Uniportal video-assisted thoracoscopic surgery (VATS) for the treatment of early-stage lung cancer with whole pleural adhesion
Introduction
Uniportal video-assisted thoracoscopic surgery (VATS) is the most advanced minimally invasive type of lung surgery (1). It was initially adopted for pulmonary wedge resection, and uniportal VATS lobectomy was first reported by Diego Gonzalez-Rivas (2,3) in 2011. Since that initial report, uniportal VATS has been actively studied and used in anatomical pulmonary resection in the treatment of lung cancer (1,4-6). Uniportal VATS has been considered more difficult than multiportal VATS because it is performed by inserting 2 or 3 surgical instruments and the thoracoscope through a single incision.
By 2017, Gonzalez-Rivas had proposed a standardized technique for uniportal VATS anatomical pulmonary resection (7,8), and a uniportal VATS training program had been established at the Shanghai Pulmonary hospital in Shanghai, China (9), an ultra-high-volume center for thoracic surgery, where more than 10,000 lung cancer resections are performed every year. We are among the many surgeons who have participated in the uniportal VATS training program and who are now conducting uniportal VATS. Since January 2017, when we participated in the training program, we have been performing all lung cancer surgeries with uniportal VATS (10).
In some cases of whole pleural adhesion, where the entire pleura and lung are attached, there may not even be space for insertion of the thoracoscope. Although multiportal VATS lobectomy with pleural adhesiolysis is possible in most cases of operable lung cancer, it can be very time consuming to separate the adhesion of the entire lung from the parietal pleura. Lung cancer surgery with whole pleural adhesion is a challenging procedure for multiportal VATS (11). We believed it would be even more challenging in uniportal VATS, as we surmised that it would be too difficult to separate the entire adhesion from only one direction through a single port. However, our thinking changed after we completed the uniportal VATS training program, and we have now been performing uniportal VATS in all lung cancer patients with whole pleural adhesion since January 2017.
The purpose of this study was to evaluate the surgical results of uniportal VATS in the treatment of lung cancer with whole pleural adhesion and to examine whether uniportal VATS can be regarded as a feasible surgical approach for lung cancer with whole pleural adhesion. We hypothesized that uniportal VATS did not have worse surgical or oncological outcomes than multiportal VATS. We present the following in accordance with the STROBE reporting checklist (available at https://tcr.amegroups.com/article/view/10.21037/tcr-21-2113/rc).
Methods
Patients
From 2012 to 2018 at a single institution, 727 patients were diagnosed with non-small cell lung cancer (NSCLC) and underwent curative surgery by two surgeons including the author at a hospital in Korea. We performed multiportal VATS from 2012 to 2016 and uniportal VATS from 2017 to 2018. There were 100 patients with whole pleural adhesion. Among them, 27 were excluded from the retrospective analysis because of open thoracotomy (3 cases), incomplete resection (2 cases), higher than stage III (10 cases), or preoperative chemotherapy (12 cases). Whole pleural adhesion is defined as the complete (100%) attachment of the entire parietal and visceral pleura. To reduce the selection bias, all data were obtained from consecutive patients. Finally, 73 consecutive patients were included.
The operations were conducted by two surgeons who had sufficient experience with multiportal VATS. They began performing uniportal VATS after attending the uniportal VATS training program at the Shanghai Pulmonary Hospital in January 2017, and they have operated all indicated lung cancers since 2017 with uniportal VATS. In this study, the surgical results of multiportal VATS before January 2017 and those of uniportal VATS after January 2017 were compared. The patients were divided into a uniportal VATS group and a multiportal VATS group. The clinicopathologic characteristics were analyzed in the two groups and perioperative and postoperative outcomes were compared.
The study was conducted in accordance with the Declaration of Helsinki (as revised in 2013). It was approved by the institutional review board of Eunpyeong St. Mary’s Hospital at the Catholic University of Korea (No. PC21RISI0115) and individual consent was waived.
Surgical procedures
Most clinical stage I and II lung cancers are operated with VATS in our institution. Operative procedures in the study included wedge resection, segmentectomy, lobectomy, and bilobectomy. Multiportal VATS was performed with 3 ports and a working incision, whereas uniportal VATS was performed using only the working incision. In multiportal VATS, the camera and several instruments are placed in separate ports to perform the surgery, whereas in uniportal VATS, the camera and two instruments are inserted together via a single working incision to perform the surgery. The surgical technique for uniportal VATS is described in detail in our previous publication (10). In whole pleural adhesion, the pulmonary resection usually began after the whole pleural adhesiolysis was completed.
