Abstract
Purpose
About 10 to 15% of patients with sporadic colorectal cancer display mutations in DNA mismatch repair (MMR) genes shown as microsatellite instability (MSI). Previous reports of colorectal cancer (CRC) indicate a better prognosis for patients with MSI tumors compared to patients with microsatellite stable (MSS) tumors. In this study, our aim was to investigate whether MSI is an independent prognostic factor in CRC.
Patients and methods
Patients with stage I–III colorectal cancer and subject to curative surgery during 2002–2006 in the Swedish low-risk colorectal cancer study group cohort were eligible for inclusion. Deficient MMR (dMMR) status was analyzed by immunohistochemistry (IHC) and/or by MSI testing with polymerase chain reaction (PCR). Prognostic follow-up and treatment data were retrieved from patient records. Statistical analyses to assess MSI-status and prognosis were done using logistic regression and survival analyses using the Kaplan-Meier method and Cox regression hazards models adjusted for age, sex, stage, comorbidity, and tumor location.
Results
In total, 463 patients were included, MSI high tumors were present in 66 patients (14%), and the remaining 397 were MSS/MSI low. Within 6 years, distant recurrences were present in 9.1% and 20.2% (P = 0.049), and death occurred in 25.8% and 31.5% in MSI and MSS patients, respectively. There was no statistically significant difference in overall mortality (HR 0.80, 95% CI 0.46–1.38), relapse-free survival (HR 0.82, 95% CI 0.50–1.36), or cancer-specific mortality (HR 1.60, 95% CI 0.73–3.51).
Conclusion
Despite distant metastases being less common in patients with MSI, there was no association between MSI and overall, relapse-free, or cancer-specific survival.
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Introduction
Inactivation of the DNA mismatch repair (MMR) system leads to an accumulation of mutations in the short repeating base pair units called microsatellites [1]. This accumulation of errors renders the microsatellite instability (MSI) phenotype, sometimes also referred to as the hypermutator phenotype [2]. In sporadic colorectal cancer (CRC), this is mainly due to epigenetic inactivation of the MMR genes, most commonly MLH1, while in the hereditary condition of Lynch’s syndrome (LS), it is caused by germline mutations [3,4,5]. LS attributes to about 3% of the CRC cases, and MSI is present in 10–15% of the sporadic cases of CRC [6,7,8]. Common clinical and pathological features of deficient mismatch repair (dMMR) CRCs include proximal tumor location, extensive tumor-infiltrating lymphocytes, higher T-stage, and poor differentiation [9]. The detection of MMR status and MSI is mainly done by immunohistochemistry (IHC) and PCR-based MSI testing, and the concordance between the methods is high and well documented [10,11,12].
When discussing the prognostic impact of MSI in CRC, one must also address the predictive value of MSI regarding chemotherapy, since a vast majority of studies come from different adjuvant trials. Several earlier studies suggested a better stage-adjusted survival for patients with MSI versus MSS tumors [13,14,15,16,17]. In a pooled analysis of stage II–III patients, MSI was associated with an improved disease free survival (DFS) in patients naïve for chemotherapy [18]. Non-interventional studies of the association between MSI and prognosis following chemotherapy are contradictive [18, 19]. The largest pooled study including patients from several different randomized 5-Fu based adjuvant treatment trials concluded that patients with MSI tumors had reduced recurrence rates, delayed time to relapse, and fewer distant recurrences [20]. Also, the rate of distant recurrences was reduced in MSI patients with stage III disease receiving adjuvant 5-Fu treatment implying a benefit for chemotherapy in MSI patients. It must be mentioned that only a subset of patients from these trials are represented in the study due to available tissue specimens. A meta-analysis of 3690 CRC patients of which 75% was stage III and investigated the predictive role of MSI in adjuvant chemotherapy treatment (mostly 5-Fu based) [21]. It showed that MSI patients that received adjuvant chemotherapy had a survival benefit compared to MSS patients. However, in analysis restricted to MSI patients, adjuvant chemotherapy was not associated with improved DFS or overall survival.
