| Literature DB >> 16879751 |
Jozien Helleman1, Iris L van Staveren, Winand N M Dinjens, Patricia F van Kuijk, Kirsten Ritstier, Patricia C Ewing, Maria E L van der Burg, Gerrit Stoter, Els M J J Berns.
Abstract
BACKGROUND: The treatment of ovarian cancer is hindered by intrinsic or acquired resistance to platinum-based chemotherapy. The aim of this study is to determine the frequency of mismatch repair (MMR) inactivation in ovarian cancer and its association with resistance to platinum-based chemotherapy.Entities:
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Year: 2006 PMID: 16879751 PMCID: PMC1557864 DOI: 10.1186/1471-2407-6-201
Source DB: PubMed Journal: BMC Cancer ISSN: 1471-2407 Impact factor: 4.430
Figure 1The mismatch repair system (MMR). A. Based on figure 3 from Bellacosa et al [8]. Initiation of MMR by recognizing the DNA damage by the MutSα or β complex and recruiting the MutLα complex. B. Excision of the damaged strand and resynthesis in which exonuclease ExoI, proliferating cell nuclear antigen (PCNA), DNA polymerase δ or ε and DNA helicase I are suggested to play a role.
Patient and tumor characteristics.
| Patient and tumor characteristics | No. of patients |
| FIGO stage | |
| Early (I-IIA) | 20 |
| Advanced (IIB-IV) | 45 |
| Unknown | 10 |
| Histological type | |
| Serous adenocarcinoma | 36 |
| Endometrioid adenocarcinoma | 13 |
| Mucinous adenocarcinoma | 10 |
| Clear cell adenocarcinoma | 3 |
| Mixed Mullerian Tumor | 8 |
| Poorly differentiated | 3 |
| Unknown | 2 |
| Tumor grade | |
| 1 | 12 |
| 2 | 29 |
| 3 | 27 |
| Unknown | 7 |
| Residual disease | |
| None | 25 |
| ≤ 1 cm | 15 |
| > 1 cm | 22 |
| Unknown | 13 |
| Chemotherapy | |
| Cisplatin & endoxan | 45 * |
| Carboplatin & endoxan | 1 * |
| Other, not platinum containing | 5 |
| No chemotherapy | 11 |
| Unknown | 12 |
| * Response to platinum-based chemotherapy | |
| No response | 11 |
| Response | 34 |
| Unknown | 1 |
| Total | 75 |
Figure 2Study design. Flow chart for study design.
Figure 3The mRNA expression data for A. eight ovarian cancer cell lines, and B. 50 ovarian carcinomas. The ovarian cancer cell lines and the ovarian carcinomas are ordered according to their cisplatin and platinum-based chemotherapy response. The MMR status deducted from the mRNA expression levels is given for the carcinomas (1: active, 0: inactive). The mRNA expression is shown in the heatmap (green color: low expression (25th percentile calculated per gene), black: median expression, red color: high expression (75th percentile calculated per gene), gray: no value). Depicted next to the heatmap is: the MLH1 promoter methylation status (black: complete or high level, gray: low level, white: no methylation, X: unknown), the microsatellite stability (black: instable, white: stable, X: unknown), the cisplatin response (Figure 3A; IC50 in nM) or platinum-based chemotherapy response (Figure 3B; black: non-responders, white: responders, X: unknown) and the histology (PD: poorly differentiated, SE: serous, CC: clear cell, MU: mucinous, EN: endometrioid, MM: mixed mullerian). Cell lines and carcinomas are ordered according to their cisplatin response or platinum-based chemotherapy response respectively.
Summary of the literature: Frequency of MSI in ovarian cancer. The total number of MSI, the number of MS markers used for the analysis and the number of MSI per histological subtype (if mentioned) is given for each study.
| MSI | MS markers | Histology | ||||||||
| NCI-CP | total | SE | EN | CC | MU | MM | PD | |||
| Helleman et al. | 0/75 | (0%) | 2 | 2 | 0/36 (0%) | 0/13 (0%) | 0/3 (0%) | 0/10 (0%) | 0/8 (0%) | 0/3 (0%) |
| Mesquita et al.2005 | 0/34 | (0%) | 1 | 2 | 0/26 (0%) | - | 0/8 (0%) | - | - | - |
| Gifford et al. 2004 | 2/138 | (1%) | 3 | 6 | Not mentioned | |||||
| Catasus et al. 2004 | 5/54 | (9%) | 5 | 5 | EN, CC and MM histology | |||||
| Cai et al.2004 | 6/42 | (14%) | 5 | 5 | - | - | 6/42 (14%) | - | - | - |
| Liu et al.2004 | 15/74 | (20%) | 4 | 4 | - | 15/74 (20%) | - | - | - | - |
| Singer et al.2004 | 6/75 | (8%) | 5 | 11 | 5/53 (9%) | 1/14 (7%) | 0/3 (0%) | 0/5 (0%) | - | - |
| Geisler et al.2003 | 21/125 | (17%) | 5 | 6 | 10/69 (14%) | 6/22 (27%) | 0/4 (0%) | 2/9 (22%) | - | 1/2 (50%) |
| Watanabe et al. 2001 | 2/24 | (8%) | 5 | 10 | Not mentioned | |||||
| Sood et al. 2001 | 13/109 | (12%) | 5 | 14 | Not mentioned | |||||
| Gras et al.2001 | 7/76 | (9%) | 5 | 10 | 0/17 (0%) | 1/48 (2%) | 1/8 (13%) | 0/2 (0%) | 0/6 (0%) | - |
| Buller et al. 2001 | 22/56 | (39%) | 5 | 6 | Not mentioned | |||||
| Chiaravalli et al.2001 | 3/16 | (19%) | 2 | 3 | 0/8 (0%) | 1/2 (50%) | - | 2/4 (50%) | - | 0/2 (0%) |
| Ohwada et al.2000 | 15/61 | (25%) | 1 | 5 | 4/32 (13%) | - | - | 11/29 (38%) | - | - |
| Allen et al.2000 | 1/25 | (4%) | 2 | 4 | 1/16 (6%) | 0/2 (0%) | 0/2 (0%) | 0/1 (0%) | - | 0/4 (0%) |
| Colella et al. 1998 | 3/20 | (15%) | 0 | 3 | Not mentioned | |||||
| Sood et al. 1997 | 13/78 | (17%) | 1 | 9 | Not mentioned | |||||
| Sood et al. 1996 | 11/68 | (16%) | 1 | 9 | 34 serous and 34 not serous | |||||
| Tangir et al.1996 | 2/31 | (6%) | 0 | 13 | 2/31 (6%) | - | - | - | - | - |
| Arzimanoglou et al. 1996 | 11/90 | (12%) | 1 | 3 | Not mentioned | |||||
| Fujita et al.1995 | 7/44 | (16%) | 0 | 4 | 2/22 (9%) | 5/10 (50%) | 0/4 (0%) | 0/8 (0%) | - | - |
| Total | 165/1315 | (13%) | 24/310 (8%) | 29/185 (16%) | 7/74 (9%) | 15/68 (22%) | 0/14 (0%) | 1/11 (9%) | ||
Abbreviations: SE serous, EN endometrioid, CC clear cell, MU mucinous, MM mixed mullerian, PD poorly differentiated, - not present, MS microsatellite, NCI-CP National Cancer Institute Consensus Panel.