Uniportal VATS adhesiolysis
The skin incision was usually made in the fifth intercostal space between the mid- and anterior axillary lines, except in right upper lobectomy, where the fourth intercostal space was chosen. The incision length was usually 3 to 3.5 cm. When pleural adhesion was detected, a surgeon’s finger was placed into the working incision to create a space by blunt dissection, allowing for insertion of the thoracoscope into the working incision (Figure 1). Meticulous pleural adhesiolysis was then conducted by electrocauterization using a curved instrument (Figure 2). We were able to approach the diaphragm easily when the working incision was made at the fifth intercostal space of the anterior axillary line. From this location, when both the thoracoscope and the surgical instruments are pointed towards the diaphragm, all parts of the diaphragm are accessible with the surgical instruments and adhesiolysis around the diaphragm can be easily performed through the single port. Curved electrocautery was used for adhesiolysis close to the working incision site, followed by adhesiolysis in areas far from the working incision by using an energy-based vessel sealing device (harmonic scalpel). In cases where a peripheral tumor was adjacent to the visceral pleura, we always performed adhesiolysis by carrying out extrapleural dissection while the parietal pleura around the tumor was attached to the lung.
Multiportal VATS adhesiolysis
The operation was performed by using a working incision and 3 additional ports. The working incision was made in the fourth intercostal space between the mid- and anterior axillary lines and the 3 additional ports were placed at the seventh intercostal space in the mid-axillary line, the fifth intercostal space under the tip of the scapula, and the sixth intercostal space at the anterior axillary line. Adhesiolysis started with a blunt dissection from the working incision site. The 3 ports were inserted after the space for the port sites was secured, and all ports and the working incision were then used for adhesiolysis.
Statistical analysis
Clinicopathologic factors were compared using a Student’s t-test or the Wilcoxon rank sum test for continuous variables and chi-squared or Fisher exact test for categorical variables. The Kaplan-Meier method was used to analyze data collected from the interval between the time of operation and the time of the last follow-up visit and to estimate the recurrence-free survival (RFS) and disease-specific survival (DSS) rates. Survival of each group was compared by log-rank test. A Cox proportional hazards model was used in a multivariate analysis to identify risk factors for recurrence after surgery. All variables with P<0.1 on univariate analysis were entered into the multivariate analysis. Any P<0.05 was considered statistically significant. Statistical analysis was performed using SPSS version 24.0 software (IBM Corp, Armonk, NY, United States).
Results
Table 1 shows the comparison of clinicopathologic characteristics between uniportal VATS and multiportal VATS. Sixteen patients underwent uniportal VATS and 57 had multiportal VATS. There were no significant differences of clinicopathologic characteristics between the two groups.
Table 1
| Variables | Uniportal VATS (n=16) | Multiportal VATS (n=57) | P value |
|---|---|---|---|
| Age (years) | 65.9±9.4 | 68.3±7.9 | 0.313 |
| Sex | 0.776 | ||
| Male | 8 (50.0) | 33 (57.9) | |
| Female | 8 (50.0) | 24 (42.1) | |
| Current or former smoker | 7 (43.8) | 29 (50.9) | 0.778 |
| Pulmonary function | |||
| FEV1 (%) | 83.8±16.9 | 88.3±17.5 | 0.361 |
| DLCO (%) | 85.8±15.2 | 76.6±20.3 | 0.096 |
