Solid Nodule Appearance as a Predictor of Tumor Spread Through Air Spaces in Patients with Lung Adenocarcinoma: A Propensity Score Matching Study.

OBJECTIVE: Spread through air spaces (STAS) has been reported to be an invasive histological pattern with poor prognosis in lung cancer; however, little is known about its intrinsic risk factors. This work analyzed the correlation between pathological and radiological features and STAS in resected lung adenocarcinomas. PATIENTS AND METHODS: We retrospectively reviewed 1821 consecutive surgically treated patients with histologically diagnosed lung adenocarcinoma (174 positive for STAS and 1647 negative for STAS) from December 2017 to November 2018 at our institution. Propensity score matching identified 170 well-balanced pairs of patients. The correlations between pathological and radiological features and the presence of STAS were analyzed.
RESULTS: Before propensity matching, the incidence rate of STAS was 9.6% in all patients. In matched cohorts, multivariate analysis showed that the presence of STAS was significantly correlated with pure solid nodules (SNs) (p = 0.001) and solid/micropapillary patterns (SMPs) (p = 0.002). The odds ratio for STAS in SN-positive and SMP-positive adenocarcinoma against that in SN-negative and SMP-negative adenocarcinoma was 10.922 (95% confidence interval, 5.826-20.475; p < 0.001). Tumor differentiation, visceral pleural invasion (VPI), lymphovascular invasion (LVI), invasive adenocarcinoma, and non-lepidic subtype were significantly associated with STAS in the univariate analysis (p < 0.05); however, the differences failed to reach a significant level in the multivariate analysis.
CONCLUSION: We found that STAS was significantly correlated with several invasive clinicopathological patterns. The presence of SNs and SMPs were revealed as independent predictors for STAS, which could offer clinicians clues to identify STAS-positive adenocarcinoma.

Introduction

The non-small cell lung cancer (NSCLC) still ranks the first common and the leading cause of cancer-related deaths word widely.1 As the major subtype of NSCLC, lung adenocarcinoma (ADC) presents with diverse histological patterns and molecular features. In recent decades, based on morphology, immunohistology, and molecular analyses, several clinicopathological features have been proven to be correlated with the prognosis of lung ADC, which is of vital significance in clinical therapeutic decision making.2 Tumor spread through air spaces (STAS), which is described as the spread of cancer cells into air spaces in the lung parenchyma beyond the edge of the main tumor, was first introduced by the 2015 WHO classification of lung tumors and further validated and analyzed.3 Several studies have reported the prognostic value of STAS and revealed its correlation with certain clinicopathological characteristics; thus, STAS was gradually recognized as a novel invasive pattern of ADC.4–6

However, the existence of STAS remains controversial, as some researchers consider STAS to be an artifact of tissue processing rather than an indicator of certain pathological change.7 Further comprehensive studies and accurate definitions are needed to settle this dispute concerning STAS. In addition, little is known about the radiological features and genetic mutations associated with STAS in lung ADC. Thus, we analyzed the clinicopathological features of surgically resected lung ADC with STAS to explore these intrinsic correlations.

Patients and Methods

Patient Cohort

We reviewed a large, single-institution database of patients with lung cancer in the Cancer Institute and Hospital of the Chinese Academy of Medical Sciences from December 2017 to November 2018. Our present study included patients who underwent surgical resection for lung cancer and histologically confirmed primary lung ADC. A total of 1841 consecutive patients were identified based on this selection. We excluded cases lacking complete medical records (n=3), received preoperative neoadjuvant therapy (n=12), accompanying with other malignancies or histological components (n=5). After the exclusion, 1821 patients met our criteria and enrolled in the study cohort. The criteria for patient selection and exclusion were also shown in . Patients’ demographics, pathological/radiological features, and genetic parameters were retrieved from the medical record database and analyzed.

