Spanish Lung Cancer Group SCAT trial: surgical audit to lymph node assessment based on IASLC recommendations
Introduction
Surgical resection is the standard treatment with curative purpose for early stage non-small cell lung cancer (NSCLC). However, published 5-year survival rates following complete resection (CR) range between 63% in stage IA and 19% in stage IIIA (1). Chemotherapy (ChT) and/or radiation (RT) are added to improve survival for patients with operable NSCLC. Adjuvant ChT seems to offer an overall absolute benefit of 4–5% (2-4). The Spanish Lung Cancer Group (SLCG) developed the Spanish Customized Adjuvant Therapy (SCAT) trial, a multicenter trial in which 500 completely resected p-stage II-IIIA NSCLC patients were randomized to receive standard adjuvant ChT or, in the experimental arm, three different therapeutic schemes based on levels of tumor BRCA1 expression (SLCG-SCAT trial) (5).
CR is a common inclusion condition in most trials analyzing adjuvant treatment. The International Association for the Study of Lung Cancer (IASLC) proposed in 2005 a definition of CR for NSCLC (6). Systematic nodal dissection (ND) or lobe-specific nodal dissection (LSND) are widely recommended, the latter implying dissection and histological examination of intrapulmonary (regions 11 and following) and hilar (region 10) nodes and at least, three N2 regions depending on lobar location of the primary tumor. Analysis of regions 7 and 10 is mandatory regardless tumor location. Minimal number of resected lymph nodes is 3 from N1 and N2 regions.
In this study we performed a surgical audit of patients from the SLCG-SCAT trial database. Our main objective was the assessment of CR criteria, with an in-depth analysis of quality of lymphadenectomy. We also analyzed the pattern of tumor lymphatic widespread according to location and histologic subtype, and the prognostic role of different patterns of hilar and mediastinal involvement.
We present the following article in accordance with the STROBE reporting checklist (available at: http://dx.doi.org/10.21037/tlcr-20-1055).
Methods
SCAT-SLCG trial consisted of a phase III multicenter prospective randomized trial including patients with CR of clinical N0 NSCLC with incidental pathological hilar and/or ipsilateral mediastinal lymph node involvement (pN1/pN2). Patients were operated on between July 2007 and May 2013. Additional inclusion criteria included: Karnofsky index (KI) >70, completely recovered from surgery within 6 weeks, no prior RT or ChT, age >18 years and signed informed consent. Previous oncological disease within five years before surgery or neoadjuvant ChT and/or RT were exclusion criteria. Patients were randomized into two groups: patients in the control arm received adjuvant treatment with docetaxel-cisplatin while those in the experimental arm received gemcitabine-cisplatin, docetaxel-cisplatin or docetaxel depending on tumor BRCA1 expression level. Stratification factors were N1 vs. N2, histology (squamous/non-squamous), extent of resection (lobectomy vs. pneumonectomy) and BRCA1 levels and quartile distribution. Primary endpoint was disease-free survival (DFS). Secondary endpoints were survival, toxicity profiles and recurrence pattern. Statistical hypothesis: randomization 1:3 (control/experimental arms); accrual: 432 patients; 5-year survival rate 45% for the control group, with an absolute improvement of 20% in the experimental group; 80% powered; two-sided type I error of 5%; and anticipated loss of 10% cases.
Patients from SLCG-SCAT trial in whom a complete pathologic report with information about hilar and mediastinal lymph node dissection (LND) was available were included for our study. We retrospectively analyzed information prospectively collected on the tumor (location, stage, histological classification), type of resection, and postoperative morbidity and mortality (30 and 90 days), and collected a large amount of data related to LND (including number of lymph nodes assessed and involved by tumor in each intrapulmonary, hilar and mediastinal region). For the design of database, surgeons from the SLCG actively participated, in order to standardize terminology and variables amenable to be analyzed. IASLC hilar and mediastinal classification was used to properly name lymph node regions.
Statistical analysis
Student t-test was used to compare independent means. Finally, we analyzed estimated overall survival (OS) and DFS from date of surgery using Kaplan-Meier curves. Multiple comparisons of survival curves were performed using Benjamini-Hochberg-Yekutieli correction. Univariate analysis to identify survival-related factors was performed using Cox regression test. All patients underwent surgical resection in high-volume departments of thoracic surgery by surgeons with expertise in oncological procedures.
