)		3 (5.4)	8 (14.3)
Radiotherapy dose fraction			0.028			0.381
4	32 (21.8)	23 (24.5)		10 (17.9)	12 (21.4)
5	53 (36.1)	43 (45.7)		30 (53.6)	24 (42.9)
8	39 (26.5)	10 (10.6)		10 (17.9)	8 (14.3)
10	23 (15.6)	18 (19.1)		6 (10.7)	12 (21.4)
BED/Gy			0.042			0.256
<105	57 (38.8)	49 (52.1)		33 (58.9)	27 (48.2)
≥105	90 (61.2)	45 (47.9)		23 (41.1)	29 (51.8)
Pathology			0.001			0.693
No	78 (53.1)	70 (74.5)		37 (66.1)	35 (62.5)
Yes	69 (46.9)	24 (25.5)		19 (33.9)	21 (37.5)
T stage			0.001			0.457
cT_is	7 (4.8)	13 (13.8)		3 (5.4)	4 (7.1)
cT_1mi	1 (0.7)	4 (4.3)		0 (0.0)	0 (0.0)
T_1a	9 (6.1)	12 (12.8)		7 (12.5)	4 (7.1)
T_1b	53 (36.1)	38 (40.4)		24 (42.9)	25 (44.6)
T_1c	41 (27.9)	20 (21.3)		15 (26.8)	17 (30.4)
T_2a	28 (19.0)	3 (3.2)		7 (12.5)	3 (5.4)
T_2b	5 (3.4)	3 (3.2)		0 (0.0)	2 (3.6)
T₃	3 (2.0)	1 (1.1)		0 (0.0)	1 (1.8)
Tumor density			<0.001			1.000
Subsolid	48 (32.7)	56 (59.6)		27 (48.2)	27 (48.2)
Solid	99 (67.3)	38 (40.4)		29 (51.8)	29 (51.8)
PET/CT			0.012			0.841
No	51 (34.7)	48 (51.1)		18 (32.1)	19 (33.9)
Yes	96 (65.3)	46 (48.9)		38 (67.9)	37 (66.1)
Underlying disease			0.394			0.850
No	56 (38.1)	41 (43.6)		26 (46.4)	27 (48.2)
Yes	91 (61.9)	53 (56.4)		30 (53.6)	29 (51.8)
Smoking status			0.071			0.847
No	88 (59.9)	67 (71.3)		34 (60.7)	33 (58.9)
Yes	59 (40.1)	27 (28.7)		22 (39.3)	23 (41.1)
Family history of tumors			0.010			0.219
No	130 (88.4)	75 (79.8)		49 (87.5)	44 (78.6)
Family history of lung cancer	8 (5.4)	16 (17.0)		4 (7.1)	10 (17.9)
Family history of other tumors	9 (6.1)	3 (3.2)		3 (5.4)	2 (3.6)
Occupational exposure			0.146			0.568
No	134 (91.2)	80 (85.1)		50 (89.3)	48 (85.7)
Yes	13 (8.8)	14 (14.9)		6 (10.7)	8 (14.3)
ECOG performance status			0.212			0.590
0	45 (30.6)	24 (25.5)		20 (35.7)	15 (26.8)
1	91 (61.9)	67 (71.3)		34 (60.7)	39 (69.6)
2	11 (7.5)	3 (3.2)		2 (3.6)	2 (3.6)
Indications for surgery			0.001			0.333
No	46 (31.3)	11 (11.7)		9 (16.1)	11 (19.6)
Yes	3 (2.0)	0 (0.0)		2 (3.6)	0 (0.0)
Uncertain	98 (66.7)	83 (88.3)		45 (80.4)	45 (80.4)

Tab. 1

Tab. 2

Fig.2

Fig. 3

Tab. 3

Univariate and multifactorial analysis of prognosis of 94 cases of multiple primary early-stage lung cancer"