The risk of selection bias is evident in previously mentioned pooled studies since only patients with available tissue material have been eligible for inclusion. This means that patients only represent a subset of the overall study cohorts. Also, patients in many previous studies were drawn from several clinical trials conducted now 30 to 40 years ago [20].
So, despite large efforts to settle the score on the prognostic and predictive impact of MSI in CRC, the results are not concordant. In this study, we have investigated a well-defined Swedish population treated for CRC to further elucidate whether MSI could be considered an independent prognostic factor.
Method
Study population
Patients were recruited from the Swedish low-risk colorectal cancer study group, which is a national multi-center collaborative including 14 different surgical clinics in the middle of Sweden [22]. From this cohort, a subset of 484 patients with CRC treated in the Stockholm area during the years 2002–2006 were evaluated, and inclusion criteria were curative surgery for stage I–III disease, radical surgery, known MMR-status, and available follow-up. After exclusion, a total of 463 patients remained for analysis (Fig. 1). All surgical specimens were evaluated by the same pathologist, and an extended detailed morphological description was made [23]. Informed consent was obtained from all patients and approval from the local Ethics Committee in Stockholm (2017/57-31/4).
Patient records were scrutinized for treatment and follow-up data according to protocol by two investigators (P.R. and S.B.). Post-operative complications and co-morbidity according to the American Society of Anesthesiologists (ASA) Physical Status Classification System were recorded.
The cohort includes 10 patients with Lynch syndrome. These patients have not been excluded since we assume that the phenotype of MSI is the determining factor for prognosis rather than how it is acquired. Due to this, a separate sensitivity analysis was conducted. A detailed description of the Lynch syndrome patients, including the pathogenic variants, is presented in a previous study [24].
Exposure
The immunohistochemistry (IHC), MSI testing, and in part of the cases mutation screening for this cohort have been described in a previous study [24] and presented here briefly as follows.
For the IHC, analyses tissue from colorectal adenocarcinomas were used. Before analysis, the material was fixed in formalin and embedded in paraffin.
Four different monoclonal antibodies for MLH1, MSH2, MSH6, and PMS2 were used and staining done in accordance with instructions from the manufacturer.
Samples were assessed as MMR deficient if they demonstrated partial or total loss of nuclear expression in invasive cancer cells with synchronous remaining expression in normal cells, functioning as an internal positive control.
For MSI-testing, a commercial kit was used in accordance with instructions from the manufacturer. Tumor tissue embedded in paraffin was dissected before MSI-analysis. A multiplex PCR was used to amplify DNA in selected microsatellite markers, namely, BAT-26, NR-21, BAT-25, MONO-27, and NR-24. Tumors were reported as MSI-high when three or more of the five mononucleotide markers showed a pattern consistent with MSI. In addition, mutation screening was performed for part of the cases mainly using Sanger sequencing.
Outcome
The patients were followed from date of surgery until event or six years of follow-up. The main outcomes were overall survival (OS), cancer-specific survival (CSS), and relapse-free survival (RFS). The outcome of interest in the OS analyses was death whereas date of migration or end of follow-up were considered censoring events. Similarly, date of CRC cancer death was the outcome of interest in the cancer-specific survival analyses and date of relapse or death in the relapse-free survival analyses.
Statistics
Median and interquartile ranges are reported for continuous variables whereas frequencies and percentages are reported for categorical variables. The P values in descriptive tables come from Wilcoxon and Chi-squared tests for continuous and categorical variables, respectively.
Kaplan-Meier curves are compared for overall survival, recurrence free survival, and cancer-specific survival. Difference in the survival between groups of interest is tested with multiple tests, including one that accounts for crossing of survival curves.
