| Literature DB >> 25884643 |
Viktor H Koelzer1,2, Pia Herrmann3, Inti Zlobec4, Eva Karamitopoulou5,6, Alessandro Lugli7,8, Ulrike Stein9,10.
Abstract
BACKGROUND: Metastasis of colorectal cancer (CRC) is directly linked to patient survival. We previously identified the novel gene Metastasis Associated in Colon Cancer 1 (MACC1) in CRC and demonstrated its importance as metastasis inducer and prognostic biomarker. Here, we investigate the geographic expression pattern of MACC1 in colorectal adenocarcinoma and tumor buds in correlation with clinicopathological and molecular features for improvement of survival prognosis.Entities:
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Year: 2015 PMID: 25884643 PMCID: PMC4371627 DOI: 10.1186/s12885-015-1150-z
Source DB: PubMed Journal: BMC Cancer ISSN: 1471-2407 Impact factor: 4.430
Figure 1Study design. 220 CRC patients with full clinicopathological features were entered into the study. Cases were analyzed for BRAF and KRAS mutations and MMR-protein expression was determined. Tumors of the CpG-Island methylator phenotype were identified using pyrosequencing. MACC1 protein expression in normal mucosa, tumor center, tumor front and tumor buds was evaluated by immunohistochemistry using full tissue sections. MACC1 expression in each geographic area of CRC was analyzed with clinicopathological features, patient survival and molecular features.
Patient characteristics and association of MACC1 expression in the tumor center with clinicopathological data
| Characteristics | Total (n = 187) | MACC1 tumor center N (%); (n = 187) | P-value | |
|---|---|---|---|---|
| Low (Score 0) | High (Score 1–3) | |||
| N = 78 (41.7%) | N = 109 (58.3%) | |||
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| Mean (min, max) | 68.6 (35–93) | 69.2 (36–93) | 68.1 (35–91) | 0.1732 |
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| Mean (min, max) | 4.5 (1.2–12) | 4.8 (2–12) | 4.3 (1.2–8) | 0.5723 |
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| Male | 88 (47.3) | 35 (44.9) | 53 (49.1) | 0.5711 |
| Female | 98 (52.7) | 43 (55.1) | 55 (50.9) | |
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| Non-mucinous | 167 (89.3) | 70 (89.7) | 97 (89.0) | 0.8695 |
| Mucinous | 20 (10.7) | 8 (10.3) | 12 (11.0) | |
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| G1-2 | 120 (64.2) | 55 (70.5) | 65 (59.6) | 0.126 |
| G3 | 67 (35.8) | 23 (29.5) | 44 (40.4) | |
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| Left | 113 (60.7) | 42 (53.9) | 71 (65.7) | 0.2027 |
| Rectum | 21 (11.3) | 9 (11.5) | 12 (11.1) | |
| Right | 52 (28.0) | 27 (34.6) | 25 (23.2) | |
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| pT1 + pT2 | 47 (25.1) | 26 (33.3) | 21 (19.3) | 0.0288 |
| pT3 + pT4 | 140 (74.9) | 52 (66.7) | 88 (80.7) | |
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| pN0 | 97 (51.9) | 51 (65.4) | 46 (42.2) | 0.0018 |
| pN1-2 | 90 (48.1) | 27 (34.6) | 63 (57.8) | |
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| pM0 | 167 (89.8) | 73 (93.6) | 94 (87.0) | 0.1454 |
| pM1 | 19 (10.2) | 5 (6.4) | 14 (13.0) | |
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| Stage I | 40 (21.5) | 26 (33.3) | 14 (13.0) | 0.0023 |
| Stage II | 53 (28.5) | 24 (30.8) | 29 (26.9) | |
| Stage III | 74 (39.8) | 23 (29.5) | 51 (47.2) | |
| Stage IV | 19 (10.2) | 5 (6.4) | 14 (13.0) | |
