Abstract
Purpose
The role of mean platelet volume (MPV) as a predictor of outcomes in various cancer entities including colorectal cancer (CRC) has already been analyzed. However, data on the prognostic and predictive value of MPV in CRC over multiple lines of systemic therapy are missing.
Methods
In this retrospective single-center cohort study, 690 patients with UICC stage II, III or IV CRC receiving adjuvant and/or palliative chemotherapy were included. Primary endpoints in the adjuvant, palliative and best supportive care (BSC) setting were 3-year recurrence-free survival (RFS), 6-months progression-free survival (PFS), and 6-months overall survival (OS), respectively. Kaplan–Meier estimators, log-rank tests, and uni- and multivariable Cox models were used to analyze RFS, PFS and OS. A cut-off defining patients with low MPV was chosen empirically at the 25th percentile of the MPV distribution in the respective treatment setting.
Results
Three-year RFS was 76%. Median 6-month PFS estimates in 1st, 2nd and 3rd line therapy were 59, 37 and 27%, respectively. Median 6-month OS in BSC was 31%. Small platelets as indicated by low MPV did not predict for shorter RFS. In the first 3 palliative treatment lines a consistent association between low MPV and decreased 6-month PFS was not observed. In the BSC setting, patients with low MPV had numerically but not significantly shorter OS. Higher MPV levels did not consistently predict for ORR or DCR across the first 3 palliative treatment lines.
Conclusion
Small platelets are not predicting CRC outcomes, and thus are hardly useful for influencing clinical decision making.
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Introduction
Colorectal cancer (CRC) is the third most common cancer among both men and women. However, due to changes in risk factors and the increased attendance in screening programs in developed countries, incident rates have been declining over the last years [1]. Nevertheless, 30% of patients with UICC stage II or III experience recurrence after resection in curative intention, 80% of which have stage III disease at diagnosis [2]. Approximately 20% of all patients present with initially metastasized UICC stage IV disease at diagnosis [3]. Therefore, it is crucial to find cost-effective and reliable prognostic biomarkers to identify patients at high risk of local or distant recurrence as well as for outcome prediction in metastasized CRC [4].
Mean platelet volume (MPV), a marker for platelet activation, is easily available in routine blood tests and has already been demonstrated to be a predictor of thrombotic events in patients with cardiovascular and cerebrovascular disease [5]. Furthermore, an association of MPV and the risk for venous thromboembolism in cancer patients has been found [6]. Evidence suggests that activated platelets might also play an important role in tumor progression by interacting with various cell types and participating in tumor proliferation related processes [7]. In addition, platelets have been shown to promote cancer angiogenesis by releasing angiogenic growth factors such as vascular endothelial growth factor (VEGF) [8].
Altered MPV has previously been analyzed as a prognostic and predictive biomarker for various tumor entities including cancers of the lung, bladder, kidney, endometrium, stomach and pancreas [9,10,11,12,13,14]. In CRC it has been shown that a higher level of MPV relates to the presence of this cancer entity, shorter overall survival (OS) and detrimental effects on progression-free survival (PFS) [15,16,17,18]. However, to the best of our knowledge MPV and its impact on the recurrence- free survival in the adjuvant setting as well as its prognostic and predictive value over multiple palliative treatment lines and best supportive care have not been investigated yet. The aim of this study is to fill this gap and evaluate the predictive and prognostic potential of pretreatment MPV in both the adjuvant and palliative setting in CRC.
