Brief Article Open Access
Copyright ©2012 Baishideng Publishing Group Co., Limited. All rights reserved.
World J Gastroenterol. Aug 14, 2012; 18(30): 4004-4011
Published online Aug 14, 2012. doi: 10.3748/wjg.v18.i30.4004
Faecal pyruvate kinase isoenzyme type M2 for colorectal cancer screening: A meta-analysis
Carolin Tonus, Gero Neupert, Asklepios Hospital North, General and Visceral Surgery, 22417 Hamburg, Germany
Markus Sellinger, Medical Practice for Gastroenterology Lusanum, 67061 Ludwigshafen, Germany
Konrad Koss, Department of Gastroenterology, Macclesfield District General Hospital, Macclesfield, Cheshire SK10 3BL, United Kingdom
Author contributions: Tonus C and Neupert G conducted the literature review and wrote the article; Sellinger M and Koss K reviewed the text and made significant revisions to drafts of this manuscript.
Correspondence to: Dr. Carolin Tonus, Professor, Asklepios Hospital North, General and Visceral Surgery, Tangstedter Landstrasse 400, 22417 Hamburg, Germany. mail@carolintonus.de
Telephone: +49-40-1818873667 Fax: +49-40-1818873112
Received: August 4, 2011
Revised: November 26, 2011
Accepted: April 22, 2012
Published online: August 14, 2012

Abstract

AIM: To present a critical discussion of the efficacy of the faecal pyruvate kinase isoenzyme type M2 (faecal M2-PK) test for colorectal cancer (CRC) screening based on the currently available studies.

METHODS: A literature search in PubMed and Embase was conducted using the following search terms: fecal Tumor M2-PK, faecal Tumour M2-PK, fecal M2-PK, faecal M2-PK, fecal pyruvate kinase, faecal pyruvate kinase, pyruvate kinase stool and M2-PK stool.

RESULTS: Stool samples from 704 patients with CRC and from 11 412 healthy subjects have been investigated for faecal M2-PK concentrations in seventeen independent studies. The mean faecal M2-PK sensitivity was 80.3%; the specificity was 95.2%. Four studies compared faecal M2-PK head-to-head with guaiac-based faecal occult blood test (gFOBT). Faecal M2-PK demonstrated a sensitivity of 81.1%, whereas the gFOBT detected only 36.9% of the CRCs. Eight independent studies investigated the sensitivity of faecal M2-PK for adenoma (n = 554), with the following sensitivities: adenoma < 1 cm in diameter: 25%; adenoma > 1 cm: 44%; adenoma of unspecified diameter: 51%. In a direct comparison with gFOBT of adenoma > 1 cm in diameter, 47% tested positive with the faecal M2-PK test, whereas the gFOBT detected only 27%.

CONCLUSION: We recommend faecal M2-PK as a routine test for CRC screening. Faecal M2-PK closes a gap in clinical practice because it detects bleeding and non-bleeding tumors and adenoma with high sensitivity and specificity.

Key Words: Faecal pyruvate kinase isoenzyme type M2, Colorectal cancer screening, Colorectal cancer, Stool, Faecal occult blood, Adenoma, Polyps



INTRODUCTION

Colorectal cancer (CRC) is the most frequent malignant disease in Europe according to an estimation of cancer incidence and mortality by the International Agency for Research on Cancer in Lyon, France[1]. In 2008, 436 000 persons were diagnosed with CRC, followed by breast cancer with 421 000 cases, lung cancer with 391 000 cases and prostate cancer with 382 000 cases. Approximately 212 000 patients died due to CRC that year, which makes it the second most common death from cancer (after lung cancer with approximately 342 000 deaths in 2008)[1]. Worldwide, in the developed countries about 1.167 million new cases of CRC and about 603 000 deaths due to CRC were estimated for 2007[2].

However, due to the long process of carcinogenesis in CRC (adenoma-carcinoma sequence), CRC has an overall good prognosis when diagnosed at an early stage. For that reason different CRC screening programs have been developed and are offered in various European countries.