| Involved lobe | 0.866 | ||
| Right upper | 7 (43.8) | 18 (31.6) | |
| Right middle | 1 (6.3) | 3 (5.3) | |
| Right lower | 3 (18.8) | 17 (29.8) | |
| Left upper | 2 (12.5) | 9 (15.8) | |
| Left lower | 3 (18.8) | 10 (17.5) | |
| Surgical procedures | 0.527 | ||
| Wedge resection | 3 (18.8) | 6 (10.5) | |
| Segmentectomy | 3 (18.8) | 6 (10.5) | |
| Lobectomy | 10 (62.5) | 43 (75.4) | |
| Bilobectomy | 0 | 2 (3.5) | |
| Histology | 0.286 | ||
| Adenocarcinoma | 14 (87.5) | 37 (64.9) | |
| Squamous cell carcinoma | 2 (12.5) | 18 (31.6) | |
| Others | 0 | 2 (3.5) | |
| Pathologic stage | 0.604 | ||
| 0 | 1 (6.3) | 1 (1.8) | |
| IA1 | 5 (31.3) | 12 (21.1) | |
| IA2 | 3 (18.8) | 12 (21.1) | |
| IA3 | 2 (12.5) | 3 (5.3) | |
| IB | 2 (12.5) | 12 (21.1) | |
| IIA | 0 | 5 (8.8) | |
| IIB | 3 (18.8) | 12 (21.1) | |
| Tumor size (invasive component size) (cm) | 1.8±1.6 | 2.5±1.8 | 0.201 |
| Tumor location | 0.281 | ||
| Central location | 1 (6.3) | 11 (19.3) | |
| Peripheral location | 15 (93.8) | 46 (80.7) | |
| Histologic tumor grade | 0.245 | ||
| Well differentiated | 8 (50.0) | 15 (26.3) | |
| Moderately differentiated | 5 (31.3) | 26 (45.6) | |
| Poorly differentiated | 3 (18.8) | 16 (28.1) | |
| Pleural invasion | 0.784 | ||
| Visceral pleural invasion | 4 (25.0) | 13 (22.8) | |
| Parietal pleural invasion | 0 | 4 (7.0) | |
| Lymphovascular invasion | 5 (31.3) | 30 (52.6) | 0.163 |
Data are shown as mean ± SD or number (percentage). VATS, video-assisted thoracoscopic surgery; SD, standard deviation; FEV1, forced expiratory volume in 1 second; DLCO, diffusing capacity for carbon monoxide.
Comparison of surgical outcomes between uniportal VATS and multiportal VATS
Table 2 shows the perioperative and postoperative outcomes for all patients. There were 5 conversions to open thoracotomy in the multiportal VATS group, whereas there were no conversions in the uniportal VATS group. However, the difference of conversion rate was not statistically significant (P=0.579). There were two conversions from uniportal VATS to multiportal VATS due to endo-stapler direction and adhesiolysis at the diaphragm.
Table 2
| Variables | Uniportal VATS (n=16) | Multiportal VATS (n=57) | P value |
|---|---|---|---|
| Conversion to open thoracotomy | 0 | 5 (8.8%) | 0.579 |
| Extent of lymph node dissection | 0.764 | ||
| No mediastinal node dissection | 4 (25.0%) | 13 (22.8%) | |
| Systematic nodal dissection | 6 (37.5%) | 27 (47.4%) | |
| Lobe-specific nodal dissection | 6 (37.5%) | 17 (29.8%) | |
| Number of dissected lymph nodes | 0.388 | ||
| Mean ± SD | 10.0±9.3 | 12.6±11.0 | |
| Median [Q1–Q3] | 9 [2.3–15.3] | 11 [4–19] | |
| Anesthetic duration (min) | 0.070 | ||
| Mean ± SD | 244.4±72.7 | 279.4±65.8 | |
| Median [Q1–Q3] | 255 [177.5–308.8] | 265 [230–320] | |
| Operative time (min) | 0.248 | ||
| Mean ± SD | 204.0±70.7 | 225.9±65.5 | |
| Median [Q1–Q3] | 224.5 [131.3–260.0] | 210 [172.5–268.0] | |
| Intraoperative blood loss (mL) | 0.101 | ||
| Mean ± SD | 125.0±414.0 | 417.0±432.3 | |
| Median [Q1–Q3] | 75 [50.0–187.5] | 300 [100–500] | |
| Postoperative chest drainage (day) | 0.733 | ||
| Mean ± SD | 8.1±7.7 | 7.2±8.6 | |
| Median [Q1–Q3] | 6 [3.3–8.0] | 5 [4–8] | |
| Postoperative hospital stay (day) | 0.768 | ||
| Mean ± SD | 9.8±9.1 | 9.0±9.7 | |
| Median [Q1–Q3] | 8 [5.0–9.8] | 6 [5.0–10.5] | |
| Postoperative complications | 5 (31.3%) | 18 (31.6%) | 1.000 |
| Prolonged air leak (>5 days) | 3 | 14 | |
| Chylothorax | 0 | 1 | |
| Atrial fibrillation | 0 | 1 | |
| Pneumonia | 2 | 2 | |
| Bronchial stenosis | 0 | 1 | |
| Operative mortality | 0 | 0 |
VATS, video-assisted thoracoscopic surgery; SD, standard deviation.