Cox regression models are used to present unadjusted and adjusted hazard ratios for MMR-status and outcome. The adjusted analyses are adjusted for sex, age, cancer stage, comorbidity, and tumor location. P values are two sided, values below 5% are deemed significant, and 95% confidence intervals are used throughout. Proportional hazard tests were also conducted. There was no violation of the proportional hazard assumption for the analyses of overall and cancer-specific survival. However, for the analysis of relapse-free survival, there was a violation for age and stage. Hence, the multivariable model for relapse-free survival was stratified for age and stage within the Cox regression model. Analyses were performed in R version 4.1.2.
Results
Patient characteristics
A total of 463 stage I–III patients undergone R0-resection surgery were divided into two groups based on their MMR status. MSI tumors were present in 66 patients (14.2%), and the rest were MSS. The median ages were similar in the two groups (Table 1). In the MSI group, a significant predominance was seen for female gender (P = 0.016) as well as for right-sided tumor location (P < 0.001). Comorbidity according to the ASA classification did not differ.
Disease and treatment characteristics
Treatment, complications, and histopathological data are presented in Table 2. There were no significant differences related to surgical or adjuvant treatment characteristics between the MSI and MSS groups. The average number of chemo cycles was 11 in the MSI group and 10 in the MSS group. Stage II was more common among MSI patients, but otherwise, there were no significant histopathological differences. Complications were evenly distributed between the groups (Table 3).
Outcomes
There was no death within 30 or 90 days after surgery. Median follow-up time was 6 years. Within the first 6 years, 15.2% and 24.4% of the patients in the MSI and MSS groups, respectively, suffered relapse. Distant metastases were most common and present in 9.1% and 20.2% of the MSI and MSS patients, respectively (P = 0.049) (Table 3). The Kaplan-Meier curves revealed no significant difference in OS, RFS, or CSS between MSI and MSS. The 6-year OS were 74.2% and 68.5% (Fig. 2) for MSI and MSS patients, respectively, and the corresponding numbers for RFS were 69.7% and 62.5% (Fig. 3), and for CSS 74.2% and 70.1% (Fig. 4). There was no statistically significant difference in overall mortality (HR 0.80, 95% CI 0.46–1.38) or cancer-specific mortality (HR 1.60, 95% CI 0.73–3.51) or relapse-free survival (HR 0.82, 95% CI 0.50–1.36 (Table 4). Sensitivity analysis, where patients with Lynch’s syndrome (n = 10) were excluded, revealed similar results as the main analyses (data not shown).
Discussion
In this well-defined cohort of patients with stage I–III colorectal cancer, there was no significant association with MSI status and prognosis.
Previous studies of prognosis and predictive value of MSI show somewhat conflicting results. A variety of different settings in terms of patient selection, study design, and heterogeneous cohorts may affect the results and contribute to the diverging results. In studies of MSI and prognosis, selection bias is a problem. To increase the number of patients, several pooled analyses have been performed originating from randomized trials. Pooled analysis can result in counterintuitive and spurious results if data is not weighted. In a systematic review, MSI was associated with improved overall survival in patients treated with surgery alone as well as with adjuvant 5-Fu [25], which was supported by a meta-analysis that showed an improved overall survival and disease-free survival in MSI patients [26]. However, systematic reviews and meta-analysis never get better than the included data, why large cohort studies with good internal validity are preferable.
Our results failed to demonstrate a prognostic advantage of MSI regarding relapse free survival, overall survival, or cancer-specific survival, which is in line with previous studies [27,28,29]. In comparison to other well-defined cohorts, one single-center study (n = 613) reported no association between MSI status and overall survival [30]. However, relapse-free survival was significantly improved in patients with MSI and sub-group analyses revealed that improved outcome applied to stage II patients. A slightly smaller study of patients with CRC stage II–III (n = 245), where most patients received adjuvant chemotherapy, showed no association between MSI status and overall survival or disease-free survival. A sub-analysis, that should be interpreted with caution, reported an impaired prognosis in stage II MSI patients compared with MSS patients [31].
In line with previous studies, distant metastases were less common in MSI compared with MSS patients [20, 32], but there was no significant difference in relapse-free survival between the two groups. Some propose that the prognostic impact of MSI is stage dependent and substantially stronger in stage II than in stage III [33]. Despite a fairly large and well-defined cohort, we still believe that sample size prevents a trustworthy subgroup analysis.