Ethical statement
The study was conducted in accordance with the Declaration of Helsinki (as revised in 2013). The study was approved by institutional/regional/national ethics/committee/ethics board of every hospital participating in the trial (2007-000067-15) and informed consent was taken from all the patients.
Results
Lymph node assessment
A total of 500 patients were included in the SLCG-SCAT trial. Complete pathologic report was available in 451 (90.2%) of the whole series. Anatomic and pathological data are summarized in Table 1. Table 2 provides information on the analysis and involvement of lymph nodes from different regions (level 1 to 14). On the whole series, in 33.7% of cases region 7 was not assessed, while in 17.7% region 10 was not evaluated. Only 3.5% of patients had no N1 regions biopsied. However, interlobar region (number 11) was not evaluated in 49.9% of patients.
Full table
Full table
As we can see in Tables S1,S2, in 19.6% of patients less than six lymph nodes were assessed, tearing up one of the main criteria of quality of LND. Mean number of mediastinal regions assessed was 3.82 (range, 1 to 10). In 21.1% of patients, lymph nodes from only one or two regions were obtained.
When we analyzed separately N1 and N2 regions, we found that in 53.4% of patients only one N1 region was assessed. The mean number of N1 lymph nodes analyzed was 5.78, with a median of 5 (range, 0–24).
Regarding N2 regions, a median of 2 stations were analyzed (range, 0 to 7). In 42 patients (9.3%) no N2 regions were assessed. In 47.9% of patients, at least three N2 regions were biopsied, which is a mandatory IASLC criterion for considering CR. A median of five N2 lymph nodes were resected (range, 0–28).
In terms of tumor-positive regions and lymph nodes, we found that 304 patients (67.4%) had one station involved, and 203 patients (45%) had only one lymph node affected. A total of 272 patients (60.3%) had only N1 disease, while 75 patients (16.6%) presented only N2 involvement (skip metastases). However, 16 patients without N1 regions assessed had N2 involvement (i.e., 21% of patients considered as having skip metastases had no N1 regions evaluated). When reviewing 179 patients with N2 involvement, we found that 16 (8.9%) had no N1 regions biopsied, 98 (54.7%) had only one and 65 (36.4%) had two or more regions analyzed.
Of 272 patients with N1 disease only, 246 (90.4%) had only one N1 region affected. Furthermore, of 75 patients with N2 involvement only, 58 (77.3%) presented single-station disease. We also found that of 409 patients with any N2 lymph node resected, N2 was the highest region involved in 120 (29.3%) of them.
The absolute number of lymph nodes resected was higher among patients undergoing pneumonectomy than in those undergoing lobectomies or bilobectomy (mean 13 vs. 11.5 lymph nodes, P=0.03). Likewise, both the number of regions and lymph nodes affected were higher for adenocarcinomas (P<0.05).
No differences were found regarding type of resection, histology and T-stage between patients with only N1, only N2 and N1+N2 disease. However, both the number of mediastinal regions assessed and affected, and the number of lymph nodes resected and affected were significantly higher in patients with N1+N2 disease than those with solely N1 or N2 involvement. Moreover, the more number of lymph nodes assessed, the higher rate of N1+N2 disease.
Next, we analyzed distribution of mediastinal regions assessed and involved regarding location of primary tumor (Tables S1,S2). We found different patterns of lymph nodes dissection. For example, for tumors in the right upper lobe (n=126), we found that regions 2R, 4R, 7 and 11R were assessed in 20.6%, 69.9%, 67.5% and 47.6% of patients, respectively. Similarly, for tumors located in the left lower lobe (n=78), at least one lymph node from regions 5, 6, 7 and 10 L was resected in 14.1%, 23.1%, 65.4% and 80.8% of patients, respectively. The pattern of lymph node region involvement regarding the location of primary tumor offers useful information about unsteady loco-regional spread of lung cancer.
Surgical morbidity and mortality
Morbidity rate was 27.7% (125 patients), being air leak (5.1%) and arrhythmias (3.8%), the complications most frequently described. Given that mortality within six weeks after surgery was an exclusion criterion, we do not have 30-day mortality rate. However, the 42- to 90-day mortality rate was 1.8% (8 patients, 3 of them due to sudden death).