Other perioperative outcomes were also similar between the two groups, as were the postoperative complication rates (31.3% uniportal VATS vs. 31.6% multiportal VATS). All complications were resolved during the hospital stay. There was no mortality in all patients.
In subgroup analysis of patients undergoing VATS lobectomy (Table 3), there was no statistical difference in perioperative and postoperative outcomes between uniportal VATS lobectomy and multiportal VATS lobectomy.
Table 3
| Variables | Uniportal VATS lobectomy (n=10) | Multiportal VATS lobectomy (n=45) | P value |
|---|---|---|---|
| Conversion to open thoracotomy | 0 | 4 (8.9%) | 1 |
| Extent of lymph node dissection | 1 | ||
| No mediastinal node dissection | 1 (10.0%) | 6 (13.3%) | |
| Systematic nodal dissection | 6 (60.0%) | 25 (55.6%) | |
| Lobe-specific nodal dissection | 3 (30.0%) | 14 (31.1%) | |
| Number of dissected lymph nodes | 0.908 | ||
| Mean ± SD | 13.9±9.2 | 14.3±10.9 | |
| Median [Q1–Q3] | 11.5 [6.8–23.5] | 13 [6.5–19.5] | |
| Anesthetic duration (min) (±SD) | 0.346 | ||
| Mean ± SD | 264.0±61.0 | 285.5±65.4 | |
| Median [Q1–Q3] | 255 [211.3–326.3] | 265 [232.5–326.5] | |
| Operative time (min) (±SD) | 0.759 | ||
| Mean ± SD | 224.1±58.6 | 231.1±65.9 | |
| Median [Q1–Q3] | 224.5 [176.3–282.3] | 225 [172.5–270.0] | |
| Intraoperative blood loss (mL) | 0.354 | ||
| Mean ± SD | 307.0±509.9 | 461.1±463.4 | |
| Median [Q1–Q3] | 125 [50.0–312.5] | 300 [100–550] | |
| Postoperative chest drainage (day) | 0.733 | ||
| Mean ± SD | 8.1±7.7 | 7.2±8.6 | |
| Median [Q1–Q3] | 6 [3.8–9.3] | 5 [4–9] | |
| Postoperative hospital stay (day) | 0.793 | ||
| Mean ± SD | 10.8±10.9 | 9.8±10.6 | |
| Median [Q1–Q3] | 8.5 [4.8–10.3] | 7 [5–11] | |
| Postoperative complications | 2 (20.0%) | 16 (35.6%) | 0.47 |
| PAL | 1 | 12 | |
| Chylothorax | 0 | 0 | |
| Atrial fibrillation | 0 | 1 | |
| Pneumonia | 1 | 2 | |
| Bronchial stenosis | 0 | 1 | |
| Operative mortality | 0 | 0 |
VATS, video-assisted thoracoscopic surgery; SD, standard deviation; Q1–Q3, quartile 1 – quartile 3; PAL, prolonged air leak (>5 days).
Survival analysis of all study patients
The comparison of RFS between uniportal VATS and multiportal VATS was conducted in all study patients. The median follow-up time for the uniportal VATS patients was 701 days (range, 195–1,169 days) and the median follow-up time for the multiportal VATS group was 1,872 days (range, 151–3,469 days). A total of 16 patients had recurrence, and the sites of recurrence were similar in uniportal VATS and multiportal VATS (Table 4). Since the follow-up time in the uniportal VATS group was short, the 3-year RFS was compared between the two groups. The 3-year RFS after uniportal VATS was 80.0%, and the 3-year RFS after multiportal VATS was 79.5% (P=0.951) (Figure 3).
Table 4
| Variables | Uniportal VATS (n=16) | Multiportal VATS (n=57) | P value |
|---|---|---|---|
| Sites of recurrence | 0.771 | ||
| Locoregional recurrence | 1 (6.3%) | 6 (10.5%) | |
| Distant recurrence | 2 (12.5%) | 4 (7.0%) | |
| Both | 0 | 3 (5.3%) |
Locoregional, recurrence within ipsilateral hemithorax including pleura and mediastinal lymph nodes; Both, locoregional recurrence + distant recurrence.