Radiological Features

A thin-section chest computed tomography (CT) scan was conducted in all patients within one month preoperatively. Examinations were performed using 64-detector row scanners (LightSpeed VCT, Discovery CT750 HD or Optima CT660, General Electric Medical Systems; TOSHIBA Aquilion, TOSHIBA Medical Systems) at full inspiration. The CT parameters were as follows: tube voltage, 120 kVp; auto mA settings (tube current, 200–350 mA, noise index, 13; pitch, 0.992 or 0.984; rotation time, 0.5 s; thickness, 5 mm). The image was reconstructed with 1.25 mm-thick slices using a standard reconstruction algorithm. The pulmonary nodule was subclassified into three categories, namely, pure ground-glass nodules (GGNs), part-solid nodules (PSNs), and pure solid nodules (SNs), according to the proportion of the solid component. PSNs were defined as lesions with both ground-glass opacity (GGO) and a solid component.8 The nodule features of all enrolled cases were independently reviewed by a thoracic radiologist (Dr. Yang) and a thoracic surgeon (Dr. Zeng). The two reviewers were both blinded to the STAS status before analysis, and the final assessment was made through a discussion if there was a disagreement.

Histopathologic Examination

The histopathologic classification of lung ADC was according to 2015 WHO criteria, including adenocarcinoma in situ (AIS), minimally invasive adenocarcinoma (MIA), and invasive adenocarcinoma which was further classified into five subtypes (lepidic, acinar, papillary, solid, and micropapillary). The percentage of each subtype was recorded in a semiquantitative manner (in 5% increments), and the predominant pattern refers to the major component with the largest percentage. Tumors without a solid or micropapillary pattern (SMP) were defined as SMP negative, tumors containing an SMP >5% but did not have an SMP as the predominant pattern were defined as SMP minor, and those with SMP as the predominant subtype were classified as SMP predominant. The definitions of other features including tumor differentiation, visceral pleural invasion (VPI), and lymphovascular invasion (LVI) were described in the previous report.9 TNM stage was based on the American Joint Committee on Cancer (AJCC) 8th edition staging manual.10 STAS was defined as detached tumor cells within alveolar spaces that were separated from the main tumor. The pattern of STAS may be presented in the morphologic forms of single cells, micropapillary clusters, or solid nests, according to Kadota’s criteria.4 Epidermal growth factor receptor (EGFR) mutation and kirsten rat sarcoma (KRAS) mutation were analyzed through direct DNA sequencing or Mutation Detection Kit in selected cases depending on clinical needs. We reviewed these data from each patient’s postoperative pathological report, which was conducted by at least two board-certified pathologists. Besides, the hematoxylin-eosin (HE) staining sections of all enrolled cases were reviewed by another independent pathologist (Dr. Wang), who was blind to the pathological reports. The disagreements were resolved by consensus of Dr. Wang with the initial reviewers.

Propensity Score Matching

On the basis of the imbalanced sample size and potential selection bias in this nonrandomized cohort, we adopted the propensity score matching to select comparable cases from the STAS-negative group for further analysis. Propensity scores were computed as the conditional probability of the presence of STAS using a multivariable logistic regression model. Age at diagnosis, sex, smoking status, forced vital capacity (FVC)/predicted, forced expiratory volume in 1 second (FEV1)/predicted, carcinoembryonic antigen (CEA), and pathologic tumor size were included as covariates to balance the two groups. The balance in covariates was assessed by the absolute standardized mean difference (SMD) before and after matching. An SMD ≤ 0.1 indicates that the covariate between the two matched groups was well balanced.11 We performed 1:1, 1:2, and 1:3 ratio matching, and 1:1 ratio matching was chosen because it achieved the most balanced data set. Propensity score matching was performed with PSMATCHING (add-on for SPSS, version 3.04) and underlying R packages (version 3.1.0).

Statistical Analysis

Continuous variables were expressed as mean ± standard deviation (SD) or median ± range and compared using Student’s t-test or nonparametric Mann–Whitney U-test according to the normality of data. Categoric variables were presented as frequency and percentage and compared using the Chi-square test or Fisher’s exact test. A multivariate logistic regression analysis was performed to identify independent predictive factors of STAS among the correlated variables from the univariate analysis. Statistical analysis was performed using SPSS (IBM, Version 23.0, Armonk, NY, USA). A p-value < 0.05 was considered statistically significant.

