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  • 1
    ISSN: 1365-2559
    Source: Blackwell Publishing Journal Backfiles 1879-2005
    Topics: Medicine
    Notes: Aims : To compare the routinely used polyclonal anti-S100 and a mouse monoclonal anti-S100B antibody for their accuracy in the detection of the S100B expression profile (pattern and intensity) in a series of 67 primary (n = 37) and lymph node metastatic (n = 30) melanoma tissues. S100B is the lineage marker of malignant melanoma. Antibodies routinely used for melanoma diagnosis are not necessarily specific for this protein. Furthermore, clinical monitoring of melanoma progression is mostly based on the determination of serum S100B protein levels without knowing the actual expression level in the primary and/or metastatic tissue.Methods and results : The profile of expression patterns (focal, heterogenous and diffuse) as well as intensity ranges (+, ++ and +++) were similar for the two antibodies in melanoma tissues. However, comparison of the patterns and intensities on the basis of individual cases revealed a high frequency of discrepancies (50.7 and 58.2%, respectively). Severe discrepancy between the two antibodies in the determination of the S100B protein expression pattern (focal versus diffuse or focal versus heterogeneous) was relatively frequent; 13.4 and 11.9%, respectively. Furthermore, a similar rate of severe discrepancy was observed between the two antibodies in the determination of the intensity of S100B expression levels (+ versus +++ or + versus ++); 19.4 and 8.9%, respectively. Separate analysis of the primary tumours and metastases gave similar results.Conclusion : For the accurate determination of S100B protein expression in malignant melanoma it is highly recommended that a monospecific antibody is used.
    Type of Medium: Electronic Resource
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  • 2
    ISSN: 1573-7276
    Keywords: c-met ; colon carcinoma ; in vitro ; metastasis ; motility ; progression
    Source: Springer Online Journal Archives 1860-2000
    Topics: Medicine
    Notes: Abstract The organ-specific metastasis characterizes several human cancers, including colon carcinoma, a disease that frequently involves metastases in the liver. The data on the molecular mechanisms of liver metastasis would therefore be highly useful for prognostic purposes. Although the upregulation/amplification of the hepatocyte growth factor (HGF) receptor, c-met, has been frequently observed in colon cancer metastasis, the actual functional significance of the feature in the liver metastatization is not yet known. We have used three human colon carcinoma cell lines (HT29, HT25 and WiDr), characterized by different liver metastatic potentials in SCID mice, to analyze the expression of c-met and the biological effects of HGF. We found that HGF induces scattering in in vitro liver-metastatic cell lines (HT25 and WiDr) only at doses which are non-mitogenic (1–20 ng/ml). Analysis of the c-met expression revealed that the metastatic cell lines express authentic c-met gene and protein material, unlike the non-metastatic HT29 cell line, which expresses only the c-terminal cytoplasmic domain of the c-met β-chain. Interestingly, c-met was found to be localized in the substrate-attached peripheral membrane and partially colocalized with phosphotyrosine-proteins in the metastatic cells only when kept on fibronectin. On the other hand, we have analyzed 86 primary human colon cancers in Dukes' B (invasive but non-metastatic) and C (invasive and lymph node metastatic) stages. Western blotting of the proteins isolated from the tumor tissues and immunohistochemical control study on the paraffin samples of a third of these cases (25/86) all indicated a significant upregulation of the c-met protein in the Dukes' C tumor glands compared to the Dukes' B stages (P〈0.001 and P〈0.05, respectively). Since the two stages differ in the involvement of the regional lymph nodes but not in the invasion depth, the clinicopathological data and our experimental findings further support the notion that the c-met expression in human colon cancer can be considered as a marker of the metastatic potential due to its involvement in the generation of the motility signal.
    Type of Medium: Electronic Resource
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  • 3
    ISSN: 1434-601X
    Keywords: PACS. 21.10.Hw Spin, parity, and isobaric spin – 21.10.Re Collective levels – 27.60.+j 90 ⩽ A ⩽ 149
    Source: Springer Online Journal Archives 1860-2000
    Topics: Physics
    Notes: Abstract: The decay out of the πh 11/2νh 11/2 band to the known low-energy levels in 132La was studied using the reaction 100Mo + 36S at 160 MeV beam energy. The low-energy level scheme has been further developed and unambiguous spin and parity values have been assigned to the levels connecting the band to the 6- isomeric state. According to the new level scheme the spins in the πh 11/2νh 11/2 band are shifted up by one unit compared to the earlier tentative experimental values. The obtained new spins prove the existence of signature inversion in 132La and give further support to the spin assignments made for the πh 11/2νh 11/2 bands in the neighbouring odd-odd La isotopes from level energy systematics.
    Type of Medium: Electronic Resource
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  • 4
    ISSN: 1434-601X
    Keywords: PACS: 21.10.Re Collective levels – 23.20.Lv Gamma transitions and level energies – 21.60.Ev Collective models – 27.60.+j 90 ≤ A ≤ 149
    Source: Springer Online Journal Archives 1860-2000
    Topics: Physics
    Notes: Abstract: High spin states of 126La have been populated using the reaction 116Sn+14N at 68 MeV. γ-rays and conversion electrons were detected with the GAREL array. Multipolarities of the lowest-lying in-band dipole transitions have been determined from the deduced internal conversion coefficients. Experimental B(M1)/B(E2) ratios have been derived for the bands and compared with calculated values using the Dönau-Frauendorf geometrical model. Configurations are proposed for the bands comparing them with cranked shell model calculations and on the basis of the measured B(M1)/B(E2) ratios. The β-decay of 126La has also been revisited. The population of the 126Ba levels gives a probable spin value of five for the decaying high-spin 126La state with T 1/2≈ 64 s which may indicate a signature inversion in the πh11/2νh11/2 band.
    Type of Medium: Electronic Resource
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