TY - JOUR
T1 - Telomerase reverse transcriptase promoter mutations in tumors originating from the adrenal gland and extra-adrenal paraganglia
AU - Papathomas, Thomas G.
AU - Oudijk, Lindsey
AU - Zwarthoff, Ellen C.
AU - Post, Edward
AU - Duijkers, Floor A.
AU - Van Noesel, Max M.
AU - Hofland, Leo J.
AU - Pollard, Patrick J.
AU - Maher, Eamonn R.
AU - Restuccia, David F.
AU - Feelders, Richard A.
AU - Franssen, Gaston J.H.
AU - Timmers, Henri J.
AU - Sleijfer, Stefan
AU - De Herder, Wouter W.
AU - De Krijger, Ronald R.
AU - Dinjens, Winand N.M.
AU - Korpershoek, Esther
PY - 2014/8
Y1 - 2014/8
N2 - Hotspot mutations in the promoter of the telomerase reverse transcriptase (TERT) gene have been recently reported in human cancers and proposed as a novel mechanism of telomerase activation. To explore TERT promoter mutations in tumors originating from the adrenal gland and extra-adrenal paraganglia, a set of 253 tumors (38 adrenocortical carcinomas (ACCs), 127 pheochromocytomas (PCCs), 18 extra-adrenal paragangliomas (ea PGLs), 37 head and neck PGLs (HN PGLs), and 33 peripheral neuroblastic tumors) was selected along with 16 human neuroblastoma (NBL) and two ACC cell lines to assess TERT promoter mutations by the Sanger sequencing method. All mutations detected were confirmed by a SNaPshot assay. Additionally, 36 gastrointestinal stromal tumors (GISTs) were added to explore an association between TERT promoter mutations and SDH deficiency. TERT promoter mutations were found in seven out of 289 tumors and in three out of 18 human cell lines; four C228T mutations in 38 ACCs (10.5%), two C228T mutations in 18 ea PGLs (11.1%), one C250T mutation in 36 GISTs (2.8%), and three C228T mutations in 16 human NBL cell lines (18.75%). No mutation was detected in PCCs, HN PGLs, neuroblastic tumors as well as ACC cell lines. TERT promoter mutations preferentially occurred in a SDH-deficient setting (P=0.01) being present in three out of 47 (6.4%) SDH-deficient tumors vs zero out of 171 (0%) SDH-intact tumors. We conclude that TERT promoter mutations occur in ACCs and ea PGLs. In addition, preliminary evidence indicates a potential association with the acquisition of TERT promoter mutations in SDH-deficient tumors.
AB - Hotspot mutations in the promoter of the telomerase reverse transcriptase (TERT) gene have been recently reported in human cancers and proposed as a novel mechanism of telomerase activation. To explore TERT promoter mutations in tumors originating from the adrenal gland and extra-adrenal paraganglia, a set of 253 tumors (38 adrenocortical carcinomas (ACCs), 127 pheochromocytomas (PCCs), 18 extra-adrenal paragangliomas (ea PGLs), 37 head and neck PGLs (HN PGLs), and 33 peripheral neuroblastic tumors) was selected along with 16 human neuroblastoma (NBL) and two ACC cell lines to assess TERT promoter mutations by the Sanger sequencing method. All mutations detected were confirmed by a SNaPshot assay. Additionally, 36 gastrointestinal stromal tumors (GISTs) were added to explore an association between TERT promoter mutations and SDH deficiency. TERT promoter mutations were found in seven out of 289 tumors and in three out of 18 human cell lines; four C228T mutations in 38 ACCs (10.5%), two C228T mutations in 18 ea PGLs (11.1%), one C250T mutation in 36 GISTs (2.8%), and three C228T mutations in 16 human NBL cell lines (18.75%). No mutation was detected in PCCs, HN PGLs, neuroblastic tumors as well as ACC cell lines. TERT promoter mutations preferentially occurred in a SDH-deficient setting (P=0.01) being present in three out of 47 (6.4%) SDH-deficient tumors vs zero out of 171 (0%) SDH-intact tumors. We conclude that TERT promoter mutations occur in ACCs and ea PGLs. In addition, preliminary evidence indicates a potential association with the acquisition of TERT promoter mutations in SDH-deficient tumors.
KW - Adrenocortical carcinomas
KW - Neuroblastomas
KW - Paragangliomas
KW - SDH deficiency
KW - Telomerase reverse transcriptase
KW - TERT promoter mutations
UR - http://www.scopus.com/inward/record.url?scp=84905982506&partnerID=8YFLogxK
UR - https://erc.bioscientifica.com/view/journals/erc/21/4/653.xml
U2 - 10.1530/ERC-13-0429
DO - 10.1530/ERC-13-0429
M3 - Article
C2 - 24951106
AN - SCOPUS:84905982506
SN - 1351-0088
VL - 21
SP - 653
EP - 661
JO - Endocrine-related Cancer
JF - Endocrine-related Cancer
IS - 4
ER -