Survival analysis for stage I non-small cell lung cancer
RFS was compared for uniportal VATS and multiportal VATS in patients with stage I NSCLC after confirming that there was no statistical difference of clinicopathologic characteristics between the two groups (Table 5).
Table 5
| Variables | Uniportal VATS (n=13) | Multiportal VATS (n=40) | P value |
|---|---|---|---|
| Age (years) | 65.5±9.8 | 66.8±8.5 | 0.663 |
| Sex | 1 | ||
| Male | 7 (53.8) | 20 (50.0) | |
| Female | 6 (46.2) | 20 (50.0) | |
| Current or former smoker | 6 (46.2) | 19 (47.5) | 1 |
| Pulmonary function | |||
| FEV1 (%) | 84.4±18.8 | 90.6±13.4 | 0.285 |
| DLCO (%) | 86.3±15.5 | 77.8±21.8 | 0.2 |
| Involved lobe | 0.93 | ||
| Right upper | 6 (46.2) | 15 (37.5) | |
| Right middle | 1 (7.7) | 3 (7.5) | |
| Right lower | 2 (15.4) | 10 (25.0) | |
| Left upper | 2 (15.4) | 4 (10.0) | |
| Left lower | 2 (15.4) | 8 (20.0) | |
| Surgical procedures | 0.446 | ||
| Wedge resection | 3 (23.1) | 4 (10.0) | |
| Segmentectomy | 2 (15.4) | 5 (12.5) | |
| Lobectomy | 8 (61.5) | 31 (77.5) | |
| Histology | 0.78 | ||
| Adenocarcinoma | 11 (84.6) | 30 (75.0) | |
| Squamous cell carcinoma | 2 (15.4) | 9 (22.5) | |
| Others | 0 | 1 (2.5) | |
| Pathologic stage | 0.537 | ||
| 0 | 1 (7.7) | 1 (2.5) | |
| IA1 | 5 (38.5) | 12 (30.0) | |
| IA2 | 3 (23.1) | 12 (30.0) | |
| IA3 | 2 (15.4) | 3 (7.5) | |
| IB | 2 (15.4) | 12 (30.0) | |
| Tumor size (invasive component size) (cm) | 1.4±1.1 | 1.6±1.1 | 0.507 |
| Tumor location | 0.317 | ||
| Central location | 0 | 5 (12.5) | |
| Peripheral location | 13 (100.0) | 35 (87.5) | |
| Histologic tumor grade | 0.651 | ||
| Well differentiated | 7 (53.8) | 15 (37.5) | |
| Moderately differentiated | 4 (30.8) | 16 (40.0) | |
| Poorly differentiated | 2 (15.4) | 9 (22.5) | |
| Visceral pleural invasion | 2 (15.4) | 9 (22.5) | 0.711 |
| Lymphovascular invasion | 3 (23.1) | 15 (37.5) | 0.504 |
Data are shown as mean ± SD or number (percentage). VATS, video-assisted thoracoscopic surgery; SD, standard deviation; FEV1, forced expiratory volume in 1 second; DLCO, diffusing capacity for carbon monoxide.
A total of 6 patients had recurrences after a median follow-up time of 683 days (range, 195–1,169 days) for the uniportal VATS group and 2,005 days (range, 176–3,366 days) for the multiportal VATS group (Table 6). Three-year RFS after uniportal VATS was 91.7% and 3-year RFS after multiportal VATS was 89.3% (P=0.999) for patients with stage I NSCLC with whole pleural adhesion (Figure 4).
Table 6
| Variables | Uniportal VATS (n=13) | Multiportal VATS (n=40) | P value |
|---|---|---|---|
| Sites of recurrence | 1 (7.7%) | 3 (7.5%) | 1.000 |
| Locoregional recurrence | |||
| Distant recurrence | 0 | ||
| Both | 0 | 2 (5.0%) |
Locoregional, recurrence within ipsilateral hemithorax including pleura and mediastinal lymph nodes; Both, locoregional recurrence + distant recurrence.
Recurrence risk
We next analyzed risk factors for recurrence after VATS in patients with stage I NSCLC with whole pleural adhesion (Table 7) by conducting univariate and multivariate analyses using a Cox proportional hazard model to identify the risk factors for recurrence. Significant factors (P<0.1) on univariate analysis included age, invasive component size, and lymphovascular invasion. No significant risk factors for recurrence emerged when these variables were entered into the multivariate model. Uniportal VATS was not a significant risk factor for recurrence in this analysis.
