Background
Postoperative chemotherapy is currently administered to patients with pathological stage (p-Stage) IB cancer, as the efficacy of postoperative adjuvant chemotherapy in these patients has been proven in several global studies [
1-
3], and postoperative oral tegafur-uracil has proved efficacious in a group of Japanese patients [
4,
5]. At present, patients with p-Stage IA cancer often only receive follow-up care after surgery because their outcome is generally favorable without postoperative chemotherapy. Therefore, it is difficult to determine the efficacy of postoperative chemotherapy in these patients. In addition, chemotherapy including tegafur-uracil is not currently administered to patients with p-Stage IA disease, because of the observed adverse effects. However, identification of patients with p-Stage IA disease who have a high risk of recurrence may result in further improvement in the outcome of these patients.
Pleural invasion (PL) is a factor used in the tumor-node-metastasis (TNM) classification, and its importance as a poor prognostic factor has been demonstrated in several studies [
6-
11]. In the 7th edition of the Union for International Cancer Control TNM Classification, published in 2009, PL was reappraised as a pathological factor that distinguishes p-Stage IA from p-Stage IB disease. While invasion at the pleural surface denoted p-Stage IB in the previous editions, invasion beyond the pleural elastic layer became a criterion for determining p-Stage IB in the 7th edition. Travis et al. [
12,
13] recommended the use of elastic fiber staining to improve the accuracy of its determination.
Despite many previously published studies reporting that vascular invasion, comprising blood vessel invasion (v) and lymphatic vessel invasion (ly), was a strong independent prognostic factor for recurrence in patients with p-Stage I primary non-small cell lung cancer (NSCLC) lesions ≤3 cm in diameter [
10,
14-
23], it was not considered a factor in the new TNM classification. This may explain why there is no standard pathological assessment method for vascular invasion.
Accordingly, we assessed vascular invasion in patients with p-Stage I NSCLC lesions ≤3 cm diameter, using hematoxylin-eosin (HE), Elastica van Gieson (EvG), and D2-40 antibody immunohistological staining to examine whether vascular invasion can be assessed using HE staining alone. In addition, we evaluated whether vascular invasion was a useful prognostic factor in patients with p-Stage I NSCLC lesions ≤3 cm in diameter. We assessed the impact of vascular invasion by using the number of invaded vascular channels as a prognostic factor and compared its prognostic accuracy with the presence or absence of PL. Furthermore, we investigated whether v and ly are independent prognostic factors for recurrence in patients with p-Stage I NSCLC by comparing them with other factors, and examined whether differences in recurrence rates according to vascular invasion are useful in reconsidering the application of additional postoperative treatment.
Discussion
In recent years, vascular invasion has been considered an important prognostic factor for patients with p-Stage I NSCLC without metastasis to the lymph nodes [
17-
23]. Although it is generally believed that HE staining alone is insufficient for vascular invasion diagnoses, few studies have compared HE staining with immunostaining or other specific staining for vascular invasion. Several vascular markers have been previously used. CD31 and CD34 are reactive with vascular endothelial cells; however, CD31 exhibits cross-reaction with platelets, monocytes, and macrophages, and CD34 displays cross-reaction with hematological stem cells and mesenchymal cells. We decided to use EvG staining and podoplanin immunostaining because the former illustrates the blood vessels and clarifies vascular destruction by tumor cells. Podoplanin depicts lymphatic endothelium in the mesenchyme only. Given the difficulty in performing EvG and D2-40 staining of the entire tumor section for all patients in a diagnostic setting, we used the largest tumor sections to ensure realistic representative values (1–5 slide glasses per patient; mean, 1.5 slide glasses per patient in the current study).
We demonstrated that HE staining alone is not sufficient to diagnose vascular invasion accurately, by first examining the diagnosis by HE staining alone, and then adding EvG and D2-40 staining. As shown in Tables
2,
3 and
4, although diagnosis of BVI on HE staining alone revealed significant differences in both univariate and multivariate analyses (HR = 3.945; p < 0.0001 and p = 0.002, respectively), it was apparent that this diagnosis had an inferior sensitivity, as the diagnosis was missed in many patients and their risk of recurrence was not accurately diagnosed. Therefore, HE staining alone cannot accurately identify vascular invasion as similar results were obtained for the diagnosis of ly. HE staining is likely to yield false-negative results in patients who have vascular channels that are difficult to recognize by HE staining alone. This can be because of the destruction of the existing vascular lumen structure, small gaps between the vascular wall and tumor cells, and extremely dense tumors with solid components which results in an indistinct vascular lumen. In contrast, possible reasons for false-positive results following HE staining include a tumor in a prominently thickened alveolar wall owing to advanced fibrosis, easily misidentified as blood vessels, and the presence of tumor cells in gaps created as artifacts during sample preparation. The diagnosis of vascular invasion on HE staining alone may be dependent on the skills of the observer. Although diagnosis by more than one observer may increase accuracy, the addition of EvG and D2-40 staining enables both experienced evaluators and other observers to diagnose vascular invasion readily, and is extremely important for a more accurate diagnosis and assessment of recurrence factors.
