| Literature DB >> 25879885 |
Florian Seyfried, Burkhard H von Rahden, Alexander D Miras, Martin Gasser, Uwe Maeder, Volker Kunzmann, Christoph-Thomas Germer, Jörg Pelz, Alexander G Kerscher.
Abstract
BACKGROUND: Comprehensive evidence on the incidence, time course and independent risk factors of metachronous peritoneal carcinomatosis (metaPC) in gastric cancer patients treated with curative intent in the context of available systemic combination chemotherapies is lacking.Entities:
Mesh:
Year: 2015 PMID: 25879885 PMCID: PMC4337241 DOI: 10.1186/s12885-015-1081-8
Source DB: PubMed Journal: BMC Cancer ISSN: 1471-2407 Impact factor: 4.430
Demographic and pathological tumour characteristics of 1072 patients without 30-day mortality constituting the basis for survival calculations
| Demographics and pathological tumor characteristics (n = 1108) | |||||
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| (1986–1994) | (1995–2003) | (2004 – 2013) | |||
| n = 363 (32.8%) | n = 349 (31.5%) | n = 396 (35.7%) | n = 1108 (100%) | ||
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| 8 | 14 | 14 | 0.37 | 36 |
| (2.2%) | (4.0%) | (3.5%) | (3.2%) | ||
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| n = 355 | n = 335 | n = 382 | n = 1072 | |
| (33.1%) | (31.2%) | (35.6%) | (100%) | ||
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| 63.81 | 65.56 | 65.70 y | 0.13* | 65.05 y |
| (19.59 -91.24) | (34.33 -91.58) | (21.78 - 93.91) | (19.59 - 93.91) | ||
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| 224/131 (63.1/36.9%) | 216/119 (64.5/35.5%) | 243/139 (63.6/36.4%) | 0.93 | 683/389 (63.7/36.3%) |
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| 82 (23.1%) | 82 (24.5%) | 103 (27.0%) | 0.47 | 267 (24.9%) |
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| 83 (23.4%) | 102 (30.4%) | 100 (26.2%) | 0.11 | 285 (26.6%) |
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| 63 (17.7%) | 42 (12.5%) | 57 (14.9%) | 0.16 | 162 (15.1%) |
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| 111 (31.3%) | 105 (31.3%) | 114 (29.8%) | 0.88 | 330 (30.8%) |
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| 16 (4.5%) | 4 (1.2%) | 8 (2.1%) | 0.02 | 28 (2.6%) |
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| 61 (17.2%) | 50 (14.9%) | 61 (16.0%) | 0.72 | 172 (16.0%) |
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| 107 (30.1%) | 141 (42.1%) | 89 (23.3%) | <0.001 | 337 (31.4%) |
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| 89 (25.1%) | 79 (23.6%) | 124 (32.5%) | 0.015 | 292 (27.2%) |
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| 76 (21.4%) | 58 (17.3%) | 92 (24.1%) | 0.084 | 226 (21.1%) |
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| 22 (6.2%) | 7 (2.1%) | 16 (4.2%) | 0.027 | 45 (4.2%) |
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| 95 (6.8%) | 99 (29.6%) | 137 (35.9%) | 0.023 | 331 (30.9%) |
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| 55 (15.5%) | 98 (29.3%) | 132 (34.6%) | <0.001 | 285 (26.6%) |
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| 168 (47.3%) | 119 (35.5%) | 82 (21.5%) | <0.001 | 369 (34.4%) |
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| 37 (10.4%) | 19 (5.7%) | 31 (8.1%) | 0.074 | 87 (8.1%) |
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| 11 (3.1%) | 5 (1.5%) | 7 (1.8%) | 0.302 | 23 (2.1%) |
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| 79 (22.3%) | 99 (29.6%) | 99 (25.9%) | 0.091 | 277 (25.8%) |