The gold standard for early detection of colorectal neoplasia is colonoscopy. A great advantage of colonoscopy is that adenomas, the potential precursors of carcinogenesis, can be simultaneously detected and removed. However, the acceptance of screening colonoscopy among patients is low. For example, in Germany only 2.7% of insured people exercise their right to a colonoscopy even though it is reimbursed for people over 55 years old[3]. The most common in-vitro diagnostic method for CRC screening is the detection of occult blood in the stool using the guaiac-based faecal occult blood test (gFOBT). This test is based on the peroxidase activity of haemoglobin, which induces an oxidation and blue colouration of guaiac in the presence of hydrogen peroxide. Red meat and a number of vegetables may result in false positive results whereas vitamin C may result in false negative staining. Therefore, dietary restriction is recommended for three days prior to and during testing. A widespread criticism of gFOBT is its low sensitivity for adenomas and carcinomas (13%-50%)[4-8]. The immunological faecal occult blood tests (iFOBTs) specifically quantify human haemoglobin with antibodies. Comparative evaluations of immunochemical faecal occult blood tests from different manufacturers have revealed great variations in their respective sensitivities for colorectal adenoma detection[9,10].

The faecal pyruvate kinase isoenzyme type M2 (faecal M2-PK) test recognises a key enzyme controlling the metabolism of cells with a high proliferation rate, such as tumour cells, and thereby detects specific alterations in intestinal cells, such as polyps and CRC, as well as high-risk patients with acute or chronic inflammatory bowel diseases (IBD) (i.e., ulcerative colitis, Crohn’s disease).

M2-PK is a special isoenzyme of pyruvate kinase, a key enzyme within glycolysis which catalyzes the ATP-producing conversion of phosphoenolpyruvate (PEP) to pyruvate. Depending upon the metabolic functions of the tissues, different isoenzymes of pyruvate kinase are expressed. During tumour formation the tissue-specific isoenzymes disappear and the pyruvate kinase isoenzyme type M2 is expressed[11]. In contrast to all other pyruvate kinase isoenzymes (type L, M1 and R) which consist of four subunits, the M2 pyruvate kinase isoenzyme may occur in a highly active tetrameric form as well as in a dimeric form with low activity. The dimeric form is nearly inactive and favours the channelling of glucose carbons into synthetic processes, such as nucleic acid, amino acid and fatty acid synthesis. The tetrameric form is highly active and favours the energy-regenerating conversion of PEP to pyruvate and lactate (the Warburg effect). In tumour cells, M2-PK is mainly found to be in the dimeric form and has therefore been termed “Tumour M2-PK”. The dimerisation of M2-PK is induced by interaction with different oncoproteins, including pp60v-src-kinase, oncogenic fibroblast growth factor1 and human papilloma virus 16 E7[11].

The dimeric form of M2-PK is released from tumours into the blood and can be quantified by a sandwich enzyme-linked immunosorbent assay (ELISA; ScheBo Biotech AG, Giessen, Germany). About 40 studies have been published on M2-PK concentrations in blood since 1997. These demonstrate a significant increase in M2-PK and correlation with staging for the following tumours: melanoma, thyroid, breast, lung, kidney, oesophageal, gastric, pancreatic, colorectal, ovarian, cervical and renal cell cancer[12-19]. The long-term determination of M2-PK in EDTA-plasma is used as a tool for follow-up studies to monitor failure, relapse or success during therapy. In CRC and adenoma M2-PK is also released into the patients’ faeces. A sandwich ELISA and a lateral flow rapid test (for doctor’s office, point-of-care and laboratory use), both based upon two monoclonal antibodies which specifically recognise the dimeric form of M2-PK, are commercially available for the quantification of M2-PK in stool. The potential of the faecal M2-PK test for CRC screening has been evaluated in at least 17 different independent international studies. The objectives of this review were to obtain an overview of the currently available studies with faecal M2-PK and to present a critical discussion of the efficacy of the faecal M2-PK test for CRC screening.