Clinical characteristic	Multiple primary early-stage lung cancer n (%)	Univariate analysis			Multivariable analysis
Clinical characteristic	Multiple primary early-stage lung cancer n (%)	HR	95% CI	P value (OS)	HR	95% CI	P value (OS)
Median follow-up (range)/month	63.5 (19-170)
Gender		0.186	0.041-0.842	0.015	0.356	0.063-2.003	0.241
Male	50 (53.2)
Female	44 (46.8)
Age/year		6.142	1.359-27.761	0.007	6.180	1.263-30.249	0.025
<70	46 (48.9)
≥70	48 (51.1)
Tumor location		2.686	0.589-12.257	0.185
Ipsilateral	27 (28.7)
Bilateral	67 (71.3)
Average BED/Gy		0.918	0.304-2.777	0.880
<105	46 (48.9)
≥105	48 (51.1)
Highest T stage		1.532	0.906-2.592	0.003	1.515	0.876-2.618	0.137
cT_1mi	1 (1.1)
T_1a	8 (8.5)
T_1b	36 (38.3)
T_1c	25 (26.6)
T_2a	19 (20.2)
T_2b	3 (3.2)
T₃	2 (2.1)
Underlying disease		0.884	0.295-2.655	0.827
No	41 (43.6)
Yes	53 (56.4)
Smoking status		3.504	1.068-11.499	0.027	2.263	0.590-8.679	0.234
No	67 (71.3)
Yes	27 (28.7)
Family history of tumors		0.412	0.066-2.550	0.581
No	75 (79.8)
Family history of lung cancer	16 (17.0)
Family history of other tumors	3 (3.2)
Occupational exposure		0.039	0.000-35.941	0.145
No	80 (85.1)
Yes	14 (14.9)
ECOG performance status		1.551	0.509-4.722	0.743
0	24 (25.5)
1	67 (71.3)
2	3 (3.2)
Clinical diagnosis before the first treatment		0.619	0.181-2.110	0.440
Synchronous (≤180 d)	65 (69.1)
Metachronous (>180 d)	29 (30.9)
Total number of treatments in multiple primary early-stage lung cancer		0.237	0.065-0.862	0.019	0.393	0.104-1.492	0.170
1	24 (25.5)
≥2	70 (74.5)
Type of treatment				-			-
Single SBRT in Single primary early-stage lung cancer	24 (25.5)
Treatment in multiple primary early-stage lung cancer
SBRT only	15 (16.0)
Surgery+SBRT	55 (58.5)
First-last treatment interval				-			-
No other local treatment after SBRT	24 (25.5)
≤1 year	17 (18.1)
>1 year, ≤3 years	16 (17.0)
>3 years, ≤5 years	17 (18.1)
>5 years	20 (21.3)

