| Literature DB >> 17592498 |
H-S Lee1, S T Kim, J Lee, Y S Choi, J-H Han, Y-C Ahn, K-S Lee, J S Ahn, M J Ahn, K Kim, Y M Shim, J Kim, K Park.
Abstract
Thymic epithelial tumours (TETs), the most common tumour of the anterior mediastinum, are epithelial neoplasms of the thymus with a wide spectrum of morphologic features. We retrospectively analysed clinical features of TET and the correlation of World Health Organisation (WHO) histologic classification and Masaoka staging system with different treatment modalities in 195 patients, from 1995 to 2005. According to the Masaoka's staging system, there were 78 (40.0 %) patients with stage I, 38 (19.5%) with stage II, 41 (21.0%) with stage III, 38 (19.5%) with stage IV. All patients were reclassified according to the WHO criteria as follows: Type A (n=9, 4.6%), AB (n=37, 18.9%), B1 (n=29, 14.8%), B2 (n=48, 24.6%), B3 (n=40, 20.5%), C (n=32, 16.4%). There was a fairly good correlation between Masaoka staging and WHO histotype (P<0.05). However, in multivariate analysis, the tumour stage and WHO histotype were two independent factors separately for predicting overall survival (P<0.001, P<0.001, respectively). Thus, both Masaoka stage and WHO histotype should be considered in risk stratification of therapy for TET patients. Patients with completely resected types B2, B3 and C and adjuvant radiotherapy (n=57) had more favourable disease-free and overall survival as compared with those without adjuvant treatment (n=20) (P=0.015, 0.015, respectively). Given that the predominant sites of recurrence after surgery was pleura/pericardium and lung, and the fact that complete resection was a significant influential factor for survival at log-rank test, an active investigation of newer treatment strategies such as neoadjuvant treatment to improve the resectability and development of optimal adjuvant treatment modality is a high priority especially for those with high-risk for recurrence or in patients with advanced stage disease.Entities:
Mesh:
Year: 2007 PMID: 17592498 PMCID: PMC2359672 DOI: 10.1038/sj.bjc.6603833
Source DB: PubMed Journal: Br J Cancer ISSN: 0007-0920 Impact factor: 7.640
Clinical findings of patients with TET
| Median age (range) | 49 years (18–81 years) |
| Gender ratio (M : F) | 103 : 92 (1.1 : 1) |
| Myasthenia Gravis | 27 (13.8%) |
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| 61 (31.3%) |
| Lung | 37 (19.0%) |
| Pericardium | 27 (13.8%) |
| Pleural seeding | 20 (10.3%) |
| Innominate vein | 16 (8.2%) |
| Superior vena cava | 8 (4.1%) |
| Pericardial seeding | 5 (2.6%) |
| Mediastinal lymph node | 4 (2.0%) |
| Pulmonary vessels | 3 (1.5%) |
| Phrenic nerve | 2 (1.0%) |
| Chest wall | 1 (0.5%) |
| Aorta | 1 (0.5%) |
| Lung metastasis | 1 (0.5%) |
| Bone metastasis | 1 (0.5%) |
| Liver | 1 (0.5%) |
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| I | 78 (40.0%) |
| II | 38 (19.5%) |
| III | 41 (21.0%) |
| IV | 38 (19.5%) |
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| A | 9 (4.6%) |
| AB | 37 (18.9%) |
| B1 | 29 (14.8%) |
| B2 | 48 (24.6%) |
| B3 | 40 (20.5%) |
| C | 32 (16.4%) |
Abbreviation: TET=thymic epithelial tumours.
Masaoka stage with reference to the WHO histologic classification system for thymic epithelial tumors
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| I | 5 (6.4) | 28 (35.9) | 12 (15.4) | 20 (25.6) | 10 (12.8) | 3 (3.8) | 78 |
| II | 2 (5.3) | 9 (2.4) | 10 (26.3) | 7 (18.4) | 6 (15.8) | 4 (10.5) | 38 |
| III | 2 (4.9) | 0 (0.0) | 2 (4.9) | 9 (22.0) | 12 (29.3) | 16 (39.0) | 41 |
| IV | 0 (0.0) | 0 (0.0) | 5 (13.2) | 12 (31.6) | 12 (31.6) | 9 (23.7) | 38 |
| Total | 9 (4.6) | 37 (19.0) | 29 (14.9) | 48 (24.6) | 40 (20.5) | 32 (16.4) | 195 |
Abbreviation: WHO=World Health Organisation.