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| 142 (40.0%) | 209 (62.4%) | 239 (62.6%) | <0.001 | 590 (55.0%) |
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| 7 (2.0%) | 1 (0.3%) | 8 (2.1%) | 0.093 | 16 (1.5%) |
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| 116 (32.7%) | 21 (6.3%) | 29 (7.6%) | <0.001 | 166 (15.5%) |
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| 13 | 8 | 7 | 0.284 | 28 |
| 3,7% | 2,4% | 1,8% | 2,6% | ||
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| 35 (9.9%) | 49 (14.6%) | 74 (19.4%) | 0.001 | 158 (14.7%) |
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| 11 (3.1%) | 30 (9.0%) | 45 (11.8%) | <0.001 | 86 (7.9%) |
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| 99 (27.9%) | 75 (22.4%) | 68 (17.8%) | 0.005 | 242 (22.6%) |
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| 75 (21.1%) | 56 (16.7%) | 39 (10.2%) | <0.001 | 170 (15.9%) |
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| 24 (6.8%) | 19 (5.7%) | 29 (7.6%) | 0.591 | 72 (6.7%) |
The characteristics are stratified for the three time period of treatment (*Kruskal-Wallis-Test)
Overview of the therapy all patients received during the three treatment time periods
| Therapy (all patients n = 1108) | |||||
|---|---|---|---|---|---|
| Time period I | Time period II | Time period III | p-value* | All time periods | |
| (1986–1994) | (1995–2003) | (2004 – 2013) | |||
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| 341 (93.9%) | 331 (94.8%) | 382 (96.5%) | 0.260 | 1054 (95.1%) |
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| 332 (91.5%) | 318 (91.1%) | 347 (87.6%) | 0.148 | 996 (90.0%) |
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| 178 (53.3%) | 196 (61.6%) | 231 (66.8%) | 0.001 | 605 (60.7%) |
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| 3 (1.7%) | 2 (1,0%) | 7 (3.0%) | 0.314 | 12 (2.0%) |
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| 8 (4.5%) | 9 (4.6%) | 16 (6.9%) | 0.456 | 33 (5.5%) |
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| 157 (88.2%) | 184 (93.9%) | 219 (94.8%) | 0.085 | 560 (92.6%) |
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| 155 (98.7%) | 182 (98.9%) | 213 (97.3%) | 0.390 | 550 (98.2%) |
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| 45 (12.4%) | 60 (17.2%) | 211 (53.3%) | <0.001 | 316 (28.5%) |
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| 40 (11.0%) | 45 (12.9%) | 3 (0.8%) | <0.001 | 88 (7.9%) |
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| 5 (1.4%) | 4 (1.1%) | 101 (25.5%) | <0.001 | 110 (9.9%) |
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| 0 (0%) | 0 (0%) | 16 (4%) | <0.001 | 16 (1.4%) |
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| 0 (0%) | 11 (3.2%) | 91 (8.2%) | <0.001 | 102 (9.2%) |
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| 155 | 182 | 213 | 550 | |
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| 0 (0%) | 0 (0%) | 64 (30.0%) | <0.001 | 65 (11.6%) |
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| 155 (100%) | 182 (100%) | 148 (70.0%) | <0.001 | 485 (88.4%) |
Chemotherapy includes perioperative as well as second-line and palliative therapy. Information on neoadjuvant chemotherapy is provided on 550 patients after R0 gastrectomy and D2 lymphadenectomy.
*Combination of 5-FU and/or oxaliplatin, irinotecane, cisplatin, epirubicin, doxorubicin, cyclophosphamide **combination as described above + antibody therapies (Trastuzumab, Panitumumab, Catumaxumab).