MATERIALS AND METHODS
Search procedure for studies

In order to find the most relevant studies about faecal M2-PK and CRC screening, a literature search in PubMed and Embase was conducted using the following search terms: fecal tumor M2-PK, faecal tumour M2-PK, fecal M2-PK, faecal M2-PK, fecal pyruvate kinase, faecal pyruvate kinase, pyruvate kinase stool, M2-PK stool. In June 2011 this search revealed 34 publications dealing with faecal M2-PK[7,8,10,18,20-49] (Table 1). The ScheBo faecal M2-PK test was used in 33 publications, whereas one publication used another antibody combination and was therefore excluded. The following were also omitted from the meta-analysis: seven publications which summarized results from previous papers as reviews; three author-replies to questions about an existing published paper; one publication written in Bulgarian; two publications which investigated neither sensitivity nor specificity; seven publications that only referred to IBD (which was outside the scope of our review) (Table 1). The remaining 13 publications were included in the meta-analysis[7,8,10,30,31,33,35,37,41,44-46,49]. In addition, three posters from conferences[50-52] and a German doctoral thesis[53] known to the authors have been added to the list of relevant studies (Table 1). Hence, 17 published studies in total have been incorporated into the meta-analysis (Tables 1 and 2). For our meta-analysis the sensitivities for CRC and adenoma, positivity rates, as well as the specificities published within the individual papers were summarized in individual tables, together with the number of cases which underlie the calculated sensitivities and specificities. mean ± SD was calculated for the sensitivities and specificities of the combined data from the different studies using the Statistics package of SigmaPlot Version 11.0. The sensitivities for CRC and adenoma in all studies are based upon colonoscopy results. Calculated specificities are either based on colonoscopy results or are authors’ estimates derived from published prevalence data of CRC and adenoma in screening populations. In the absence of colonoscopies or estimated specificities, only the percentages of test-negative individuals were included in the tables.

Table 1 Results of the literature search.
ResultsReference
All papers dealing with faecal M2-PK found in a literature search of Pubmed and Embase[7, 8, 10,18, 20-49]
Additional published studies known to the authors[50-53]
Excluded papers - reasons for exclusion
Unique combination of antibodies[47]
Reviews[18, 24, 26, 28, 34, 38, 42]
Author replies or comments[27, 32, 40]
Paper in Bulgarian language[29]
No sensitivities or specificities calculated[21, 48]
Studies referred to IBD[20, 22, 23, 25, 36, 39, 43]
Included papers
Studies found in Pubmed and Embase[7, 8, 10, 30, 31, 33, 35, 37, 41, 44-46, 49]
Published studies known to the authors[50-53]
Figure 1
Figure 1 Faecal pyruvate kinase isoenzyme type M2 in healthy controls, patients with colorectal adenoma and colorectal cancer[51]. Faecal M2-PK: Faecal pyruvate kinase isoenzyme type M2.
Table 2 Overview of included studies.
ReferenceCountry of studyConflict of interest regarding faecal M2-PK
Shastri et al[7], 2006GermanyNone declared
Koss et al[8], 2008United KingdomNone declared
Möslein et al[10], 2010GermanyNone declared
Haug et al[30], 2008GermanyNone declared
Shastri et al[31], 2008GermanyCoauthor Stein: Conference speaker for ScheBo Biotech AG
Haug et al[33], 2007GermanyNone declared
Mulder et al[35], 2007The NetherlandsNone declared
Ewald et al[37], 2007GermanyNone declared
Tonus et al[41], 2006GermanyNon declared
Vogel et al[44], 2005GermanyTests performed by ScheBo Biotech AG
Naumann et al[45], 2004GermanyNone declared
Hardt et al[46], 2004GermanyNone declared
Tonus et al[49], 2009GermanyNone declared
Kloer et al[50], 2005GermanyNone declared
McLoughlin et al[51], 2005IrelandNone declared
Bellutti et al[52], 2005GermanyNone declared
Schmidt et al[53], 2009GermanyNone declared
Figure 2
Figure 2 Distribution of faecal pyruvate kinase isoenzyme type M2 concentrations in a screening collective of 2787 participants aged from 45 to 65 years[52]. n: Number of test negative; N: Total number of subjects; M2-PK: Pyruvate kinase isoenzyme type M2.
Faecal M2-PK test

