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Suppression of the neoplastic phenotype by transfection of phospholipase C3 to neuroendocrine tumor cells

Stålberg, Peter (author)
Uppsala universitet,Medicin,Onkologisk endokrinologi, K Öberg
Wang, Shu (author)
Uppsala universitet,Medicin,Onkologisk endokrinologi, K Öberg
Larsson, Catharina (author)
Karolinska Institutet,Uppsala universitet,Molekylär medicin
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Weber, Günther (author)
Uppsala universitet,Molekylär medicin
Öberg, Kjell (author)
Uppsala universitet,Medicin,Onkologisk endokrinologi, K Öberg
Gobl, Anders (author)
Uppsala universitet,Medicin,Onkologisk endokrinologi, K Öberg
Skogseid, Britt (author)
Uppsala universitet,Medicin,Onkologisk endokrinologi, K Öberg
Weber, C (author)
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 (creator_code:org_t)
1999
1999
English.
In: FEBS Letters. - 0014-5793 .- 1873-3468. ; 450:3, s. 210-216
  • Journal article (peer-reviewed)
Abstract Subject headings
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  • The expression of phospholipase C beta 3 (PLCB3) is low or absent in several neuroendocrine neoplasias. To investigate the role of PLCB3 in the neuroendocrine tumorigenesis, we transfected a PLCB3 construct to three neuroendocrine tumor cell lines with a low PLCB3 expression. The growth rate and tumorigenicity were assessed in vitro by [3H]thymidine incorporation and cell counting, in vivo, by xenografting to nude mice. In vitro, PLCB3 expressing clones showed a significant growth inhibition. The tumor weight was reduced for one of the two xenografted PLCB3-transfected cell lines and in both, a reduced number of proliferating (Ki-67 positive) cells was observed. This study implies an essential role for PLCB3 in the neuroendocrine tumorigenesis.

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