Table 7
| Variables | HR | 95% CI | P value |
|---|---|---|---|
| Univariate analysis | |||
| Age | 1.141 | 1.019–1.277 | 0.022 |
| Sex (male) | 0.907 | 0.183–4.498 | 0.905 |
| Smoker | 0.574 | 0.105–3.136 | 0.522 |
| FEV1 (%) | 1.021 | 0.963–1.084 | 0.485 |
| DLCO (%) | 1.002 | 0.961–1.045 | 0.912 |
| Lobe | 0.731 | ||
| Right upper (reference) | 1 | ||
| Right middle | 0 | 0 | 0.991 |
| Right lower | 3.176 | 0.288–35.049 | 0.346 |
| Left upper | 5.201 | 0.322–83.975 | 0.245 |
| Left lower | 5.152 | 0.466–56.976 | 0.181 |
| Sublobar resection | 0.669 | 0.077–5.803 | 0.715 |
| Uniportal VATS | 1.002 | 0.109–9.190 | 0.999 |
| Extent of Lymph node dissection | 0.948 | ||
| No mediastinal node dissection (reference) | 1 | 0.745 | |
| Systematic nodal dissection | 1.457 | 0.151–14.101 | 0.797 |
| Lobe-specific nodal dissection | 1.370 | 0.124–15.122 | |
| Histology | 0.105 | ||
| Adenocarcinoma (Reference) | 1 | ||
| Squamous cell carcinoma | 3.765 | 0.757–18.717 | 0.105 |
| Tumor size | 2.803 | 1.176–6.680 | 0.020 |
| Central location | 0.041 | 0–2906.452 | 0.576 |
| Histologic tumor grade | 0.220 | ||
| Well differentiated (reference) | 1 | ||
| Moderately differentiated | 6.758 | 0.785–58.195 | 0.082 |
| Poorly differentiated | 0 | 0 | 0.982 |
| Number of dissected lymph nodes | 1.029 | 0.949–1.115 | 0.491 |
| Visceral pleural invasion | 2.890 | 0.337–24.809 | 0.333 |
| Lymphovascular invasion | 5.565 | 1.002–30.914 | 0.050 |
| Multivariate analysis | |||
| Age | 1.092 | 0.974–1.225 | 0.131 |
| Invasive component size | 1.662 | 0.623–4.437 | 0.310 |
| Lymphovascular invasion | 2.553 | 0.354–18.426 | 0.353 |
VATS, video-assisted thoracoscopic surgery; HR, hazard ratio; CI, confidence interval; FEV1, forced expiratory volume in 1 second; DLCO, diffusing capacity for carbon monoxide.
Discussion
VATS is considered a challenging procedure when there is severe whole pleural adhesion during pulmonary resection for lung cancer (11). Pleural adhesiolysis through VATS became possible with advances in surgical instruments and surgical skills, and lung cancer surgery with whole pleural adhesion can now be performed with multiportal VATS (12). However, until we completed the uniportal VATS training program at the Shanghai Pulmonary Hospital, we thought that lung cancer surgery with uniportal VATS would be impossible in patients with whole pleural adhesion. Since completing the training program, we have realized that all lung cancer surgery can be performed with uniportal VATS (10). In fact, when adhesiolysis is performed with uniportal VATS, the field of view is better than with multiportal VATS, and the adhesion can be lysed in all directions using a curved instrument. The surgical instruments and techniques in uniportal VATS are continuously evolving, and the potential for uniportal VATS in lung cancer surgery now seems to be without further limitation (1,3,7,13).
In this study, the surgical outcome of uniportal VATS was not inferior to that of multiportal VATS. The operative time was similar between uniportal VATS and multiportal VATS. The thoracotomy conversion rates were not statistically different between the two groups. Conversion to thoracotomy occurred in 5 patients who underwent multiportal VATS (4 due to severe pleural adhesion, and 1 due to calcified perivascular lymph nodes), while there were no conversions to thoracotomy in the patients who underwent uniportal VATS. There were two conversions from uniportal VATS to multiportal VATS. In the first case, all adhesiolysis was completed with uniportal VATS, but when dividing the pulmonary artery, the direction of the endostapler was unsatisfactory, and one additional thoracoscopic port was created. In the end, we did not use the newly created thoracoscopic port, as we were eventually able to divide the pulmonary artery through the working port. In the second case, a thoracoscopic port was added to help detach the adhesions between the diaphragm and lungs, but the contribution of the additional port to adhesiolysis was minimal. Both of these cases were in the early stages of initiating uniportal VATS, and since the additional port was not used for the main surgery, we kept both cases in the uniportal VATS group.
