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    <title>Homan, M.</title>
    <link>http://repub.eur.nl/res/aut/11042/</link>
    <description>List of Publications</description>
    <language>en</language>
    <image>
      <url>http://repub.eur.nl/static-eur/img/logo.png</url>
      <title>RePub, Erasmus University Rotterdam</title>
      <link>http://repub.eur.nl</link>
    </image>
    <item>
      <title>Expression of apoptosis related proteins during malignant progression in chronic ulcerative colitis (Article)</title>
      <link>http://repub.eur.nl/res/pub/8371/</link>
      <pubDate>2005-01-01T00:00:00Z</pubDate>
      <description>BACKGROUND: Chronic ulcerative colitis (CUC) is associated with increased
      risk of developing colon cancer through a dysplasia (intraepithelial
      neoplasia)-carcinoma sequence. AIMS: To investigate the expression of
      apoptosis and inflammatory related proteins in CUC. METHODS: The
      expression of proteins involved in apoptosis and inflammation (inducible
      nitric oxide synthase (iNOS), cyclooxygenase 2 (COX-2), Bcl-xl, Fas, and
      active caspase 3) was investigated and compared with that seen in sporadic
      colon carcinoma. RESULTS: COX-2 was negative in the epithelium of all
      samples. iNOS was clearly present in inflammatory areas in CUC epithelium,
      weakly expressed in dysplasia, and absent or weakly expressed in tumour
      cells. Bcl-xl was absent in CUC, increased in dysplasia, and highly
      expressed in most carcinomas. Fas expression was positive in the surface
      epithelium of CUC, dysplasia, and most tumour cells. Activated caspase 3
      was weakly positive in all samples, indicating limited apoptosis. Compared
      with CUC associated carcinoma, iNOS was consistently expressed in sporadic
      colon carcinoma cells, whereas Bcl-xl was almost absent in these tumour
      cells and Fas was only weakly expressed. Activated caspase 3 was present
      in normal mucosal samples and some tumour cells. CONCLUSION: Apoptosis
      related proteins--particularly iNOS, Bcl-xl, and Fas-show a distinct
      pattern of expression in the CUC to carcinoma sequence, which differs from
      that seen in sporadic carcinoma, but bears a striking resemblance to that
      seen during neoplastic progression in Barrett's oesophagus. These results
      support a causal role for chronic inflammation in cancer development in
      CUC, and treatment of ulcerative colitis should aim to minimise
      inflammation.</description>
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