HSV epithelial keratitis reactivation after subconjunctival bevacizumab injection: A case report

Proliferating cells, especially tumour cells, express a special isoenzyme of pyruvate kinase, termed M2-PK, which can occur in a tetrameric form with a high affinity to its substrate, phosphoenolpyruvate (PEP), and in a dimeric form with a low PEP affinity. In tumour cells, the dimeric form is usually predominant and is therefore termed Tumour M2-PK. The levels of Tumour M2-PK within tumours and in EDTA-plasma correlate with staging and the ability of the tumour cells to metastasise. Since most colorectal tumours grow intraluminally, it appeared interesting to determine whether Tumour M2-PK is detectable in the faeces of tumour patients. Stool samples were tested by ELISA from controls without colorectal cancer and colorectal cancer patients. Whereas Tumour M2-PK levels were low in the control group (mean value7s.e.m.: 3.370.4, n ¼ 144), they were high in the case of colorectal cancer (56.1715.3, n ¼ 60). At a cutoff value of 4 U ml À1 , the sensitivity was 73%. TNM and Dukes' classification of the tumours revealed a strong correlation between faecal Tumour M2-PK levels and staging. The determination of Tumour M2-PK in faeces provides a new promising screening tool for colorectal tumours.

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Pyruvatkinase M2 (Tumor M2-PK) im Stuhl als Screeningparameter für kolorektale Neoplasien. Eine Übersicht über bisher publizierte Daten

Ewald

Toepler

Akıncı

et al. 2005

Z Gastroenterol

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Compared to FOBT or genetic testing the M2-PK test seems to be superior for CRC screening. Concerning handling, effectiveness and analysis, M2-PK seems to be a good possibility for large scale-screening of colorectal carcinoma. It might even be used to detect larger adenomas. Elevated levels of M2-PK in patients with acute and/or chronic inflammatory bowel diseases are probably due to proliferation of epithelial cells and leucocytes in the inflammatory area.

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The tumor metabolic marker Tumor M2-PK in stool: A new biomarker for colorectal cancer

Kloer

Hardt

Schlierbach

et al. 2005

JCO

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Material and Methods The present study includes 338 patients who underwent complete colonoscopy after providing a sample for the determination of Tumor M2-PK. Stool samples of patients with CRC and patients without patholog ical findings were tested. Histology was obtained from the routine biopsies and/or from surgery. Tumor M2-PK in stool extracts was determined immunologically with a quantitative ELISA which is based on two monoclonal antibodies (ScheBo ® • Biotech AG, Germany). Results Data from 191 controls with no pathological finding upon colonoscopy and 147 patients with CRC have been evaluated to date (Table 1 and Figure 1). There is a highly significant difference (p < 0.001) between tumor patients and controls. At a cutoff point of 4 U/ml, the calculated sensitivity is 85% for colon cancer and 71% for rectal cancer and the specificity is 79%. Fecal Tumor M2-PK levels of 88 patients with CRC were correlated with tumor staging according to TNM (Figure 2) and Dukes classification (Figure 3). There is a significant difference between controls and tumor stages T1 and T2, and a highly significant difference (p < 0.00 1) between controls and tumor stages T3 and T4. Sensitivity for T1, T2, T3, and T4 is 56%, 61%, 82%, and 83%, respectively (Figure 2). Staging according to Dukes' classification revealed a significant difference between controls and Dukes A, and a highly significant difference (p < 0.001) between controls and Dukes B to Dukes D. Sensitivity is 52% for Dukes A, 76% for Dukes B, 81% for Dukes C, and 82% for Dukes D (Figure 3).

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M Toepler

Faecal tumour M2 pyruvate kinase: a new, sensitive screening tool for colorectal cancer

Pyruvatkinase M2 (Tumor M2-PK) im Stuhl als Screeningparameter für kolorektale Neoplasien. Eine Übersicht über bisher publizierte Daten

The tumor metabolic marker Tumor M2-PK in stool: A new biomarker for colorectal cancer

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