If the independent impact of MSI in CRC was evident, additional studies on the subject would be redundant and the matter settled already. A majority of studies point in the direction of MSI as a prognostically beneficial factor, and our study does not contradict that. It is speculated that the possible prognostic advantage of MSI is related to immunosurveillance. Many other parameters seem to affect prognosis more than MSI, but it is still one piece of the puzzle to be taken into consideration. Especially in right-sided cancers, MSI may be of considerable importance, since the proportion of MSI is higher than on the left side of colon and rectum. Also, it seems that MMR status is an important factor in relation to immunotherapy treatment such as checkpoint blockade, for which we can hope for therapeutic progress in the future [34].
The problem with many studies including ours might be that MSI itself could be due to heterogenous mechanisms where the evasion of immune cells is of severe importance. The high load of mutational neoantigens in dMMR/MSI-cancers leads to a pronounced anti-tumoral response such as infiltration of CD8T cells, an important reaction within MSI tumors [35]. The immunoselection during the development of the tumor, caused by possible mechanisms mentioned above, might be an answer to diverging results, which in turns requires even more distinctive subclassification of the MSI phenomenon. Antigen expression, or the loss of it, might explain why MSI in itself is not that easily classified as one group of patients with similar mechanisms and response to immunotherapy.
This is a large cohort of colorectal cancer patients with high quality data of patient and tumor characteristics and treatment. There was no loss to follow-up, and it could be presumed that all recurrences of clinical impact have been identified. In difference from the pooled studies, the study population in the current study has been systematically collected for evaluation and is not a mix from several different trials. Hence, the risk of selection bias is low. In addition, IHC/MSI testing has been performed in a homogenous manner decreasing the risk of information bias. The patients are included from several centers in the Stockholm area, and results are most likely generalizable to Swedish patients as well as other European countries.
However, despite a comparatively large cohort, the study is still limited by its size only including 66 patients with MSI, making it impossible to analyze the effect of MSI in different subgroups. In addition, the number of patients that received chemotherapy is limited. Therefore, we have not addressed the issue of MSI as a predictive factor for chemotherapy response.
Conclusion
In this large cohort of CRC-patients, distant recurrences were less common in MSI-patients. Despite the difference in recurrences, MSI was not significantly associated with prognosis. Larger studies are needed to explore MSI as a prognostic marker, possibly in subgroups defining the effect of immune evasion, especially in the new era of immunotherapy.
Data availability
The datasets generated during and analyzed during the current study are available from the corresponding author on reasonable request.
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Acknowledgements
Great thanks to David Grannas and Laimei Yip Lundström, Division of Biostatistics, Karolinska Institutet, for statistical help and analyses.
Funding
Open access funding provided by Karolinska Institute. The project was supported financially by the Regional agreement on medical training and clinical research between the Stockholm County Council and Karolinska Institutet (ALF-project).
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Study concepts and design—Annika Linblom and Ulrik Lindforss. Data acquisition—Petri Rantanen, Shabane Barot, Anne Keränen, and Sam Ghazi. Quality control of data—Petri Rantanen, Shabane Barot, Anne Keränen, and Sam Ghazi. Data analysis and interpretation—Petri Rantanen, Caroline Nordenvall, Anne Keränen, and Annelie Liljegren. Statistical analysis—Petri Rantanen and Caroline Nordenvall. Figures and tables—Petri Rantanen and Caroline Nordenvall. Manuscript preparation—Petri Rantanen, Caroline Nordenvall, and Ulrik Lindforss. Manuscript editing and review—all authors.
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Rantanen, P., Keränen, A., Barot, S. et al. The prognostic significance of microsatellite instability in colorectal cancer: a Swedish multi-center study. Int J Colorectal Dis 38, 197 (2023). https://doi.org/10.1007/s00384-023-04480-z
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DOI: https://doi.org/10.1007/s00384-023-04480-z