Results

Propensity Score Matching results and Patient Characteristics

From December 2017 to November 2018, a total of 1821 patients (174 cases in the STAS-positive group and 1647 cases in the STAS-negative group) were enrolled into analysis, and the incidence rate of STAS was 9.6%. Before propensity score matching, the baseline variables between the two groups were unbalanced, with a mean propensity score of 0.090 for the STAS-negative group and 0.145 for the STAS-positive group (SMD = 0.554). After 1:1 propensity matching using the nearest neighbor matching algorithm (caliper = 0.05), 170 matched pairs (340 cases) were finally included in the analysis. All included covariates were well balanced (SMD < 0.01) with an equal mean propensity score of 0.137 (). For a more intuitive presentation, we also show the distribution of the propensity scores and SMDs for both groups before and after propensity matching in .

The clinical characteristics of the patients in the two groups are shown in . The mean age of all matched patients was 59.0 years (range, 31–82 years), including 148 men (43.5%) and 192 women (56.5%). Patients who never smoked (234 of 340, 68.8%) were predominant in our study. No significant differences were found between the two groups in lung cancer family history and other comorbidities before or after matching. A minority of patients (96 of 340, 28.2%) experienced abnormally elevated CEA levels and achieved balanced covariates. To achieve a better comparison of the pathological or radiological features between patients with or without STAS, tumor size was also included in the covariates. After matching, the two groups had similar tumor sizes, with a median of 2.1 cm (range, 0.5–8.5 cm).

Pathological and Radiological Features According to STAS Status

The pathological and radiological features according to STAS status are summarized in Table 1, and examples of three cases of lung ADC with STAS stratified by different CT appearances are shown in Figure 1. In terms of pathological characteristics, STAS was found to be significantly associated with tumor differentiation, VPI, and LVI (p < 0.05). Lymph nodal metastasis was observed more frequently in STAS (+) patients (29.4%, 50 of 170) than in STAS (-) patients (20.6%, 35 of 170); however, the difference between the two groups failed to reach significant level (p = 0.079). Moreover, the two groups did not differ in pathological TNM stage (p = 0.211). Similar rates of multiple primary lung lesions were found in STAS (-) and STAS (+) patients [8.8% (15 of 170) vs 10.6% (18 of 170), p = 0.715]. Notably, no AIS or MIA was found in STAS (+) patients, which was in obvious contrast to STAS (-) patients (5.3%, 9 of 170, p = 0.010). Furthermore, in terms of histological subtypes, STAS was more frequently found in solid predominant tumors (11.2%, 19 of 170, p = 0.080) and micropapillary predominant tumors (6.5%, 11 of 170, p < 0.001) but was rarely found in lepidic predominant tumors (2.4%, 4 of 170, p = 0.002). We also performed a subanalysis of SMPs between the two groups and found that 131 (77.1%) STAS (+) patients showed predominant or minor SMP, whereas only 38 (22.4%) STAS (+) patients were negative for SMPs (p < 0.001). Information on genetic mutations was available in 315 (92.6%) patients, and no significant difference was observed in either EGFR mutations or KRAS mutations between STAS (-) and STAS (+) patients (p = 0.486, p = 0.347, respectively). When the EGFR mutations were further subdivided into wild type, exon 19 deletion, exon 21 missense, or miscellaneous, no significant differences were observed (p = 0.210). In terms of radiological features, the distribution of nodule patterns differed between the two groups (p < 0.001). Only 1 (0.6%) STAS (+) patient showed a pure GGN, whereas nearly all STAS (+) tumors manifested as either SNs (81.8%, 139 of 170) or PSNs (17.6%, 30 of 170). Correspondingly, a relatively lower rate (44.1%, 75 of 170) of SN patterns was found in STAS (-) tumors.

Table 1

Comparison of Pathological Characteristics, Radiological Features, and Genetic Mutations Between STAS (-) and STAS (+) Groups After Propensity Matching

