Literature DB >> 7518353

CD44H expression by human neuroblastoma cells: relation to MYCN amplification and lineage differentiation.

N Gross1, C Beretta, G Peruisseau, D Jackson, D Simmons, D Beck.   

Abstract

The human CD44 cell surface glycoprotein has been involved in a variety of functions including lymphocyte homing, extracellular cell matrix attachment, and tumor metastasis. Due to the alternative splicing of the single gene, a large family of different variants or isoforms is generated. Several reports have indicated an up-regulation of CD44 variant (v) isoforms in malignant process, conferring metastatic potential to non-metastatic cells. Neuroblastoma is a tumor characterized by an aggressive and metastatic behavior in advanced stages with amplification of the MYCN protooncogene. In this report we show that the CD44 standard molecule is highly expressed in 100% of stage I-III, IVs neuroblastomas and ganglioneuromas but only in a subset of stage IV tumors. In contrast, no expression of CD44 was detected on MYCN amplified stage IV tumors, thus demonstrating a highly significant negative relationship between MYCN amplification and CD44 expression in neuroblastoma. The expression of CD44 on neuroblastoma cultured cell lines was not shown to be related to MYCN amplification but rather linked to the S-type, schwann/glial differentiation lineage. Immunochemical analysis of tumor samples with anti-CD44v3 and -v6 antibodies and Northern blot analysis of mRNA from cell lines with probes spanning exons 4-10 did not reveal any expression of splice variants on neuroblastomas of all stages and cell lines, thus ruling out a major role of these isoforms in neuroblastoma progression and metastasis.

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Year:  1994        PMID: 7518353

Source DB:  PubMed          Journal:  Cancer Res        ISSN: 0008-5472            Impact factor:   12.701


  20 in total

1.  Immunohistochemical detection of p140trkA and p75LNGFR neurotrophin receptors in neuroblastoma.

Authors:  C Dominici; M R Nicotra; S Alemà; C Bosman; M A Castello; A Donfrancesco; P Gallo; H McDowell; P G Natali
Journal:  J Neurooncol       Date:  1997-01       Impact factor: 4.130

Review 2.  The clinical significance of malfunction of the CD44 locus in malignancy.

Authors:  D Tarin; J Bolodeoku; S J Hatfill; T Sugino; A C Woodman; K Yoshida
Journal:  J Neurooncol       Date:  1995-12       Impact factor: 4.130

Review 3.  Expression of the CD44 adhesion molecule in tumours of the central and peripheral nervous system.

Authors:  G H Baltuch; N de Tribolet; E G Van Meir
Journal:  J Neurooncol       Date:  1995-12       Impact factor: 4.130

Review 4.  CD44 and the adhesion of neoplastic cells.

Authors:  Z Rudzki; S Jothy
Journal:  Mol Pathol       Date:  1997-04

5.  Oncogene-dependent expression of CD44 in Balb/c 3T3 derivatives: correlation with metastatic competence.

Authors:  P Kogerman; M S Sy; L A Culp
Journal:  Clin Exp Metastasis       Date:  1996-01       Impact factor: 5.150

6.  Progressive loss of CD44 gene expression in invasive bladder cancer.

Authors:  T Sugino; H Gorham; K Yoshida; J Bolodeoku; V Nargund; D Cranston; S Goodison; D Tarin
Journal:  Am J Pathol       Date:  1996-09       Impact factor: 4.307

7.  Neuroblastoma cells negative for CD44 possess tumor-initiating properties.

Authors:  Elena K Siapati; Erasmia Rouka; Despina Kyriakou; George Vassilopoulos
Journal:  Cell Oncol (Dordr)       Date:  2011-03-22       Impact factor: 6.730

8.  CD44 isoform expression in the diffuse neuroendocrine system. II. Benign and malignant tumors.

Authors:  P Komminoth; W K Seelentag; P Saremaslani; P U Heitz; J Roth
Journal:  Histochem Cell Biol       Date:  1996-12       Impact factor: 4.304

9.  Binding of gastrointestinal tumor cells to endothelial E- and P-selectin adhesion receptors leads to transient down-regulation of sLeX ligands in vitro.

Authors:  Horst Schuldes; Daniel Schleicher; Gottfried Mayer; Bernd H Markus; Jindrich Cinatl; Roman A Blaheta
Journal:  Int J Colorectal Dis       Date:  2003-02-01       Impact factor: 2.571

Review 10.  CD44: physiological expression of distinct isoforms as evidence for organ-specific metastasis formation.

Authors:  M Zöller
Journal:  J Mol Med (Berl)       Date:  1995-09       Impact factor: 4.599

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