In all seventeen studies included in our meta-analysis, the M2-PK stool test from ScheBo Biotech AG in Giessen, Germany was used. This test is a sandwich ELISA based on two monoclonal antibodies which specifically recognise the dimeric form of M2-PK.

In accordance with the manufacturer’s protocol all studies included a cut-off value of 4 U/mL. One study also included a lower cut-off value (3.33 U/mL[8]) and another also incorporated additional higher cut off values (5 U/mL and 6 U/mL[45]) to calculate the resultant sensitivities and specificities. To ensure comparability only those results obtained with the cut-off value of 4 U/mL are included in the meta-analysis.

RESULTS
Sensitivity of faecal M2-PK for colorectal carcinoma

Sensitivity of the faecal M2-PK test for CRC was investigated and calculated in twelve independent studies (Table 3 and Figure 1), which found sensitivities of faecal M2-PK for detection of CRC between 68% and 97%. The mean sensitivity of all twelve studies is 80.3% ± 7.1%. These twelve studies measured faecal M2-PK concentrations in a total of 704 stool samples of patients with CRC, whereby 559 tested positive. Five studies considered the tumor node metastases and/or Dukes classification and showed a close correlation between the sensitivity of the faecal M2-PK test and staging (Table 4). The mean sensitivities ranged from 59% for T1 to 90% for T4 and from 60% for Dukes A to 91% for Dukes D. gFOBT studies from various countries showed much lower sensitivities for CRC which ranged between 13% and 50%[4-6]. The higher sensitivity of faecal M2-PK compared to gFOBT was confirmed in four studies which measured faecal M2-PK and gFOBT head-to-head in the same patients (Table 5). Combining all four studies, 155 samples from patients with CRC were tested for faecal M2-PK and gFOBT. M2-PK correctly detected 81.1% whereas the gFOBT detected only 36.9%.

Table 3 Published sensitivities of the faecal pyruvate kinase isoenzyme type M2 test for colorectal cancer.
Referencen (%)
Hardt et al[46], 200460 (73)
Naumann et al[45], 200427 (85.2)
Kloer et al[50], 2005147 (79.6)
McLoughlin et al[51], 200535 (97)
Vogel et al[44], 200522 (77)
Shastri et al[7], 200674 (81.1)
Tonus et al[41], 200654 (78)
Haug et al[33], 200765 (68)
Mulder et al[35], 200752 (85)
Koss et al[8], 200832 (81)
Shastri et al[31], 200855 (78.2)
Schmidt et al[53], 200981 (80.3)
Sum704
mean ± SD80.3 ± 7.1
Table 4 Correlation of faecal pyruvate kinase isoenzyme type M2 sensitivity with tumor node metastasis and Dukes classification n (%).
ReferenceTumor node metastasis classificatoin
Dukes classification
T1T2T3T4Dukes ADukes BDukes CDukes D
Kloer et al[50], 20059 (55.5)18 (61.1)49 (81.6)12 (83.3)23 (52.2)24 (76.0)26 (80.8)17 (82.4)
Tonus et al[41], 20065 (60)11 (64)25 (89)4 (100)5 (60.0)17 (76.0)9 (89)10 (90.0)
Haug et al[33], 20076 (67)16 (44)34 (71)4 (100)12 (67.0)18 (61.0)12 (67.0)6 (100.0)
Schmidt et al[53], 20098 (57)20 (84)42 (79)11 (91)
Hardt et al[46], 20047 (57)11 (64)33 (78)9 (78)
Sum35761834040594733
mean ± SD59 ± 563 ± 1480 ± 790 ± 1060 ± 771 ± 979 ± 1191 ± 9
Table 5 Head-to-head comparison of the sensitivity for colorectal cancer of faecal pyruvate kinase isoenzyme type M2 and guaiac-based faecal occult blood test n (%).
ReferenceCRC M2-PKCRC gFOBT
Naumann et al[45], 200427 (85.2)27 (62.9)
Vogel et al[44], 200522 (77)22 (27)
Shastri et al[7], 200674 (81.1)74 (36.5)
Koss et al[8], 200832 (81)32 (21)
Sum155155
mean ± SD81.1 ± 3.336.9 ± 18.5
Sensitivity of faecal M2-PK for adenoma

