Tumor-M2-Pyruvatkinase beim Nierenzellkarzinom

Roigas, Jan; Schulze, G; Raytarowski, S.; Jung, Klaus; Schnorr, Dietmar; Loening, S.A.

doi:10.1007/s001200050410

Der Urologe A

2000

DOI: 10.1007/s001200050410

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Tumor-M2-Pyruvatkinase beim Nierenzellkarzinom

Jan Roigas

G Schulze²,

S. Raytarowski³

et al.

Abstract: Tumor cell metabolism is characterized by a high rate of aerobic glycolysis. The metabolic differences require changes in glycolytic enzyme activities and isoenzyme patterns. The inactive form of the M2 pyruvate kinase (Tu M2-PK) is specifically expressed in tumor cells and has been detected immunohistochemically in tumor tissue but also in peripheral blood of patients with different malignant tumors. In this study, Tu M2-PK in the plasma of patients with renal cell carcinoma (RCC) was compared with healthy vo… Show more

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High frequency of serum DNA alterations in renal cell carcinoma detected by fluorescent microsatellite analysis

Knobloch¹,

Hegele²,

Brandt³

et al. 2002

Intl Journal of Cancer

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To date there are no reliable serological markers for renal cell carcinoma (RCC). We applied fluorescent microsatellite analysis (MSA) to detect serum DNA alterations in patients with RCC. Fresh tumour, peripheral blood and serum specimens from 60 consecutive patients treated for malignant renal tumours (n= 53 RCC and n= 7 non-RCC) were prospectively collected. After DNA extraction, we performed MSA with a total of 9 markers from the chromosomal regions 3p, 5q, 7p, 7q, 9p, 13q, 17p and 17q to identify tumour specific serum DNA alterations in Group I (n= 53 RCC); 11 additional markers were used in the first 23 RCCs (Group II) in order to increase sensitivity; and 20 healthy controls were investigated with 10 markers. Besides the histomorphological diagnosis the RCCs were genetically stratified according to the "Heidelberg Classification" of renal tumours. Detection of allelic imbalance and loss of heterozygosity (LOH) was carried out on an automated laser sequencer. In Group I we identified serum DNA alterations in 74% (39/53) of cases. When applying 20 markers, the sensitivity was elevated to 87% (20/23) in Group II. Investigating 20 healthy controls with 10 markers, the method rendered 85% specificity. The highest incidence of alterations was detected for chromosomal regions 3p and 5q. The presence of serum DNA alteration was not associated with tumour nuclear grade but exhibited a trend towards advanced stages (p = 0,044). In RCC, the microsatellite analysis has a high sensitivity in the detection of serum DNA alterations when a sufficient number of markers from various chromosomal regions are used. Advanced tumours tend to express serum DNA alterations more frequently.

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High frequency of serum DNA alterations in renal cell carcinoma detected by fluorescent microsatellite analysis

Knobloch¹,

Hegele²,

Brandt³

et al. 2002

Intl Journal of Cancer

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Plasma levels of tumor M2-pyruvate kinase should not be used as a tumor marker for hematological malignancies and solid tumors

Staib

Hoffmann²,

Schinköthe³

2006

Clinical Chemistry and Laboratory Medicine (CCLM)

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It has been reported that the dimeric isoform of the enzyme pyruvate kinase M2 was overexpressed in various solid tumor cells. Hence, it was suggested that circulating levels of the so-called tumor M2-pyruvate kinase (Tu M2-PK) could be used as a tumor marker for monitoring systemic therapies of various solid tumors. We analyzed its validity as a tumor marker by comparing plasma levels of Tu M2-PK in patients with different non-malignant diseases to levels in healthy individuals and in patients with hematological diseases. Plasma levels of Tu M2-PK were measured using an ELISA assay in a total of 284 patients. The mean Tu M2-PK concentration of 32 U/mL was significantly higher in the group of patients with hematological malignancies (n = 121) (p < 0.001). However, 37% of healthy individuals (n = 63) and 44% of patients with non-malignant diseases (n = 100), especially patients with an acute inflammatory reaction (67%), were found to have elevated levels of Tu M2-PK using a cutoff level of 15 U/mL. The specificity was 59% and the sensitivity was 51%. There was no significant correlation between the prevalence of a hematological malignancy and positive Tu M2-PK result. Thus, our data imply that Tu M2-PK is not a useful tumor marker for hematological malignancies and solid tumors, as a significant number of false positive results were detected in healthy individuals and patients with non-malignant diseases.

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Tumor type M₂pyruvate kinase expression in gastric cancer, colorectal cancer and controls

Zhang

Chen²,

Daoda³

et al. 2004

WJG

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Tumor-M2-Pyruvatkinase beim Nierenzellkarzinom

Cited by 3 publications

References 1 publication

High frequency of serum DNA alterations in renal cell carcinoma detected by fluorescent microsatellite analysis

High frequency of serum DNA alterations in renal cell carcinoma detected by fluorescent microsatellite analysis

Plasma levels of tumor M2-pyruvate kinase should not be used as a tumor marker for hematological malignancies and solid tumors

Tumor type M₂pyruvate kinase expression in gastric cancer, colorectal cancer and controls

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Tumor-M2-Pyruvatkinase beim Nierenzellkarzinom

Cited by 3 publications

References 1 publication

High frequency of serum DNA alterations in renal cell carcinoma detected by fluorescent microsatellite analysis

High frequency of serum DNA alterations in renal cell carcinoma detected by fluorescent microsatellite analysis

Plasma levels of tumor M2-pyruvate kinase should not be used as a tumor marker for hematological malignancies and solid tumors

Tumor type M2pyruvate kinase expression in gastric cancer, colorectal cancer and controls

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Product

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Tumor type M₂pyruvate kinase expression in gastric cancer, colorectal cancer and controls