OS
Median follow-up was 52.3 months. A total of 212 patients (47%) died during the follow-up. Figure 1 shows the OS curves for the whole series (Figure 1A) and divided according to N1 and/or N2 involvement (Figure 1B). Median OS was 79.3 months (95% CI: 63.7–106.4 months). Two-year OS was 76.7% (95% CI: 72.4–80.3%). Five-year OS was 55.7% (95% CI: 50.8–60.3%). Differences were found in OS regarding type of lymph node involvement (N1, N2 or both). When analyzing these groups in pairs, differences were found only between N1+N2 involvement and N1 disease only. The outcome of patients with skip metastases was similar to those with N1 and N2 disease. Median survival was 42.7 and 65.2 months for patients with N1+N2 and N2 only disease, respectively. Median was not reached among patients with only N1 involvement. Five-year OS for the three groups was 61.7% (95% CI: 55.4–67.4%), 51.5% (95% CI: 39.2–62.4%) and 42.3% (95% CI: 32.1–52.2%) for patients with N1, N2 and N1+N2 disease, respectively (P=0.02). Among patients with one or more N2 regions biopsied, no differences were found in survival in terms of the total number of N2 regions evaluated (P=0.97). Similarly, among patients with at least one N1 regions biopsied, number of regions did not affect OS (P=0.25). Table 3 shows the univariate model using Cox regression to evaluate the impact of pathological factors on OS. The number of mediastinal regions assessed did not affect OS. Patients with more than eight lymph nodes resected showed significant better overall survival (P=0.03). Both the number of regions involved and the number of tumor-positive lymph nodes were significantly related to a worse prognosis. Likewise, multistation N2 disease indicated a poor prognosis, with a hazard ratio (HR) of 2.16 (1.41–3.32: P<0.001). Type of resection did not appear to affect prognosis. Histology other than adenocarcinoma and squamous disease (30 cases) had a better prognosis (P=0.03).
Full table
DFS
Median DFS was 36.6 months (95% CI: 26.7–45.8). Two- and five-year DFS was 58.1% (95% CI: 53.3–62.5%) and 41.3% (95% CI: 36.6–45.8%), respectively. During the follow-up, 222 patients (49.2%) experienced disease relapse, being lung, lymph nodes and bone the most frequent foci of progression. In 148 cases (66.7%) progression involved a single site. No major differences were found in the pattern of progression regarding lymph node involvement. However, tumors with only N1 involvement showed significantly higher lymph node progression than those with only N2 or N1+N2 disease.
Figure 2 shows DFS curves for the whole series (Figure 2A) and for the three groups with N1, N2 and N1+N2 disease (Figure 2B). As in OS, significant differences were found between patients with N1+N2 disease and those with N1 involvement only. No significant differences were found in other comparisons between groups. Median DFS was 44.6, 38.1 and 24.7 months for patients with N1, N2 and N1+N2 disease, respectively. Five-year DFS was 45.8% (95% CI: 39.7–51.6%) for N1, 40.1% (95% CI: 28.8–51.1%) for N2 and 30% (95% CI: 21.2–39.3%) for N1+N2.
Table 4 shows the univariate model using Cox regression to evaluate the impact of pathological factors on DFS. Number of mediastinal regions assessed did not affect OS. The number of lymph nodes resected was significantly associated with worse DFS (P=0.018). Again three or more regions involved and three or more lymph nodes with tumor associated worse prognosis in terms of DFS. Again, multistation N2 was associated with worse DFS, with an HR of 1.65 (1.41–2.46; P=0.013). Pneumonectomy was associated with better DFS rates with an HR of 0.38 (0.20–0.72; P=0.002). Finally, squamous cell carcinoma and other histological subtypes had worse prognosis in terms of DFS compared to adenocarcinoma (P=0.02).
Full table
Discussion
Surgery still remains the most effective treatment with curative purpose for early-stage (IA-IIB) and selected cases of stage III NSCLC. Adjuvant therapy attempts to eradicate the remaining cancer cells in a subset of resected patients in order to achieve cure in a higher number of cases. However, it is difficult to predict who will benefit from adjuvant treatment.
Careful pathological staging is mandatory to better predict prognosis, facilitate patient selection for adjuvant regimen, avoid biases and permit proper comparisons of treatment outcomes among trials (7).
The standard surgical approach to resectable early-stage NSCLC is anatomical resection and mediastinal LND. Types of anatomic resection (typical segmentectomy, lobectomy, bilobectomy or pneumonectomy) are well defined. However, the approach to mediastinal surgical staging is rarely established when designing trials.
Most important randomized studies evaluating the role of ChT in surgical series are imprecise when defining eligibility criteria with respect to mediastinal LND (2,4,8,9).