Tumour related overall survival of the entire patient cohort without 30-day-mortality (n = 1072) and of patients that were R0 after gastrectomy and D2-lymphadenectomy, stratified for the three time periods of treatment
| Follow up of patients w/o 30d-mortality of operated patients (n = 1072) | |||||
|---|---|---|---|---|---|
| Time period I | Time period II | Time period III | p-value* | ||
| (1986–1994) | (1995–2003) | (2004 – 2013) | |||
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| 45,3 | 41,5 | 25,0 | <0.001 | 36.9 |
| (0 – 257.97) | (0–212.99) | (0–111.97) | (0 – 257.97) | ||
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| 21.9 (±4.36) | 21.0 (±2.27) | 32.4 (±5.75) | 0.037 | 25.2 (±2.20) |
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| 49.7% | 47.2% | 57.3% | <0.007 | 51.4% |
| (±2.8) n = 148 | (±2.8),n = 143 | (±2.9) n = 148 | (±1.6) n = 439 | ||
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| 36.5% | 35.1% | 41.6% (±3.2) | <0.043 | 37.8% (±1.7) |
| (±2.8) n = 88 | (±2.7) n = 95 | n = 46 | n = 229 | ||
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| 33.8% (±2.8) n = 68 | 29.7% (±2.7) n = 45 | 38.5% (±3.4) n = 50 | < 0.037 | 33.4% (±1.7), n = 113 |
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| 83.1 (1.02 – 257.97) | 66.4 (1.02 – 212.99) | 34.7 (1.0 - 111.97) | 58.8 (1.02 – 257.97) | |
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| Not reached | Not reached | Not reached | Not reached | |
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| 47.0 (±5.7) | 28.0 (±5.7) | 33.0 (±7.0) | 0.313 | 34.3 (±4.1) |
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| 86.9% (±2.8) | 79.5% (±3.1) | 83.6% (±2.9) | 0.188 | 83.2% (±1.7) |
| n = 119 | n = 129 | n = 124 | n = 372 | ||
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| 68.7% (±4.0) | 61.9% (±3.9) | 68.7% (±4.0) | 0.340 | 65.7% (±2.3) |
| n = 78 | n = 90 | n = 42 | n = 210 | ||
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| 61.9% (±4.4) | 54.3% (±4.1) | -- | 0.270 | 59.0% (±2.6) |
| n = 60 | n = 44 | n = 104 | |||
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| 10.5% (±2.8) | 16.1% (±3.1) | 18.9% (±3.3) | 0.074 | 15.5% (±1.8) |
| n = 13 | n = 23 | n = 28 | n = 64 | ||
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| 49.5% (±6.7) | 46.4% (±4.0) | 38.2% (±4.4) | 0.523 | 49.6% (±5.4) |
| n = 59 | n = 74 | n = 55 | n = 188 | ||
Overview of stage, overall survival and tumour-free survival of 550 tumour-free patients after initial therapy stratified for neoadjuvant systemic therapy
| Perioperative vs. no perioperative therapy (n = 550) | |||
|---|---|---|---|
| Perioperative therapy | No perioperative therapy | P | |
| n = 64 | n = 486 | ||
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| 24 | 224 | 0.47 |
| (37.5%) | (46.1%) | ||
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| 28 | 197 | |
| (43.8%) | (40.5%) | ||
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| 11 | 56 | |
| (17.2%) | (11.5%) | ||
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| 1 | 9 | |
| (1.6%) | (1.9%) | ||
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| Not reached | Not reached | 0.41 |
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| 28.9% (±6.1) | 36%.9 (±4.4) | |
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| 17.0 (±5.5) months | 25.0 (±2.5) months | 0.82 |
Figure 1Survival. a) Overall survival among the different time periods of patients without 30-day mortality (n = 1072). b) Overall survival after R0 resection/vs. residual tumour. c-e) Survival among the different time periods based on UICC staging system.
Figure 2Peritoneal carcinomatosis. a) Cumulative hazard ratio for the development of metaPC (550 after R0 resection, stratified for the three time periods.) b) Tumour related overall survival of 167 patients with synchronous peritoneal carcinomatosis (synPC) stratified for time periods I and III. c) Tumour related overall survival from the time of diagnosis metachronous peritoneal carcinomatosis (metaPC) in the group of 550 patients that were R0 after initial therapy.
Analysis using Cox regression model for independent risk factors after R0 D2 gastrectomy (n = 550)
| Risk factors for metachronous peritoneal carcinomatosis | |||
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| Risk factor | P | Factor* (CI 95% confidence interval) | |
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| T3/4 (serosapositive) | 0,003 | 2,35 (1,35 - 4,12) |
| Signet ring cell | 0,004 | 3,88 (1,56 - 9,71) | |
| Nodal positive | 0,003 | 2,39 (1,34 - 4,26) | |
| Grading 3/4 | 0,018 | 2,03 (1,13 - 3,65) | |
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| Time period (I) | 0,247 | 1,39 (0,69 - 2,81) |
| Age (<50y) | 0,776 | 0,82 (1,65 - 0,41) | |
| Sex (male) | 0,399 | 1,25 (2,08 - 0,75) | |
| Perioperative chemotherapy | 0,392 | 0,68 (1,64 - 0,28) | |
*Is the factor by witch the risk for development of metachronous PC is increased.
Figure 3Cox regression multivariate analysis for independent risk factors for the development of metaPC. X-axis shows the factor by which the risk is influenced (logarithmic diagram). P-Values and risk factors are summarized in the table below the graph.