Characteristics	Matched Patients	STAS (-)	STAS (+)	P value
No. of patients	340	170	170
Tumor differentiation				<0.001a
Well Moderate/poor N/A	2628826	24 (14.1)126 (74.1)20 (11.8)	2 (1.2)162 (95.3)6 (3.5)
Bronchial involvement				0.496
Positive Negative	39301	17 (10.0)153 (90.0)	22 (12.9)148 (87.1)
VPI				0.005
Positive Negative	94246	35 (20.6)135 (79.4)	59 (34.7)111 (65.3)
LVI Positive Negative	67273	25 (14.7)145 (85.3)	42 (24.7)128 (75.3)	0.029
Lymph nodal metastasis				0.079
Yes No	85255	35 (20.6)135 (79.4)	50 (29.4)120 (70.6)
Pathological stage				0.211a
AIS I II III IV	1228455610	1 (0.6)121 (71.2)22 (12.9)21 (12.4)5 (2.9)	0107 (62.9)23 (13.5)35 (20.6)5 (2.9)
Multiple primary lesion				0.715
Yes No	33307	15 (8.8)155 (91.2)	18 (10.6)152 (89.4)
Adenocarcinoma subtypes				0.010a
AIS MIA Invasive adenocarcinoma Variants of invasive adenocarcinoma	1832110	1 (0.6)8 (4.7)156 (91.8)5 (2.9)	00165 (97.1)5 (2.9)
Predominant subtype				<0.001
Lepidic predominant Acinar predominant Papillary predominant Solid predominant Micropapillary predominant N/A	2217678291124	18 (10.6)93 (54.7)31 (18.2)10 (5.9)018 (10.6)	4 (2.4)83 (48.8)47 (27.6)19 (11.2)11 (6.5)6 (1.8)
Solid/micropapillary pattern				<0.001a
SMP negative SMP predominant SMP minor N/A	134401579	96 (56.5)10 (5.9)56 (32.9)8 (4.7)	38 (22.4)30 (17.6)101 (59.4)1 (0.6)
EGFR mutation				0.486
Positive Wild type N/A	19512025	101 (59.4)55 (32.4)14 (8.2)	94 (55.3)65 (38.2)11 (6.5)
EGFR mutation type				0.201
Wild type Exon 19 deletion Exon 21 missense Miscellaneous	120909114	55 (32.4)54 (31.8)41 (24.1)6 (3.5)	65 (38.2)36 (21.2)50 (29.4)8 (4.7)
KRAS mutation				0.347
Positive Wild type N/A	3528025	21 (12.4)135 (79.4)14 (8.2)	14 (8.2)145 (85.3)11 (6.5)
Nodule pattern				<0.001a
Pure GGN PSN SN	2799214	26 (15.3)69 (40.6)75 (44.1)	1 (0.6)30 (17.6)139 (81.8)

Note: aComparison between variables was performed using the Fisher exact test.

Abbreviations: STAS, spread through air spaces; VPI, visceral pleural invasion; LVI, lymphovascular invasion; AIS, adenocarcinoma in suit; MIA, minimally invasive adenocarcinoma; SMP, solid/micropapillary pattern; GGN, ground glass nodule; PSN, part-solid nodule; SN, solid nodule; N/A, non-applicable.

Figure 1

CT features (width, 1600 HU; level, −600 HU) and their corresponding STAS manifestations: (A) Pure GGN; (C) PSN; and (E) SN. (B, D and F) show the corresponding STAS features of the above nodules, respectively. Photomicrograph shows detached clusters of tumor cells (arrows) detached within alveolar spaces beyond the edge of the main tumor (dotted lines) by hematoxylin-eosin staining (magnification, ×100). Boxed region in (B and D) shows the high-power view of the STAS feature (magnification, ×400).

Multivariate Analysis of the Correlation Between Pathological and Radiological Features and the Presence of STAS

The multivariate logistic regression model included variables that were significant in the univariate analysis: tumor differentiation, VPI, LVI, adenocarcinoma subtype, lepidic predominant subtype, SMP, and nodule pattern. STAS was significantly correlated with SMPs and nodule patterns in the multivariate analysis (p < 0.01). As shown in Table 2, the presence of STAS showed a significant correlation with SMP-positive tumors (odds ratio [OR], 2.575; 95% confidence interval [CI], 1.412–4.696; p = 0.002) and SNs (OR, 3.223; 95% CI, 1.803–5.761; p < 0.001). However, the other included parameters failed to reach significance. When stratifying the tumors according to the SMP or nodule pattern, the frequency of STAS increased as the frequency of SMPs or solid appearances on imaging increased, both p < 0.001 (Figure 2).