More than 90% of colorectal carcinomas evolve from adenoma via the adenoma-carcinoma sequence within 10 to 15 years. Therefore, the early detection and removal of adenoma is an important aspect in the prevention of CRC. The sensitivity of faecal M2-PK for adenoma was investigated in eight studies and ranged between 20% and 76%, whereby a clear dependency with the diameter of the adenoma is described (Table 6). In total, 339 adenomas with a diameter < 1 cm and 117 adenomas with a diameter > 1 cm were investigated. Twenty-five percent of the adenomas < 1 cm in diameter tested positive with the faecal M2-PK test and 44% of the adenomas > 1 cm were correctly detected. Three studies included a total of 98 stool samples from patients with adenoma of unclassified diameter. Faecal M2-PK concentrations above the cut-off were found in 51% of the samples. In direct comparisons of faecal M2-PK with gFOBT, 25% of patients with polyps < 1 cm tested positive with the M2-PK test whereas only 9% were identified by the gFOBT (Table 7). Fourty-seven percent of adenomas > 1 cm in diameter tested positive with the M2-PK test whereas the gFOBT detected only 27% (Table 7). One study with adenomas of unclassified diameter revealed a sensitivity of 48% for M2-PK in comparison to 9% for gFOBT. Möslein et al[10] combined adenomas > 1 cm in diameter and CRC to form a group with 55 cases of “advanced neoplasia”. The resultant sensitivity of faecal M2-PK for advanced neoplasia was 27.3% whereas the sensitivity of gFOBT was only 9.1%. This study also included a head-to-head comparison of four iFOBTs from different manufacturers using the same 55 samples of patients with advanced neoplasia. With sensitivities of 7.3%, 8.5%, 18.9% and 20%, respectively, all four iFOBTs were less sensitive than faecal M2-PK.

Table 6 Sensitivity of faecal pyruvate kinase isoenzyme type M2 for adenoma n (%).
ReferenceAdenoma without diameterAdenoma < 1 cmøAdenoma > 1 cmø
Naumann et al[45], 200411 (27.3)13 (61.5)
McLoughlin et al[51], 200530 (76)
Vogel et al[44], 200521 (48)
Shastri et al[7], 200621 (28.6)10 (20.0)
Mulder et al[35], 200747 (28)
Koss et al[8], 20085 (20)5 (60)
Shastri et al[31], 200848 (29.2)21 (57.1)
Haug et al[30], 2008254 (22.1)68 (23.5)
Sum98339117
mean ± SD51 ± 2425 ± 444 ± 21
Table 7 Head-to-head comparison of sensitivity for adenoma of faecal pyruvate kinase isoenzyme type M2 and guaiac-based faecal occult blood test n (%).
ReferenceAdenoma < 1 cmøM2-PKAdenoma < 1 cmøgFOBTAdenoma > 1 cmøM2-PKAdenoma > 1 cmøgFOBTAdenoma w/oøM2-PKAdenoma w/oøgFOBT
Naumann et al[45], 200411 (27.3)11 (18.2)13 (61.5)13 (30.8)
Vogel et al[44], 200521 (48)21 (9)
Shastri et al[7], 200621 (28.6)21 (9.5)10 (20.0)10 (30.0)
Koss et al[8], 20085 (20.0)5 (0.0)5 (60.0)5 (20.0)
Sum373728282121
mean ± SD25 ± 59 ± 947 ± 2427 ± 6
Specificity of faecal M2-PK for colorectal carcinoma