The next two steps in the evaluation of the role of adjuvant ChT were the selection of the subset of patients who may benefit more, and the selection of targeted therapies according to patient and tumor characteristics. In this respect, the SLCG developed the SCAT Ph III trial, assessing the role of adjuvant ChT based on BRCA1 levels in NSCLC node-positive resected patients, under the hypothesis that analysis of the expression of the genes involved in DNA repair could be used to individualize optimal ChT drugs and regimens. Patients undergoing R0 major resection (lobectomy/pneumonectomy) of NSCLC with pathological N1 and/or N2 nodal status were included. Detailed information regarding the surgical lymph node approach was available in 90.2% of patients. Insufficient data was available for 49 patients included for the analysis of the main trial endpoint (targeted adjuvant treatment regimens). The first idea to bear in mind is that the trial analyzed a cohort of patients with preoperative unsuspected pathological N disease in which LND demonstrated this involvement. Homogeneous algorithms of preoperatory mediastinal staging were not mandatory for the inclusion of patients. Thus, some patients included could have not been properly staged preoperatively so that they could be amenable to received neoadjuvant treatment. The ability of surgeons to identify N disease among patients with clinical N0 NSCLC cannot be evaluated here. LND among patients of our series had enough quality to detect N disease.
The IASLC has established minimum recommendations regarding surgical evaluation of lymph node involvement in NSCL (6). Rates of attainment of these recommendations define nodal staging quality. Analysis of large databases from different countries and groups are discouraging: 50% of resections for NSCLC did not include N2 lymph nodes (10,11). Up to nearly 20% failed to examine any lymph node (12). Up to 20% showed no N1 regions assessed (13) and pN0 patients did not accomplish the minimum criteria for mediastinal assessment (14). In our series, if we focus on lymph node stations whose evaluation is fully recommended, we find that 33.7% and 17.7% of regions 7 and 10 respectively, were not assessed. Furthermore, 15.4% of patients with N1 involvement only had no N2 regions biopsied, and 20.2% had only one N2 region evaluated. Finally, in less than half of the patients three or more N2 regions were assessed, as recommended.
The role of surgical mediastinal lymph node assessment has been widely analyzed in early-stage NSCLC. Data suggest that the higher the number of lymph nodes evaluated, the better the survival outcomes (15). However, among patients with hilar and/or mediastinal pathologic lymph node involvement, the focus moves to the role of adjuvant therapies, regardless of the extension of lymph node disease. Beyond N1 (stage II) or N2 (stage IIIA) disease, further classifications have been proposed for pathological N-positive NSCLC. Legras et al. [2014] analyzed patients with NSCLC undergoing curative resection with complete mediastinal LND in two French centers over 29 years. Among pN2 patients, the combination of N1 involvement and number of involved N2 stations were independent prognostic factors (16). Zheng et al. [2011] reappraised N2 disease and found differences in survival regarding lymphatic drainage pattern (17). Finally, Yoo et al. [2015] found that the number of pathologic lymph nodes involved was an independent prognostic factor for OS and DFS among patients with IIIA-N2 NSCLC undergoing CR (18). In our series, survival differences were found when comparing N1 versus N1+N2 disease. The role of the type of LND as a confounding factor should be assessed in clinical trials evaluating outcomes of patients undergoing surgery for NSCLC. In this respect, Smeltzer et al. [2018] analyzed more than two thousand patients undergoing surgical resection for NSCLC and detected different patterns of LND, demonstrating that the prognostic value of pN stratification depends on the thoroughness of examination (19). The authors recommended that future updates of TNM staging system should include more quality restraints.
The role of skip metastases (i.e., N2 involvement without N1 disease) has also been widely analyzed. Yazgan et al. [2018] found similar survival rates among patients with N1 disease and single-station N2 disease without N1 involvement (20). The analysis of information from the IASLC database led it to recommend the recording of the number of metastatic lymph nodes (or stations) and to further classify the N category using a new proposal of N1 and N2 sub-classification (21). Even the examination of regions 13 and 14 (only available in the surgical specimen) seems to play a role in better selection of N-positive patients and probably in survival itself (22). In our series, 75 patients (16.6%) were presented as having only N2 involvement. However, when analyzed in detail, 16 of these patients we could consider having skip metastases (21%) had no N1 regions evaluated. Furthermore, when reviewing 179 patients with N2 involvement, we found that 16 (8.9%) had no N1 regions biopsied, 98 (54.7%) had only one and 65 (36.4%) had two or more regions analyzed. Thus, we consider that N1 lymph node assessment in particular was suboptimal in our study. Interlobar region is the most proximal station that is usually biopsied separately from the surgical specimen when the surgeon performs a lobectomy. Stations 12 to 14 are intrapulmonary, so they are completely resected with the lobe, being frequently identified by the pathologist in the lab. Therefore, lymph nodes from region 11 are sometimes considered a type of sentinel node. Moreover, for many authors, assessment of region 11 and detection of lymph node involvement at this level could even explain the better results of lobectomy over sublobar resections (23). In our series, in nearly half of the patients (49.8%) region 11 was not assessed.