Currently, vascular invasion is often assessed using vague qualitative expressions such as “present”, “slight”, and “moderate”. Therefore, we assessed whether there was a significant difference in evaluation of vascular invasion by counting the number of invaded blood vessels on the entire surface of the largest tumor section. A significant difference was noted in the initial comparison between v(+) and v(−), probably because of the predominance of patients with ≥2 v. The most important aspect of the diagnosis of v is not whether it is present or absent, but instead, it is the presence of ≥2 v in the largest tumor section, i.e., the “degree” of v at a given level (assessment considering the BVI). In the diagnosis of ly, a significant difference was observed between the 0 ly and 1 ly groups (p <0.0001), with no further significant difference observed between the 1 ly and ≥2 ly groups. These findings indicate the importance of “presence” in ly diagnosis (assessment considering the LVI).
Many authors have reported that the presence of vascular invasion was a significant prognostic factor [
10,
15-
17,
19-
23]; however, these studies only included patients with a high degree of vascular invasion. Recently, Kaseda et al. reported that the presence, but not the extent of invasion, was a significant prognostic factor; however, they used glass slides that were previously stained using two different elastic fiber staining methods, which might have resulted in discoloration and have affected the certainty of the evaluation [
24]. The assessment should be performed under controlled conditions wherever possible, as applied in this study. Some authors studied other aspects of vascular invasion. Brechot et al. found no prognostic significance when they compared invasion of arteries and veins [
14]. Saijo et al. reported the prognostic significance of the location of lymphatic vessels (inside vs. outside the tumor nodule) [
18]. The location of vascular invasion might be an important prognostic factor, and further evaluation is warranted.
Image analysis of NSCLC microvasculature is one of the methods used for vessel evaluation. Kayser et al. measured tumor vascularization with an anti-CD34 antibody and quantitative image analysis [
25,
26]. Szöke et al. reported that an increase in microvessel volume fraction pointed to a poorer survival rate [
27]. Generalization of image analysis on specimens would ensure reproducible and accurate vessel evaluation in daily practice.
The current TNM classification states that T1 should be upstaged to T2 when PL is identified. However, the presence of vascular invasion is still not a factor considered in the p-Stage classification despite it being believed to be significantly associated with recurrence [
17-
23]. Accordingly, we assessed vascular invasion by multivariate analyses and found that PL, BVI, and LVI were independent factors for recurrence. In addition, the prognostic value of BVI (HR = 5.669) was superior to that of PL (HR = 2.799), indicating that BVI is more strongly associated with recurrence than PL. As there is no criterion for changing the p-Stage classification according to vascular invasion, patients with NSCLC lesions ≤3 cm in diameter without PL are all diagnosed with p-Stage IA disease. However, given that the classification of such patients according to BVI results in significantly different recurrence rates, the present classification of these patients in the same p-Stage could be improved.
Consequently, we compared p-Stage IA patients with 168 p-Stage IB patients who underwent resection using the same operative procedure at approximately the same time. Figure
5A shows that the survival of the IA(−) group was significantly different from that of both the IA(+) and IB groups, whereas no difference in survival was noted between the IA(+) and IB groups. However, the IB(−) group tended to have better survival than the IA(+) group (Figure
5B). Although postoperative chemotherapy is currently recommended for p-Stage IB patients [
1-
6], p-Stage IA patients with TVI are only monitored and do not receive treatment postoperatively. The administration of postoperative treatment equivalent to that given to p-Stage IB patients could lead to an improved outcome for p-Stage IA patients u.
Competing interests
The authors declare that they have no competing interests.
Authors’ contributions
RH and TY designed the study, carried out the experiments and drafted the manuscript. YS participated in data analysis. MT, HI, HN and KY contributed cases/case information. RM and MI confirmed the contents of the article. All authors approved the final version of the manuscript.