Table 2

Multivariate Analysis of the Correlation of Pathological Characteristics, Radiological Features and Genetic Mutations with the Presence of STAS

	No.	STAS (+)	OR	95% CI	P value
Tumor differentiation
Well	26	2 (1.2)	1.000
Moderate/poor	288	162 (95.3)	5.451	0.915–32.484	0.063
VPI
Positive	94	59 (34.7)	1.000
Negative	246	111 (65.3)	0.750	0.432–1.301	0.306
LVI
Positive	67	42 (24.7)	1.000
Negative	273	128 (75.3)	1.200	0.643–2.237	0.567
Adenocarcinoma subtypes
Invasive adenocarcinoma	321	165 (97.1)	1.000
Others	19	5 (2.9)	0.663	0.056–7.817	0.744
Predominant subtype
Lepidic	22	4 (2.4)	1.000
Non-lepidic	294	160 (97.6)	0.565	0.129–2.479	0.449
Solid/micropapillary pattern
SMP negative	134	38 (22.4)	1.000
SMP positive	197	131 (77.1)	2.575	1.412–4.696	0.002
Patterns of nodule
Pure GGN or PSN	126	31 (18.2)	1.000
SN	214	139 (81.8)	3.223	1.803–5.761	<0.001

Abbreviations: STAS, spread through air spaces; OR, odds ratio; CI, confidence interval; SMP, solid/micropapillary pattern; GGN, ground-glass nodule; PSN, part-solid nodule; SN, solid nodule.

Figure 2

The histogram shows the relative proportions of STAS stratified by increases in solid components (A) or SMPs (B). The frequency of STAS increased in proportion with the solid components and SMPs (p < 0.001).

ORs for STAS Based on the Presence or Absence of SNs and SMPs

Additionally, we also analyzed the ORs for STAS based on the presence or absence of SNs and SMPs. In comparison with SN (-)/SMP (-) adenocarcinomas, the OR for STAS in SN (+)/SMP (-) or SN (-)/SMP (+) adenocarcinomas was 3.495 (95% CI, 1.751–6.976, p < 0.001), and the OR for STAS in SN (+)/SMP(+) adenocarcinomas was 10.922 (95% CI, 5.826–20.475, p < 0.001), as shown in Table 3 and Figure 3.

Table 3

ORs for STAS According to the Presence or Absence of SNs with SMPs

	No.	STAS (+)	OR	95% CI	P value
SN (-)/SMP (-)	27	1 (0.6)	1
SN (+)/SMP (-) or SN (-)/SMP (+)	107	37 (21.8)	3.495	1.751–6.976	< 0.001
SN (+)/SMP (+)	197	131 (77.1)	10.922	5.826–20.475	< 0.001

Abbreviations: STAS, spread through air spaces; SN, pure solid nodule; SMP, solid/micropapillary pattern; OR, odds ratio; CI, confidence interval.

Figure 3

According to the presence or absence of SNs and SMPs, the following three groups were created: the SN (-)/SMP (-) group, the SN (+)/SMP (-) or SN (-)/SMP (+) group, and the SN (+)/SMP (+) group. The ORs for STAS are shown as histograms using the SN (-)/SMP (-) group as a reference.

Discussion

In the current study, STAS was observed in 174 of 1821 (9.6%) cases of surgically resected lung ADC and was revealed to be significantly associated with certain histological characteristics, especially SMPs. In addition, a solid appearance on CT was also revealed as an independent predictive parameter for STAS in tumors. Our findings show that STAS-positive ADC suggests aggressiveness and warrants intensive management; moreover, this tumor type may be predicted with the combination of an SN appearance with a pathological SMP.

The pathological phenomenon of STAS was recently recognized and then extensively studied. Among all the published studies, the definition of STAS has slightly changed. Onozato et al12 implied tumor nests to be the criterion for STAS. Kadota et al4 subsequently broadened the definition to include cell clusters or even single cells, which were henceforth widely applied. Several studies have revealed the negative effect of STAS on prognosis. The initial two large cohorts2,4 concerning STAS in lung ADC both indicated that STAS was significantly associated with reduced overall survival. Then, several subsequent studies also confirmed the negative impact of STAS on patient survival as well as on cancer recurrence in early-stage lung ADC.13–17 Thus, as a certain invasive pattern, the significance of STAS was further acknowledged.