Tab. 3

Fig. 4

Fig. 5

Tab. 4

Fig. 6

Fig.7

References 28

[1]	SIEGEL R, MA J M, ZOU Z H, et al. Cancer statistics, 2014[J]. CA A Cancer J Clin, 2014, 64(1): 9-29. doi: 10.3322/caac.v64.1
[2]	ZENG H M, RAN X H, AN L, et al. Disparities in stage at diagnosis for five common cancers in China: a multicentre, hospital-based, observational study[J]. Lancet Public Health, 2021, 6(12): e877-e887. doi: 10.1016/S2468-2667(21)00157-2 pmid: 34838194
[3]	OUDKERK M, LIU S Y, HEUVELMANS M A, et al. Lung cancer LDCT screening and mortality reduction-evidence, pitfalls and future perspectives[J]. Nat Rev Clin Oncol, 2021, 18(3): 135-151.
[4]	MURPHY S J, AUBRY M C, HARRIS F R, et al. Identification of independent primary tumors and intrapulmonary metastases using DNA rearrangements in non-small cell lung cancer[J]. J Clin Oncol, 2014, 32(36): 4050-4058. doi: 10.1200/JCO.2014.56.7644
[5]	CHANG Y L, WU C T, LIN S C, et al. Clonality and prognostic implications of p53 and epidermal growth factor receptor somatic aberrations in multiple primary lung cancers[J]. Clin Cancer Res, 2007, 13(1): 52-58. doi: 10.1158/1078-0432.CCR-06-1743
[6]	BATTAFARANO R J, MEYERS B F, GUTHRIE T J, et al. Surgical resection of multifocal non-small cell lung cancer is associated with prolonged survival[J]. Ann Thorac Surg, 2002, 74(4): 988-993;discussion 993-994. doi: 10.1016/s0003-4975(02)03878-x pmid: 12400733
[7]	ZUIN A, ANDRIOLO L G, MARULLI G, et al. Is lobectomy really more effective than sublobar resection in the surgical treatment of second primary lung cancer?[J]. Eur J Cardiothorac Surg, 2013, 44(2): e120-e125;discussione125. doi: 10.1093/ejcts/ezt219
[8]	STELLA F, LUCIANO G, DELL’AMORE A, et al. Pulmonary metastases from NSCLC and MPLC (multiple primary lung cancers): management and outcome in a single centre experience[J]. Heart Lung Circ, 2016, 25(2): 191-195. doi: 10.1016/j.hlc.2015.07.016 pmid: 26525847
[9]	MASCALCHI M, COMIN C E, BERTELLI E, et al. Screen-detected multiple primary lung cancers in the ITALUNG trial[J]. J Thorac Dis, 2018, 10(2): 1058-1066. doi: 10.21037/jtd.2018.01.95 pmid: 29607181
[10]	ZHAO L S, LIU C Y, XIE G Y, et al. Multiple primary lung cancers: a new challenge in the era of precision medicine[J]. Cancer Manag Res, 2020, 12: 10361-10374. doi: 10.2147/CMAR.S268081 pmid: 33116891
[11]	BOYLE J M, TANDBERG D J, CHINO J P, et al. Smoking history predicts for increased risk of second primary lung cancer: a comprehensive analysis[J]. Cancer, 2015, 121(4): 598-604. doi: 10.1002/cncr.29095 pmid: 25283893
[12]	HOWINGTON J A, BLUM M G, CHANG A C, et al. Treatment of stage Ⅰ and Ⅱ non-small cell lung cancer: diagnosis and management of lung cancer, 3rd ed: American College of Chest Physicians evidence-based clinical practice guidelines[J]. Chest, 2013, 143(5 Suppl): e278S-e313S. doi: 10.1378/chest.12-2359
[13]	WALLER D A. Surgical management of lung cancer with multiple lesions: implication of the new recommendations of the 8th edition of the TNM classification for lung cancer[J]. J Thorac Dis, 2018, 10(Suppl 22): S2686-S2691. doi: 10.21037/jtd
[14]	HAMAJI M, ALI S O, BURT B M. A meta-analysis of resected metachronous second non-small cell lung cancer[J]. Ann Thorac Surg, 2015, 99(4): 1470-1478. doi: 10.1016/j.athoracsur.2014.11.033 pmid: 25725930
[15]	DALWADI S M, SZEJA S S, BERNICKER E H, et al. Practice patterns and outcomes in elderly stage Ⅰ non-small-cell lung cancer: a 2004 to 2012 SEER analysis[J]. Clin Lung Cancer, 2018, 19(2): e269-e276. doi: 10.1016/j.cllc.2017.11.004