Methods
Study design and patients
In this single-center observational cohort study, we retrospectively included patients with histologically-confirmed non-metastatic (UICC stage II and III) and metastatic (UICC stage IV) carcinomas of the colon or rectum who were referred to our department (Division of Oncology, Department of Internal Medicine, Medical University of Graz, Austria) between Jan, 1st, 2010 and March, 1st 2016. From these 1054 patients, we excluded 364 patients according to pre-defined criteria (Supplementary Fig. 1). Data at baseline were extracted from the electronic health record system of our hospital trust (which includes all public hospitals in the Austrian county of Styria), the internal documentation system of our department, and from paper-chart archives of our hospital. MPV results derived from routine laboratory analyses of whole blood samples drawn into EDTA-coated collection tubes (Vacuette®, Greiner Bio-One, Kremsmünster, Austria). MPV was computed as the ratio of plateletcrit (PCT) to the number of platelets (PLT). In detail, PLT is determined via impedance after hydrodynamic cell focusing, while PCT results from the summation of the single impulses during PLT measurement. All measurements were performed on analyzers by Sysmex®, during that 6-year span various models (XN-1000™, XE-5000™) were used in the local clinical laboratory. The models do not differ in method of detection. For patients with metastatic disease, we extracted MPV values from the day of treatment initiation (for each one of the first three systemic treatment lines and at the timepoint of Best Supportive Care (BSC) initiation). For patients with non-metastatic disease, we extracted MPV values which were closest to the time of histological tumor diagnosis (within 1 week before and at a maximum of 2 weeks after histological diagnosis), but always before definitive surgery.
Endpoints
We defined the date of definitive surgery as the baseline date for patients with non-metastatic tumors. In the metastatic setting, we defined start date of the respective chemotherapy line (1st, 2nd, and 3rd) or date of BSC initiation as the baseline date, respectively. Co-Primary endpoints were Recurrence-Free Survival (RFS) in the non-metastatic setting, Progression-Free Survival (PFS) in the first three treatment lines in the metastatic setting, and Overall Survival (OS) in Best Supportive Care (BSC). Follow-up was truncated at 3 years for RFS analyses, and at 6 months for PFS and OS analyses, respectively.
Ethics statement
The study was approved by the local ethics committee (Ethikkommission der Medizinischen Universität Graz, IRB00002556) prior any patient-related activities were performed (No. 25-458 ex 12/13). Written informed consent was not obtained from individual patients, because the local ethics committee specifically granted a “waiver of consent” for this retrospective database study. All investigations have been in accordance with the principles embodied in the declaration of Helsinki.
Statistical analysis
All statistical analyses were performed using Stata (Windows version 15.0, Stata Corp., Houston, TX, USA). Continuous variables were summarized as medians [25th–75th percentile], whereas categorical variables were reported as absolute counts (%). The association between response rates and MPV under study were analyzed with uni- and multivariable generalized linear models from the Bernoulli family with an identity link. Median follow-up was estimated with a reverse Kaplan–Meier (KM) estimator according to Schemper and Smith. PFS and OS was estimated with KM estimators, compared between two groups using log-rank tests, and modelled with uni- and multivariable Cox proportional hazards models. For dichotomization of MPV (necessary for all figures), an empirical cut-off at the 25th percentile of the MPV distribution in the respective treatment setting was used.
Results
Analysis at baseline
In total, 690 patients were included in the analysis of which 425, 231, 117, 55 and 212 patients accounted for the adjuvant, 1st-line metastatic, 2nd-line metastatic, 3rd-line metastatic, and BSC setting, respectively (Table 1). The average MPV levels were highly similar across all treatment settings (Table 1).
Analysis of response patterns in the 1st to 3rd-line metastatic setting and their association with MPV
Objective response rates (ORR) were 33% (95% CI 27–40) in 1st-line therapy, 24% (16–34) in 2nd-line therapy, and 19% (8–33) in 3rd-line therapy, respectively (Supplementary Fig. 2). Corresponding disease control rates (DCR) were 65% (58–72), 57% (47–67), and 42% (27–58), respectively. Higher MPV levels did not consistently predict for ORR or DCR across treatment lines, and this prevailed in multivariable analysis adjusting for polychemotherapy (Table 2).
Uni- and multivariable analysis of clinical outcomes across treatment settings
Median PFS was not reached in 1st-line, 4.8 months in 2nd-line, and 4.1 months in 3rd-line therapy, respectively. 9-month PFS was 59% (52–65), 37% (28–46) and 27% (15–41) in 1st-line, 2nd-line, and 3rd-line therapy, respectively. Median OS was 2.6 month in BSC, and 6-month OS in BSC was 31% (23–40, Supplementary Fig. 3). Median RFS was not reached in the adjuvant setting, while 3-year RFS was 76% (72–81, Supplementary Fig. 4).
