Molecular Characteristics of Neuroblastoma with Special Reference to Novel Prognostic Factors and Diagnostic Applications
Korja, Miikka (2009-08-15)
Molecular Characteristics of Neuroblastoma with Special Reference to Novel Prognostic Factors and Diagnostic Applications
(15.08.2009)
Turun yliopisto
Julkaisun pysyvä osoite on:
https://urn.fi/URN:ISBN:978-951-29-3989-3
https://urn.fi/URN:ISBN:978-951-29-3989-3
Kuvaus
Siirretty Doriasta
Tiivistelmä
Molecular Characteristics of Neuroblastoma with Special Reference to
Novel Prognostic Factors and Diagnostic Applications
Department of Medical Biochemistry and Genetics
Annales Universitatis Turkuensis, Medica-Odontologica, 2009, Turku, Finland
Painosalama Oy, Turku, Finland 2009
Background: Neuroblastoma, which is the most common and extensively
studied childhood solid cancer, shows a great clinical and biological
heterogeneity. Most of the neuroblastoma patients older than one year have
poor prognosis despite intensive therapies. The hallmark of neuroblastoma,
biological heterogeneity, has hindered the discovery of prognostic tumour
markers. At present, few molecular markers, such as MYCN oncogene status,
have been adopted into clinical practice.
Aims: The aim of the study was to improve the current prognostic
methodology of neuroblastoma, especially by taking cognizance of the
biological heterogeneity of neuroblastoma. Furthermore, unravelling novel
molecular characteristics which associate with neuroblastoma tumour
progression and cell differentiation was an additional objective.
Results: A new strictly defined selection of neuroblastoma tumour spots of
highest proliferation activity, hotspots, appeared to be representative and
reliable in an analysis of MYCN amplification status using a chromogenic in
situ hybridization technique (CISH). Based on the hotspot tumour tissue
microarray immunohistochemistry and high-resolution oligo-array-based
comparative genomic hybridization, which was integrated with gene expression
and in silico analysis of existing transcriptomics, a polysialylated neural cell
adhesion molecule (NCAM) and poorly characterized amplicon at 12q24.31
were discovered to associate with outcome. In addition, we found that a
previously considered new neuroblastoma treatment target, the mutated c-kit
receptor, was not mutated in neuroblastoma samples.
Conclusions: Our studies indicate polysialylated NCAM and 12q24.31
amplicon to be new molecular markers with important value in prognostic
evaluation of neuroblastoma. Moreover, the presented hotspot tumour tissue
microarray method together with the CISH technique of the MYCN oncogene
copy number is directly applicable to clinical use.
Key words: neuroblastoma, polysialic acid, neural cell adhesion molecule,
MYCN, c-kit, chromogenic in situ hybridization, hotspot
Novel Prognostic Factors and Diagnostic Applications
Department of Medical Biochemistry and Genetics
Annales Universitatis Turkuensis, Medica-Odontologica, 2009, Turku, Finland
Painosalama Oy, Turku, Finland 2009
Background: Neuroblastoma, which is the most common and extensively
studied childhood solid cancer, shows a great clinical and biological
heterogeneity. Most of the neuroblastoma patients older than one year have
poor prognosis despite intensive therapies. The hallmark of neuroblastoma,
biological heterogeneity, has hindered the discovery of prognostic tumour
markers. At present, few molecular markers, such as MYCN oncogene status,
have been adopted into clinical practice.
Aims: The aim of the study was to improve the current prognostic
methodology of neuroblastoma, especially by taking cognizance of the
biological heterogeneity of neuroblastoma. Furthermore, unravelling novel
molecular characteristics which associate with neuroblastoma tumour
progression and cell differentiation was an additional objective.
Results: A new strictly defined selection of neuroblastoma tumour spots of
highest proliferation activity, hotspots, appeared to be representative and
reliable in an analysis of MYCN amplification status using a chromogenic in
situ hybridization technique (CISH). Based on the hotspot tumour tissue
microarray immunohistochemistry and high-resolution oligo-array-based
comparative genomic hybridization, which was integrated with gene expression
and in silico analysis of existing transcriptomics, a polysialylated neural cell
adhesion molecule (NCAM) and poorly characterized amplicon at 12q24.31
were discovered to associate with outcome. In addition, we found that a
previously considered new neuroblastoma treatment target, the mutated c-kit
receptor, was not mutated in neuroblastoma samples.
Conclusions: Our studies indicate polysialylated NCAM and 12q24.31
amplicon to be new molecular markers with important value in prognostic
evaluation of neuroblastoma. Moreover, the presented hotspot tumour tissue
microarray method together with the CISH technique of the MYCN oncogene
copy number is directly applicable to clinical use.
Key words: neuroblastoma, polysialic acid, neural cell adhesion molecule,
MYCN, c-kit, chromogenic in situ hybridization, hotspot
Kokoelmat
- Väitöskirjat [2889]