[16]	DETTERBECK F C, BOFFA D J, KIM A W, et al. The Eighth Edition Lung Cancer Stage Classification[J]. Chest, 2017, 151(1): 193-203. doi: S0012-3692(16)60780-8 pmid: 27780786
[17]	VIDETIC G M, PAULUS R, SINGH A K, et al. Long-term follow-up on NRG oncology RTOG 0915 (NCCTG N0927): a randomized phase 2 study comparing 2 stereotactic body radiation therapy schedules for medically inoperable patients with stage Ⅰ peripheral non-small cell lung cancer[J]. Int J Radiat Oncol Biol Phys, 2019, 103(5): 1077-1084. doi: 10.1016/j.ijrobp.2018.11.051
[18]	CHI A, WEN S J, LIAO Z X, et al. What would be the most appropriate α/β ratio in the setting of stereotactic body radiation therapy for early stage non-small cell lung cancer[J]. Biomed Res Int, 2013, 2013: 391021.
[19]	Department of Health and Human Services. Common Terminology Criteria for Adverse Events (CTCAE) version 5.0[R]. Bethesda: NIH, 2017.
[20]	SHIN J Y, YOON J K, MARWAHA G. Progress in the treatment and outcomes for early-stage non-small cell lung cancer[J]. Lung, 2018, 196(3): 351-358. doi: 10.1007/s00408-018-0110-1 pmid: 29550987
[21]	TURNER K, BROWNSTEIN N C, THOMPSON Z, et al. Longitudinal patient-reported outcomes and survival among early-stage non-small cell lung cancer patients receiving stereotactic body radiotherapy[J]. Radiother Oncol, 2022, 167: 116-121. doi: 10.1016/j.radonc.2021.12.021
[22]	GULSTENE S, RUWANPURA T, PALMA D, et al. Stereotactic ablative radiotherapy in the treatment of early-stage lung cancer-A done deal?[J]. Clin Oncol (R Coll Radiol), 2022, 34(11): 733-740. doi: 10.1016/j.clon.2022.08.027
[23]	CHANG J Y, SENAN S, PAUL M A, et al. Stereotactic ablative radiotherapy versus lobectomy for operable stage Ⅰ non-small-cell lung cancer: a pooled analysis of two randomised trials[J]. Lancet Oncol, 2015, 16(6): 630-637. doi: 10.1016/S1470-2045(15)70168-3
[24]	RAJU S C, PETERS G W, DECKER R H, et al. Clinical outcomes and safety profile in the treatment of synchronous nonmetastatic lung tumors with stereotactic body radiation therapy[J]. Pract Radiat Oncol, 2022, 12(2): e110-e116. doi: 10.1016/j.prro.2021.11.006
[25]	STEBER C R, HUGHES R T, SOIKE M H, et al. Stereotactic body radiotherapy for synchronous early stage non-small cell lung cancer[J]. Acta Oncol, 2021, 60(5): 605-612. doi: 10.1080/0284186X.2021.1892182
[26]	NIKITAS J, DEWEES T, REHMAN S, et al. Stereotactic body radiotherapy for early-stage multiple primary lung cancers[J]. Clin Lung Cancer, 2019, 20(2): 107-116. doi: S1525-7304(18)30294-8 pmid: 30477740
[27]	VERSTEGEN N E, LAGERWAARD F J, HASHEMI S M, et al. Patterns of disease recurrence after SABR for early stage non-small-cell lung cancer: optimizing follow-up schedules for salvage therapy[J]. J Thorac Oncol, 2015, 10(8): 1195-1200. doi: 10.1097/JTO.0000000000000576 pmid: 26200274
[28]	MIYAZAKI T, YAMAZAKI T, SATO S, et al. Surgery or stereotactic body radiotherapy for metachronous primary lung cancer? a propensity score matching analysis[J]. Gen Thorac Cardiovasc Surg, 2020, 68(11): 1305-1311. doi: 10.1007/s11748-020-01394-3

Number of lesions	Follow-up/year	Before PSM			After PSM
Number of lesions	Follow-up/year	LC	PFS	OS	LC	PFS	OS
Single primary early-stage lung cancer	1	91.4	88.8	95.1	96.3	92.7	94.5
	3	80.3	71.6	83.0	87.8	77.4	83.8
	5	70.9	51.8	59.6	87.8	63.5	65.2
Multiple primary early-stage lung cancer	1	93.5	91.4	96.8	90.8	87.3	94.6
	3	87.1	84.0	93.3	83.6	78.5	88.7
	5	71.3	66.9	79.3	70.1	62.5	72.7