Distribution of treatment modalities according to the masaoka tumour stage
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| 78 (40.0) | 38 (19.5) | 41 (21.0) | 38 (19.5) | 195 | |
| Complete | 78 (100.0) | 38 (100.0) | 35 (85.3) | 10 (26.3) | 161 (82.5) |
| Incomplete | 0 (0.0) | 0 (0.0) | 4 (36.4) | 7 (63.6) | 11 (5.6) |
| Biopsy only | 0 (0.0) | 0 (0.0) | 2 (8.7) | 21 (91.3) | 23 (11.8) |
| R0 only | 43 (55.1) | 19 (50.0) | 5 (12.2) | 3 (7.9) | 70 (35.9) |
| R0+RT | 35 (44.9) | 17 (44.7) | 23 (56.1) | 3 (7.9) | 78 (40.0) |
| R0+CT | — | 2 (5.3) | — | 3 (7.9) | 5 (2.6) |
| R0+CRT | — | — | 7 (17.1) | 1 (2.6) | 8 (4.1) |
| R1/R2+RT | — | — | 2 (8.7) | 1 (2.6) | 3 (1.5) |
| R1/R2+CT or CRT | — | — | 2 (8.7) | 4 (10.5) | 6 (3.1) |
| CT only | — | — | 1 (2.4) | 16 (42.1) | 17 (8.7) |
| CRT only | — | — | 1 (2.4) | 5 (13.1) | 6 (3.1) |
| R1/R2 alone | — | — | — | 2 (5.3) | 2 (1.0) |
Abbreviations: CT=chemotherapy; CRT=chemoradiation; R0=R0 resection; RT=radiation therapy; R1=R1 resection; R2=R2 resection.
Distribution of treatment modalities according to the WHO subtypes
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| n (%) | 9 (4.6) | 37 (18.9) | 29 (14.8) | 48 (24.6) | 40 (20.5) | 32 (16.4) | 195 (%) |
| Complete | 9 (100.0) | 37 (100.0) | 27 (93.1) | 39 (81.2) | 30 (75.0) | 19 (59.3) | 161 (82.5) |
| Incomplete | — | — | 1 (3.4) | 4 (8.3) | 3 (7.5) | 3 (9.4) | 11 (5.6) |
| Biopsy only | — | — | 1 (3.4) | 5 (10.4) | 7 (17.5) | 10 (31.3) | 23 (11.8) |
| R0 only | 6 (66.7) | 31 (83.8) | 13 (44.8) | 14 (29.2) | 4 (10.0) | 2 (6.3) | 70 (35.9) |
| R0+RT | 3 (33.3) | 6 (16.2) | 12 (41.4) | 24 (50.0) | 22 (55.0) | 11 (34.4) | 78 (40.0) |
| R0+CT | — | — | 2 (6.9) | 1 (2.1) | 1 (2.5) | 1 (3.1) | 5 (2.6) |
| R0+CRT | — | — | — | — | 3 (7.5) | 5 (15.6) | 8 (4.1) |
| R1/R2+RT | — | — | — | 1 (2.1) | — | 2 (6.3) | 3 (1.5) |
| R1/R2+CT or CRT | — | — | — | 2 (4.2) | 3 (7.5) | 1 (3.1) | 6 (3.1) |
| CT only | — | — | 1 (3.4) | 4 (8.3) | 6 (15.0) | 6 (18.8) | 17 (8.7) |
| CRT only | — | — | — | 1 (2.1) | 1 (2.5) | 4 (12.5) | 6 (3.1) |
| R1/R2 alone | — | — | 1 (3.4) | 1 (2.1) | — | — | 2 (1.0) |
Abbreviations: CT=chemotherapy; CRT=chemoradiation; R0=R0 resection; RT=radiation therapy; R1=R1 resection; R2=R2 resection.
Figure 1Overall survival (A) and disease-free survival (B) in thymic epithelial tumours.
Figure 2Disease-free survival (A) and overall survival (B) according to the Masaoka stage.
Figure 3Disease-free survival (A) and survival (B) according to the WHO histologic classification.
Figure 4Survival according to the complete resection of thymoma.
Figure 5Influence of adjuvant radiotherapy on (A) disease-free survival (B) overall survival of patients with type B2-C TETs.