As we have seen, another IASLC requirement for a surgical CR is the absence of tumor in the highest resected lymph node (6). Moreover, IASLC recommends the isolation and specific labelling of the highest resected lymph node. Despite this is a factor usually overlooked when analyzing survival in resected NSCLC, it has been properly validated (24). In our series, nearly 30% of 409 patients with any N2 lymph node resected showed involvement of the highest region removed.
In our univariate model, the number of mediastinal regions evaluated did not affect OS. The number of resected lymph nodes was associated with a better prognosis but did not reach statistical significance. The number of regions and lymph nodes involved was associated with lower OS rates. Combined N1-positive and one N2 region affected had an HR of 1.49 (P=0.026). The HR for N1 and more than one mediastinal region affected increased to 3.101 (P<0.001). However, in our series, N2 involvement with negative N1 (skip metastases) did not affect OS. A major limitation of this finding is the aforementioned rate of “false-skip metastases”. Furthermore, our cohort of patients is different from most studies analyzing mediastinal LND, provided that pN0 patients are usually included, being in many cases the target of those studies.
In our series mediastinal regions examined for location of the primary tumor did not follow international recommendations with respect to lobe-specific mediastinal LND. The heterogeneous pattern of disease spread found in our study is consistent with that of Liang et al. [2018] showing that, among pN2 patients, each mediastinal region can be involved in more than 5% of cases, and advocating systematic mediastinal LND as the preferred procedure for surgical mediastinal evaluation (25).
Two frequently underestimated cornerstones when defining lymph node regions are surgical and pathological issues. A well-defined and widely accepted mediastinal lymphatic map is based on radiological static anatomic landmarks. Boundaries in the surgical field are not so precise, provided that tissue mobilization during dissection shifts lymph nodes. Moreover, mediastinal tissue extends as a continuous network without well-defined boundaries. With respect to the pathological approach, no universal criteria for measuring the quality of lymph node examination quality are available. Management and labeling of samples are not always standardized. Interventions aimed at surgical and pathology teams have proven to improve the quality of nodal staging of NSCLC (26). Interesting findings in our series are those related to N1 evaluation. The highest number of lymph nodes obtained was from region 10 (median 4.64). Anatomic landmarks in this region are limited. The gap between region 11 and region 4R (right side) and 5 (left side) in which 10 lymph nodes are located is, in the surgeon’s eyes, quite small (when compared to other N1 and N2 regions). Another noteworthy finding is that region 12 was only assessed (usually once the specimen had been excised) in 9% of resections. However, a mean of 4.4 lymph nodes were separated and almost 30% of them were positive, suggesting that the more accurately the specimen is managed, the more information that may be obtained. Even sublobar node collection (regions 13 and 14) has been proven to be a prognostic factor for completely resected pN0 cases (22).
Another major limitation when analyzing a surgical series is the fact that postoperative mortality cannot be evaluated. Only patients with a good clinical status and having properly completed adjuvant treatment after six weeks were included. Even for surgical series, the trial design usually focuses on oncological aspects more than surgical issues that could work as confounding factors when evaluating outcomes. In our series, rate of pneumonectomies was 25.5%. A 30-day mortality rate for pneumonectomy of 5–20% has been classically reported in the literature and thus we consider it an important confounding bias. A significant morbidity rate of 27.7% has been reported in the literature. Furthermore, eight patients died between days 42 (6 weeks) and 90, a period within which first cycle of adjuvant ChT is usually administered. We think that the presence of three cases of sudden death requires additional investigation.