The specificity of an in-vitro diagnostic test reflects the proportion of correctly identified negatives. Consequently, the composition of the control group has a profound effect on the specificity. By its very definition, screening is used in a population to detect a disease in individuals without signs or symptoms of that disease. Therefore, symptoms in the gastrointestinal tract, such as pain, visible blood in the stool or known inflammation are not appropriate for inclusion into the control group of a CRC screening study. In total, seventeen publications calculated specificities for the M2-PK stool test. Nine of these studies included patients from hospitals (clinical settings instead of screening settings) with positive gFOBTs and with inflammation and/or other symptoms in the gastrointestinal tract into the control group and hence these studies have been discounted from our evaluation of the specificity of faecal M2-PK[7,30,31,35,44-46,50,53]. Eight studies, comprising 11 412 samples in total, had control groups which conformed to the correct composition for screening studies (Table 8, Figures 2 and 3). Ninty one point five percent tested negative which means that about 9% of those tested had a faecal M2-PK value above the cut-off value of 4 U/mL. Colonoscopies were performed in four studies[8,10,51,41] (Table 8) and revealed specificities of 98% (n = 97), 93% (n = 42), 100% (n = 13) and 89.5% (n = 796). In study 49 with 4854 participants, the authors calculated an estimated specificity of 93.4% based on a prevalence of CRC of 2%. Based on a prevalence of 0.5% for CRC and 18% for advanced adenoma, the authors of study 52 with 2787 participants calculated an estimated specificity for colorectal neoplasia of 97.4%. The screening in study 49 with 4854 participants describes a continuous increase in the percentage of faecal M2-PK positive volunteers with age from 30 years old upwards (Figure 3).

Figure 3
Figure 3 Percentage of faecal pyruvate kinase isoenzyme type M2-positive volunteers by age group (from Tonus et al[49]).
Table 8 Measurements of faecal pyruvate kinase isoenzyme type M2 in stool samples of healthy individuals.
ReferenceNo. of healthy participantsTest-negative participants (%)Colonoscopy (yes/no)Specificity (%)
Belluti et al[52], 2005278791.6No97.4 (e)
McLoughlin et al[51], 20059798Yes98
Tonus et al[41], 20064293Yes93
Ewald et al[37], 2007190690.4No
Haug et al[33], 200791778.6No
Koss et al[8], 200813100.0Yes100.0
Tonus et al[49], 2009485491.2No93.4 (e)
Möslein et al[10], 201079689.5Yes89.5
Sum11 412
mean ± SD91.5 ± 6.495.2 ± 3.9
DISCUSSION

With a sensitivity of about 80% for CRC and 44% for adenoma > 1 cm, faecal M2-PK outclasses the gFOBT which has sensitivity between 13% and 50% for CRC (Tables 3-7, and literature[4-6]). The superiority of faecal M2-PK may be due to the fact that M2-PK is a metabolic biomarker which is characteristic for the metabolic state of tumour cells and their precursors, whereas detection of bowel cancer using the gFOBT is restricted to bleeding tumours and adenoma. Therefore, faecal M2-PK has the advantage that it detects both bleeding as well as non-bleeding tumours and adenoma and will close a gap in clinical practice. Conversely, faecal M2-PK does not have false positive results due to various non-cancerous sources of bleeding, e.g., haemorrhoids and fissures. Screening studies involving a total of more than 11 000 healthy subjects have demonstrated a mean specificity of 95.2% for the detection of CRC/advanced neoplasia with faecal M2-PK. The specificities were 100%, 98%, 93% and 89.5%, respectively, in studies which incorporated colonoscopies; 97.4% and 93.4% in studies with estimated specificities; and 90.4% and 78.6 % in studies without colonoscopies (Table 8). This demonstrates that specificities were higher in studies with confirmatory colonoscopies in comparison to studies without colonoscopies. Whilst gFOBT specificities ≥ 94% are reported in the literature[5,6], the authors of a meta-analysis of over 440 000 subjects from six independent studies concluded that more than 80% of the positive gFOBT results are actually false positives[54]. In most studies the calculated specificities are based on the results of colonoscopy. Colonoscopy is the gold standard for early detection of CRC and polyps and has the advantage that polyps, the potential precursors of carcinogenesis, can be simultaneously detected and removed. However, recent studies have revealed that colonoscopies may have false negative results, e.g., due to suboptimal bowel preparation. For example, a systematic review which summarized six studies totaling 465 patients who had undergone two colonoscopies on the same day revealed a pooled miss rate of 22% for polyps of any size[55].