Three-year RFS was highly similar in patients with low MPV (as defined by an empirical cut-off < the 25th percentile (< Q1) of its distribution) and patients with MPV above this cut-off, respectively (log-rank p = 0.566, Fig. 1). In univariable Cox regression, MPV levels were not associated with the rate of recurrence [Hazard Ratio (HR) per 1 fL increase in MPV = 0.96, 95% CI 0.82–1.12, p = 0.600, Table 3]. This result prevailed after multivariable adjustment for stage III disease (Adjusted HR = 0.95, 0.81–1.12, p = 0.556, Table 3).
Rates of progression in 1st- to 3rd-line therapy were higher in patients with low MPV (as defined by an empirical cut-off < the 25th percentile (< Q1) of its distribution in the respective treatment setting) than in patients above this cut-off (Fig. 2a–c), although this did only reach statistical significance in the 2nd-line setting. This pattern was confirmed in uni- and multivariable Cox regression, where higher MPV levels were numerically but not statistically significantly associated with a lower rate of progression in 1st- to 3rd-line metastatic settings, as well as BSC, respectively (Table 3 and Fig. 3).
Discussion
Previous studies have already analyzed MPV and its potential role as a diagnostic and prognostic biomarker in different disease and treatment settings in CRC [16,17,18,19]. However, there is a lack of information on MPV and its impact on recurrence in the adjuvant setting as well as its association with outcome in metastatic CRC over multiple systemic treatment lines. In our study, pretreatment MPV was neither a predictor for RFS in patients undergoing potentially curative resection nor significantly associated with shorter PFS in metastasized CRC, except for 2nd line treatment. Patients in BSC with MPV below the 25th percentile had numerically but not significantly shorter OS. There was no consistent influence on clinical response rates (ORR and DCR) in patients receiving 1st, 2nd and 3rd line palliative treatment, respectively.
Platelets enhance tumor progression as they carry multiple granules containing growth factors, chemokines and proteases and form a shield around tumor cells preventing them from the immune response of natural killer cells [8]. In addition, they carry prothrombotic and proinflammatory mediators and are involved in inflammatory processes and diseases [5]. MPV is a marker of platelet size and raises due to enhanced platelet activation and inflammation, the last of which plays a major role in cancer progression [5, 20]. Markers of inflammation were already shown to relate to cancer prognosis and clinical response in metastatic CRC [21], but although an increase of MPV in some cancer entities is assumed to be the result of cancer related inflammation [13, 19, 22, 23], the observation of decreased platelet size in cancer may also be explained by cancer-associated platelet activation and exhaustion [24]. Small platelets and consequently low MPV might be the result of further enhanced inflammation and a high consumption of large activated platelets at the tumor site, causing the release and production of smaller exhausted platelets [5, 10]. This mechanism was shown in other diseases with systemic inflammation [5].
Interestingly, opposing MPV levels could be found in different cancer entities. On the one hand, increased MPV was present in gastric, endometrial, ovarian and liver cancer whereas on the other hand, it was decreased in non-small cell lung cancer and renal cell carcinoma [9, 12, 13, 15, 22, 23, 25]. In CRC the role of MPV is still not clear. Higher preoperative MPV values could be found in patients with colon cancer compared to controls, implicating that MPV might indicate the presence of colon cancer. In addition, MPV values were associated with disease progression and raised with higher stages [19]. Kilincalp et al. [26] could further show that increased MPV in CRC patients decreased after surgical removal of the tumor. Conversely, the analysis of MPV in rectal cancer alone revealed lower values at diagnosis but an increase of MPV after curative resection [18]. This might indicate a difference in the role of platelets in colon and rectal cancer but may also indicate that the cancer cells themselves influence the tumor macroenvironment (i.e. platelet function and size) [27].
In contrast to our results, prior studies found increased MPV at diagnosis to be a predictor of poor prognosis in CRC, associated with shorter pooled OS and shorter PFS in metastatic patients receiving bevacizumab-combined chemotherapy. This was explained by a linkage between increased platelet size and increased platelet activation and consecutive greater inflammation [16, 17].