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| Low-grade | 101 (54.0) | 54 (69.2) | 47 (43.1) | 0.0004 |
| High-grade | 86 (46.0) | 24 (30.8) | 62 (56.9) | |
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| Present | 32 (17.1) | 8 (10.3) | 24 (22.0) | 0.0352 |
| Absent | 155 (82.9) | 70 (89.7) | 85 (78.0) | |
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| Present | 74 (39.6) | 24 (30.8) | 50 (45.9) | 0.0373 |
| Absent | 113 (60.4) | 54 (69.2) | 59 (54.1) | |
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| Untreated | 66 (35.3) | 39 (50.0) | 27 (24.8) | 0.0004 |
| Treated | 121 (64.7) | 39 (50.0) | 82 (75.2) | |
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| Proficient | 170 (91.4) | 71 (91.0) | 99 (91.7) | 0.8777 |
| Deficient | 16 (8.6) | 7 (9.0) | 9 (8.3) | |
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| Wild-type | 124 (67.0) | 54 (70.1) | 70 (64.8) | 0.4484 |
| Mutation | 61 (33.0) | 23 (29.9) | 38 (35.2) | |
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| Wild-type | 165 (91.2) | 69 (92.0) | 96 (90.6) | 0.7378 |
| Mutation | 16 (8.8) | 6 (8.0) | 10 (9.4) | |
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| Negative/Low | 90 (87.4) | 40 (90.9) | 50 (84.8) | 0.3887 |
| High | 13 (12.6) | 4 (9.1) | 9 (15.3) | |
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| Median | 60 (50-ne) | Not reached | 58 (43-ne) | 0.2585 |
ne = survival endpoint not reached.
Figure 2MACC1 protein expression analysis in CRC. A: MACC1 expression in normal mucosa (1), tumor center (2), tumor front (3) and tumor buds (4; arrows) was evaluated by immunohistochemistry. B: Four representative cases of colorectal adenocarcinoma showing a significant increase of MACC1 expression from the tumor center towards the invasive front and MACC1 over-expressing tumor budding cells.
Association of MACC1 expression in the tumor front and tumor buds with clinicopathological data
| Characteristics | MACC1 tumor front N (%); (n = 187) | P-value | MACC1 tumor buds N (%); (n = 187) | P-value | ||
|---|---|---|---|---|---|---|
| Low (Score 0) | High (Score 1–3) | Low (<median) | High (>median) | |||
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| Mean (min, max) | 69.9 (38–88) | 68.1 (35–93) | 0.1141 | 70.1 (36–89) | 67.6 (41–91) | 0.0408 |
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| Mean (min, max) | 5.0 (2–12) | 4.4 (1.2–8.0) | 0.4457 | 4.6 (2–12) | 4.5 (1.2–8) | 0.7134 |
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| Male | 18 (35.3) | 70 (51.9) | 0.0436 | 23 (46.0) | 32 (45.1) | 0.9195 |
| Female | 33 (64.7) | 65 (48.2) | 27 (54.0) | 39 (54.9) | ||
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| Non-mucinous | 46 (90.2) | 121 (89.0) | 0.8092 | 45 (90.0) | 61 (85.9) | 0.502 |
| Mucinous | 5 (9.8) | 15 (11.0) | 5 (10.0) | 10 (14.1) | ||
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| G1-2 | 36 (70.6) | 84 (61.8) | 0.2624 | 30 (60.0) | 35 (49.3) | 0.2449 |
| G3 | 15 (29.4) | 52 (38.2) | 20 (40.0) | 36 (50.7) | ||
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| Left | 27 (52.9) | 86 (63.7) | 0.3547 | 30 (60.0) | 43 (61.4) | 0.7867 |
| Rectum | 6 (11.8) | 15 (11.1) | 7 (14.0) | 7 (10.0) | ||
| Right | 18 (35.3) | 34 (25.2) | 13 (26.0) | 20 (28.6) | ||
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| pT1 + pT2 | 22 (43.1) | 25 (18.4) | 0.0005 | 15 (30.0) | 3 (4.2) | <0.0001 |