IBD may also be a cause of increased faecal M2-PK levels and hence detection of previously undiagnosed patients by faecal M2-PK is another advantage of the test, whereas those patients with known IBD are subject to their own endoscopic monitoring program and are not categorized as suitable for inclusion in a non-invasive CRC screening program.

The cost of one faecal M2-PK ELISA test is about 15-25 US$. In comparison, based on 2004 data from privately insured beneficiaries, costs were estimated to be about 557 US$ (range: 150-1112 US$) for a colonoscopy, 174 US$ (range: 54-392 US$) for a flexible sigmoidoscopy and 7 US$ (range: 2-16 US$) for a guaiac faecal occult blood test[56].

In conclusion, faecal M2-PK, either as an ELISA or as a lateral flow rapid test, is a cost-effective and easy-to-perform routine test. In contrast to the gFOBT, only one small stool sample (from a single stool passage), which may be collected with a convenient stool sample device, is necessary and no dietary restrictions are needed. Faecal M2-PK is an appropriately sensitive tool to pre-select those patients who require colonoscopy for further diagnostic confirmation or exclusion of CRC. Based on the current data we recommend the use of faecal M2-PK as a routine in-vitro diagnostic test for CRC screening.

COMMENTS
Background

Colorectal cancer (CRC) is the most frequent malignant disease worldwide. The gold standard for early detection of colorectal neoplasia is colonoscopy. However, the acceptance of screening colonoscopy by potential screenees is low. Faecal pyruvate kinase isoenzyme type M2 (faecal M2-PK) is an in-vitro diagnostic test which recognizes a specific metabolic characteristic of proliferating cells in 4 mg stool samples. The simplicity of sample collection can encourage participation in CRC screening programs.

Research frontiers

The sensitivity and specificity of faecal M2-PK for CRC screening has been investigated in numerous publications. Here the paper presents a critical discussion of the efficacy of faecal M2-PK for CRC screening based on the accumulated data from currently available studies.

Innovations and breakthroughs

The most established in-vitro diagnostic test for CRC screening is the guaiac-based faecal occult blood test (gFOBT). In contrast to the FOBTs, faecal M2-PK detects bleeding and non-bleeding tumors. With a sensitivity of about 80% for CRC and 44% for adenoma > 1 cm, faecal M2-PK outclasses the gFOBT which has a sensitivity between 13% and 50% for CRC.

Applications

This meta-analysis summarizes the results of 17 published studies evaluating the faecal M2-PK test for CRC screening. The data will help to critically assess the efficiency of the faecal M2-PK test in comparison to other in-vitro diagnostic tests for CRC screening.

Peer review

This is a meta-analysis about screening CRC with fecal MK-pyruvate kinase.

Footnotes

Peer reviewers: Dr. Cuneyt Kayaalp, MD, Professor, Department of General Surgery, Staff Surgeon of Gastrointestinal Surgery, Turgut Ozal Medical Center, Inonu University, Malatya 44315, Turkey; Dr. Jose Perea, Department of Surgery, 12 De Octubre University Hospital, Rosas De Aravaca, 82A, 28023 Madrid, Spain

S- Editor Cheng JX L- Editor Logan S E- Editor Xiong L

.

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