STAS has also been studied for its correlation with clinicopathological factors in lung ADC (). In terms of clinical characteristics, the results showed obvious heterogeneity among previous studies, as only a few reported STAS to be associated with the male sex, smoking, or elevated CEA levels.2,13,14 Hence, we first applied a propensity score matching method to balance the baseline features of enrolled patients to achieve better analysis results. Although not significant in the multivariate logistic analysis, STAS was correlated with tumor differentiation, VPI, LVI, the invasive adenocarcinoma subtype, and papillary or micropapillary predominant ADC in the univariate analysis after matching. As noninvasive subtypes, AIS and MIA have been confirmed to indicate a favorable prognosis with a 5-year survival rate near 100%.18 In our study, no STAS was found in cases of either AIS or MIA, which seems reasonable for noninvasive histological patterns. However, Toyokawa et al17 reported that the incidence of atypical adenomatous hyperplasia (AAH)/AIS/MIA subtypes in STAS-positive patients was 5.8% (11 of 191). Therefore, it appears premature to confirm that STAS is absent in noninvasive ADC subtypes. As a more aggressive histological pattern of invasive adenocarcinoma, the SMP was proven to indicate an unfavorable prognosis, even if it was not the predominant subtype.19,20 Therefore, we also investigated the difference in SMPs between the STAS (-) and STAS (+) groups. In the final multivariate analysis, the SMP was the only pathological parameter associated with STAS. The proportion of STAS (+) SMP-positive patients was significantly higher than that of STAS (+) SMP-negative patients (77.1% vs 22.4%; OR, 2.575; p = 0.002). These results are inconsistent with other previous studies concerning STAS in lung ADC.2,4,6,9,13-17,21,22 It is noteworthy that several studies also suggested that STAS was associated with a larger tumor size. Uruga et al15 revealed that in 208 cases of stage I (tumor size ≤ 2 cm) lung ADC, STAS was significantly correlated with a larger tumor size (p = 0.037). Toyokawa et al16 also revealed that STAS positivity was correlated with a pathologically larger tumor size (p = 0.004). Regretfully, both studies were based on cohorts containing early-stage lung ADC only. Warth et al2 reported that in 569 cases of stage I to IV lung ADC, the presence of STAS was associated with a higher N and M stage but not T stage. Kim et al21 reached similar results in a cohort of 316 stage I to III cases. The contradictions among those studies may be attributed to the heterogeneity of the enrolled patients, and perhaps nodal metastasis may influence the correlation between STAS and TNM stage. Hu et al9 reported that in a multivariate analysis of 500 cases of lung ADC, STAS was significantly correlated with T stage (p = 0.001) and N stage (p = 0.032). To further study the underlying pathological factors associated with STAS, we enrolled all pathological stages from AIS to stage IV tumors, and the tumor size was also balanced with propensity matching. Although significant differences existed before propensity matching, similar distributions were found for both lymph node metastasis (p = 0.079) and TNM stage (p = 0.211) between the STAS (+) and STAS (-) groups after matching. Thus, the relationships between STAS and nodal metastasis and TNM stage remain controversial and warrant further study in large cohorts.

The association between STAS and genetic features in lung ADC remains unclear due to the limited number of relevant studies and lack of adequate data. Previous studies revealed that STAS had a significant relationship with wild-type EGFR.2,6,12,13,21 In addition, two of these studies also stated that KRAS and BRAF mutations were found predominantly in STAS-positive patients.2 Although not routinely tested for, lung ADC-related driver mutations were analyzed in most surgically resected cases in our institution. We found that STAS was prone to exist in wild-type EGFR or wild-type KRAS tumors; however, the difference between the two groups failed to reach a significant level. Toyokawa et al17 also reported that the presence of STAS showed no significant association with EGFR mutations or PD-1 expression. To date, no previous studies have analyzed the detailed EGFR mutation types, so we conducted a subanalysis of different EGFR mutation types (including wild type, exon 19 deletion, exon 21 missense, and others); however, no differences were found between the two groups.

Several studies have confirmed the adverse effect of STAS on postoperative recurrence in lung ADCs treated with limited resection.4,5,16,23,24 In case of that, limited resection for STAS-positive ADCs should be cautiously considered. The detection of STAS preoperatively seems vitally important for clinicians to achieve optimal therapeutic planning. Intraoperative frozen section pathology appears to be a feasible method; however, its feasibility remains unclear. In addition to the main tumor, the non-neoplastic lung parenchyma is also required in the frozen section specimen of STAS analysis. In 2017, Kameda et al25 conducted a study evaluating STAS with frozen sections and reported satisfactory sensitivity, specificity, and accuracy (71%, 92.4%, and 80%, respectively). However, Walts et al26 reported a low sensitivity of 50% and a high specificity of 100%. In a recent propensity score-matched analysis of 698 T1 lung ADCs, Eguchi et al27 selected cases with adequate normal lung parenchyma in frozen sections to detect STAS and reported a relatively better sensitivity (71%) and specificity (92%). These findings preliminarily indicate that the detection of STAS through frozen section analysis is feasible and should be further validated in prospective studies given the sparsely available data.