| pT3 + pT4 | 29 (56.9) | 111 (81.6) | 35 (70.0) | 68 (95.8) | ||
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| pN0 | 38 (74.5) | 59 (43.4) | 0.0001 | 26 (52.0) | 24 (33.8) | 0.0453 |
| pN1-2 | 13 (25.5) | 77 (56.6) | 24 (48.0) | 47 (66.2) | ||
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| pM0 | 50 (98.0) | 117 (86.7) | 0.0223 | 47 (94.0) | 60 (85.7) | 0.1499 |
| pM1 | 1 (2.0) | 18 (13.3) | 3 (6.0) | 10 (14.3) | ||
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| Stage I | 22 (43.1) | 18 (13.3) | <0.0001 | 13 (26.0) | 1 (1.4) | 0.0004 |
| Stage II | 15 (29.4) | 38 (282.) | 12 (24.0) | 20 (28.6) | ||
| Stage III | 13 (25.5) | 61 (45.2) | 22 (44.0) | 39 (55.7) | ||
| Stage IV | 1 (2.0) | 18 (13.3) | 3 (6.0) | 10 (14.3) | ||
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| Low-grade | 38 (74.5) | 63 (46.3) | 0.0006 | 28 (56.0) | 20 (28.2) | 0.0021 |
| High-grade | 13 (25.5) | 73 (53.7) | 22 (44.0) | 51 (71.8) | ||
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| Present | 3 (5.9) | 29 (21.3) | 0.0125 | 7 (14.0) | 19 (26.8) | 0.0924 |
| Absent | 48 (94.1) | 107 (78.7) | 43 (86.0) | 52 (73.2) | ||
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| Present | 11 (21.6) | 63 (46.3) | 0.002 | 24 (48.0) | 38 (53.5) | 0.5496 |
| Absent | 40 (78.4) | 73 (53.7) | 26 (52.0) | 33 (46.5) | ||
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| Untreated | 29 (56.9) | 37 (27.2) | 0.0002 | 24 (48.0) | 9 (12.7) | <0.0001 |
| Treated | 22 (43.1) | 99 (72.8) | 26 (52.0) | 62 (87.3) | ||
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| Proficient | 44 (86.3) | 126 (93.3) | 0.1256 | 46 (92.0) | 63 (90.0) | 0.7607 |
| Deficient | 7 (13.7) | 9 (6.7) | 4 (8.0) | 7 (10.0) | ||
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| Wild-type | 32 (64.0) | 92 (68.2) | 0.594 | 33 (66.0) | 46 (65.7) | 0.974 |
| Mutation | 18 (36.0) | 43 (31.9) | 17 (34.0) | 24 (34.3) | ||
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| Wild-type | 45 (90.0) | 120 (91.6) | 0.772 | 44 (89.8) | 60 (89.6) | 0.966 |
| Mutation | 5 (10.0) | 11 (8.4) | 5 (10.2) | 7 (10.5) | ||
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| Negative/Low | 27 (90.0) | 63 (86.3) | 0.7514 | 21 (84.0) | 36 (83.7) | 1.0 |
| High | 3 (10.0) | 10 (13.7) | 4 (16.0) | 7 (16.3) | ||
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| Median | Not reached | 58 (43-ne) | 0.0217 | 53.0 (43–61) | 55.0 (36-ne) | 0.839 |
ne = survival endpoint not reached.
Figure 3Prognostic effects of MACC1 expression at the invasive front of CRC. MACC1 overexpression at the tumor front is a significant adverse prognostic indicator (p = 0.0217) in univariate survival analysis.
Multivariable Cox-regression analysis of MACC1 expression at the tumor front TNM-stage and adjuvant therapy
| Parameter | HR (95%CI) | P-value | |
|---|---|---|---|
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| Low (Score 0) | 1.0 | 0.7827 | |
| High (Score 1–3) | 1.1 (0.56-2.16) | ||
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| pT1-2 | 1.0 | 0.3425 | |
| pT3-4 | 1.52 (0.64-3.57) | ||
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| pN0 | 1.0 | 0.0003 | |
| pN1-2 | 3.48 (1.77-6.85) | ||
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| pM0 | 1.0 | <0.0001 | |
| pM1 | 4.12 (2.2-7.68) | ||
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| None | 1.0 | 0.3284 | |
| Treated | 0.74 (0.4-1.36) | ||