In our previous study, pleural adhesion was not a risk factor for recurrence when lung cancer was treated by multiportal VATS (12). To date, there have been few studies to evaluate the effect of uniportal VATS on the prognosis of NSCLC with whole pleural adhesion. In this study, the uniportal and multiportal VATS groups had similar 3-year RFS and DSS rates, and uniportal VATS was not a risk factor for recurrence in patients with stage I NSCLC with whole pleural adhesion. Therefore, we have concluded that uniportal VATS need no longer be limited in lung cancer surgery with whole pleural adhesion. Of course, it is difficult to generalize the results of this study because the number of cases in this study is small and the follow-up period is short. This study is an initial study to evaluate whether it is appropriate to perform uniportal VATS regardless of the presence or absence of pleural adhesion even as the efficacy of uniportal surgery in treating lung cancer with whole pleural adhesion is not well known. We now believe that there is no difference in difficulty between uniportal VATS and multiportal VATS when performing whole pleural adhesiolysis. Therefore, if more cases are gathered in the future, more accurate results will be obtained.
Pleural adhesions are usually caused by past inflammation of the pleura, and the degree of pleural adhesion varies from patient to patient. Some pleural adhesions can be detached easily by blunt dissection, and some can be detached only by sharp dissection with electrocauterization. The degree of difficulty of surgery will inevitably vary for each patient with pleural adhesion. However, there is no uniform measure of the degree of pleural adhesion. In this study, for a more precise analysis, all patients with partial pleural adhesion were excluded and only patients with whole pleural adhesion were included. Patients with whole pleural adhesion posed similar difficulty in surgery because the pleura was not well separated by blunt dissection. Therefore, unlike other studies related to pleural adhesion (14), this study compared uniportal VATS and multi-portal VATS only for patients with whole pleural adhesion.
This study had several limitations that should be considered. Firstly, we used a retrospective study design. Secondly, we obtained data from a single institution with a small sample size, so generalizing our results is difficult. However, there are advantages to the use of data of patients undergoing surgery in one hospital. It may be more accurate to compare uniportal VATS and multiportal VATS because the treatment protocols are standardized and we are comparing surgical techniques with the same surgeons. If more cases are gathered in the future, more robust results will be obtained. Finally, it has only been a few years since uniportal VATS was initiated, and long-term survival rates have not been compared. However, most cases of NSCLC are known to recur within two years after surgery (15), and early recurrence has proven to be an accurate reflection of long-term outcomes (16). In addition, this study is more focused on the feasibility of uniportal VATS as a surgical technique in cases of lung cancer with whole pleural adhesion than on comparing the prognosis between uniportal VATS and multiportal VATS. More detailed results can be derived in the future if more and longer follow-up data are accumulated.
In conclusion, uniportal VATS may be a feasible surgical approach for the treatment of lung cancer with whole pleural adhesion. Uniportal VATS was not inferior to multiportal VATS in surgical outcome or short-term prognosis in patients with whole pleural adhesion. Additional research in a larger pool of data may more accurately depict patient outcomes.
Acknowledgments
We thank the native English-speaking professional (BioMed Proofreading, LLC) for refining the written content.
Funding: None.
Footnote
Reporting Checklist: The authors have completed the STROBE reporting checklist. Available at https://tcr.amegroups.com/article/view/10.21037/tcr-21-2113/rc
Data Sharing Statement: Available at https://tcr.amegroups.com/article/view/10.21037/tcr-21-2113/dss
Conflicts of Interest: All authors have completed the ICMJE uniform disclosure form (available at https://tcr.amegroups.com/article/view/10.21037/tcr-21-2113/coif). The authors have no conflicts of interest to declare.
Ethical Statement: The authors are accountable for all aspects of the work in ensuring that questions related to the accuracy or integrity of any part of the work are appropriately investigated and resolved. The study was conducted in accordance with the Declaration of Helsinki (as revised in 2013). This study was approved by the institutional review board of Eunpyeong St. Mary’s Hospital at the Catholic University of Korea (Referral number: PC21RISI0115) and individual consent was waived.
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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