OS and DFS rates were similar to other comparable trials. Five-year OS was 55.7% while 5-year DFS was 41.3%. As expected, mediastinal lymph node involvement was associated with a worse prognosis. OS was 61.7%, 51.5% and 42.3% for patients with N1 only, N2 only and N1+N2 disease. Five-year DFS was 41.3%. Again, DFS rates decreased with lymphatic spread (45.8% for N1, 40.1% for N2 and 30% for N1+N2). Interestingly, when analyzing in pairs, only the combination of N1+N2 involvement significantly influenced prognosis. Skip metastases were not associated with a worse prognosis. The number of mediastinal regions assessed did not affect OS, but the number of lymph nodes resected was significantly associated with a better prognosis in terms of OS and DFS. This seems to oppose our results showing that the more accurate the LND, the higher the likelihood of detecting N1+N2 disease (and therefore, a prediction of worse prognosis). We found that detection of N positive disease after resection of less than 8 lymph nodes, was associated to worse prognosis when compared to DFS of patients subjected to a more accurate lymphadenectomy, suggesting that detection of low number of N-positive lymph nodes after a more accurate LN-dissection (meaning higher number of lymph nodes resected) may identify a cohort of patients with better prognosis. The use of the number of tumor-positive lymph nodes resected as a prognostic factor in NSCLC patients has been previously reported (27,28). The lack of a relationship between the type of resection and prognosis suggests that resection of the primary tumor is well established and was properly performed. Only pneumonectomy was related with better DFS rates, but with no differences on OS. Nevertheless, we should not forget that the number of lymph nodes assessed was significantly higher in pneumonectomies than in lobectomies or bilobectomies. Adenocarcinoma was associated with better outcomes than other non-small cell histological subtypes.
In conclusion, after evaluating the quality of surgical issues relating to hilar and mediastinal examination in our SCAT trial series, we found that international recommendations were not considered for the design of the trial and were not followed in a high proportion of surgical procedures. Hilar and mediastinal lymph node assessment and involvement showed to impact prognosis. Important issues for the analysis of a surgical series, such as postoperative mortality, could not be evaluated owing to trial design. Even when it comes to analyze systemic treatments, in the face of a surgical series, surgical audit of the minimum quality criteria defined by the IASLC must be followed. The role of surgeons throughout the design of trials and control of potential biases in terms of the surgical procedure itself seems essential.
Acknowledgments
A total of 47 centers participated in SLCG-SCAT trials. We appreciate the role of all surgeons involved. Besides those included as authors, we also recognize the participation of R. Paniagua, R. Arrabal, AJ. Torres, D. Agero, C. Baamonde, JJ. Rivas, S. Quevedo, JM. Prim, J. Rodríguez, A. Sánchez Palencia, J. Moradiellos, A. Varela, F. Sebastián, M. Jiménez, R. Guijarro, A. Arnau, JA. Torrecilla, J. Gimferrer, C. Montero, AM. Gómez, J. Calatayud, N. Mañés, J. Astudillo, J. Galbis, E. Martínez, A. Carvajal, JL. Martín de Nicolás, JM. Izquierdo, L. Molins, J. Lago, I. Muguruza, Mariñán, J. Maestre, R. Rami-Porta, FJ. Belda and C. Hernández. Authors thank Medical Statistics Consulting S.L (Valencia) for proof reading and editing services.
Funding: SCAT-SLCG trial was sponsored by Sanofi-Aventis.
Footnote
Reporting Checklist: The authors have completed the STROBE reporting checklist. Available at: http://dx.doi.org/10.21037/tlcr-20-1055
Data Sharing Statement: Available at: http://dx.doi.org/10.21037/tlcr-20-1055
Conflicts of Interest: All authors have completed the ICMJE uniform disclosure form (available at: http://dx.doi.org/10.21037/tlcr-20-1055). The authors have no conflicts of interest to declare.
Ethical Statement: The authors declare that they are all accountable for all aspects of the work (if applied, including full data access, integrity of the data and the accuracy of the data analysis) in ensuring that questions related to the accuracy or integrity of any part of the work are appropriately investigated and resolved. The study was approved by institutional/regional/national ethics/committee/ethics board of every hospital participating in the trial (2007-000067-15) and informed consent was taken from all the patients.
Open Access Statement: This is an Open Access article distributed in accordance with the Creative Commons Attribution-NonCommercial-NoDerivs 4.0 International License (CC BY-NC-ND 4.0), which permits the non-commercial replication and distribution of the article with the strict proviso that no changes or edits are made and the original work is properly cited (including links to both the formal publication through the relevant DOI and the license). See: https://creativecommons.org/licenses/by-nc-nd/4.0/.
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