Nonetheless, although not statistically significant, regression coefficients across all treatment settings were in the direction that small platelets are associated with worse outcomes. This at least partly corroborates prior research in CRC and other tumors types which implicate low MPV in adverse prognosis. Moreover, our clinical data are at least hypothesis-generating for further basic research studies on platelet activation and cancer progression in CRC.
Riedl et al. [6] found a decreased MPV to be significantly associated with shorter OS when they analyzed the impact of altered MPV in cancer patients on the risk of venous thromboembolism and mortality in a prospective cohort study including 1544 cancer patients. However, the study summarizes both patients with solid as well as hematological malignancies and amongst others the subgroup analysis for 159 CRC cases showed no significant result. In addition, a recent study of our department found a highly significant association of decreased MPV and RFS as well as cancer specific death in patients with non-metastatic renal cell carcinoma [11]. Low MPV values were also shown to be associated with poor prognosis in cancers of the bladder and the lung [9, 10, 28].
Yet the prognostic and predictive value of MPV might be varyingly strong in different cancer entities. Despite a relatively large sample size in many settings, the results of our study failed to reach significance in most cases, indicating that MPV is only a weak predictor for disease outcome in CRC. Since to date only positive, significant results regarding the association of MPV and CRC prognosis have been published a possible publication bias must be considered. Therefore, taking the results of the present study into account further research is warranted to clarify the impact of MPV on CRC prognosis.
Some limitations of this study are worth to be mentioned. First, selection bias cannot be excluded entirely due to the retrospective single center study design. Second, we did not exclude patients with conditions that might influence laboratory MPV values as did other studies before, but we think that therefore our results are closer and more relevant to clinical practice. The intention was to analyze a potential biomarker applicable for many CRC patients in different settings rather than for a selected cohort. All patients included in this study who underwent surgery or received chemotherapy were fit enough for treatment, and therefore altered MPV levels due to other severe diseases seem unlikely. Third, the relatively small sample size in later treatment lines must be noticed.
In conclusion, the prognostic and predictive role of MPV in CRC patients remains unclear. Based on our study results, MPV is a weak biomarker in CRC and therefore hardly viable for clinical practice.
Abbreviations
- MPV:
-
Mean platelet volume
- BSC:
-
Best supportive care
- RFS:
-
Recurrence-free survival
- PFS:
-
Progression-free survival
- OS:
-
Overall survival
- ORR:
-
Objective response rate
- DCR:
-
Disease control rate
- HR:
-
Hazard ratio
- CI:
-
Confidence interval
- mCRC:
-
Metastatic colorectal cancer
- CTX:
-
Chemotherapy
- CR:
-
Complete remission
- PR:
-
Partial remission
- SD:
-
Stable disease
- PD:
-
Progressive disease
- NE:
-
Not evaluable
- NA:
-
Not applicable
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Conceived and designed the study: DAB FP MS AG. Performed statistical analyses: FP. Interpreted the results: DAB FP HS MS AG. Wrote the first draft of the manuscript: DAB FP. Contributed to the writing of the manuscript: DAB JMR FP MAS AKK TN JS HS MP MS AG Agree with the manuscript’s results and conclusions: DAB JMR FP MAS AKK TN JS HS MP MS AG. ICMJE criteria for authorship read and met DAB JMR FP MAS AKK TN JS HS MP MS AG
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Ethics approval
The study was approved by the IRB of the medical university of Graz prior any patient-related activities were performed (No. 25-458 ex 12/13).
Informed consent
Written informed consent was not obtained from individual patients, because this is not mandated in Austria for retrospective database studies given approval by an ethics committee.
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The dataset for this study is not publicly available by request of the local ethic committee in order to protect the anonymity of the patients.
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Barth, D.A., Riedl, J.M., Posch, F. et al. Critical evaluation of platelet size as a prognostic biomarker in colorectal cancer across multiple treatment settings: a retrospective cohort study. Clin Transl Oncol 21, 1034–1043 (2019). https://doi.org/10.1007/s12094-019-02037-7
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DOI: https://doi.org/10.1007/s12094-019-02037-7