Pheochromocytomas (PCC) are rare tumours of the adrenal medulla. These
tumours are derived from the neural crest, similar to paraganglioma
(PGL), which are located in the head and neck region and along the
sympathetic chain. Histomorphologically these tumours are identical,
although the pathogenesis of these two tumour types are mainly different
with a minor overlap between the tumours. In the last decades the genes
that are associated with the development of PCC and PGL have been
identified. Also, the recognition of germline mutations in patients with
PCC and PGL has been improved. In patients with PGL germline mutations
are identified in more than 50% of the patients and in PCC the
percentage of germline mutations is about 25%. Genes involved in the
development of PCC are: the RET oncogene and the tunoursupressorgenes
VHL, NF1, SDHB, SDHC en SDHD.
In the development of PGL the genes mostly involved the SDHB, SDHC en
SDHD genes, but also a small percentage is due to mutations in VHL
germline mutations. Very recently the SDHA-F2 gene is identified in a
subset of hereditary paraganglioma. No clinical of histological markers
are available to predict behaviour of PCC and PGL. Some clinical
correlation has been found; in patients with PCC and germline RET
mutations malignant behaviour is rare. This is in contrast to patients
with PCC and SDHB germline mutations that develop metastasis in a large
proportion of patients. In this thesis the molecular aberrations in
benign and malignant PCC are described and various techniques that can
distinguish a subset of PCC and PGL.http://repub.eur.nl/res/pub/20825/100611_Nederveen%2C%20Francien%20Heleen%20van.pdf
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