In addition to intraoperative frozen section analysis, preoperative radiological features have also been revealed to be a potential predictor for STAS. Several studies have indicated that the solid appearance of a nodule on CT represents a more invasive pattern and worse prognosis than a GGN appearance.28,29 Some investigators also suggested that different percentages of solid components (calculated by the consolidation to tumor ratio, CTR) represent distinct prognoses in part-solid lung ADCs.30,31 However, in recent published studies conducted by Ye et al,32 the CTR was unable to predict the prognosis of lung ADC, and the authors suggest that part-solid lung ADC should be defined as one special clinical entity regardless of the percentage of solid components. For these reasons, we simply subclassified the nodules into pure GGNs, PSNs, and SNs. In our study, a solid nodule appearance was revealed to be an independent predictor for STAS. Similar results were reported by other researchers. Shiono et al13 first reported in their study that solid nodules on CT were significantly correlated with STAS (p = 0.032). Furthermore, Toyokawa et al17 conducted a study to analyze the detailed CT features of patients with lung ADC. They showed that the presence of notches (OR, 1.93; p = 0.01) and the absence of GGOs (OR, 0.37; p <0.01) were independently associated with the presence of STAS. To date, as a radiologist, Kim et al21 conducted the first propensity-matched study for predicting STAS in lung ADC through CT imaging. They revealed that, apart from the solid component, STAS was also significantly associated with the CT features of central low attenuation, ill-defined opacity, and air bronchogram. The researchers also found that the percentage of solid components was an independent predictor of STAS (OR, 1.06; 95% CI, 1.03–1.08) with a sensitivity of 89.2% and a specificity of 60.3%. Notably, in the study conducted by Kim et al, no STAS was found in the pure GGN cases, which is similar to our results. The rare incidence of STAS in pure GGNs highlights the minimally invasive features of GGNs.

Given that the pathological diagnosis of SMPs and radiological features of SNs were both significant predictors for the presence of STAS in lung ADC and the inconvenience and relative immature method of frozen section pathology to diagnose STAS, we then conducted a combined analysis of the presence or absence of SNs with SMPs and obtained an OR of 10.922 (95% CI, 5.826–20.475) for STAS in SN (+)/SMP (+) lung ADCs. This indicates that tumors with a pure solid appearance and SMP were approximately ten times more likely to present with STAS than tumors without either an SN or SMP. Surgeons should be aware that for SNs with SMPs according to intraoperative frozen section pathology, limited resection should be cautiously selected regardless of the tumor size due to the high probability for STAS.

To the best of our knowledge, this is the first comprehensive study to evaluate STAS with clinicopathological and radiological features of lung ADC using propensity score matching. However, several limitations still exist in this study. First, given the nature of this nonrandomized and retrospective study, certain biases may still exist even though we performed propensity score matching. Second, we enrolled ADC patients and excluded only those with squamous or small cell lung cancer, which were recently reported to be associated with the presence of STAS as well. Third, as an important feature with the strongest correlation with pathological pattern or prognosis, the solid appearance of nodules was mainly analyzed, however, further analysis was lack in the percentage of solid components in PSNs as well as other radiological features, such as air bronchograms, spiculation or calcifications. Recent studies33,34 regarding using radiomics to assess lung nodules (especially the STAS) have reported inspiring results and may offer guide for our following research. Moreover, due to the limited follow-up period, we failed to analyze the prognostic effect and related factors in this study, which warrant further evaluation. To gain a comprehensive understanding of STAS, well-designed prospective studies are needed to increase the number of cases and broaden the histological subtypes.

In conclusion, we revealed that STAS is a certain pathological entity that correlates with several invasive clinicopathological parameters, especially the pathological diagnosis of SMPs and radiological features of SNs, which may help predict the presence of STAS.